WO2006131850A2 - Method and apparatus for distinguishing between clinically significant changes and artifacts in patient physiological information - Google Patents

Method and apparatus for distinguishing between clinically significant changes and artifacts in patient physiological information Download PDF

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Publication number
WO2006131850A2
WO2006131850A2 PCT/IB2006/051743 IB2006051743W WO2006131850A2 WO 2006131850 A2 WO2006131850 A2 WO 2006131850A2 IB 2006051743 W IB2006051743 W IB 2006051743W WO 2006131850 A2 WO2006131850 A2 WO 2006131850A2
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Prior art keywords
physiological
patient
physiological information
set forth
morphogram
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PCT/IB2006/051743
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French (fr)
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WO2006131850A3 (en
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Walid S. Ali
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Koninklijke Philips Electronics N.V.
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Priority to US11/916,767 priority Critical patent/US8070677B2/en
Priority to CN2006800204411A priority patent/CN101194271B/en
Priority to JP2008515336A priority patent/JP2008541976A/en
Priority to EP06756028.4A priority patent/EP1897028B1/en
Publication of WO2006131850A2 publication Critical patent/WO2006131850A2/en
Publication of WO2006131850A3 publication Critical patent/WO2006131850A3/en

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    • GPHYSICS
    • G16INFORMATION AND COMMUNICATION TECHNOLOGY [ICT] SPECIALLY ADAPTED FOR SPECIFIC APPLICATION FIELDS
    • G16HHEALTHCARE INFORMATICS, i.e. INFORMATION AND COMMUNICATION TECHNOLOGY [ICT] SPECIALLY ADAPTED FOR THE HANDLING OR PROCESSING OF MEDICAL OR HEALTHCARE DATA
    • G16H40/00ICT specially adapted for the management or administration of healthcare resources or facilities; ICT specially adapted for the management or operation of medical equipment or devices
    • G16H40/60ICT specially adapted for the management or administration of healthcare resources or facilities; ICT specially adapted for the management or operation of medical equipment or devices for the operation of medical equipment or devices
    • G16H40/63ICT specially adapted for the management or administration of healthcare resources or facilities; ICT specially adapted for the management or operation of medical equipment or devices for the operation of medical equipment or devices for local operation
    • GPHYSICS
    • G06COMPUTING; CALCULATING OR COUNTING
    • G06FELECTRIC DIGITAL DATA PROCESSING
    • G06F2218/00Aspects of pattern recognition specially adapted for signal processing
    • G06F2218/12Classification; Matching
    • G06F2218/16Classification; Matching by matching signal segments
    • G06F2218/18Classification; Matching by matching signal segments by plotting the signal segments against each other, e.g. analysing scattergrams

