CA1301927C - Multiple-pulse method and apparatus for use in oximetry - Google Patents

Multiple-pulse method and apparatus for use in oximetry

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Publication number
CA1301927C
CA1301927C CA000544672A CA544672A CA1301927C CA 1301927 C CA1301927 C CA 1301927C CA 000544672 A CA000544672 A CA 000544672A CA 544672 A CA544672 A CA 544672A CA 1301927 C CA1301927 C CA 1301927C
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Prior art keywords
pulse
signal
magnitude
systole
oxygen saturation
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CA000544672A
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French (fr)
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Stephen J. Prosser
Robert E. Smith
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Physio Control Inc
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Physio Control Inc
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61BDIAGNOSIS; SURGERY; IDENTIFICATION
    • A61B5/00Measuring for diagnostic purposes; Identification of persons
    • A61B5/145Measuring characteristics of blood in vivo, e.g. gas concentration, pH value; Measuring characteristics of body fluids or tissues, e.g. interstitial fluid, cerebral tissue
    • A61B5/1455Measuring characteristics of blood in vivo, e.g. gas concentration, pH value; Measuring characteristics of body fluids or tissues, e.g. interstitial fluid, cerebral tissue using optical sensors, e.g. spectral photometrical oximeters
    • A61B5/14551Measuring characteristics of blood in vivo, e.g. gas concentration, pH value; Measuring characteristics of body fluids or tissues, e.g. interstitial fluid, cerebral tissue using optical sensors, e.g. spectral photometrical oximeters for measuring blood gases

Abstract

MULTIPLE-PULSE METHOD AND APPARATUS
FOR USE OXIMETRY
Abstract The disclosed invention is for use in extracting more accurate information from signals employed in pulse oximetry. Basically, pulse oximetry involves the illumination of arterial blood flowing in tissue with light at two wavelengths. Upon emerging from the tissue the light is received by a detector (38) that produces signals that are proportional to the intensity of the light received at each of the wavelengths. Each signal includes a slowly varyingbaseline component representing the attenuation .beta. (t) of light produced by bone, tissue, skin, and hair. The signals also include pulsatile components representing the attenuation .alpha. (t) produced by the changing blood volume and oxygen saturation within the finger. The signals produced by the detector (38) are converted by an analog-to-digital (A/D) converter (72) for subsequent analysis by a microcomputer (16). The microcomputer (16) extracts the following information from the signal corresponding to each wavelength. VH is determined to be the signal magnitude at a second pulse diastole. VL is, similarly, the signal magnitude at systole of the same pulse. A term .DELTA.V is identified equal in value to the difference in signal magnitudes at the adjacent systoles. Finally, valuesare determined for .DELTA.ts and .DELTA.tp, being the interval between an adjacent systole and diastole and the pulse period, respectively. The microcomputer (16) then determines a value for ROS in accordance with the relationship:

ROS =

Description

~L3 [)~92~

liqULT~LE!-PVISI~ MET~ODANDAPPARATUS
FOP~ llS3~ LN o~e aOETRY
Back~round of the Invention This invention re~ates to oximetry and, more partic~arly, to 5 ir~ormation extraction techniques developed for pulse o~metry.
The arterial oxygen saturation and pulse rate of an individual may be of interest for a variety of reasons. For example, in the operating room u~
;~ t~dQte information regarding oxygen saturation can be used to signal changing physialogical factors, the malfunction of anaesthesia equipment, or physician error. Similarly, in the intensive care unit, oxygen saturation information can be used to confilm the provision of proper patient ventilation and allow the patient to be withdrawn from a ventilator at an optimal rate.
In many applications, particldarly including the operating room and intensive care unit, continual information regarding p~se rate and oxygen saturation is important if the presence of harmful physiological conditions is to be detected before a substantiQl risk to the patient is presented. A noninvasiveteehnique is also desirable in many app3ications, for example, when a home health care nurse is performing a routine check-up, because it increases both operator convenience and patient comfort. Pulse transmittance oximetry is addressed to these problems and provides noninvasive, continual informfltion about pulse rate and oxygen saturation. The information produced, however, is only useful when the operator can depend on its accuracy. The method and apparatus of the present invention are, therefore, directed to the improved accuracy of such information without undue cost.
As will be discussed in greater detail below, pulse tr~nsrnittance - oximetry basically involves measurement of the effect arterial blood in tissue has on the intensity of light passing therethrough. More partic~darly, the volume of blood in the tissue is a function of the arterial pulse, with a greater volume present at systole and a lesser volume present at ~iastole. Because blood absorbs 3~ some of the light passing through the tissue, the intensity of the light emerging '~

` 130~92'7 from the tissue is inversely proportional to the volume of blood in the tissue.
Thus, the emergent light intensity will vary with the arterial pulse and can be used to indicate Q patient's pulse rate. In addition, the absorption coefficient of oxyhemoglobin (hemoglobin combined with oxygen in the blood, HbO2) is different from that o~ deoxygenated hemoglobin (Hb) for most wavelengths of light. Por that reason, differences in the amount of light absor~ed by the bloodat two different wavelengths can be used to indicate the hemoglobin oxygen saturation, 96SaO2 (OS), which equals ([HbO2]/([Hbl ~ ~HbO2]))x100%.
Thus, measurement of the amount of light transmitted through, for example, a 10 finger can be used to determine both the patient's pulse rate and hemoglobin oxygen saturation.
As will be appreciated, the intensity of light transmitted through R
finger is R function of the absorption coefficient of both "fixed' components, such as bone9 tissue, skin, and hair, as well as "variable" components, such as the vc~ume of blood in the tissue. The intensity of light transmitted through the tissue, when expressed as a function of time, is often said to include a DC
component, representing~ the effect of the fixed components on the light, and anAC pulsatile component, representing the effect that changing tissue blood volume has on the lighto Because the attenuation produced by the fixed tissue 20 components does not contain information about pulse and arterial oxygen saturation, the pulsatile signal is of primary interest. In that regard, many ofthe prior art transmittance oximetry techniques eliminate the DC component from the signal analyzed.
For example, in U.S. Patent No. 2,706,927 (Wood) measurements of 25 liht absorption at two wavelengths are taken under a ~'bloodless" condition and a "normal" condition. In the blooclless condition, RS much blood as possible is squeezed fro~ the tissue being analyzed. Then, light at both wavelengths is transmitted through the tissue and absorption measurements made. These measurements indicate the effect that aJl nonblood tissue components have on 30 the light. When normal blood flow hRs been restored to the tissue, a second set of measurements is made that indicates the influence of both the blood and nonblood components. The difference in light absorption between the two conditions is then used to determine the average oxygen saturation of the tissue, including the effects of both arterial and venous blood. As will be readily apparent, this process basically eliminates the DC, nonblood component from the signal that the oxygen saturation is extracted from.
For a number of reasons, however, the Wood method fails to provide the necessary accuracy. For example, a true bloodless condition is not ` ~3~9~927 practical to obtain. In addition, efforts to obtain a bloodless condition, such as by squee~ing the tissue, may result in a different light transmission path for the two conditions. In addition to problems with accuracy, the Wood approach is both inconvenient and time consuming.
A more refined approach to pulse transmittance oximetry is disclosed in U5O Patent No. 4,086,915 (Kofsky et ~1.). The Kofsky et al. refer-ence is of interest for two reasons. First, the technique employed automaticallyeliminates the effect that fixed components in the tissue have on the light transmitted therethrough, avoiding the need to produce bloodless tissue. More s 10 particularly, as developed in the Kofsky et al. reference frorn the Beer-Lambert law of absorption, the derivatives of the intensity of the light transmitted through the tissue at two different wavelengths, when multiplied by predete~
- mined pseudocoefficients, can be used to determine oxygen saturation. Basic mathematics indicate that such derivatives are substantiaUy independent of the DC component of the intensity. The pseudocoefficients are determined through measurements taken during a calibration procedure in which a patient first respires air having a normal oxygen content and, later, respires air of a reduced oxygen content. As will be appreciated, this calibration process is at best curn bersom e.
The second feature of the Kofsky et al. arrangement th~t is of interest is its removal of the DC component of the ~signal prior to being amplified for subsequent processing. More particularly, the signal is amplified to allow its slope (i.e, the derivative) to be more accurately determined. To avoidamplifier saturation, a portion of the relatively large DC component of the SigtlSl is removed prior to amplification. To accomplish this .emoval, the signal from the light detector is applied to the two inputs of a differenti~l amplifier as follows. The signal is directly input to the positive terminal of the amplifier.The signal is also passed through a low-resolution A/D converter, followed by a D/A con~rerter, before being input to the negative terminal of the amplifier. The A/D converter has a resolution of approximately 1/10 that of the input signal.
~or example, if the signal is at 6.3 volts, the output of the A/D converter would be 6 volts. Therefore, the output of the converter represents a substanti~l portion of the signal, which typically can be used to approxin~ate the DC signallevel~ Combination of that signal with the directly applied detector signal at the 3~ amplifier produces an output that can be used to approximate the AC signal. As will be readily appreciated, however~ the process may be relatively inaccurate because the output of the A/D converter is often a poor indicator of the DC
signal.

0~9~7 U.S. Patent NoO 4,167,331 (Nielson) discloses another pulse trans-mittance oximeter. The dis~osed oximeter is based upon the principle that the absorption of light by a material is directly proporffonal to the logarithm of the l;ght intensity after having been attenuated by ths ~bsor~er, as derived from the Beer-Lambert law. The oximeter employs light-emitting diodes (LEDs) to produce ligm at red and infrared wavelengths for transmission through tissue. A
photosensitive device responds to the light produced by the I,EDs and attenuatedby the tissue, producing an output current. That output current is amplified by a logarithmic amplifier to produce a signal having AC and DC components and containing imormation about the intensity of light transmitted at both wave-length~. Sampl~an~hold circuits demodulate the red and infrared wavelength signals. The DC components of each signal are then blocked by a serie~ bandpass amplifier and capacitors, eliminating the effect of the fix~d absorptive com-ponents from the signal. The resultarlt AC signal components are unaffected by fixed absorption components, such as hair, bone~ tissue, skin. An average value OI each AC signal is then produced. The ratio of the two averages is then used to determine the oxygen saturation from empirically determined values associated with the ratio. The AC components are also used to determine the pulse rate.
Another reference addressed to pulse transmittance oximetry is U.S. Patent No. 4,407,290 (Wilber). In that referen~e, light pulses produced by LRDs at two different wavelengths are applied to, for example, an earlobe. A
sensor responds to the light transmitted through the earlobe, producing a signalfor each wavelength having a DC and AC component res~dting from the presence Of constant and pulsatile absorptive components in the earlobe. A normalization circuit employs feedback to scale both signals so that the DC nonpulsatile components of each are equal and the offset voltages removed. Decoders separate the two signals, so controlled, into channels A and B where the DC
component is removed from each. The remaining AC components of the signals are amplified and combined at a multiplexer prior to analog-t~digital (A/D~
conve~sion. Oxygen saturation is determined by a digital processor in acco~
dence with the following relationship:
X1R( ~1) + X2R( ~2) OS =X3R( ~lJ + X4R~ A2) whereîn empirically derived data for the constants Xl, X2, X3 and X4 is stored in the processor.

