AU1186197A - Bioenergetic data collection apparatus - Google Patents

Bioenergetic data collection apparatus

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Publication number
AU1186197A
AU1186197A AU11861/97A AU1186197A AU1186197A AU 1186197 A AU1186197 A AU 1186197A AU 11861/97 A AU11861/97 A AU 11861/97A AU 1186197 A AU1186197 A AU 1186197A AU 1186197 A AU1186197 A AU 1186197A
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bioenergetic
pulse
signals
processing means
data
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AU11861/97A
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AU719852B2 (en
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Robert John Grace
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Larkace Pty Ltd
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CIRCUITY SYSTEMS Ltd
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Priority claimed from AUPN7407A external-priority patent/AUPN740796A0/en
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Publication of AU1186197A publication Critical patent/AU1186197A/en
Assigned to LARKACE PTY LTD reassignment LARKACE PTY LTD Alteration of Name(s) of Applicant(s) under S113 Assignors: CIRCUITY SYSTEMS LIMITED
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Publication of AU719852B2 publication Critical patent/AU719852B2/en
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  • Measurement Of The Respiration, Hearing Ability, Form, And Blood Characteristics Of Living Organisms (AREA)
  • Nitrogen And Oxygen Or Sulfur-Condensed Heterocyclic Ring Systems (AREA)
  • Other Investigation Or Analysis Of Materials By Electrical Means (AREA)
  • Farming Of Fish And Shellfish (AREA)

Description

"BIOENERGETIC DATA COLLECTION APPARATUS" FIELD OF THE INVENTION This invention relates to a method and apparatus for the collection of biomedical data. In particular, it relates to a bioenergetic approach to the evaluation of observed cardiovascular response as recorded in terminal tissue, such as the fingertip. The invention finds primary application with humans but may also be applied to animals.
BACKGROUND TO THF INVENTION Biomedical data can be collected using electronic instruments that utilize electromagnetic energy in various ways. A useful summary of known devices and techniques has been presented by Dr. Dennis W Remmington to the Joint Committee Meeting ofthe Utah State Medical Association and published in July 1990. He summarises the known devices in two categories: instruments which measure passive electrical energy, and instruments which measure response to stimuli.
The first category includes instruments such as the electrocardiograph (ECG), the electroencephalograph (EEG), Chinese electric pulse testing, and Chinese gastrointestinal analysis. In the second category are instruments that measure response to stimuli, such as galvanic skin response devices, and instruments that measure response to electromagnetic stimuli, such as electromyelography, brain stem audiometry, magnetic resonance imaging (MRI) and electroacupuncture according to Voll (EAV). The galvanic skin response technique measures the electrical conductance between two electrodes placed on the skin. The patient is then subjected to various stimuli, and any change in skin conductance is recorded. Any stimuli causing increased sweat production will increase the conductance and give a change in the readings, which are usually recorded on a graph.
In the EAV method a low voltage electrical charge is introduced into the body, and the precise level of electric current conducted through the acupuncture points are measured. Information about various organ systems and musculoskeletal regions is obtained by the level of the readings.
The known devices have proven useful to various degrees in providing biomedical data to assist medical practitioners in diagnosis. However, the majority of the known techniques are invasive and require the application of electric current to the patient. Furthermore, the known techniques are subjective in nature and subject to wide variation in interpretation of indicative measures. A method and apparatus for passively collecting bioenergetic data is desirable. The collection of bioenergetic data, such as pulse rate, by monitoring of blood movement in the fingertip is known. Common devices for performing this function comprise a red or infrared light source and detector. The light incident on the fingertip penetrates a small distance into the fingertip and is modulated by absoφtion in the blood in the capillaries. A portion of the light is reflected or transmitted and this is measured by the detector. Thus the signal from the detector mimics the flow of blood through the fingertip.
These devices are not limited to use at the fingertip or with humans. Devices for use with animals commonly measure blood movement at the ear lobe, lip or tongue.
The majority ofthe applications of the device described above are for simple monitoring of pulse rate. In some applications, the signals from the device are analysed in more detail to separately identify the systolic and diastolic pulses. In recent times the devices have become more sophisticated with the advent of more intense light sources and more sensitive detectors. It is now possible to estimate the partial pressure of oxygen in the body by monitoring absoφtion of infrared light in the blood and making a number of assumptions. Devices performing this function are generally known as oximeters.
