WO2004073563A2 - In-situ formed intervertebral fusion device - Google Patents
In-situ formed intervertebral fusion device Download PDFInfo
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- WO2004073563A2 WO2004073563A2 PCT/US2004/004284 US2004004284W WO2004073563A2 WO 2004073563 A2 WO2004073563 A2 WO 2004073563A2 US 2004004284 W US2004004284 W US 2004004284W WO 2004073563 A2 WO2004073563 A2 WO 2004073563A2
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- A61L2300/64—Animal cells
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L2430/00—Materials or treatment for tissue regeneration
- A61L2430/02—Materials or treatment for tissue regeneration for reconstruction of bones; weight-bearing implants
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L2430/00—Materials or treatment for tissue regeneration
- A61L2430/38—Materials or treatment for tissue regeneration for reconstruction of the spine, vertebrae or intervertebral discs
Definitions
- a leading cause of lower back pain arises from lumbar intervertebral disc pathology, including rupture or degeneration ofthe disc. Radicular pain in the lower extremities may be caused by the compression of spinal nerve roots by a bulging disc. Additionally, lower back pain may be caused by collapse ofthe disc and the dysarthrosis of an unstable or degenerative vertebral facet joint.
- One proposed method of managing these problems is to remove the problematic disc and replace it with a porous device that restores disc height and allows for bone growth therethrough for the fusion ofthe adjacent vertebrae. These devices are commonly called “fusion devices.”
- Intervertebral body fusion devices typically must carry extremely high loads (on the order of 1-4 kN) for a period of several months, or until fusion occurs. Accordingly, a fusion device or bone graft substitute designed for promoting bony fusion at another location in the body (such as long bone fusion) may not be suitable for use as an intervertebral body fusion device.
- many bony fusion devices disclose the use of a gel such as a hydrogel as the structural carrier for an osteoinductive or an osteogeneic component.
- such gels typically do not posses the stiffness or mechanical strength found to be required for lumbar intervertebral fusion devices.
- a number of such prosthetic implants have been described for serving as an intervertebral disc, or nucleus pulposus, replacement, involving the delivery of prosthetic materials through a small diameter cannula no larger than is needed to perform an adequate discectomy. Therefore, the injectable prosthetic devices are typically delivered in a first fluid form and then harden to a second form once inside the disc space to span the disc space height and preferably fill the disc space following discectomy.
- the requirements for a bone fusion system are very different from those of injectable prosthetic devices.
- an intervertebral strut injectable into the disc space that can create or maintain a preferred spatial relationship between adjacent vertebral body endplates (curvature and distraction) and comprises an osteogenic component to promote bony fusion between the two adjacent vertebra.
- the present invention relates to a device for intervertebral spinal fusion and method of making thereof.
- the present invention is an orthopedic device for implanting between adjacent vertebrae comprising a generally arcuate balloon and a hardenable material within said balloon.
- the present invention is an intervertebral spinal fusion device comprising at least one arcuate inflatable balloon whereby at least partially filling the balloon between two adjacent vertebrae at least partially restores a natural angle between the adjacent vertebrae, and wherein said arcuate balloon contains a load-bearing component within a lumen defined by the balloon.
- the present invention is an intervertebral spinal fusion device comprising a anterior frame having an upper inflatable rim and a lower inflatable rim, and a rigid inflatable posterior frame attached to the upper and lower inflatable rims of the anterior frame.
- the anterior frame is detachably connected to the first fluid communication means.
- the posterior frame is detachably connected to the second fluid communication means.
- the present invention is a method of implanting an intervertebral spinal fusion device, comprising the steps of (a) performing a discectomy while preserving an outer annular shell; (b) inserting an inflatable device that includes a deflated arcuate balloon into an intervertebral space; (c) directing an osteobiologic omponent into the deflated arcuate balloon in an amount sufficient to inflate the balloon and distract the disc space.
- the present invention is a method of implanting an intervertebral spinal fusion device, comprising the steps of (a) inserting an inflatable device tlirough a cannula into an intervertebral space, said inflatable device including an arcuate balloon connected to at least one fluid communication means, wherein said inflatable device upon expansion between two adjacent vertebrae at least partially restores a natural angle between the adjacent vertebrae; (b) orienting said inflatable device so that upon expansion a natural angle between vertebrae will be at least partially restored; (c) directing a load-bearing component into the inflatable device through the fluid communication means.
- the present invention is a method of at least partially restoring a natural angle between two adjacent vertebrae, comprising the steps of (a) inserting an inflatable device through a cannula into an intervertebral space; (b) orienting said inflatable device so that upon expansion of the device a natural angle between vertebrae will be at least partially restored; and (c) expanding said inflatable device by directing a load-bearing component into said inflatable device.
- the present invention is a method of delivering an osteobiologic material comprising (a) inserting an inflatable device into an intervertebral space wherein at least a portion of the device upon expansion has a substantially toroidal shape thereby forming an open cavity defined by an outer surface of the toroidal shape and having an axial dimension and a radial dimension; (b) orienting at least a portion ofthe device so that so that the axial dimension ofthe open cavity is substantially parallel to a major axis of a spinal column of a patient in which the device has been implanted; (b) inflating said inflatable device by directing a load-bearing component into said inflatable device; (c) directing an osteobiologic material into the open cavity, said material including at least one water-soluble material; (d) directing an aqueous fluid into into the open cavity defined by the inflated device thereby dissolving at least one said water-soluble material, and fo ⁇ riing a porous matrix; and (e) delivering additional osteobiologic component into
- the present invention is a pharmaceutical composition
- a pharmaceutically acceptable carrier or diluent and (a) at least one polymer flowable between 38 °C and 45 °C selected from the group consisting of homopolymers of poly(e-caprolactone), poly(p-dioxanone), or poly(trimethylene carbonate) or copolymers or mixtures thereof, or copolyesters of p-dioxanone or trimethylene carbonate and glycolide or lactide or mixtures thereof, and in particular, copolymers of p-dioxanone/glycolide, p-dioxanone/lactide, trimethylene carbonate/glycolide and trimethylene carbonate/lactide, or copolyesters of .
- epsilon -caprolactone and glycolide or mixtures thereof, or mixtures of homopolymers of e -caprolactone and lactide; and (b) at least one growth factor resistant to denaturing at at least about 45 °C selected from the group consisting of bone morphogenetic proteins.
- the present invention is an intervertebral fusion device comprising an in-situ formed osteobiologic component comprising (a) a matrix having an internal surface defining an open porosity suitable for bone growth therethrough, and (b) an osteogenic component located within the open porosity.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space, comprising (a) a strut having a upper surface for bearing against the upper endplate and a lower surface for bearing against the lower endplate, and (b) an in-situ formed osteobiologic component.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space, comprising a strut comprising (a) an upper surface for bearing against the upper endplate, (b) a lower surface for bearing against the lower endplate, and (c) an injectable load bearing composition disposed between the upper and lower surfaces.
- the present invention is an intervertebral fusion device comprising a matrix having an internal surface defining an open porosity suitable for bone growth therethrough, wherein the matrix is formed by a plurality of in-situ bonded beads.
- the present invention is an intervertebral fusion device comprising a strut comprising (a) a first component comprising (i) a lower bearing surface adapted for bearing against a lower vertebral endplate, and (ii) an upper surface comprising a leading end, an angled middle portion and a trailing end; and (b) a second component comprising (i) an upper bearing surface adapted for bearing against an upper vertebral endplate and (ii) an upper surface comprising a leading end, an angled middle portion and a trailing end.
- the angled portion ofthe first component mates with the angled portion ofthe second component.
- the present invention is a kit for providing interbody fusion across an intervertebral disc space, comprising (a) a cannula defining an inner diameter; (b) a hardenable material capable of supporting intervertebral load; and (c) a flowable osteobiologic composition.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space, comprising (a) a strut having a upper surface for bearing against an upper endplate and a lower surface for bearing against a lower endplate, the upper surface and lower surface defining a height therebetween, and (b) an in-situ formed osteobiologic component.
- the height ofthe strut is no greater than the height ofthe disc space.
- the present invention is a method of providing interbody fusion across an intervertebral disc space, comprising the steps of (a) providing a cannula defining an inner diameter; (b) moving a load bearing composition through the cannula and into the disc space to form a in-situ formed load bearing strut; and (c) moving an osteobiologic composition through the cannula and into the disc space to form an in-situ formed osteobiologic composition.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space, comprising a strut comprising (a) an upper surface for bearing against the upper endplate and (b) a lower surface for bearing against the lower endplate.
- the strut comprises an in-situ formed load bearing composition.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space, comprising a strut comprising (a) an upper surface for bearing against the upper endplate, (b) a lower surface for bearing against the lower endplate, and (c) an in-situ formed load bearing composition disposed between the upper and lower surfaces.
- the present invention is an intervertebral fusion device comprising (a) a strut have a shape memory and comprising (i) an upper surface for bearing against the upper endplate, (ii) a lower surface for bearing against the lower endplate, and (b) an in-situ formed osteobiologic component.
- the present invention is an intervertebral fusion device comprising (a) a strut comprising an upper surface for bearing against the upper endplate and a lower surface for bearing against the lower endplate, and (b) an in-situ formed osteobiologic component comprising a matrix component having an internal surface defining a scaffold having open porosity suitable for bone growth therethrough, and an osteogenic component located within the open porosity.
- the present invention is an intervertebral fusion device comprising a strut comprising an upper surface for bearing against the upper endplate and a lower surface for bearing against the lower endplate, and an in-situ formed osteobiologic component comprising an injectable matrix component, an an osteoinductve component embedded within the matrix.
- the present invention is an intervertebral fusion device comprising a strut comprising an upper surface for bearing against the upper endplate a lower surface for bearing against the lower endplate, and an in-situ formed osteobiologic component comprising an injectable matrix component, and a porogen embedded within the matrix.
- the present invention is an intervertebral fusion device comprising a strut comprising an upper surface for bearing against the upper endplate, a lower surface for bearing against the lower endplate, and an in-situ fonned osteobiologic component comprising an expandable device defining a cavity, and an injectable osteobiologic composition located witiiin the cavity.
- the present invention is an intervertebral fusion device comprising a strut comprising an expandable device having a cavity, an upper surface for bearing against the upper endplate, a lower surface for bearing against the lower endplate, and an inner wall defining a through hole and an injectable load bearing composition located within the cavity, and an osteobiologic component located in the throughhole.
- the present invention is an intervertebral fusion device comprising a strut comprising an upper surface for bearing against the upper endplate, and a lower surface for bearing against the lower endplate; and an in-situ formed osteobiologic component comprising an injectable, matrix component essentially free of monomer.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space, comprising a strut comprising (a) an upper surface for bearing against the upper endplate, (b) a lower surface for bearing against the lower endplate, and (c) an in-situ formed load bearing composition disposed between the upper and lower surfaces and made of a material comprising a cross-linked resorbable polymer.
- the advantages ofthe present invention are numerous.
- One advantage is that the present invention makes possible minimally invasive surgical procedures to restore a natural angle and increase disc height between two adjacent vertebrae .
- the same device used used to create distraction/lordosis can function as the intervertebral implant needed to maintain height and natural angle.
- Another advantage is that the present invention makes possible a minimally invasive procedure to create in situ a structural scaffold filled with osteoinductive materials.
- FIG. 1 is a plot of strength over time of a resorbable polymer and bone growth.
- FIGs. 2 (a) through 2 (e) are schematic representations of preferred embodiments of a semicircular, circular, bilateral and generally crescent, arcuate, or toroidal shapes ofthe device ofthe present invention.
- FIGs. 2 (f) and 2 (g) show a perspective and a top view, respectively, of a preferred embodiment of a device ofthe present invention.
- FIG. 3 (a) and FIG. 3 (b) show a perspective and a top view, respectively, of a preferred method ofthe introduction of a cannula into the disc space.
- FIG. 4 (a) and FIG. 4 (b) show a perspective and a top view, respectively, of a preferred method ofthe deployment of an inflatable device into the disc space through the cannula.
- FIG. 5 (a) and FIG. 5 (b) show a perspective and a top view, respectively, of an embodiment o the present invention wherein the device comprises a generally toroidal balloon and the osteobiologic component is injected into an open cavity defined by the outer surface ofthe generally toroidal balloon.
- FIG. 6 (a) and FIG. 6 (b) show a perspective and a top view, respectively, of an embodiment ofthe present invention comprising more than one balloon.
- FIG. 7 (a) and FIG. 7 (b) show a perspective and a top view, respectively, of another embodiment ofthe present invention comprising more than one balloon.
- FIG. 8 (a) and FIG. 8 (b) show an embodiments ofthe present invention comprising an arcuate inflatable balloon with reinforced walls.
- FIGs. 9 (a) through (d) show an embodiment of an inflatable device and a method of inserting an inflatable device ofthe present invention into the disc space, wherein a pair of semi-circular flexible members is used for guiding the device.
- FIGs. 10 (a) and 10 (b) represent plan and lateral views, respectively, of an embodiment of an inflatable device ofthe invention whereby a pair of semi-circular flexible upper and lower wall components, which can be used for guiding the device, are joined by an inflatable balloon.
- FIGs. 11 (a) and (b) show an embodiment ofthe present invention wherein the device comprises four semi-circular flexible components for guiding the inflatable device into the disc space.
- FIGs. 12 (a) and (b) show another embodiment of device ofthe present invention that includes guiding members.
- FIGs.13 (a) through (d) shows a preferred embodiment ofthe method ofthe present invention.
- FIG. 13 (a) and FIG. 13 (b) show inserting a cannula into an intervertebral space, followed by inserting an inflatable balloon of a generally toroidal shape into an intervertebral space through the cannula. The balloon is expanded by directing a load-bearing component into said balloon.
- FIG. 13 (c) shows injecting an osteobiologic component comprising a water-soluble component into an open cavity, defined by the outer surface ofthe balloon, and
- FIG. 13 (d) shows dissolving the water-soluble component.
- FIGs. 14 (a) and (b) show a top and a lateral view, respectively, of another embodiment of a device ofthe present invention employing a ramp.
- FIG. 14 (c) is a cross section ofthe device of FIGs. 14 (a) and (b).
- FIG. 14 (d) is a perspective view ofthe device of FIGs. 14 (a) - (c).
- FIG. 15 shows one embodiment of a method of deployment of the device of
- FIG. 16 shows another embodiment of a mthod of deployment ofthe device of FIGs. 14 (a) - (d).
- FIGs.17 (a) and (b) show a particularly preferred embodiment ofthe device ofthe present invention in collapsed and expanded configuration, respectively.
- the present invention relates to a vertebral fusion device for simultaneously distracting two adjacent vertebral bodies and delivering a flowable material into a disk space.
- vertebral fusion refers to a medical procedure that results in maintaining separation between vertebrae.
- vertebral fusion provides for bony ingrowth that fixes two adjacent vertebrae in a desired, for example, distracted and/or angulated, position.
- a natural angle between two adjacent vertebral plates is replicated by fusing the two adjacent vertebrae.
- the "natural angle” refers either to natural lordosis or to natural kyphosis.
- the angle can be positive, negative or zero (i.e., when the opposing surfaces ofthe adjacent vertebrae are essntially coplanar).
- a natural lordosis is replicated or restored.
- natural lordosis refers to a natural angle between two adjacent vertebral plates within the lumbar or cervical spine segments wherein the distance between the anterior portions of the two adj acent vertebral plates is not smaller than the distance between the posterior portions ofthe two adjacent vertebral plates.
- a natural kyphosis is replicated or restored.
- natural kyphosis refers to a natural angle between two adjacent vertebral plates within the thoracic spine segment wherein the distance between the anterior portions ofthe two adjacent vertebral plates is not geater than the distance between the posterior portions ofthe two adjacent vertebral plates.
- a fusion means maintains the separation between the vertebrae.
- the fusion means at least partially restore the natural function of nucleus pulposis by permitting relative freedom of movement while substantially maintaining the separation between the vertebrae.
- the components ofthe device comprise at least one member selected from the group consisting of a load-bearing component and an osteobiologic component. Preferably, both components are used.
- load-bearing component includes osteobiologic component.
- load- bearing component or material refers to any material capable of supporting vertebrae in distracted position.
- the load-bearing component can include a hardenable material or a noncompressible fluid contained within an inflatable balloon.
- strut refers to any part, portion or component ofthe device, including a flowable material, that either alone or in combination with other parts, portions or components ofthe device is capable of supporting vertebrae in distracted position.
- a strut examples include a hardened flowable material, a balloon with rigid walls and an inflatable balloon or bag filled with a hardenable material or a noncompressible fluid.
- the purpose ofthe strut is to bear the high spinal loads.
- the strut can be used to increase the disc space height and/or at least partially restore or create natural curvature ofthe spinal region being fused. Increasing disc height is often critical for decompressing nerve roots and restoring or creating healthy spine curvature is important for preventing accelerated degeneration of adjacent intervertebral discs.
- arcuate refers to a shape having curvature roughly corresponding to the perimeter of a vertebral endplate, but does not include enclosed rings or generally annular structures.
- the "osteobiologic" component or material refers to any material that can induce and/or support existing or new bone growth.
- the load-bearing material includes osteobiologic material.
- a material comprising bone growth factors or mesynchemal stem cells is an osteobiologic component.
- Osteobiologic component can further include either one or both an osteoinductive component and an osteoconductive component.
- the "osteoinductive” component or material refers to any material that can induce bone growth.
- osteoinductive components includes signal molecules required to induce the osteoprogenitor cells to form new bone. Examples of osteoinductive components are bone morphogenetic proteins (BMP's), growth differentiation factors (GDF's) and transforming growth factors (TGF).
- BMP's bone morphogenetic proteins
- GDF's growth differentiation factors
- TGF transforming growth factors
- the "osteoconductive" component or material refers to any material that can provide support for bone growth subsequent to induction.
- osteoconductive components include natural collagen-based materials including bone, and synthetic porous resorbable polymers and ceramics.
- the present invention relates to in situ formed intervertebral fusion devices.
- the components ofthe in situ formed device can be delivered percutaneously (e.g., through a cannula having a diameter of no more than 5 mm, preferably no more than 2 mm).
- the precursor components ofthe in-situ formed device can also be delivered in cannulae of much larger dimension (such as up to 18 mm, or through a Craig needle).
- the components ofthe in-situ formed device are delivered into the disc space in the form of injectable compositions.
- the term “in situ formed” refers to any material that is delivered into the disc space in a first form and takes on a different form after placed in the disc space.
- “in situ formation” includes delivering a viscous fluid into the disc space and hardening that fluid.
- “in situ formation” includes delivering discrete components into the disc space and bonding (preferably, heat bonding or by reaction) together those components.
- “in situ formation” includes delivering discrete components into an opening in an inflatable device located in the disc space and preventing their escape from the inflatable device by closing off the opening ofthe inflatable device.
- “in situ formation” includes delivering discrete components into the disc space and assembling together those components within the disc space.
- In situ formation excludes simply packing particles such as autograft or allograft particles into the disc space, as well as simply delivering a gel into the disc space.
- FIG. 1 the hypothetical strength profiles of a conventional resorbable implant (dotted line) and ofthe bone that replaces the implant (solid line) are provided.
- the strength ofthe system is defined as the lesser ofthe strength ofthe resorbable implant and the strength ofthe healing bone. It then follows that between the time ofthe surgical procedure (To) and the time for complete bone healing to take place (Tp), the load applied to the system must never be above the strength, of the system at point C (shown as Sc)- It is known in the art that the maximum in vivo average daily living load on the human lumbar spine is approximately 4,000 N. Assuming that this is the maximum load to be experienced by the system, then the system strength should not fall below 4,000 N.
- the strut can be made relatively strong (e.g., capable of supporting about 15 1 ⁇ N in axial compression), even when the load applied to the system is relatively high, the strength ofthe system will still be sufficient to support the disc space and fusion will occur. Once sufficient bone growth through the osteobiologic component occurs, the strut may degrade without endangering support ofthe disc space.
- the strut supports the disc space while the osteobiologic composition grows bone.
- the strut ofthe present invention acts in a manner similar to the cortical rim of a vertebral body. Desirable features for the load bearing composition ofthe strut are as follows: a) sufficient strength to bear the typical loads borne by vertebral bodies; b) stiffness similar to that of cortical bone (or, in relatively thick embodiments, cortico-cancellous bone) ; c) degradation resistance (e.g., capable of bearing at least 15 MPa, preferably at least 25 MPa) for at least one year, preferably at least 18 months; d) resorbability.
- the present invention is an intervertebral spinal fusion device comprising a resorbable load-bearing material wherein the combination ofthe resorbable load-bearing material and the new bone growth provides a load-carrying capacity that is at least sufficient to support spinal load.
- the load-bearing material includes or is supplemented by an osteobiologic component.
- the present invention is a method of making an intervertebral fusion device comprising selecting a resorbable load- bearing material wherein the combination ofthe resorbable load-bearing material and the new bone growth provides a load-carrying capacity that is at least sufficient to support spinal load.
- the strut should have a size sufficient to provide a footprint covering between about 3 % and about 40 % ofthe area ofthe corresponding vertebral endplate.
- the strut foot covers between about 10% and about 30%, more preferably between about 10% and about 20% ofthe corresponding vertebral endplate.
- the osteobiologic component contains at least one of a) a growth factor and b) an osteogenic component, e.g. a source of cells (such as stem cells), it is believed that the strut footprint can be in the range of about 10%) to about 20% ofthe disc space. This is because it is believed that these additives sufficiently shorten the time to fusion so that the danger of strut subsidence is sufficiently low.
- the osteobiologic component contains both a) a growth factor and b) stem cells, it is believed that the strut footprint can be in the range of about 5% to about 10% ofthe disc space.
- osteobiologic component with both a) a growth factor and b) stem cells provides further desirable design options.
- These additives may also reduce or eliminate the need for posterior or supplemental fixation.
- posterior fixation is generally thought to be highly desirable to achieve a fusion success in the interbody space.
- the provision of effective amounts of such additives can increase the speed for fusion so as to render superfluous the posterior or supplemental fixation, and patients would no longer need to endure a more invasive pedicle screw procedure to apply the stability needed for fusion.
- the device can comprise a balloon of semicircular, circular, bilateral (comprising more than one balloon) and generally toroidal shape.
- Preferred embodiments and positions of a device ofthe present invention on an endplate 8 of a vertebra 10 are shown in FIGs. 2 (a) through (e).
- this shape allows the balloon 12 to essentially cover at least the anterior periphery 14 ofthe corresponding vertebral endplate 8, and thereby bear a substantial portion ofthe spinal load.
- This shape further allows the surgeon to first place the device in place and then fill the remaining portion ofthe disc space with, for example, an osteobiologic component.
- the balloon 12 has a quasi-circular shape.
- This device has the advantage of providing even more of a load-bearing footprint than the embodiment of FIG. 2 (a), and also substantially prevents unwanted leakage ofthe osetobiologic component during subsequent filling of an open cavity defined by an outer surface ofthe balloon.
- the device comprises two balloons 12 that can be used to support the vertebral load.
- the use of two balloons allows a surgeon to evenly support the load on each side ofthe endplate 8.
- the balloon 12 has a generally toroidal (“banana”) shape.
- the banana shape allows the surgeon to put in place a single device preferably on the anterior half 14 ofthe disc space.
- the strut has the footprint of a banana cage such as that described in Attorney Docket #DEP 5012, "Novel Banana Cage", filed December 31, 2002, US Serial No. 10/334599, the specification of which is incorporated by reference in its entirety.
- the strut 12 is introduced translaterally so as to form a single ramp stretching essentially transversely across the endplate 8.
- This design in advantageous when used in a posterolateral approach of surgery, as this approach takes advantage ofthe fact that the muscle planes in the vicinity ofthe approach allow the implant to be delivered in a less invasive manner.
- the device 12 ofthe present invention has a substantially semiannular footprint.
- the device 12 is placed on the anterior portion ofthe endplate 8 of a vertebra 10 so that height D of a anterior portion ofthe device is equal or greater than height h of a posterior portion ofthe device 12.
- the device 12 defines an internal radius r an external radius r e and thickness t.
- r ⁇ is approximately about 22 mm
- r e is approximately about 25 mm
- t is approximately about 3 mm.
- the height ofthe strut is at least 90%, and preferably at least equal to, the height ofthe natural disc space. This allows the surgeon to distract the disc space and restore at least a portion ofthe disc height, h some embodiments, the height ofthe strut is greater than that ofthe natural disc space.