Definitions

  • the following relates to patient monitoring. It finds particular application to determining whether physiological changes captured by patient monitoring devices are clinically significant or artifacts.
  • Many intensive/critical care unit (ICU/CCU) patients have changing physiological conditions. Such patients are prone to deterioration and may periodically need immediate intervention when a clinically significant physiological change occurs. Thus, overall treatment is improved by close and accurate monitoring of physiological changes. Such monitoring is achieved through various patient monitoring devices. Of particular importance are physiological changes that invoke patient monitoring device alarms. When valid alarms are triggered, hospital staff (e.g., doctors, nurses...) begin evaluating and treating the patient.
  • hospital staff e.g., doctors, nurses
  • hospital staff learn to decipher between clearly erroneous alarms (e.g., by looking at the signal or value invoking the alarm) and alarms that potentially could be associated with a clinically significant physiological change.
  • clearly erroneous alarms e.g., by looking at the signal or value invoking the alarm
  • alarms that potentially could be associated with a clinically significant physiological change.
  • the staff is not always able to ascertain when a sounding false alarm obscures a later occurring critical event.
  • morphograms of physiological signals acquired by patient monitoring devices are decomposed via wavelet decomposition to generate unique signatures that are compared with each other to determine whether a physiological change is associated with a change in all related signatures (a clinically significant change) or whether the physiological change is only associated with a subset of signatures with a common signal (artiiact).
  • a patient physiological information monitoring system in another aspect, includes a plurality of patient monitoring devices and a physiological information analyzer.
  • the plurality of patient monitoring devices monitor physiological information from a patient and generate corresponding physiological signals.
  • the physiological information analyzer processes the monitored physiological information and determines whether a physiological change is a clinically significant event or an artifact.
  • the physiological information analyzer includes at least one receiver that receives the physiological signals from the patient monitoring devices; a signal correlator that generates morphograms from pairs of the received physiological signals; a signature generator that applies a wavelet decomposition to each morphogram to compute a signature for each morphogram; and a decision component that compares the morphogram signatures within and across sampling intervals and determines if a physiological change is a clinically significant change or an artifact.
  • One advantage includes determining whether a physiological change captured with a patient monitoring device is a clinically significant change or an artifact.
  • Another advantage resides in mitigating patient monitoring device false alarms.
  • Another advantage resides in reducing monitoring cost relative to other approaches that achieve a similar accuracy.
  • Another advantage lies in increased patient monitoring resolution.
  • FIGURE 1 illustrates a system that facilitates distinguishing between clinically significant changes and artifact in patient physiological information.
  • FIGURE 2 illustrates an exemplary ECG-ABP morphogram.
  • FIGURE 3 illustrates an exemplary Symlet wavelet.
  • FIGURE 4 illustrates a routine for signature comparison over N-K sampling intervals.
  • FIGURE 5 illustrates an exemplary graphical user interface for displaying signature coefficients.
  • FIGURE 6 shows several plots of a typical set of physiological signals captured over time for a patient with respiratory failure.
  • FIGURES 7-9 illustrate three example morphograms generated from pairs from an
  • FIGURES 10-12 show graphical examples of morphograms perturbed due to physiological changes in a patient's condition.
  • FIGURES 13-15 show graphical examples of morphograms perturbed due to an artifact.
  • FIGURE 1 illustrates a patient physiological information monitoring system for alerting clinical staff when a physiological change captured by a patient monitoring device is a clinically significant change.
  • the patient physiological information monitoring system includes a physiological information analyzer ("analyzer") 2 that analyzes monitored patient physiological information and renders a decision whether any particular perturbation in the physiological information is associated with a clinically significant physiological change.
  • the analyzer 2 includes one or more receivers 4 that receive patient physiological information indicative of a physiological state of a patient.
  • Such physiological information is obtained from one or more patient monitoring devices 6 (e.g., a cardiac monitor, a hemodynamic monitor%) and/or directly from sensors (not shown) located on or proximate to the patient.
  • a patient with chest pain typically is monitored at a health care facility with an electrocardiograph (ECG) device that collects heart-related electrical signals from multiple ECG leads (e.g., 3 leads, 5 leads...) strategically positioned on the patient's body.
  • ECG electrocardiograph
  • the collected signals are processed and visually displayed (e.g., on paper or a monitor) for observance by a doctor or other medical staff.
  • Such signals can be provided by the ECG device to one or more of the receivers 4 (e.g., through a wireless and/or wired connection).
  • physiological information e.g., ECG signals
  • Each of the receivers 4 is independently configured to collect physiological information from one or more of the patient monitoring devices 6.
  • a receiver configured to collect physiological information from more than one of the patient monitoring devices 6 can collect such information concurrently through parallel channels or serially through a shared or one or more dedicated channel. Where more then one of the receivers 4 collects physiological information from more than one of the patient monitoring devices 6, a subset of the receivers 4 may collect physiological information from the same monitoring device or a similar group of monitoring devices.
  • Each of the receivers 4 periodically collects physiological information during a sampling interval at a sampling rate (e.g. collect data for X seconds every Y seconds, where X and Y are positive real numbers and X ⁇ Y).
  • the sampling interval and rate for any one receiver is based at least in part an alarm configuration of the patient monitoring device that is monitoring the physiological information, resolution, processing power and memory size of the analyzer 2, and the discretion of the attending clinician. For instance, with a typical patient monitoring device, physiological conditions in the alarm range are monitored over a period of time (latency period) before a related alarm occurs in order to reach stability (e.g., and trigger an alarm with a high degree of correctness) and mitigate false alarms due to patient movement, erroneous signals, etc.
  • a series of anomalous blood pressure readings may be monitored for about a twelve second (e.g., the actual time is patient monitoring device / manufacturer dependent) period of analysis preceding invocation of a blood pressure alarm. If the blood pressure readings move out of the alarm range prior to lapse of the latency period, the blood pressure alarm is not triggered; but, if the blood pressure readings remain within the alarm condition range, the blood pressure alarm triggers upon lapse of the latency period.
  • the sampling rate of a particular receiver is a fraction of the latency period of the associated monitoring device so that the analyzer 2 may render a decision as to whether a significant physiological change has occurred prior to or when a patient monitoring device sounds an alarm.
  • the analyzer 2 sounds an alarm (e.g., its own alarm displays at a central monitoring station or it invokes a monitoring device to prematurely alarm) when it determines a clinically significant physiological change has occurred.
  • Such alarm condition may be determined by the analyzer 2 well before the monitoring device latency period lapses, thereby reducing the time between a clinically significant physiological change and treatment thereof.
  • the analyzer 2 can send a signal to the patient monitoring device to prevent or turn off an alarm when the analyzer 2 determines a physiological change is an artifact.
  • the receivers 4 convey the physiological information to a signal correlater 10 for further processing or for storing the received physiological information in a storage medium 8 (e.g., RAM, cache).
  • the physiological information is conveyed/stored such that the data is separable based at least in part on monitoring device and sampling interval and time.
  • physiological information associated with a particular monitoring device and/or collected during a particular sampling interval can be identified and retrieved.
  • physiological information from an ECG that was collected during a kth (where k is an integer greater than one) sampling interval can be identified from within all the physiological information collected over all the sampling intervals.
  • the signal correlater 10 generates a morphogram for pairs of signals with physiological information captured during contemporaneious sampling intervals.
  • physiological information includes information from N different monitoring devices, then the theoretical maximum number of morphograms generated for
  • sampling interval is ⁇ X , where X is the variable summed over.
  • N-I maximum number of morphograms at any given time is L V X .
