• 专利附录
  • 专利说明
  • 权利要求
  • 类似技术
  • 同族专利
  • 引用文献
  • 法律状态
  • 优先权
    • 专利摘要:
    A technicue for determining blood flow in a living body by changing the thermal energy level by a predetermined amount at a site in a blood flow path and detecting temperatures at locations upstream and downstream of the site. The temperature difference at such locations is determined and the blood flow is calculated as a function of the change in energy level and of the temperature differences measured prior to and following the change in energy level.
    公开号:US20010000792A1
    申请号:US09/733,595
    申请日:2000-12-08
    公开日:2001-05-03
    发明作者:Harry Bowman
    申请人:Bowman Harry Frederick;
    IPC主号:A61B5-028
    专利说明:
    [0001] This invention relates generally to techniques for measuring blood flow in a body and, more particularly, to the use preferably of one or more temperature sensors for measuring thermal energy changes in the blood flowing through the heart and to the use of unique data processing techniques in response thereto for determining cardiac output. [0001] BACKGROUND OF THE INVENTION
    [0002] While the invention can be used generally to measure blood flow at various locations in a body, it is particularly useful in measuring blood flow in the heart so as to permit the measurement of cardiac output. Many techniques for measuring cardiac output have been suggested in the art. Exemplary thermodilution techniques described in the technical and patent literature include: “A Continuous Cardiac Output Computer Based On Thermodilution Principles”, Normann et al., Annals of Biomedical Engineering, Vol. 17, 1989; “Thermodilution Cardiac Output Determination With A single Flow-Directed Catheter”, Forrester, et al., American Heart Journal, Vol. 83, No. 3, 1972; “Understanding Techniques for Measuring Cardiac Output”, Taylor, et al., Biomedical Instrumentation & Technology, May/June 1990; U.S. Pat. No. 4,507,974 of M. L. Yelderman, issued Apr. 2, 1985; U.S. Pat. No. 4,735,823, Eggers et al., issued on Nov. 22, 1988; and U.S. Pat. No. 5,000,190, of John H. Petre, issued on Mar. 19, 1991. [0002]
    [0003] A principal limitation in the quanification of cardiac output is the existence of thermal fluctuations inherent in the bloodstream. Previous methods work with those fluctuations while observing the effects of an input signal to calculate cardiac output. The invention described herein uses a differential measurement technicue to substantially eliminate the effect of the thermal fluctuations, permitting the use of a minimal thermal input signal, which allows frequent or continuous measurements. [0003]
    [0004] It is desirable to obtain accurate cardiac output measurements in an effectively continuous manner, i.e., several times a minute, so that a diagnosis can be achieved more rapidly and so that rapid changes in a patient's condition can be monitored on a more continuous basis than is possible using current techniques. Moreover, it is desirable to obtain instantaneous measurements of the cardiac output on a beat-to-beat basis to evaluate the relative changes which occur from beat to beat, as well as to determine the presence of regurgitation. [0004] BRIEF SUMMARY OF THE INVENTION
    [0005] In accordance with general principal of the invention, blood flow and/or cardiac output is determined rapidly, using a technique by which an indicator substance, or agent, is introduced into the bloodstream between a pair of detectors. The detectors are sensitive to a parameter functionally related to the concentration or magnitude in the bloodstream of the selected indicator agent. The detectors are positioned apart by a distance functionally sufficient to allow a measurement to be made of the differential value of the selected parameter as it exists from time-to-time between the two detectors. The indicator agent, for example, may be a substance to change the pH of the blood, a fluid bolus carrying thermal energy, or a substance to change a selected characteristic of the blood, or the direct introduction of thermal energy, or the like. [0005]
    [0006] A determination is made of the difference in the values of the selected blood parameter as it exists at the two detectors, prior to the introduction of indicator agent (i.e., the first differentIal value). The selected indicator agent is then introduced in a predetermined magnitude. Then again a determination is made of the difference in values of the selected parameter as it exists at the locations of the two detectors (i.e., the second differential value). [0006]
    [0007] Blood flow or cardiac output, depending on the specific location of the detectors, can then be determined as a function of the difference between the first differential value and the second differential value. Because the ultimate measurement of blood flow or cardiac output is based on the difference of the differences, the system operates effectively with the introduction of the indicator agent in a very low magnitude. In turn, this allows measurements to be made rapidly so that effectively continuous measurements are obtained. [0007]
    [0008] In accordance with a preferred embodiment of the invention, for example, cardiac output can be determined rapidly and with low levels of thermal energy input. To achieve such operation, in a preferred embodiment, the technique of the invention uses a pair of temperature sensors positioned at two selected locations within a catheter which has been inserted into the path of the blood flowing through the heart of a living body. The sensors detect the temperature difference between the two locations. Depending on the location of the temperature sensors in the circulatory system, the measured temperature difference varies over time. It has been observed that when the temperature sensors are placed within the heart, e.g., so that one sensor lies in the vena cava, for example, and the second in the right ventricle or pulmonary artery, the temperature difference varies in a synchronous manner with the respiratory cycle. [0008]
    [0009] Thus, in the preferred embodiment of the invention the temperature difference over at least one respiratory cycle is measured and averaged to provide an average temperature difference. The averaging, or integrating, action effectively eliminates, as a confounding factor in the determination of cardiac output, the effect of instantaneous blood temperature fluctuations, such as cyclical, respiratory-induced fluctuations. [0009]
    [0010] To make such determinations, an average temperature difference is first calculated over a time period of at least one respiratory cycle in which no thermal energy is introduced into the blood flow path. Thermal energy of a predetermined and relatively low magnitude is then introduced into the blood flow path to produce a heating action therein at a location between the two temperature sensors. Once the temperature rise induced by the heating stabilizes, the average temperature difference between the two locations isagain calculated from temperature difference measurements over a time period of at least one respiratory cycle at the higher temperature level. The difference between the average temperature differences which occurs when the thermal energy is turned on, referred to as the rising temperature change, is determined. The difference between the average temperature differences which occurs when the thermal energy is turned off, referred to as the falling temperature change, is similarly determined. The cardiac output is calculated as a function of the thermal energy input and the rising and falling temperature changes. Because a relatively low level of thermal energy is used in making measurements, the overall sequence of determinations can be safely repeated multiple times per minute, for example, so that an effectively continuous, or quasi-continuous, determination of cardiac output is obtained. [0010]
    [0011] In accordance with a further embodiment of the invention, a temperature sensor that also acts as a source of thermal energy, e.g., a thermistor, is positioned at a third location in the cardiac blood flow path. Power is supplied to the sensor sufficient to elevate the temperature of the sensor from a first temperature level to a second temperature level. In one embodiment of the invention, the temperature of the sensor is changed from the first to the second level and is maintained constant at said second level by varying the power that is supplied thereto. Such varying power is proportional to the instantaneous flow velocity and, hence, assuming a constant flow area, is proportional to the instantaneous cardiac output. Measurement of the sensor heating power and the temperature increment at the sensor can thus be used to continuously effect a determination of the instantaneous cardiac output. Further, for example, when the sensor is placed downstream at the outlet of one of the heart chambers, the variation in flow output over the cardiac cycle can be analyzed to provide an indication of the regurgitation characteristics of the heart outlet valve over the cardiac cycle. Moreover, such instantaneous cardiac output determination can be further refined to compensate for fluctuations in the temperature of the blood flowing through the heart by measuring the instantanecus temperature of the blood with another temperature sensor at a nearby location and appropriately taking into account such temperature variations when determining the cardiac output. [0011]
    [0012] In another application, both the continuous cardiac output determinations and the instantaneous cardiac output determinations, as described above, can be combined. Thus, three temperature sensors and a source of thermal energy can all be used in combination to simultanecusly provide an accurate and effectively continuous determination of time-averaged cardiac output, and a determination of instantaneous cardiac output at each instant of the cardiac cycle. In still another application, two temperature sensors and a source of thermal energy can be used in an apcropriate sequence to provide the averaged cardiac output determination and the instantaneous cardiac output determination. [0012] DESCRIPTION OF THE INVENTION
    [0013] The invention can be described in more detail with the help of the accompanying drawings wherein [0013]
    [0014] FIG. 1 shows a simplified diagrammatic view of a human heart; [0014]
    [0015] FIG. 2 shows a simplified diagrammatic view of a catheter useful in the invention; [0015]
    [0016] FIG. 3 shows a flow chart depicting steps in a process used in the invention; [0016]
    [0017] FIG. 3A shows a smooth temperature dirference curve obtained in the process depicted in FIG. 3; [0017]
    [0018] FIG. 4 shows a flow chart depicting steps in another process used in the invention; [0018]
    [0019] FIG. 5 shows a flow chart depicting steps in still another process of the invention; [0019]
    [0020] FIG. 6 shows a graph depicting a temperature/time relation used in the invention; [0020]
    [0021] FIG. 7A shows a simplified diagrammatic view or another catheter used in the invention; [0021]
    [0022] FIG. 7B shows a flow chart depicting steps in still another process of the invention; [0022]
    [0023] FIGS. 8A, 8B, and [0023] 8C show flow charts depicting still other processes of the invention;
    [0024] FIGS. 9A, 9B, and [0024] 9C show graphs of parameter relationships used in the invention; and
    [0025] FIG. 10 shows a graph useful for calibrating the flow values for a catheter used in the invention. [0025]
    [0026] As can be seen in FIG. 1, which represents a human heart [0026] 10 in a much simplified diagrammatic form, a flexible catheter 11 is inserted through the veins into the right atrium, or auricle, 12 of the heart and, thence, through the right ventricle 13 until the end of the catheter resides in or near the exit, or pulmonary, artery 14 which leads to the lungs. As is well known, blood flows (as represented by the arrows) from the input vein 15, i.e., the vena cava, into the right atrium and right ventricle and thence outwardly to the lungs and subsecuently returns from the lunge into the left atrium 15, through the left ventricle 17 and thence outwardly into the aorta 13.
