DE3841397C2 - - Google Patents

Description

The invention relates to a drug carrier from a porous, resorbable material such as collagen, this being Drug carrier with a resorbable degradable aliphatic polyester, which serves as a coating agent, is coated. In the drug carrier and / or Laking agent is also at least one Contain drug active ingredient.

The modern development in medicine sees one controlled local application of drugs in Body inside. For this purpose, implantable Drug forms using absorbable and also used non-absorbable systems. With help of modern techniques, especially in combination with drug carriers, drugs targeted into the body be introduced. In addition to usual, surgical Interventions in the body are also endoscopic Techniques available. Through the targeted implantation high local concentrations can be reached. At the same time, those with systemic administration common side effects completely or at least partially avoided. This is especially true with septic Interventions, but also for the treatment of malignancies  Swollen desirable. Especially in tumor surgery is a longer, targeted action on site of a cytostatic is desirable.

Non-absorbable drug delivery systems, e.g. B. on Basis of the bone cements such as polymethyl methacrylate (PMMA) plastics, can be combined with drugs will. But here is the release of the drug, regardless of the location of the implantation in the body, often at short notice and there is often only one incomplete delivery of the incorporated drugs, such as has been shown for various antibiotics and cytostatics.

Absorbable drug delivery systems, e.g. B. such Basis of collagen, fibrin, albumin, chitin, oxycellulose, or also other resorbable or degradable synthetically produced drug carriers, prove Combination with one or more Active pharmaceutical ingredients, depending on the location of the implantation, different availabilities. In well perfused Tissues are released quickly Active pharmaceutical ingredient before the carrier is complete is absorbed.

Absorbable porous drug carriers are also known active substances contained therein. Are also known resorbable and degradable polyester, e.g. B. such based on polyglycolic acid (PGS), polylactic acid (PLS), Polyhydroxybutyric acid (PHB) or polyhydroxy propionic acid (PHP), or copolymers of the aforementioned compounds. These absorbable and degradable polyesters are as absorbable sutures have been tried and tested in part in trade. They are caused by hydrolysis in the body tissues Course from several hours to several days - in  Depending on the thickness of the threads, or their Surface area, and the molecular weight of the polyester - reduced.

DE-OS 28 43 963 is an absorbable in the body shaped mass known on the basis of collagen. It will there is a resorbable shaped mass in the body on the Basis of collagen which can contain an active ingredient described. Collagen and a bio-absorbable Binders are exposed to pressure and / or Heat processed together. You get pretty tough and mechanically stable materials that are then used as tubes, Strands, foils, as tablets, balls or granules can be used. However, these preparations are not actually porous. Furthermore, from US-PS 45 63 489 known, drugs in the form of a powder in one resorbable degradable drug carrier To suspend the base of PLS and thereby a delayed release.

The object of the invention is a drug carrier in Combination with a drug ingredient for the to provide incorporeal application where a targeted sustained release of the active ingredient he follows. This task is done by a porous resorbable drug carrier according to claim 1 solved.

The release can be targeted depending on Implantation site, d. that is, in the area with good or poor perfusion due to the choice and thickness of the applied varnish can be controlled. The Drug carrier in the form of a film or a sponge has a porous structure and is resorbable. Are particularly suitable as a carrier material Foils or sponges based on collagen. The collagen can optionally be chemically modified, e.g. B. by Introduction of functional groups or through Cross-linking. The production of foils and sponges is known from collagen. You can for example by Freeze-drying a collagen-containing solution. Also resorbable as drug carriers Suitable for products of plant or animal origin, such as fibrin, chitin or oxycellulose.

Depending on the intended use, the drug carrier lies as a sponge or film, or as a powder or granulate in front.  

The invention provides the combination of a porous, absorbable drug carrier, e.g. B. a sponge from collagen, with a so-called lacquering agent. They serve as varnishing agents beforehand mentioned absorbable polyester based on Polyglycolic acid (PGS), polylactic acid (PLS), Polyhydroxybutyric acid (PHB), polyhydroxy propionic acid (PHB) or copolymers thereof, or mixtures of these polyesters or copolyester with each other.

In at least one of these two components, i.e. the Carrier and the varnish, is a Contain drug active ingredient. The nature of this Drug ingredient depends on the intended Therapy off. In addition to the cytostatics mentioned at the beginning, the play a role in tumor control for example the wide range of antibiotics in Question. The active pharmaceutical ingredient can thus either in or on the porous substrate or in the lacquering agent be included and it can also be both in the carrier as active ingredients are also incorporated in the coating agent, these active ingredients in the carrier and in the varnish can also be different from each other.

The varnish, one of the aforementioned Polyester, releases the active ingredient depending on that gradual hydrolytic degradation of the varnish, thus retarded free, whereby this active ingredient either from the varnish is released and / or from the porous support or the surface of the porous support in the extent to which this surface is hydrolysed Lacquer is released is available. Through the Control of the thickness of the varnish, the selection of the  Varnishing agent itself and the choice of Molecular weight of the polymeric varnish can controlled the release of the active ingredient (s) will.