  • morphograms generated and/or saved depends on factors such as a resolution and processing power, the size of storage medium 8, and the monitoring clinician.
  • the generated morphograms are conveyed to a signature generator 12 for further processing, displaying, or storage in the storage medium 8.
  • Each morphogram is a mapping of one physiological signal against another. It illustrates how the two physiological signals move together. The ability of one type of physiological signal to follow another type of physiological signal depends on the correlation between the two types of physiological signals.
  • the morphogram depicts a relationship between physiological data such as an ECG signal and an arterial blood pressure (ABP) signal. This relationship can be mapped and visually presented using tools such as plot or graphs. For instance, the ECG data can be mapped to one axis and the ABP data can be mapped to another axis, such that the relationship is visually depicted through multi-dimensional graph.
  • FIGURE 2 illustrates an ECG-ABP morphogram, or characteristic signature, in which an ECG signal is mapped to a vertical axis and an ABP signal is mapped to a horizontal axis. This mapping between physiological signals can also be represented symbolically through an equation.
  • the signature generator 12 computes a signature for each morphogram in each of the sampling intervals and stores the signatures in the storage medium 8.
  • the signatures are stored based on patient monitoring device and sampling interval. For example, a signature for an ECG-ABP morphogram generated using ECG and ABP signals from an ith (where i is an integer greater than one) sampling interval can be identified from the other signatures. Because all physiological conditions do not have the same cycle periodicity, some morphograms may be based on different sampling intervals.
  • the number of signatures stored at any given time is based at least in part on a size of the storage medium 8, the computation power of the analyzer 2, and the clinician monitoring the patient, for example.
  • the signature of each morphogram is a unique shape descriptor that represents morphogram shape characteristics such as inflection points, curvature, etc.
  • Suitable transforms for generating shape descriptors include wavelet transforms and the like.
  • the morphograms are processed with a two-dimensional (2D) wavelet transform (2D wavelet decomposition).
  • FIGURE 3 illustrates a Symlet wavelet, which is the preferable 2D wavelet to use with ECG and ABP based morphograms since they have similar shape characteristics.
  • 3D wavelet transforms can be used where three signals are correlated, and so on for higher orders.
  • Two-dimensional wavelet decomposition of a morphogram renders a set of coefficients that describe each morphogram in a horizontal, a vertical, and a diagonal (which includes both horizontal and vertical components) detail.
  • a set of three coefficients fully characterizes the 2D morphogram.
  • More levels of detail can be employed, if desired or needed, to generate more coefficients and, potentially, more accurate analysis at the cost of computational resources.
  • more levels of decomposition facilitate capturing shape variability for morphograms generated from less correlated signals. For instance, characterizing a sine wave with a square wavelet (low degree of correlation) generally requires more levels of decomposition than characterizing the sine wave with a sine wavelet (higher degree of correlation).
  • a decision component 14 compares signatures (coefficients) within and across a set of sampling intervals. Such comparison detects perturbations in related signatures, which are indicative of physiological changes. For example, a physiological change in the heart can result in changes to either or both of ECG and ABP signals which result in changes to the morphograms and signatures generated therefrom.
  • the signature can be retained (e.g., for further use or as a historical record) or discarded (e.g., deleted, written over). The comparison is also used to determine whether a detected physiological change is a clinically significant physiological changes or artifact.
  • a change in the signature can be clinically significant even if neither monitor condition changes beyond its alarm threshold. In this way, clinically significant events may be detected early.
  • the decision component 14 determines a physiological change is a clinically significant change base on the shape perturbation is in the signatures with signals related to the physiological change, and the decision component 14 determines a physiological change is an artifact if the shape perturbation is in a subset of signatures with at least one common signal.
  • FIGURE 4 shows an example in which signatures of morphograms generated over N-K sampling intervals are compared to render a decision.
  • a display component 16 visualizes the signatures for observance by the clinical staff.
  • FIGURE 5 illustrates an exemplary graphical user interface displaying coefficients for a two level, 2D Symlet wavelet decomposition of the ECG-ABP morphogram depicted in FIGURE 2.
  • a first level of decomposition (Ll) 18 includes a horizontal detail 20, a vertical detail 22, and a diagonal detail 24, and a second level of decomposition (L2) 26 includes a horizontal detail 28, a vertical detail 30, and a diagonal detail 32.
  • FIGURES 6-15 provide a particular example in which the analyzer 2 receives at least an ABP and two ECG signals from the patient monitoring devices 6.
  • FIGURE 6 shows several plots of a typical set of physiological signals captured over time for a patient with respiratory failure.
  • the set of signals includes an ECG lead II signal 34, an ECG lead V signal 36, and an ABP signal 38.
  • the signal correlater 10 generates morphograms for at least the ECG lead II signal 30, the ECG lead V signal 36, and the ABP signal 38. Examples of three morphograms generated from pairs of the signals 34-38 without changes or artifact are depicted in FIGURES 7-9.
  • FIGURE 7 illustrates a morphogram generated from the ECG signal II / ECG signal V pair
  • FIGURE 8 illustrates a morphogram generated from the ECG signal II / ABP signal pair
  • FIGURE 9 shows a morphogram generated from the ECG signal V / ABP signal pair.
  • the morphograms in FIGURES 7-9 all have well-defined shapes that repeat with each as long as there are no artifacts and the patient is not undergoing physiological changes. Since ABP and the various ECG signals are highly correlated, the resulting morphogram represent characteristic morphology that represent the correlated signals for a single heart beat when the sampling rate is greater than one heart beat. In many instances, the ECG-ECG and ABP-ECG morphograms have characteristic shapes that can be generalized across patients. Since the ABP wave lags behind the QRS complex, the ABP-ECG morphograms in
  • FIGURES 8 and 9 have a characteristic "L" shape (or a backwards "L” shape).
  • the ABP is at a low value
  • the ECG approaches its maximum (or minimum).
  • the ECG approaches a neutral value
  • the ABP approaches a maximum.
  • This correlation between ABP and ECG signals accounts for the characteristic "L" shape.
  • the pattern of the ECG-ECG morphogram in FIGURE 7 lies along a diagonal typically about 45 degrees or 135 degrees (e.g., as a bar or an oval). This shape results since both signals reach extremes (e.g., some point in the QRS complex) in unison.
  • Morphograms showing significant departures from the signature are easily detected.
  • a morphogram that is changing over time e.g., a gradual shorting along one leg of the "L"
  • L a morphogram that is changing over time
  • these departures indicate either a physiologically change or an artifact.
  • the underlying heuristic is that physiologically change is more likely to affect all signals, and thus there will be perturbations in all morphograms, whereas artifacts are more likely to affect only a single signal, and thus there will be perturbations only in the morphograms involving that signal.
  • FIGURES 10-12 show graphical examples where the morphograms are perturbed due to physiological changes in the patient's condition.
  • FIGURES 13-15 shows a graphical example for a patient with pulmonary edema during a time period in which an artifact occurs in the ABP signal.
  • FIGURES 14 and 15 are perturbed; the morphogram in FIGURE 13 for the two ECG signals retains its characteristic diagonal-oval shape; whereas, the two morphograms in FIGURES 14 and 15 with the ABP signal and either of the two ECG signals are highly distorted.
  • the change in only the morphograms in FIGURES 14 and 15 indicate an artifact (e.g., a mechanical problem for that signal).
  • the signature generator 12 computes a signature or unique shape descriptor that characterizes the ECG-ECG and two ECG-ABP morphograms. As noted previously, in the preferred embodiment (and in this example) a 2D Symlet wavelet is used to generate morphogram signatures.
  • the decision component 14 compares signatures (coefficients) within and across a predefined number of sampling intervals. Such comparison is used to detect physiological changes and determine whether they are clinically significant physiological changes or artifact. The decision component 14 determines a physiological change is a clinically significant change if the shape perturbation is in the signatures generated from signals related to the physiological change.
  • the decision component 14 determines a physiological change is an artifact if the shape perturbation is only in a subset of signatures with at least one common signal and signatures of related signals from different monitors are not.
  • One or more of the signatures are displayed in an interlace for monitoring by the medical staff.

