The present invention generally relates to a system, method and apparatus for detection of circulatory anomalies in the mammalian body. Important types of such anomalies involve the heart and include anomalies generally referred to as right-to-left cardiac shunts.
An anomaly commonly encountered in humans is an opening between chambers of the heart, particularly an opening between the left and right atria, i.e., an Atrial Septal Defect, creating a right-to-left atrial shunt, or between the left and right ventricles, i.e., a Ventricular Septal Defect (VSD), creating a right-to-left ventricular shunt. A right-to-left shunt may occur as a defect within the vasculature leading to and from the heart, for example a Pulmonary Arteriovenous Malformation (PAVM) may be present, reflecting a direct connection between the pulmonary vein and pulmonary artery. Alternatively, a right-to-left shunt may occur as a defect between great vessels. For example, a Patent Ductus Arteriosus may be present, allowing shunting between the aortic arch and the pulmonary artery.
Over 780,000 patients suffer strokes each year in the U.S. resulting in 250,000 stroke related deaths. The total cost associated with stroke was reported to be $66 billion in the U.S. in 2007 (Rosamond 2008). Of the patient population presenting with stroke or the early warning sign known as transient ischemic attack (TIA or mini stroke), as many as 260,000 are postulated to be the result of a right-to-left shunt in the heart and/or pulmonary vasculature, allowing paradoxical emboli.
The most common form of right-to-left shunt is a patent foramen ovale (PFO), which is an opening in the wall of the heart that separates the right side of the heart from the left side of the heart. The right side of the heart receives oxygen-depleted blood from the body and then pumps this blood into the lungs for oxygenation. The lungs not only oxygenate the blood, but also serve as a “filter” for any blood clots or other emboli, as well as to metabolize other agents that naturally reside within the venous blood. During the fetal stage of development, an opening naturally exists between the right and left atria of the heart to enable circulation of the mother's oxygenated blood throughout the vasculature of the fetus. This opening between the right and left side of the fetal heart (known as the foramen ovale) permanently seals shut in consequence of the closure of an overlying tissue flap in approximately 80% of the population within the first eighteen months following birth. The noted flap often remains in a sealing orientation because of a higher pressure at the left side of the heart. However, in the remaining approximate 20% of the population, this opening fails to permanently close and is referred to as a PFO.
Most of the population with a PFO never experience any symptoms or complications associated with the presence of a PFO, since many PFOs are small enough to remain effectively “closed”, or emboli may not form and travel to the right atrium, or they may not pass through a PFO even if it is present and open; thus the paradoxical nature of these emboli. However, for some subjects, this normally closed flap covering the foramen ovale temporarily opens, allowing blood to flow directly from the right side to the left side of the heart. As a consequence, any emboli such as blood clots or other active agents escaping through the PFO bypass the critical filtering functions of the lungs and flow through the temporary open (patent) foramen ovale and directly to the left side of the heart. Once in the left side of the heart, these emboli pass directly into the arterial circulatory system. Since a significant portion of the blood exiting the left side of the heart flows to the brain, any unfiltered blood clots or agents, such as serotonin, may be delivered to the brain. The presence of these now cerebral emboli in the brain arterial flow can produce debilitating and life-threatening consequences. These consequences are known to include stroke, heart attack and are also believed to be one of the causes of certain forms of severe migraine headaches. For further background on circulatory anomalies, see:
A relatively large number of patients (approximately three million) have had or may be undergoing sclerotherapy, treating, for instance, varicose veins. This therapy involves an injection of sclerosing solution that in effect creates emboli. If patients undergoing sclerotherapy are among the portion of the population with a PFO, creation of emboli that may bypass the filtering aspect of the lungs creates a significant risk of initiating a TIA, stroke or heart attack. This risk could be avoided by effectively and efficiently screening for a right-to-left shunt and administering appropriate therapy.
Based on the growing clinical evidence linking strokes, transient ischemic attacks (TIAs) and migraine headaches to right-to-left shunts, at least 16 companies have now entered the field of transcatheter shunt treatment devices for closure of the most common form, viz., a PFO, and certain of these devices are approved for sale in one or more principalities.