The inventors have found that a great deal more information can be obtained by monitoring blood flow in the fingertip than has previously been realised.
OBJECT OF THE INVENTION It is an object of the present invention to provide an apparatus for the monitoring and evaluation of observed cardiovascular response.
A further object of the present invention is to provide a method of monitoring and evaluating cardiovascular response.
Further objects will be evident from the following description.
DISCLOSURE QF THE INVENTION
In one form, although it need not be the only or indeed the broadest form, the invention resides in an apparatus for the collection of bioenergetic data comprising: monitoring means adapted to produce signals characteristic of blood flow; processing means in signal connection with said monitoring means and adapted to receive and analyse said signals to indicate the bioenergetic status of a body; and display means adapted to display the bioenergetic status so indicated. In preference the apparatus further comprises an isolation means in signal connection with the monitor means and processing means. The isolation means preferably provides electrical isolation between the monitoring means and the processing means so as to ensure that the relatively high voltages in the processing means cannot be transmitted to a patient through the monitoring means.
In preference the monitoring means comprises an oximeter adapted to monitor blood flow in an extremity, such as a fingertip or ear lobe. The oximeter preferably comprises a light source, detector means and interface means. The detector is preferably a photodiode. The light source may be a light emitting diode (LED) or diode laser emitting infrared or visible radiation. Preferably, there are two light sources, one emitting infrared radiation and one emitting visible radiation. The signals from the detector are indicative of the nature of the blood flow in the extremity. The interface means performs preliminary processing of the signals from the detector including converting the analogue detector signals to digital signals suitable for the processing means.
In preference the processing means is a microprocessor programmed to measure characteristics of the received signals. The measured characteristics include such characteristics as: the ratio of heart activity to heart rest the variation in systolic pulse amplitude over time the ratio of systolic pulse amplitude to diastolic amplitude variation in shape from pulse to pulse variation in pulse shape over time.
In preference the bioenergetic status of the body is indicated according to such functions as: pulse rate oxygen saturation in terminal tissue (SpO2) blood flow rate elasticity of blood vessels strength and regularity of the heart beat cardiac sufficiency cardiac valve activity cardiac or vascular metabolic abnormalities cell energy change latent hypertension myocardium damage cardiac or vascular inflammation allergic reactions immune system response changes pulmonary/cardiac function variations bioenergetic reactions at lining of intestine
The display means is suitably a high resolution video display adapted to display graphical and alphanumeric data. The graphical data preferably includes a representation of the measured pulse shape or a series of measured pulses. The alphanumeric data preferably includes indications of one or more of the above characteristics or functions.
In preference, the apparatus further comprises memory means in signal connection with the processing means. The memory means may provide transient storage of data, permanent storage of data or both.
The apparatus may further comprise an EKG module to provide an electrical readout of the heart function for an objective profile of the cardiac function, an allergy module for providing an objective computer based evaluation and assessment of electrodermal readings of known allergens by registering before and after microvoltage changes in response to allergens, and a pulse blood pressure module for providing diastolic, systolic and mean arterial pressure.
In a further form the invention resides in a method of collecting bioenergetic data of a body including the steps of: transmitting visible and infrared radiation into terminal tissue; measuring a voltage signal proportional to visible and infrared radiation transmitted through the terminal tissue; converting the voltage signal to a digital signal; passing the digital signal to a processing means; processing the digital signal in the processing means to produce a displayable waveform; and displaying the displayable waveform on a display means.
The method may include the further steps of analysing the waveforms to provide indicative measures of the cardiovascular health of the body.