62839-10~9 European Patent Publication No. 0102816, published March 14, 1984 (New, Jr. et al.l discloses an additional pulse transmittance oxime~er. Two LEDs expose a body member, for example, a finger, to light haviny red and infrared wavelenyths, with each LED having a one-in-four duty cycle. A detector produces a siynal in response that is then split into two channels. The one-in-four du-ty cyc:Le allows negatively amplified noise signals ~o be in~egrated with positively amplified si~nals, including the detector response and noise, thereby eliminating the effect of noise on the signal produced. The resultant signals include a substantially eonstant DC component and a pulsatile AC
component. To improve the accuracy of a subsequent analog-to-digital (A/D) conversion, a fixed DC value is subtracted from the slgnal prior to the conversion. This level is then added back in by a microprocessor after the conversion. Logarithmic analysis is avoided by the microprocessor in the following manner. For each wavelength of liyht transmitted through the finger, a quotient of the pulsatile componen~ over the constant component is determined.
The ratio of the two quotients is ~hen determined and fitted to a curve of independently derived oxygen saturations. To compensate for the diierent transmlssion characteristics of different patients' finyers, an adjustable. drive source for the LEDs is provided. In addition, an apparatus ~or automatically calibrating the device ls disclosed.
The prior art of oximetry has, however, failed to produce the type of highly accura~e, quiclcly responsive information needed to ensure user ~onfidence in the equipment.
This is particularly important in, for example, the operating room, where the availability of fast, reliable information about oxygen saturation may determine the success o~ the operation. The disclosed invention addresses this problem and produces an accuracy previously unattainable by oxlmeters.
Summarv of the Invention The present invention discloses a method of determining the oxygen saturation of arterial blood flowing in tissue that is illuminated with ligh~ at two waveleny~hs, the light being ~30~9~7 received upon emergence from the tissue by a detector that produces signals that are proportional to the intensity of the light received at each of the wavelengths. The method includes the steps of storing the magnitude of the signals at a plurality of sample times spaced over an interval greater than the period of one pulse and produ~ing a single indication of the oxygen sa~uratlon of ~he arterial blood from the sample times and the magnitudes of the signals stored at the sample times.

Sa 13~927 In accordance with particular aspects of the invention, the sample times and magnitudes of the signals stored at the sample times may ba proces ed in accordance with the relationships including~.
ln(Tl/TO)- mln(T3/T~ A
OS ln(Tl/TO) mln(T37~ 2 where: RoS = the single indication of the oxygen saturation;
~1- the first of the two wave~engths of the transilluminatin~
light;
~2 = the sscond of the two wavelengths of the transilluminating light;
To = 1:he m~gnitude of the signal at the diastole of a first pulse exhibited by the arterial blood, for the wav01ength indicated;
Tl = the magnitude of the signal at the systole of the first pulse, 5 for the wnvelength indicated;
T3 = the magnitude of the signal at the systole o~ a second ~se, for the wavelength indicated9 and m = the ratiC of the time between an adjacent diastole and systole to the time between adjacent diastole~.
ln[ VN ] @~ A

ln[VL _ ~ts~V/~tp)~ @ ~2 2 5 where~ RoS = the sin~le indication of the oxygen saturation;
?~1 = the first of the two wavelengths of the transilluminating light;
A2 = the seeond of the two wavelengths of the transilluminating light, VH = the magnitude of the signal at the diastole OI a second pulse exhibited by the arterial blood, for the wavelength indicated;
VL = the magnitude of the sign~l at the systole of the second pulse, :~ for the wavelength indicated;
V = the difference in the magnitude o~ the sign~l between the 35 systole of the second pulse and the systole of a first pulse, for the wavelength indicated;
~ ts = the difference in time between the systole and diastole of one of the first and second pulses, as measured from the signal eorresponding tothe wavelength indicated; and ~tp = the period of the pulse, as measured from the signal corresponding to the wavelength indicated.
In accordance with a further aspect of the invention, the method also includes the step of comparing the value of RoS produced with independently derived oxygen saturation curves to determine the oxygen satur~-tion of the arterial blood in the tissue. L;kewise, the step of producing an output indicative of the oxygen saturation determined can be included.
In accordance with another aspect of the invention, an apparat~
for performing the method as outlined above is provided. In its most basic form,0 the apparatus includes a sampler îor determining the signal magnitude at theplurality of sample times spaced over an interval greater than the period of snepulse. A processor then produces a single indication of the oxygen saturation from the sample times and signal magnitudes at those sample times. The appQratus m~y further include the detector, which produces the signals contain-in~ the oxygen saturation information, and a light source, which produces the light flt two wavelengths. A red filter may be used to filter the light received by the detector and the signals may be amplified by a differential current-to-voltage amplifier bef~re being sampled.
Brief Descri~tion of the Drawings The invention can best be understood by reference to the following portion of the specificAtion, talcen in conjunction with the accompanying dr~wings in which:
FI(~URE 1 is a block diagram of an oximeter including a sensoF
input/output (I/O) circuit, microcomputer, alarm, displays, power supply, and 2 5 keyboard;
FIGUXE 2 is a block diagram illustrating the transmission of light through an absorptive medium;
FIGURE 3 is a block diagram illustrating the transmission of light through the absorptive medium of FIGURE 2, wherein the medium is broken up 30 into elemental components;
FIGURE 4 is a graphical comparison of the incident light intensity to the emergerlt light intensity as modeled in EIGURE 2;
FIGURE 5 is a graphical comparison of thc specific absorption coefficients for oxygenated hemoglobin and deoxygenated h~moglobin as a 3 5 function of the wavelength of light transmitted therethrough;
FIGURE 6 is a block diagram illustrating the transmission of light through a block model of the components of a firlger;

FIGURE 7 is a graphical comparison of empiric~lly derived oxygen satur~tion measurements related to a measurable value determined by the oximeter;
FIGURE 8 is a graphical illustration of the transrnittQnce of light, 5 through tissue supplied with arterial blood, as a function of time over an interval encompassing two diastoles and systoles;
FIGURE 9 is a schematic illustration of the transmission of light at two wavelengths through a Iinger in accordarlce with the inven'don;
FIC~URE l 0 is ~ graphical plot ~s a function of time of the lO transmittance of light at the red wavelength through the finger, FIGURE ll is a graphical plot as a function of ffme of the transmission of infrared light through the finger;
FIGURE la is a more detailed schematic OI the I/O circuit illustrated in the system of FIGURE l;
15FIGURE 13 is a schematîc diagrarn of a conventional current-to-voltage amplifier circuit;
FIC~URE 1~ is a schematic diagram of a differential, current-to-voltage preamplifier circuit included in the I/O circuit of FIGURE 1;
FIGURE l5 is a graphical representation of the possible ranges of 20the I/O circuit output showing the de~ired response of the I/O circuit and microcomputer at each of the various possible ranges; and FIGURE 16 is a more complete schematic diagram of the micr~
computer illustrated in FIGURE l.
Detailed Descr~e~n 25Referring to the overall system block diagram shown in FIGURE l, a pulse transmittance oximeter lO employing this invention incl~des a sensor 12,input/output (I/O) circuit 14, microcomputer 16, power sou~oe 18, displays 2û, keyboard 22 and alarrn 24. Before discussing these elements in detail, however, an outline of the theoretic~l basis of pulse transmittance oximetry as practiced30by the oximeter of FIGURE l is provided.
~; An understanding of the relevant theory begins with a discu3sion of the Beer-Lambert law. This law governs the absorpffon OI optical radiaffon by homogeneous absorbing media and can best be understood with reference to FIGURES 2 and 3 in the follswing manner.
35As shown in FIGURE 2, incident light having an intensity lo impinges upon an absorptive medium 26. Medium 26 has a charflcteristic absorbance factor A that indicates the attenuating affect medium 26 has on the - incident light. SimilarlyJ a transmission factor T for the medium is defined as ~' ~' , . .

~3~ 27 g the reciprocal of the absorbance factor, I/A. The intensity of the light 11 emerging from medium 26 is less than To and can be expressed functionPlly QS theproduct Tlo. With medium 26 divided into a number of identic~l components, each of unit thickness lin the direction of light transmission) and hence the same transmission factor T, the effect of Tnedium 26 on the incident light lo is as shown in ~IGURE 3.
There, mediu~n 26 is illustrated as consisting of three comp onents 28, 30, and 32. As will be appreciated, the intensity 11 of the light emerging from component as is equal to the incident light intensity Io multiplied by the transmission factor T. Component 30 has a similar effect on light passingtherethrou~h. Thus, because the light incident upon component 30 is equal to theproduct TIo, the emergent light intensity I2 is equal to the produet TI1 or T-Io.
Component 32 has the same effect on light and, as shown in ~IGURE 3, the intensity o~ the emergent light I3 for the entire medium 26 so modeled is equ~l to TIa or T310. If the thickness of medium 26 is n unit lengths, it can be modeled as including n components of unit thickness. It will then be appreciated that the intensity of light emerging from medium 26 can be designated I,t and is equal toTnlo. Expressed as a function of the absorbance constant A, In ean also be written RS (l/An) Io~
From the preceding discussion, it will be readily appreciated that the absorptive effect of medium 26 on the intensity of the incident light Io is one of exponenti~l decay. Because A may be an inconvenient base to work with, In can be rewritten as a function of a more convenient base, b, by recogni~ing thatA~ is equal l;-u B ~ n, where is the absorbance coefficient of medium 26 per unit length. The term ~ is frequently referred to as the relative extinction coefficient and is equal to logbA.
Given the preceding discussion,- it will be appreciated that the intensity of the light In emerging from rnedium 26 can be expressed in base 10 as IolO ~ln, or in base e as 1Oe ~2n, where ~1 and a2 are the appropriate relative extinction coefficients for base 10 and base e respectively. The effectthat the thickness of medium 26 has on the en)ergent light intensity In is graphically depicted in FIGURE 4. If the light incident upon medium 26 is established as having unit intensity, FIGURE 4 also represents the transmission factor T of the entire medium as Q function of thickness.
The discussion above can be applied generally to the medium 26 shown in FIGURE 2 to produce:
Il= IOe 1 ~1) ~`

~3~927 -1~

where I1 is the emergent light intensity, Io is the incident light intensity, is the absorbance coefficient of the medium per unit length, 1 is the thickness of the medium in unit l~ngths, and the exponential nature of the relationship has arbitrarily been expressed in terms of bas~ e. Equation (l) is commor~y referredto as the Beer Lambert law of exponential light decay through a homogenous Qbsorbing medium.
With this basic understandling of the Bee~Lambert law, a discus-sion of its application to the problems of pulse rate and hemoglobin oxygen saturation measurement i9 now presented. As shown in FI(~URE 5, the absor~
tion coefficients for oxygenated and deoxygenated hemoglobin ~re different at e~rery wavelength, except an isobestic wavelength. Thus, it will be appreciated that if a person's finger is e~posed to incident light and the emergent light intensity measured, the difference in intensity between the two, which is the amount of light absorbed, contain~ Information relating to the oxygenated hemoglobin content of the blood in the finger. The manner in which this information is extracted from the Bee~Lambert law is discussed below. In addition, it will be appreciated that the volume of blood contained within an individual's finger varies with the indi~idual's pulse. Thus, the l~hickness of the flnger also varies slightly with each arterial pldse, creating a changing path 2~ length for li~ht transmitted through the finger. Bec~use a longer lightpath allows addition~l light to be absorbed, time-dependent information relating to the difference between the incident and emergent light intensities can be used to determine the individual's ~ulse. The manner in which this information is extracted from the Beer-Lambert law is also discussed below.
As noted in the preceding paragraph, inform~tion about the inci-dent an~ emergent intensities of light transmitted through a finger can be used to determine oxygen saturation and pulse rate. The theoretical basis for extracting the required information, however, is complicated by several pro~
lems. For example, the precise intensity of the incident light applied to the finger is not easily determined. Thus, it may be necessary to extract the required information independently of the intensity of the incident light.
~urther, because the changing volume of blood in the finger and, hence, thickness of the lightpath therethrough, are not exclusively dependent upon the indivi~ual's pulse, it is desirable to eliminate the changing path len~h as a 3 5 variable from the computations.
~; The manner in which the Beel~Lambert l~w is refined to eliminate the incident intensity and path length as variables ls as follows. With reference to ~IGURE 6~ a human finger is modeled by two components 34 and 36, in a manner similar to that shown in ~IGURE 3. Component 34 models the unchang~

130~927 ing absorptive elements of the finger. This component includes, for example, bone, tissue, skin, hair, and baseline venous and arterial blood, and has a thickness designated d and an absorption ~.
Component 36 represents the changing absorptive portion of the 5 finger, the arterial blood volume. As shown, the thickness of this eomponent is designated ~1, representing the variable nature of the thickness, ~md the arterial absorption o~ this component is designated c~ representing the arterial blood absorbance.
As will be appreciated from the earlier analysis with respect to - 10 FIGURE 3, the light I1 emerging from component 3~ can be written ~s a function OI the incident light intensity lo as follows:

I1 IOe (2) Likewise, the intensity of light I2 emerging from component 36 is a function of its incident light intensity I1, and:

Ia = Ile a ~ 1 (3 Substitution of the expression for Il developed in equation (2) for that used inequation (3), when simplified, results in the following expression for the ;ntensity I2 of light emerging from the finger as a function of the intensity of light Io incident upon tile finger;

12 = 10e~ [ ~ 1 + o~ ~ 1] (4) Because our interest lies in the effect on the light produced by the arterial blood volume, the relationship between I2 and Il is of partic~ar i~terest. Defining the change in transmission produced by the arterial component 36 as T~A, we 30 have:
: I2 '1`
' ;~ A I~ (5) Substituting the e2cpressions for Il and I2 obtained in equations (2) and (3), res 35 pectively, equation (5~ becomes:
I e~[ ~1+~1]
T~ A = ~ (6) ~ 13~927 lt will be appreciated that the Io term can be cancelled from both the numerator~nd denominator of equation (6), thereby eliminating the input light intensity as a variable in the equation. With equation (6) fully simplified, the change in arterial transmission can be expressed as:

T ~A= e a~l (7) A device employing this principle of operation is effectively self-calibrating9 being independent of the incident light intensity Io~
At this point, a considerQtion of equation (7) reveals that the 10 changing thickness of the finger, ~1, produced by the changing arterial bloodvolume still remains as a variable. The ~I variable is eliminQted in the following rnanner. For convenience of expression, the logarithms of the terms in equation (7) are produced with respect to the same base originally employed in equation (1). Thus, equation (7) becotnes:

ln T~ A = ln (e ~ a~l (8) A preferred technique for eliminating the Ql variable utilizes information drawnfrom the change in arterial transmission experienced at two wavelengths.
The particul~r wavelengths se~ected are deterrr~ined in part by consi~eration of a more cornplete expression of the arterial ~bsorbance a:
, L = t ~ o)(~)S~ D~ ) (g) where a O is the oxygenated arterial absorbance9 a. D is the deoxygenated arterial absorbance, and OS is the hemoglobin oxygen saturation of the arterial blood volume. As will be appreciated from FIGURE 5, ~O and ~D are substantially unequal at all light wavelengths in the red and near infrared wav~Length regions except for an isobestic wavelength occurring at a wavelength of approx~mately 805 nanometers. With an arterial oxygen saturation OS of approximately 90 percent, it will be appreciated from equation (9) that the arterial absorbance a is 90 percent attributable to the oxygenated arterial absorbance aO and 10 percent attributable to the deoxygenated arterial absor-bance ~D. At the isobestic point wavelength9 the relative contribution of these two coefficients to the arterial absorbance a is of minimal significance in thatboth O and aD are equ~l. Thus, a wavelength roughly approximating the isobestic wavelength of the curves illustrated in FIGURE 5 is ~ convenient one ~:30~27 for use in eliminating the change in finger thickness A1 attributable to arterial blood flow.
A second wavelength is selected at a distance from the approxi-mRtely isobestic wavelength that is sufficient to aUow the two signals to be 5 easily distinguished. In addition, the relative dif~erence of the oxygenated and deoxygenated arterial absorbances at this wavelength is more pronounced. In light of the foregoing considerations, it is generaUy preferred that the two wavelengths selected faLI within the red and infrared regions of the electro-magnetic spectrum.
The foregoing information, when combined with equation (8) is used to produce the following ratio:
.. . .

~T~ ~ ~IR (10 where T~AR equals $he change in arterial transmission of light at the red wavelength 1~ R and T ~ AIR is the change in arteri~l transmission at the infrared wavelength ~ IR. It wiU be appreciated that if two sources are positioned at substantially the same location on the finger, the length of the lightpath through the finger is substantially the same for the light emitted by 20 each. Thus, the change in the lightpath resulting from arteri~l blood flow, ~1, is substantially the same for both the red and infrared wavelength sources. ~or that reason, the Q 1 term in the numerator and denominator of the right-hand side of equation (10) cancel, producing ln T ~kR ~ @
l T = ~~
As will be appreciated, equation (11) is independent of both the incident light intensity Io and the change in finger thickness ~1 attributable to arterial blood flow. The foregoing derivations form the theoretic~l basis of pulse oximetry measurement. Because o~ the complexity of the physiological process, howeYer, the ratio indicated in equation (11) does not directly provide an accurate measurement of oxygen saturation. The correlation between the ratio of equation (11) and actual arterial blood gas measurements is, therefore, relied on to produce indication oî the oxygen saturation. Thus, if the ratio of the arterial absorbance at the red and infrared wavelengths can be determined, the oxygen saturation of the arterial blood flow can be extracted from such independently derived calibration curves in a manner independent of Io Qnd ~1-~L3~1~27 For simplicity, a measured ratio RoS is defined from eguation (11) as:
Ratîo = RoS = ~ ' R (12) It is this value for RoS that is plotted on the X-QXiS of independently derived oxygen saturation curves, as shown in FIGURE 7 and discussed in greater detail below, with the hemoglobin oxygen saturation being referenced on the y-axis.
The preceding discussion treats the absorption coefficients ~ and a for the unchanging and changing absorptive components in the finger as being constant as a function of time. It has been found, however, th~t the production of highly accurate oxygen saturation informQtion requires that the time depen-dency of ~ ~nd o~ be considered. Thusg the discussion below of the manner in which RoS is measured begins with a brief outline of the time-dependent 15 fun~tions ~ (t) and a (t). The effect of these functions is then included in the synthesis of an easily measurable expression for Ros~
Variations in the absorption coefficients as a flmction of time may result for a variety of reasons. For example, changes in patient physiology other than arterial blood flow characteristics may significantly affect the "fixe~' 20 component absorption coefficient ~(t). Similarly, relatively smaU changes in blood composition may significantly nffect the arterial absorption coefficient a (t).
The transmission of light through a finger is illustrated in ~; FIGI~RE 8, as a function of time, and shows the eYIect of the t`ixed and arterial 25 absorption coefficients ~ (t) and ~ (t), expressed as a function of time. Thetransmittance plotted in FIGURE 8 includes two maxima and minima eorrespond-` ing to adjacent diastales and systoles of the arteri~l blood flow in the finger. A
first diastole occurs at time to and the transmittance at that point is designated To~ As will be appreciated, arterial blood volume is at a minimum during 30 diastole and, therefore, the transmittance To is at a maximum. That diastole is followed by a systole at time tl where the transmittance is indicated as Tl.
Because arterial blood volume is at a maximum at systole, the amount of light absorbed is likewise at a maximum and the transmittance Tl is at a minimum.
After t~, a second diast~le occurs at time t2 having fl transmittance of T2 and is 3~ followed by a systole ~t tinne t3 having a transmittance of T3.
Turning now to the derivation of a measurable exp~ession of RoS~
as will be appreciated from the previous discussion of the Beer-Lambert law, the ~0~ 7 intensity of light emerging from the finger 12 ean be expressed as a function ofthe incident light intensity lo in the following manner:

= I e~ [ ~ (t) + ~ (t)] (13) Adopting the convention of FlGURE 8, wherein subscripts are used to identify points in time, the relationship of equation (13) is expressed at a partic~ar time n as:

I2n = Ibe [ ~(tn) (tn)~ (14) The lack of a subscript n for the incident light intensity lo indieates that Io is presumed constant and not a function of time.
To obtain a measurable expression of RoS~ more complete expres-sions of the two absorption coeIficients ~s ~ funetion of time are needed. This requires that several assumptions be made. As apparent from FIGURE 8, any change in transmittance between adjacent diastoles is determined substantially entire3y by the changing attenuation in emergent light intensity I2 produced by the fixed absorptivc component. Thus, the change in transmittance between adjacent diastoles is proportional to the change in the absorption coefficient B(t) and9 for the r~ilatively short intervQI between adjacent diastoles, can be approximated as a strai~ht line. Expanding the expression of ~ as a function of ~` time, we get:

13(t)= Bog~t? (15) where ~0 is the magnitude of the absorption coefficient at time to and g(t) is an expression of the change in ~ as a function of time following time to~ As noted,this change can be approximated linearly and, therefore, can be expressed as:

g(t3 = 1 + b(t to) (16) where b is the slope of the linear change in transmittance between the diastolesat to and t2. Arbitrarily establishing tiMe tl~ as a reference point having a zero 35 value9 substitution o~ equation (16) into equation (15) produces:

~ (t) = ~ o(1 ~ bt) (17) An expanded expression of the arterial absorption coefficient a as a function of time ean be produced in a similar manner. As will be appreciated from FIGURE 8, the change in transmittance between the systoles at times t1 and t3 is proportional both to the changing fixed and arterial absorptive 5 components in the finger. With ~ (t) expressed as a linear function during this interval, the change in transmittance due to the arteri~d absorption coefficienta(t) can likewise be approximated as a linear function. Therefore, a(t) can be expressed more completely as:
a(t)= ~oK~lf(t3 (18) where ~0 is the magnitude of the arterial absorption eoefficient at tirne to~ K is a constant, ~l is the length of the path through which the light must pass as a function of blood volume, and f(t) is an expression of the change in a as a 15 flmction of time following to~ Assuming that f(t) is approximately linear over a short interval following to~ it can be expressed more completely as:
f(t) = 1 + a(t - to) (19) 20 where a is the portion of the slope of the transmittance between times t1 and t3 that is attributable to the change in a (t) rather than ~(t). Recognizing that time to has been established as a reference point having a zero value, substitution of equation (19) into equation (18) yields:

a (t) - aOK ~1(1 + at) (20) $ As defined in equation (12), the rE~tio RoS~ from which the oxygen saturation is determined by reference to empirically derived calibration curves,is a function of the arterial a~sorption coefficient at the R and IR wavelengths.
30 From equation (20~, it will be appreciated that further development is required to produce an expression OI Ros in terms of parameters that can be easily measured by instrumentation. More partic1llarly, an expression of Ros that is independer.t of aO, ~0, K, Ql, a, and b is needed. Because the transmittances at adjacent systoles and diastoles can be represented as voltages, an expression35 of RoS dependent or~y upon the transmittances is sought. In that regard, the following equations are àeveloped to express the variables to be eliminated (e.g., aO) as a function of the transmittances.