Percutaneous shunt closure devices are expected to soon be widely available in the U.S. for PFO closure, and approximately 20% of the adult population is estimated to have a congenital PFO. Unfortunately, there is currently no available method suitable for widespread screening for the presence of a PFO when the patient experiences early warning signs signaling an ischemic incident, or the patient exhibits or is exposed to an elevated risk of a stroke. Consequently, the “at risk” fraction of the population with a right-to-left shunt is most often resigned to the possibility of experiencing a stroke before definitive right-to-left shunt testing is performed. Only then are methods such as transesophageal echocardiography (TEE) performed to detect the presence of a right-to-left shunt. If detected, the patient may elect to be treated with anti-clotting agents or elect to undergo transcatheter right-to-left shunt closure or the more conventional open-heart procedure for right-to-left shunt closure.
TEE in conjunction with the injection of agitated saline contrast “bubbles” is used somewhat as a last resort. While the so-called TEE “bubble study” has not been reviewed by the U.S. Food and Drug Administration and so is performed “off-label”, it is still considered the “gold standard” for determining the presence of a right-to-left cardiac shunt. In carrying out this test, microbubble contrasts, produced by the agitation of a saline solution, is injected into a vein leading to the right side of the heart. As this is underway, the somewhat sedated patient is required to bear down with their abdominal muscles (as during defecation) to perform a “Valsalva” maneuver, the release of which will momentarily reverse the pressure differential between the right and left atria and cause a PFO, if present, to open, while an ultrasound transducer, positioned in the esophagus at the level of the heart, is used to record the passage of the microbubbles across the shunt into the left atrium. Because of gagging problems, the patient is partially anesthetized. Typically, patients experience discomfort and the test is hardly suited for screening. The TEE test is also expensive, with an equipment total cost of between $75,000 and $322,000. It additionally requires a physician with a specialized two year fellowship and an anesthesiologist or anesthetist, along with several nurses to assist with operation of the equipment.
A related test is referred to as transthoracic echocardiography (TTE). Again, a microbubble contrast is injected into a vein leading to the right side of the heart. Since the ultrasound detector is positioned externally over the chest wall in a TTE, the Valsalva maneuver for this procedure is performed by having the patient blow forcefully into a small tube, sometimes connected to a manometer, while ultrasonic echocardiograms are made through the chest wall. The TTE procedure also requires the use of expensive equipment and exhibits relatively poor sensitivity, by some reports as low as 60%.
A third test, incorporating transcranial Doppler (TCD) technology, also uses microbubbles as a contrast agent along with the Valsalva maneuver. Here, however, ultrasonic sensors located bilaterally on the skull are used to measure embolic signals produced by any microbubbles transiting the mid cerebral artery. This TCD method exhibits a relatively high sensitivity when it can be used. Unfortunately, approximately 20% of the population has a cranial bone that is too thick for sonic transducing to “see” the mid-cerebral artery, and equipment costs range between approximately $30,000 to $45,000. U.S. Patent Publication US2006/0264759 describes such systems and methods for grading microemboli in blood associated with ultrasound contrast agenda (e.g., small air bubbles) within targeted vessels by using Doppler Ultrasound system.
Additional description of existing methods of analyzing circulation and detecting certain circulatory anomalies are present in the following:
A continuing difficulty with existing methods is the efficacy of using microbubble contrasts as a circulatory tracking indicator. Microbubbles are created just prior to use, are a transient structure, and decidedly non-uniform in creation and application. It is difficult if not impossible for microbubbles to be used for quantitative measurements, and thus clinicians are forced to rely on a simple binary positive or negative result assessment. In part, the inability to effectively quantify the conductance of a shunt is revealed in the relatively low sensitivity of the existing methods.
A further problem with existing methods is the difficulty in effectively detecting the circulatory tracking indicator in the form of microbubbles. Each of the existing methods, including the TEE, TTE and TCD methods, suffer from barriers for routine use for screening, whether due to the need for anesthesia or expensive equipment. There is a need for more efficient circulatory tracking reagents, i.e. a reagent that can be reproducibly introduced into the circulatory system, be quantitatively detectable, and utilize relatively straightforward detection systems that are easily tolerated by patients.
One difficulty with improving the present technology in circulatory tracking reagents is that there heretofore has been no animal model available for screening a variety of different circulatory tracking reagents and their compatible detection systems.