Abstract

A patient physiological information monitoring system includes a plurality of patient monitoring devices (6) and a physiological information analyzer (2). The plurality of patient monitoring devices (6) monitor physiological information from a patient and generate corresponding physiological signals. The physiological information analyzer (2) processes the monitored physiological information and determines whether a physiological change is a clinically significant event or an artifact. The physiological information analyzer includes at least one receiver (4) that receives the physiological signals from the patient monitoring devices; a signal correlator (10) that generates morphograms from pairs of the received physiological signals; a signature generator (12) that applies a wavelet decomposition to each morphogram to compute a signature for each morphogram; and a decision component (14) that compares the morphogram signatures within and across sampling intervals and determines if a physiological change is a clinically significant change or an artifact.

Description

METHOD AND APPARATUS FOR DISTINGUISHING
BETWEEN CLINICALLY SIGNIFICANT CHANGES AND ARTIFACTS
IN PATIENT PHYSIOLOGICAL INFORMATION
DESCRIPTION
The following relates to patient monitoring. It finds particular application to determining whether physiological changes captured by patient monitoring devices are clinically significant or artifacts. Many intensive/critical care unit (ICU/CCU) patients have changing physiological conditions. Such patients are prone to deterioration and may periodically need immediate intervention when a clinically significant physiological change occurs. Thus, overall treatment is improved by close and accurate monitoring of physiological changes. Such monitoring is achieved through various patient monitoring devices. Of particular importance are physiological changes that invoke patient monitoring device alarms. When valid alarms are triggered, hospital staff (e.g., doctors, nurses...) begin evaluating and treating the patient. Many times, the evaluation results in concluding that the physiological change is not representative of a clinically significant change (e.g., a false alarm) or that no physiological change actually occurred (e.g., an artifact). Such alarms hinder clinical practice, obscure tru critical events, and increase the amount of human intervention in intensive/critical care situations.
To mitigate attending to every false alarm, hospital staff learn to decipher between clearly erroneous alarms (e.g., by looking at the signal or value invoking the alarm) and alarms that potentially could be associated with a clinically significant physiological change. Thus, it is not uncommon for staff to ignore a sounding alarm. However, the staff is not always able to ascertain when a sounding false alarm obscures a later occurring critical event.
In one aspect, morphograms of physiological signals acquired by patient monitoring devices are decomposed via wavelet decomposition to generate unique signatures that are compared with each other to determine whether a physiological change is associated with a change in all related signatures (a clinically significant change) or whether the physiological change is only associated with a subset of signatures with a common signal (artiiact).
In another aspect, a patient physiological information monitoring system includes a plurality of patient monitoring devices and a physiological information analyzer. The plurality of patient monitoring devices monitor physiological information from a patient and generate corresponding physiological signals. The physiological information analyzer processes the monitored physiological information and determines whether a physiological change is a clinically significant event or an artifact. The physiological information analyzer includes at least one receiver that receives the physiological signals from the patient monitoring devices; a signal correlator that generates morphograms from pairs of the received physiological signals; a signature generator that applies a wavelet decomposition to each morphogram to compute a signature for each morphogram; and a decision component that compares the morphogram signatures within and across sampling intervals and determines if a physiological change is a clinically significant change or an artifact.
One advantage includes determining whether a physiological change captured with a patient monitoring device is a clinically significant change or an artifact.
Another advantage resides in mitigating patient monitoring device false alarms.
Another advantage resides in reducing monitoring cost relative to other approaches that achieve a similar accuracy.
Another advantage lies in increased patient monitoring resolution.
Still further advantages will become apparent to those of ordinary skill in the art upon reading and understanding the detailed description of the preferred embodiments.
FIGURE 1 illustrates a system that facilitates distinguishing between clinically significant changes and artifact in patient physiological information. FIGURE 2 illustrates an exemplary ECG-ABP morphogram. FIGURE 3 illustrates an exemplary Symlet wavelet. FIGURE 4 illustrates a routine for signature comparison over N-K sampling intervals. FIGURE 5 illustrates an exemplary graphical user interface for displaying signature coefficients.
FIGURE 6 shows several plots of a typical set of physiological signals captured over time for a patient with respiratory failure. FIGURES 7-9 illustrate three example morphograms generated from pairs from an
ABP and two ECG signals.
FIGURES 10-12 show graphical examples of morphograms perturbed due to physiological changes in a patient's condition.
FIGURES 13-15 show graphical examples of morphograms perturbed due to an artifact.
FIGURE 1 illustrates a patient physiological information monitoring system for alerting clinical staff when a physiological change captured by a patient monitoring device is a clinically significant change. The patient physiological information monitoring system includes a physiological information analyzer ("analyzer") 2 that analyzes monitored patient physiological information and renders a decision whether any particular perturbation in the physiological information is associated with a clinically significant physiological change. The analyzer 2 includes one or more receivers 4 that receive patient physiological information indicative of a physiological state of a patient. Such physiological information is obtained from one or more patient monitoring devices 6 (e.g., a cardiac monitor, a hemodynamic monitor...) and/or directly from sensors (not shown) located on or proximate to the patient. By way of example, a patient with chest pain typically is monitored at a health care facility with an electrocardiograph (ECG) device that collects heart-related electrical signals from multiple ECG leads (e.g., 3 leads, 5 leads...) strategically positioned on the patient's body. The collected signals are processed and visually displayed (e.g., on paper or a monitor) for observance by a doctor or other medical staff. Such signals can be provided by the ECG device to one or more of the receivers 4 (e.g., through a wireless and/or wired connection). Using normally captured and processed physiological information (e.g., ECG signals) from the patient monitoring devices 6 enables seamless incorporation of the analyzer 2 into existing patient monitoring equipment without any need for software, hardware, or architectural changes to the patient monitoring equipment. Other monitoring devices monitor other physiological data, such as blood pressure, blood oxygen, respiration, and the like, and communicate the monitor inform the receivers 4. Each of the receivers 4 is independently configured to collect physiological information from one or more of the patient monitoring devices 6. A receiver configured to collect physiological information from more than one of the patient monitoring devices 6 can collect such information concurrently through parallel channels or serially through a shared or one or more dedicated channel. Where more then one of the receivers 4 collects physiological information from more than one of the patient monitoring devices 6, a subset of the receivers 4 may collect physiological information from the same monitoring device or a similar group of monitoring devices.
Each of the receivers 4 periodically collects physiological information during a sampling interval at a sampling rate (e.g. collect data for X seconds every Y seconds, where X and Y are positive real numbers and X < Y). The sampling interval and rate for any one receiver is based at least in part an alarm configuration of the patient monitoring device that is monitoring the physiological information, resolution, processing power and memory size of the analyzer 2, and the discretion of the attending clinician. For instance, with a typical patient monitoring device, physiological conditions in the alarm range are monitored over a period of time (latency period) before a related alarm occurs in order to reach stability (e.g., and trigger an alarm with a high degree of correctness) and mitigate false alarms due to patient movement, erroneous signals, etc. For example, a series of anomalous blood pressure readings may be monitored for about a twelve second (e.g., the actual time is patient monitoring device / manufacturer dependent) period of analysis preceding invocation of a blood pressure alarm. If the blood pressure readings move out of the alarm range prior to lapse of the latency period, the blood pressure alarm is not triggered; but, if the blood pressure readings remain within the alarm condition range, the blood pressure alarm triggers upon lapse of the latency period.
The sampling rate of a particular receiver is a fraction of the latency period of the associated monitoring device so that the analyzer 2 may render a decision as to whether a significant physiological change has occurred prior to or when a patient monitoring device sounds an alarm. In another embodiment, the analyzer 2 sounds an alarm (e.g., its own alarm displays at a central monitoring station or it invokes a monitoring device to prematurely alarm) when it determines a clinically significant physiological change has occurred. Such alarm condition may be determined by the analyzer 2 well before the monitoring device latency period lapses, thereby reducing the time between a clinically significant physiological change and treatment thereof. In still another embodiment, the analyzer 2 can send a signal to the patient monitoring device to prevent or turn off an alarm when the analyzer 2 determines a physiological change is an artifact.
In the illustrated embodiment, the receivers 4 convey the physiological information to a signal correlater 10 for further processing or for storing the received physiological information in a storage medium 8 (e.g., RAM, cache...). The physiological information is conveyed/stored such that the data is separable based at least in part on monitoring device and sampling interval and time. Thus, physiological information associated with a particular monitoring device and/or collected during a particular sampling interval can be identified and retrieved. For example, physiological information from an ECG that was collected during a kth (where k is an integer greater than one) sampling interval can be identified from within all the physiological information collected over all the sampling intervals.