    [0027] In accordance with the embodiment of the invention, shown with reference to FIG. 1, temperature sensors, e.g., thermistors, are carried by the catheter so that, when inserted as shown in FIG. 1, a first sensor [0027] 19 is positioned at a location within the vena cava 15 or right atrium 12 and a second sensor 20 is positioned at a location in or near the pulmonary artery 14.
    [0028] For simplicity, the flexible catheter [0028] 11 is determined in FIG. 2 in an extended condition with temperature sensors 19 and 20 at two different locations for measuring temperatures T1 and T2, respectively. A power source 21 of thermal energy which is borne, or carried, by the catheter 11 is positioned in the right atrium at a location between sensors 19 and 20. In a particular embodiment, the catheter-borne source is, for example, a coil of resistive wire placed on or embedded in the surface of catheter 11, to which an AC or a DC voltage (not shown) at a controllable level is supplied so as to generate thermal energy, i.e. heat. The magnitude of the thermal energy can be suitably controlled to insert a predetermined amount of thermal energy at a selected time, which thermal energy is transferred to the blood flowing through the heart so as to raise its temperature. The energy source is positioned at a sufficient distance from the sensor 19 that the latter is effectively thermally isolated from the site of the thermal energy source.
    [0029] While the locations of the sensors [0029] 19 and 20 and the energy source 21 can be as shown in FIG. 1, alternative locations can also be used. Thus, the sensor 19 can be positioned in the vena cava 15, while the energy source 21 is located in the right atrium 12 and the sensor 20 in either the right atrium or the right ventricle. Moreover, if sensor 19 is positioned in the vena cava 15, the entire energy source 21, which is normally elongated, need not be located in the right atrium and can have a portion thereof in the vena cava and a portion thereof in the right atrium. Such source should preferably be at least partially located in the right atrium. Further, sensor 20 may be positioned in the right ventricle near the pulmonary artery 14 or may be located in the pulmonary artery itself at or near the right ventricle.
    [0030] The temperatures T[0030] 1 and T2 at locations 19 and 20 upstream and downstream, respectively, from the thermal energy source 21 are monitored and processed appropriately by a digital microprocessor. In accordance with the invention, the instantaneous temperatures are obtained as the outputs T1(t) and T2(t) of the temperature sensors 19 and 20, respectively. The outputs are connected to a differential amplifier to generate an analog signal which is proportional o the temperature difference Δ(t)=T1(t)−T2(t) between them. The temperature difference signal ΔT(t) is digitized and sampled at selected time intervals by an analog-to-digital/sampling circuit. The digitized sampled temperature difference values and the known thermal energy values are supplied to a digital microprocessor which then suitably processes the data to provide the desired cardiac output information. The processing stages used in the host microprocessor are implemented by suitable programming of the microprocessor and are discussed below with the help of FIGS. 3-6.
    [0031] The source [0031] 21 of thermal energy is alternately turned on and off. If it is assumed that thermal stability is reached after each change and that there is a substantially constant rate of blood flow, a stable temperature difference can be measured in each case. The quantity of blood flowing past the thermal energy source, i.e., the cardiac output, can be derived from such temperature difference measurements. However, such derivation is complicated by two factors which may affect the measurement of blood flow. First, the rate of blood flow through the heart is not substantially constant but surges with each heart contraction. Second, the temperature of the blood flowing through the heart is not constant but varies with each respiratory (breathing) cycle. In a preferred embodiment, the processing of the data takes such factors into account, as discussed below.
    [0032] The process for determining cardiac output is performed in a microprocessor [0032] 2 which in a first embodiment is programmed to respond to the temperatures sensed at T1 and T2 and to perform the steps depicted in accordance with the flow charts shown in FIGS. 3-5. From a knowledge of such flow charts, it would be well within the skill of those in the art to appropriately program any suitable and known digital microprocessor, such as a personal computer, to perform the steps shown.
    [0033] FIG. 3 depicts a basic process, identified as Process I, which is used in the overall processing of temperature data for determining cardiac output, as subsequently depicted in FIGS. 4 and 5. In the basic process shown in FIG. 3, a temperature difference as a function of time ΔT(t) is determined by a differential amplifier which responds to T[0033] 1(t) and T2(t). Such differences may be effectively smoothed, or filtered, to produce a smooth temperature difference curve, as shown in FIG. 3A, which varies as a function of time in a cyclic manner which depends principally on the respiratory cycle of the person whose cardiac output is being determined.
    [0034] The periods τ[0034] 1, τ2 . . . τn for each respiratory cycle are determined over n cycles. A characteristic of the temperature difference at each cvcle is determined. For example, such characteristic preferably is the averaged temperature difference during each cycle (ΔTτ1, ΔTτ2 . . . ΔTτ2 . . . ΔTτn).
    [0035] (Alternatively, for example, the peak temperature differences may be the determined characteristic.) These averaged temperature differences (ΔT[0035] τn) are added for the n cycles involved and are divided by n to determine an averaged temperature difference per cycle (ΔTτn). The use of Process I is depicted in the process steps shown in FIG. 4, identified as Process II.
    [0036] As seen therein, the steps so Process are first performed when the source [0036] 21 or thermal energy (i.e., a heater) is turned off and the average {overscore (ΔT)}off value per cycle is determined and suitably stored. The sampling time at which such determination is made is depicted in FIG. 6 as the sample time period S1.
    [0037] The heater [0037] 21 is then turned on for a specific time period to supply a known amount of power P to the blood flowing through the heart and, accordingly, the temperature of the blood flowing past the heater rises and the temperature difference ΔT(t) rises over a transition, or delay, rise time period, tR1, shown in FIG. 6 and designated as D1, after which the temperature difference generally stabilizes over a second sample time period S2. As seen in FIG. 4, after the heater 21 is turned on and the temperature has stabilized, Process I is performed, again over n cycles, e.g., over the time period S2, and the averaged temperature difference {overscore (ΔT)}on is determined with the heater turned an and is suitably stored. The heater is then turned off and the temperature falls over a transition, or delay, fall time period tF1, shown in FIG. 6 and designated as D2, generally to its former value.