There exists a growing body of clinical evidence linking the presence of right-to-left shunts to the risk of embolic strokes and occurrence of migraine headaches. In spite of this evidence, there remains a significant unmet need for a high sensitivity, low-cost and non-invasive method to screen those patients at increased risk of stroke in order to detect PFOs or other circulatory anomalies. The ability to screen at-risk patients is a critically unmet need, since shunt-related strokes can only be prevented if the presence of the shunt is detected and closed, or the patient receives anti-clotting therapy, in advance of the occurrence of a stroke. In addition, there is likewise a significant unmet need for a highly sensitive, quantitative low-cost method for evaluating the effectiveness and durability of the shunt closure at three to four time points following the percutaneous closure of the right-to-left shunt. This follow-up testing following shunt closure continues to be essential for the effective titration of the medical therapy administered prior to closure, and for assuring adequacy of the “seal” closing a PFO or other shunt, in order to minimize the risk of future shunt-related strokes.
The present application is directed to systems, methods and apparatus for detecting and quantifying right-to-left cardiac shunts and/or pulmonary shunts. The preferred indicator, which is employed, is indocyanine green dye (ICG) that will fluoresce when exposed to an appropriate wavelength of higher energy light, for example, a laser in the red region. The procedure is under the control of a controller/monitor having a visual display and being capable of providing cues to both the operator and the patient.
A venous access catheter is employed in connection with a peripheral vein such as the antecubital vein in an arm. This delivery system utilizes a unique resistance feedback-controlled heater-type fluid sensor to control injection times for both the indicator and a predetermined volume of isotonic saline used to “flush” flow sensor extension tubing, the venous catheter and peripheral vein so that all injected indicator is promptly delivered to the right atrium of the heart.
Sensing of the indicator concentration takes place at an arterial vasculature, for example, the pinna or fossa/scapha of the human ear. Additionally, heart rate may be monitored.
Embodiments of a system may use one or more optical sensors that are positioned along a patient's skin for transcutaneously analyzing the arterial vasculature therein. These optical sensors may include a plurality of laser/photodetector pairs, such as an array of three laser/photodetector pairs, which are directed to the arterial vasculature underlying the skin of the patient at the selected location. As mentioned above, this location may be the fossa/scapha or other portion of the ear pinna, or another location where relatively thin tissue contains an arterial blood network.
Where a test is to be carried out with a Valsalva maneuver, the mouthpiece of a manometer tubing set or of a Valsalva maneuver pressure sensing unit is positioned in the mouth of the patient and connected to a pressure transducer in the controller/monitor. The patient then performs a Valsalva maneuver by exhaling into the mouthpiece to produce some threshold exhalation pressure for some required period of time.
A visual readout of instantaneous exhalation pressure is made available both to the operator and the patient as well as the threshold level of pressure which must be achieved and maintained in order to successfully carry out the Valsalva maneuver. Alarms and visual error messages are introduced where the Valsalva maneuver is not carried out properly. The controller/monitor preferably instructs the operator with an audible cue to inject indicator and immediately inject isotonic saline flush. These are generally carried out with two syringes working in conjunction with a three-way valve. If the injection interval is not appropriate, again an audible alarm and error message may be provided to the operator. For the relief of the patient, an audible cue is also given when the Valsalva maneuver can be stopped (released).
The controller/monitor then calculates average heart rate and cardiac output, using that average heart rate, calculated body surface area, and a known normal value for stroke index of the heart. The system then calculates an area under a normal indicator/dilution curve associated with indicator and blood flow through a normal pathway in the lungs. Additionally, the controller/monitor calculates the area under any premature indicator dilution curve which will be associated with a right-to-left shunt. The controller/monitor further corrects the main indicator/dilution curve for a recirculation phenomenon and quantifies any right-to-left shunt by calculating the conductance associated with such shunts.
Other aspects and features of the invention will become apparent to those skilled in the art upon review of the following detailed description of exemplary embodiments along with the accompanying drawing figures.
In the following descriptions of the drawings and associated exemplary embodiments, like reference numerals across several views refer to identical or equivalent features, and:
When a right-to-left shunt is present in the heart or the pulmonary circulation of the human body, a system with two or more alternative blood flow pathways effectively exists. As described above, the most common form of right-to-left shunt in the heart is known as a PFO. During the fetal stage of development, an opening naturally exists between the right and left side of the heart to enable circulation of the mothers oxygenated blood throughout the vasculature of the fetus. This opening between the right and left side of the fetus' heart (known as the Foramen Ovale) permanently seals shut in about 80% of the population within the first eighteen months following birth. This opening fails to permanently close in the remaining about 20% of the population.