BRIEF DETAILS OF THE DRAWINGS To further assist in understanding the invention reference will be made to the following drawings in which:
FIG 1 is a block diagram of the components of an apparatus for collection of bioenergetic data; FIG 2 is a detailed sketch of an oximeter;
FIG 3 is a schematic block diagram of the interface of the apparatus; FIG 4 shows a comparison of the waveform of a healthy person with a not so healthy person; FIG 5 is a trace showing the heart activity and amplitude ratio measurements;
FIG 6 is a trace showing an ATP ramp measurement;
FIG 7 is a trace showing an expansion of a dichotic notch region;
FIG 8 is a trace showing an expansion of a systolic pulse;
FIG 9 shows a comparison of a waveform for a patient before and after exposure to a therapeutic magnetic field;
FIG 10 is an expanded section of FIG 9; F FIIGG 1111 is a comparison of a waveform for a patient before and after exposure to an allergen;
FIG 12 is a flowchart of the operation of the apparatus; and
FIG 13 is a block diagram of additional modules for the apparatus.
DETAILED DESCRIPTION OF THE DRAWINGS In the drawings, like reference numerals refer to like parts. Referring now to the drawings in detail there is shown in FIG 1 a block diagram of a bioenergetic data collection apparatus according to a first embodiment. The apparatus comprises a monitor means 1, which in the preferred embodiment is an oximeter comprising a finger probe 2 and interface 3. Signal processing is performed in processing means 4. Associated with the processing means 4 is a display unit 5 and memory 6. In the preferred embodiment the processing means 4, display unit 5 and memory 6 together comprise a personal computer 7. The personal computer 7 may conveniently be a laptop computer thereby making the whole apparatus portable. The interface 3 is in signal connection with an isolation means, such as opto-isolator 8, which is in signal connection with the processing means 4. The interface 3 has its own power supply so the only requirement for connection between the oximeter 3 and personal computer 7 is for the transmittal of signals from the interface 3 to the computer 7 via the opto- isolator 8. The opto-isolator 8 primarily provides electrical isolation between the interface 3 and the processing means 4 to avoid any risk of electrical injury to persons using the apparatus.
The operation of the pulse monitor and finger probe are shown in more detail in FIG 2. A commercially available device such as a model 71000A2 pulse oximeter from BCI International may be modified for use in the bioenergetic data collection apparatus. The finger probe comprises an infrared light source 9, a red light source 10 and a detector 11. In normal operation the oximeter determines SpO2 and pulse rate by passing two wavelengths of light, one red and one infrared, through body tissue 12 to the photodetector 11. The light sources are pulsed and the photodetector signal is sampled at 120Hz. During measurement, the signal strength resulting from each light source depends on the colour and thickness of the body tissue, the probe placement, the intensity of the light sources, and the absorption of the arterial and venous blood (including the time varying effects of the pulse) in the body tissues.
The oximeter processes these signals, separating the time invariant parameters (tissue thickness, skin colour, light intensity, and venous blood) from the time variant parameters (arterial volume and pO2) to identify the pulse rate and calculate oxygen saturation. Oxygen saturation calculations can be performed because oxygen saturated blood predictably absorbs less red light than oxygen depleted blood.
The signal from the interface 3 is a time varying voltage with fast amplitude changes. The processing means 4 requires signals in a digital form so the interface 3 is required to sample and digitise the signal from the probe 2. Prior art devices have applied a relatively course digitising filter which has resulted in the loss of information rich high frequency components of the signal.
The commercially available oximeter requires two primary modifications for use in the bioenergetic data collection apparatus. Firstly, the output port of the interface 3 is adapted for connection to a standard serial port of a personal computer. Secondly, the bandpass of the interface 3 is modified to allow high frequency components to be transmitted to the processing means. Commercial devices routinely include a band-pass filter to remove high frequency components and thereby obtain a more stable reading of the relatively low frequency pulse rate and SpO2 values. The interface 3 provides a local readout of pulse and SpO2.
The inventor has found it useful to filter out very low frequency signals that are caused by movement of the patient. Although the filtering can be performed in hardware by modification of the oximeter it is convenient to provide software filtering in the processing means. A schematic block diagram of the interface 3 is shown in FIG 3. A standard microprocessor kernel 13 is formed by microprocessor 14, RAM 15 and EPROM 16. Communication is provided on address bus 17. A current to voltage converter 18 converts the current output of the detector 11 to a voltage readable by the analogue to digital converter 19. The analogue to digital converter 19 performs a 12-bit conversion and places the digital result on data bus 20. The microprocessor 14 analyses the data to provide the local display and outputs the digital data through serial port 21.