    [0038] Cardiac output is calculated using the averaged temperature differences when the energy is off and the averaged temperature differences when the energy is on, by the relationship: [0038] F = P C p  ( Δ     T _ on -Δ     T _ off )
    [0039] where: [0039]
    [0040] F=Flow [0040]
    [0041] P=Power [0041]
    [0042] C[0042] P=heat capacitance
    [0043] {overscore (ΔT)}[0043] on=average temperature for power on
    [0044] {overscore (ΔT)}[0044] off=average temperature for power off
    [0045] As seen in FIG. 5, the steps of Process II are repeated indefinitely for N data collection cycles, a data collection cycle being designated as including the time periods S[0045] 1, D1, S2, and D2, as shown in FIG. 6. For each data collection cycle the rise time temperature difference ΔTR between the averaged temperature difference {overscore (ΔT)}on at S2 and the averaged temperature difference {overscore (ΔT)}off at S1 and the fall time temperature difference ΔTF between the averaged temperature difference {overscore (ΔT)}off at S1 and the averaged temperature difference {overscore (ΔT)}on at S2 are determined.
    [0046] The flow, F[0046] R, is calculated for each data collection cycle from the known amount of power P introduced into the blood flow stream by the energy source, or heater 21, from the known heat capacitance of blood, CP, and from the difference in the averaged temperature differences {overscore (ΔT)}on and {overscore (ΔT)}off, which occurs over the data collection cycle S1+D1+S2 in accordance with the following relationship: F R = P C p ( Δ     T _ on -Δ     T _ off )
    [0047] In a similar manner, the flow F[0047] F is calculated from P, CP and the difference in the averaged temperature differences {overscore (ΔT)}on and {overscore (ΔT)}off which occurs over the later portion of the data collection cycle S1+D1+S2 in accordance with the following relationship: F F = P C p ( Δ     T _ on -Δ     T _ off )
    [0048] F[0048] R and FF can be averaged to obtain the averaged flow ({overscore (F) over one data collection cycle as shown in FIG. 6. F _ =F R + F F 2
    [0049] A suitable calibration constant can be used to adjust the values of F[0049] R, FF and F)}.
    [0050] Accordingly, by using two temperature sensors [0050] 19 and 20, cardiac output can be determined several times a minute in accordance with FIGS. 3-6, yielding an effectively continuous cardiac output value. Because such measurements can be made using relatively low power levers, the danger that the heart may be damaged by the introduction of thermal energy is substantially eliminated.
    [0051] It will be apparent that the foregoing technique, which has been described in connection with the direct introduction of heat as an indicator agent and the measurement of temperature, can readily be performed by those skilled in the art by using indicator agents which affect the pH of the blood or change other blood parameters. [0051]
    [0052] In some situations it may be desirable to provide more frequent indications of cardiac output, such as, for example, the instantaneous cardiac output or the cardiac output averaged over each individual cardiac cycle (i.e. each heart beat). Such information can be provided using the further embodiments of the invention discussed below with reference to FIGS. [0052] 7-8. A single temperature sensor 30 at a location near the distal end of the catheter 31 (as shown in FIG. 7A) can be used to determine the instantaneous or beat-to-beat blood velocity V(t). The blood velocity can be combined with the cardiac output averaged over one or more data collection cycles to calculate instantaneous cardiac output. The process used is shown in the process depicted in FIG. 7B, identified as Process IV.
    [0053] As seen therein, the initial temperature T[0053] 3i(t) sensed at temperature sensor 30 as a function of time is smoothed, or filtered, in the manner as previously discussed above, and suitably measured and stored at an initial time t0. A predetermined rise in temperature ΔT3 of the temperature sensor itself is selected. Power is then supplied at time to to the temperature sensor 30 from a power source 30A connected thereto to cause its temperature T3(t) to rise by a predetermined amount.
    [0054] Power may be supplied to the sensor in different ways according to the needs of the particular measurement and the relative simplicity or complexity of the required circuitry, three such ways being depicted in FIGS. 8A, 8B, and [0054] 8C.
    [0055] For example, in a first mode of operation (FIG. 8A), heating power may be supplied to the sensor in such a manner as to keep the final sensor temperature T[0055] 3f(t) constant at an initial level ΔT3 above the initial temperature T3i(t0), i.e. T3f=T3i(t0)+ΔT3 even when the local blood temperature varies with time, as illustrated in FIG. 9A. Under such conditions, the sensor is maintained at a time-varying temperature increment ΔT3(t) above the instantaneous local blood temperature, Tb(t).
    [0056] Alternatively, in a second mode of operation, power can be supplied to the sensor so as to continuously maintain the sensor at a fixed temperature increment above the time varying local blood temperature, as illustrated in FIG. 9B. Under such conditions, ΔT[0056] 3(t)=ΔT3, a constant, and the sensor temperature varies according to T3f(t) ΔT3+T3i(t).
    [0057] A third mcde of heating may also be convenient when the temperature sensors are temperature-sensitive resistors, or thermistors. Thus, when a thermistor is used, it may be more convenient to design an electrical heating circuit that maintains the sensor at a constant resistance increment above the resistance of the sensor that corresponds to the local blood temperature. If R is the corresponding resistance for a sensor temperature T, then these conditions are represented by ΔR[0057] 3(t)=ΔR3, a constant, and the sensor resistance varies according to R3f(t)=ΔR3+R3i(t), as illustrated in FIG. 9C. The change in temperature ΔT3(t) is then replaced by the change in resistance R3(t) in the ratio which is integrated over a cardiac cycle. Further details and exemplary apparatus for such modes of operation are presented and described in U.S. Pat. No. 4,059,982, issued to H. F. Bowman on Nov. 29, 1977. With all three of the above approaches, power (P) is supplied to produce a temperature rise (ΔT) both of which are then related to the instantaneous blood velocity and, hence, blood flow.
    [0058] Techniques in which sensor heating power and temperature can be measured and used to provide more detailed information on cardiac output are described below. The technique involved can be applied to measure both instantaneous cardiac output, and the cardiac output for an individual cardiac cycle. Such detailed measurement information greatly enhances the diagnostic capability of a physician. [0058]
    [0059] First, a method is described to measure instantaneous volumetric flow (which flow if measured at the location described above is the cardiac output). For each of the particular implementations described above, the power P[0059] 3(t) applied to the temperature sensor 30 is controlled so as to maintain the final temperature of the sensor at a desired value T3f. The power applied to the temperature sensor 30 or, more generally, the ratio of the power applied to the sensor to the temperature increment, P3(t)/ΔT3(t), is directly correlated with the fluid and flow properties of the flowing liquid about the sensor.
    [0060] For example, the relationship between required sensor power and local fluid velocity, V(t), is given by a correlation of the form: [0060]
    [0061] Where [0061]
    [0062] P(t)=instantaneous power to sensor [0062]
    [0063] k=thermal conductivity of fluid [0063]
    [0064] a=sensor radius [0064]
    [0065] ΔT(t)=instantaneous temperature difference between heated sensor and unheated fluid temperature. [0065]
    [0066] C[0066] 1=constant of calibration
    [0067] P[0067] r=a non-dimensional “Prandtl” number which relates to the viscosity μ, heat capacity Cp and thermal conductivity k of a fluid.
    [0068] n,m=power factors which are determined from experimental data [0068]
    [0069] ρ=fluid density [0069]
    [0070] μ=viscosity [0070]
    [0071] V(t)=instantaneous fluid velocity [0071]
    [0072] The fluid flow velocity in the vicinity of the sensor can be determined from the required sensor heating power. Volumetric flow in the vessel can then be determined with one further assumption for the distribution of the fluid flow within the vessel. For example, assuming a uniform velocity profile within the vessel, volumetric flow F[0072] 3 is given by
    [0073] where V is the fluid velocity in the vessel and A is the flow area. If the fluid flow area A is not previously known, it may be inferred from the measurement of average volumetric flow in the vessel. Such average volumetric flow can be determined, for example, by using the techniques of the invention already described above herein or by using other techniques for yielding comparable information. For example, if F is the average cardiac output, typically measured over several cardiac cycles, as described above, and V is the average fluid velocity, determined by calculating an average value for the instantaneous flow velocity over at least one cardiac cycle, then one such estimate for the average flow area A is given by [0073]
    [0074] Therefore, given the sensor measured heating power, first the fluid velocity and then volumetric flow can be calculated at any desired instant in time, i.e., F[0074] 3(t)=V(E){overscore (A)}, yielding an instantaneous measure of volumetric lcw, i.e., cardiac output.