For some individuals, the normally closed overlying tissue flap covering the Foramen Ovale temporarily opens allowing blood to flow directly from the right side to the left side of the heart. As a consequence, any emboli such as blood clots or other metabolically active agents bypass the critical filtering/metabolic functions of the lungs and flow through the temporarily open Foramen Ovale directly to the left side of the heart. Once in the left side of the heart, these emboli pass directly into the circulatory system. Since a portion of the blood exiting the left side of the heart flows to the brain as well as the coronary arteries of the heart, any unfiltered blood clots or agents can produce debilitating and life-threatening consequences. These consequences are known to include stroke, heart attack and are also now believed to be one of the principal causes of certain forms of severe migraine headaches.
For further discussion, see the following publications:
When a right-to-left shunt is present in the heart or the pulmonary circulation of the human body, a system with two or more alternative blood flow pathways effectively exists. As described above, the most common form of right-to-left shunt in the heart is known as a PFO. During the fetal stage of development, an opening naturally exists between the right and left side of the heart to enable circulation of the mothers oxygenated blood throughout the vasculature of the fetus. This opening between the right and left side of the fetus' heart (known as the Foramen Ovale) permanently seals shut in about 80% of the population within the first eighteen months following birth. This opening fails to permanently close in the remaining about 20% of the population.
For some individuals, the normally closed overlying tissue flap covering the Foramen Ovale temporarily opens allowing blood to flow directly from the right side to the left side of the heart. As a consequence, any emboli such as blood clots or other metabolically active agents bypass the critical filtering/metabolic functions of the lungs and flow through the temporarily open Foramen Ovale directly to the left side of the heart. Once in the left side of the heart, these emboli pass directly into the circulatory system. Since a portion of the blood exiting the left side of the heart flows to the brain as well as the coronary arteries of the heart, any unfiltered blood clots or agents can produce debilitating and life-threatening consequences. These consequences are known to include stroke, heart attack and are also now believed to be one of the principal causes of certain forms of severe migraine headaches.
For further discussion, see the following publications:
Embodiments of a method, apparatus, and system are described herein for effectively monitoring subject patients for circulatory anomalies. These methods, apparatus, and systems are useful for determining the magnitude of the flow rate associated with a right-to-left cardiac shunt and/or within the pulmonary vasculature, for instance.
In a preferred embodiment, a non-invasive optical sensor is positioned on the surface of the subject's skin at a location (e.g., the auricle of the ear). A biocompatible indicator is next injected at a predetermined rate into a peripheral (e.g., antecubital) vein of the subject while the subject may be directed to engage in a breathing maneuver (i.e., a Valsalva maneuver), such as by exhaling into a manometer mouthpiece. A pressure differential may be thus produced that is effective for causing the opening of a PFO, for instance, allowing blood to flow across a right-to-left cardiac shunt. The non-invasive optical sensor is used to transcutaneously measure the concentration of the injected indicator as a function of time. As seen below in connection with FIG. 10, if a premature inflection or peak occurs in the indicator concentration level at a point in time t1 that is prior to the rise and fall of the concentration associated with the majority of the indicator flowing through the normal pathway of the lungs and arriving at the sensor at a point in time t2, then a right-to-left cardiac shunt (PFO). As described herein, exemplary systems, apparatus and methods provide for calculating and quantifying the extent of circulatory anomalies in a manner superior to any other systems, apparatus and methods available, and are capable of providing diagnostics effective for determining the appropriate clinical treatment of circulatory anomalies.
In the discourse to follow research activities are somewhat tracked as the invention developed. In this regard, bench tests are described looking to basic studies that lead to subsequent animal (pig) tests. Fundamentals of measuring cardiac output led to the evolution of a method and system wherein right-to-left cardiac shunts could not only be detected but also quantified.