More specifically, the signal correlater 10 generates a morphogram for pairs of signals with physiological information captured during contemporaneious sampling intervals. Thus, if the physiological information includes information from N different monitoring devices, then the theoretical maximum number of morphograms generated for
N-I that sampling interval is ∑X , where X is the variable summed over. If data is collected
1 for L (where L is an integer greater than one) sampling intervals, then the theoretical
N-I maximum number of morphograms at any given time is L V X . The actual number of
morphograms generated and/or saved depends on factors such as a resolution and processing power, the size of storage medium 8, and the monitoring clinician. The generated morphograms are conveyed to a signature generator 12 for further processing, displaying, or storage in the storage medium 8.
Each morphogram is a mapping of one physiological signal against another. It illustrates how the two physiological signals move together. The ability of one type of physiological signal to follow another type of physiological signal depends on the correlation between the two types of physiological signals. In the patient monitoring domain, the morphogram depicts a relationship between physiological data such as an ECG signal and an arterial blood pressure (ABP) signal. This relationship can be mapped and visually presented using tools such as plot or graphs. For instance, the ECG data can be mapped to one axis and the ABP data can be mapped to another axis, such that the relationship is visually depicted through multi-dimensional graph. FIGURE 2 illustrates an ECG-ABP morphogram, or characteristic signature, in which an ECG signal is mapped to a vertical axis and an ABP signal is mapped to a horizontal axis. This mapping between physiological signals can also be represented symbolically through an equation.
The signature generator 12 computes a signature for each morphogram in each of the sampling intervals and stores the signatures in the storage medium 8. The signatures are stored based on patient monitoring device and sampling interval. For example, a signature for an ECG-ABP morphogram generated using ECG and ABP signals from an ith (where i is an integer greater than one) sampling interval can be identified from the other signatures. Because all physiological conditions do not have the same cycle periodicity, some morphograms may be based on different sampling intervals. The number of signatures stored at any given time is based at least in part on a size of the storage medium 8, the computation power of the analyzer 2, and the clinician monitoring the patient, for example.
The signature of each morphogram is a unique shape descriptor that represents morphogram shape characteristics such as inflection points, curvature, etc. Suitable transforms for generating shape descriptors include wavelet transforms and the like. In a preferred embodiment, the morphograms are processed with a two-dimensional (2D) wavelet transform (2D wavelet decomposition). FIGURE 3 illustrates a Symlet wavelet, which is the preferable 2D wavelet to use with ECG and ABP based morphograms since they have similar shape characteristics. Of course, 3D wavelet transforms can be used where three signals are correlated, and so on for higher orders.
Two-dimensional wavelet decomposition of a morphogram renders a set of coefficients that describe each morphogram in a horizontal, a vertical, and a diagonal (which includes both horizontal and vertical components) detail. With highly correlated physiological signals, a set of three coefficients fully characterizes the 2D morphogram. More levels of detail can be employed, if desired or needed, to generate more coefficients and, potentially, more accurate analysis at the cost of computational resources. Typically, more levels of decomposition facilitate capturing shape variability for morphograms generated from less correlated signals. For instance, characterizing a sine wave with a square wavelet (low degree of correlation) generally requires more levels of decomposition than characterizing the sine wave with a sine wavelet (higher degree of correlation).
A decision component 14 compares signatures (coefficients) within and across a set of sampling intervals. Such comparison detects perturbations in related signatures, which are indicative of physiological changes. For example, a physiological change in the heart can result in changes to either or both of ECG and ABP signals which result in changes to the morphograms and signatures generated therefrom. Upon using a signature to determine whether a physiological change is a clinically significant event or an artifact, the signature can be retained (e.g., for further use or as a historical record) or discarded (e.g., deleted, written over...). The comparison is also used to determine whether a detected physiological change is a clinically significant physiological changes or artifact. It is to be appreciated that a change in the signature can be clinically significant even if neither monitor condition changes beyond its alarm threshold. In this way, clinically significant events may be detected early. The decision component 14 determines a physiological change is a clinically significant change base on the shape perturbation is in the signatures with signals related to the physiological change, and the decision component 14 determines a physiological change is an artifact if the shape perturbation is in a subset of signatures with at least one common signal. FIGURE 4 shows an example in which signatures of morphograms generated over N-K sampling intervals are compared to render a decision. A display component 16 visualizes the signatures for observance by the clinical staff. Such display can be at the bedside of the patient and/or at a remote monitoring station (e.g., a nurse station, over the Internet...). FIGURE 5 illustrates an exemplary graphical user interface displaying coefficients for a two level, 2D Symlet wavelet decomposition of the ECG-ABP morphogram depicted in FIGURE 2. A first level of decomposition (Ll) 18 includes a horizontal detail 20, a vertical detail 22, and a diagonal detail 24, and a second level of decomposition (L2) 26 includes a horizontal detail 28, a vertical detail 30, and a diagonal detail 32. FIGURES 6-15 provide a particular example in which the analyzer 2 receives at least an ABP and two ECG signals from the patient monitoring devices 6. FIGURE 6 shows several plots of a typical set of physiological signals captured over time for a patient with respiratory failure. The set of signals includes an ECG lead II signal 34, an ECG lead V signal 36, and an ABP signal 38.
The signal correlater 10 generates morphograms for at least the ECG lead II signal 30, the ECG lead V signal 36, and the ABP signal 38. Examples of three morphograms generated from pairs of the signals 34-38 without changes or artifact are depicted in FIGURES 7-9. In particular, FIGURE 7 illustrates a morphogram generated from the ECG signal II / ECG signal V pair; FIGURE 8 illustrates a morphogram generated from the ECG signal II / ABP signal pair; and FIGURE 9 shows a morphogram generated from the ECG signal V / ABP signal pair.
The morphograms in FIGURES 7-9 all have well-defined shapes that repeat with each as long as there are no artifacts and the patient is not undergoing physiological changes. Since ABP and the various ECG signals are highly correlated, the resulting morphogram represent characteristic morphology that represent the correlated signals for a single heart beat when the sampling rate is greater than one heart beat. In many instances, the ECG-ECG and ABP-ECG morphograms have characteristic shapes that can be generalized across patients. Since the ABP wave lags behind the QRS complex, the ABP-ECG morphograms in
FIGURES 8 and 9 have a characteristic "L" shape (or a backwards "L" shape). When the ABP is at a low value, the ECG approaches its maximum (or minimum). Similarly, when the ECG approaches a neutral value, the ABP approaches a maximum. This correlation between ABP and ECG signals accounts for the characteristic "L" shape. The pattern of the ECG-ECG morphogram in FIGURE 7 lies along a diagonal typically about 45 degrees or 135 degrees (e.g., as a bar or an oval). This shape results since both signals reach extremes (e.g., some point in the QRS complex) in unison.
Morphograms showing significant departures from the signature are easily detected. Similarly, a morphogram that is changing over time (e.g., a gradual shorting along one leg of the "L") can be detected, and its rate of change can be clinically significant. These departures indicate either a physiologically change or an artifact. The underlying heuristic is that physiologically change is more likely to affect all signals, and thus there will be perturbations in all morphograms, whereas artifacts are more likely to affect only a single signal, and thus there will be perturbations only in the morphograms involving that signal. FIGURES 10-12 show graphical examples where the morphograms are perturbed due to physiological changes in the patient's condition. The changes in the patterns (relative to the patterns with no physiological changes or artifact shown in FIGURES 7-9) are obvious in the morphograms generated from that signal; there are perturbations in each of the morphograms' morphology. FIGURES 13-15 shows a graphical example for a patient with pulmonary edema during a time period in which an artifact occurs in the ABP signal. As depicted, only the morphograms that include the ABP signal (FIGURES 14 and 15, are perturbed; the morphogram in FIGURE 13 for the two ECG signals retains its characteristic diagonal-oval shape; whereas, the two morphograms in FIGURES 14 and 15 with the ABP signal and either of the two ECG signals are highly distorted. Given that the signals in this example are highly correlated, the change in only the morphograms in FIGURES 14 and 15 indicate an artifact (e.g., a mechanical problem for that signal).
The signature generator 12 computes a signature or unique shape descriptor that characterizes the ECG-ECG and two ECG-ABP morphograms. As noted previously, in the preferred embodiment (and in this example) a 2D Symlet wavelet is used to generate morphogram signatures. The decision component 14 compares signatures (coefficients) within and across a predefined number of sampling intervals. Such comparison is used to detect physiological changes and determine whether they are clinically significant physiological changes or artifact. The decision component 14 determines a physiological change is a clinically significant change if the shape perturbation is in the signatures generated from signals related to the physiological change. Similarly, the decision component 14 determines a physiological change is an artifact if the shape perturbation is only in a subset of signatures with at least one common signal and signatures of related signals from different monitors are not. One or more of the signatures are displayed in an interlace for monitoring by the medical staff.
The invention has been described with reference to the preferred embodiments. Modifications and alterations may occur to others upon reading and understanding the preceding detailed description. It is intended that the invention be constructed as including all such modifications and alterations insofar as they come within the scope of the appended claims or the equivalents thereof.