The degree of drug release may continue be controlled by the fact that as a laking agent a combination of different polyesters Molecular weights used. By breaking down the polyester then with a smaller molecular weight early release of the drug while by the delayed degradation of the polyester with higher Molecular weight release of the drug ingredient only at a later date. In this way you can control the drug level so that a high one immediately after the implantation local drug level is present and the Concentration of active ingredient released over time, from several hours to several days, gradually decreased. It is also possible to have a multiple Make varnishing and in the individual Varnish layers a drug ingredient gradient build up. Within the scope of the present invention are here given many variations. One of these Opportunities is e.g. B. that one in the porous carrier or active pharmaceutical ingredient contained in the varnish from the outset already in a slow release form or in a mixture of non-delayed and delayed release Material. Over time, the release of the non-retarded and the retarded Active pharmaceutical ingredient, the retarded form then ensures that at a later date after the Implantation of the drug ingredient is available.

The following examples describe the invention.

Example 1 Production of a gentamicin-collagen-PGS combination

• 1. 0.2 g per 10 ml of 6-fluoroisopropanol
  0.02 g
  0.002 g or
  0.0002 g PGS (molecular weight 4000-8000) dissolved.
• 2. In a 5 × 5 × 2 cm glass tub Collagen gentamicin sponge size 5 × 5 × 0.5 cm, with the 2 mg gentamicin per cm² is loaded. In these Then 25 ml of the varnish solutions with the given under 1 given concentrations of PGA and the Solution becomes careful at a temperature of 30 ° C evaporated and dried in vacuo. You get on this way using 4 collagen gentamicin sulfate sponges different PGA concentrations.

Example 2

The procedure is as in Example 1, but instead of PGA, PHB (molecular weight 400,000-800,000) used becomes. PHB concentrations are initially set per 10 ml 6-fluoroisopropanol from

0.2 g
0.1 g
0.01 g
0.001 g or
0.0001 g

forth. The further procedure is as in Example 1.  

Example 3

Examples 1 and 2 are repeated. To the gradual degradation of the varnish (PGH or PHB) show, one adds to the varnishing solutions from PGS or PHB methylene blue. For this, 0.2 mg methylene blue, dissolved in water, per batch in a petri dish (Diameter: 3 cm) freeze-dried and then each time 0.5 ml of the aforementioned varnish solutions and these solutions are then cautious at one temperature dried from 30 ° C as indicated above.

The release of methylene blue from the respective paints from PGS or PHB is carried out in Ringer's lactate and the determination the concentration of methylene blue depending on time Photometer; the buried from the unpainted control Methylene blue serves as the internal standard. The release of gentamicin is carried out analogously. To determine the released aminoglycoside is used with common microbiological process determines the base released.  

Example 4 4.1 Production of the polyester-biopolymer-drug carrier combinations

4.1.1 A commercially available collagen sponge is washed with an aqueous Methylene blue solution, corresponding to 1 mg methylene blue per area, of 1 cm² the sponge surface, offset and freeze-dried. After this The freeze-drying process produces the methylene blue collagen Combinations with an absorbable polyester (poly-D, L-lactide-coglycolide (RG 504 from Boehringer) coated. 45 mg RG 504 in 1 ml Dimethyl sulfoxide (DMSO) dissolved and in a corresponding glass tub 1 cm³ Collagen materials are mixed with 1 ml of the RG 504 DMSO solution, frozen and freeze-dried.

4.1.2 as above, but using a commercially available one Fibrin foam for hemostatic purposes.

4.1.3. A commercially available gentamicin collagen sponge, the 2 mg gentamicin contains per area of 1 cm², in a corresponding glass tub per Cubic centimeters with 25 mg RG 504, dissolved in 1 ml DMSO, as stated above, spiked, frozen and then freeze-dried.

4.2 Production of the powder

The RG 504 polyester-biopolymer Drug combinations are covered with a ball mill Cooling powdered with liquid nitrogen.

Example 5

A gentamicin collagen sponge that contains 2 mg gentamicin per area, is powdered with a ball mill while cooling with liquid nitrogen. Then 1 cm³ of this powder is mixed with 20 mg of the polyester of the type Poly D, L-lactide (R 203 from Boehringer) dissolved in 1 ml of DMSO, mixed and then after freezing freeze-dried.

Example 6

As above, but using the RG 504 polyester Freeze drying the compact composite is pulverized using the ball mill.

Example 7

Commercially available oxicellulose gauze is pulverized with a ball mill and 100 mg of this powder are mixed with 2 ml of chloroform, the 3 mg of methylene blue contains dissolved. After the chloroform has been evaporated off, the coating is carried out with the polyester RG 504 in DMSO (according to Example 4.1.3) and after Freeze-drying again using the ball mill.  

Example 8

Commercially available chitin fiber fleece is powdered as described in Example 7, Methylene blue incorporated and chloroform removed. Then the coating 100 mg of this powder with 45 mg of polyester RG 504, dissolved in 1 ml of chloroform, carried out. After removing the chloroform under vacuum, there is a repeated pulverization with the ball mill.

Claims (4)

1. Porous resorbable drug carrier in the form a sponge or a film with a resorbable, degradable aliphatic Polyester is coated as a varnish and on or in the drug carrier and / or in the Varnish at least one Active pharmaceutical ingredient is included. 2. Drug carrier according to claim 1 based on Collagen, fibrin, chitin or oxycellulose. 3. Drug carrier according to one of the preceding Claims in which the resorbable, degradable aliphatic polyester polyglycolic acid (PGS), Polylactic acid (PLS), polyhydroxybutyric acid (PHB), Polyhydroxy propionic acid (PHP), a copolymer based on glycolic acid and lactic acid or is a mixture of the aforementioned polyesters. 4. Drug carrier according to one or more of the previous claims in which in the Drug carrier and in the varnish same or different active pharmaceutical ingredients are located.