    [0075] In another embodiment, a method to measure cardiac output over a single cardiac cycle is described. As described above in different implementations, the power P[0075] 3(t) applied to the temperature sensor 30 is controlled so as to maintain the temperature of the sensor at a desired signal value T3f. The power applied to the temperature sensor 30, or more generally, as discussed above, the ratio of the power applied to the sensor to the temperature increment, i.e., P3(t)/ΔT3(t), is directly correlated with the properties of the fluid flow in the vicinity of the sensor.
    [0076] Thus, the integrated value of the sower to temperature ratio over a single cardiac cycle is directly correlated with, i.e., is proportional to the average cardiac output over the cardiac cycle, [0076] ∫ cardiac     cycle  P 3  ( t )Δ     T 3  ( t )   t∝ F _
    [0077] or, alternatively expressed [0077] 1 T  ∫ cardiac     cycle  P 3  ( t )Δ     T 3  ( t )   t ∝ F _
    [0078] where T represents the period of the cardiac cvcle and {overscore (F)} correspondingly represents cardiac output averaged over the cardiac cycle. Thus, the average cardiac output {overscore (F)} over an individual cardiac cycle then can be determined from the measured and integrated tower and temperature signals from the sensor. [0078]
    [0079] Furthermore, an explicit correlation for integrated power and average cardiac output over the cardac cycle may be dispensed with if a simple qualitative indication of the change in cardiac output on a cardiac cycle-to-cardiac cycle basis is desired. To obtain such information, a given measurement of cardiac output is taken as associated with a corresponding measured value of the integrated sensor signal over a cardiac cycle. The measurement of cardiac output could be obtained intermittently by the techniques described in this invention or other similar techniques. Since cardiac output is known to be correlated with the value of the integrated sensor signal over the cardiac cycle, any changes in the sensor signal indicate a corresponding change in cardiac output. [0079]
    [0080] In certain situations, it may be desirable to compensate for temperature variations in the blood which is flowing past the sensor, as this may affect the value of F(t). A process for such compensation is depicted as Process IV in FIG. 7B wherein a temperature T[0080] 2(t) is sensed by a second sensor (which may be, for example, sensor 19 or sensor 20) at a location remote from sensor 30 (see FIG. 7A). For example, knowledge of the instantanecus blood temperature is required for the process in which the heated sensor is maintained at a constant increment above the local blood temperature. In this case, the temperature T2(t) is used as a proxy for the temperature T3(t) which would be measured in the absence of sensor heating.
    [0081] In a further alternative embodiment, where only two sensors [0081] 19 and 20 are utilized (as shown in FIG. 2), sensor 20 can be used as the primary sensor when calculating instantaneous cardiac output (equivalent to sensor 30 in FIG. 7A) and sensor 19 can be used as the secondary temperature compensation sensor. In such an embodiment, the averaged cardiac output can be determined using sensors 19 and 20, as set forth in FIGS. 3-5 and the instantaneous cardiac output can then subsequently be determined using sensors 19 and 20, as set forth in FIGS. 7B and either FIGS. 8A, 8B or 8C, such average and instantaneous cardiac output determinations being made in sequence by the microprocessor to provide the cardiac information in both forms, as desired.
    [0082] As mentioned above, when using the above described catheter, the various flow values which are determined in accordance with the processes as discussed above are proportional to flow but may not be equal to the actual flow values unless they are suitably calibrated since the correspondence between the calculated and actual values depends on the manner in which a particular catheter is constructed and used. A calibration constant for a particular carrier can be represented by the slope and intercept of a curve which relates the calculated flow and the actual flow, in accordance with the following relationship: [0082]
    [0083] where, as illustrated in FIG. 10, “a” is the slope of a straight line [0083] 35 and “b” is the intercept thereof along the vertical axis. Curve 35 can be obtained by using a known catheter and shown flow values therein to construct a curve 36. The best straight line fit is determined as line 35. The slope “a” and intercept “b” are thereby determined. Such deternined values for “a” and “b” can be used with the calculated flow values in each case to determine the actual flow from the calculated flow.
    [0084] While the above description discusses preferred embodiments of the invention, modifications thereof may occur to those in the art within the spirit and scope of the invention. Hence, the invention is not to be construed as limited to particular embodiments described, except as defined by the appended claims. [0084]
    权利要求:
    Claims (46)
    [1" id="US-20010000792-A1-CLM-00001] 1. A method for determining blood flow in a living body comprising the steps of:
    changing the thermal enery level by a predetermined amount at a site in a blood flow path of said living body;
    detecting the temperatures at a first location upstream of said site and a second location downstream of said site;
    determining the temperature difference between said first and second locations at one energy level;
    determining the temperature difference between said first and second locations at a changed energy level; and
    calculating blood flow as a function of the change in energy level and of the temperature differences measured prior to and following the change in energy level.
    [2" id="US-20010000792-A1-CLM-00002] 2. A method in accordance with
    claim 1 wherein said first location is substantially thermally isolated from thermal energy changes occurring at said site.
    [3" id="US-20010000792-A1-CLM-00003] 3. A method in accordance with
    claim 2 wherein said blood flow path includes at least a portion of the heart of a living body and the blood flow represents cardiac output.
    [4" id="US-20010000792-A1-CLM-00004] 4. A method in accordance with
    claim 3 wherein said site is at least partially in the right atrium of the heart, said first location is in the vena cava of the heart, and the second location is in or near the pulmonary artery of the heart.
    [5" id="US-20010000792-A1-CLM-00005] 5. A method in accordance with
    claim 3 wherein said site is at least partially the right atrium of the heart, said first location is in the vena cava of the heart, and the second location is in or near the right ventricle of the heart.
    [6" id="US-20010000792-A1-CLM-00006] 6. A method in accordance with claims 1, 2, 3, 4, or 5 wherein said thermal energy is changed by applying thermal energy from a catheter borne thermal energy source which is positioned in the blood flow path and wherein temperatures are detected by temperature sensors in said catheter at said first and second locations, respectively.
    [7" id="US-20010000792-A1-CLM-00007] 7. A method for determining blood flow in a living body comprising the steps of:
    changing the thermal energy at a site in a blood flow path of said living body, from a first level to a second level;
    determining a characteristic of the temperature difference between the temperatures in said blood flow path at a first location upstream of said site and at a second location downstream of said site at said first level;
    determining a characteristic of the temperature difference between the temperatures in said blood flow path at the first location and at the second location at said second level;
    determining the difference between the characteristics of said temperature differences;
    calculating blood flow as a function of the difference between the characteristics of said temperature differences and the change in thermal energy from said first level to said second level.
    [8" id="US-20010000792-A1-CLM-00008] 8. A method in accordance with
    claim 7 wherein each of said characteristics is determined over a specified time period.
    [9" id="US-20010000792-A1-CLM-00009] 9. A method in accordance with
    claim 8 wherein each of said characteristics is the average of the temperature differences.
    [10" id="US-20010000792-A1-CLM-00010] 10. A method in accordance with
    claim 8 wherein the specified time period is at least one respiratory cycle.
    [11" id="US-20010000792-A1-CLM-00011] 11. A method in accordance with
    claim 7 ,
    8 , 9, or 10 wherein said blood flow path includes at least a portion of the heart of a living body where the blood flow represents cardiac output.
    [12" id="US-20010000792-A1-CLM-00012] 12. A method in accordance with
    claim 11 wherein said site is at least partially in the right atrium of the heart, said first location is in the vena cava of the heart, and the second location is in or near the pulmonary artery of the heart.
    [13" id="US-20010000792-A1-CLM-00013] 13. A method in accordance with
    claim 11 wherein said site is at least partially in the right atrium of the heart, said first location is in the vena cava of the heart, and the second location is in or near the right ventricle of the heart.
    [14" id="US-20010000792-A1-CLM-00014] 14. A method in accordance with
    claim 7 wherein each of said characteristic temperature difference determining steps includes the steps of:
    detecting temperatures at said first location upstream of said site and at said second location downstream of said site during each cycle of one or more respiratory cycles, when said thermal energy is at said first level and when said thermal energy is at said second level;
    determining temperature differences between said temperatures for each respiratory cycle, when said thermal energy is at said first level and when said thermal energy is at said second level; and
    determining the average of said temperature differences over multiple respiratory cycles.