Effective utilization of the system requires an indicator, i.e., a circulatory tracking reagent, or an analyte capable of passing through the lungs, and which provides information with respect to the left atrium of the heart. Previous systems for detecting PFOs, which relied on ultrasonic detection of microbubbles, are almost completely incapable of providing information on the size of as PFO, and require semi-invasive detection methods such as trans-esophageal ultrasound. The inventors had earlier studied techniques for monitoring total circulating blood volume and cardiac output as described at U.S. Pat. No. 6,299,583 by Eggers, et al., issued Oct. 9, 2001, and incorporated herein by reference.
Referring initially to
As illustrated in
The present disclosure describes exemplary embodiments of a system and method for detecting and quantifying atypical or abnormal blood flow, particularly left to right atrial shunts, and other arterial-venous malformations and disruptions in typical blood circulation. The method relies on effectively quantifying the relative blood flow or blood flow volume passing through normal and aberrant pathways. One example of such aberrant pathways are openings, or shunts between the right and left atria.
In order to provide for effective quantification of shunts between arterial and venous blood flow, an indicator (circulatory tracking reagent) is used. It was initially determined that a high degree of sensitivity would be achieved in screening capabilities for detecting atypical blood flow through the utilization of a fluorescing moiety as an indicator in a cardiac output (CO) emulating system. Accordingly, fluorescing dyes were examined and, in particular, fluorescing dyes which have been approved for use in humans. Two such exemplary dyes were available, fluorescein and indocyanine green dye (ICG).
As discussed further below, a number of additional circulatory tracking reagents are available for use with the system, including such indicators as spectrophotometric, densitometric and radiometric indicators. A variety of previous efforts to utilize circulatory tracking indicators is disclosed in, for example: U.S. Pat. No. 3,412,728, which describes a method and apparatus for monitoring blood pressure, utilizing an ear oximeter clamped to the ear to measure blood oxygen saturation using photo cells which respond to red and infrared light; U.S. Pat. No. 3,628,525, which describes an apparatus for transmitting light through body tissue for purposes of measuring blood oxygen level; U.S. Pat. No. 4,006,015, which describes a method and apparatus for measuring oxygen saturation by transmission of light through tissue of the ear or forehead; and U.S. Pat. No. 4,417,588, which describes a method and apparatus for measuring cardiac output using injection of indicator at a known volume and temperature and monitoring temperature of blood downstream. This and similar art suffer from an inability to effectively quantify the magnitude (i.e., functional conductance) of shunts, in part because of the failure and or inability to effectively quantify cardiac output.
A number of existing patents also describe potential reagent systems that if adapted, could be utilized with present systems, methods and apparatus. For example, U.S. Pat. No. 4,805,623 describes a spectrophotometric method used for quantitatively determining concentration of a dilute component in an environment (e.g., blood) containing the dilute component where the dilute component selected from group including corporeal tissue, tissue components, enzymes, metabolites, substrates, waste products, poisons, glucose, hemoglobin, oxy-hemoglobin, cytochrome. The corporeal environment described includes the head, fingers, hands, toes, feet and earlobes. Electromagnetic radiation is utilized including infrared radiation having a wavelength in the range of 700 to 1,400 nanometers. U.S. Pat. No. 6,526,309 describes an optical method and system for transcranial in vivo examination of brain tissue (e.g., for purpose of detecting bleeding in the brain and changes in intracranial pressure), including the use of a contrast agent to create image data of the examined brain tissue.
Detailed examination of the desirable properties of fluorescein and ICG dye demonstrate how other indicators can be applied to present systems and methods. Notably, these fluorescing dyes are excited by one wavelength of electromagnetic radiation, and emit a detectable signal at a second wavelength. Looking to
Looking to the ICG dye spectrum, an excitation curve is shown at 34, having a peak excitation wavelength at about 785 nanometers. Correspondingly, the fluorescence emission from excitation at curve 34 is represented at curve 36 with a peak emission wavelength of about 830 nanometers. Directed across
Turning again to the ICG dye spectrum, note that the excitation signal 34 for ICG intersects curve 38 at a depth allowing for readily reaching blood vessels, for example within the pinna (e.g., scaphoid fossa) of the ear. Accordingly, ICG dye is usable as a circulatory tracking agent when detecting through skin, and ICG dye was the indicator elected for subsequent study.