- distraction will refer to the separation of joint surfaces to a desired extent, without rupture of their binding ligaments and without displacement.
- Distraction can be accomplished by any suitable means, for example mechanical or hydrostatic means.
- Mechanical means can include, for instance, attaching hooks or jacks to the bony endplates and using those hooks or jacks to separate the bones.
- the surgeon can employ external traction.
- an in-situ foaming material is used as a distraction device.
- Other means include, for example, hydrostatic means, e.g., by pressurized injection ofthe biomaterial itself. By the use of distraction, the disc space can be sufficiently re- established to achieve any desired final dimensions and position.
- the means used to accomplish distraction also serves the purpose of forming one or more barriers (e.g., balloons) for the flowable load bearing strut material.
- the disc space can be distracted prior to and/or during either a discectomy itself and/or delivery of a flowable biomaterial.
- a constricted disc space is generally on the order of 3 to 4 mm in height.
- Suitable distraction means are capable of providing on the order of about 3 atmospheres to about 4 atmospheres, (or on the order of about 40 psi to about 60 psi) in order to distract that space to on the order of 8 to 12 mm in height.
- the strut has a wedged shape so that the height ofthe anterior portion ofthe expanded device is greater than the height ofthe posterior portion ofthe expanded device. This allows the surgeon to restore lordosis when the interbody fusion device is used in either the lumbar or cervical regions ofthe spine.
- the wedged shape produces an angle of between 5 and 20 degrees, more preferably between 5 and 15 degrees.
- the strut has a wedged shape so that the height ofthe anterior portion ofthe expanded device is smaller than the height ofthe posterior portion ofthe expanded device. This allows the surgeon to restore kyphosis when the interbody fusion device is used in thoracic regions ofthe spine.
- the wedged shape produces an angle of between 5 and 20 degrees, more preferably between 5 and 15 degrees.
- the height ofthe medial portion ofthe strut is greater than the height ofthe lateral portion ofthe expanded device. This geometry more closely mimics the natural doming ofthe disc space.
- a "custom" implant formed to the anatomy ofthe patient's endplates.
- the provision of a conformable implant may provide a faster and more consistent fusion.
- the annulus fibrosus can itself serve as a suitable mold for the delivery and solidification of either the flowable load-bearing material (in one embodiment) or the osteobiologic component (in another embodiment). Free injection may optimize the extent to which the injectable device conforms to the contour ofthe disc space, thereby enhancing resistance to retropulsion.
- the interior surface ofthe annulus fibrosus can be treated or covered with a suitable material in order to enhance its integrity and use as a mold.
- at least one ofthe flowable materials is delivered into an inflatable device (such as a balloon) previously placed in the disc space.
- the load bearing composition is delivered into an inflatable device (such as a balloon) previously placed in the disc space.
- a cannula 18, having an inner diameter of no more than 6 mm is inserted into the disc space.
- the inflatable device 12 is deployed tlirough the exit opening ofthe cannula 18 and the flowable load bearing composition is introduced into the inflatable device at a pressure and volume suitable to expand the inflatable device and distract the disc space.
- the fixed shape ofthe expanded device allows the surgeon to predetermine the shape ofthe flowable material and simply fill the device with the flowable material.
- the device substantially prevents unwanted flow ofthe material.
- the prevention of unwanted flow desirably prevents the material from damaging important surrounding structures such as the spinal cord, aorta and vena cava.
- the inflatable device can be tailored to fill any portion ofthe disc space. Further, the present inventors believe that inclusion of an inflatable balloon in a strut can assure that the opposing trends of degradation of bioabsorbable materials and new bone growth will result in fusion ofthe vertebrae in a position approximating the natural angle between two adjacent vertebrae.
- the balloon will effectively shield the load-bearing composition from water during the initial stages of fusion and so delay the onset of hydrolysis and degradation ofthe load-bearing material.
- the balloon begins to degrade within about 1-2 months after fusion ofthe osteobiologic composition, thereby allowing the load-bearing material it contains to slowly degrade and grow bone.
- the distraction ofthe disc space is accomplished by an inflatable, yet rigid, balloon or bladder. The balloon can be delivered in deflated form to the interior ofthe annulus and there inflated in order to distract the disc space and provide a region for the delivery of biomaterial.
- the balloon is preferably of sufficient strength and of suitable dimensions to distract the space to a desired extent and to maintain the space in distracted position for a period of time sufficient for the biomaterial to be delivered and, optionally, to harden.
- One ofthe primary functions ofthe balloon is to influence or control the shape ofthe hardenable material, following injection therein.
- the implantable balloon is not normally required to restrain pressure over an extended period of time. Thus, a greater design flexibility may be permitted, as compared to conventional angioplasty or other dilatation balloons.
- the balloon may be porous, either for drug delivery as has been discussed, or to permit osteoincorporation and/or bony ingrowth.
- a method for fusing an intervertebral disc space comprising the steps of: a) using microsurgical techniques to perform a discectomy while preserving an outer annular shell; b) inserting a deflated balloon into the disc space; c) injecting a flowable load bearing composition into the deflated balloon (preferably, in an amount sufficient to distract the disc space), and d) solidifying the flowable strut material.
- a method for fusing an intervertebral disc space comprising the steps of: a) using microsurgical techniques to perform a discectomy while preserving an outer annular shell, b) inserting a deflated balloon having peripheral struts into the disc space, c) injecting an osteobiologic component into the deflated balloon in an amount sufficient to inflate the balloon and distract the disc space with the strut component of the balloon.
- the space is distracted by the use of one or more suitable insertable or inflatable devices, e.g., in the form of inflatable balloons. When inflated, such balloons provide rigid walls (e.g., fiber supported) that are sufficiently strong to distract the space.
- an inflatable device providing sufficient strength and dimensions can be prepared using conventional materials.
- the uninflated balloon can be delivered to the center ofthe annular shell, and there inflated to expand the annular shell and in turn, distract the space.
- the uninflated balloon can be delivered to the anterior rim of the annular shell, and there inflated to provide a cavity for the injection ofthe load bearing flowable material.
- the load bearing composition is injected in an amount sufficient to distract the space.
- the inflatable device can be delivered to the disc space by any suitable means, e.g., in deflated form retained within or upon the end of a rigid or semi-rigid rod.
- a suitable gas e.g., nitrogen or carbon dioxide
- the flowable load- bearing material can be delivered through the rod in order to inflate the balloon in situ, in a substantially radial or longitudinal direction.
- beads ofthe load bearing strut material are simply packed into the balloon. The fact that the balloon is properly placed can be confirmed by the use of ancillary means, such as using a C-arm, or by self-effecting means embodied within the balloon itself or its delivery apparatus.
- an inflatable device in one preferred balloon delivery system ofthe present invention there is provided an inflatable device, a motor drive unit, with a remote controller, associated tube sets, a nonscope inflow delivery cannula having independent fluid dynamics pressure and flow rate adjustments, attachments for the flush, vacuum, waste canister, and overflow jars.
- Suitable materials for preparing balloons ofthe present invention may include those that are presently used for such purposes as balloon angioplasty. Suitable materials provide an optimal combination of such properties as compliance, biostability and biocompatability, and mechanical characteristics such as elasticity and strength. Balloons can be provided in any suitable form, including those having a plurality of layers and those having a plurality of compartments when expanded.
- a useful balloon apparatus will include the balloon itself, together with a delivery catheter (optionally having a plurality of lumen extending longitudinally therewith), and fluid or gas pressure means.
- suitable materials for making balloons include, but are not limited to, polyolefin copolymers, polyethylene, polycarbonate, polyethylene terephthalate and etfier-ketone polymers such as poly(etheretherketone).
- polyolefin copolymers polyethylene, polycarbonate, polyethylene terephthalate and etfier-ketone polymers such as poly(etheretherketone).
- Such polymeric materials can be used in either unsupported form, or in supported form, e.g., by the integration of DacronTM or other fibers.
- the materials of construction ofthe balloon are resistant to softening or melting at a temperature of at least 80 °C, preferably at least 100 °C, more preferably at least 250 °C.
- the balloon (or balloon-like structure) may be made out of any of a wide variety of woven or nonwoven fibers, fabrics, metal mesh such as woven or braided wires, and carbon. Biocompatible fabrics or sheet material such as ePTFE and DacronTM may also be used. Balloons can also take several forms, depending on the manner in which the biomaterial is to be delivered and cured. A single, thin walled balloon can be used, for instance, to contact and form a barrier along the interior surface ofthe remaining annular material. Once positioned, the flowable load bearing component can be delivered and solidified within the balloon to serve as a load bearing strut ofthe present invention. In such an embodiment, the balloon is preferably of a type that will allow it to remain in position, without undue detrimental effect, between the annular material and the solidified load-bearing component.
- a balloon can be provided that fills essentially only the central portion ofthe disc space.
- the balloon can be, for instance, in the shape of a cylinder.
- Such a balloon can be provided such that its upper and lower walls can be positioned to contact the opposing vertebral bodies, and its side walls will provide sufficient strength to cause distraction ofthe space upon inflation.
- the load-bearing component is delivered to the perimeter ofthe annular space, i.e., the space between the annular material and the balloon, and there solidified.
- the balloon can be gradually deflated as additional biomaterial is inserted into the space. Then, once the load bearing material is stably positioned, the osteobiologic component is introduced into the balloon, thereby filling the balloon.
- the balloon has metallic wires or other imageable means incorporated into it. Any material that can be seen under fluoroscopy would be acceptable. Potential materials include any metal, metal alloys, or ceramics that could be combined with a polymer. The material can be in the fonn of wires, a mesh, or particles incorporated into the balloon or on its surface.
- the balloon has an inner surface that is chemically active so as to bond with the balloon filler as it polymerizes.
- a chemical "bond” is said to exist between two atoms or groups of atoms when the forces acting between them are strong enough to lead to the formation of an aggregate with sufficient stability to be regarded as an independent species.
- chemically active means capable of forming a chemical bond.
- the surface is chemically modified by means such as plasma polymerization. In this case, the balloon is placed in a vacuum chamber and plasma containing a small molecule (an amine for example) is created. The balloon surface is bombarded by the small molecule and the small molecule is chemically attached to its surface.
- the balloon's surface with its amine groups can then react with the polymer that is injected into the balloon (i.e., an epoxy), forming a device that would have greater fatigue properties since the "composite" of balloon and balloon filler are chemically bonded to one another.
- the desired quantities ofthe load-bearing and osteobiologic components of the present invention are delivered by minimally invasive means to the prepared site. Prior to delivery, these components can be stored in suitable storage containers, e.g., sterile, teflon-lined metal canisters.
- the flowable components can be delivered, as with a pump, from a storage canister to the delivery cannula on demand.
- the components can be delivered in the form of a single composition, or can be delivered in the form of a plurality of components or ingredients.
- the inflatable device can be filled with a viscous material that later solidifies to form the strut or osteobiologic component.
- the viscous material can be a heated polymer (such as a composition containing polycaprolactone), or polymer precursor components (such as the photopolymerizable anhydrides disclosed by A.K. Burkoth, Biomaterials (2000) 21 :2395-2404, the entire teachings of which are incorporated herein by reference).
- a flowable load bearing composition such as polycaprolactone
- heated to a temperature yielding a viscosity in the range of from about 100 to about 500 cps is injected into the balloon under pressure such as by using a pump and pressure within the range of from about 4 ATM to about 10 ATM or more depending upon viscosity, balloon strength and other design considerations.
- the pump is run for a sufficient duration and under a sufficient pressure to ensure that the polycaprolactone wets all ofthe p-dioxanone fibers. This may range from about 10 minutes or more to about an hour, and, in one application where the pump was run at about 5 ATM pressure, requires at least about 1 hour.
- Specific method parameters may be optimized depending upon the viscosity ofthe polycaprolactone, infusion pressure, infusion flow rate, density ofthe packed fibers, and other variables as will be apparent to those of skill in the art in view ofthe disclosure herein.
- the inflatable device upon expansion, forms an upper surface having a first plurality of teeth projecting outwards from the upper surface. Upon expansion ofthe device, these teeth will project in the direction ofthe upper endplate and, upon complete expansion ofthe device, will engage the endplate to from a secure interlock with the endplate and resist retropulsion.
- the teeth are made of a stiff resorbable material, such as polyetheretherketone (PEEK).
- PEEK polyetheretherketone
- the teeth have a height of between 0.5 and 1.5 mm, and have a triangular cross-section.
- the inflatable device upon expansion, forms an upper surface formed of a material having a high coefficient of friction.
- the high coefficient of friction ofthe upper and lower surfaces will case a drag upon any movement ofthe upper surface and therefore keep the device in place and resist retropulsion.
- the upper and lower surfaces ofthe inflatable device are made from a material selected from a group consisting of polyether block copolymer (PEBAX), ABS (acrylonitrile butadiene styrene); ANS (acrylonitrile styrene); Delrin ® ; PVC (polyvinyl chloride); PEN (polyethylene napthalate); PBT (polybutylene terephthalate); polycarbonate; PEI (polyetherimide); PES (polyether sulfone); PET (polyethylene terephthalate); PETG (polyethylene terephthalate glycol), high and medium melt temperature: polyamides, aromatic polyamides, polyethers, polyesters, Hytrell ® , polymethylmethacrylate, polyurethanes: copolymers, EVA (ethylene vinyl acetate) or ethylene vinyl alcohol; low, linear low, medium and high density polyethylenes, latex rubbers, FEP, TFE, PFA, polypropylene
- the vertebral endplates opposing the disc space are roughened.
- the roughening provides hills and valleys into which a flowable polymer can flow and harden, thereby forming a mechanical interlock between the device and the bony surface and resisting retropulsion.
- the roughening can be provided mechanically (as with a curette), or chemically (as by an acid), or by an energy-transmitting device (as with an ablation unit preferably assisted with hyperconductive fluid, such as hypertonic saline).
- the flowable polymer forming a mechanical interlock can be a separate layer.
- the flowable polymer can be a component ofthe strut.
- the flowable polymer can be a component ofthe osteobiologic composition.
- the strut portion ofthe device can have an outer layer of a scaffold material appropriately seeded with osteogenic factors and/or growth factors to produce quick bone ingrowth, thereby effectively locking the strut in place.
- an outer layer of a scaffold material appropriately seeded with osteogenic factors and/or growth factors can also be applied to a balloon component ofthe osteobiologic component.
- the seeding again produces quick bone ingrowth, thereby effectively locking the osteobiologic component in place.
- Balloons ofthe present invention can be made using materials and manufacturing techniques used for balloon angioplasty devices.
- U.S. Patent No. 5,807,327 by Green, the entire teachings of which are incorporated herein by reference, (hereinafter "Green") discloses balloons that may be used in the present invention.
- the materials disclosed by Green for the formation ofthe balloon include tough non-compliant layer materials (col. 8, lines 18-36) and high coefficient of friction layer materials (col. 8, lines 42-54).
- the load-bearing component is delivered into the disc space through an inflatable balloon 12, and the osteobiologic component 20 is freely injected.
- This embodiment is desirable because the balloon 12 can act as a barrier to hydrolysis ofthe load-bearing component, thereby increasing the longevity ofthe load-bearing component.
- the absence ofthe balloon covering the osteobiologic component may be desirable in instances in which it is desirable to immediately begin the bone growth process.
- both the load bearing and the osteobiologic components are delivered into the disc space using a device comprising two separate inflatable balloons 12.
- This embodiment is desirable in instances in which both the annulus fibrosis has been functionally breached, and there is a concern that flowable materials would flow from the disc space and through the breach and into the remainder ofthe body.
- the balloon containing the osteobiologic material be at least semi- permeable to nutrients and preferably resorbable.
- semi-permeable refers to a material that is non-permeable to the flowable materials described above yet permeable to important water and nutrients to support bone growth therein.
- Suitable semi-permeable materials include both porous and non- porous polymeric constructs such as films, fabrics (woven and non-woven) and foams. fti some embodiments, both the load bearing and the osteobiologic components are delivered into the disc space through the same inflatable device.
- FIGs. 7 (a) and (b) another embodiment ofthe device and method ofthe present inevtion is shown wherein the device comprises at least two inflatable balloons 12.
- the load-bearing component is delivered into the disc space through at least two inflatable balloons 12 and the osteobiologic component 20 is freely injected into the disk space using the space between the ballons.
- the osteobiologic component is delivered into the disc space through an inflatable device, and the load-bearing component is freely injected.
- the osteobiologic component comprises an in situ hardenable composition such as a calcium containing cement, or a crosslinkable polymer such as poly(propylene fumarate), polyanhydri.de, or polyoxaester, and the surgeon desires to cordon off the patient from the precursors during their reaction.
- the balloon containing the osteobiologic material be at least semi-permeable to nutrients and preferably resorbable.
- the load-bearing composition comprises growth factors and the surgeon desires to immediately begin the bone growth process in the load-bearing component.
- the load-bearing component is delivered into the disc space through an inflatable device, and the osteobiologic component is freely injected.
- This embodiment may also be desirable in instances in which the annulus fibrosis in essentially intact and the surgeon desires to immediately begin the bone growth process in the load-bearing component.
- the inflatable device comprises a single peripheral wall having an upper and lower surface, upper and lower walls, and a cavity formed therebetween.
- this shape of this embodiment is referred to as a "puck".
- the peripheral wall and upper and lower walls ofthe puck could be designed so as to be percutaneously deliverable through a cannula having an inside diameter of between 0.5 and 18 mm, preferably no more than 4 mm.
- the peripheral wall ofthe puck is designed to be load bearing when the inflatable device is disposed in its inflated position.
- the peripheral wall is made of a shape-memory metal, such as Nitinol, or a thin film alloy.
- the periphery ofthe balloon is reinforced with fibers.
- the peripheral wall comprises polymer fibers. These fibers can be made into a weave that is sufficiently flexible (in the longitudinal direction ofthe fiber) to pass through the cannula and expand into the expanded state. Typically, these fibers have high tensile strengths so that they can very efficiently accommodate the problematic hoop stresses that may be transferred from the osteobiologic component contained within the middle annulus ofthe balloon.
- the fibers form X-shaped cross- hatching pattern.
- the fibers form a continuous wave-like pattern having peaks and troughs, where said peaks and troughs approach upper and lower surfaces.
- the walls ofthe device are reinforced by an internal frame forming a polygonal structure having sides on the upper, lower and peripheral surfaces.
- the peripheral reinforcement is made of a resorbable polymer fiber.
- the upper and lower walls of this puck embodiment are designed to initially accept and contain the osteobiologic component that is flowed into the puck cavity. Accordingly, the upper and lower walls should be at least semi-permeable so as to contain the osteobiologic component.
- the upper and lower walls are made of a resorbable material that quickly resorbs, thereby exposing the contained osteobiologic material to blood flowing from the decorticated endplates.
- this absorbable material has an elastomeric quality.
- This elastomeric quality allows the resorbable upper and lower walls to be delivered through the cannula, and flatten upon device expansion.
- this elastomeric polymer is selected from the materials disclosed in U.S. Patent No. 6,113,624 by Bezwada, the entire teachings of which are incorporated herein by reference (hereinafter "Bezwada").
- this absorbable material is not elastomeric, and is preferably made of a thin film metal alloy or a braided metal alloy.
- FIGs. 8 (a) and 8 (b) there is provided a device 30 ofthe present invention comprising an inflatable portion 32 that includes an arcuate inflatable balloon.
- the inflatable portion 32 ofthe device 30 in its pre-deployed state, is conveniently repeatedly folded upon itself, thereby decreasing the size ofthe device 30 and allowing for minimally invasive insertion into the disc space.
- the device 30 is preferably inserted in the sandwich orientation as shown in FIG. 8 (a) wherein the structural walls 34 are disposed essentially parallel to the vertebral endplates.
- the sandwich orientation allows height H of the structural walls 34 to meet or exceed the disc space height, while the folded width W does not exceed the disc space height.
- FIG. 8 (b) after insertion into the disc space, fluid is flown into the inflatable portion 32 ofthe device 30, thereby expanding the device 30 into the configuration as shown.
- the height H of the structural walls 34 is sufficient to restore the natural height ofthe disc space.
- the cavity, formed by the expanded portion 32 is filled by an osteobiologic component.
- the structural walls 34 of this embodiment are preferably attached to the inflatable portion 32 by an adhesive.
- the structural walls 34 should be designed so that the width I and the strength and modulus ofthe material of construction allow for both support ofthe disc space and bony fusion through the osteobiologic component.
- the height H of the structural wall 34 is at least equal to the height ofthe natural disc space. This condition desirably restores the height ofthe disc space when the inflatable portion 32 is expanded. In some embodiments, the height H ofthe anterior portion ofthe wall 34 is greater than the height h ofthe posterior portion ofthe wall 34. This condition desirably provides a lordotic effect upon expansion ofthe inflatable portion 32.
- the walls 34 are made of allograft bone, and preferably comprise cortical bone. In others, the walls are made of a synthetic resorbable polymeric material. In some embodiments, the walls may be sufficiently porous to provide an effective scaffold, thereby allowing bony fusion therethrough.
- the wall component 34 of this embodiment is made of bone graft
- component 34 comprises additional inflatable portions. After insertion into the disc space, a load bearing composition may be flowed into the cavities of these additional inflatable portions, thereby expanding these additional inflatable portions and eventually producing the desired dimensions ofthe walls 34.
- each wall 34 is translaterally oriented in the expanded device.
- a first wall supports essentially the anterior portion ofthe opposing cortical rims
- the second wall supports essentially the posterior portion ofthe opposing cortical rims, so that one of these walls will essentially bear the entire load during flexion and the other wall will bear essentially the entire load during extension.
- these walls have a length L corresponding to the anterior and posterior aspects ofthe cortical rim.
- the inflatable portion 32 has upper and lower surfaces 36 and 38 for contacting the adjacent vertebral endplates, a peripheral side surface 40 connecting the upper and lower surfaces 36 and 38, and an opening 42 in the peripheral side surface 40.
- the inflatable portion 32 Upon a flow of fluid through the opening 42 from a cannula 18, the inflatable portion 32 is expanded and surfaces 36, 38 and 40 are pushed apart sufficiently to form an internal cavity suitable for containing an osteobiologic component. Because the osteobiologic component retained within this cavity is preferably at least semipermeable in order to provide bony fusion, the upper and lower surfaces 36 and 38 ofthe inflatable portion 32 preferably do not act as barriers to bony fusion. Accordingly, it is preferred that the upper and lower surfaces 36 and 38 are either porous (preferably, semipermeable) or quickly resorbable.
- the upper and lower surfaces 36 and 38 are made of a material that resorbs within 7 days, preferably 3 days, preferably one day.
- fast-resorbing materials include denatured collagen, polysaccharide-based materials such as starch and oxidized regenerated cellulose, and hydroxylated lactide-glycolide copolymers.
- the opening in the side surface 40 is formed closely adjacent to the structural wall 34, positioned anteriorly on a vertebral endplate.
- the inflatable device 30 of this embodiment has a configuration designed to match the geometry ofthe disc space, and is selected from the group consisting of an anterior lumbar interbody fusion (ALIF) configuration, a posterior lumbar interbody fusion (PLLF) configuration, a vertebral body replacement (VBR) configuration, and an anterior cervical discectomy and fusion (ACDF) configuration.
- ALIF anterior lumbar interbody fusion
- PLLF posterior lumbar interbody fusion
- VBR vertebral body replacement
- ACDF anterior cervical discectomy and fusion
- the device 60 comprises an outer side- wall component 62, an inner side-wall component 64, and a balloon 66 disposed between and attached to said inner and outer wall components.
- the short cranial- caudal height ofthe inner and outer walls allows for the device to be inserted into the disc space without having to distract the disc space prior to insertion.
- the sidewalls prevent expansion ofthe balloon such that the thickness ofthe device is minimized upon inflation. Minimized wall thickness is important for ensuring maximum area for bone growth (fusion) between the adjacent vertebrae.
- the footprints ofthe outer and inner side- wall components 62 and 64 represent substantially equal arcs of two concentric circumferences. This allows placing device 60 along the periphery ofthe anterior portion 14 of a vertebral endplate 8 and filling a cavity therewithin with a load bearing material.
- the outer and inner walls 62 and 64 are made of a flexible plastic such as poly(ethyleneterephthalate), a superelastic metal such as Nitinol, or a flexible material/geometry combination, whereby each wall can be deformed into a relatively elongated shape for delivery to the disc space through a cannula 18.