Claims

1. A patient physiological information monitoring system, comprising: a plurality of patient monitoring devices (6) that monitor physiological information from a patient and generate corresponding physiological signals; and a physiological information analyzer (2) that processes the monitored physiological information and determines whether a physiological change is a clinically significant event or an artifact, the physiological information analyzer including: at least one receiver (4) that receives the physiological signals from the patient monitoring devices; a signal correlator (10) that generates morphograms from pairs of the received physiological signals; a signature generator (12) that applies a wavelet decomposition to each morphogram to compute a signature for each morphogram; and a decision component (14) that compares the morphogram signatures within and across sampling intervals and determines if a physiological change is a clinically significant change or an artifact.
2. The patient physiological information monitoring system as set forth in claim 1, wherein the decision component (14) determines the physiological change is an artifact if the shape perturbation is only in a subset of signatures with at least one common signal.
3. The patient physiological information monitoring system as set forth in claim 1, wherein the decision component (14) determines an alarm is valid if a shape perturbation is present in the signatures with signals related to the physiological change.
4. The patient physiological information monitoring system as set forth in claim 1, further including a display component (16) that visually presents at least some of the signatures for observation by a clinical staff.
5. The patient physiological information monitoring system as set forth in claim 1, wherein the analyzer (2) discards signatures that include artiiact and stores signatures that include clinically significant physiological changes in a storage component (8).
6. The patient physiological information monitoring system as set forth in claim 1, wherein the wavelet is a Symlet wavelet.
7. The patient physiological information monitoring system as set forth in claim 1, wherein the signature of a morphogram is represented by one or more coefficients that fully describe morphogram shape variability.
8. The patient physiological information monitoring system as set forth in claim 7, wherein the one or more coefficients include a horizontal detail, a vertical detail, and a diagonal detail that includes both a horizontal component and vertical component.
9. The patient physiological information monitoring system as set forth in claim 1, wherein the wavelet decomposition includes one or more levels of decomposition.
10. The patient physiological information monitoring system as set forth in claim 1, wherein the sampling intervals occur at a sampling rate that is less than or equal to an alarm latency period of the corresponding patient monitor device (6), the alarm latency period corresponds to a time over which an alarm condition exits in order to trigger an alarm with a high degree of correctness.
11. The patient physiological information monitoring system as set forth in claim 1, wherein the physiological information includes at least one or more ECG signals and an arterial blood pressure (ABP) signal.
12. The patient physiological information monitoring system as set forth in claim 1, wherein the physiological information analyzer (2) sounds an alarm and/or prematurely invokes a monitoring device (6) to alarm when it determines a clinically significant physiological change has occurred.
13. The patient physiological information monitoring system as set forth in claim 1, the physiological information analyzer (2) prevents or turns off a patient monitoring device alarm when the analyzer (2) determines a monitored physiological change is an artifact.
14. A method for determining whether a physiological change captured by a patient monitoring device is a clinically significant change or an artifact, comprising: receiving physiological signals indicative of physiological information monitored from patient; generating a morphogram for pairs of the physiological signals as the physiological information for each sampling interval is received; applying a wavelet decomposition on each morphogram to generate a signature for each morphogram; and comparing the signatures within and across sampling intervals; and determining whether signatures perturbations are a result of clinically significant changes or artifacts.
15. The method as set forth in claim 1, wherein the wavelet is a Symlet wavelet.
16. The method as set forth in claim 1, wherein each signature is a unique descriptor represented as coefficients that describe morphogram shape variability.
17. The method as set forth in claim 15, further including using the result of the determination to invoke or override a patient monitoring device related alarm, the patient monitoring device alarm being invoked when the perturbation is determined to be due to a clinically significant physiological.
18. The method as set forth in claim 15, further including displaying at least the signatures for observation by clinical staff.
19. A computer programmed to perform the method of claim 14.
20. A method of patient monitoring, comprising: generating morphograms from related patient monitoring signals; decomposing the morphograms via a wavelet decomposition to generate signatures; comparing changes in the signatures relative to each other or over time; and based on the signature comparisons, determining whether a clinically significant event or an artifact has occurred.
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Families Citing this family (55)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US8932227B2 (en) 2000-07-28 2015-01-13 Lawrence A. Lynn System and method for CO2 and oximetry integration
US9468378B2 (en) 1997-01-27 2016-10-18 Lawrence A. Lynn Airway instability detection system and method
US9042952B2 (en) 1997-01-27 2015-05-26 Lawrence A. Lynn System and method for automatic detection of a plurality of SPO2 time series pattern types
US6024089A (en) 1997-03-14 2000-02-15 Nelcor Puritan Bennett Incorporated System and method for setting and displaying ventilator alarms
US9521971B2 (en) 1997-07-14 2016-12-20 Lawrence A. Lynn System and method for automatic detection of a plurality of SPO2 time series pattern types