The processing means 4 may be a personal computer programmed to analyze the signals received from the interface 3. The personal computer may conveniently be a laptop computer which facilitates mobility of the apparatus. In the described embodiment the display means 5 is included as the monitor of the personal computer or laptop computer. In an alternative embodiment a purpose built processing means may be packaged into a compact container. The apparatus may be operated in two main modes. In a first mode the apparatus monitors and collects data on the pulse of a subject. In this mode the apparatus is able to provide data in a form that facilitates diagnosis by a skilled medical practitioner. An example of the graphical data obtainable in this mode is given in FIG 4. Fig 4a shows a pulse trace recorded for a 20 year old male in good physical condition. The systolic 22 and diastolic 23 pulses are well-defined and clean. In contrast, Fig 4b shows a pulse trace for an individual in poor physical condition. The systolic and diastolic traces are poorly defined and very irregular. This trace indicates serious vascular problems.
Further analysis can be conducted on the recorded traces. Fig 5 is a screen dump of a display demonstrating the calculation of heart activity. The X-axis 24 is marked in seconds and the Y-axis 25 is in arbitrary units. Identifying information including the date, file number, scale, SpO2 and pulse rate are printed below the X-axis.
Heart activity is defined as the ratio of heart action to heart rest, which in the figure is calculated by D-B/H-B. The result ofthe calculation is shown on the screen at 26. The value provides useful information to a physician to aid in diagnosis. An amplitude ratio can also be calculated. The amplitude ratio is defined as C-A E-A. The result may also be shown on screen.
Fig 6 shows how the apparatus can be used to display and compare the ATP ramp angle. The angle of dotted line 27 can be set by the physician at the ATP ramp angle considered to be ideal for the patient and situation. The variation of a trace from the ideal angle is immediately evident. In the example of Fig 6 the region 28 is good but the other regions, such as 29, deviate to a small degree. It will be appreciated that the example of Fig 4b would show a marked deviation. Regions of the pulse trace can be windowed and expanded as demonstrated in Fig 7. In Fig 7 the region around the dichotic notch has been expanded to show the high frequency components. It is generally accepted that this region of the pulse trace is indicative of gastrointestinal tract health. A bowel irritation may be manifest in an increase in high frequency components in this region. If every pulse in the trace shows a 'bump' in the ATP ramp region there is likely to be a colon problem. If the 'bump' is intermittent, the problem is probably with ATP production (eg fatigue). The apparatus provides a display of this region to assist the physician to make a correct diagnosis.
In Fig 8 the region around the top of the systolic pulse trace is enlarged. The shape of the trace in this region is generally accepted as indicative of the health of the aortic valve. A double peak is bad, whereas a single peak, such as 30, indicates good aortic valve condition. The physician can also obtain an estimate of the volumetric blood flow by measuring the height and width ofthe systolic pulse. This may also be used to diagnose overall heart condition. In a second mode the data before a change can be stored in memory
6 and compared with data obtained after the change and an analysis provided. The change may be the application of a therapeutic magnetic field such as could be applied by the device described in United States patent number 5527259. Fig 9 indicates the differences that can be observed before and after the application of therapeutic magnetic fields.
In Fig 9 the entire trace acquired over 30 seconds is shown. The lower trace, trace B, is the first acquired trace prior to application of a therapeutic magnetic field. The full trace is useful for showing pulse trends such as the variation in the pulse baseline 31. It Is clear in the lower trace that there is considerable variation in the baseline. In contrast the baseline 32 in the upper trace is relatively flat.
The scale can be expanded to highlight a subset of pulses. The first five seconds ofthe traces in Fig 9 are shown in Fig 10. This mode of display is useful for identifying changes in the pulse shapes as opposed to the pulse trends identified from Fig 9. It is clear from Fig 10 that the 'bumps* 33 evident in the ATP ramp of the lower trace are gone from the upper trace after application of therapeutic magnetic fields.
A comparison between traces can also be made to detect the impact of detrimental influences on the body. One such application is the identification of allergic response. Fig 11 shows a comparison of traces taken without (lower trace) and with (upper trace) allergenic influence. The allergenic influence may be applied by a patient simply holding a vial containing allergenic materials. Kits of allergens can be obtained from homeopathic suppliers such as the Practitioner Test Kit obtainable from Brauer Biotherapies Pty Ltd. Fig 11 clearly shows a disruption of the ATP ramp as indicated by 34a in the lower trace and 34b in the upper trace. This disruption can be used by a physician to diagnose allergic reaction to different allergens.