- the sidewalls are sufficiently rigid to guide the device into the desired location in the disc space but sufficiently flexible to allow delivery through the cannula. Referring to FIG. 9 (c), during the insertion ofthe device 60, upon release from the cannula 18, components 62 and 64 can then take on the desired arcuate shape. Referring to FIG.
- the device 60 is expanded by injecting a load-bearing component, an osteobiologic component or a combination thereof into a cavity formed by the components 62, 64, and 66.
- a load-bearing component an osteobiologic component or a combination thereof into a cavity formed by the components 62, 64, and 66.
- Any suitable injection means can be used, for example, a syringe pump 70.
- FIGs. 10 (a) and (b) An alternative embodiment of inflatable device of the present invention is shown in FIGs. 10 (a) and (b).
- Device 260 comprises an upper wall component 266 and a lower wall component 268 joined by an inflatable balloon 270.
- the footprints ofthe upper and lower wall components 266 and 268 represent substantially equal arcs of two concentric circumferences. This allows placing device 260 along the periphery ofthe anterior portion 14 of a vertebral endplate 8 and filling a cavity therewithin with a load bearing material.
- the upper and lower wall components 266 and 268 are made of a superelastic material such as Nitinol, or a flexible material/geometry combination, whereby each wall can be deformed into a relatively elongated shape for delivery to the disc space through a caimula 18.
- device 260 is similar to device 60. Insertion of device 260 can be accomplished in a manner depicted in FIG. 9 (c). Upon release from cannula 18, components 266 and 268 can then take on the desired arcuate shape. Subsequent to insertion, device 260 is inflated by injecting a load-bearing component, an osteobiologic component or a combination thereof into balloon 270.
- balloon 270 is semi-permeable.
- balloon 270 is made of a material that quickly resorbs, thereby exposing the contained osteobiologic material to blood flowing from the decorticated endplates.
- the strut is deliverable through a cannula having an inside diameter of between 3 mm and 18 mm, preferably between 4 mm and 12 mm, more preferably between 5 mm and 10 mm.
- the strut is preferably deliverable through a cannula having an inside diameter of between 0.5 mm and 6 mm, preferably between 1 mm and 4 mm, more preferably between 2 mm and 3 mm.
- the upper and lower surfaces ofthe upper and lower walls, respectively, have teeth that prevent excessive movement ofthe strut after implantation.
- the device 80 comprises four rail components 82 wherein the footprints ofthe rail components 82 represent substantially equal arcs of two concentric circumferences. Components 82 are joined by an inflatable balloon 84 such that the device can be inserted in a collapsed configuration as shown in FIG. 11 (b) and then expanded as shown in FIG. 11(a) once filled with a load-bearing material to increase disc height and provide thickness for load bearing support.
- device 80 is shown in FIGs. 12 (a) and (b).
- device 80 is delivered in a generally diamond- shaped configuration, shown in plan view on FIG. 12 (a) and in lateral view in FIG. 12 (b).
- the upper and lower rails 82 will cause slight subsidence ofthe vertebral body endplates, thus providing stability ofthe implanted device.
- FIGS. 13 (a) through (d) a preferred embodiment ofthe method ofthe present invention is shown.
- a cannula 18 is inserted into an intervertebral space.
- an inflatable balloon 12 of a generally toroidal shape is inserted through the cannula 18 into the intervertebral space.
- the balloon 12 is expanded by directing a load-bearing component into said balloon.
- osteobiologic component 20 is injected into the open cavity defined by the outer surface ofthe balloon 12.
- the osteobiologic component comprises a water-soluble component.
- the water-soluble component is dissolved, thus forming a porous matrix shown in FIG. 13 (d).
- the load-bearing component is delivered through a balloon, and the osteogenic component is provided in a hydrogel phase ofthe osteobiologic component.
- suitable hydrogels are provided hereinbelow.
- the strut is formed by bonding together two bondable components.
- the bondable materials are selected from the group consisting of heat bondable materials such as polycaprolactone, and polymerizable materials such as ⁇ oly(propylene fumarate) and polyoxaesters including photo-curable materials such as polyanhydrides.
- load-bearing materials in the form of beads is delivered into the inflatable device and packed into the device so as to create a stable strut having an open interstitial porosity.
- the beads may be packed without subsequent stabilization other than closing off the opening of the balloon, h these embodiments, the beads are preferably polyarylether ketone (PAEK), more preferably polyetherether ketone (PEEK) with chopped carbon fiber.
- a bonding material may be subsequently flowed into the interstitial porosity to further stabilize the packed beads.
- this bonding material comprises an aliphatic polyester such as polycaprolactone (PCL).
- the bonding material may be resorbable and may include osteogenic additives such as growth factors and stem cells.
- the beads ofthe load-bearing material are made of a heat-bondable material, such as polycaprolactone.
- heat may be delivered into the packing and soften the contacting surfaces ofthe beads. Upon subsequent cool down to body temperature, the contacting surfaces solidify to further stabilize the packed structure.
- the heat is provided exogenously. h other embodiments, the heat is provided by the patient's body heat ( ⁇ 37 °C). Now referring to FIGs.
- another embodiment ofthe device ofthe present invention 300 comprises at least two bondable components 310 and 320, that are delivered into the disc space in unassembled form, placed closely adjacent one another, and then bonded together, preferably by heat bonding.
- FIG. 14 (b) representing a lateral view ofthe device of FIG. 14
- device 300 comprises first and second portions 310 and 320.
- First portion 310 has a lower bearing wall 312, upper angled wall 314, and a leading wall 316 and a trailing wall 318.
- Second portion 320 has an upper bearing wall 322, lower angled wall 324 and a leading wall 326 and a trailing wall 328.
- the combined height ofthe assembled portion H exceeds that ofthe disc space.
- the angled walls form the same angle so that the leading edge ofthe second portion can be ramped up the angled wall ofthe first portion.
- the first portion 310 is placed in the disc space. Because the height of the first portion is less than the disc space, the first portion 310 is easily positionable anywhere within the disc space.
- the second portion 320 is introduced into the disc space and ramped up the angled wall ofthe first portion. Corresponding rails and groove are provided on the angled walls ofthe first and second portion so as to guide the second portion along the anlong wall ofthe first portion (see below). Because the second portion only contacts the lower portions ofthe first portion, the upper wall 322 ofthe second portion 320 does not touch the adjacent endplate during ramping and so the ramping is easy. Only when the ramping is essentially complete does the upper wall ofthe second portion contact the adjacent upper endplate.
- the overall height ofthe ramp H is slightly greater than that of the disc space, so that distraction is achieved when the leading edge ofthe second portion reaches the leading edge ofthe first portion.
- a cross-section ofthe device of FIG. 14 (a) is shown, taken along arrows B.
- angled wall 314 of first portion 310 includes a grove 330
- angled wall 324 of second portion 320 includes a ridge 332, designed to fit into a slide against grove 330.
- ridge 332 further includes a metal filament 334. It is understood that the locations of grove 330 and ridge 332 can be interchanged to between angled walls 314 and 324 of upper and lower portions 310 and 320.
- the rail and groove feature ofthe ramps has a Morse taper so as to lock the ramp in its assembled form when the leading edge ofthe second portion reaches the leading edge ofthe first portion.
- the ramp of this embodiment is not flowed into the disc space, and the heating is very localized, extremely strong, high temperature materials such as PEEK may be used as the material of construction, hi some embodiments, the ramp is made of a high temperature resorbable material.
- the high temperature absorbable material is amorphous and has a glass transition temperature of above 100 °C.
- the amorphous absorbable is PLA.
- the high temperature absorbable material is crystalline and has a melting point of above 100 °C.
- the crystalline absorbable is p- dioxanone.
- a guidewire is guided through the center of the ramp guide.
- the guidewire would allow the ramps to be inserted over the guidewire.
- the guidewire could be remotely steered into place via IGS or equivalent, and then the ramps could be passed over the guidewire into place.
- the ramps could be semi-rigid which would allow them to follow the guidewire through the soft tissue, over the wire.
- an 'T'-Beam ramp cage is provided.
- the ramp cage discussed above could incorporate or mate with modular tops and bottoms. These tops and bottoms would have tracks, which would locate on guides fixed to the ramps (or the guides could be on the modular top, and tracks on the ramps) wliich would aid insertion and ensure the ramps were connected to these modular tops and bottoms.
- the surfaces of the modular tops and bottoms would go between the ramps and the vertebral bodies such that when assembled, a cross-section of the ramp/top bottom assembly would resemble an "I"-Beam.
- the ramps and modular tops could be shaped hi several configurations, inserted assembled, or assembled within the disk space.
- a ribbon-shaped ramp having a longitudinal through-hole.
- a threaded rod is inserted through the middle of the ribbon so that, as the threaded rod is turned, the ribbon would “accordion” itself, increasing its height witiiin the disk space.
- This " accordion” -ing could be achieved by other methods, such as a spring, a cable, etc.
- FIG. 15 one embodiment of a method of use of device 300 shown in FIGs. 14 (a) - (d) is depicted, hi this embodiment, the first and second ramp portions 310 and 320 are introduced translaterally so as to form a single ramp stretching essentially transversely across the disc space.
- This design in advantageous when used in a posterolateral approach, as this approach takes advantage ofthe fact that the muscle planes in the vicinity ofthe approach allow the implant to be delivered in a less invasive manner.
- the medial portion ofthe ramp has a height that is higher than the lateral portions. This feature provides the doming that is advantageous in interbody fusions
- FIG. 16 another embodiment of a method of use of device 300, shown in FIGs. 14 (a) - (c) is depicted.
- the ramp ofthe present invention may be advantageously used in a PLIF procedure, hi particular, two ramps may be constructed in-situ so as to form bilateral struts similar to the Steffee struts.
- an intervertebral fusion device comprising a strut comprising: a) a first component comprising: i) a lower bearing surface adapted for bearing against a lower vertebral endplate, and, ii) an upper surface comprising a leading end, an angled middle portion and a trailing end; and b) a second component comprising: i) an upper bearing surface adapted for bearing against an upper vertebral endplate, and, ii) an upper surface comprising a leading end, an angled middle portion and a trailing end, wherein the angled portion ofthe first component mates with the angled portion ofthe second component.
- the struts are completely dense. This feature maximizes the strength ofthe strut, and so is desirable for the load bearing.
- the strut has openings sized to permit bony fusion therethrough.
- the upper and lower walls have openings designed to promote bony fusion from the upper endplate to the lower endplate.
- the sidewalls ofthe strut also have such openings.
- the openings have a diameter of at least 2 mm. In other embodiments, the openings are in the range of from 50-500 um, more preferably between 100 and 300 um, preferably between 100 and 250 um. These preferred opening sizes are believed to be more conductive to bone growth.
- second phase refers to an additive that enhances the performance ofthe material, for example carbon fibers enhance the strength of the material and calcium phosphate particulates enhance the osteoconductivity ofthe material.
- aqueous phase refers to a component ofthe material capable of maintaining cell viability, e.g. an alginate hydrogel.
- load-bearing components that satisfy the above Table include at least one compound selected from the group consisting of poly(lactic acid), poly(glycolic acid), p-dioxanone fibers, polyarylethyl, polymethylmethacrylate, polyurethane, amino-acid-derived polycarbonate, polycaprolactone, aliphatic polyesters, calcium phosphate, unsaturated linear polyesters, vinyl pyrrolidone and polypropylene fumarate diacrylate or mixtures thereof.
- poly(lactic acid), poly(glycolic acid), p-dioxanone fibers polyarylethyl, polymethylmethacrylate, polyurethane, amino-acid-derived polycarbonate, polycaprolactone, aliphatic polyesters, calcium phosphate, unsaturated linear polyesters, vinyl pyrrolidone and polypropylene fumarate diacrylate or mixtures thereof.
- osteobiologic components that satisfy the above Table include at least one member selected from the group consisting of mesenchymal stem cells, a growth factor, cancellous bone chips, hydroxyapatite, tri-calcium phosphate, polylactic acid, polyglycolic acid, polygalactic acid, polycaprolactone, polyethylene oxide, polypropylene oxide, polysulfone, polyethylene, polypropylene, hyaluronic acid, bioglass, gelatin, collagen and a polymeric fiber.
- some matrix components may be used in some instances as the matrix for the load bearing component and in other instances as the matrix for the osteobiologic component.
- polycaprolactone may be used in conjunction with p-dioxanone reinforcing fibers as a matrix for a load bearing component, and may also be used in conjunction with polylactic acid and hydroxyapatite as a matrix for an osteobiologic component.
- the term “hardenable” refers to a material that can be delivered through a cannula into the disc space in a viscous form.
- material that can be delivered through a cannula having at least about 6 mm internal diameter, hi another embodiment, a cannula has a diameter of no more than about 6 mm.
- the flowable load-bearing composition and osteobiologic component ofthe present invention are flowable, meaning they are of sufficient viscosity to allow their delivery through a cannula of on the order of about 2 mm to about 6 mm inner diameter, and preferably of about 3 mm to about 5 mm inner diameter.
- Such biomaterials are also hardenable, meaning that they can solidify, in situ, at the tissue site, in order to retain a desired position and configuration.
- the hardenable material is simply a material (such as a low temperature polymer) having a melting point (for crystalline materials) or a glass transition temperature (for amorphous materials) less than 100 °C, and is solid a body temperature (37 °C).
- these low temperature materials are simply heated to the point where they are viscous and flowable and then injected into the disc space. The subsequent cooling ofthe viscous material to body temperature then solidifies them. Because these materials do not need to react in- situ, they are desirable for their relative inertness. Accordingly, in some embodiments, they may be freely injected into the disc space without a protective balloon.
- the hardenable material comprises a cross-linkable component (or "cross-linking agent").
- cross-linkable component or "cross-linking agent”
- the load-bearing component comprises, a cross-linking agent, hi such embodiments, it is desirable that the cross-linking agent be delivered into the disc space tlirough a balloon so that the balloon may protect the surrounding tissue from the reactive components during the reaction.
- the load-bearing component comprises a cross- linking agent
- the osteobiologic component comprises a cross-linking agent
- the hardenable material comprises a polymer and a cross-link agent, h some embodiments, the hardenable material may further comprise a monomer. In some embodiments, the hardenable material may further comprise an initiator, hi some embodiments, the hardenable material may further comprise an accelerant.
- the cross-linking component is made from a two-part composition comprising a monomer and a crosslinking agent.
- the cross-linked composition is flowable at a temperature of between 37 °C and 40 °C.
- the cross-linkable component is resorbable.
- a resorbable material loses 50% of its initial strength within no more than two years after implantation.
- Providing a resorbable cross-linkable component is desirable because it not only provides the high initial strength required for supporting the disc space in an intervertebral fusion application, but also allows for the eventual replacement by bone fusion.
- the resorbable cross-linkable component comprises those cross-linkable components disclosed by Wise in U.S. Patent No. 6,071,982, the entire teachings of which are incorporated herein by reference.
- the cross-linkable component is UV curable.
- UV curable cross-linkable components are disclosed in Biomaterials (2000), 27:2395-2404 and by Shastri in U.S. Patent No. 5,837,752, the entire teachings of which are incorporated herein by reference.
- the cross-linkable component is water-curable, hi such instances, the resulting body is typically somewhat weak, and so it is preferred that the water-curable cross-linkable compound be used as a matrix for the osteobiologic component.
- the strut is made of a non-resorbable material. Since the non-resorbable material does not degrade over time, the use ofthe non- resorbable material provides the surgeon with a measure of safety and prevents collapse ofthe disc space in the event the osetobiologic composition does not produce a fusion.
- the non-resorbable material is a polymer.
- the selection of a polymer allows the material to be flowed into place.
- the load bearing polymer is a polyarylethyl ketone (PAEK). More preferably, the PAEK is selected from the group consisting of polyetherether ketone PEEK, polyether ketone ketone PEKK and polyether ketone PEK. h preferred embodiments, the PAEK is polyetherether ketone.
- PAEK-type polymers have a very high melting point (e.g., 250 °C) and so are not amenable to flow at desirable temperatures. Accordingly, embodiments ofthe present invention using PAEK as the load bearing composition would typically deliver PAEK in a solid fonn, such as in bead form or as pre-constructed components, and then assemble and heat bond the components in the disc space under very high temperatures (e.g., 250 °C). These high temperatures would likely require the use of a highly insulated expanded device.
- the strut is a composite comprising fiber, preferably carbon fiber. Composite struts comprising carbon fiber are advantageous in that they typically have a strength and stiffness that is superior to neat polymer materials such as a polyarylethyl ketone PAEK.
- the fiber, preferably, carbon fiber comprises between
- the fiber comprises between 10 vol % and 50 vol % ofthe composite.
- the polymer and carbon fibers are homogeneously mixed.
- the composite strut is a laminate
- the carbon fiber is present as chopped state.
- the chopped carbon fibers have a median length of between 1 mm and 12 mm, more preferably between 4.5 mm and 7.5 mm.
- the carbon fiber is present as continuous strands.
- the composite strut comprises: a) about 40 % to about 99 % (more preferably, about 60 % to about 80 vol %) polyarylethyl ketone PAEK, and b) about 1 % to about 60 % (more preferably, about 20 vol % to about 40 vol%) carbon fiber, wherein the polyarylethyl ketone PAEK is selected from the group consisting of polyetherether ketone PEEK, polyether ketone ketone PEKK and polyether ketone PEK.
- the composite strut consists essentially of PAEK and carbon fiber. More preferably, the composite strut comprises about 60 wt % to about 80 wt % PAEK and about 20 wt % to about 40 wt% carbon fiber. Still more preferably the composite strut comprises about 65 wt % to about 75 wt % PAEK and about 25 wt % to about 35 wt % carbon fiber.
- the physical requirements of the flowable load bearing component will depend upon the length and diameter of the arc as well as the physical requirements imposed by the implantation site.
- certain load-bearing compositions may or may not exhibit sufficient physical properties.
- Physical properties of the load bearing components can also be modified through the addition of any of a variety of reinforcements, such as carbon fibers, KevlarTM or Titanium Rods, woven or laser etched metallic tubular stents, or other strength enhancers as will be understood in the art.
- Certain composite materials such as carbon fibers embedded in a bonding agent such as a polycaprolactone are believed to be particularly useful in forming the load bearing component ofthe present invention.
- graphite (carbon fibers) having a diameter within the range of from about 0.003 to about 0.007 inches is provided in bundles (tows) composed of from about 3,000 to about 12,000 fibers.
- One typical fiber useful for this purpose is manufactured by Hexcel Carbon Fibers, Salt Lake City, Utah, Part No. HS/CP-5000/IM7-GP 12K.
- the Tow tensile strength is in the range of from about 5,000 to about 7,000 Mpa.
- Tow tensile modulus is within the range of from about 250 to about 350 Gpa.
- bundles ofthe carbon fiber described above is packed in a deflated balloon, optionally along with a Ni-Ti stent having an 8 mm diameter and 8 cm length.
- a Ni-Ti stent having an 8 mm diameter and 8 cm length.
- one useful structure is similar to the Smart Stent (Cordis), and it helps keep the structure intact and also adds structural strength to the implanted structure.
- carbon fibers having within the range of from about 15 to about 45 degrees of braids are utilized within the inflatable device to reinforce the load bearing material.
- the braid may be in the form of a plain weave, and may be obtained, for example, from Composite Structures Technology (Tehachapi, Calif.).
- a 0.5 inch diameter of 45 degrees braided carbon fiber sleeve is positioned within the center ofthe balloon. This braided sleeve conforms dimensionally to the inside diameter ofthe balloon. A 0.3 inch diameter braided carbon sleeve may also be positioned concentrically within the balloon, within the outer braided carbon fiber sleeve. Unidirectional fibers are thereafter introduced inside ofthe ID ofthe inner braided carbon sleeve. Unidirectional fibers are also introduced into the annular gap between the two braided sleeves. The volume ofthe fiber per volume of balloon is generally within the range of from about 40% to about 55%).
- the flowable load bearing material ofthe present invention having a viscosity within the range of from about 100 cps to about 500 cps is injected under 10 atmospheres pressure into the balloon.
- the use of braided sleeves will produce higher structural resistance to sheer stress as a result of torsional loads, plus the ability to distribute unidirectional fibers in a homogenous manner within the balloon at all times.
- the polymer comprises polymethylmethacrylate (PMMA).
- the matrix comprises a radio-opaque agent.
- the load bearing composition comprises polyurethane.
- the polyurethane materials disclosed in US Patent No. 6,306,177 by Felt hereinafter "Felt", the specification of which is incorporated by reference to the extent it is not inconsistent with the remainder ofthe specification, is selected.
- Polyurethanes can be tailored to have optimal stiffness by adjusting the ratio of soft segment to hard segment ratio in the polymer. Furthermore, polyurethanes can be prepared as two-part systems that will cure upon mixing. Preferred polyurethanes, e.g., thermoplastic polyurethanes ("TPU"), are typically prepared using three reactants: an isocyanate, a long-chain macrodiol, and a short-chain diol extender. The isocyanate and long-chain diol form a "soft" segment, while the isocyanate and short-chain diol form a "hard” segment. The hard segments form ordered domains held together by hydrogen bonding. These domains act as crosslinks to the linear chains, making the material similar to a cross-linked rubber. It is the interaction of soft and hard segments that determines and provides the polymer with rubber-like properties.
- TPU thermoplastic polyurethanes
- the strut comprises a photocurable material.
- the material comprises organophosphorous compounds. These compounds are advantageous because the resulting product is calcium phosphate based, and so is both biocompatible and resorbable.
- the strut has a resorbable matrix material.
- a resorbable matrix material is desirable because it is eventually resorbed by the body, and may eventually be replaced by bone.
- the resorbable strut is a high temperature material.
- a high temperature material flows above 100°C.
- the high temperature absorbable material enters the disc space as a plurality of components in a solid form. The components are then contacted in the disc space, and heat is applied to bond the components without deforming the assembled shape.
- the load bearing composition includes a matrix comprising an amino-acid derived polycarbonate.
- the osteobiologic component comprises a matrix comprising a biodegradable polyurethane.
- the osteobiologic component comprises a matrix comprising an amorphous polymer and has a glass transition temperature of below 100 °C.
- the amorphous absorbable is D,L-polylactic acid (PLA).
- PLA D,L-polylactic acid
- the properties of these polymers is to form copolymers with residues having more diverse side chain structures, e.g., lysine.
- a poly(lactide-co-lysine) functionalized with peptide containing the arginine-glycine-aspartate (RGD) sequence was prepared by removal ofthe benzyoxycarbonyl protecting group on the lysyl residue and peptide coupling.
- the peptide concentration was found to be approximately 3.1 mmol/g, which could be translated into a peptide surface density of 310 fmol/cm 2 .
- a surface density of as low as 1 fmol/cm 2 of an RGD peptide has been previously determined to promote cell adhesion to an otherwise nonadherent surface (Massia and Hubbell, 1991). Therefore, by carefully processing the copolymer, biodegradable films with cell adhering properties can be prepared from the copolymer of lactide and lysine.
- polylactic acid has also been synthesized as an acrylic macromonomer and subsequently copolymerized with polar acrylic monomers (e.g., 2-hydroxyethylmethacrylate) (Barakat et al., 1996). These polymers were studied as amphiphihc graft copolymers for drug delivery purposes.
- the surface properties of these polymers maybe controlled by the ratio ofthe polylactic acid graft length and copolymer content, and can be potentially used to control the drag release profile and biodistribution.
- the high temperature resorbable material is semi- crystalline and has a melting point of above 100 °C.
- the semi-crystalline absorbable is selected from the group consisting of p-dioxanone, L-polylactic acid and poly(glycolic acid) (PGA), and mixtures thereof.
- the strut comprises at last 90 wt % of an aliphatic polyster.
- the aliphatic polyester is polycaprolactone ("PCL").
- Polycaprolactone is a linear polyester formed through the ring opening ofthe monomer epsilon-caprolactone.
- Polycaprolactone is a semi- crystalline thermoplastic resin, which can be readily molded at moderate temperatures to yield tough translucent products. Its crystalline melting point is about 60 °C, which represents a theoretical upper temperature limit of use for the present invention. Above its melting point the material is characterized by a high degree of conformability and workability.