US20070191697A1 (en) 2006-02-10 2007-08-16 Lynn Lawrence A System and method for SPO2 instability detection and quantification
US20060195041A1 (en) 2002-05-17 2006-08-31 Lynn Lawrence A Centralized hospital monitoring system for automatically detecting upper airway instability and for preventing and aborting adverse drug reactions
US9053222B2 (en) 2002-05-17 2015-06-09 Lawrence A. Lynn Patient safety processor
US7668579B2 (en) 2006-02-10 2010-02-23 Lynn Lawrence A System and method for the detection of physiologic response to stimulation
US20070239061A1 (en) * 2006-04-05 2007-10-11 Jacob Carter Systems and methods for providing multi-variable measurement diagnostic
US8021310B2 (en) 2006-04-21 2011-09-20 Nellcor Puritan Bennett Llc Work of breathing display for a ventilation system
EP2023812B1 (en) 2006-05-19 2016-01-27 The Queen's Medical Center Motion tracking system for real time adaptive imaging and spectroscopy
US7784461B2 (en) 2006-09-26 2010-08-31 Nellcor Puritan Bennett Llc Three-dimensional waveform display for a breathing assistance system
WO2009137682A1 (en) 2008-05-07 2009-11-12 Lynn Lawrence A Medical failure pattern search engine
US8676303B2 (en) 2008-05-13 2014-03-18 The Regents Of The University Of California Methods and systems for treating heart instability
CN104873190A (en) 2008-10-09 2015-09-02 加利福尼亚大学董事会 Machine and process for automatic localization of sources of biological rhythm disorders
WO2010102069A2 (en) 2009-03-04 2010-09-10 Masimo Corporation Medical monitoring system
US9323894B2 (en) 2011-08-19 2016-04-26 Masimo Corporation Health care sanitation monitoring system
US10032002B2 (en) 2009-03-04 2018-07-24 Masimo Corporation Medical monitoring system
US10007758B2 (en) 2009-03-04 2018-06-26 Masimo Corporation Medical monitoring system
WO2010126731A2 (en) * 2009-04-30 2010-11-04 Research Foundation Of City University Of New York Patient monitoring and alarm system
US10434319B2 (en) 2009-10-09 2019-10-08 The Regents Of The University Of California System and method of identifying sources associated with biological rhythm disorders
US9282910B2 (en) 2011-05-02 2016-03-15 The Regents Of The University Of California System and method for targeting heart rhythm disorders using shaped ablation
US10398326B2 (en) 2013-03-15 2019-09-03 The Regents Of The University Of California System and method of identifying sources associated with biological rhythm disorders
US9392948B2 (en) 2011-12-09 2016-07-19 The Regents Of The University Of California System and method of identifying sources for biological rhythms
US9332915B2 (en) 2013-03-15 2016-05-10 The Regents Of The University Of California System and method to identify sources associated with biological rhythm disorders
USD638852S1 (en) 2009-12-04 2011-05-31 Nellcor Puritan Bennett Llc Ventilator display screen with an alarm icon
USD649157S1 (en) 2009-12-04 2011-11-22 Nellcor Puritan Bennett Llc Ventilator display screen with a user interface
US8924878B2 (en) 2009-12-04 2014-12-30 Covidien Lp Display and access to settings on a ventilator graphical user interface
US9119925B2 (en) 2009-12-04 2015-09-01 Covidien Lp Quick initiation of respiratory support via a ventilator user interface
US8335992B2 (en) 2009-12-04 2012-12-18 Nellcor Puritan Bennett Llc Visual indication of settings changes on a ventilator graphical user interface
US9262588B2 (en) 2009-12-18 2016-02-16 Covidien Lp Display of respiratory data graphs on a ventilator graphical user interface
US8499252B2 (en) 2009-12-18 2013-07-30 Covidien Lp Display of respiratory data graphs on a ventilator graphical user interface
EP2555673B1 (en) 2010-04-08 2019-06-12 The Regents of The University of California Methods, system and apparatus for the detection, diagnosis and treatment of biological rhythm disorders
WO2012051300A2 (en) * 2010-10-12 2012-04-19 Worcester Polytechnic Institute Method and system for detection and rejection of motion/noise artifacts in physiological measurements
US9107600B2 (en) 2011-05-02 2015-08-18 The Regents Of The University Of California System and method for reconstructing cardiac activation information
US9050006B2 (en) 2011-05-02 2015-06-09 The Regents Of The University Of California System and method for reconstructing cardiac activation information
US8165666B1 (en) 2011-05-02 2012-04-24 Topera, Inc. System and method for reconstructing cardiac activation information
US9606209B2 (en) 2011-08-26 2017-03-28 Kineticor, Inc. Methods, systems, and devices for intra-scan motion correction
US20130131993A1 (en) * 2011-11-14 2013-05-23 Lawrence A. Lynn Iterative time series matrix pattern enhancer processor
US10362967B2 (en) 2012-07-09 2019-07-30 Covidien Lp Systems and methods for missed breath detection and indication
US20140032241A1 (en) * 2012-07-26 2014-01-30 General Electric Company Method, apparatus and computer program product for monitoring clinical state of a subject
US10354429B2 (en) 2012-11-14 2019-07-16 Lawrence A. Lynn Patient storm tracker and visualization processor
US9953453B2 (en) 2012-11-14 2018-04-24 Lawrence A. Lynn System for converting biologic particle density data into dynamic images
CN105392423B (en) 2013-02-01 2018-08-17 凯内蒂科尔股份有限公司 The motion tracking system of real-time adaptive motion compensation in biomedical imaging
WO2014134460A1 (en) 2013-02-28 2014-09-04 Lynn Lawrence A Time lapsable motion image responsive to features of pathophysiologic perturbations
FR3011963B1 (en) * 2013-10-11 2015-12-11 Novacyt METHOD, MODULE AND COMPUTER PROGRAM, SCREENING DISEASE (S) BY SAMPLING ON AN INDIVIDUAL
EP4218559A1 (en) 2014-02-25 2023-08-02 ICU Medical, Inc. Patient monitoring system with gatekeeper signal
EP3188660A4 (en) 2014-07-23 2018-05-16 Kineticor, Inc. Systems, devices, and methods for tracking and compensating for patient motion during a medical imaging scan
US9950129B2 (en) 2014-10-27 2018-04-24 Covidien Lp Ventilation triggering using change-point detection
US9943247B2 (en) * 2015-07-28 2018-04-17 The University Of Hawai'i Systems, devices, and methods for detecting false movements for motion correction during a medical imaging scan
JP6674553B2 (en) 2015-10-19 2020-04-01 アイシーユー・メディカル・インコーポレーテッド Hemodynamic monitoring system with detachable display unit
DE102016118673A1 (en) 2016-09-30 2018-04-05 Isar-M Gmbh System for the early detection of post-operative bleeding
KR102079530B1 (en) * 2018-01-26 2020-02-20 고려대학교 산학협력단 Apparatus and method for detecting artifact of blood pressure, and computer readable recording medium storing the method
US11672934B2 (en) 2020-05-12 2023-06-13 Covidien Lp Remote ventilator adjustment