2~

As a first step in that process, the transmittances at the adjucent diastoles and systoles i]lustrated in EiIGURE 8 are developed using the ~eer-Lambert law. As will be appreciated, the transmittance T1l at any time t~ can be expressed as:

Tn l (21) o Substitution of equation (14) into equation (21) produces:

I e~ [ e (tn) + ~ (tn)] e~ [ ~ (tn) + (x (tn)] (22) As noted previously, at the diastoles, a minimum blood volume is present. This minimum blood volume causes the al term in the expression of the arterial absorption coefficient shown in equation (20) to approach & zero value. There-15 fore, at times to and t2) the expression of the arterial absor~ption coefficient as afunction of time in the exponential term of equation (22) goes to zero and can be ignored. Thus, the transmittance at time to can be expressed as:

To = e [ ~(to) ] = e ~ (to) (23) ~0 Substitution of equation (17) into equation (23) produces:

T0=e ~o(1 ~bto)-e-~o(l+b(o))=e-~o (24) given the establishment of the time to as a reference point having a zero value.At systole, both absorption coefficients remain in the exponential term of equation (22). Therefore, the substitution of equations (17) and (20) into equation (22) allows the transmittance at time t1 to be expressed as:

Tl = e [ ~ (tl~ + ~ (tl~] = e~ [ ~ o(l + btl) + cl oKa l(1 + atl)]

ReturniIlg to the second diastole, because the value of ~
- approaches zero, the arterial absorption coefficient in equation (22) is again 35 substantially equal to zero and the substitution of equation (17~ into equation (22) produces a transmittance at time t2 that is equal to:

T [ ~ (t2) + a (t2~] = e~ [ ~ o(l + bt2) ~ ] = e ~ D(1 2) ~26) Substitution of equations (17) and (20) into equation (22) allows the transmittance at the second systole, occurring at time t3, to be expressed as:
T3=e ~(t33~o~(t3)~ =e-[~O(l+bt3)+ ~OK~l(l+at3)]

Thus, we now have expressions for the transmittances at adjacent systoles and diastoles expressed as functions of the variables that are to be eliminated.
To simplify the expressions of equations (24), (25), (26), and (27), several expressions relating to the timing of the systoles and diastoles are lO developed. For example, the pulse interval between adjacent systoles or diastoles can be designated tp and, as will be appreciated from FIGURE 8, expressed QS:

tp = t2-to = t2 ~ 0 = t2 1 (28) where time to has been established as a referellce point having a zero value, and a unit pulse duration has been assumed. Thus, as n result of these arbitrary assignments, we have:

t = 0 arld t = 1 (29) E;rom FI~URE 8, it will be appreciated that the ratio of the time between an adjacellt diastole and systole to the time between fldjflcent diastoles, designated m~ can be expressed as:
m =~di~sto]e 0 = a ts = tl to (30) tdiastole 2 tdiastole o ~tp t2 to Equation (30) can be simplified by use of the relationsllips expressed at (29), re3ulting ;n:
t1 0 m = 1 _ 0 = tl (3l) Because the interval between an adjacent systole and diastole will not change significantly between adjacent pulses, the ratio m can also be 35 expressed as:
m = ts~stole 3 diastole 2 = ~ ts = t3 t2 (32) diastole 2 diastole 0 ~ ~P t2-to ~3~9;~7 Substitution of the relationships expressed at equation (29) into equation (32),when simplified, yields:
t3 - 1 (33) and:
t3 = rn + 1 (34) In summary, tlle timing of the adjacent systoles and diastoles can be expressed in simplified form as:

to = ~ tl = m, t2 = l, t3 = m~1 (35) Substitution o~ tlle vnlues expressed in (35) for the transmittances determined in equations (24), (25), (26) anc] (27) produce the following expressions for transmittance:

To = e ~0 (3G) T1 = e [ ~ O(1~bm) + a ok ~ am)] (37) T =e-[ ~o(l~b)] (38) T3 = e ~ [ ~ o(1-~b(l+m)) + ~ ok ~ l(l+a(1-~m))] (39) While tlle development of the transmittance equations (36)-(39) brings us closer to a measurable expression of ~Ros~ further simplification is still required. For that reason, the ratio between the transmittances at an adjacent systole and diastole, as well as the ratio between the transmittance at adjacent30 systoles and at adjacent diastoles, will now be computed. This process eliminates terms from the exponentials, making them more manageable~ and its use in producing an easily measurable expression of RoS will be shown below.
The ratio of transmittances between an adjacent systole and diastole can be expressed and simplified in the following manner:
Tl -[ B0(1~bm) + ~ok ~l(l+~m)~ = e~[ ~bm + OLok~l~l am)]
To e ~0 3~)~92'7 where the values for Tl and To were obtained from equations (37) and !36),respectively.
Similarly, the ratio between adjacent diastolic transmittanc~s is produced from the equations (38) and (36) as:
T2 = e ~= e~ ~ob (41) Finally, the ratio between adjacent systolic transmittances is produced from equations (39) and (37) as:

T3 = e~[ ~(l+b(1+m)) + t~Ok~ a(l+m))] - ( ~ b + o~ k~la) (42) Tl _~-- ~~- = e o e [ B 0(1+bm) + c~ ok ~ l(l+am)]
l 5 Because exponentials are somewhat awkward to work with, equa-tions (40), (41) and (42) cnn be simplified by taking the natural logarithm of each side of the equations. Thus, we have:
ln Tl = ~ [ ~Qbm + ~Ok~l(l~am)] (43) ln T2 =- ~ob (44) ln T = ~ ( ~ob ~ aOk~la) (45) As noted earlier, to develop an easily measurable expression for R~S requires that expressions for aO, k, and al be produced as a function of the transmitta~ces. To this end, equations ~43) and (45) can be rewritten to 3 produce:
- ~ln (T3/Tl) + I) ~0] - [ln (Tl/T0) _ (463 0 a l~am Equation ~46), however, still includes a number of terms which cannot be directly measured. Thus, an equation independent of the ter]ns a, b, a~d ~0 is desired.
If the negative Sigfls are canceled and each of the two right-hand portions of 3~ 9;~'7 equation (46) multiplied by the term a(l+am), equation (46) can be developed into the following relationship:

(l+am) [ln (T3/T1)+b ~ 0] = a [ln (Tl/TO) bm ~ O

Equation (47) is simplified in equations (48~(51) as follows:

In (T3/T1) + b ~ 0 + am ln ~T3/T1) + amb ~ 0 = a ~ln (T1/To) -~ bm ~ 0] (48) ln (T3/Tl) + b ~ O + a[mln (T3/T1) + mb ~0] = a [ln (Tl/TO)bm ~ 0] (49) ln (T3/T1) + b ~ 0 - a [ln (T1/To) + bm ~ 0 - mln (T3/T1) - mb ~ 0~ (50) ( 3/11) b ~ O = a [ln (Tl/To) - mln (T3/TI)] (51) Equation (51) can then be solved for "a" in the following manner:

ln (T3/T1) + b ~ 0 (52) a=ln`~;r--/'r~ mln~;~7T ) Substitution of equation (44) illtO equation (52) produces:
ln (T3/T1)- ln (T2/T0) (53) a lll-(~l~o~- mln~;l' 7T ) As will be remembered, equation (46) provides:
aOk~ o _~

and the substitution of equations (44) and (53) into equation (54) produces:
- ln (T1/To) - mln (T2/T0) (55) aOIc A 1 =
rln (T3/T1)- ln (T2/To) l+ m Ll -rT-7;~

~3(~9~'7 As will be appreciated from equations (10), (11) and ~12) of the basic theoretical discussions, the ratio used in oxygen saturation meRsurement, Ros~ can be expressed as:

OS a~l @ AIR ~@ A2 (56) Expanding the arteri~1 absorption coefficient a in terms of the foregoing nomenclature, equation (56) becomes:~

RoS ao-k~l @ A (57) As will be appreciated, substitution of equation (55) into the numerator and denominator of equation (57) results in:

1~ ln (Tl/To) - mln (T2/10) 1 -~ m ~rln (T37~ ln ~ 7iFu~7rln ~rl IU~
Ros = ln (Tl/'[`o~~ mln r2~10~ (58) 1 + m !lli rT3/rl) ~ T2/r0)7(l~ll~Fl/rro) - Inlll (T3/'--~`1~ @ ~ 2 Thus, an expression l`or the oxygen saturatioll ratio is produced that is independent of a, ~, Ic, and ~ s will be readily appreciRted"lowever, the resultnnt expression is somewhat unwieldy. Therefore, a more concise expres-sion is desired. In that regard, simplification of the numerator and denominator, identical except for the required solution at di:fferent wavelengths, is desired.
This common term is simply the right-hand side of equation (55) and, for conveniellce, is designated l~ A R ~ may be simplified RS follows:
[ln (TlTo) - mln (T3Tl)] [ ln (T1/To) - mln (T2/To)]
A [ln (T1/To) - mln (T3/Tl)3 ~ln (T3/T~ n ('r2/'rO) 1 L ( 1To) mln ~T3To)~
~ln (T1/To) - mln (T3/T1)] [ln (T1/To) - mln (T2/To)]
ln~T1/TO~nln~i~/T~ mln(T3/T-~- mln~

[ln (T1To) - mln (T3/T1)] [ln (T1To) - mln (T2/To)]
[ln (T1 jTo) - mln (T2/To)]
- ln (T~/To) ~ mln (T3/T1) (59) l9~

where In(Tl/T0) can be considered an uncorrected value of R~, and -mln(T3/Tl) is a corrective term. Given this expression of R~, Ro3 can be written:
ln(TI/TO)- mln(T3/T~
RoS i~;~t/T3~=mln(T3/Tl~ @ ~2 (60) Another expression of RoS can be produced from (59) by recogniz-ing that ln (y/x) = -ln (x/y). Thus, RA can be written:

R = -~ln (To/Tl~+ mln (T3/Tl)] (61) Further, because (z)ln (x/y) = ln (x/y)~, equation (Gl) can be reduced to:
l 5 R;~ = -[ln ~To/T1) ~ ln (T3/T1) 3 (62) which can be approximated as:

R ;~ [ln (To/Tl) + ln (l~m(T3/Tl-1))] (63) Given that ln x ~ ln y = ln xy, equation (63) can further be reduced to:

R;~ ^ - ln ~(TO/T~ m(T3/T1-1))] (64) Substitution of R~, as more simply expressed in equation (64), back into the numerator and denominator of equation (58) yields:
lnl(T0/T~ m(T3/Tl-l)~] @ ~1 (65) R~)S l~l~o/Tl~+m~T3/T~ ] @ ~ 2 As shown in FIGURE 9, a detector 38 placed on the side of a finger opposite red and infrared wavelength light sources 40 and 42 receives light at both wavelengths transmitted through the finger. The intensity of the red wavelength light received is plotted in FIGURE 10 as a function of time. I~ith aunitized input intensity, FIGURE 10 is essentially a more expansive depiction ofthe transmittance of FIGURE 8, considered for a particular wavelength. The intensity varies with, among other things, the arterial pulse, and has high and low values RH and RL. RL occurs substantially at systole, when arterial blood volume is at its greatest. RH, on the other hand, occurs substantially at " 3l30~9~7 --2~--diastole, when the arterial blood volume is lowest. As will be appreciated from FIGURE ll, the intensity of the infrared wavelength light received at detector 38 varies in a similar manner and has maxima and minima identified as IRH and IRL, respectively. As will be discussed in greater detail below, 5 detector 38 produces an output signal that includes information about RH, RL, IRH, and IRL, thereby allowing values for To~ Tl, T2, and T3 to be determined.
For convenience of expression, To may be desi~lated VH(indicating the voltage level at R~I or IR~I), while Tl may be designated VL (indicating the voltage level at l~L or IRL). Similarly, the change in systolic transmittance over one pulse, 10 T3-Tl, may be designated av. Thus, in derivative forrn:

T - l = ~I~ = V (66) 15 In addition, m can be expressed as:

m - Q ts (67) Substitution of equ(ltions (G6) and (67) into equatioll (6~i) yields the 20 equiv~lent of equation (65) in derivative form:
ln[(VEI/V~ ts/ atp)( QV/VL))] @ ~l (68) ln [ (V~ ~VL)(l ~( Q ts/ ~ tp)( QV/VL))] @ ~ 2 where ~ l and ~2 are broader expressions of the wavelellgths of light to which 25 the finger is exposed. Rquation (68) can then be simplified to:

ln [ (VH/VL)((VL+ ~ V ~ ts/ a tp)/VL)] @ A l ( 69) R~ =
vS ln [(VH/VL)((VL+ ~V ~ ts/ ~tp)/VL)] @ 2 The expression for Ros shown in equation (69) is, however, only - one expression usefu] in the performance of multiple-pulse measurement oximetry. More particularly, QS will be appreciated from equation (59) in FIC~URE 8, the development of equation (69) introduces a one-pulse time lag between the occurrence of the first information used in the computation of Ros and the actual computatioll of RoS~ To avoid this one-pulse time lag, another expression of RoS is produced. Initially, we rely upon the fact that the time-., ~3~927 dependent nature of the absorption coefficients is linear over the relatively small interval defined between pulses. Therefore, the corrective term mln (T3/Tl) of equation (59) can be included in the computation of Ro3 for the pulse defined by T2 and T3, as well as for the pulse defined by To and Tt. This 5 use of the corrective factor applicable to the preceding pulse for the current pulse detected allows equation (59) to be r eexpressed as:

R~ - ln T2 + mln T3 - ln [~ m(T3/rrl-l)3 (70) From equations (56) and (67) it will be appreciated that the equivalent of equation (70) can be e~Ypressed with derivatives as:
VH
R~ - ln VL(l + (~tS/~tP)(~V/VL)) (71) Use of the relationship 1 + x = l/(l-x) allows us to express equation (71) as:
V
R - ln VL- ~ts~V (72) ~tp ~ and, thus, RoS can be expressed as:

Ros ~ [VL - ~ts/\V/Z~-t-p7~ @ Al ln~vL - (~tS~V/.~t-~)] @ A2 which is our currently preferred manner of computing Ros~
A second expression useful in multiple pulse oximetry retains the one-pulse delay but includes an empirically useful averaging of the high and lowpeaks. According to this technique, the second term OI equation (59) is modified3 resulting in:

R~ = ln (To/Tl) + (m/2) [ln (T2/To) -~ ln (T3/Tl)]

~ ln ~To/Tl(l + ~m/2)(T2/TO-l) + (m/2)(T3/Tl-1))] (74) Thus, RoS may be expressed as:
ln~To/T~ (m/2)(T2/T~ - 1) + (m/2)(T3/TL ~ 1))] A1 OS r~O~TlTl + (~2~T27To ~ ~2~r3/rr~ ] A2 ( ~æ~

As will be appreciated, equation (70) can be expanded to include additional terms, increasing accuracy at the expense of computational com-plexity. Thus, equation (70) can be written:

L i J, k 6~ ] (76) where i, j, and k are positive and negative integers. RoS can then be expressed as:
ln [ T2/T3( 1 + i~k m l~(T./T . - 1))] @ ~ 1 Ros ln~ mk~ @ A 2 An expression of Ros can also be developed that is free from the one-pulse lag discussed above and includes the empirically usefLl averaging of 15 the high and low peaks. As will be appreciated from the discussion above, according to this technique, equation (70) can be developed into:

~ ln (T2/T3) ~ (m/2) [ln (T2/To) ~ ln (T3/Tl)]

~ ln T--(1-~ (m/2)(T2/T0-~ ' (m/2~(T3/T1-1)) (78) The formulations outlined above are b~ed on the linear interpola-tion of two pulses and worlc well for relatively slow changes in the absorption coefficients with time. For additional accuracy when the absorption coe~ficients25 change more rapidly, a higher order interpolation technique call be used. More particularly, with respect to FlGURE 17, a plurality of pulses of a signal produced in response to absorption coefficients that exhibit nolllinear change with time is illustrated. Thus, the var;ation in ~ ~t) over the interval may be represented as some interpolating function Po(t) and the combined change 30 attributable to the time-dependency of ~ (t) and ~ (t) represented as some interpolating function P1(t).
As will be appreciated from the preceding discussions and particu-larly equation (59), a representation of R ~, incorporating these nonlinear varia-tions can be produced that is expressed as:
` 35 R ;~ = ln (To/T~ n[Pl(t1)/P1(to)]

~3~

where Pl(t1) is equal to Tt and P1(to) is a term that must be interpolated from the norlinear change in absorption coefficients. Thus, Ros may be written:
l~l(To/rrl)+ ~ P1~t1)/P1(to)] @ ~1 RoS = In(TO/~rl) + ~ll[-Plrt-l)/pl-r~-o~ @ ~ 2 (80) Equation (74) can be further expressed with averaged high and low peaks as:

R = ln(T /T ) + 1/2 [ln(P1(t1)/P1(t~ ln(PO(tl)/ O O (81) 10 where Pt(tl) is equal to Tl, Po(to) is equal to To~ ~nd both Pl(tU) and Po(tl) must be interpolated from the nonlinear fu~ctions. This allows Ros to be computed as:
ln(Tu/'rl) + 1/2[11l(Pl(tl)/Pl(to)) + lll(Po(tl)/Po(to))]@Al ~OS = ln(TO/T~ 172 [ ln(~t l~/Pl~to~ + ln(PO~t~o(to~]@ ~2 ( An advantage of the foregoing measurement techniques is that in every form produced, the corrected value of E~ includes an initial ullcorrected term and a corrective term. When ~ (t) and a (t) are substantially constant withrespect to time, the corrective term equals zero and does not affect the 20 otherwise normally calculated value of E~;~ . With B (t) and ~(t) changing, however, the corrective terrn always improves the uncorrected value o R~.
Ei urther, even i~ the correction provided is incomplete, an effect like averaging is produced but within near-zero time lag. Therefore, a measurement that accurately tracks the changes in ~ (t) and a (t) is produced without time lag, 25 allowing re~l-time information to be developed.
It should be noted that the technique described does not necessarily require an accurately measured value for m. Even if the value of M is only approximated, a significant improvement over uncorrected computations res~ts.
For maximum correction, however, rn can be measured. For example, m can be 30 set initially, updated only occasionally, or continually updated.
Because ~V is the difference in VL between adjacent systoles, determination of RoS in this manner, unlike prior art techniques, requires that information be extracted from multiple pulses rather than one. Thus, the microprocessor software must not only determine the magnitude of the voltage 35 produced in response to the transmittance detected at an adjacent diastole and systole, but must also determine that corresponding to a second pulse systole. In addition, timing information indicating pulse duration as well as the interval between an adjacent diastole and systole must be obtained and all the informa-. ,.~ , , ' ' :

~3~l~2~

tion combined to determine RoS~ As w;ll be appreciated, the determination of oxygen saturation in this manner also differs from prior art techniques, such asthat disclosed by Wilber, by using both the DC and AC components of the signals.The advantage of tw~pulse measurement oximetry can be roug1~y 5 described in the ~ollowing m anner. It has been found that m easurem ents produced with single-pulse measurement oximetry from dynamic data may have an error of greater than 4.5 percent until 10 to 15 pulses have been processed.
This error may even exceed 8 percent initially. It has been found that the preceding described two pulse measurement oximetric technique reduces the 10 maximum error to slightly above 3 percent initially and to less than 1/2 percent after two pulses are measured.
The implementation of this two-pulse measurement technique will be readily understood by one of ordinary skill in conjunction with the followingbrief discussion of the oximetric circuitry. The first component of oximeter 10 l 5 to be discussed is sensor 12.
The function of sensor 12 is substanti~lly to provide the desired orientation of light sources 40 and 42, for example, light-emitting diodes (LEOs), and light detector 38 with respect to a suitable portion of a patient's body. For example, the sensor must align LEDs 40 and 42 with detector 3~ in a manner 20 such that the path of light from each LRD to the detector 38 is substantially the same distance. In addition, the path must traverse a portion of the patient's body througl7 which a usable amount of light is passed, for example, a finger, toe, earlobe, or the nasal septum. Because changes in the lightpath can significantlyaffect the readings taken, as noted above, the sensor must mailltain the posit;on 25 of LEDs 40 and 42 and detector 38 with respect to the transmission path through the patient's skin at all times. Otherwise, signal fluctuations known as motion-arti~act may be produced. In addition, the sensor should apply only insubstantial presssure to the patient's skin. Otherwise, normal arterial blood Elow upon which the pulse oximeter relies for accurate operation, may be disrupted. Finally, the30 sensor should be quickly attachable to the patient and should cause no discom-fort.
LEDs 40 and 42 are supplied with current by transistor drivers 44 located in the I/O circuit 14, as shown in FIGURE 12. Drivers 44 are controUed by microcomputer 16 to produce current pulses at a 960 Ilz repetition rate. The 35 duration of each pulse is 70 microseconds and a pulse is supplied to the red wavelength L~D 40 first and then to the infrared wavelength LED 42. The voltage drop across scaling resistors in the drivers 44 allows the magnitude of the current pulses to be determined and, thus, maintained in a manner described %7 in greater detail below. LEDs 40 and 42 respond to the current pulses by producing corresponding light pulses transmitted through the finger to detector 38. Dectector 38, in turn, produces a signal that includes information about the pulsatile response of the finger to the red and infrared wavelength light, intermixed at the 960 Hz LED pulse repetition rate.
In a preferred embodiment of the invention, a red optical filter 45 interrupts the lightpath between the LEDs 40 atld 42 and the detector 38, as shown in FIGURE 9. Preferably, filter 45 is a l~odak No. ~9 wratten gel filter.
Its function is to eliminate the influence of fluorescent light ~licker on the oxygen saturation determination made. As will be appreciated, although the body of sensor 12 may be made of an opaque material that blocks a significant portion of the ambient light, some ambietlt light may still reach detector 38.
Light from the sun and incandescent lamps is substantially colltinuous. Fluor-escent lighting, on the other hand, includes alternatillg energized and deenergized intervals that ~orm a visu~l]y imperceptible ~licker. The frequellcyof the fluorescent light f]icker is such lhat it might influence th~ signal produced by detector 38 in response to light received îrom l,ED 40 at the red wavelellgth.
Thus, the red optical filter ~5 is placed over the detector 38 at~d filters out any ~luorescent light present, eliminatillg the effect its Elicker might have on theoxygen saturation determillatioll made.
~t the l/O circuit 14, the signal from detector 38 is received by a preamplifier 46. In n preferred embodiment, preampliîier 46 inc]udes a current-to-voltage transimpedance amplifier ~8 and a single-elld~d output ampli~ier S0.
To understand the advantages of using the differential current-to-voltnge amplifier 48, it mfly first be helpeul to consider the operation of a trans-impedance amplifier as shown in FIGURE l3. As shown, a transimpedance amplifier 52 is substantially comprised of an operational amplifier 54 and gain determination resistor RF. With a detector 38 connected to the inputs of the amplifier as shown, a current ID is input to the amplifier upon the detection ofsuitable wavelength light. The output of amplifier 52 is designated V0 and, as will be appreciated, is equal to the product of the detector current ID and the gain determination resistor RF. The primary problem with such a construction is that it also amplifies the externa] interference noise produced, making the signal extracted ]ess accurate.
Adoption of the differential current-to-voltage amplifier 48, when combined with the single ended output amplifier S0 as shown in EIGURE 14, however, eliminates this problem. As shown, the differential transimpedance amplifier 48 produces positive and negative versions of the output, the absolute ~3~

value o~ each version being equal to the product of the gnin determination resistance RF and the detector current ID. These outputs are then supplied to the single-ended output amp 50, which provides unity gain, thus producing an output signal h~ving a magnitude that is twice that of the inputs. An advantage 5 of this arrangement is that external interference noise is cancelled at the single-ended output amplifier 50 by the opposing signs of the two differenti.ql transimpedance amplifier outputs. In addition, twice the signal is produced withthe current noise only increasing by a magnitude of 1.414. Therefore, an improved signal-t~noise ratio results.
l O At this point, the mixed signal indicative of the red and infraredw~velength responses of detector 38 has been amplified and is input to a demodulator 56 to extract the red pulsatile and infrared pulsatile waveforms shown in FIGURES 10 and 1l. In a preferred arrangement, the demodulator 56 includes a sample-an~hold (S/H) circuit 58 that responds to the detector signal l 5 produced in response to red wavelength light and a sample-and-hold (S/H) circuit 60 that responds to the infrared wavelength response of detector 38. Thetiming of circuits 58 and 60is controlled so that each circuit samples the signal input to demodulator 56 during the portion of the signal corresponding to the wavelength to which it responds. In tllis manner, two signals are reconstructed from the single input to demodulator 56. As noted above, these signals correspond to the red pulsatile signal and infrared pulsatile signals shown in ~IGURES 10 and 11.
To remove higl~frequency noise from the outputs of circuits 58 and 60, they are input to lowpass filters 62 and 64. In a preferred embodiment, the "red" lowpass filter 62 and "infrared" lowpass filter 64 each include two stages.
The first stage of each filter utilizes a fifth-order, monolithic integrated circuit switched capacitor filter because of its low cost and relatively small physical size. Since both the "red" and "infrared" signals pass through identical first-stage filters, their gain and phase frequency responses are matched. The second stage of each filter is a secon~order Bessel Eilter having a slightly higher roll-off frequency than the first stage. Thi~s insures that the first-stage filter is the dominant filter of the two-stage combination, producing the desired filtering accuracy. The second stage then filters the switching noise from the ïirst-stageoutput.
The filtered red and infrared pulsatile signals are next prepared for conversion and transmission to the microcomputer 1~. ~s will be discussed in greater detail below, this process involves the ~se of a prograrn mable OC
subtractor or offset 66 followed by a programmable gain amplifier 68 having a ~3~