- Other polymers such as ⁇ oly(dodecene- 1) and transpolyisoprene are also useful in this invention. These polymers are characterized by being crystalline at room temperature, non-crystalline at about 70 °C and having a relatively rapid rate of crystallization when cooled to body temperature. These polymers do not crystallize like simple compounds so that there is a reasonable time lag after the polymer reaches body temperature before crystallization is complete. This permits sufficient time for the flowable composition to be positioned in the disc space while the polymer is still pliable.
- an absorbable component comprising a polymer formed from aliphatic lactone monomers selected from the group consisting of p-dioxanone, trimethylene carbonate, e -caprolactone, glycolide, lactide (1, d, dl, meso), delta-valerolactone, beta-butyrolactone, epsilon-decalactone, 2,5-diketomorpholine, pivalolactone, alpha, alpha-diethylpropiolactone, ethylene carbonate, ethylene oxalate, 3-methyl-l,4-dioxane-2,5-dione, 3,3-diethyl-l,4- dioxan-2,5-dione, gamma-butyrolactone, l,4-dioxepan-2-one, l,5-dioxepan-2-one, l,4-dioxan-2-one, 6,8-d
- the strut comprises a load bearing composition consisting essentially of polycaprolactone.
- the compressive strength of essentially solid polycaprolactone is about 15 MPa, and its compressive modulus is about 0.5 GPa.
- the higher molecular weight polycaprolactones (PCLs) are preferred, as they tend to have a higher strength and degrade more slowly.
- the molecular weight ofthe polycaprolactone is at least 30,000 Daltons. More preferably, the molecular weight ofthe polycaprolactone is at least 40,000 Daltons.
- the strut comprises a load bearing composition of cross-linked polycaprolactone.
- the load bearing composition comprises a self-interpenetrating network (S-IPN) comprising a network of host polycaprolactone and cross-linked polycaprolactone.
- S-IPN self-interpenetrating network
- certain mechanical properties of polycaprolactone increased by about 3 fold when it was formed as a S-IPN.
- the tensile modulus increased to 6 fold over conventional polycaprolactone.
- the compressive strength ofthe S-IPN of polycaprolactone maybe about 45 MPa, and its compressive modulus may be about 1.5 GPa.
- the polycaprolactone is heat treated to enhance its crystallinity, and thereby even further enhance its resistance to degradation.
- the above described polymers ofthe present invention may be liquid or low melting temperature, low molecular weight polymers, with or without photocurable groups.
- the liquid or low melting polymers are of sufficiently low molecular weight, having an inherent viscosity of about 0.05 to about 0.5 dL/g, to yield materials which can easily flow, with or without heat being applied, through a small diameter delivery device such as a syringe or cannula, with or without mechanical assistance, a caulking gun, a soft- sided tube, and the like.
- the aliphatic polyesters useful in the practice ofthe present invention will typically be synthesized by conventional techniques using conventional processes.
- the lactone monomers are polymerized in the presence of an organometallic catalyst and an initiator at elevated temperatures.
- the organometallic catalyst is preferably tin based, e.g., stannous octoate, and is present in the monomer mixture at a molar ratio of monomer to catalyst ranging from about 10,000/1 to about 100,000/1.
- the initiator is typically an alkanol, a glycol, a hydroxyacid, or an amine, and is present in the monomer mixture at a molar ratio of monomer to initiator ranging from about 100/1 to about 5000/1.
- the polymerization is typically carried out at a temperature range from about 80 °C to about 220 °C, preferably from about 160 °C to about 200 °C, until the desired molecular weight and viscosity are achieved.
- the homopolymers and copolymers of aliphatic polyesters will typically have a weight average molecular weight of about 5,000 grams per mole to about 200,000 grams per mole, and more preferably about 10,000 grams per mole to about 100,000 grams per mole. Polymers of these molecular weights exhibit inherent viscosities between about 0.05 to about 3.0 deciliters per gram (dL/g), and more preferably about 0.1 to about 2.5 dL/g as measured in a 0.1 g/dL solution of hexafluoroisopropanol (HFIP) or chloroform at 25 °C.
- HFIP hexafluoroisopropanol
- Suitable lactone monomers used in the matrices ofthe present invention may be selected from the group consisting of glycolide, lactide (1, d, dl, meso), p-dioxanone, trimethylene carbonate, € -caprolactone, delta-valerolactone, beta-butyrolactone, epsilon-decalactone, 2,5-diketomorpholine, pivalolactone, alpha, alpha- diethylpropiolactone, ethylene carbonate, ethylene oxalate, 3 -methyl- 1,4-dioxane- 2,5-dione, 3,3-diethyl-l,4-dioxan-2,5-dione, gamma-butyrolactone, l,4-dioxepan-2- one, l,5-dioxepan-2-one, l,4-dioxan-2-one, 6,8-dioxabicycloc
- the aliphatic polyesters used in the matrices ofthe present invention consist of homopolymers of poly(e-caprolactone), polyfjp-dioxanone), or poly(trimethylene carbonate) or copolymers or mixtures thereof, or copolyesters of p-dioxanone or trimethylene carbonate and glycolide or lactide or mixtures thereof, and in particular, copolymers of p-dioxanone/glycolide, p-dioxanone/lactide, trimethylene carbonate/glycolide and trimethylene carbonate/lactide, or copolyesters of .epsilom-caprolactone and glycolide or mixtures thereof, or mixtures of homopolymers of e-caprolactone and lactide.
- a biocompatible, non- absorbable, flowable polymer whose melting point is. from about 45 °C to about 75 °C and which is a rigid solid at body temperatures below about 42 °C is placed in a standard Toomeytype disposable syringe with a 35mm diameter and appropriate capacity of about 50-100 milliliters.
- the filled syringe is placed in a peel-apart package for sterile delivery and sterilized with cobalt radiation or heat, the former being preferred.
- the polymer can be placed in a squeeze bottle of suitable capacity and having a slit orifice.
- the strut comprises at least 90 wt % calcium phosphate.
- the compressive strength of hydroxyapatite is about 65 MPa and the tensile strength of hydroxyapatite is about 10.6 MPa. The present inventors believe that these values should satisfy typical strut load requirements.
- the matrix is made of a cross-linkable compound. In general, cross-linkable compounds cross-link in-situ and provide higher compressive strengths (typically on the order of 20-120 MPa) than heat-flowable polymers (typically on the order of 1-20 MPa.
- the cross-linkable compound comprises an unsaturated linear polyester.
- the unsaturated linear polyester comprises a fumarate double bond, and more preferably comprises polypropylene fumarate.
- the cross-linkable compound is cross-linked by a monomer, preferably a vinyl monomer, more preferably vinyl pyrrolidone.
- the links produced by the cross-linking agent are biodegradable. Preferred embodiments thereof include polypropylene fumarat- diacrylate.
- the cross-linking reaction is aided by an initiator.
- the initiator is benzoyl peroxide.
- light is used as the photoinitiator.
- the cross-linking reaction is aided by an accelerant, h preferred embodiments, the accelerant is NN-Dimethyl-j-)-toluidine. It is believed that the terminal functional groups affect the strength and degradation resistance ofthe cross-linked matrix.
- the cross- linked compound is terminated by a terminal group selected from the group consisting of diepoxide, or diacryal functional groups. In preferred embodiments, the terminal groups are diepoxide functional groups. These terminal functional groups were shown to be more resistant to degradation than di vinyl terminated polypropylene fumarat (Domb 1996).
- a porogen such as NaCI or a foaming agent is added to the cross-linkable composition.
- the porogen is water soluble, more preferably it is a water soluble salt or sucrose.
- a calcium phosphate based compound such as hydroxyapatite or tricalcium phosphate, is added to the cross-linkable composition.
- these compounds are desirable because they can provide an osteoconductive pathway for bone growth, they can neutralize any acid produced from hydrolysis of the polymer matrix, and provide reinforcement.
- the calcium phosphate is nano high aspect hydroxyapatite.
- the strut ofthe present invention comprises a load bearing composition comprising a fumarate-based polymer (such as polypropylene fumarate) cross-linked with a cross-linking agent containing a polupropylene fumarate-unit, such as polypropylene fumarate-diacrylate.
- compositions are disclosed in Timmer, Biomaterials (2003) 24:571-577, the entire teachings of which are incorporated herein by reference. These compositions are characterized by a high initial compressive strength (about 10-30 MPa) that typically increases over the first 12 weeks, high resistance to hydrolytic degradation (about 20-50 at 52 weeks), and an acceptable modulus for use as a strut (0.5-1.2 GPa).
- the polypropylene fumarate: polypropylene fumarate-diacrylate double bond ratio is between about 0.1 and about 3. In more preferred embodiments, the polypropylene fumarate-diacrylate double bond ratio is between about 0.25 and about 1.5.
- the load bearing composition comprising polypropylene fumarate cross-linked by polypropylene fumarate-diacrylate further comprises tricalcium phosphate (TCP), preferably in an amount of between about 0.1 wt % and about 1 wt %.
- TCP tricalcium phosphate
- the strut or load bearing composition comprises two cross-linkable polymer compositions. Upon exposure to appropriate cross-linking agents, each ofthe cross-linkable compositions cross-links with itself, but not with the other cross-linked polymer. The result thereof is a matrix comprising two cross- linked polymers. These are called “inte enetrating networks" (“IPN").
- IPN integer enetrating networks
- the strut or load bearing composition comprises a first cross-linkable polymer composition and a second non-cross linkable polymer composition.
- first cross-linkable compound cross-links with itself, while the second polymer remains unaffected.
- second polymer remains unaffected.
- the result thereof is a matrix comprising a first cross linked polymer and a second non-cross linked polymers.
- the S-IPNs comprise a first biodegradable polymer capable of producing acidic products upon hydrolytic degradation; a second biodegradable polymer, which, preferably via crosslinking, provides a biopolymer scaffolding or internal reinforcement; and optionally a buffering compound that buffers the acidic products within a desired pH range.
- the second biodegradable polymer comprises polypropylene fumarate (PPF) which is cross-linked, desirably by a vinyl monomer such as vinyl pyrrolidone (VP) to form the biopolymer scaffolding which provides the semi-IPN with the requisite dimensional and geometric stability.
- the S-IPN comprises a bone cement containing a biodegradable polymeric semi-IPN alloy comprising a first biodegradable polymer (such as PLGA) capable of producing acidic products upon hydrolytic degradation; and a second biodegradable polymer (such as polypropylene fumarate), which provides a biopolymer scaffolding or internal reinforcement, wherein the second biodegradable polymer is polymerized in vivo to provide a hardened, semi-IPN alloy bone cement.
- a biodegradable polymeric semi-IPN alloy comprising a first biodegradable polymer (such as PLGA) capable of producing acidic products upon hydrolytic degradation; and a second biodegradable polymer (such as polypropylene fumarate), which provides a biopolymer scaffolding or internal reinforcement, wherein the second biodegradable polymer is polymerized in vivo to provide a hardened, semi-IPN alloy bone cement.
- Both the bone cement and dimensionally and geometrically stable IFDs ofthe disclosure ofthe invention may advantageously also contain other agents such as bone repair proteins (BRPs) and antibiotics, to, e.g., actively promote bone growth and prevent infection while the bone cement or IFD is in place.
- BRPs bone repair proteins
- antibiotics to, e.g., actively promote bone growth and prevent infection while the bone cement or IFD is in place.
- S-IPNs ofthe present invention include at least two components.
- the first component is a linear, hydrophobic biodegradable polymer, preferably a homopolymer or copolymer which includes hydroxy acid and/or anhydride linkages or a linear, non-biodegradable hydrophilic polymer, preferably polyethylene oxide or polyethylene glycol.
- the second component is one or more crosslmkable monomers or macromers. At least one ofthe monomers or macromers includes a degradable linkage, preferably an anhydride linkage.
- the linear polymer preferably constituted between 10 and 90% by weight ofthe composition, more preferably between 30 and 70% ofthe composition.
- the crosslinked polymer preferably constitutes between about 30 and 70% by weight ofthe semi- interpenetrating network composition, more preferably, between 40 and 60 percent ofthe composition, with the balance being excipients, therapeutic agents, and other components.
- the compositions form semi-interpenetrating polymer networks when these components are mixed, and the crosslmkable component is crosslinlced.
- Semi- interpenetrating networks are defined as compositions that include two independent components, where one component is a crosslinked polymer and the other component is a non-crosslinked polymer.
- S-IPN compositions can have a viscosity before crosslinking anywhere between a viscous liquid suitable for injection to a moldable, paste-like putty.
- the viscosity can be adjusted by adding reactive diluents and/or by adding appropriate solvents.
- the compositions When crosslinked, however, the compositions are solid semi- interpenetrating networks, which are capable of supporting, bone growth and repair.
- Linear polymers are defined as homopolymers or block copolymers that are not crosslinked.
- Hydrophobic polymers are well known to those of skill in the art.
- Biodegradable polymers are those that have a half-life under physiological conditions of between about two hours and one year, preferably less than six months, more preferably, less than three months.
- biodegradable polymers examples include polyanhydrides, polyorthoesters, polyhydroxy acids, polydioxanones, polycarbonates, and polyaminocarbonates.
- Preferred polymers are polyhydroxy acids and polyanhydrides.
- Polyanhydrides are the most preferred polymers.
- Linear, hydrophilic polymers are well known to those of skill in the art.
- Non- biodegradable polymers are those that have a half-life longer than approximately one year under physiological conditions.
- suitable hydrophilic non- biodegradable polymers include poly(ethylene glycol), poly(ethylene oxide), partially or fully hydrolyzed poly(vinyl alcohol), poly(ethylene oxide)-co- poly(propylene oxide) block copolymers (poloxamers and meroxapols) and poloxamines.
- Preferred polymers are poly( ethylene glycol), poloxamines, poloxamers and meroxapols.
- Poly(ethylene glycol) is the most preferred polymer.
- the composition includes one or more monomers or macromers. However, at least one ofthe monomers or macromers includes an anhydride linkage. Other monomers or macromers that can be used include biocompatible monomers and macromers, wliich include at least one free-radical polymerizable group. For example, polymers including ethylenically unsaturated groups, which can be photochemically crosslinked, may be used, as disclosed in WO 93/17669 by the Board of Regents, University of Texas System, the entire teachings of which are incorporated by reference. i some embodiments, the cross-linking polymer ofthe S-IPN comprises a fumarate, preferably polypropylene fumarate.
- the non-cross-linkable polymer of an S-IPN may also be referred to as a host polymer.
- the host polymer for the S-IPN is selected from the group consisting of polylactic acid, polyglycolic acid, and their copolymers.
- the present inventors have observed that both Hao and Timmer report significantly greater mechanical properties and resistance to degradation when the host polymer is cross linked by a monomer having the same repeating unit as the host polymer.
- the cross-linkable compound in the S-IPN is cross- linked by N-vinyl pyrrolidone, polyethylene glycol dimethacrylate (PEG-DMA), ethylene dimethacrylate (EDMA), 2-hydroxyethyl methacrylate (HEMA) or methylmethacrylate (MMA).
- a photopolymerized anhydride is used as the matrix material. These materials are characterized as being strong (compressive strength 30-40 MPa), and relatively stiff (tensile modulus of about 600 MPA to about 1400 MPa).
- A.K. Burkoth, Biomaterials (2000) 27:2395-2404 discloses a number of photopolymerizable anhydrides as suitable for orthopaedic use.
- the repeating unit of these anhydrides comprises a pair of diacid molecules linked by anhydride bonds that are susceptible to hydrolysis. Because the diacid molecules are hydrophobic, there is a limited diffusion of water into the polymer, and so the polymer is subject only to surface degradation (not bulk degradation). This is advantageous because the strength ofthe polymer will essentially correspond to the mass ofthe polymer.
- the photopolymerized anhydride is selected from the group consisting of polymers of methacrylated sebacic acid (MSA), methacrylated l,6-fe(p-carboxyphenoxy) hexane (MCPH), l,3-t>w(p-carboxyphenoxy) propane (CPP), methacrylated cholesterol (MC), methacrylated stearic acid (MstA) and blends and copolymers therefrom.
- MSA methacrylated sebacic acid
- MCPH methacrylated l,6-fe(p-carboxyphenoxy) hexane
- CPP methacrylated propane
- MC methacrylated cholesterol
- MstA methacrylated stearic acid
- the photopolymerization is carried out by adapting a light source to the distal end ofthe delivery cannula that enters the disc space.
- a photo-optic cable is used to transmit light energy into the precursor components that have been deposited in the disc space.
- light is transmitted through the skin (i.e, transcutaneously) or through the annulus fibrosus.
- a photobleaching initiating system is used.
- a linear polyanhydride is first dissolved in a monomer, and then photopolymerized to form a S-IPN of a photopolymerized anhydride.
- the load bearing composition ofthe present invention comprises a S-IPN comprising a photopolymerized anhydride.
- poly (1,6 -bis (p-carboxyphenoxy)hexane (PCPH) is used. This polymer has a degradation of about 496 days, and so is desirably used as the load bearing composition in a strut ofthe present invention.
- Photoinitiators that generate an active species on exposure to UV light are well known to those of skill in the art. Active species can also be formed in a relatively mild manner from photon absorption of certain dyes and chemical compounds. These groups can be polymerized using photoinitiators that generate active species upon exposure to UV light, or, preferably, using long-wavelength ultraviolet light (LWUV) or visible light. LWUV and visible light are preferred because they cause less damage to tissue and other biological materials than UV light.
- Useful photoinitiators are those, which can be used to initiate polymerization ofthe macromers without cytotoxicity and within a short time frame, minutes at most and most preferably seconds.
- Exposure of dyes and co-catalysts such as amines to visible or LWUV light can generate active species. Light absorption by the dye causes the dye to assume a triplet state, and the triplet state subsequently reacts with the amine to form an active species, which initiates polymerization. Polymerization can be initiated by irradiation with light at a wavelength of between about 200-700 nm, most preferably in the long wavelength ultraviolet range or visible range, 320 nm or higher, and most preferably between about 365 and 514 nm.
- dyes can be used for photopolymerization. Suitable dyes are well known to those of skill in the art. Preferred dyes include erythrosin, phloxime, rose bengal, thonine, camphorquinone, ethyl eosin, eosin, methylene blue, riboflavin, 2,2- dimethyl-2-phenylacetophenone, 2-methoxy-2-phenylacetophenone, 2,2-dimethoxy- 2-phenyl acetophenone, other acetophenone derivatives, and camphorquinone.
- Suitable cocatalysts include amines such as N-methyl diethanolamine, N,N-dimethyl benzylamine, triethanol amine, triethylamine, dibenzyl amine, N- benzylethanolamine, N-isopropyl benzylamine. Triethanolamine is a preferred cocatalyst.
- Photopolymerization of these polymer solutions is based on the discovery that combinations of polymers and photoinitiators (in a concentration not toxic to the cells, less than 0.1% by weight, more preferably between 0.05 and 0.01% by weight percent initiator) will crosslink upon exposure to light equivalent to between one and three mWatts/cm.sup.2 applied to the skin of nude mice.
- the matrix comprises a co-polymer having shape memory qualities.
- the shape memory polymer comprises a first crosslmkable monomer and a second monomer having shape memory qualities.
- the linear polyester has a molecular weight of at least 10,000.
- the first monomer is a linear polyester.
- the second shape memory monomer is n-butyl acrylate.
- cross-linking is induced without an initiator.
- the shape memory polymer comprises between about 70 wt % and about 90 wt % ofthe first crosslmkable monomer and between 10 and 30 wt% of the a second monomer having shape memory qualities.
- the shape memory polymer matrix has a compressive strength of at least 15 MPa. This would make it a suitable candidate as a load bearing composition in a strut ofthe present invention.
- polylactic acid is the first linear polyester. It is believed that polylactic acid would provide a strong, stiffer matrix, more suitable for use as a load bearing composition in the strut ofthe present invention.
- the S-IPN comprises: a) a first part comprising a first bioerodible polymer capable of producing acidic products upon hydrolytic degradation, and b) a second part comprising a second bioerodible scaffolding polymer, which upon crosslinking provides a biopolymeric scaffolding or internal reinforcement for the S-IPN, and a crosslinking agent for the second bioerodible scaffolding polymer.
- the S-IPN comprises: a) a first part comprising a first bioerodible polymer capable of producing acidic products upon hydrolytic degradation, a crosslinking initiator, and preferably, a therapeutically effective amount of a biologically active or therapeutic agent and a combination of citric acid and sodium bicarbonate; and b) a second part comprising a second bioerodible scaffolding polymer, which upon crosslinking provides a biopolymeric scaffolding or internal reinforcement for the S-IPN, and a crosslinking agent for said second bioerodible scaffolding polymer.
- the resorbable materials are believed to have only moderate strength and stiffness. Therefore, it may be desirable to increase the strength and stiffness ofthe strut's matrix material by adding reinforcements to the matrix.
- the fibers can be made of non-resorbable materials (such as chopped carbon fibers), preferably the reinforcements are made of materials that are also resorbable.
- the fiber comprises carbon fiber.
- carbon fiber comprises between about 1 vol % and about 60 vol % (more preferably, between about 10 vol %> and about 50 vol%) ofthe load bearing composition, h some embodiments, the polymer and carbon fibers are homogeneously mixed.
- the material is a laminate.
- the carbon fiber is present as chopped state.
- the chopped carbon fibers have a median length of between 1 mm and 12 mm, more preferably between about 4.5 mm and about 7.5 mm.
- the carbon fiber is present as continuous strands.
- Biodegradable polymers are known, commercially available, or can be synthesized into fibers using known and published methods.
- polymers useful in the present invention include poly(L-lactic acid), poly(D,L-lactic acid), poly(D L-lactic-co-glycolic acid), poly(glycolic acid), poly(epsilon-caprolactone), polyorthoesters, and polyanhydrides. These polymers may be obtained in or prepared to the molecular weights and molecular weight distribution needed for service as either the matrix polymer or the pore-forming polymer by processes known in the art. Preferred polymers are poly(alpha-hydroxy esters). Suitable solvent systems are known in the art and are published in standard textbooks and publications. See, for example, Lange's Handbook of Chemistry, Thirteenth Edition, John A.
- polymers may be formed into fibers and webs by standard processing techniques including melt extrusion and spin casting, and are commercially available in woven or non-woven form.
- p-dioxanone fibers are used as the reinforcing phase ofthe strut. These fibers are advantageous because the high melting point of p- dioxanone resists any thermal degradation ofthe fibers during injection into the disc space.
- the strut compositions comprise aliphatic polyesters reinforced with p-dioxanone fibers. In more preferred embodiments, those compositions disclosed in U.S. Patent No. 6,147,135 by Yuan (hereinafter "Yuan”), the specification of which is incorporated herein by reference in its entirety, are selected. ⁇
- both the osetobiologic composition and the strut are bioresorbable.
- the selection of a bioresorbable strut is advantageous because it reduces the amount of foreign materials left in the body.
- load-bearing component is used alone.
- the strut material can also include bone growth materials, such as growth factors and stem cells that promote bone growth upon eventual resorption of the resorbable strut.
- bone growth materials such as growth factors and stem cells that promote bone growth upon eventual resorption of the resorbable strut.
- stem cells must typically be housed in an aqueous phase (such as a hydrogel)
- the inclusion of stem cells likely requires the introduction of a porosity into the strut that may significantly degrade the strength of the strut.
- the primary purpose ofthe strut is to support the disc space while the osteogeneic composition promotes fusion, adding stem cells to the strut composition may not be fully desirable in all circumstances. Therefore, in preferred embodiments, only growth factors are added to the strut composition.
- the growth factors are first provided in an aqueous solution and particles ofthe resorbable strut material are added to the solution. The growth factors cling to the outer surface ofthe particles. Next, the growth factor- laden particles are separated from the growth factor solution. Next, the growth factor-laden particles are added to the viscous resorbable material.
- the device of the present invention has at least one of the following characteristics:
- the material comprising the strut ofthe present invention has at least one ofthe following intrinsic properties:
- the strut device ofthe present invention has at least one ofthe following mechanical performance characteristics: Mechanical Property Preferred Value More Preferred Value
- the arcuate shape has a thickness (t) of 3 mm, inner radius (r;) of 22 mm, an outer radius (r 0 ) of 25 mm and an average height if 15 mm.
- the novel struts ofthe present invention can be used with conventional osteobiologic materials, such as platelet-rich plasma (PRP), allograft particles (such as demineralized bone matrix (DBM) and cancellous chips) and autograft.
- conventional osteobiologic materials such as platelet-rich plasma (PRP), allograft particles (such as demineralized bone matrix (DBM) and cancellous chips) and autograft.