Family Cites Families (11)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3636941A (en) * 1970-01-12 1972-01-25 Hoffmann La Roche Sphygmomanometer alarm reset technique
US4852570A (en) 1989-02-09 1989-08-01 Levine Alfred B Comparative medical-physical analysis
US5464012A (en) * 1993-09-13 1995-11-07 Hewlett-Packard Company Patient alarm detection using target mode
US5438983A (en) 1993-09-13 1995-08-08 Hewlett-Packard Company Patient alarm detection using trend vector analysis
JP3521654B2 (en) * 1996-11-07 2004-04-19 セイコーエプソン株式会社 Pulse meter
US6105015A (en) * 1997-02-03 2000-08-15 The United States Of America As Represented By The Secretary Of The Navy Wavelet-based hybrid neurosystem for classifying a signal or an image represented by the signal in a data system
US6002952A (en) * 1997-04-14 1999-12-14 Masimo Corporation Signal processing apparatus and method
JP3107020B2 (en) * 1997-11-14 2000-11-06 日本電気株式会社 Characteristic brain electromagnetic wave detection device
US6287328B1 (en) * 1999-04-08 2001-09-11 Agilent Technologies, Inc. Multivariable artifact assessment
JP4318062B2 (en) * 2000-05-16 2009-08-19 日本光電工業株式会社 Biological signal monitor
US20040024532A1 (en) 2002-07-30 2004-02-05 Robert Kincaid Method of identifying trends, correlations, and similarities among diverse biological data sets and systems for facilitating identification

Non-Patent Citations (4)

* Cited by examiner, † Cited by third party
Title
ALI W ET AL: "Morphograms: Exploiting Correlation Patterns to Efficiently Identify Clinically Significant Events in Intensive Care Units" SAN FRANCISCO, CA, USA 1-5 SEPT. 2004, PISCATAWAY, NJ, USA,IEEE, US, 1 September 2004 (2004-09-01), pages 554-557, XP002323631 ISBN: 0-7803-8439-3 *
INGRID DAUBECHIES: "Ten Lectures on Wavelets" 1992, SIAM , PHILADELPHIA, PENN., USA , XP002408618 page 194 - page 202 page 254 - page 257 page 313 - page 319 *
PEREDA ET AL: "Nonlinear multivariate analysis of neurophysiological signals" PROGRESS IN NEUROBIOLOGY, PERGAMON PRESS, GB, vol. 77, no. 1-2, September 2005 (2005-09), pages 1-37, XP005174115 ISSN: 0301-0082 *
STEPHANE MALLAT: "A Wavelet Tour of Signal Processing" 1998, ACADEMIC PRESS , SAN DIEGO, USA , XP002408619 page 250 - page 252 *

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