To utilize this fluorescing form of indicator in carrying out cardiac output related procedures, a sensor or probe apparatus having the capability to direct laser excitation illumination to a blood vessel as well as to collect and filter an emitted fluorescent response (i.e., a sensor having both excitation and detection components) was developed utilizing fiber optic technology. Looking to
When an ICG indicator within the bloodstream reaches the site of irradiation with 785 nm (laser) light, the fluorescent moiety within the ICG indicator is excited as described in connection with
It is important that the interface between this interferential filter and the fiber optic sensor be accurately aligned. With alignment at a preferred angle of about 7 degrees, the filter will reflect unwanted wavelengths. Angles of photon incidence of greater than about 45 must be avoided since interferential filters will become ineffective.
Looking to
In the course of investigation, a variety of bench top jigs or the like were developed. One such arrangement is revealed in
A collected fluorescence output is directed from splice 64 via glass fiber 66 to an interferential filter passing generally 830 nanometers and represented at block 68. Filter 68 was provided as a model No. 679-3230 marketed by OptoSigma, Inc. As represented by line 70, filter 68 is connected such that it operatively cooperates with a photomultiplier tube 72. Tube 72 was provided as a model No. H7712-10 marketed by Hamanatsu, Inc.
During initial testing, signals from photomultiplier tube 72 were directed as represented at arrows 74-76 to a phase one digital oscilloscope provided as a model No. DT03054 marketed by Techtronics, Inc. At a later time, such signals would be further directed as represented at arrows 79 and 80 to a phase 2 controller/monitor 82, comprising a controller/data acquisition system discussed later herein.
The transmitting and receiving end of sensor 58 performed in conjunction with a sealed glass capillary cylinder sample tube, e.g., 84, carrying ICG fluorescing dye of given concentrations. In general, such tubes as at 84 have an inside diameter of 1-2 milliliters. To simulate performance transcutaneously, the tube 84 is positioned just below the surface of a human skin phantom material represented at 86. For many of the tests, sensor 58 was moved along tube 84 or transversely across a plurality of tubes of varying ICG dye concentrations as represented by the motion arrow 88. The movement was imparted through a DC motor driven apparatus.
As shown in
Bench top testing also evolved the information set out at curve 90 in
As the investigation continued, the ability to simply and quickly screen patients for right-to-left cardiac shunts was envisioned. Referring to
A patient being screened is shown at 100 sitting on a chair 102. A nurse or clinician is shown at 104 administering the test under cueing guidance from the logic within controller/monitor 82. Patient 100 is shown exhaling or blowing into a mouth-piece 106 which, in turn, extends via a delivery tube 108 to a manometer within the controller/monitor 82. Thus, the hemodynamic testing according to present systems and methods may employ a “Valsalva manuever,” wherein the patient 100 blows into mouth-piece 106, creating backpressure within the lungs of the patient.
As mentioned previously, the Valsalva maneuver, by inducing a positive pressure difference between the right and left side of the heart, simulates conditions under which transient cardiac shunts (e.g., right-to-left atrial shunts such as a PFO) tend to open and allow a cross-flow of blood between the arterial and venous blood circulation. As maintenance of lung back-pressure is preferable for effectively identifying shunts, controller/monitor 82 may terminate the test during the Valsalva maneuver if pressure is seen to drop below 40 mm of mercury for some period of time.
A small sensor 110 is shown attached to the ear of patient 100. Sensor 110, in a preferred embodiment, incorporates three paired laser excitation components (emitters) and filtered fluorescence pick up (detector) components. These are polled to find the strongest output signal of fluorescence, such control being provided by the cable 112 operating in conjunction with the controller/monitor 82. The sensor 110 is preferably positioned on the surface of the ear pinna, such as along the scaphoid fossa region thereof. Additionally, during a period of about 60 seconds following the injection of the indicator, the heart rate of patient 100 is monitored using a conventional non-invasive heart rate monitor such as that marketed by Nellcor Pulse Oximeter, Inc. of Boulder Colo. The heart rate monitor is shown at 114 operatively associated with the controller/monitor 82 as represented at cable 116.
In
The test at hand is temporal in nature, thus proper timing of each aspect of the test is quite important. Accordingly, the controller/monitor 82 both monitors and cues each step in the process. In this regard, the controller/monitor 82 may provide patient 100 with visual feedback that helps the patient regulate his/her exhalation pressure level and may also time the Valsalva maneuver. The Valsalva maneuver should last about 15 seconds, and may be represented as a bar on the display 98 of the controller/monitor 82.