    [15" id="US-20010000792-A1-CLM-00015] 15. A method in accordance with
    claim 7 wherein:
    said thermal energy level changing step includes applying a predetermined amount of power P at said site to change said thermal energy level from said first level to said second level and said cardiac output calculating step includes the steps of
    calculating a rise-time cardiac output component as a function of the power P, the calculated average rise-time temperature difference, and the heat capacity of blood;
    calculating a fall-time cardiac output component as a function of the power P, the calculated fall-time difference, and the heat capacity of blood; and
    calculating the cardiac output as a function of the rise-time and fall-time cardiac components.
    [16" id="US-20010000792-A1-CLM-00016] 16. A method in accordance with claims 7, 8, 9, 10 and 15 wherein the steps therein can be successively repeated a plurality of times to provide repeated calculations of the cardiac output to provide an effectively continuous calculation thereof.
    [17" id="US-20010000792-A1-CLM-00017] 17. A method in accordance with
    claim 16 wherein the repeated calculations of the cardiac output can be averaged over a selected number of said plurality of times to provide an averaged cardiac output over said selected number of times.
    [18" id="US-20010000792-A1-CLM-00018] 18. A svstem for termining blood flow in a living body comprising:
    means for changing the thermal energy level by a predetermined amount at a site in a blood flow path of said living body;
    means for detecting the temperatures at a first location upstream of said site and a second location downstream of said site;
    means for determining the temperature difference between said first and second locations at one energy level;
    means for determining the temperature difference betweem said fast and second locations at a changed energy level; and
    means for calculating blood flow as a function of the change in energy level and of the temperature differences measured prior to and following the change in energy level.
    [19" id="US-20010000792-A1-CLM-00019] 19. A system in accordance with
    claim 18 wherein said first location is substantially thermally isolated from thermal energy changes occurring at said site.
    [20" id="US-20010000792-A1-CLM-00020] 20. A system in accordance with
    claim 19 wherein said blood flow path includes at least a portion of the heart of a living body and the blood flow represents cardiac output.
    [21" id="US-20010000792-A1-CLM-00021] 21. A system in accordance with
    claim 20 wherein said site is at least partially in the right atrium of the heart, said first location is in the vena cava of the heart, and the second location is in or near the pulmonary artery of the heart.
    [22" id="US-20010000792-A1-CLM-00022] 22. A system in accordance with
    claim 20 wherein said site is at least partially the right atrium of the heart, said first lccation is in the vena cava of the heart, and the second location is in or near the right ventricle of the heart.
    [23" id="US-20010000792-A1-CLM-00023] 23. A system in accordance with claims 18, 19, 20, 21 or 22 wherein said system includes a catheter, said thermal energy changing means is a thermal energy source carried by said catheter and positioned in the blood flow past, and said temperature detecting means are temperature sensors positioned in said catheter so that when said catheter is positioned in said blood flow path said thermal energy source is at said site and said temperature sensors are at said first and second locations, respectively.
    [24" id="US-20010000792-A1-CLM-00024] 24. A system for determining blood flow in a living body comprising:
    means for changing the thermal energy at a site in a blood flow path of said living body, from a first level to a second level;
    means for determining a characteristic of the temperature difference between the temperatures in said blood flow path at a first location upstream of said site and at a second location downstream of said site at said first level;
    means for determining a characteristic of the temperature difference between the temperatures in said blood flow path at the first location and at the second location at said second level;
    means for determining the difference between the characteristics of said temperature differences;
    means for calculating blood flow as a function of the difference between the characteristics of said temperature differences and the change in thermal energy from said first level to said second level.
    [25" id="US-20010000792-A1-CLM-00025] 25. A system in accordance with
    claim 24 wherein said characteristic determining means determines said characteristics over a specified time period.
    [26" id="US-20010000792-A1-CLM-00026] 26. A system in accordance with
    claim 25 wherein each of said characteristics is the average of the temperature differences.
    [27" id="US-20010000792-A1-CLM-00027] 27. A system in accordance with
    claim 25 wherein the specified time period is at least one respiratory cycle.
    [28" id="US-20010000792-A1-CLM-00028] 28. A system in accordance with claims 24, 25, 26 or 27 wherein said blood flow path includes at least a portion of the heart of a living body where the blood flow represents cardiac output.
    [29" id="US-20010000792-A1-CLM-00029] 29. A system in accordance with
    claim 20 wherein said site is at least partially in the right atrium of the heart, said first location is in the vena cava of the heart, and the second location is in or near the pulmonary artery of the heart.
    [30" id="US-20010000792-A1-CLM-00030] 30. A system in accordance with
    claim 28 wherein said site is at least partially in the right atrium of the heart, said first location is in the vena cava of the heart, and the second location is in or near the right ventricle of the heart.
    [31" id="US-20010000792-A1-CLM-00031] 31. A system in accordance with
    claim 24 wherein each of said characteristic temperature difference determining means includes:
    means for detecting temperatures at said first location upstream of said site and at said second location downstream of said site during each cycle of one or more respiratory cycles, when said thermal energy is at said first level and when said thermal energy is at said second level;
    means for determining temperature differences between said temperatures for each respiratory cycle, when said thermal energy is at said first level and when said thermal energy is at said second level; and
    means for determining the average of said temperature differences over multiple respiratory cycles.
    [32" id="US-20010000792-A1-CLM-00032] 32. A method in accordance with
    claim 24 wherein:
    said thermal energy level changing means includes means for applying a predetermined amount of power P at said site to change said thermal energy level from said first level to said second level; and
    said cardiac output calculating means includes
    means for calculating a rise-time cardiac output component as a function of the power P, the calculated average rise-time temperature difference, and the heat capacity of blood;
    means for calculating a fall-time cardiac output component as a function of the power P, the calculated fall-time difference, and the heat capacity of blood; and
    means for calculating the cardiac output as a function of the rise-time and fall-time cardiac components.
    [33" id="US-20010000792-A1-CLM-00033] 33. A system in accordance with claims 24, 25, 26 or 27 wherein said system calculates the cardiac output repeatedly to provide an effectively continuous calculation thereof.
    [34" id="US-20010000792-A1-CLM-00034] 34. A system in accordance with
    claim 33 and further including means responsive to the repeated calculations of the cardiac output can For averaging said calculation over a selected number of repeated calculations to provide an averaged cardiac output over said selected number of calculations.
    [35" id="US-20010000792-A1-CLM-00035] 35. A methcd for determining blood flow in a living body comprising the steps of:
    changing the value of the selected parameter of blood at a site in a blood flow path of said living body, from a first level to a second level;
    determining the difference between the value of the selected parameter in said blood flow path at a first location upstream of said site and at a second location downstream of said site at said first level;
    determining the difference between the value of the selected parameter in said blood flow path at the first location and at the second location at said second level;
    determining the difference between the value obtained in the first said difference determining steps and the value obtained in the second said difference determining steps; and
    calculating blood flow as a function of the difference between the values obtained in said first and second difference determining steps and the change in the value of the selected parameter from said first level to said second level.
    [36" id="US-20010000792-A1-CLM-00036] 36. A method in accordance with
    claim 35 wherein said blood flow path includes at least a portion of the heart or a living body where the blood flow represents cardiac output.
    [37" id="US-20010000792-A1-CLM-00037] 37. A svstem for determining blood flow in a living body comprising:
    means for changing the value of the selected parameter of blood at a site in a blood flow path of said living body, from a first level to a second level;
    means for determining the difference between the value of the selected parameter in said blood flow path at a first location upstream of said site and at a second location downstream of said site at said first level;
    means for determining the difference between the value of the selected parameter in said blood flow path at a first location upstream of said site and at a second location downstream of said site at said first level;
    means for determining the difference between the value of the selected parameter in said blood flow path at the first location and at the second location at said second level;
    means for determining the difference between the value obtained in the first said difference determining steps and the value obtained in the second said difference determining steps; and
    means or calculating blood flow as a function of the difference between the values obtained in said first and second difference determining steps and the chance in the value of the selected parameter from said first level to said second level.
    [38" id="US-20010000792-A1-CLM-00038] 38. A system in accordance with
    claim 37 where n said blood flow path includes at least a portion of the heart of a living body where the blood flow represents cardiac output.
    [39" id="US-20010000792-A1-CLM-00039] 39. A method for determining instantaneous blood flow in a living body comprising the steps of:
    determining the temperature level at a selected location in a blood flow path of said living body;
    heating said selected location in said blood flow path to a final temperature level;
    determining the final temperature level;
    determining the ratio of the heating power required to heat said selected location to said final temperature level to the change in temperature level at said selected location.