gain range from approximately one to 256. The appropriately processed signals are combined at multiplexer 70, sampled and held, and converted to digital form by A/D converter 7? for transmission to microcomputer 16.
Before a more complete discussion of the operation of prograrn-mable subtractor 66, programmaMe gain amplifier 68, multiplier 70 and A/D
converter 72 is provided, several details regarding the signals to be transferred to microcomputer 16 should be noted. For exarnple, as shown in FIGURES 10 and 11, the signal produced by detector 30 in response to light at each wavelength includes components that, for convenience, are termed baseline and pulsatile.
0 The baseline component approximates the intensity of light received at dete~
tor 38 when only the "fixed" nonpulsatile absorptive component is present in thefinger. This component of the signal is relatively constant over short intervalsbut does vary with nonpulsatile physio]ogical changes or system changes, such asmovement of probe 12 on the finger. Over a relatively long interval this baseline component may vary significantly. I~s will be appreciated, the magnitude of the baseline component at a given point in time is substantially equal to the level identified in FlaURE 10 as RH. For convellience, however, tlle ba3eline component may be thought of as the level indicated by RL, witll the pulsatile componellt varying between thç values for RH and ~L over a given pulse. That pulsatile comporlent is attributable to light transmissioll challges through thefinger resulting from blood volurne challges in the ~inger dul ing n pulse as ~Nell ns oxygen saturntion concelltratioll ~luctuations. Typically, the pulsatile componellt may be relatively small in comparison to the baselille component and is sl~own out of proportion in FIGURI~S 10 and 11.
Because the baseline signal does not direclly convey informatioll relating to oxygen snturation or pulse, the pulsatile signal is pri~arily of interest. ~s will be readily uppreciated, if the ent;re signal shown in FIGURES 10 and It, including the AC and ~C componellts, was amplified and converted to a digital format for use by microcomputer lG, a great deal o~ the accuracy of the conversion would be wasted because a substantial portion of the resolution would be used to break down the baseline component. For example, with an A/D converter employed having an input range of between +10 and -lû
volts, a signal having a baseline component that is four times that of the pulsatile component can be amplified until the baseline component is representedby a 16-volt difference and the pulsatile signal represented by a 4-volt difference. With a 12-bit A/D converter 72, the total signal can be resolved into ~096 components. Therefore, the number of incrernental levels representing the pulsatile signal would be approximately 820. If, on the other hand, the baseline ~3~27 com ponent is removed prior to the conversion, the pulsatile signal could be resolved into 4096 intervals, substantially improving accu~acy.
The disclosed invention employs this technique, as the first h~lf of fl construction-reconstruction process controlled by microcomputer lG. Accord-5 ingly, an input signal received from each filter ~2 and 6~ includes the entiretranslnission signal. The programmable subtractors 66 remove a substllnti-al ofEset portion of the total signal of each waveform and the prog~rammable gain amplifiers ~8 gain-up the remaining signal for conversion by ~/D converter 72.
A digital reconstruction of the original signal is then produeed by the micro-10 computer, which through the use of digital feedback in~ormation, removes thegain and adds the offset voltages back to the sign~l.
Feedback from microcomputer lG to I/O circuit t4 is 1~SO reCJUired to maintain the values for the o~set voltage, gain, and driver currents at levels appropriate to produce optimal A/D converter 72 resolution. Proper control 15 requires that the microcomputer continually analy7.e, and respond to, the orfset voltage, gain, driver currents and the output of ~/D converter in a manner to bedescribed ne~ct.
Briefly, with reference to FIGURE 15, thresholds Ll and L2 slightly below and above the maximum positive and negative excurs;ons L3 and 20 L4 allownble for the ~/D converter 72 input, nre established and monitored bymicrocomputer 16 at the A/D converter 72 output. Wllell the magnitude of the signal input to, and output from, ~/D converter 72 exceeds either of the thresholds L1 or L2, the driver currents ID, are readjusted to decrease the intensity of light impinging upon the det0ctor 38. In this manner, the A/D
25 converter 72 is not overdriven and the margin between Ll and L3 and between L2 and L4 helps assure this even for rapidly varying signals. An operable voltage margin for ~/D converter 72 e~ists outside of the thresholds, allowing A/D
converter 72 to continue operating while the appropriate feedback adjustments to A and Vos are made.
When the signal from A/D converter 72 exceeds positive and negative thresholds L5 or L6, microcomputer 16 responds by signaling the programmable subtractor 66 to increase the offset voltage being subtracted.
This is done through thc formation and transmission bf an offset code whose magnitude is dependent upon the level of the signal received from converter 72.
Three different gain Qdjustments are emp~oyed in the arrangement graphically dep;cted in FIGURE 15. For example, if microcomputer lG deter-rnines that the A/D converter 72 signal has not exceeded positive and negative thresholds L7 and L8, the current value of a gain code is increased. This revised gain code is then transrnitted to the programmable amplifier fi8, which rnakes the appropriate adjustrnent to the guin A. If the ~/D converter signal exceeds positive and negative thresholds L9 and LtO, the gain code is adjusted doY~nwardas a function of the signal magnitude. Similarly, if separate lower positive and5 negative thresholds L11 and L12 are exceeded, the gain code is also adjusted downward as a separate function of the signal magnitude.
The manller in which the various thresholds are established and the relationship of the gain and offset codes to the signal received can be altered to produce substantially any form of control desired. Thus, the arr~ngement shown l0 in ~IGURE 15 is illustrative only and represents the currently preferred embodi-m ent.
As will be appreciated from FIGURE 16, the instructions for the microcom puter program that controls the signal construction-reconstruction discussed above are stored in erasable, programmable, read-only memory 15 (EPROM) 74 of microcomputer 16. Similarly, values for V~l, VL, ~V, ats and A tp at wavelengths ~1 and ~ 2 are determined pursuant to peak-detection software contained in EPROM 74. These values are stored in random-access memory (R~M) 76 for operation UpOIl by a central processing unit (CPU) 78 in accordance with further computatiollal instructions stored in EPROM 74. Inter-20 faces 80 act as input and output buffers for microcomputer 1~.
l'he computational software in EPROM 74 initially causes CPU 78to determine the present value for RoS by substitutillg the measured values for VH, VL, QV, ~ts and ~ tp at wavelengths ~ and A 2 into equation (73):

~--VH
RoS = ~VL ~ ( ~ts ~V/ ~tp~ ~ @ ~1 (83) LVL - ( ~tS ~V/ A tp) ] @ A2 Then, the computational software instructs CPU 78 to determine the oxygen 30 saturation from Ros by use of a calibration curve, such as the one depicted in FIGURE 7. The calibration curve is a plot of the relationship between independently determined oxygen saturatiolls corresponding to values of Ros produced by oximeter 10 in accordance with the technique described above.
With sufficiently large space in EPE~OM 74, enough points along the 35 calibration curve can be stored in a look-up table to allow CPU 78 to extract an accurate indication of oxygen saturation from the value of Ros input to EPROM 74. The storage of a su~ficient number of calibration curve data points may, however, necessitate the use of an undesirably large capacity EPROM 74.

-` ~3~%'7 For that reason, a second method of storing the calibration curve information ispreferred.
Pursuant to that method, independently derived data associating RoS with the oxygen saturation is obtained, a mathematical expression between 5 the two can be derived from a plot of the curve. The basic formula and the coeîficients of the formula's variables are then stored in EPROM 7~. When a value for RoS is measured, CPU 78 extracts the coefficients from EPROM 74 and computes a value for the oxygen saturation. This technique allows inforrnation completely identifying the entire calibration curve, or a family of10 such curves, to be stored within a relatively small amount of EPROM 74 space.The computational software in EPROM 74 also instructs CPU 78 to determine the pulse rate from the signal period tp. Displays 20 then provide visible and audible outputs of the oxygen saturation and pulse rate in a manner conveniently used by the operator of oximeter 10.
While the references have been described with reference to a preferred embodiment, it is to be clearly understood by those skilled in the artthat the invention is not limited thereto, and that the scope of the invention is to be interpreted only in conjunction with the following claims.

Claims (27)

1. An apparatus for determining the oxygen saturation of arterial blood flowing in tissue that is illuminated with light at two wavelengths, the light being received upon emergence from the tissue by detection means that produces signals that are proportional to the intensity of the light received ateach of the wavelengths, said apparatus comprising:
sampling means for determining the magnitude of said signals at a plurality of sample times spaced over an interval greater than the period of onepulse as exhibited by said arterial blood flowing in said tissue; and processing means for producing a single indication of said oxygen saturation from said sample times and the magnitudes of said signals at said sample times.
2. The apparatus of Claim 1, wherein said processing means produces said single indication of said oxygen saturation in accordance with the relationship:

ROS = where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
T0 = the magnitude of the signal at the diastole of a first pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T1 = the magnitude of the signal at the systole of the first pulse, for the wavelength indicated;
T3 = the magnitude of the signal at the systole of a second pulse, for the wavelength indicated, and m = the ratio of the time between an adjacent diastole and systole to the time between adjacent diastoles.
3. The apparatus of Claim 1, wherein said processing means produces said single indication of said oxygen saturation in accordance with therelationship:

ROS = where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
VH = the magnitude of said signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
VL = the magnitude of said signal at the systole of said second pulse, for the wavelength indicated;
.DELTA.V = the difference in the magnitude of said signal between said systole of said second pulse and said systole of a first pulse, for the wavelength indicated;
.DELTA.ts = the difference in time between the systole and diastole of one of said first and second pulses, as measured from said signal corresponding to the wavelength indicated; and .DELTA.tp = the period of said pulse, as measured from said signal corresponding to the wavelength indicated.
4. The apparatus of Claim 1, wherein said processing means produces said single indication of said oxygen saturation in accordance with therelationship:

ROS = where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;

.lambda.2 = the second of said two wavelengths of said transilluminating light;
VH = the magnitude of said signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
VL = the magnitude of said signal at the systole of said second pulse, for the wavelength indicated;
.DELTA.V = the difference in the rnagnitude of said signal between said systole of said second pulse and said systole of a first pulse, for the wavelength indicated;
.DELTA.ts = the difference in time between the systole and diastole of one of said first and second pulses, as measured from said signal corresponding to the wavelength indicated; and .DELTA.tp = the period of said pulse, as measured from said signal corresponding to the wavelength indicated.
5. The apparatus of Claim 1, wherein said processing means produces said single indication of said oxygen saturation in accordance with therelationship:

ROS = where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
VH = the magnitude of said signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
VL = the magnitude of said signal at the systole of said second pulse, for the wavelength indicated;
.DELTA.V = the difference in the magnitude of said signal between said systole of said second pulse and said systole of a first pulse, for the wavelength indicated;

.DELTA.ts = the difference in time between the systole and diastole of one of said first and second pulses, as measured from said signal corresponding to the wavelength indicated; and .DELTA.tp = the period of said pulse, as measured from said signal corresponding to the wavelength indicated.
6. The apparatus of Claim 1, wherein said processing means produces said single indication of said oxygen saturation in accordance with therelationship:
ROS = where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
T0 = the magnitude of the signal at the diastole of a first pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T1 = the magnitude of the signal at the systole of the first pulse, for the wavelength indicated;
T3 = the magnitude of the signal at the systole of a second pulse, for the wavelength indicated; and m = the ratio of the time between an adjacent diastole and systole to the time between adjacent diastoles.
7. The apparatus of Claim 1, wherein said processing means produces said single indication of said oxygen saturation in accordance with therelationship:
ROS = where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;