A flow chart of the operation of the apparatus is shown in Figs 12a, 12b and 12c. An initial set-up routine sets up the apparatus according to parameters selected by the user. These parameters include the communications, display and analysis parameters (such as ATP ramp angle).
The name of the patient is keyed into the apparatus for data storage purposes. If the patient is a new patient a new database is opened. If the program detects the name of an existing patient the historical data for that patient is retrieved .
Once the equipment is set-up and the patient information is entered, data collection is commenced. A sub-routine checks synchronisation between the oximeter and the processing means. If the units are not synchronised or synchronicity is lost, the data collection process is recommenced.
The collected data is high pass filtered, displayed on the display means in real time and stored in a temporary buffer. The pulse rate and SpO2 values are read from the oximeter interface and displayed. Data collection continues for a timed period or until terminated by the operator. Upon completion of data collection the patient record number is advanced by one and the data is saved to the patient data base. Notes can be entered by the operator if desired.
Comparative data is then retrieved and displayed on the display means with the recorded data. The comparative data may be previous data from the same or a different patient or may be standard data from a compiled library. The operator is able to make a number of comparisons between the new recorded data and the other data on screen. The waveforms can be shifted or scaled as desired.
The patient records or patient data can be deleted or renamed if required. Certain fragments ofthe waveforms can be zoomed for calculation of indicative diagnostic values. Indicative diagnostic ratios include the heart activity or time ratio and the amplitude ratio.
The ATP ramp line may be drawn by using a mouse or cursor keys to move a cursor to the start of an ATP ramp. The line is drawn at an angle provided at set-up.
A printer interface is provided in the software so that the waveforms and notes may be printed as required. Help files are also provided to assist users ofthe apparatus. The help files provide details of operating procedures as well as descriptions of common waveforms.
The apparatus may incorporate additional modules to extend the data collection functions to include a diagnostic capability. Fig 13 is a schematic of the modular nature of the invention. The primary module, as described in detail above, is known by the inventors as the Magnagraph ™ 35. An EKG Module 36 may interface to the Magnagraph ™ 35 to provide an electrical readout of the heart function which, added to the Magnagraph ™ physical and mechanical evaluation, renders a complete and objective profile of the cardiac function. A Pulse Blood Pressure Module 37 provides diastolic, systolic and mean arterial pressure, creating a comprehensive and objective evaluation of the profile of the cardiac function. An Allergy Module 38 provides an objective computer based evaluation and assessment of electrodermal readings of known allergens by registering before and after microvoltage changes in response to allergens.
Previously, the allergen response described earlier could only be interpreted subjectively. The Allergy Module 38 provides objective evaluation by comparing measured waveforms with a library of known responses. It will be appreciated that the apparatus and method described herein are useful for collecting and displaying bioenergetic data collected from a body. Although the description has been in terms of application to a human body it may equally be applied to animals. It will be further appreciated that the collected data can be analysed to varying degrees to provide information of greater value to a medical practitioner or veterinarian. It should be emphasised that the invention is not a prognostic device but only provides data for further consideration by an appropriately skilled practitioner.
The preferred embodiments described herein are intended to illustrate the principles of the invention, but not to limit its scope. Other embodiments and variations to the preferred embodiments may be evident to those skilled in the art and may be made without departing from the spirit and scope ofthe invention.

Claims (19)

1. An apparatus for the collection of bioenergetic data comprising: monitoring means adapted to produce signals characteristic of blood flow; processing means in signal connection with said monitoring means and adapted to receive and analyze said signals to indicate the bioenergetic status of a body; and display means adapted to display the bioenergetic status so indicated.
2. The apparatus of claim 1 further comprising an isolation means in signal connection with the monitor means and processing means, said isolation means providing electrical isolation between the monitoring means and the processing means.
3. The apparatus of claim 1 wherein the monitoring means comprises an oximeter adapted to monitor blood flow in an extremity, such as a fingertip or ear lobe.
4. The apparatus of claim 3 wherein the oximeter comprises at least one light source, detector means and interface means.