    [40" id="US-20010000792-A1-CLM-00040] 40. A method in accordance with
    claim 39 wherein said indicating step includes integrating said ratio over a single cardiac cycle and dividing the integrated value by the period of said cardiac cycle to obtain the average instantaneous blood flow in said living body over said cardiac cycle.
    [41" id="US-20010000792-A1-CLM-00041] 41. A. method in accordance with claims 39 or 40 wherein said heating and said fInal temperature level determining steps include
    determining the initial temperature level at said selected location before heating said selected location;
    heating said selected location to said final temperature level;
    maintaining said final temperature level at a constant value while heating said selected location over time; and
    determining the time varying change in the temperature level at said selected location which is recuired to maintain said final temperature level at said constant value.
    [42" id="US-20010000792-A1-CLM-00042] 42. A method in accordance with claims 39 or 40 wherein said heating and said final temperature level determining steps include
    heating said selected location from an initial temperature level to a final temperature level by changing the temperature level by a fixed amount; and
    maintaining the changing temperature level at said fixed amount over time and
    determining the time varying temperature level over said time.
    [43" id="US-20010000792-A1-CLM-00043] 43. A method in accordance with claims 39 or 40 wherein said heating step includes heating a sensor positioned at said selected location, said sensor having a resistance R which varies as a function of the temperature thereof and further including the steps of:
    heating said sensor to a final resistance value thereby changing the resistance value of said sensor;
    maintaining the changing resistance value of said sensor during heating at a fixed amount over time; and
    determining the time varying final resistance value of said sensor during the heating over said time;
    and further wherein said ratio determining step includes
    determining the ratio of the heating power required to heat said sensor to said final resistance value to the fixed changing resistance value thereof.
    [44" id="US-20010000792-A1-CLM-00044] 44. A device for insertion into the bloodstream of a living organism to obtain physiological data comprising:
    an elongated flexible catheter adapted to be inserted into the venous or arterial system of the living organism;
    first temperature sensing means carried by said catheter;
    second temperature sensing means carried by said catheter positioned to be upstream of said first temperature sensing means when in use; and
    heating means carried by said catheter between said first and second temperature sensing means and positioned to be substantially thermally isolated from said second temperature sensing means when in use;
    said rst and second temperature sensing means and said heating means being adapted to be in communication with a data processing system.
    [45" id="US-20010000792-A1-CLM-00045] 45. A device in accordance with
    claim 44 and further comprising
    thermistor means carried by said catheter and positioned to be downstream of said heating means when in use, said thermistor means being adapted to be in communication with said data processing system.
    [46" id="US-20010000792-A1-CLM-00046] 46. A device for insertion into the bloodstream of a living organism to obtain physiological data comprising:
    an elongated flexible catheter adapted to be inserted into the venous or arterial system of the living organism;
    temperature sensing means carried by said catheter; and
    thermistor means carried by said catheter and positioned to be downstream of said temperature sensing means when in use;
    said temperature sensing means and said thermistor means being adapted to be in communication with a data processing system.
    类似技术:
    公开号 | 公开日 | 专利标题
    US6565516B2|2003-05-20|Method and apparatus for measuring continuous blood flow at low power
    US7753854B2|2010-07-13|Blood flow monitor with arterial and venous sensors
    US5509424A|1996-04-23|Continuous cardiac output monitoring system
    US5526817A|1996-06-18|Process for determining a patient's circulatory fill status
    US6736782B2|2004-05-18|Apparatus, computer program, central venous catheter assembly and method for hemodynamic monitoring
    JP3692035B2|2005-09-07|Narrow channel flow measurement method including temperature and pressure sensors
    AU668688B2|1996-05-16|Heated catheter for monitoring cardiac output
    US4236527A|1980-12-02|Cardiac output detection by multiple frequency thermodilution
    US8016766B2|2011-09-13|Central venous catheter assembly for measuring physiological data for cardiac output determination and method of determining cardiac output
    EP1645226A2|2006-04-12|A system for measuring blood flow rate by thermodilution
    US4542748A|1985-09-24|Apparatus and method for measuring cardiac output
    US4015593A|1977-04-05|Apparatus and method for measuring cardiac output
    WO2004086976A1|2004-10-14|Blood flow monitor with venous and arterial sensors
    WO1996034557A1|1996-11-07|Method and apparatus for measuring blood flow
    US20140081157A1|2014-03-20|Apparatus and Method for determining a volume amount of a physiological volume
    US6858013B1|2005-02-22|Method and apparatus for determining the cardiac output of a patient
    CA2144600A1|1996-09-15|Method and apparatus for measuring continuous blood flow at low power
    JP2554082B2|1996-11-13|Arterial blood oxygen gas partial pressure measuring device
    JP3069128B2|2000-07-24|Cardiac output measurement device
    同族专利:
    公开号 | 公开日
    US20030120162A1|2003-06-26|
    JP2004195251A|2004-07-15|
    EP0712290A4|1996-07-03|
    EP0712290A1|1996-05-22|
    US6913576B2|2005-07-05|
    US5692514A|1997-12-02|
    JPH09501591A|1997-02-18|
    JP3557211B2|2004-08-25|
    US6565516B2|2003-05-20|
    US6203501B1|2001-03-20|
    US6165132A|2000-12-26|
    US5797398A|1998-08-25|
    CA2169374A1|1995-02-23|
    WO1995005115A3|1995-04-13|
    WO1995005115A2|1995-02-23|
    引用文献:
    公开号 | 申请日 | 公开日 | 申请人 | 专利标题
    US20030219719A1|2002-04-05|2003-11-27|Thermal Technologies, Inc.|System for quantifying blood flow in tissue with periodic updating of tissue baseline conditions|
    US20080051838A1|2006-08-24|2008-02-28|Shuros Allan C|Integrated cardiac rhythm management system with heart valve|US3075515A|1958-10-17|1963-01-29|Albert M Richards|Blood flow meter|
    US3359974A|1963-10-07|1967-12-26|Hassan H Khalil|Device for the thermal determination of cardiac volumetric performance|
    US3438253A|1966-11-15|1969-04-15|Frederick W Kuether|Thermal device for measuring direction and velocity of fluid flow|
    FR2112767A5|1970-11-09|1972-06-23|Durand Herve||
    NL161664C|1972-04-05|1980-03-17|Philips Nv|HEART RATE VOLUME METER.|
    US4059982A|1975-08-29|1977-11-29|Massachusetts Institute Of Technology|Apparatus for the measurement of thermal properties of biomaterials|
    US4105022A|1976-05-24|1978-08-08|Becton, Dickinson And Company|Method of determining cardiac output by thermodilution principles and utilization of a catheter assembly|
    FR2411392B1|1977-12-09|1980-10-17|Ebauches Sa||
    US4217910A|1978-10-10|1980-08-19|The United States Of America As Represented By The Secretary Of The Navy|Internal jugular and left ventricular thermodilution catheter|
    US4236527A|1978-10-20|1980-12-02|Massachusetts General Hospital|Cardiac output detection by multiple frequency thermodilution|
    US4230126A|1978-11-20|1980-10-28|Elings Virgil B|Apparatus and method for measuring extravascular lung water|