.lambda.2 = the second of said two wavelengths of said transilluminating light;
T2 = the magnitude of the signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T3 = the magnitude of the signal at the systole of a second pulse, for the wavelength indicated; and Ti = the magnitude of the signal at a time ti, for the wavelength indicated;
Tj = the magnitude of the signal at a time tj, for the wavelength indicated;
mk = the ratio of the time between an adjacent diastole and systole to the time between adjacent diastoles; and i, j, and k = positive and negative integers.
8. The apparatus of Claim 1, wherein said processing means produces said single indication of said oxygen saturation in accordance with therelationship:
where: RoS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
T0 = the magnitude of the signal at the diastole of a first pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T1 = the magnitude of the signal at the systole of the first pulse, for the wavelength indicated;
P0(t) = a first interpolating function indicative of a time-varying characteristic of said tissue;
P1(t) = a second interpolating function indicative of a time-varying characteristic of said tissue and said arterial blood;
t0 = a first point in time used to identify corresponding points on said signals; and t1 = a second point in time used to identify corresponding points on said signals.
9. The apparatus of Claim 1, further comprising means for comparing the indication produced by said processing means with independently derived oxygen saturation curves to further indicate said oxygen saturation of said arterial blood in said tissue.
10. The apparatus of Claim 9, further comprising means for producing an output representative of said oxygen saturation indicated.
11. The oximeter of Claim 1, further comprising a differential current-to-voltage amplifier for amplifying said signals produced by said detec-tion means before the magnitude of said signals is determined by said sampling means.
12. An oximeter, comprising:
a light source for exposing tissue having arterial blood flowing therein to light at two wavelengths;
detection means, responsive to the exposure of said tissue to said light, for producing signals that are proportional to the intensity of said light received at each of said wavelengths, said signals containing information about the oxygen saturation of said arterial blood;
sampling means for determining the magnitude of said signals at a plurality of sample times spaced over an interval greater than the period of onepulse as exhibited by said arterial blood flowing in said tissue; and processing means for producing a single indication of said oxygen saturation from said sample times and the magnitudes of said signals at said sample times.
13. The oximeter of Claim 12, wherein said processing means produces said single indication in accordance with the relationship:

where Ros = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;

To = the magnitude of the signal at the diastole of a first pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T1 = the magnitude of the signal at the systole of the first pulse, for the wavelength indicated;
T3 = the magnitude of the signal at the systole of a second pulse, for the wavelength indicated; and m = the ratio of the time between an adjacent diastole and systole to the time between adjacent diastoles.
14. The oximeter of Claim 12, wherein said processing means products said single indication of said oxygen saturation in accordance with the relationship:

where RoS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
VH = the magnitude of said signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
VL = the magnitude of said signal at the systole of said second pulse, for the wavelength indicated;
.DELTA.V = the difference in the magnitude of said signal between said systole of said second pulse and said systole of a first pulse, for the wavelength indicated;
.DELTA.ts = the difference in time between the systole and diastole of one of said first and second pulses, as measured from said signal corresponding to the wavelength indicated; and .DELTA.tp = the period of said pulse, as measured from said signal corresponding to the wavelength indicated.
15. The oximeter of Claim 12, wherein said two wavelengths comprise red and infrared wavelengths.
16. The oximeter of Claim 15, further comprising a red optical filter for filtering said light received by said detection means.
17. The oximeter of Claim 12, further comprising a differential current-to-voltage amplifier for amplifying said signals produced by said detection means before the magnitude of said signals is determined by said sampling means.
18. A method of determining the oxygen saturation of arterial blood flowing in tissue that is illuminated with light at two wavelengths, the light being received upon emergence from the tissue by detection means that produces signals that are proportional to the intensity of the light received ateach of the wavelengths, said method comprising the steps of:
storing the magnitude of said signals at a plurality of sample times spaced over an interval greater than the period of one pulse as exhibited by said arterial blood flowing in said tissue; and producing a single indication of said oxygen saturation of said arterial blood from said sample times and the magnitudes of said signals at saidsample times.
19. The method of Claim 18, wherein said single indication of said oxygen saturation is produced in accordance with the relationship:

where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
T0 = the magnitude of the signal at the diastole of a first pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;

T1 = the magnitude of the signal at the systole of the first pulse, for the wavelength indicated;
T3 = the magnitude of the signal at the systole of a second pulse, for the wavelength indicated; and m = the ratio of the time between an adjacent diastole and systole to the time between adjacent diastoles.
20. The method of Claim 18, wherein said single indication of said oxygen saturation is produced in accordance with the relationship:

where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
VH = the magnitude of said signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
VL = the magnitude of said signal at the systole of said second pulse, for the wavelength indicated;
.DELTA.V = the difference in the magnitude of said signal between said systole of said second pulse and said systole of a first pulse, for the wavelength indicated;
.DELTA.ts = the difference in time between the systole and diastole of one of said first and second pulses, as measured from said signal corresponding to the wavelength indicated; and .DELTA.tp = the period of said pulse, as measured from said signal corresponding to the wavelength indicated.
21. The method of Claim 18, wherein said single indication of said oxygen saturation is produced in accordance with the relationship:

where: RoS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
VH = the magnitude of said signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
VL = the magnitude of said signal at the systole of said second pulse, for the wavelength indicated;
.DELTA.V = the difference in the magnitude of said signal between the systole of said second pulse and the systole of a first pulse, for the wavelength indicated;
.DELTA.ts = the difference in time between the systole and diastole of one of said first and second pulses, as measured from said signal corresponding to the wavelength indicated; and .DELTA.tp = the period of said pulse, as measured from said signal corresponding to the wavelength indicated.
22. The method of Claim 18, wherein said single indication of said oxygen saturation is produced in accordance with the relationship:

where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
VH = the magnitude of said signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;

VL = the magnitude of said signal at the systole of said second pulse, for the wavelength indicated;
.DELTA.V = the difference in the magnitude of said signal between said systole of said second pulse and said systole of a first pulse, for the wavelength indicated;
.DELTA.ts = the difference in time between the systole and diastole of one of said first and second pulses, as measured from said signal corresponding to the wavelength indicated; and .DELTA.tp = the period of said pulse, as measured from said signal corresponding to the wavelength indicated.
23. The method of Claim 18, wherein said single indication of said oxygen saturation is produced in accordance with the relationship:

where Ros = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
T0 = the magnitude of the signal at the diastole of a first pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T1 = the magnitude of the signal at the systole of the first pulse, for the wavelength indicated;
T3 = the magnitude of the signal at the systole of a second pulse pulse, for the wavelength indicated; and m = the ratio of the time between an adjacent diastole and systole to the time between adjacent diastoles.
24. The method of Claim 18, wherein said single indication of said oxygen saturation is produced in accordance with the relationship:

where ROS = said single indication of said oxygen saturation produced;
.lambda.1 = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;
T2 = the magnitude of the signal at the diastole of a second pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T3 = the magnitude of the signal at the systole of a second pulse, for the wavelength indicated; and Ti = the magnitude of the signal at a time t1, for the wavelength indicated;
Tj = the magnitude of the signal at a time tj, for the wavelength indicated;
mk = the ratio of the time between an adjacent diastole and systole to the time between adjacent diastoles; and i, j, and k = positive and negative integers.
25. The method of Claim 18, wherein said single indication of said oxygen saturation is produced in accordance with the relationship:

where: ROS = said single indication of said oxygen saturation produced;
.lambda.l = the first of said two wavelengths of said transilluminating light;
.lambda.2 = the second of said two wavelengths of said transilluminating light;