- the osteobiologic component of the present invention acts in a manner similar to the cancellous core of a vertebral body. Desirable features for the osteobiologic composition ofthe strut are as follows:
- the in-situ formed osteobiologic composition comprises: a) a matrix material (preferably, a polymer flowable at between 40 °C and 80 °C; a linear anhydride, or a fumarate, b) osteogenenic component (preferably, mesenchymal stem cells present in a concentrated amount), and c) an osteoinductive factors (preferably, a bone morphogenetic protein).
- a matrix material preferably, a polymer flowable at between 40 °C and 80 °C; a linear anhydride, or a fumarate
- osteogenenic component preferably, mesenchymal stem cells present in a concentrated amount
- an osteoinductive factors preferably, a bone morphogenetic protein
- calcium phosphate such as, for example, hydroxyapatite or tri-calcium phosphate
- polylactic acid polyglycolic acid
- polygalactic acid polycaprolactone
- polyethylene oxide polypropylene oxide
- polysulfone polyethylene
- polypropylene polysulfone
- polyethylene polypropylene
- hyaluronic acid which may be purified with or without crosslinking, bioglass, gelatin and collagen.
- the matrix is a resorbable composition that resorbs within a 2-4 month time period after in-situ formation and comprises: a) a polymer phase that flows or softens at a temperature of between 40 °C and 80 °C (more preferably, comprising an aliphatic polyester such as polycaprolactone) and is preferably present in an amount of between 50 vol% and 70 vol% ofthe osteobiologic composition, and b) an osteoconductive calcium phosphate phase (more preferably hydroxyapatite) preferably present in an amount of between 10 vol% and 30 vol% ofthe osteobiologic composition.
- a polymer phase that flows or softens at a temperature of between 40 °C and 80 °C (more preferably, comprising an aliphatic polyester such as polycaprolactone) and is preferably present in an amount of between 50 vol% and 70 vol% ofthe osteobiologic composition
- an osteoconductive calcium phosphate phase more preferably hydroxyapatite
- a reinforcing phase (preferably, resorbable polymeric chopped fiber) is also preferably present in an amount of between about 10 vol % and about 30 vol % ofthe osteobiologic composition.
- the osteogenic component comprises an aqueous phase
- the aqueous phase is present as an interconnected phase throughout the osetobiologic composition, and is present in an amount of between about 25 vol % and about 35 vol % ofthe osteobiologic composition and has an average diameter of between 100 and 250 ⁇ m.
- the osteoinductive factor is selected from the group consisting of a bone morphogenetic protein and a transforming growth factor. More preferably, the osteoinductive factor is a bone morphogenetic protein.
- the bone morphogenetic protein may be present in any phase of the osteobiologic composition. When immediate delivery ofthe bone morphogenetic protein is desirable, the bone morphogenetic protein is present in the hydrogel phase. When intermediate delivery of the bone morphogenetic protein is desirable, the bone morphogenetic protein is present in the polymer phase. When long term delivery ofthe bone morphogenetic protein is desirable, the bone morphogenetic protein is present in the ceramic phase. It is preferable to have at least twice the autologous level of bone morphogenetic protein, and more preferably, at least 10 times the autologous level of bone morphogenetic protein.
- the matrix comprises a material having a melting point between about 42 °C and about 95 °C , (preferably between about 42 °C and about 90 °C) which allows it to be flowed into the disc space without causing tissue necrosis, and then in-situ solidified to provide the needed structural support.
- the scaffold material further comprises a porogen that allows it to be made into a porous scaffold by conventional leaching techniques.
- growth factors and osteoprogenitor cells such as mesenchy nal stem cells can be flowed through the open porosity ofthe scaffold to induce bone growth throughout the scaffold.
- mesenchymnal stem cells are isolated from a bone marrow aspirate taken from the patient and incorporated into bioabsorbable particles capable of maintaining cell viability, such as hydrogels.
- the hydrogels will absorb quickly such that the cells will be released to form bone.
- the particulate are then mixed with a scaffold material in a first liquid form that will solidify upon implantation.
- the scaffold material resorbs slowly such that bone can be formed throughout the porosity before the scaffold degrades away.
- Preferred scaffold materials are polymers that can be dissolved in a cell-friendly solvent such as dimethyl sulfoxide (DMSO), which will leach out once implanted, causing the polymer to precipitate out of solution and create a solid scaffold.
- DMSO dimethyl sulfoxide
- a growth/nutritive factor cocktail for inducing the osteoprogenitor cells to form bone and continue to support the bone formation process is incorporated into the cell-seeded hydrogel as well as the scaffold material. Following disc space preparation the system is injected to the disc space and no other surgical steps are required.
- a growth/nutritive factor cocktail for inducing the osteoprogenitor cells to form bone and continue to support the bone formation process is incorporated into the cell-seeded hydrogel as well as the scaffold material. Following disc space preparation the system is injected to the disc space and no other surgical steps are required.
- intervertebral fusion device comprising: a) a porous scaffold having a porosity suitable for new bone formation, b) viable osteoprogenitor cells, and c) osteoinductive factors required to signal the osteoprogenitor cells to form new bone.
- Porous scaffolds that can form upon injection through a minimally invasive surgical procedure can be made of a material selected from the group consisting of crosslinlced natural and synthetic polymers, low melting point polymers, polymers dissolved in biocompatible solvents, and setting ceramics.
- Porous scaffolds suitable for use in the present invention are disclosed in U.S. Patent Nos. 6,280,474 and 6,264,695 (swellable polymers), U.S. Patent No. 5888220
- the resorbable polymers, calcium phosphates and reinforcing phases disclosed above in the description ofthe strut may be used to form the preferred matrix.
- the matrix is substantially weaker (owing to the presence of either open porosity or an interconnected hydrogel phase) than the strut, and hydrolyzes quicker.
- the matrix has a first absorbable phase of about 1 weight percent to about 99 weight percent of any ofthe aliphatic homopolyesters of ⁇ -caprolactone, p-dioxanone, or trimethylene carbonate or copolymers or mixtures thereof, with the remaining resorbable phase comprising a bone osteoconductive or osteoinductive calcium containing, non-fibrous, powdered compound, preferably a calcium phosphate such as hydroxyapatite, tri- or tetra- calcium phosphate, or a bioactive glass, or mixtures thereof.
- a bone osteoconductive or osteoinductive calcium containing, non-fibrous, powdered compound preferably a calcium phosphate such as hydroxyapatite, tri- or tetra- calcium phosphate, or a bioactive glass, or mixtures thereof.
- the matrix has a first absorbable phase of about 1 weight percent to about 99 weight percent of aliphatic copolyesters of p-dioxanone or trimethylene carbonate, and glycolide or lactide or mixtures thereof, and in particular, copolymers of p-dioxanone/glycolide, p- dioxanone/lactide, trimethylene carbonate/glycolide and trimethylene carbonate/lactide, with a remaining resorbable phase comprising a bone osteoconductive or osteoinductive calcium containing, non-fibrous, powdered compound, preferably a calcium phosphate such as hydroxyapatite, tri- or terra- calcium phosphate, or a bioactive glass, or mixtures thereof.
- a bone osteoconductive or osteoinductive calcium containing, non-fibrous, powdered compound preferably a calcium phosphate such as hydroxyapatite, tri- or terra- calcium phosphate, or a bioactive glass, or mixtures thereof.
- the matrix has a first absorbable phase of about 1 weight percent to about 99 weight percent of aliphatic copolyesters of e-caprolactone and glycolide or mixtures thereof, or mixtures of homopolymers of e-caprolactone and lactide, with a remaining resorbable phase comprising a bone osteoconductive or osteoinductive calcium containing, non-fibrous, powdered compound, preferably a calcium phosphate such as hydroxyapatite, tri- or terra- calcium phosphate, or a bioactive glass, or mixtures thereof.
- a bone osteoconductive or osteoinductive calcium containing, non-fibrous, powdered compound preferably a calcium phosphate such as hydroxyapatite, tri- or terra- calcium phosphate, or a bioactive glass, or mixtures thereof.
- the above-noted matrices will contain sufficient amounts ofthe absorbable polymer phase and sufficient amounts ofthe resorbable second bone regenerating phase to effectively function as bone cements or bone substitutes.
- the composites will contain about 1 to about 99 weight percent of polymer phase, and more preferably about 5 to about 95 weight percent.
- the composites will typically contain about 1 to about 99 weight percent ofthe bone regenerating phase, and more preferably about 5 to about 95 weight percent.
- the relative amounts of the first absorbable, polymeric phase to the second resorbable phase in the above- noted matrices will depend upon various parameters including, inter alia, the levels of strength, stiffness, and other physical and thermal properties, absorption and resorption rates, setting and hardening rates, deliverability, etc., which are required.
- the desired properties ofthe composites ofthe present invention and their level of requirement will depend upon the body structure area where the bone cement or substitute is needed. Accordingly, the composites ofthe present invention will typically contain about 1 weight percent to about 99 weight percent, and more preferably about 5 weight percent to about 95 weight percent of aliphatic polyester homo- or co-polymers, or blends thereof.
- a further aspect ofthe present invention is a process by which the matrix component ofthe osteobiologic composition is prepared.
- the matrix can be prepared by a one-step or a two-step process in which a bone regenerating material is mixed in the reaction vessel with a just-formed polymer (one-step process), or mixed with a pre-formed polymer in a separate vessel (two-step process).
- the composites ofthe present invention can be manufactured in the following two-step process.
- the preformed polymers and bone regenerating materials are individually charged into a conventional mixing vessel having a conventional mixing device mounted therein such as an impeller.
- the polymers and bone substitutes are mixed at a temperature of about 150 °C to about 220 °C, more preferably about 160 °C to about 200 °C, for about 5 to about 90 minutes, more preferably for about 10 to about 45 minutes, until a uniformly dispersed composite is obtained.
- the composite is further processed by removing it from the mixing device, cooling to room temperature, grinding, and drying under pressures below atmospheric at elevated temperatures for a period of time.
- the composites can be prepared by a one-step process by charging the bone regenerating material to a reaction vessel which contains the just-formed polymers. Then, the polymers and bone substitutes are mixed at a temperature of about 150 °C to about 220 °C, more preferably about 160 °C to about 200 °C, for about 5 to about 90 minutes, more preferably for about 10 to about 45 minutes, until a uniformly dispersed composite is obtained. Then, the composite is further processed by removing it from the mixing vessel, cooling to room temperature, grinding, and drying under pressures below atmospheric at elevated temperatures for a period of time.
- the matrix ofthe present invention includes a bone implant material, which can be readily molded at a selected temperature at or below about 60 °C.
- the material is formed as a cohesive mixture of hard filler particles and a binder composed of a biocompatible, biodegradable thermoplastic polymer having fluid-flow properties at the selected temperature at or below about 60 °C.
- Any hard biocompatible filler particles including autogenous bone chips, can be used in this invention.
- hydroxyapatite is a preferred filler for its permanance and biological profile. Tricalcium phosphate and glass granules may also be used alone or in combination with hydroxyapatite, particularly if some degree of resorption is desired in the filler.
- the binder preferably ranges in fluid-flow properties (flowability) between a highly viscous fluid and a putty-like semi-solid, at the selected temperature. With too low a binder viscosity, the implant material suffers the same problems seen in loose-particle implants: poor shape retention, once molded, and poor cohesiveness, leading to exfoliation of particles before or during the tissue ingrowth period, hi a preferred embodiment, the polymer includes polylactic acid having a molecular weight between about 400 and about 5,000 daltons. The binder preferably constitutes no more than about one-third ofthe total solid volume ofthe material, leaving void space in the material, wliich can accommodate tissue ingrowth.
- the minimum amount of binder is that necessary to give easy formability and provide sufficient particle cohesion and shape retention during the period of tissue ingrowth.
- polylactic acid having progressively greater molecular weights between about 2,000 and about 5,000 daltons were prepared and tested for binder characteristics when formulated with hydroxyapatite particles. Above about 2,000 daltons, the implant material was quite hard and difficult to mold by hand at 40 °C, and at 5,000 daltons, temperatures up to about 60 °C were required to achieve moldability.
- the binder from above is mixed with hydroxyapatite particles, and the components are thoroughly blended.
- the material contains some void space, to allow tissue ingrowth independent of polymer breakdown. Since the void space of a mass of spherical particles is about one-third that ofthe particle mass, the implant material preferably contains less than about one-third by volume of binder.
- the minimum amount of binder needed to produce good particle cohesiveness typically between about 5% and 20% ofthe total solid volume ofthe material, is added, hi one embodiment, implant material containing 80% hydroxyapatite particles (average particle size of about 650 microns), and 20%> of polylactic acid polymer having average polymer molecular weights of about 1,100 daltons was prepared. The material was easily moldable by hand at 50 °C, and showed good cohesiveness and shape retention at 37 °C. h practicing the invention, there is provided a moldable hydroxyapatite bone- implant material. As described above, implant material having a range of molding temperatures and biodegradability can be provided, by adjusting the composition and amount of binder in the material.
- Material having a relatively high molding temperature e.g., between about 40 °C to about 60 °C, is generally preferred where the implant needs to be in a relatively rigid condition during the process of tissue ingrowth, for example, to prevent significant shape deformation.
- the material is applied and shaped to the bone site in a heated state; after cooling, it assumes the desired rigid condition.
- the material can be formulated with thermoplastic polymer binders of various composition and molecular weights, to achieve a selected molding temperature, rigidity in the bone site, and rate of binder breakdown. By varying the relative proportions of binder and particles, selected changes in the void space and cohesiveness ofthe material are possible.
- Matrix scaffold polymers can also be produced by first dissolving the polymer in a biocompatible, water-soluble solvent, injecting the material into the disc space, and then allowing the solvent to leach out ofthe polymer into the body, thereby causing the polymer to solidify in vivo.
- Suitable polymers compatible with such solvents include, but are not limited to, poly(lactic acid), poly(glycolic acid) and copolymers therefrom.
- Suitable biocompatible, water-soluble solvents include dimethylsulfoxide (DMSO).
- DMSO dimethylsulfoxide
- the volume ratio of polymer to solvent is at least 1 :5, more preferably at least 1 :2.
- injectable ceramics can also serve as components in the matrix ofthe osteobiologic component.
- Preferred injectable, resorbable ceramics are amorphous calcium phosphates or hydroxyapatites. (See U.S. patent 6,214,368 and 6,331,312, the entire teachings of which are incorporated herein by reference.)
- porosity is produced in the matrix to produce a porous scaffold material.
- the surgeon can then inject an osteogenic component (such as mesenchymnal stem cells) or an osteoinductive component (such as bone morphogenetic protein) into the porosity, thereby enhancing the ostobiologic nature ofthe composition.
- an osteogenic component such as mesenchymnal stem cells
- an osteoinductive component such as bone morphogenetic protein
- the matrix ofthe osteobiologic composition to comprise materials such as polymers that flow at temperatures only well above body temperature.
- materials such as polymers that flow at temperatures only well above body temperature.
- many polymers such as polycaprolactone flow at about 60 °C, a temperature that may well destroy the viability of mesenchymnal stem cells contained within the flowable polymer.
- polymeric materials that become flowable above 45 °C are first made flowable by raising their temperature to at least 45 °C, the flowable polymer is then injected into the disc space, the in-situ formed material is then made porous, and porous material is then injected with mesenchymnal stem cells.
- in-situ porosity is accomplished by first delivering the matrix material into the disc space as beads, then tightly packing the beads within the disc space, and then bonding the beads, preferably by heat bonding, into a stable structure.
- porosity is produced in the matrix to including a foaming agent in the matrix material.
- porous injectable graft materials are optionally made by adding a degradable gas-producing compound. As gas bubbles are produced from the gas-producing compound, pores are formed in the bone-like materials. The size ofthe pores are preferably controlled by adjusting the amount of gas-producing compound and the viscosity ofthe mineral matrix in the fluid used to mix the materials.
- sodium bicarbonate and/or calcium bicarbonate is added to the flowable matrix material and a precise amount of acid (e.g. citric acid, formic, acetic, phosphoric acids, hydrochloric acid) is added to the mixing fluid.
- acid e.g. citric acid, formic, acetic, phosphoric acids, hydrochloric acid
- the acidity ofthe mixing fluid causes carbon dioxide to be released from the sodium bicarbonate, wherein the carbon dioxide ultimately forms pores in the matrix material
- hydrogen peroxide is combined with peroxidase in the graft material. The peroxidase releases oxygen from the hydrogen peroxide, which has the added advantage of sterilizing the wound site.
- in-situ porosity can be produced in the matrix material including a porogen with the matrix material, and then in-situ leaching out ofthe porogen.
- a porogen is a water-soluble materials.
- Biodegradable materials can be fabricated into three dimensional anatomical shapes having load bearing properties similar to or exceeding that of natural bone.
- a matrix component ofthe osteobiologic component has the capability of being rendered porous and can serve to foster bony fusion.
- the osteobiologic composition can be implanted without first being rendered to its porous state.
- Porosity can be achieved after implantation by a faster rate of biodegradation of a pore-forming component ofthe osteobiologic component relative to a slower rate of degradation ofthe matrix component ofthe osteobiologic component.
- the porous osteobiologic component has sufficient compressive strength and modulus to serve as a bone replacement prosthesis during that period wherein the body regenerates new natural bone within and to the shape ofthe osteobiologic component.
- the osteobiologic component is replaced by natural bone as the osteobiologic component biodegrades and by such process is displaced or eliminated from the body by natural processes.
- the osteobiologic composition comprises at least two components, a continuous matrix component and an included pore-forming component.
- the matrix component comprises a biodegradable material having a rate of degradation, which at least matches the rate at which the body regenerates natural bone tissue.
- the pore-forming component is a material, which differs from the matrix material such that it may be differentiated from the matrix component and ultimately be removed therefrom by differential dissolution or biodegradation to provide porosity to the prosthetic template either prior to or after implantation. Unless wholly removed from the matrix polymer ofthe implant before implantation, the molecular weight, molecular weight distribution and degree of crystallinity ofthe pore-forming polymer is also of significant concern.
- the pore-forming polymer should biodegrade and/or bioresorb at a rate that is at least four times greater than that ofthe matrix polymer. Further, the pore-forming polymer should have a polydispersity index of at least 3 to provide for a controlled degradation over a period of time that avoids intolerable localized pH concentrations due to its degradation by-products.
- the osteobiologic compositions of these embodiments can contain a relatively high ultimate porosity capacity. That is, the osteobiologic composition is fabricated in a manner, wliich results in an osteobiologic component capable of being rendered highly porous prior to implantation.
- the matrix may be formed around included particles or fibers which particles or fibers are subsequently removed from the matrix by solvent dissolution or other methods of degradation, leaving a highly porous matrix scaffold structure.
- the particles or fibers embedded within the formed matrix may be retained in the osteobiologic composition for dissolution or degradation in situ after implantation.
- portions ofthe pore-creating material may be removed prior to implantation ofthe osteobiologic composition providing a range of actual to ultimate porosities ofthe implantable osteobiologic components.
- the ultimate porosity capacity may be defined as the percent porosity ofthe matrix after at least 90% ofthe pore forming material has been removed from the template, either in vitro or in vivo.
- the ultimate porosity capacity ofthe biodegradable/bioresorbable osteobiologic component be in the range of between about 20% and about 50% volume ofthe osteobiologic component.
- the biodegradable osteobiologic composition of the present invention which has the porogen features described above, including high mechanical strength necessary for replacement of load bearing bones, high ultimate porosity capacity to permit bony fission therethrough, and a rate of degradation approximately matching the rate of new tissue growth may, for example, be formed by the methods described below.
- these osteobiologic compositions ofthe present invention are formed by distributing within a polymeric matrix a pore-creating substance (or "porogen"). Regardless ofthe specific methods used to form the osteobiologic composition, the product will include a three-dimensional, anatomically-shaped osteobiologic composition having a high ultimate porosity capacity due to the presence of a pore creating substance dispersed within the matrix.
- the pore creating substance may be formed for example of salts, polysaccharides, protein, polymers other than the matrix polymers, or other nontoxic materials such as gelatin which are, for example, soluble in a solvent which does not dissolve the matrix polymer; made fluid at a higher glass transition temperature (Tg) or melting temperature (Tm) than the matrix polymer; or otherwise differentiated from the matrix polymer so as to retain an independent structure from the polymeric matrix.
- Tg glass transition temperature
- Tm melting temperature
- the temperature required to fluidize polymers is that which permits non- hindered flow of polymer chains.
- this "flow temperature” is the glass transition temperature (Tg).
- this "flow temperature” is the melting temperature (Tm).
- flow temperature is meant to be that temperature which permits non-hindered flow of polymer chains and includes, as appropriate, Tg for amorphous polymers and Tm for at least semi-crystalline polymers.
- the pore creating substance may be in the form of particles such as salt, which after forming a matrix in which the particles have been included, the particles are leached out or otherwise removed from the matrix leaving a polymeric matrix with high porosity.
- the pore creating substance may be in the form of fibers such as polymeric fibers or webs dispersed within a formed polymeric matrix.
- the dispersed fibers and the surrounding matrix possess differential rates of degradation, with the fibers being degraded at a faster rate than the matrix, thereby being removed from the osteobiologic composition and creating a highly porous polymeric, osteobiologic composition.
- the porogen-containing osteobiologic composition may be formed by dispersing the pore-creating substance in a body of powdered polymer.
- the pore-creating substance is a first polymer in fiber or web form dispersed in a body of powdered second polymer.
- the second polymer has a lower flow temperature (Tf) such that when the dispersion is heated above the flow temperature ofthe powder, the powder is fluid, but the dispersed fibers are not.
- the fluid polymer is next solidified, e.g., by permitting the dispersion to return to ambient temperature, resulting in a polymeric matrix having entrapped therein the pore- forming substance.
- a first polymer is used to form the matrix and a second polymer is used to form the pore-creating substance dispersed within the first polymer.
- Both first and second polymers are biodegradable but the second degrades at a faster rate than the first polymer, e.g., approximately two to eight times faster, and preferably about four times faster creating the desired porous body for ingrowth and proliferation of cells.
- poly(glycolic acid) (PGA) fiber meshes may be dispersed within poly(L-lactic acid) (PLLA). Upon curing ofthe PLLA matrix, the PGA fiber mesh is embedded within the PLLA matrix. The PGA fibers biodegrade at a more rapid rate than PLLA, thus creating a template having a high ultimate porosity capacity.
- the pore creating substance may be formed of a low molecular weight polymer while the matrix is formed of a high molecular weight polymer. Because the low molecular weight polymers degrade at a faster rate than the high molecular weight polymers an implant having a desired rate of degradation of each ofthe pore creating substance and the matrix can be formed.
- the pore-creating substance in vivo degradation ofthe pore-creating substance at a faster rate than the template matrix, such as PGA fibers which degrade within months of implantation in a PLLA matrix which may take more than one year to degrade, permits gradual replacement ofthe pore-creating substance with growing bone cells.
- the resorbing pore-creating substance is gradually replaced with newly formed bone tissue, maintaining a mechanically strong bone prosthesis.
- the more slowly degrading polymeric matrix is then resorbed and replaced with bone tissue proliferating from the network of growing tissue already present throughout the prosthetic template.
- the matrix has a sufficient number of pores or passageways so that the total accessible surface area ofthe substrate is at least five times greater than a solid object having' the same external dimensions.
- the preferred total surface area can be achieved by using a substrate, which comprises a mass of powder, a mass of granules, a mass of fibers, or a highly porous block of substrate material.
- a substrate which comprises a mass of powder, a mass of granules, a mass of fibers, or a highly porous block of substrate material.
- the average pore size in the matrix is greater that 20 ⁇ m, more preferably greater than 50 ⁇ m, more preferably greater than 100 ⁇ m. In some embodiments, the pore size is between about 100 ⁇ m and 250 ⁇ m.
- the osteobiologic compositions ofthe present invention have a high ultimate porosity capacity, resulting in a highly porous matrix containing a uniformly distributed and interconnected pore structure.
- Pore volume ofthe porous osetobiologic composition is approximately 20% to 90%, and the average pore diameter is approximately 50 to 250 ⁇ m.
- the pore volume and diameter also directly relate to the rate of tissue ingrowth and matrix degradation.
- the porous matrix ofthe present invention accommodates large number of cells adhering to the matrix, permits cells to be easily distributed throughout the template, and allows an organized network of tissue constituents to be formed.