    IT1165014B|1979-03-27|1987-04-22|Innocenti Santeustacchio Spa|GEOMETRIC CONTROL SYSTEM, TO INCREASE THE ACCURACY OF A MACHINE TOOL, PARTICULARLY OF A LARGE DIMENSION MACHINE TOOL|
    US4354504A|1979-09-04|1982-10-19|Bro William J|Thermal diffusion flow probe|
    US4562843A|1980-09-29|1986-01-07|Ljubomir Djordjevich|System for determining characteristics of blood flow|
    US4509526A|1983-02-08|1985-04-09|Lawrence Medical Systems, Inc.|Method and system for non-invasive ultrasound Doppler cardiac output measurement|
    NL189547C|1983-04-12|1993-05-17|Univ Erasmus|SYSTEM FOR DETERMINING THE CURRENT STRENGTH OF A PATIENT'S HEART.|
    US4507974A|1983-04-21|1985-04-02|The Board Of Trustees Of The Leland Stanford Jr. University|Method and apparatus for measuring flow|
    JPH0368690B2|1984-11-21|1991-10-29|Terumo Corp||
    US4730623A|1985-06-14|1988-03-15|Lee Arnold St J|Cardiac output estimation method and apparatus|
    JPH0434408B2|1986-03-07|1992-06-05|Terumo Corp||
    DE3714027C2|1987-04-27|1989-04-06|Eckhard Dr. 8000 Muenchen De Alt||
    US4785823A|1987-07-21|1988-11-22|Robert F. Shaw|Methods and apparatus for performing in vivo blood thermodilution procedures|
    US4901734A|1987-08-17|1990-02-20|Nova Medical Specialties|Dual-thermistor thermodilution catheter|
    DK161260C|1988-05-06|1991-12-30|Paul Verner Nielsen|flow measurement|
    US5000190A|1988-06-22|1991-03-19|The Cleveland Clinic Foundation|Continuous cardiac output by impedance measurements in the heart|
    JPH0562539B2|1988-11-09|1993-09-08|Terumo Corp||
    JPH0579327B2|1989-01-13|1993-11-02|Terumo Corp||
    US5056526A|1989-10-27|1991-10-15|Khalil Hassan H|Device for global evaluation of the left ventricular ejection fraction by thermodilution|
    US5146414A|1990-04-18|1992-09-08|Interflo Medical, Inc.|Method and apparatus for continuously measuring volumetric flow|
    GB9011259D0|1990-05-19|1990-07-11|Nashef Samer A|Catheters|
    JPH0693886B2|1990-10-31|1994-11-24|日本光電工業株式会社|Cardiac function measuring device|
    US5553622A|1991-01-29|1996-09-10|Mckown; Russell C.|System and method for controlling the temperature of a catheter-mounted heater|
    US5682899A|1991-05-16|1997-11-04|Ami-Med Corporation|Apparatus and method for continuous cardiac output monitoring|
    US5174299A|1991-08-12|1992-12-29|Cardiac Pacemakers, Inc.|Thermocouple-based blood flow sensor|
    US5217019A|1991-12-27|1993-06-08|Abbott Laboratories|Apparatus and method for continuously monitoring cardiac output|
    US5305760A|1992-02-07|1994-04-26|Interflo Medical Inc.|Method for rejecting electrical interference from physiological measurements|
    US5797398A|1993-08-13|1998-08-25|Thermal Technologies, Inc.|Method and apparatus for measuring continuous blood flow at low power|
    US5509424A|1994-01-28|1996-04-23|Aws Salim Nashef|Continuous cardiac output monitoring system|US5797398A|1993-08-13|1998-08-25|Thermal Technologies, Inc.|Method and apparatus for measuring continuous blood flow at low power|
    US7527598B2|1993-08-13|2009-05-05|Thermal Technologies, Inc.|Blood flow monitor with venous and arterial sensors|
    US5954659A|1996-02-16|1999-09-21|Curley; Michael G.|Method and apparatus for invasively measuring cardiac output by detecting temperature differences of blood heated by radiation|
    US5989192A|1997-09-25|1999-11-23|Medtronic, Inc.|Cardiac flow sensor|
    US6391005B1|1998-03-30|2002-05-21|Agilent Technologies, Inc.|Apparatus and method for penetration with shaft having a sensor for sensing penetration depth|
    NL1011339C2|1999-02-18|2000-08-22|Johannes Jacobus Schreuder|A method and apparatus for determining the blood flow of a patient's heart.|
    US7217245B1|1999-04-15|2007-05-15|University Of Utah Research Foundation|Noninvasive methods for detecting abnormalities in a subject such as disease or dysfunction|
    US6277082B1|1999-07-22|2001-08-21|C. R. Bard, Inc.|Ischemia detection system|
    AT367117T|1999-12-17|2007-08-15|Hove Jens|METHOD AND DEVICE FOR MEASURING FLOW RATE|
    US8641644B2|2000-11-21|2014-02-04|Sanofi-Aventis Deutschland Gmbh|Blood testing apparatus having a rotatable cartridge with multiple lancing elements and testing means|
    US7892183B2|2002-04-19|2011-02-22|Pelikan Technologies, Inc.|Method and apparatus for body fluid sampling and analyte sensing|
    US8372016B2|2002-04-19|2013-02-12|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for body fluid sampling and analyte sensing|
    US6551250B2|2001-03-29|2003-04-22|Hassan Khalil|Transit time thermodilution guidewire system for measuring coronary flow velocity|
    CA2445450C|2001-05-17|2008-08-12|Thermal Technologies, Inc.|Blood flow monitor for shock and resuscitation|
    US7491178B2|2002-04-19|2009-02-17|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    DE60238119D1|2001-06-12|2010-12-09|Pelikan Technologies Inc|ELECTRIC ACTUATOR ELEMENT FOR A LANZETTE|
    US9795334B2|2002-04-19|2017-10-24|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for penetrating tissue|
    AU2002348683A1|2001-06-12|2002-12-23|Pelikan Technologies, Inc.|Method and apparatus for lancet launching device integrated onto a blood-sampling cartridge|
    US9427532B2|2001-06-12|2016-08-30|Sanofi-Aventis Deutschland Gmbh|Tissue penetration device|
    US9314194B2|2002-04-19|2016-04-19|Sanofi-Aventis Deutschland Gmbh|Tissue penetration device|
    US7981056B2|2002-04-19|2011-07-19|Pelikan Technologies, Inc.|Methods and apparatus for lancet actuation|
    US9248267B2|2002-04-19|2016-02-02|Sanofi-Aventis Deustchland Gmbh|Tissue penetration device|
    US7976476B2|2002-04-19|2011-07-12|Pelikan Technologies, Inc.|Device and method for variable speed lancet|
    US8267870B2|2002-04-19|2012-09-18|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for body fluid sampling with hybrid actuation|
    US7547287B2|2002-04-19|2009-06-16|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US7909778B2|2002-04-19|2011-03-22|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US8221334B2|2002-04-19|2012-07-17|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for penetrating tissue|
    US7331931B2|2002-04-19|2008-02-19|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US7041068B2|2001-06-12|2006-05-09|Pelikan Technologies, Inc.|Sampling module device and method|
    CA2448902C|2001-06-12|2010-09-07|Pelikan Technologies, Inc.|Self optimizing lancing device with adaptation means to temporal variations in cutaneous properties|
    US7229458B2|2002-04-19|2007-06-12|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US7297122B2|2002-04-19|2007-11-20|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US7198606B2|2002-04-19|2007-04-03|Pelikan Technologies, Inc.|Method and apparatus for a multi-use body fluid sampling device with analyte sensing|
    US8360992B2|2002-04-19|2013-01-29|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for penetrating tissue|
    US8784335B2|2002-04-19|2014-07-22|Sanofi-Aventis Deutschland Gmbh|Body fluid sampling device with a capacitive sensor|
    US7674232B2|2002-04-19|2010-03-09|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US9226699B2|2002-04-19|2016-01-05|Sanofi-Aventis Deutschland Gmbh|Body fluid sampling module with a continuous compression tissue interface surface|
    US8579831B2|2002-04-19|2013-11-12|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for penetrating tissue|
    US8337419B2|2002-04-19|2012-12-25|Sanofi-Aventis Deutschland Gmbh|Tissue penetration device|
    US7901362B2|2002-04-19|2011-03-08|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US7232451B2|2002-04-19|2007-06-19|Pelikan Technologies, Inc.|Method and apparatus for penetrating tissue|
    US7175642B2|2002-04-19|2007-02-13|Pelikan Technologies, Inc.|Methods and apparatus for lancet actuation|