T0 = the magnitude of the signal at the diastole of a first pulse exhibited by said arterial blood flowing in said tissue, for the wavelength indicated;
T1 = the magnitude of the signal at the systole of the first pulse, for the wavelength indicated;
P0(t) = a first interpolating function indicative of a time-varying characteristic of said tissue;
P1(t) = a second interpolating function indicative of a time-varying characteristic of said tissue and said arterial blood;
t0 = a first point in time used to identify corresponding points on said signals; and t1 = a second point in time used to identify corresponding points on said signals.
26. The method of Claim 18, further comprising the step of comparing the indication produced by the processing of said sample times and said magnitudes with independently derived oxygen saturation curves to further indicate said oxygen saturation of said arterial blood in said tissue.
27. The method of Claim 26, further comprising the step of producing an output representative of said oxygen saturation determined.
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Families Citing this family (96)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4911167A (en) * 1985-06-07 1990-03-27 Nellcor Incorporated Method and apparatus for detecting optical pulses
US4819646A (en) * 1986-08-18 1989-04-11 Physio-Control Corporation Feedback-controlled method and apparatus for processing signals used in oximetry
US5078136A (en) * 1988-03-30 1992-01-07 Nellcor Incorporated Method and apparatus for calculating arterial oxygen saturation based plethysmographs including transients
US5299120A (en) * 1989-09-15 1994-03-29 Hewlett-Packard Company Method for digitally processing signals containing information regarding arterial blood flow
AU658177B2 (en) 1991-03-07 1995-04-06 Masimo Corporation Signal processing apparatus and method
US5490505A (en) 1991-03-07 1996-02-13 Masimo Corporation Signal processing apparatus
MX9702434A (en) 1991-03-07 1998-05-31 Masimo Corp Signal processing apparatus.
US5632272A (en) 1991-03-07 1997-05-27 Masimo Corporation Signal processing apparatus
US5987346A (en) 1993-02-26 1999-11-16 Benaron; David A. Device and method for classification of tissue
JP3364819B2 (en) * 1994-04-28 2003-01-08 日本光電工業株式会社 Blood absorption substance concentration measurement device
US8019400B2 (en) 1994-10-07 2011-09-13 Masimo Corporation Signal processing apparatus
EP1905352B1 (en) 1994-10-07 2014-07-16 Masimo Corporation Signal processing method
US6018673A (en) * 1996-10-10 2000-01-25 Nellcor Puritan Bennett Incorporated Motion compatible sensor for non-invasive optical blood analysis
US5935076A (en) * 1997-02-10 1999-08-10 University Of Alabama In Huntsville Method and apparatus for accurately measuring the transmittance of blood within a retinal vessel
US5776060A (en) * 1997-02-20 1998-07-07 University Of Alabama In Huntsville Method and apparatus for measuring blood oxygen saturation within a retinal vessel with light having several selected wavelengths
US6002952A (en) 1997-04-14 1999-12-14 Masimo Corporation Signal processing apparatus and method
US6675031B1 (en) 1999-04-14 2004-01-06 Mallinckrodt Inc. Method and circuit for indicating quality and accuracy of physiological measurements
US8224412B2 (en) 2000-04-17 2012-07-17 Nellcor Puritan Bennett Llc Pulse oximeter sensor with piece-wise function
US6801797B2 (en) 2000-04-17 2004-10-05 Nellcor Puritan Bennett Incorporated Pulse oximeter sensor with piece-wise function
US6748254B2 (en) 2001-10-12 2004-06-08 Nellcor Puritan Bennett Incorporated Stacked adhesive optical sensor
US6947131B2 (en) * 2002-05-07 2005-09-20 Chf Solutions, Inc. Blood leak detector for extracorporeal treatment system
US7190986B1 (en) 2002-10-18 2007-03-13 Nellcor Puritan Bennett Inc. Non-adhesive oximeter sensor for sensitive skin
DE10333075B4 (en) * 2003-07-21 2011-06-16 Siemens Ag Method and device for training adjustment in sports, especially in running
US7162288B2 (en) 2004-02-25 2007-01-09 Nellcor Purtain Bennett Incorporated Techniques for detecting heart pulses and reducing power consumption in sensors
US7976472B2 (en) * 2004-09-07 2011-07-12 Masimo Corporation Noninvasive hypovolemia monitor
US7657295B2 (en) 2005-08-08 2010-02-02 Nellcor Puritan Bennett Llc Medical sensor and technique for using the same
US7657294B2 (en) 2005-08-08 2010-02-02 Nellcor Puritan Bennett Llc Compliant diaphragm medical sensor and technique for using the same
US7590439B2 (en) 2005-08-08 2009-09-15 Nellcor Puritan Bennett Llc Bi-stable medical sensor and technique for using the same
US20070060808A1 (en) 2005-09-12 2007-03-15 Carine Hoarau Medical sensor for reducing motion artifacts and technique for using the same
US7899510B2 (en) 2005-09-29 2011-03-01 Nellcor Puritan Bennett Llc Medical sensor and technique for using the same
US8092379B2 (en) 2005-09-29 2012-01-10 Nellcor Puritan Bennett Llc Method and system for determining when to reposition a physiological sensor
US7869850B2 (en) 2005-09-29 2011-01-11 Nellcor Puritan Bennett Llc Medical sensor for reducing motion artifacts and technique for using the same
US7904130B2 (en) 2005-09-29 2011-03-08 Nellcor Puritan Bennett Llc Medical sensor and technique for using the same
US7486979B2 (en) 2005-09-30 2009-02-03 Nellcor Puritan Bennett Llc Optically aligned pulse oximetry sensor and technique for using the same
US8062221B2 (en) 2005-09-30 2011-11-22 Nellcor Puritan Bennett Llc Sensor for tissue gas detection and technique for using the same
US7555327B2 (en) 2005-09-30 2009-06-30 Nellcor Puritan Bennett Llc Folding medical sensor and technique for using the same
US8233954B2 (en) 2005-09-30 2012-07-31 Nellcor Puritan Bennett Llc Mucosal sensor for the assessment of tissue and blood constituents and technique for using the same
US7881762B2 (en) 2005-09-30 2011-02-01 Nellcor Puritan Bennett Llc Clip-style medical sensor and technique for using the same
US7483731B2 (en) 2005-09-30 2009-01-27 Nellcor Puritan Bennett Llc Medical sensor and technique for using the same
US7477924B2 (en) 2006-05-02 2009-01-13 Nellcor Puritan Bennett Llc Medical sensor and technique for using the same
US7522948B2 (en) 2006-05-02 2009-04-21 Nellcor Puritan Bennett Llc Medical sensor and technique for using the same
US8073518B2 (en) 2006-05-02 2011-12-06 Nellcor Puritan Bennett Llc Clip-style medical sensor and technique for using the same
US8145288B2 (en) 2006-08-22 2012-03-27 Nellcor Puritan Bennett Llc Medical sensor for reducing signal artifacts and technique for using the same
US8219170B2 (en) 2006-09-20 2012-07-10 Nellcor Puritan Bennett Llc System and method for practicing spectrophotometry using light emitting nanostructure devices
US8190225B2 (en) 2006-09-22 2012-05-29 Nellcor Puritan Bennett Llc Medical sensor for reducing signal artifacts and technique for using the same
US8175671B2 (en) 2006-09-22 2012-05-08 Nellcor Puritan Bennett Llc Medical sensor for reducing signal artifacts and technique for using the same
US8396527B2 (en) 2006-09-22 2013-03-12 Covidien Lp Medical sensor for reducing signal artifacts and technique for using the same
US7869849B2 (en) 2006-09-26 2011-01-11 Nellcor Puritan Bennett Llc Opaque, electrically nonconductive region on a medical sensor
US7574245B2 (en) 2006-09-27 2009-08-11 Nellcor Puritan Bennett Llc Flexible medical sensor enclosure
US7890153B2 (en) 2006-09-28 2011-02-15 Nellcor Puritan Bennett Llc System and method for mitigating interference in pulse oximetry
US7796403B2 (en) 2006-09-28 2010-09-14 Nellcor Puritan Bennett Llc Means for mechanical registration and mechanical-electrical coupling of a faraday shield to a photodetector and an electrical circuit
US8068891B2 (en) 2006-09-29 2011-11-29 Nellcor Puritan Bennett Llc Symmetric LED array for pulse oximetry
US8175667B2 (en) 2006-09-29 2012-05-08 Nellcor Puritan Bennett Llc Symmetric LED array for pulse oximetry
US7476131B2 (en) 2006-09-29 2009-01-13 Nellcor Puritan Bennett Llc Device for reducing crosstalk
US7680522B2 (en) 2006-09-29 2010-03-16 Nellcor Puritan Bennett Llc Method and apparatus for detecting misapplied sensors
US7684842B2 (en) 2006-09-29 2010-03-23 Nellcor Puritan Bennett Llc System and method for preventing sensor misuse
US8414499B2 (en) 2006-12-09 2013-04-09 Masimo Corporation Plethysmograph variability processor
US8265724B2 (en) 2007-03-09 2012-09-11 Nellcor Puritan Bennett Llc Cancellation of light shunting
US7894869B2 (en) 2007-03-09 2011-02-22 Nellcor Puritan Bennett Llc Multiple configuration medical sensor and technique for using the same
US8280469B2 (en) 2007-03-09 2012-10-02 Nellcor Puritan Bennett Llc Method for detection of aberrant tissue spectra
US8352004B2 (en) 2007-12-21 2013-01-08 Covidien Lp Medical sensor and technique for using the same
US8346328B2 (en) 2007-12-21 2013-01-01 Covidien Lp Medical sensor and technique for using the same
US8366613B2 (en) 2007-12-26 2013-02-05 Covidien Lp LED drive circuit for pulse oximetry and method for using same
US8577434B2 (en) 2007-12-27 2013-11-05 Covidien Lp Coaxial LED light sources
US8442608B2 (en) 2007-12-28 2013-05-14 Covidien Lp System and method for estimating physiological parameters by deconvolving artifacts
US8452364B2 (en) 2007-12-28 2013-05-28 Covidien LLP System and method for attaching a sensor to a patient's skin
US8070508B2 (en) 2007-12-31 2011-12-06 Nellcor Puritan Bennett Llc Method and apparatus for aligning and securing a cable strain relief
US8092993B2 (en) 2007-12-31 2012-01-10 Nellcor Puritan Bennett Llc Hydrogel thin film for use as a biosensor
US8897850B2 (en) 2007-12-31 2014-11-25 Covidien Lp Sensor with integrated living hinge and spring
US8199007B2 (en) 2007-12-31 2012-06-12 Nellcor Puritan Bennett Llc Flex circuit snap track for a biometric sensor
US8437822B2 (en) 2008-03-28 2013-05-07 Covidien Lp System and method for estimating blood analyte concentration
US8112375B2 (en) 2008-03-31 2012-02-07 Nellcor Puritan Bennett Llc Wavelength selection and outlier detection in reduced rank linear models
US7887345B2 (en) * 2008-06-30 2011-02-15 Nellcor Puritan Bennett Llc Single use connector for pulse oximetry sensors
US7880884B2 (en) 2008-06-30 2011-02-01 Nellcor Puritan Bennett Llc System and method for coating and shielding electronic sensor components
USD626561S1 (en) 2008-06-30 2010-11-02 Nellcor Puritan Bennett Llc Circular satseconds indicator and triangular saturation pattern detection indicator for a patient monitor display panel
US8071935B2 (en) 2008-06-30 2011-12-06 Nellcor Puritan Bennett Llc Optical detector with an overmolded faraday shield
USD626562S1 (en) 2008-06-30 2010-11-02 Nellcor Puritan Bennett Llc Triangular saturation pattern detection indicator for a patient monitor display panel
US8364220B2 (en) 2008-09-25 2013-01-29 Covidien Lp Medical sensor and technique for using the same
US8914088B2 (en) 2008-09-30 2014-12-16 Covidien Lp Medical sensor and technique for using the same
US8417309B2 (en) 2008-09-30 2013-04-09 Covidien Lp Medical sensor
US8423112B2 (en) 2008-09-30 2013-04-16 Covidien Lp Medical sensor and technique for using the same
US8452366B2 (en) 2009-03-16 2013-05-28 Covidien Lp Medical monitoring device with flexible circuitry
US8221319B2 (en) 2009-03-25 2012-07-17 Nellcor Puritan Bennett Llc Medical device for assessing intravascular blood volume and technique for using the same
US8509869B2 (en) 2009-05-15 2013-08-13 Covidien Lp Method and apparatus for detecting and analyzing variations in a physiologic parameter
US8634891B2 (en) 2009-05-20 2014-01-21 Covidien Lp Method and system for self regulation of sensor component contact pressure
US20100331640A1 (en) * 2009-06-26 2010-12-30 Nellcor Puritan Bennett Llc Use of photodetector array to improve efficiency and accuracy of an optical medical sensor
US8311601B2 (en) 2009-06-30 2012-11-13 Nellcor Puritan Bennett Llc Reflectance and/or transmissive pulse oximeter
US9010634B2 (en) 2009-06-30 2015-04-21 Covidien Lp System and method for linking patient data to a patient and providing sensor quality assurance
US8505821B2 (en) 2009-06-30 2013-08-13 Covidien Lp System and method for providing sensor quality assurance
US8391941B2 (en) 2009-07-17 2013-03-05 Covidien Lp System and method for memory switching for multiple configuration medical sensor
US8417310B2 (en) 2009-08-10 2013-04-09 Covidien Lp Digital switching in multi-site sensor
US8428675B2 (en) 2009-08-19 2013-04-23 Covidien Lp Nanofiber adhesives used in medical devices
TWI452996B (en) * 2010-10-27 2014-09-21 私立中原大學 No balloon blood pressure measurement device
US9949675B2 (en) * 2012-10-19 2018-04-24 Convergence Biometrics, LLC Noninvasive blood measurement platform
CN103479363B (en) * 2013-09-30 2015-03-18 深圳市倍轻松科技股份有限公司 Method and system for measuring oxyhemoglobin saturation in blood
CN110833422A (en) * 2018-08-16 2020-02-25 康泰医学系统(秦皇岛)股份有限公司 Blood oxygen instrument

Family Cites Families (15)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2706927A (en) * 1949-08-04 1955-04-26 Research Corp Apparatus for determining percentage oxygen-saturation of blood
US3704706A (en) * 1969-10-23 1972-12-05 Univ Drexel Heart rate and respiratory monitor
CA971768A (en) * 1972-02-01 1975-07-29 Robert F. Shaw Oximeter and method
JPS5725217B2 (en) * 1974-10-14 1982-05-28
CA1037285A (en) * 1975-04-30 1978-08-29 Glenfield Warner Ear oximetry process and apparatus
US4114604A (en) * 1976-10-18 1978-09-19 Shaw Robert F Catheter oximeter apparatus and method
US4167331A (en) * 1976-12-20 1979-09-11 Hewlett-Packard Company Multi-wavelength incremental absorbence oximeter
JPS5524004A (en) * 1978-06-22 1980-02-20 Minolta Camera Kk Oxymeter
JPS56104646A (en) * 1980-01-25 1981-08-20 Minolta Camera Kk Optical analyzer for forming ratio of element contained in organism
US4357105A (en) * 1980-08-06 1982-11-02 Buffalo Medical Specialties Mfg., Inc. Blood diagnostic spectrophotometer
US4523279A (en) * 1980-11-24 1985-06-11 Oximetrix, Inc. Apparatus for determining oxygen saturation levels in blood
US4407290A (en) * 1981-04-01 1983-10-04 Biox Technology, Inc. Blood constituent measuring device and method
EP0102816A3 (en) * 1982-09-02 1985-08-28 Nellcor Incorporated Pulse oximeter
US4621643A (en) * 1982-09-02 1986-11-11 Nellcor Incorporated Calibrated optical oximeter probe
ATE51134T1 (en) * 1982-09-02 1990-04-15 Nellcor Inc CALIBRATED OPTICAL OXYMETRY PROBE.

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DE3785717T2 (en) 1993-12-23
AU608529B2 (en) 1991-04-11
WO1988001148A1 (en) 1988-02-25
EP0261788A1 (en) 1988-03-30
DE3785717D1 (en) 1993-06-09
ATE88877T1 (en) 1993-05-15
US4859056A (en) 1989-08-22
JPH01500493A (en) 1989-02-23
EP0261788B1 (en) 1993-05-05
AU7718387A (en) 1988-02-25

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