5. The apparatus of claim 4 wherein the light source is a light emitting diode (LED) or diode laser emitting infrared or visible radiation.
6. The apparatus of claim 5 comprising two light sources, one emitting infrared radiation and one emitting visible radiation.
7. The apparatus of claim 4 wherein the detector is a photodiode, said photodiode producing signals responsive to light received from the light source, said signals being indicative of the nature of the blood flow in the extremity.
8. The apparatus of claim 4 wherein the interface means performs preliminary processing of the signals from the detector means including converting the analogue detector signals to digital signals suitable for processing by the processing means.
9. The apparatus of claim 1 wherein the processing means is a microprocessor programmed to measure characteristics of the signals.
10. The apparatus of claim 9 wherein the measured characteristics are chosen from a list of measurable characteristics including: the ratio of heart activity to heart rest; the variation in systolic pulse amplitude over time; the ratio of systolic pulse amplitude to diastolic amplitude; variation in shape from pulse to pulse; and variation in pulse shape over time.
11. The apparatus of claim 1 wherein the bioenergetic status of the body is indicated according to indicative functions chosen from a list including: pulse rate; oxygen saturation in terminal tissue (SpO2); blood flow rate; elasticity of blood vessels; strength and regularity of the heart beat; cardiac sufficiency; cardiac valve activity; cardiac or vascular metabolic abnormalities; cell energy change; latent hypertension; myocardium damage; cardiac or vascular inflammation; allergic reactions; immune system response changes; pulmonary/cardiac function variations; and bioenergetic reactions at lining of intestine.
12. The apparatus of claim 1 wherein the display means is a high resolution video display adapted to display graphical and alphanumeric data.
13. The apparatus of claim 12 wherein the graphical data includes a representation of measured pulse shape or a series of measured pulse shapes.
14. The apparatus of claim 12 wherein the alphanumeric data includes indications of one or more measurable characteristics or indicative functions.
15. The apparatus of claim 1 further comprising an EKG module providing an electrical readout of heart function.
16. The apparatus of claim 1 further comprising an allergy module providing an objective computer based evaluation and assessment of electrodermal readings of known allergens by registering before and after microvoltage changes in response to said known allergens.
17. The apparatus of claim 1 further comprising a pulse blood pressure module for providing diastolic, systolic and mean arterial pressure.
18. A method of collecting bioenergetic data of a body including the steps of: transmitting visible and infrared radiation into terminal tissue; measuring a voltage signal proportional to visible and infrared radiation transmitted through the terminal tissue; converting the voltage signal to a digital signal; passing the digital signal to a processing means; processing the digital signal in the processing means to produce a displayable waveform; and displaying the displayable waveform on a display means. 19. The method of claim 18 further including the steps of analysing the waveforms to provide indicative measures ofthe cardiovascular health ofthe body.
AMENDED CLAIMS
[received by the International Bureau on 20 May 1997 (20.05.97); original claims 1-19 replaced by new claims 1-19
(3 pages)]
1. An apparatus for the collection of bioenergetic data indicative of bioenergetic status comprising: optical monitoring means adapted to produce time-varying signals characteristic of cardiovascular response, said time-varying signals including high frequency components; processing means in signal connection with said monitoring means and adapted to extract bioenergetic data from the time-varying signals and analyse said bioenergetic data to indicate bioenergetic status; and display means adapted to display the bioenergetic status so indicated.
2. The apparatus of claim 1 further comprising an isolation means in signal connection with the optical monitor means and processing means, said isolation means providing electrical isolation between the monitoring means and the processing means. 3. The apparatus of claim 1 wherein the optical monitoring means is adapted to monitor blood flow in an extremity, such as a fingertip or ear lobe, and comprises at least one light source, at least one optical detection means and interface means.
4. The apparatus of claim 3 wherein said at least one light source is a light emitting diode (LED) or diode laser emitting infrared or visible radiation.
5. The apparatus of claim 4 comprising a first light source emitting infrared radiation and a second light source emitting visible radiation.
6. The apparatus of claim 3 wherein said at least one detector is a photodiode, said photodiode producing time-varying signals responsive to light received from said at least one light source, said time-varying signals being characteristic of cardiovascular response evident in blood flow in terminal tissue at the extremity.