At a cued time provided by the controller/monitor 82, injection of the indicator bolus (e.g., 2 ml of 2.5 mg/ml) ICG dye over about a period of one second is performed by the nurse or clinician 144, followed immediately by the injection of a clearing bolus of isotonic saline (e.g., 5 ml injected over a period of 2 seconds). The rapid injection of the indicator bolus and the clearing bolus is carried out to assure that all of the injected indicator is rapidly transported from the injection site to the right atrium of the heart. If the indicator and isotonic saline are not injected within a predefined period, for example, 5 seconds before the end of the Valsalva maneuver, then a warning may be provided by the controller/monitor 82.
Once the injection of the indicator bolus and isotonic saline clearing bolus have been successfully completed in the prescribed time period, the sensor 110 detects the relative concentration of the ICG indicator as it passes through the vasculature of the ear. Digital filtering of the output signal from the fluorescence detectors of the sensor 110 is performed using, for example, Finite Impulse Response Digital Filtering (see Lyons, R. G., “Understanding digital signal processing”, Addison-Wellsley Publishing Company, Reading, Mass. 1997:157-204). The controller/monitor 82 tracks the passage of the indicator bolus from the peripheral vein where injected, through the right atrium and pulmonary circuit to the left atrium and ventricle and subsequent passage to the arterial blood. If any part of the indicator bolus diverges from the typical blood flow pathway, for instance via a right-to-left cardiac shunt, then the system is designed to detect and quantify such aberrations. For instance, if a premature increase in the indicator concentration occurs prior to the main indicator/dilution curve that is associated with that much larger portion of the injected indicator which takes the longer and more time consuming pathway through the lungs, then the premature increase indicates the presence of a right-to-left cardiac shunt.
In contrast to typical mammalian cardiovascular flow systems involving a single flow pathway between the injection site and the exit of the heart, a method for calculating the total flow rate of a system involving two or more individual flow pathways is described below. These abnormal cardiovascular flow systems comprise two or more indicator/dilution curves corresponding to two or more flow pathways determined at two or more physical locations corresponding to two or more separate pathways. The areas under (1) the premature smaller indication/dilution curve and (2) the much larger indicator/dilution curve can be used to ratiometrically quantify the magnitude of the right-to-left cardiac shunt.
This indicator bolus premature arrival and the delay by traveling through the lungs can be represented schematically. Looking to
One conduit of the conduit array 158 is depicted at 160 as being analyzed by the sensor 110 and controller/monitor 82, as collectively represented in
Looking momentarily to
It is also possible for the pulmonary system to exhibit both a PFO and a pulmonary arterial venous malformation (PAVM). The ability to distinguish between a PFO and a PAVM is valuable, since the closure device and method for remediating these two types of shunts is distinctly different. Referring to
The lungs are represented at dashed boundary 198. Note that venous blood is shown to extend along introductory conduit 200 while filtered blood returns from the lungs to the left side of the heart as represented at conduit 202. Note, however, that in this case a second right-to-left shunt, as represented by conduit 204, exists within the pulmonary system. Conduit 204 may, for example, also represent a PAVM from the blood stream arterial conduit array 196.
Another conduit is shown extending from arterial array 196 at 206. Indicator within a conduit as at 206 is subjected to excitation illumination and responds to resultant fluorescence as represented at arrow 206 and 208 and display 210. Display 210 shows a recirculation corrected principal dye dilution curve 212, a dye dilution curve 214 representing the cardiac shunt at conduit 192 and a later occurring dye dilution curve 216 representing the pulmonary shunt described in connection with conduit 204.