- the matrix preferably promotes cell adhesion and permits the attached cells to retain differentiated cell function.
- the leachate produces an open porosity having an average pore size of between 20 ⁇ m and 500 ⁇ m, preferably 50-250 ⁇ m. This range is preferred for bone growth.
- the matrices ofthe osteobioloigic component are fabricated of polymers and by methods which result in implants which are capable of being rendered porous for tissue ingrowth while retaining sufficient mechanical , strength to be suitable for supporting a disc space.
- the osteobiologic compositions ofthe present invention possess a compressive strength of approximately 5 MPa to 50 MPa and a compressive modulus of approximately 50 MPa to 500 MPa as tested by an h stron Materials Testing Machine according to American Society for Testing and Materials (ASTM) Standard F451-86.
- the values of 5 MPa compressive strength and 50 MPa compressive modulus correspond to the mid-range values for human trabecular bone.
- the biodegradable, bioresorbable matrices ofthe present invention preferably are formed of polymeric materials, the matrix polymer having a rate of degradation which is matched to the rate of tissue in-growth.
- the matrix polymeric substance preferably ranges in weight average molecular weight from approximately 50,000 to 200,000. Crystallinity ofthe matrix polymer of implant is approximately 0 to 25%).
- the molecular weight and molecular weight distribution ofthe matrix polymer is related to the rate at which the matrix biodegrades. hi a matrix of broad molecular weight distribution, e.g., having a polydispersity index (Mw/Mn) greater than 2 fractions ofthe material exist in short to long polymeric chains.
- the polydispersity index of the matrix is preferably in the range of 3-6.
- mesenchymnal stem cells are then delivered into the porous matrix.
- the mesenchymnal stem cells are delivered into the porosity ofthe scaffold by simply directing an aqueous solution containing mesenchymnal stem cells into the scaffold.
- an additional cannula can be placed near the porous matrix to serve as an exit cannula for the fluid.
- a hydrophilic matrix material such as polylactic acid may be used, h these instances, it has been found that mesenchymnal stem cells do not tenaciously adhere to the surface ofthe polylactic acid.
- a lining material such as hydroxyapatite (HA) may be used to line the inner surface ofthe scaffold with a material to which mesenchymnal stem cells more tenaciously adhere.
- HA hydroxyapatite
- the linings disclosed in U.S. Patent No. 5,133,755 by Brekke, the entire teachings of which are incorporated herein by reference (hereinafter "Brekke") are selected.
- cell adhesion molecules may be bound to the inner surface ofthe matrix in order to enhance the adhesion ofthe mesenchymnal stem cells to the scaffold.
- cell adhesion molecules refers collectively to laminins, fibronectin, vitronectin, vascular cell adhesion molecules (V-CAM), intercellular adhesion molecules (I-CAM), tenascin, thrombospondin, osteonectin, osteopontin, bone sialoprotein, and collagens.
- the mesenchymnal stem cells are delivered into the in-situ porosity under pressure, such as by injection.
- the envelope is the strut component having a 360 degree span.
- the envelope can be an inflatable device component ofthe osteobiologic composition.
- it may be useful to create in-situ porosity it may sometimes be problematic to evenly distribute the mesenchymnal stem cells throughout the in-situ created porosity under normal injection pressures.
- the mesenchymnal stem cells are delivered into the in-situ porosity under a higher pressure that is sufficient to fill 90 %> ofthe porosity.
- the pressure is high enough to completely fill the porosity.
- a method delivering an osteogenic component comprising the steps of: a) injecting an osteobiologic composition into a disc space, b) creating in-situ porosity in the osteobiologic component, and c) delivering an osteogenic component into the in-situ porosity under a pressure of at least sufficient to fill at least 90 % ofthe porosity.
- the osteobiologic component ofthe present invention further comprises a gelled aqueous phase, wherein viable mesenchymnal stem cells are located in the aqueous phase.
- mesenchymnal stem cells and many growth factors are very heat sensitive, it is desirable to deliver mesenchymnal stem cells and growth factors at or near body temperature.
- many ofthe bioabsorbable polymers are flowable at temperatures well in excess of body temperature.
- many cross-linked polymers experience an exotherm of over 100 °C. It is not known whether mesenchymnal stem cells and growth factors could remain viable after prolonged exposure to these temperatures.
- calcium phosphate can be made flowable at body temperature, it is desirable to select an osteobiologic composition having a matrix comprising calcium phosphate when also choosing to deliver the mesenchymnal stem cells or growth factors to the disc space during the delivery ofthe matrix component ofthe osteobiologic composition.
- an osteobiologic composition that is flowable at body temperature, the composition comprising a matrix comprising calcium phosphate and an osteogenic component.
- Hydrogels are useful in this respect because they can adequately protect bone growth cells contained therein.
- a “hydrogel” is a substance formed when an organic polymer (natural or synthetic) is set or solidified to create a three- dimensional open-lattice structure that entraps molecules of water or other solution to form a gel.
- the solidification can occur, e.g., by aggregation, coagulation, hydrophobic interactions, or cross-linking.
- the hydrogels employed in this invention rapidly solidify to keep the cells at the application site, thereby el ninating problems of phagocytosis or cellular death and enhancing new cell growth at the application site.
- the hydrogels are also biocompatible, e.g., not toxic, to cells suspended in the hydrogel.
- a “hydrogel-cell composition” is a suspension of a hydrogel containing desired tissue precursor cells. These cells can be isolated directly from a tissue source or can be obtained from a cell culture.
- a “tissue” is a collection or aggregation of particular cells embedded within its natural matrix, wherein the natural matrix is produced by the particular living cells.
- the hydrogel-cell composition forms a uniform distribution of cells with a well-defined and precisely controllable density. Moreover, the hydrogel can support very large densities of cells, e.g., 50 million cells/ml. These factors improve the quality and strength ofthe new tissue, h addition, the hydrogel allows diffusion of nutrients and waste products to, and away from, the cells, which promotes tissue growth.
- Hydrogels suitable for use in the osteobiologic composition ofthe present invention are water-containing gels, i.e., polymers characterized by hydrophilicity and insolubility in water. See, for instance, "Hydrogels", pages 458-459 in Concise Encyclopedia of Polymer Science and Engineering, Eds. Mark et al, Wiley and Sons, 1990, the disclosure of which is incorporated herein by reference. Although their use is optional in the present invention, the inclusion of hydrogels is highly preferred since they tend to contribute a number of desirable qualities.
- hydrogels generally can: a) house mesenchymal stems cells, b) assist the cured composite with load bearing capabilities ofthe cured composite, and c) decrease frictional forces on the composite and add thermal elasticity.
- Suitable hydrogels generally exhibit an optimal combination of such properties as compatibility with the matrix polymer of choice, and biocompatability.
- the hydrogel phase is preferably between about 50 and about 90 volume percent ofthe total volume, more preferably between about 70 and about 85 volume percent.
- the osteobiologic component is a stand-alone component (i.e., there is essentially no strut)
- the osetobiologic composition will preferably contain a hydrogel phase at a concentration of between about 15 and 50 volume percent, and preferably between about 20 and about 30 volume percent of the osteobiologic composition.
- the lower levels ofthe hydrogel phase provide additional opportunity to use a strong matrix in the osteobiologic component.
- Polymer-hydrogel composites demonstrate an optimal combination of physical chemical properties, particularly in terms of their conformational stability, resorption characteristics, biocompatability, and physical performance, e.g., physical properties such as density, thickness, and surface roughness, and mechanical properties such as load-bearing strength, tensile strength, static shear strength, fatigue ofthe anchor points, impact absorption, wear characteristics, and surface abrasion.
- an unsupported hydrogel is not sufficiently stiff or strong to survive the high spinal loads experienced during the fusion process.
- the hydrogel is supported not only by the strut component ofthe present invention, but also by the matrix component of the osteobiologic component, hi these cases, the hydrogel is either delivered into the disc space along with the matrix component (as is preferred when the matrix component ofthe osteobiologic component comprises CaPO 4 ), or is delivered after in-situ porosity has been produced in the matrix component ofthe osteobiologic component (as with flowable polymers).
- the strut component ofthe present invention may span a sufficiently large portion ofthe disc space and have sufficient stiffness to adequately support and contain the hydrogel phase within the disc space without the need of a supplemental matrix in the osetobiologic component.
- the strut component preferably describes an arc of at least 200 degrees about the disc space, more preferably at least 270 degrees, more preferably at least 350 degrees, and most preferably is about 360 degrees.
- Such struts are exemplified in FIGs. 2 (a) through (e), FIGs. 4 (a) and (b) and FIGs. 5 (a) and (b).
- an intervertebral body fusion device comprising: a) an in situ produced load bearing strut having a shape that spans at least 200 degrees, and b) an osteobiologic component consisting essentially of: -an aqueous phase comprising an osteogenic component.
- the hydrogel can include any ofthe following: polysaccharides, proteins, polyphosphazenes, poly(oxyethylene)-poly(oxypropylene) block polymers, poly(oxyethylene)-poly(oxypropylene) block polymers of ethylene diamine, poly(acrylic acids), poly(methacrylic acids), copolymers of acrylic acid and methacrylic acid, poly( vinyl acetate), and sulfonated polymers.
- these polymers are at least partially soluble in aqueous solutions, e.g., water, or aqueous alcohol solutions that have charged side groups, or a monovalent ionic salt thereof.
- acidic groups include carboxylic acid groups, sulfonic acid groups, and halogenated (preferably fluorinated) alcohol groups.
- polymers with basic side groups that can react with anions are poly(vinyl amines), poly(vinyl pyridine), and poly(vinyl imidazole).
- Water soluble polymers with charged side groups are cross-linked by reacting the polymer with an aqueous solution containing multivalent ions ofthe opposite charge, either multivalent cations if the polymer has acidic side groups, or multivalent anions if the polymer has basic side groups.
- Cations for cross-linlcing the polymers with acidic side groups to form a hydrogel include divalent and trivalent cations such as copper, calcium, aluminum, magnesium, and strontium. Aqueous solutions ofthe salts of these cations are added to the polymers to form soft, highly swollen hydrogels.
- Anions for cross-linking the polymers to form a hydrogel include divalent and trivalent anions such as low molecular weight dicarboxylate ions, terepthalate ions, sulfate ions, and carbonate ions. Aqueous solutions ofthe salts of these anions are added to the polymers to form soft, highly swollen hydrogels, as described with respect to cations.
- a useful polymer size in the hydrogel is in the range of between 10,000 D and 18,500 D. Smaller polymers result in gels of higher density with smaller pores.
- Ionic polysaccharides such as alginates or chitosan
- the hydrogel is produced by cross-linking the anionic salt of alginic acid, a carbohydrate polymer isolated from seaweed, with ions, such as calcium cations.
- the strength ofthe hydrogel increases with either increasing concentrations of calcium ions or alginate.
- U.S. Pat. No. 4,352,883 describes the ionic cross-linking of alginate with divalent cations, in water, at room temperature, to form a hydrogel matrix. Tissue precursor cells are mixed with an alginate solution, the solution is delivered to an already implanted support structure and then solidifies in a short time due to the presence in vivo of physiological concentrations of calcium ions.
- the solution is delivered to the support structure prior to implantation and solidified in an external solution containing calcium ions.
- the hydrogel comprises alginate. Alginate can be gelled under mild conditions, allowing cell immobilization with little damage.
- Binding of Mg 2+ and monovalent ions to alginate does not induce gelation of alginate in aqueous solution.
- exposure of alginate to soluble calcium leads to a preferential binding of calcium and subsequent gelling.
- These gentle gelling conditions are in contrast to the large temperature or solvent changes typically required to induce similar phase changes in most materials.
- Alginates have been utilized as immobilization matrices for cell, as an injectable matrix for engineering cartilaginous tissue to treat vesicoureteral reflux in various animal models, and as injectable microcapsules containing islet cells to treat animal models of diabetes.
- alginate membrane can be modified by incorporating other polymeric elements (e.g., lysine, poly(ethylene glycol), poly( vinyl alcohol) or chitosan). These modified systems have been used to control the release of proteins from alginate beads.
- Haemostatic swabs made of calcium alginate have also been clinically utilized to reduce blood loss during surgical procedures.
- the calcium ions in alginate may assist the blood clotting process by activating platelets and clotting factor VII.
- CoUagen-polysaccharide-hydroxyapatite compositions suitable for a matrix of the present invention have been disclosed by Liu in U.S . Patent No. 5,972,385, the entire teachings of which are incorporated herein by reference.
- a polysaccharide is reacted with an oxidizing agent to open sugar rings on the polysaccharide to form aldehyde groups.
- the aldehyde groups are reacted to form covalent linkages to collagen.
- polysaccharides which can be used include hyaluronic acid, chondroitin sulfate, dermatan sulfate, keratan sulfate, heparan, heparan sulfate, dextran, dextran sulfate, alginate, and other long chain polysaccharides.
- the polysaccharide is hyaluronic acid.
- a crosslinked collagen-polysaccharide matrix ofthe present invention may be used alone to conduct the growth of tissue; in combination with a growth factor to induce the growth of tissue; in combination with fibrin to anchor the matrix into sites of tissue defect, or in combination with both growth factor and fibrin.
- the method of making a collagen-polysaccharide matrix ofthe present invention comprises the steps of oxidizing an exogenous polysaccharide to form a modified exogenous polysaccharide having aldehyde groups, and reacting the modified exogenous polysaccharide with collagen under conditions such that the aldehyde groups covalently react with collagen to form a crosslinlced matrix.
- the method may further comprise the step of adding a growth factor to the matrix.
- a growth factor can be added before or after the step of reacting the modified polysaccharide with the collagen.
- the fibrin used in a crosslinked collagen-polysaccharide matrix ofthe present invention is prepared by contacting a preformed matrix with a source of fibrinogen and thrombin or by combining the fibrinogen and thrombin with the modified exogenous polysaccharide and collagen at the time of reaction.
- fibrinogen and thrombin in a collagen polysaccharide matrix may be added to another preformed collagen polysaccharide matrix. Therefore, the present invention also comprises a method for preparing a crosslinlced collagen-polysaccharide matrix comprising fibrin.
- the hydrogel comprises a microbial polysaccharide.
- Microbial polysaccharides are ubiquitous in nature and very abundant biopolymers. They are of interest because of their unusual and useful functional properties. Some of these properties are summarized as follows: (i) film-forming and gel-forming capabilities, (ii) stability over broad temperature ranges, (iii) biocompatibility (natural products avoid the release/leaching of toxic metals, residual chemicals, catalyst, or additives), (iv) unusual rheological properties, (v) biodegradability, (vi) water solubility in the native state or reduced solubility if chemically modified, and (vii) thermal processability for some of these polymers. It is worthy to note that gellan, one ofthe microbial polysaccharides, has been investigated as immobilization materials for enzymes and cells.
- the hydrogel is a synthetic hydrogel.
- One synthetic hydrogel is polyphosphazene.
- Polyphosphazenes contain inorganic backbones comprised of alternating single and double bonds between nitrogen and phosphorus atoms, in contrast to the carbon-carbon backbone in most other polymers.
- the uniqueness of polyphosphazenes stems from the combination of this inorganic backbone with versatile side chain functionalities that can be tailored for different applications.
- the degradation of polyphosphazenes results in the release of phosphate and ammonium ions along with the side groups.
- Linear, uncross-linlced polymers such as polyphosphazenes can be prepared by thermal ring opening polymerization of (NPC1 2 ) 3 and the chloro group replaced by amines, alkoxides or organometallic reagents to form hydrolytically stable, high molecular weight poly(organophosphazenes).
- the polyphosphazenes can be hydrophobic, hydrophilic or amphiphihc.
- the polymers can be fabricated into films, membranes and hydrogels for biomedical applications by cross-linking or grafting.
- Bioerodible polymers for drug delivery devices have been prepared by incorporating hydrolytic side chains of imidazole for skeletal tissue regeneration.
- Polyphosphazenes are polymers with backbones consisting of nitrogen and phosphorous atoms separated by alternating single and double bonds. Each phosphorous atom is covalently bonded to two side chains. Polyphosphazenes that can be used have a majority of side chains that are acidic and capable of forming salt bridges with di- or trivalent cations. Examples of acidic side chains are carboxylic acid groups and sulfonic acid groups.
- Bioerodible polyphosphazenes have at least two differing types of side chains, acidic side groups capable of forming salt bridges with multivalent cations, and side groups that hydrolyze under in vivo conditions, e.g., imidazole groups, amino acid esters, glycerol, and glucosyl.
- Bioerodible or biodegradable polymers i.e., polymers that dissolve or degrade within a period that is acceptable in the desired application (usually in vivo therapy), will degrade in less than about five years and most preferably in less than about one year, once exposed to a physiological solution of pH 6-8 having a temperature of between about 25 °C. and 38 °C. Hydrolysis ofthe side chain results in erosion ofthe polymer. Examples of hydrolyzing side chains are unsubstituted and substituted imidizoles and amino acid esters in which the side chain is bonded to the phosphorous atom through an amino linkage.
- PVA is not synthesized directly but is the deacetylated product of poly(vinyl acetate).
- Polyvinyl acetate is usually prepared by radical polymerization of vinyl acetate (bulk, solution or emulsion polymerizations).
- PVA is formed by either alcoholysis, hydrolysis or aminolysis processes of poly(vinyl acetate).
- the hydrophilicity and water solubility of PVA can be readily controlled by the extent of hydrolysis and molecular weight.
- PVA has been widely used as thickening and wetting agent.
- PVA gels can be prepared by cross-linking with formaldehyde in the presence of sulfuric acid. These formaldehyde-cross-linked PVA materials have been used as prosthesis for a variety of plastic surgery applications including breast augmentation, diaphragm replacement and bone replacement. However, a variety of complications were found after long term implantation, including calcification ofthe PVA. More recently, PVA was made into an insoluble gel using a physical cross- linking process. These gels were prepared with a repeated freezing-thawing process. This causes structural densification ofthe hydrogel due to the formation of semicrystalline structures. The use of this gel in drag delivery applications has been reported. However, PVA is not truly biodegradable due to the lack of labile bonds within the polymer bond. Only low molecular weight materials are advisable to be used as implant materials.
- PEO polyethylene oxide
- PEO polyethylene oxide
- PEO can be produced by the anionic or cationic polymerization of ethylene oxide using a variety of initiators.
- PEO is highly hydrophilic and biocompatible, and has been utilized in a variety of biomedical applications including preparation of biologically relevant conjugates, induction of cell membrane fusion and surface modification of biomaterials.
- Different polymer architectures have been synthesized and some of their applications in medicine have been recently reviewed.
- PEO can be made into hydrogels by ⁇ -ray or electron beam irradiation and chemical crosslinking. These hydrogels have been used as matrices for drag delivery and cell adhesion studies.
- Pluronic polyols or polyoxamers are block copolymers of PEO and poly(propylene oxide) and are usually synthesized by anionic polymerization in the form of an ABA triblock using a difunctional initiator.
- Pluronics F 127 which contains 70% ethylene oxide and 30% propylene oxide by weight with an average molecular weight of 11,500, is the most commonly used gel-forming polymer matrix to deliver proteins. This polymer exhibits a reversible thermal gelation in aqueous solutions at a concentration of 20% or more. Thus, the polymer solution is a liquid at room temperature but gels rapidly in the body. Although the polymer is not degraded by the body, the gels dissolve slowly and the polymer is eventually cleared. This polymer has been utilized in protein delivery and skin burn treatments.
- PGA is not water soluble
- bioerodible hydrogels based on photopolymerized PGA-PEO copolymers have been synthesized and their biological activities investigated. Macromonomers having a poly(ethylene glycol) central block, extended with oligomers of .alpha. -hydroxy acids (e.g., oligo(dl-lactic acid) or oligo(glycolic acid)) and terminated with acrylate groups were synthesized. These hydrogels were designed to form direct contacts with tissues or proteins following photopolymerization, and act as a barrier.
- the degradation rate of these gels could be tailored from less than 1 day to 4 months by appropriate choice ofthe oligo(.alpha. -hydroxy acid).
- the macromonomer could be polymerized using non-toxic photoinitiators with visible light without excess heating or local toxicity.
- the hydrogels polymerized in contact with tissue adhere tightly to the underlying tissue. In contrast, the gels were nonadhesive if they were polymerized prior to contact with tissue.
- hydrogels that can be used in the methods ofthe invention are solidified by either visible or ultraviolet light.
- These hydrogels are made of macromers including a water soluble region, a biodegradable region, and at least two polymerizable regions as described in U.S. Pat. No. 5,410,016, the entire teachings of which are incorporated herein by reference.
- the hydrogel can begin with a biodegradable, polymerizable macromer including a core, an extension on each end ofthe core, and an end cap on each extension.
- the core is a hydrophilic polymer
- the extensions are biodegradable polymers
- the end caps are oligomers capable of cross-linking the macromers upon exposure to visible or ultraviolet light, e.g., long wavelength ultraviolet light.
- Examples of such light solidified hydrogels include polyethylene oxide block copolymers, polyethylene glycol polylactic acid copolymers with acrylate end groups, and 10 K polyethylene glycol-glycolide copolymer capped by an acrylate at both ends.
- the copolymers comprising these hydrogels can be manipulated by standard techniques to modify their physical properties such as rate of degradation, differences in crystallinity, and degree of rigidity. It is known that stem cells are fairly sensitive to temperatures greatly in excess of body temperature.
- the osteobiologic composition is delivered into the disc space at a temperature of between about 37 °C and about 60 °C, preferably between about 40 °C and about 50 °C, more preferably between about 40 °C and about 45 °C.
- a semipermeable membrane is formed around the hydrogel to protect the cells inside.
- the instant invention provides a method of encapsulating bone growth cells or growth factors in a semipermeable membrane.
- the basic approach involves suspending the bone growth cells or growth factors to be encapsulated in a physiologically compatible medium containing a water-soluble substance that can be made insoluble in water, that is, gelled, to provide a temporary protective environment for the tissue.
- the medium is next formed into droplets containing the bone growth cells or growth factors and gelled, for example, by changing conditions of temperature, pH, or ionic environment.
- the "temporary capsules" thereby produced are then subjected to a treatment, which can be a known treatment, that results in the production of membranes of a controlled permeability (including impermeability) about the shape-retaining temporary capsules.
- the temporary capsules can be fabricated from any nontoxic, water soluble substance that can be gelled to form a shape retaining mass by a change of conditions in the medium in which it is placed, and also may comprise plural groups that are readily ionized to form anionic or cationic groups. The presence of such groups in the polymer enables surface layers ofthe capsule to be cross-linked to produce a "permanent" membrane when exposed to polymers containing multiple functionalities ofthe opposite charge.
- the presently preferred material for forming the temporary capsules is polysaccharide gums, either natural or synthetic, ofthe type which can be (a) gelled to form a shape retaining mass by being exposed to a change in conditions such as a pH change or by being exposed to multivalent cations such as Ca " * "4" ; and (b) permanently "crosslinked” or hardened by polymers containing reactive groups such as amine or imine groups which can react with acidic polysaccharide constituents.
- the presently preferred gum is alkali metal alginate.
- Other water soluble gums which may be used include guar gum, gum arabic, carrageenan, pectin, tragacanth gum, xanthan gum or acidic fractions thereof.
- gelatin or agar When encapsulating thermally refractory materials, gelatin or agar may be used in place ofthe gums.
- the preferred method of formation ofthe droplets is to force the gum- nutrient-tissue suspension through a vibrating capillary tube placed within the center ofthe vortex created by rapidly stirring a solution of a multivalent cation. Droplets ejected from the tip ofthe capillary immediately contact the solution and gel as spheroidal shaped bodies.
- the preferred method of forming a permanent semipermeable membrane about the temporary capsules is to "crosslink" surface layers of a gelled gum ofthe type having free acid groups with polymers containing acid reactive groups such as amine or imine groups. This is typically done in a dilute solution ofthe selected polymer.
- the lower the molecular weight ofthe polymer the greater the penetration into the surface ofthe temporary capsule, and the greater the penetration, the less permeable the resulting membrane.
- Permanent crosslinks are produced as a consequence of salt formation between the acid reactive groups ofthe crosslinking polymer and the acid groups ofthe polysaccharide gum.
- semipermeability can be controlled by setting the molecular weight ofthe crosslinking polymer, its concentration, and the duration of reaction.