7. The apparatus of claim 5 comprising a photodiode producing time- varying signals responsive to light received from said first light source and producing time-varying signals responsive to light received from said second light source. 8. The apparatus of claim 3 wherein the interface means performs preliminary processing of the time-varying signals from the detector means including converting analogue signals from said at least one detector to digital signals suitable for processing by the processing means. 9. The apparatus of claim 1 wherein the processing means is a microprocessor programmed to perform an algorithm to calculate bioenergetic date from said time-varying signals and analyse said bioenergetic data to indicate bioenergetic status. 10. The apparatus of claim 1 wherein the bioenergetic data includes one or more measurable characteristics chosen from a list including : ATP ramp angle, the ratio of heart activity to heart rest; the variation in systolic pulse amplitude over time; the ratio of systolic pulse amplitude to diastolic amplitude; variation in shape from pulse to pulse; and variation in pulse shape over time. 11. The apparatus of claim 1 wherein the bioenergetic status of the body is indicated according to indicative functions chosen from a list including: pulse rate; oxygen saturation in terminal tissue (SpO2); blood flow rate; elasticity of blood vessels; strength and regularity of the heart beat; cardiac sufficiency; cardiac valve activity; cardiac or vascular metabolic abnormalities; cell energy change; latent hypertension; myocardium damage; cardiac or vascular inflammation; allergic reactions; immune system response changes; pulmonary/cardiac function variations; and bioenergetic reactions at lining of intestine.
12. The apparatus of claim 1 wherein the display means is a high resolution video display adapted to display graphical and alphanumeric data.
13. The apparatus of claim 12 wherein the graphical data includes a representation of measured pulse shape or a series of measured pulse shapes.
14. The apparatus of claim 12 wherein the alphanumeric data includes indications of one or more measurable characteristics or indicative functions. 15. The apparatus of claim 1 further comprising an EKG module in signal connection with said processing means, said EKG module adapted to produce signals characteristic of heart function, wherein said processing means analyses said bioenergetic data and said signals characteristic of heart function to indicate bioenergetic status.
16. The apparatus of claim 1 further comprising an allergy module in signal connection with said processing means, said allergy module comprising recording means adapted to record electrodermal readings in the form of before and after microvoltage changes occurring in response to known allergens, and analysis means adapted to provide signals characteristic of allergic reaction to known allergens by analysing said electrodermal readings and performing an objective computer based evaluation and assessment, wherein said processing means analyses said bioenergetic data and said signals characteristic of allergic reaction to indicate bioenergetic status.
17. The apparatus of claim 1 further comprising a pulse blood pressure module in signal connection with said processing means, said pulse blood pressure module adapted to provide signals characteristic of pulse pressure including diastolic, systolic and mean arterial pressure, wherein said processing means analyses said bioenergetic data and said signals characteristic of pulse pressure to indicate bioenergetic status.
18. A method of collecting bioenergetic data including the steps of : transmitting visible and infrared radiation into terminal tissue; measuring a voltage signal proportional to visible and infrared radiation transmitted through the terminal tissue; converting the voltage signal to a digital signal; passing the digital signal to a processing means; processing the digital signal in the processing means to produce a displayable waveform; and displaying the displayable waveform on a display means.
19. The method of claim 18 further including the steps of analysing the waveforms to provide indicative measures of cardiovascular health.
AU11861/97A 1996-01-04 1996-12-30 Bioenergetic data collection apparatus Ceased AU719852B2 (en)

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AUPN7407A AUPN740796A0 (en) 1996-01-04 1996-01-04 Biomedical data collection apparatus
AUPN7407 1996-01-04
PCT/AU1996/000841 WO1997024980A1 (en) 1996-01-04 1996-12-30 Bioenergetic data collection apparatus
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EP0597875A4 (en) * 1991-06-06 1995-02-08 Somanetics Corp Optical cerebral oximeter.
WO1994027492A1 (en) * 1993-05-21 1994-12-08 Nims, Inc. Discriminating between valid and artifactual pulse waveforms
EP0700267A4 (en) * 1993-05-28 1998-06-24 Somanetics Corp Method and apparatus for spectrophotometric cerebral oximetry

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