    AU2003220474A1|2002-03-21|2003-10-08|Radiant Medical, Inc.|Measuring blood flow rate or cardiac output|
    US8702624B2|2006-09-29|2014-04-22|Sanofi-Aventis Deutschland Gmbh|Analyte measurement device with a single shot actuator|
    US8574895B2|2002-12-30|2013-11-05|Sanofi-Aventis Deutschland Gmbh|Method and apparatus using optical techniques to measure analyte levels|
    US7534207B2|2003-02-07|2009-05-19|Alfred E. Mann Institute For Biomedical Engineering At The University Of Southern California|Implantable device with sensors for differential monitoring of internal condition|
    WO2004071279A2|2003-02-07|2004-08-26|Alfred E. Mann Institute For Biomedical Engineering At The University Of Southern California|Surgical drain with sensors for tissue monitoring|
    US7631382B2|2003-03-10|2009-12-15|Adidas International Marketing B.V.|Intelligent footwear systems|
    JP2006521179A|2003-03-26|2006-09-21|サーマル・テクノロジーズ・インコーポレイテツド|Blood flow monitor with arteriovenous sensor|
    EP2238892A3|2003-05-30|2011-02-09|Pelikan Technologies Inc.|Apparatus for body fluid sampling|
    WO2004107964A2|2003-06-06|2004-12-16|Pelikan Technologies, Inc.|Blood harvesting device with electronic control|
    US8282576B2|2003-09-29|2012-10-09|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for an improved sample capture device|
    US9351680B2|2003-10-14|2016-05-31|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for a variable user interface|
    US20090214741A1|2003-11-12|2009-08-27|Chandrani Atapattu|Low density stable whipped frosting|
    US8668656B2|2003-12-31|2014-03-11|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for improving fluidic flow and sample capture|
    US7520862B2|2004-02-03|2009-04-21|Neuro Diagnostic Devices, Inc.|Cerebral spinal fluid shunt evaluation system|
    US20080214951A1|2004-02-03|2008-09-04|Neuro Diagnostic Devices, Inc.|Cerebrospinal Fluid Evaluation Systems|
    WO2006011062A2|2004-05-20|2006-02-02|Albatros Technologies Gmbh & Co. Kg|Printable hydrogel for biosensors|
    US9775553B2|2004-06-03|2017-10-03|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for a fluid sampling device|
    EP1765194A4|2004-06-03|2010-09-29|Pelikan Technologies Inc|Method and apparatus for a fluid sampling device|
    WO2006001797A1|2004-06-14|2006-01-05|Pelikan Technologies, Inc.|Low pain penetrating|
    US8652831B2|2004-12-30|2014-02-18|Sanofi-Aventis Deutschland Gmbh|Method and apparatus for analyte measurement test time|
    US7822454B1|2005-01-03|2010-10-26|Pelikan Technologies, Inc.|Fluid sampling device with improved analyte detecting member configuration|
    US20070167865A1|2005-11-29|2007-07-19|Lopez George A|Cardiac output measurement devices and methods|
    US7749249B2|2006-02-21|2010-07-06|Kardium Inc.|Method and device for closing holes in tissue|
    US20070270688A1|2006-05-19|2007-11-22|Daniel Gelbart|Automatic atherectomy system|
    US9119633B2|2006-06-28|2015-09-01|Kardium Inc.|Apparatus and method for intra-cardiac mapping and ablation|
    US8449605B2|2006-06-28|2013-05-28|Kardium Inc.|Method for anchoring a mitral valve|
    US8920411B2|2006-06-28|2014-12-30|Kardium Inc.|Apparatus and method for intra-cardiac mapping and ablation|
    US10028783B2|2006-06-28|2018-07-24|Kardium Inc.|Apparatus and method for intra-cardiac mapping and ablation|
    US7837610B2|2006-08-02|2010-11-23|Kardium Inc.|System for improving diastolic dysfunction|
    US8906011B2|2007-11-16|2014-12-09|Kardium Inc.|Medical device for use in bodily lumens, for example an atrium|
    ES2385603T3|2007-11-23|2012-07-27|Pulsion Medical Systems Ag|Central venous sensor assembly for measuring physiological data for the determination of cardiac output and procedure for determining cardiac output|
    US8489172B2|2008-01-25|2013-07-16|Kardium Inc.|Liposuction system|
    WO2009126900A1|2008-04-11|2009-10-15|Pelikan Technologies, Inc.|Method and apparatus for analyte detecting device|
    US20090287304A1|2008-05-13|2009-11-19|Kardium Inc.|Medical Device for Constricting Tissue or a Bodily Orifice, for example a mitral valve|
    JP2012501218A|2008-08-26|2012-01-19|カーディアックペースメイカーズ,インコーポレイテッド|Cardiac output estimation device using pulmonary artery pressure|
    US9375169B2|2009-01-30|2016-06-28|Sanofi-Aventis Deutschland Gmbh|Cam drive for managing disposable penetrating member actions with a single motor and motor and control system|
    US8939914B2|2009-02-27|2015-01-27|Thermimage, Inc.|Radiometers and related devices and methods|
    US8939912B2|2009-02-27|2015-01-27|Thermimage, Inc.|Tissue heating and monitoring system with seat|
    WO2011041571A2|2009-10-01|2011-04-07|Kardium Inc.|Medical device, kit and method for constricting tissue or a bodily orifice, for example, a mitral valve|
    US8965476B2|2010-04-16|2015-02-24|Sanofi-Aventis Deutschland Gmbh|Tissue penetration device|
    US9795747B2|2010-06-02|2017-10-24|Sanofi-Aventis Deutschland Gmbh|Methods and apparatus for lancet actuation|
    US8940002B2|2010-09-30|2015-01-27|Kardium Inc.|Tissue anchor system|
    US9486273B2|2011-01-21|2016-11-08|Kardium Inc.|High-density electrode-based medical device system|
    USD777925S1|2012-01-20|2017-01-31|Kardium Inc.|Intra-cardiac procedure device|
    CA2764494A1|2011-01-21|2012-07-21|Kardium Inc.|Enhanced medical device for use in bodily cavities, for example an atrium|
    USD777926S1|2012-01-20|2017-01-31|Kardium Inc.|Intra-cardiac procedure device|
    US9452016B2|2011-01-21|2016-09-27|Kardium Inc.|Catheter system|
    US9072511B2|2011-03-25|2015-07-07|Kardium Inc.|Medical kit for constricting tissue or a bodily orifice, for example, a mitral valve|
    WO2013063377A1|2011-10-28|2013-05-02|The Feinstein Institute For Medical Research|Microchip sensor for continuous monitoring of regional blood flow|
    US9011423B2|2012-05-21|2015-04-21|Kardium, Inc.|Systems and methods for selecting, activating, or selecting and activating transducers|
    US9198592B2|2012-05-21|2015-12-01|Kardium Inc.|Systems and methods for activating transducers|
    US10827977B2|2012-05-21|2020-11-10|Kardium Inc.|Systems and methods for activating transducers|
    US10448843B1|2014-07-16|2019-10-22|Verily Life Sciences Llc|Flow detection|
    US10368936B2|2014-11-17|2019-08-06|Kardium Inc.|Systems and methods for selecting, activating, or selecting and activating transducers|
    US10722184B2|2014-11-17|2020-07-28|Kardium Inc.|Systems and methods for selecting, activating, or selecting and activating transducers|
    法律状态:
    2006-05-24| FPAY| Fee payment|Year of fee payment: 4 |
    2010-07-12| FPAY| Fee payment|Year of fee payment: 8 |
    2014-12-24| REMI| Maintenance fee reminder mailed|
    2015-05-20| LAPS| Lapse for failure to pay maintenance fees|
    2015-06-15| STCH| Information on status: patent discontinuation|Free format text: PATENT EXPIRED DUE TO NONPAYMENT OF MAINTENANCE FEES UNDER 37 CFR 1.362 |
    2015-07-07| FP| Lapsed due to failure to pay maintenance fee|Effective date: 20150520 |
    优先权:
    申请号 | 申请日 | 专利标题
    US08/106,068|US5797398A|1993-08-13|1993-08-13|Method and apparatus for measuring continuous blood flow at low power|
    US08/946,366|US6203501B1|1993-08-13|1997-10-07|Method and apparatus for measuring continuous blood flow at low power|
    US09/733,595|US6565516B2|1993-08-13|2000-12-08|Method and apparatus for measuring continuous blood flow at low power|US09/733,595| US6565516B2|1993-08-13|2000-12-08|Method and apparatus for measuring continuous blood flow at low power|
    US10/364,773| US6913576B2|1993-08-13|2003-02-11|Method for measuring blood flow|
    US10/809,120| US7527598B2|1993-08-13|2004-03-24|Blood flow monitor with venous and arterial sensors|
    US12/380,623| US7753854B2|1993-08-13|2009-03-02|Blood flow monitor with arterial and venous sensors|
    [返回顶部]