- Crosslinking polymers which have been used with success include polyethylenimine and polylysine. Molecular weight can vary, depending on the degree of permeability required, between about 3,000 and about 100,000 or more. Good results have been obtained using polymers having an average molecular weight on the order of about 35,000.
- the capsules can be engineered to have a selected in vivo useful life by astute selection ofthe cross-linking polymer.
- Proteins or polypeptide crosslinkers e.g., polylysine
- Cross-linkers not readily degradable in mammalian bodies, e.g., polyethyleneimine, result in longer lasting membranes.
- the temporary capsules it is possible to improve mass transfer within the capsule after formation ofthe permanent membrane by re-establishing the conditions under which the material is liquid, e.g., removing the multivalent cation. This can be done by ion exchange, e.g., immersion in phosphate buffered saline or citrate buffer. In some situations, such as where it is desired to preserve the encapsulated tissue, or where the temporary gelled capsule is permeable, it may be preferable to leave the encapsulated gum in the crosslinked, gelled state.
- An alternative method of membrane formation involves an interfacial polycondensation of polyaddition.
- This approach involves preparing a suspension of temporary capsules in an aqueous solution ofthe water soluble reactant of a pair of complementary monomers which can form a polymer. Thereafter, the aqueous phase is suspended in a hydrophobic liquid in which the complementary reactant is soluble. When the second reactant is added to the two-phase system, polymerization takes place at the interface. Permeability can be controlled by controlling the makeup ofthe hydrophobic solvent and the concentration ofthe reactants. Still another way to form a semipermeable membrane is to include a quantity of protein in the temporary capsule which can thereafter be crosslinked in surface layers by exposure to a solution of a crossliriking agent such as gluteraldehyde.
- a crossliriking agent such as gluteraldehyde.
- the foregoing process has been used to encapsulate viable mesenchymal stems cells which, in a medium containing the nutrients and other materials necessary to maintain viability and support in vitro metabolism ofthe tissue, provide bone growth.
- the instant invention provides a tissue implantation method which does not require surgery and which overcomes many ofthe problems of immune rejection, hi accordance with the invention, the capsules are injected into a suitable site in a mammalian body, and function normally until the tissue expires, or until natural body processes succeed in isolating the capsules so that substances required for viability ofthe tissue are no longer available. At this point, because surgery is not required for the implant, fresh tissue may be readily provided by another injection. The mammalian body may accordingly be provided with the specialized function ofthe tissue as long as desired.
- mammalian mesenchymal stems cells are encapsulated in polylysine and polyethyleneimine cross-linked alginate membranes. These may be injected into the polymer matrix ofthe osteobiologic component.
- Another objects ofthe invention are to provide a method of implanting living tissue in mammalian bodies and to provide a non-surgical tissue implantation technique. Still another object is to provide a method of encapsulating living tissue which allows the production of capsules having a high surface area to volume ratio and membranes with a preselected in vivo residence time.
- IPNs and S-IPNs are extremely desirable because cells can be suspended in the polymer solutions which can be cross-linked by a non-toxic active species, such as by photoinitiation.
- both the active species and the initiator are present in an amount that is non-toxic to cells, hi other embodiments, the active species is present in an amount that is non-toxic to cells and the initiation occurs via photoinitiation.
- Cells can be obtained directed from a donor, from cell culture of cells from a donor, or from established cell culture lines, hi the preferred embodiments, cells are obtained directly from a donor, washed and implanted directly in combination with the polymeric material. The cells are cultured using techniques known to those skilled in the art of tissue culture.
- Cell attachment and viability can be assessed using scanning electron microscopy, histology, and quantitative assessment with radioisotopes.
- the function ofthe implanted cells can be determined using a combination ofthe above- techniques and functional assays. For example, in the case of hepatocytes, in vivo liver function studies can be performed by placing a cannula into the recipient's common bile duct. Bile can then be collected in increments.
- Bile pigments can be analyzed by high pressure liquid chromatography looking for underivatized tetrapyrroles or by thin layer chromatography after being converted to azodipyrroles by reaction with diazotized azodipyrroles ethylanthranilate either with or without treatment with P-glucuronidase.
- Diconjugated and monoconjugated bilirubin can also be determined by thin layer chromatography after alkalinemethanolysis of conjugated bile pigments, hi general, as the number of functioning transplanted hepatocytes increases, the levels of conjugated bilirubin will increase. Simple liver function tests can also be done on blood samples, such as albumin production.
- Analogous organ function studies can be conducted using techniques known to those skilled in the art, as required to determine the extent of cell function after implantation.
- islet cells ofthe pancreas maybe delivered in a similar fashion to that specifically used to implant hepatocytes, to achieve glucose regulation by appropriate secretion of insulin to cure diabetes.
- Other endocrine tissues can also be implanted.
- Studies using labeled glucose as well as studies using protein assays can be performed to quantitate cell mass on the polymer scaffolds. These studies of cell mass can then be correlated with cell functional studies to determine what the appropriate cell mass is.
- function is defined as providing appropriate structural support for the surrounding attached tissues.
- This technique can be used to provide multiple cell types, including genetically altered cells, within a three-dimensional scaffolding for the efficient transfer of large number of cells and the promotion of transplant engraftment for the purpose of creating a new tissue or tissue equivalent. It can also be used for immunoprotection of cell transplants while a new tissue or tissue equivalent is growing by excluding the host immune system.
- the osteobiologic component comprises an osteoconductive phase.
- the osteoconductive phase comprises a particulate phase comprising a hard tissue, osteoconductive or osteoinductive calcium containing, non-fibrous, powdered compound, wherein the calcium containing compound comprises a material having the formula:
- M and N are alkali or alkaline earth metals, preferably calcium, magnesium, sodium, zinc and potassium.
- ZO 4 is an acid radical, where Z is preferably phosphorus, arsenic, vanadium, sulfur or silicon, or is substituted in whole or part with carbonate (CO 3 2" .
- Y is an anion, preferably halide, hydroxide, or carbonate.
- the calcium containing compound comprises mono-, di-, octa-, .alpha. -tri-, .beta.-tri-, or tetra-calcium phosphate, hydroxyapatite, fluorapatite, calcium sulfate, calcium fluoride and mixtures thereof.
- the calcium containing bone regenerating compound can also contain a bioactive glass comprising metal oxides such as calcium oxide, silicon dioxide, sodium oxide, phosphorus pentoxide, and mixtures thereof, and the like.
- the calcium containing compound used in the composites ofthe present invention will have a particle size of about 10 microns to about 1000 microns, and most preferably about 100 microns to about 500 microns.
- the particles are prepared by conventional processes such as pulverizing, milling, and the like.
- hydroxyapatite particles are preferably the type of dry free-flowing hydroxyapatite particles supplied for use in forming wetted, loose-mass implants, and can be obtained commercially from Orthomatrix Corporation (Dublin, CA) or Calcitek (San Diego, CA). Particle sizes of between about 250 and 2000 microns are preferred, smaller particles showing increased difficulty in allowing tissue ingrowth and larger particles requiring increased quantities of binder for ease of application.
- the material comprising the osteobiologic component ofthe present invention has at least one ofthe following intrinsic properties:
- the osteobiologic component ofthe present invention has the following mechanical performance characteristics:
- the polymer has a Tm of no more than about 80 °C.
- the polymer has a Tm of less than 100 °C, and so is less likely to damage surrounding tissue.
- preferred embodiments in the solidifed form, exhibit mechanical properties approximating those ofthe cancellous bone.
- preferred embodiments ofthe osetobiologic composition exhibit a load bearing strength of between about 50 and about 200 psi (pounds per square inch), and preferably between about 100 and about 150 psi.
- Such composites also exhibit a shear stress of between about 10 and 100 psi, and preferably between about 30 and 50 psi, as such units are typically determined in the evaluation of natural tissue and joints.
- growth factors encompasses any cellular product that modulates the growth or differentiation of other cells, particularly connective tissue progenitor cells.
- the growth factors that may be used in accordance with the present invention include, but are not limited to, FGF- 1 , FGF-2, FGF-4, PDGFs, EGFs, IGFs, PDGF-bb, bone morphogenetic protein- 1, bone morphogenetic protein- 2, OP-1, transforming growth factor- ⁇ , osteoid-inducing factor (OIF), angiogenin(s), endothelins, hepatocyte growth factor and keratinocyte growth factor, osteogenin (bone morphogenetic protefn-3); bone morphogenetic protein-2; OP-1; bone morphogenetic protein-2A, -2B, and -7; transforming growth factor- ⁇ , HBGF-1 and -2; isoforms of platelet-derived growth factors (PDGF), fibroblast growth factors, epithelial growth factors, isoforms of
- Growth factors which can be used with a matrix ofthe present invention include, but are not limited to, members ofthe transforming growth factor- ⁇ superfamily, including transforming growth factor- ⁇ 1,2 and 3, the bone morphogenetic proteins (BMP's), the growth differentiation factors(GDF's), and ADMP-1; members ofthe fibroblast growth factor family, including acidic and basic fibroblast growth factor (FGF-1 and -2); members ofthe hedgehog family of proteins, including indian, sonic and desert hedgehog; members ofthe insulin-like growth factor (IGF) family, including IGF-I and -II; members ofthe platelet-derived growth factor (PDGF) family, including PDGF-AB, PDGF-BB and PDGF-AA; members ofthe interleulcin (IL) family, including IL-1 thru -6; and members ofthe colony-stimulating factor (CSF) family, including CSF-1, G-CSF, and GM-CSF.
- BMP's bone morphogenetic proteins
- GDF's
- osteogenic components and osteoinductive components in a heated polymer matrix may render nonviable or denature these components.
- growth factors known to those skilled in the art that are more heat resistant than the majority of growth factors. It is believed that these high temperature growth factors in osteobiologic compositions may be included in osteobiologic compositions that are to be flowed into the disc space at temperatures between body temperature and about 45 °C.
- the present invention is a pharmaceutical composition
- a pharmaceutically acceptable carrier or diluent and (a) at least one polymer flowable between 38 °C and 45 °C selected from the group consisting of homopolymers of poly(e-caprolactone), poly(p-dioxanone), or poly(trimethylene carbonate) or copolymers or mixtures thereof, or copolyesters of p-dioxanone or trimethylene carbonate and glycolide or lactide or mixtures thereof, and in particular, copolymers of p-dioxanone/glycolide, p-dioxanone/lactide, trimethylene carbonate/glycolide and trimethylene carbonate/lactide, or copolyesters of .epsilon.-caprolactone and glycolide or mixtures thereof, or mixtures of homopolymers of e-caprolactone and lactide, and (b) at least one growth factor resistant to denatur
- a "pharmaceutical composition” is a formulation comprising the disclosed compounds and a pharmaceutically acceptable diluent or carrier, in a form suitable for administration to a subject.
- the quantity of active ingredient (e.g. a growth factor) in a unit dose of composition is an effective amount and may be varied according to the particular treatment involved.
- an "effective amount" of a compound is the quantity which, when administered to a subject in need of treatment, improves the prognosis ofthe subject, e.g. reduces the severity of one or more ofthe subject's symptoms associated with a spinal injury. It may be appreciated that it may be necessary to make routine variations to the dosage depending on the age and condition ofthe patient.
- the amount ofthe active ingredient to be administered to a subject will depend on the type of injury and the characteristics ofthe subject, such as general health, other diseases, age, sex, genotype, body weight and tolerance to drags. The skilled artisan will be able to determine appropriate dosages depending on these and other factors.
- the compounds described herein can be used in pharmaceutical preparations in combination with a pharmaceutically acceptable carrier or diluent.
- suitable pharmaceutically acceptable carriers include inert solid fillers or diluents and sterile aqueous or organic solutions.
- the compounds will be present in such pharmaceutical compositions in amounts sufficient to provide the desired dosage amount in the range described herein. Techniques for formulation and administration of the compounds of the instant invention can be found in
- the matrix material becomes flowable in the temperature range of at least 40 °C and 55 °C, more preferably in the temperature range of at least 45 °C and 50 °C.
- the growth factor is resistant to denaturing at a temperature of at least 40 °C.
- the growth factor is a dimer.
- the growth factor is a bone morphogenetic protein dimer.
- substances such as antibiotics, antibacterial agents, and antifungal agents may also be admixed with the polymer.
- antimicrobial agents which may be employed include tetracycline, oxytetracycline, chlorotetracycline, neomycin, erithromycin, and its derivative, bacitracin, streptomycin, rifampicin and its derivatives such as N-dimethylrifampicin, kanamycin and chloromycetin.
- Useful antifungal agents include griseofulvin, mycostatin, miconazole and its derivatives as described in U.S. Pat. No.
- cetyl trimethyl ammonium bromide as well as benzethonium chloride and methylbenzethonium chloride such as described in U.S. Pat. Nos.
- the matrix has antibodies that have affinity for connective tissue progenitor stem cells bound to the surface thereof.
- Suitable antibodies include by way of example, STRO-1, SH-2, SH-3, SH-4, SB-10, SB-20, and antibodies to alkaline phosphatase.
- STRO-1, SH-2, SH-3, SH-4, SB-10, SB-20 antibodies to alkaline phosphatase.
- Such antibodies are described in Haynesworth et al., Bone (1992),13:69-80; Bruder, S. et al, Trans Ortho Res Soc (1996), 27:574; Haynesworth, S.
- Mac Phee discloses that drugs, polyclonal and monoclonal antibodies and other compounds, including, but not limited to, DBM and bone mo ⁇ hogenetic proteins may be added to the matrix, such as a matrix ofthe present invention. They accelerate wound healing, combat infection, neoplasia, and/or other disease processes, mediate or enhance the activity ofthe growth factor in the matrix, and/or interfere with matrix components which inhibit the activities ofthe growth factor in the matrix.
- antibiotics such as tetracycline and ciprofloxacin
- antiproliferative/cytotoxic drags such as 5- fluorouracil (5-FU), taxol and/or taxotere
- antivirals such as gangcyclovir, zidovudine, amantidine, vidarabine, ribaravin, trifluridine, acyclovir, dideoxyuridine and antibodies to viral components or gene products
- cytokines such as ⁇ - or ⁇ - or ⁇ -hiterferon, ⁇ - or ⁇ -tumor necrosis factor, and interleukins
- colony stimulating factors erythropoietin
- antifungals such as diflucan, ketaconizole and nystatin
- antiparasitic agents such as pentamidine
- anti-inflammatory agents such as ⁇ -1 - anti-trypsin and ⁇ -1-antichymotrypsin
- steroids anesthetic anesthetic agents
- Other compounds which may be added to the matrix include, but are not limited to: vitamins and other nutritional supplements; hormones; glycoproteins; fibronectin; peptides and proteins; carbohydrates (both simple and/or complex); proteoglycans; antiangiogenins; antigens; oligonucleotides (sense and/or antisense DNA and/or RNA); bone mo ⁇ hogenetic proteins; DBM; antibodies (for example, to infectious agents, tumors, drugs or hormones); and gene therapy reagents. Genetically altered cells and/or other cells may also be included in the matrix of this invention. If desired, substances such as pain killers and narcotics may also be admixed with the polymer for delivery and release to the disc space.
- the additive is embedded within the matrix material ofthe scaffold.
- the additive resides on the inner surface ofthe open porosity created by the leaching ofthe leachate.
- the additive resides within the hydrogel phase.
- the osteobiologic composition comprises one or more bone mo ⁇ hogenetic proteins
- they are preferably located on the inner surface ofthe open porosity in the case where the scaffold is formed prior to being populated with cells, and are preferably located within the hydrogel phase in the case where a hydrogel is used to deliver cells at the same time the scaffold is delivered. This is done so that the cells will contact the bone mo ⁇ hogenetic proteins as soon as possible following implantation in order to initiate the bone forming process.
- the bone mo ⁇ hogenetic proteins have a limited time in which they are active in inducing cells to form bone, it is important to expose the cells to the bone mo ⁇ hogenetic proteins as soon as possible to take maximum advantage of their potency.
- osteoprogenitor cells When osteoprogenitor cells are seeded onto the scaffold following in situ formation ofthe scaffold, they preferably adhere to the surface ofthe inner porosity ofthe scaffold. This is important because osteoprogenitor cells must attach to a substrate in order to begin forming bone.
- osteoprogenitor cells are delivered to the fusion site while encapsulated in a hydrogel, they preferably attach to the inner porosity of the hydrogel.
- bone mo ⁇ hogenetic protein is present in the scaffold in a concentration of at least 2 times the atologus concentration. More preferably, the bone mo ⁇ hogenetic protein is present in the scaffold in a concentration of at least 100 times the autologous concentration.
- mesenchymnal stem cells are present in the scaffold in a concentration of at least 2 times the autologous concentration. More preferably the mesenchymnal stem cells are present in the scaffolding in a concentration of 10 times the autologous concentration, and most preferably they are present in a concentration of 100 times the autologous concentration.
- the osteobiologic composition has a sufficiently high osteobiologic nature and a matrix that is sufficiently resistant to degradation that the bone growth essentially fills the entire porosity ofthe scaffold ofthe osteobiologic composition before there is any significant degradation ofthe matrix.
- the new bone can begin to significiantly share the compressive load experienced by the device before the device undergoes a significant loss in strength.
- bony ingrowth penetrates at least 50% ofthe distance to the center ofthe implant before the matrix loses 50% of its weight
- bony ingrowth penetrates at least 75% ofthe distance to the center ofthe implant before the matrix loses 25% of its weight.
- bony ingrowth penetrates at least 90% ofthe distance to the center ofthe implant before the matrix loses 10% of its weight.
- bony ingrowth penetrates at least 50% ofthe distance to the center ofthe implant before the matrix loses 50% of its compressive strength
- bony ingrowth penetrates at least 75% of the distance to the center ofthe implant before the matrix loses 25% of its compressive strength.
- bony ingrowth penetrates at least 90%) ofthe distance to the center ofthe implant before the matrix loses 10% of its compressive strength.
- the injectable implants ofthe invention can be used to fuse facets and to fuse the interspinous region, hi some embodiments, the implants ofthe present invention use an elastomer to tension the interspinous region to correct lordotic angle.
- osteobiologic compositions can be advantageously used in vertebroplasty procedures, particularly when delivered into the porosity of a skeleton created in the vertebral body, as disclosed in U.S. Patent Application by Martin Reynolds entitled “Method of Performing Embolism Free Vertebroplasty and Devise Therefore,” which was filed on November 21, 2002, the entire teachings of which are inco ⁇ orated herein by reference.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space.
- the device comprises a strut.
- the strut includes an upper surface for bearing against the upper endplate, a lower surface for bearing against the lower endplate, and an in-situ formed load bearing composition disposed between the upper and lower surfaces.
- the present invention is an intervertebral fusion device comprising a strut, having a shape memory, and an in-situ formed osteobiologic component.
- the strut further includes (i) an upper surface for bearing against the upper endplate and (ii) a lower surface for bearing against the lower endplate.
- the ⁇ esent invention is an intervertebral fusion device comprising a strut and an in-situ formed osteobiologic component.
- the strut includes an upper surface for bearing against the upper endplate, and a lower surface for bearing against the lower endplate.
- the in-situ formed osteobiologic component includes a matrix component having an internal surface defining a scaffold having open porosity suitable for bone growth therethrough, and an osteogenic component located within the open porosity.
- the present invention is an intervertebral fusion device comprising a strut and an in-situ formed osteobiologic component.
- the strut includes an upper surface for bearing against the upper endplate, and a lower surface for bearing against the lower endplate.
- the in-situ formed osteobiologic component includes an injectable matrix component, and an osteoinductive component embedded within the matrix.
- the present invention is an intervertebral fusion device comprising a strut and an in-situ formed osteobiologic component.
- the strut includes an upper surface for bearing against the upper endplate, and a lower surface for bearing against the lower endplate.
- the in-situ formed osteobiologic component includes an injectable matrix component, and a porogen embedded within the matrix.
- the present invention is an intervertebral fusion device comprising a strut and an in-situ fonned osteobiologic component.
- the strut includes an upper surface for bearing against the upper endplate, and a lower surface for bearing against the lower endplate.
- the in-situ formed osteobiologic component includes an expandable device defining a cavity, and an injectable osteobiologic composition located within the cavity.
- the present invention is an intervertebral fusion device comprising a strut that includes an expandable device having a cavity, an upper surface for bearing against the upper endplate, a lower surface for bearing against the lower endplate, and an inner wall defining a through hole.
- the strut further includes an injectable load bearing composition located within the cavity.
- the fusuion device further includes an osteobiologic component located in the throughhole.
- the present invention is an intervertebral fusion device comprising a strut and an in-situ formed osteobiologic component.
- the strut includes an upper surface for bearing against the upper endplate a lower surface for bearing against the lower endplate.
- the in-situ formed osteobiologic component includes an injectable, matrix component essentially free of monomer.
- the present invention is an intervertebral fusion device for providing bony fusion across a disc space, comprising a strut.
- the strut includes an upper surface for bearing against the upper endplate, a lower surface for bearing against the lower endplate, and an in-situ formed load bearing composition disposed between the upper and lower surfaces and made of a material comprising a cross-linked resorbable polymer.
- the term "toroid" refers to a surface obtained by at least partially rotating a closed curve, which lies in a plane, about an axis parallel to the plane and which does not intersect the curve.
- An example of an "open cavity defined by an outer surface of a toroid" is a hole.
- the present invention is an intervertebral spinal fusion device comprising at least one arcuate inflatable balloon that upon expansion between two adjacent vertebrae at least partially restores natural a natural angle between two adjacent vertebrae, said device having a footprint that substantially co ⁇ esponds to a perimeter of a vertebral endplate.
- the intervertebral spinal fusion device has an upper area, a lower area, an anterior area and a posterior area.
- said device Upon inflation, said device can have a footprint that substantially corresponds to a rim of a vertebral endplate and said anterior area height being greater than said posterior area height. More preferably, upon expansion, at least a portion ofthe device has a generally toroidal shape thereby defining an open cavity having an axial dimension and a radial dimension.
- the device comprises at least one exandable balloon that contains a plurality of lumena.
- the device comprises at least one said balloon including a resorbable, semi-permeable material selected from the group consisting of polyolefin copolymers, polyethylene, polycarbonate, polyethylene terephthalate, ether-ketone polymers, woven fibers, nonwoven fibers, fabrics and metal mesh.
- the balloon defines at least one opening.
- the upper and lower areas ofthe device have a plurality of outward proj ections.
- the outward proj ections preferably include polyetherether ketone (PEEK).
- the upper area ofthe device can include at least one material selected from the group consisting of polyether block copolymer (PEBAX), ABS (acrylonitrile butadiene styrene), ANS (acrylonitrile styrene), delrin acetal; PVC (polyvinyl chloride), PEN (polyethylene napthalate), PBT (polybutylene terephthalate), polycarbonate, PEI (polyetherimide), PES (polyether sulfone), PET (polyethylene terephthalate), PETG (polyethylene terephthalate glycol), polyamide, aromatic polyamide, polyether, polyester, polymethylmethacrylate, polyurethane copolymer, ethylene vinyl acetate (EVA), ethylene vinyl alcohol, polyethylene, latex rubber, FEP (fluorinated ethylene polymer), PTFE (polytetrafluoroethylene), PFA (perfluoro-alkoxyalkane), polypropylene, polyole
- the device ofthe present invention has at least one balloon that contains at least one member ofthe group consisting of a load- bearing component and an osteobiologic component.
- the load-bearing and the osteobiologic components can be used alone or in combination. Combination is prefe ⁇ ed. In a particularly prefe ⁇ ed embodiment, the load-bearing and the osteobiological components are resorbable.
- the the load-bearing component can compnse at least one compound selected from the group consisting of poly(lactic acid), poly(glycolic acid), p- dioxanone fibers, polyarylethyl, polymethylmethacrylate, polyurethane, amino-acid- derived polycarbonate, polycaprolactone, aliphatic polyesters, calcium phosphate, unsaturated linear polyesters, vinyl py ⁇ olidone and polypropylene fumarate diacrylate, or mixtures thereof.
- the osteobiologic component can include at least one element selected from the group consisting of mesenchymal stem cells, growth factors, cancellous bone chips , hydroxyapatite, tri-calcium phosphate, polylactic acid, polyglycolic acid, polygalactic acid, polycaprolactone, polyethylene oxide, polypropylene oxide, polysulfone, polyethylene, polypropylene, hyaluronic acid, bioglass, gelatin, collagen and chopped polymeric fibers or mixtures thereof.
- the term "cancellous” refers to a bone having a porous structure.
- the normal type of adult mammalian bone, whether cancellous or compact, is composed of parallel lamellae in the former and concentric lamellae in the latter; lamellar organization reflects a repeating pattern of collagen fibroarchitecture.
- Adult bone consisting of mineralised regularly ordered parallel collagen fibres more loosely organised than the lamellar bone ofthe shaft of adult long bones, such as bone found in the end of long bones, is known as “cancellous bone”.
- the device can further comprise an osteoinductive component and an osteoconductive component.
- the osteoinductive component can include at least one compound selected from the group consisting of fibroblast growth factors, such as (FGFs) FGF-1, FGF- 2 and FGF-4; platelet-derived growth factors (PDGFs), such as PDGF-AB, PDGF- BB, PDGF-AA; epithelial growth factors EGFs; insulin-like growth factors (IGF), such as IGF-I, IGF-II; osteogenic protein- 1 (OP-1); transforming growth factors (TGFs), such as transforming growth factor- ⁇ , transforming growth factor- ⁇ 1, transforming growth factor- ⁇ 2, transforming growth factor- ⁇ 3; osteoid-inducing factor (OIF); angiogenin(s); endothelins; hepatocyte growth factor and keratinocyte growth factor; bone mo ⁇ hogenetic proteins (BMPs), such as osteogenin (bone mo ⁇ hogenetic protein-3), bone mo ⁇ hogenetic protein-2; bone mo ⁇ hogenetic protein-2A, bone mo ⁇ hogenetic protein-2B,
- ZO 4 is an acid radical, where Z is phosphorus, arsenic, vanadium, sulfur or silicon;
- Y is an anion, preferably halide, hydroxide, or carbonate.
- the osteoconductive component can further include at least one of material selected from the group consisting of mono-calcium phosphate, di-calcium phosphate, octa-calcium phosphate, alpha-tri-calcium phosphate, beta-tri-calcium phosphate, or tetra-calcium phosphate, hydroxyapatite, fluorapatite, calcium sulfate, calcium fluoride, calcium oxide, silicon dioxide, sodium oxide, and phosphorus pentoxide or mixtures thereof.
- the osteobiologic component can further include at least one water-soluble materials selected from the group consisting of gelatin, salts, polysaccharides and proteins.
- a particularly prefe ⁇ ed embodiment ofthe present invention is an intervertebral spinal fusion device shown in FIGs. 17 (a) (collapsed) and (b) (expanded).
- the device 100 comprises (a) a partially rigid anterior frame 110 detachably connected to a first fluid communication means 120, said frame having an upper inflatable rim 130 and a lower inflatable rim 140; and (b) a rigid posterior expandable frame 150, detachably connected to a second fluid communication means 122, said frame having a rigid upper rim 160 and a rigid lower rim 170, connected respectively to the upper inflatable rim 130 and lower inflatable rim 140 ofthe anterior frame 110.
- the device further comprises at least one mesh element 180 connected to the upper and the lower inflatable rims 130 and 140 ofthe anterior frame 110.
- At least one ofthe upper and the lower inflatable rims 130 and 140 of the anterior frame 110 of the device 100 can have a plurality of outward proj ections
- the posterior frame 150 ofthe device further includes at least one telescopically expandable supporting element 200, each said supporting element being connected to the upper and the lower rigid rims 160 and 170 ofthe posterior frame 150.
- Device 100 can be inserted into an intervertebral space in a collapsed state
- Device 100 can next be oriented so that the anterior frame 110 ofthe device is oriented to face an anterior aspect of a vertebra, the posterior frame 150 ofthe device is oriented to face a posterior aspect ofthe vertebra and the upper and lower rims 130, 140, 160 and 170 of each frame face upper and lower vertebral endplates endplates, respectively.
- At least one ofthe load-bearing component and the osteobiologic component is directed into the device by directing at least one component under pressure through at least one ofthe first and the second fluid communication means 120 and 122, thereby causing the device to expand and directing the upper inflatable rim 130 and the lower inflatable rim 140 ofthe anterior frame and a posterior frame 150 ofthe device against the respective vertebral endplates, thereby at least partially restoring a natural angle between two adjacent vertebrae.
- upon at least partially filling the upper and lower inflatable rims 130 and 140 and the posterior frame 150 between two adjacent vertebrae upon at least partially filling the upper and lower inflatable rims 130 and 140 and the posterior frame 150 between two adjacent vertebrae (not shown), natural angle between said two vertebrae is at least partially restored.
- the distance D between the upper and the lower inflatable rims is different from the height h ofthe posterior frame.
- said rims each have a footprint substantially co ⁇ esponding to a rim of a vertebral endplate.
- the device upon at least partially filling the upper and the lower inflatable rims 130 and 140 and the posterior frame 150, the device defines an open cavity 205 having an axial and a radial dimensions.
- the present invention is a method of making an intervertebral spinal fusion device comprising (a) inserting an inflatable device through a cannula into an intervertebral space; (b) orienting said inflatable device so that upon expansion a natural angle between two adjacent vertebrae will be at least partially restored; and (c) directing at least one member ofthe group consisting of a load-bearing component and an osteobiologic component into the inflatable device through the fluid communication means.
- the method ofthe present invention further includes the step of hardening the load- bearing component.
- said inflatable device includes an arcuate balloon connected to at least one fluid communication means, wherein said inflatable device upon expansion between two adjacent vertebrae has a footprint that substantially co ⁇ esponds to a perimeter of a vertebral endplate and at least partially restores a natural angle between two adjacent vertebrae.
- said inflatable device includes at least one inflatable balloon, said device having an upper area, a lower area, an anterior area and a posterior area, and where upon expansion ofthe upper and the lower areas against the respective vertebral endplates, said anterior area is unequal to than said posterior area height, and a footprint of the device substantially co ⁇ esponds to a rim of a vertebral endplate.
- the at least one balloon can contain a plurality of lumena.
- the anterior area ofthe inflatable device is oriented to face an anterior aspect of a vertebra and the posterior area ofthe device is oriented to face a posterior aspect ofthe vertebra.
- at least one ofthe load-bearing component and the osteobiologic component is directed into the balloon by directing at least one component under pressure through the fluid communication means, thereby causing the balloon to expand and directing the upper area and the lower area ofthe device against the respective vertebral endplates, thereby at least partially restoring a natural angle between two adjacent vertebrae.
- At least a portion ofthe device used to practice the method ofthe present invention upon expansion, has a generally toroidal shape thereby forming an open cavity defined by an outer surface ofthe toroidal shape having an axial dimension and a radial dimension.
- the at least a portion ofthe device is oriented so that the axial dimension ofthe open cavity is substantially parallel to a major axis of a spinal column of a patient in which the device has been implanted.
- at least one of a load-bearing component and an osteobiologic component can be directed into the open cavity defined by the expanded device.
- the method ofthe present invention can further include the step of dissolving at least one water-soluble material, thereby forming a porous matrix.
- the method ofthe present invention further includes the step of directing into the inflatable device osteoinductive and/or osteoconductive components.
- the present invention is a method of at least partially restoring a natural angle between two adjacent vertebrae comprising: (a) inserting an inflatable device through a cannula into an intervertebral space; (b) orienting said inflatable device so that upon expansion a natural angle between two adjacent vertebrae will be at least partially restored; and (c) expanding said inflatable device by directing at least one of a load-bearing component and an osteobiologic component, into said inflatable device.
- the inflatable devices suitable for practicing the method ofthe present invention are described above.
- the method ofthe present invention includes the step of inflating said inflatable device.
- Inflating includes introducing at least one of a load-bearing component and an osteobiologic component into said device by directing at least one component through the fluid communication means, thereby allowing the lower area and the upper area to engage the respective endplates and the anterior area height of said inflatable device to be greater than the posterior area height, thereby at least partially restoring or creating a natural angle between two adjacent vertebrae.
- the method further includes the step of hardening at least one ofthe load- bearing component and an osteobiologic component.
- the device upon expansion has a generally toroidal shape thereby forming an open cavity defined by an outer surface ofthe toroidal shape and having an axial dimension and a radial dimension and the step of orienting said inflatable device includes orienting at least a portion ofthe device so that so that the axial dimension ofthe open cavity is substantially parallel to a major axis of a spinal column of a patient in which the device has been implanted.
- the method further includes the step of introducing at least one ofthe load-bearing component and the osteobiologic component into the cavity and the step of hardening at least one ofthe load-bearing component and an osteobiologic component.
- the method can further includes the step of dissolving at least one water-soluble material, thereby forming a porous matrix.
- the patient is brought to the pre-surgical area and prepped. Anesthesia is then induced and the area ofthe spine is further prepped. A small incision through the muscles is opened under dissecting microscopic visualization. The incision is made as small as possible and is longitudinal in the plane of the spine. The paravertebral muscles are separated by blunt dissection and held apart with forceps and dividers. The intervertebral disc area is visualized, with initial exposure down to the lamina. The area below the lamina, at the point ofthe intervertebral foramina, can also be exposed.
- the disc is examined for extruded material and any extruded material is removed.
- Magnetic resonance imaging (“MRI") data can be used to determine the integrity ofthe annulus fibrosis at this point.
- An arthroscope is inserted into the disc and used to examine the inside ofthe annulus.
- an intraoperative discogram can be performed, in which a dye material is inserted and visualized in order to substantiate the integrity ofthe annulus fibrosis.
- Points of weakness, or rents, in the annulus fibrosis are identified and located and suitable means, e.g., a bioabsorbable glue is employed to block these rents. If balloons are used to deliver all ofthe flowable materials used in the present invention, then the rents need not be patched.
- Distraction ofthe intervertebral disc space can then be accomplished, as described above, by inserting a deflated balloon into the disc space and delivering a fluid (preferably, the flowable load bearing component ofthe present invention) into the balloon cavity.
- a fluid preferably, the flowable load bearing component ofthe present invention
- the endplates ofthe opposing vertebral body are partially decorticated , typically through the use of a curette, in order to allow blood flow into the disc space.
- the application cannula is inserted into the joint or disc space and under visualization from the fiberoptic scope the biomaterial is delivered.
- the flow ofthe biomaterial is controlled by the operator via a foot pedal connected to the pumping mechanism on the polymer canister.
- the biomaterial flows from the tip ofthe application catheter to fill the space provided.
- the flowable component is preferably solidified within 3 to 5 minutes, and preferably within 1 to 2 minutes.
- the osteobiologic component ofthe present invention is introduced to the distracted space, thereby filling the remainder ofthe disc space.
- the arthroscopic cannula and the application cannula are removed.
- the flowable materials are further allowed to harden over 15 to 20 minutes.
- the delivered biomaterial is allowed to cure, or cured by minimally invasive means and in such a manner that the cured biomaterial is retained in apposition to the prepared site.
- the biomaterial can be cured by any suitable means, either in a single step or in stages as it is delivered. Once cured, the biomaterial surface can be contoured as needed by other suitable, e.g., endoscopic or arthroscopic, instruments. The joint is irrigated and the instruments removed from the portals.
- a surgical procedure to fuse the vertebrae using methods and devices ofthe present invention can comprise the following steps: i. Puncture or cut a flap in the annulus fibrosus and insert a small diameter tube into the slit, ii. Perform a conventional discectomy to remove the nucleus pulposus, iii. Insert a small diameter tube, e.g. a cannula, into the disc space through the slit, iv. Insert a strat, e.g. a balloon or a ramp having a partially annular shape, into the disc space through the tube, v.
- Puncture or cut a flap in the annulus fibrosus and insert a small diameter tube into the slit ii. Perform a conventional discectomy to remove the nucleus pulposus, iii. Insert a small diameter tube, e.g. a cannula, into the disc space through the slit, iv. Insert a strat, e.g. a balloon or
- Flow glucose-containing polycaprolactone into the disc space including the volume defined by the outer surface ofthe partially annular balloon or a ramp, tlirough the tube at about 70 °C.
- the polycaprolactone should become solid, thereby supplementing the mechanical attributes ofthe strut, vi.
- the tube can also have a vacuum port to collect the eluted solution. viii. remove the tube(s), seal the flap, and wait a month for bone growth.
- the result of this procedure is a formation of a fusion cage.
- This procedure has numerous advantages. First, the resulting cage fills and supports the entire disc space, and so it is stable and is not prone to subsidence. Second, the minimally invasive treatment ofthe annulus fiborsus allows the resulting cage to be held in place by the retained annulus fibrosus. Third, the in situ formation of a scaffold eliminates the need in high impaction forces. Four, by the very nature of an inflatable device, it is adjusted to fit the desired disc height.
- Example 3 Harvesting Progenitor Cells for Use in Osteobiolo Jc Material
- approximately 5cc of bone marrow is aspirated from the iliac crest ofthe patient into a heparinized syringe tube.
- the heparinized ma ⁇ ow is then passed through a selective cell attachment filter.
- the filter is designed for selective attachment of osteoprogenitor cells such as mesenchymal stem cells and osteoblasts.
- the cells are tripsinized off of the filter and collected in a flask.
- the flask is then centrifuged to precipitate a cell pellet on the bottom ofthe flask and the supernatant is poured off.
- the cells are then mixed with the injectable precursor form ofthe hydrogel.
- the precursor hydrogel is then poured into molds that are between 50 - 250 um in any dimension.
- the precursor hydrogel is then cured, for example with a photoinitiator, to yield cell loaded hydrogel particles. These cell-hydrogel particles are then mixed with the viscous form ofthe hardenable material and injected as the osteobiologic composition.
- each vertebral endplate of a patient has a 1500 mm cross-sectional area, b) the maximum in vivo load experienced by a patient is 3.4 kN; c) the ultimate strength of a vertebral body is about 8.2 kN; d) the device should initially be able resist the maximum in vivo load; e) after one year, the device should be able to resist half the maximum in vivo load, f) the strut portion of the device will have a footprint of 20 areal% of the disc space.
- the initial minimum strength required by the device may be decreased. If the OB composition is chosen to provide a 5 MPa strength and a 0.05 GPa modulus for at least 6-12 weeks in order to mimic cancellous bone, then the OB composition may share about 10% ofthe applied compressive load when the modulus ofthe strat is 2 GPa (assuming no annulus fibrosis). Therefore, the strength ofthe strut may be about 10% lower. Modulus of a Load-Bearing Component
- the devices ofthe present invention have a stiffness of at least 0.5 kN/mm. This lower prefe ⁇ ed limit co ⁇ esponds to the stiffness of conventional allograft cages. However, it is believed by some that the low stiffness ofthe allograft cages may sometime cause too much microfracture in the remodeling process. Therefore, in some embodiments, the stiffriess ofthe devices ofthe present invention is preferably at least 5 kN/mm. Because it is believed that excessive device stiffness may undesirably cause stress shielding ofthe osteobiologic composition (and bone reso ⁇ tion), the stiffness ofthe device ofthe present invention is desirably no more than 50 kN/mm.
- the stiffness ofthe device of the present invention is between 10 and 20 kN/mm. This range of values is comfortably between the range of stiffnesses found in conventional allograft cages (0.6-2.6 kN/mm) and CFRP cages (20-30 kN/mm). Accordingly, it is believed that the devices ofthe present invention will have stiffness appropriate for the support of bony fusion through the disc space.
- the imtial minimum modulus required by the device may be decreased. If the OB composition is chosen to provide a 5 MPa strength and a 0.05 GPa modulus for at least 6-12 weeks in order to mimic cancellous bone, then the OB composition may share about 10% ofthe applied compressive load when the modulus ofthe strat is 2 GPa (assuming no annulus fibrosis). Therefore, the modulus ofthe strut may be about 10% lower.
- the strat stiffness should be about 1 GPa. As noted above, the material reported by Timmer meets this requirement.
- compositions and materials suitable for use in the present invention will be described below.
- compositions suitable for use as load-bearing component ofthe present invention that include a fumarate-based polymer (such as polypropylene fumarate) cross-linked with a cross-linking agent containing a polypropylene fumarate-unit, such as polypropylene fumarate-diacrylate are disclosed in Timmer, Biomaterials (2003) 2 ⁇ :571-577 (hereinafter, "Timmer"), the entire teachings of which are inco ⁇ orated herein by reference. These compositions are characterized by a high initial compressive strength (about 10-30 MPa) that typically increases over the first 12 weeks, high resistance to hydrolytic degradation (about 20-50 at 52 weeks), and an acceptable modulus for use as a strat (0.5-1.2 GPa).
- a fumarate-based polymer such as polypropylene fumarate
- a cross-linking agent containing a polypropylene fumarate-unit such as polypropylene fumarate-diacrylate
- compositions suitable for use as resorbable cross-linkable component comprises those cross-linkable components disclosed by Wise in U.S. Patent No. 6,071,982 (hereinafter, “Wise”), the entire teaching of which are herein inco ⁇ orated by reference.
- Exemplary injectable osteobiologic polymer-based compositions suitable for use in the present invention are described in the U.S. Patent No. 5,679,723 by Cooper (herein after, “Cooper”), the entire teachings of which are inco ⁇ orated herein by reference.
- Exemplary osteobiologic compositions in which porosity is produced in situ are described in the U.S. Patent No. 5,522,895 by Milcos (hereinafter, “Milcos”), the entire teachings of which are inco ⁇ orated herein by reference.
- PCL polycaprolactone
- PLA poly(lactic acid)
- PPF polypropylene fumarate
- PMMA polymethylmethacrylate
- 'TPN or “inte ⁇ enetrating networks” is a composition comprising two cross-linkable polymers, wherein two cross-linkable polymers, upon exposure to appropriate cross-linking agents, cross-links with itself, but not with the other cross-linked polymer.
- S-IPN or “Semi-inte ⁇ enetrating networks” is a composition comprising a first cross-linkable polymer and a second non-cross- linkable polymer whrein, upon exposure to an appropriate cross-linking agent, the first cross-linkable polymer cross-links with itself, while the second polymer remains unaffected.
- Hao Biomaterials (2003), 24:1531-39, the entire teachings of which are inco ⁇ orated herein by reference, certain mechanical properties of polycaprolactone increased by about 3 fold when it was formed as a S- IPN. When at least 15 wt % HAP was added, the tensile modulus increased to 6 fold over conventional polycaprolactone.
- the Timmer IPN composition is chosen as the load bearing composition in the strat because it has sufficient initial and long term strength, acceptable modulus, and is resorbable.
- the Timmer composition contains monomers, it is desirable to contain the composition in an inflatable device during curing. Since the Timmer composition is relatively resistant to degradation , the inflatable device can be made of a resorbable material having a short half life. Since the strut should also act as the distractor, the balloon should be non-compliant.
- the Wise composition is chosen as the osteobiologic composition because is forms a scaffold having a strength and modulus essentially similar to that of cancellous bone. It can be infiltrated in-situ with a hydrogel containing osteogenic cells and osteoinductive growth factors.
- the Wise composition contains monomers, it is desirable to contain the composition in an inflatable device during curing. Since bone in-growth is desirable through the region occupied by the balloon, the inflatable device should be made of a resorbable material having a very short half life (such as one day). Since the Wise composition a 25% expansion during pore formation, it would be desirable for the balloon to be compliant to allow the Wise composition conform to the disc space contour.
- solid neat polycaprolactone is chosen as the load bearing composition in the strat because it has sufficient initial strength (15 MPa), is very resistant to degradation, has an acceptable modulus (0.5 GPa), and is resorbable. Since solid polycaprolactone is relatively resistant to regradation, the inflatable device need not be relatively resistant to degradation, and so can be made of a resorbable material having a short half life. Since the strut should also act as the distractor, the balloon should be non-compliant.
- the Cooper composition is chosen as the osteobiologic composition because it is flowable at 40°C, and degrades sufficiently within a few months to form an hydroxyapatite based-scaffold. Because of its low delivery temperature, certain dimer bone mo ⁇ hogenetic proteins can also be delivered during the injection of this composition.
- the inflatable device should be made of a resorbable material having a very short half-life (such as one day).
- the polycaprolactone S-IPN composition (as reported in Hao) is chosen as the load bearing composition in the strat because it may have mechanical properties about 3-6 fold greater than neat polycaprolactone, and is resorbable. Since the polycaprolactone-polycaprolactone composition contains monomers, it is desirable to contain the composition in an inflatable device during curing. Since the polycaprolactone composition is relatively resistant to degradation, the inflatable device can be made of a resorbable material having a short half life. Since the strut should also act as the distractor, the balloon should be non-compliant.
- CaPO 4 is chosen as the load bearing composition in the strat because it has sufficient initial and long term strength, acceptable modulus, and is resorbable. Since CaPO 4 is very susceptable to degradation, the inflatable device need be relatively resistant to degradation, and so should be made of a resistant material that can contain the CaPO 4 for at least one year. Since the strat should also act as the distractor, the balloon should be non-compliant. One material that is resistant and non-compliant is polyetherether ketone.
- the CaPO 4 composition is chosen as the osteobiologic composition because it is flowable at body temperature, and degrades sufficiently within a few months to form an hydroxyapatite based-scaffold. Because of its delivery at body temperature, hydrogels containing temperature sensitive additives, such as osteogenic cells and osteoinductive components (such as bone mo ⁇ hogenetic proteins), can also be delivered during the injection of this composition.
- the Wise composition is chosen as the load bearing composition in the strut because it has sufficient initial strength, acceptable modulus, and is resorbable.
- the inflatable device need be relatively resistant to degradation, and so should be made of a resistant material that can contain the Wise Composition for at least one year. Since the strut should also act as the distractor, the balloon should be non-compliant.
- One material that is resistant and non-compliant is polyetherether ketone.
- the Mikos composition is chosen as the osteobiologic composition because it is injectable at body temperature, forms an in-situ scaffold in which hydrogels containing temperature sensitive additives, such as osteogenic cells and osteoinductive components (such as bone mo ⁇ hogenetic proteins), can be delivered. Since a hydrogel should be injected into the Mikos composition during surgery, it is desirable to inect the Mikos composition without the aid of a balloon.
- CaPO 4 is chosen as the load bearing composition in the strat because it has sufficient initial and long term strength, acceptable modulus, and is resorbable.
- the inflatable device need be relatively resistant to degradation, and so should be made of a resistant material that can contain the CaPO 4 for at least one year. Since the strut should also act as the distractor, the balloon should be non-compliant.
- One material that is resistant and non-compliant is polyetherether ketone.
- the polylactic acid beads are chosen as the matrix ofthe osteobiologic composition because they can be packed into the disc space at body temperature and heat bonded with hot water to form an in-situ formed scaffold. If the beads are selected to have a 2 mm diameter, the porosity ofthe resulting scaffold will be about 40 vol% with a pore size of about 500 um. Hydrogels containing temperature sensitive additives, such as osteogenic cells and osteoinductive components (such as bone mo ⁇ hogenetic proteins), can then be delivered the in-situ scaffold. Since the packed beads must be packed into the disc space and then heat bonded with a high temperature fluid, it may be desirable to contain both the beads and the hot fluid in a balloon.
- Nitonol reinforced balloon is desirable because the reinforcements can help the balloon withstand the high pressures needed during packing. Since the polylactic acid beads have sufficient initial and long term strength, acceptable modulus, there is no need for a strut.
- Timmer polypropylene fumarate-polypropylene fumarate-diacrylate with tricalcium phosphate (Embodiment B) with 50 vol% porosity (or seeded hydrogel phase) will still have a 25 MPa compressive strength after one year. If it takes the whole disc space, only 11.3 MPa is required. 2X safety factor.
Abstract
Description
Claims
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MXPA05008653A MXPA05008653A (en) | 2003-02-14 | 2004-02-13 | In-situ formed intervertebral fusion device and method. |
CA002515862A CA2515862A1 (en) | 2003-02-14 | 2004-02-13 | In-situ formed intervertebral fusion device |
EP04711129A EP1594423B1 (en) | 2003-02-14 | 2004-02-13 | In-situ formed intervertebral fusion device |
JP2006503557A JP2006517842A (en) | 2003-02-14 | 2004-02-13 | Apparatus and method for in situ forming intervertebral fusion |
AU2004212942A AU2004212942A1 (en) | 2003-02-14 | 2004-02-13 | In-situ formed intervertebral fusion device |
BR0407142-5A BRPI0407142A (en) | 2003-02-14 | 2004-02-13 | In situ intervertebral fusion device |
DE602004018903T DE602004018903D1 (en) | 2003-02-14 | 2004-02-13 | IN-SITU MANUFACTURED INTERVERTEBRALE FUSION DEVICE |
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2012
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