Referring now to
Method for Estimating Cardiac Output Using Indicator/Dilution Method
The indicator-dilution method for measuring Cardiac Output was originally developed by Hamilton during the 1920's for use with dyes as the indicator. This work by Hamilton was based on earlier work by Stewart in 1897 and led to the following equation for calculation of the Cardiac Output of the heart, COt:
where
D is the amount of indicator (e.g., grams);
C(t) is the measured concentration of the indicator at any time t (e.g., grams/ml); and
∫0tmC(t)dt represents the area under the concentration vs. time curve as seen in
An exemplary indicator/dilution curve is illustrated in
An exemplary measured indicator/dilution curve for an adult pig is shown in
As the ICG indicator within the blood stream reaches the site of irradiation with 785 nm light, the fluorescent component within the ICG indicator is excited to an elevated energy state for a brief period. As the excited component returns to its normal energy state, it emits light at a longer wavelength (viz., 830 nm). As previously disclosed, the (nominally 45 nm) difference between the excitation wavelength (viz., 785 nm) and the fluorescence emission wavelength (viz., 830 nm) is known as the Stokes Shift, and it allows the fluorescence emission to be extracted by using an interferential or other type of optical filter to reflect or otherwise attenuate all but the wavelength band of interest (viz., 820 to 840 nm). The fluorescence emissions collected in this example by seven 600 micron diameter optical fibers surrounding the excitation fiber (see
In addition to optical filtering, Fast Fourier Transform filtering methods or Finite Impulse Response (nonrecursive) filtering methods can be used to remove spectral content from the measured fluorescence signal that is outside the frequency band of interest. In the present example, the digital filtering of the fluorescence signal serves as a “low pass” filter allowing only signals with a frequency component in the range from 0 to 0.8 Hz to be included in the digitally filtered form of the measured data.
Referring again to
For further discussion of measuring cardiac output and calculating the area under the dye dilution curve, see:
Utilizing the presently derived method, the area A under the indicator/dilution curve with the recirculation component removed can be calculated as follows:
A=Y
m
*a*c (Eq. 2)
where
A=area under indicator/dilution curve without recirculation component (millivolt-seconds);
Ym=maximum signal amplitude (millivolts);
a=width of indicator/dilution curve to right of time, tm at Y=0.607*Ym (seconds); and
c=constant value=2.20.
As seen in
Another method which can be used to estimate the shape of the down slope curve without the recirculation component involves the use of least mean squares regression for the exponential curve fit to obtain the coefficient, a in the equation.
Y=Y
2
e
−∝(t-t2) (Eq. 3)
where
Y is the signal amplitude at time, t (millivolts);
Y2 is the signal amplitude at time, t2 (millivolts);
t−t2 is the elapsed time following time t2 (seconds);
α is the exponential coefficient which defines the signal amplitude down-slope curve and is derived by an exponential curve fit to the actual measured signal amplitude values in time interval between t1 and t2;
t1 is the time at which Y1=*Ym;
t2 is the time at which Y2=F2*Ym; and
F1 and F2=0.9 and 0.6, respectively.
Referring again to Eq. 1, note that the integral in the denominator of the expression for Cardiac Output, COt is in terms of a concentration value, C(t) and it is in the same unit as the amount of the indicator injected D. By way of example, the amount of indicator injected D is in units of micrograms and the concentration of the indicator C(t) is in units of microgram/milliliter or microgram/ml. However, the presently disclosed non-invasive method for measuring the Shunt Conductance, C involves the measurement of a relative concentration value which, by way of example, is in unit of millivolts. Therefore, Eq. 1 can be rewritten in terms of measurement of a signal amplitude, V(t) as a function of time to obtain a volumetric flow rate as follows:
where
COt=volumetric flow rate (milliliter/second);
D=amount of indicator injected (micrograms);
V(t)=measured signal level as a function of time which is directly proportional to the concentration of the indicator in the blood stream (millivolts); and
CCF=indicator concentration conversion factor used to convert measured signal level (in millivolts) into indicator concentration (micrograms/ml) and which has the unit (micrograms/ml-millivolt).
The indicator concentration conversion factor, CCF is a constant value for a specific set of transcutaneous measurement fluorescence measurement parameters which include (1) excitation light intensity (e.g., laser power in units of milliwatts), (2) thickness of skin between surface of light source/fluorescence detector and blood vessel(s) carrying blood-borne indicator, (3) quantum efficiency of the fluorescing indicator or indicators (4) light scattering characteristics of the skin and skin type, (5) amplifier gain in fluorescence detection circuit, and (6) attenuation of fluorescence light flux through optical filtering component(s).
As discussed above related to the calculation of Cardiac Output using indicator/dilution methods, the integral term corresponds to the area under the curve defined by the measured signal level as a function of time. Also, as seen before in
The new method described is useful for detecting the presence of a right-to-left cardiac shunt as has been shown in
The calculation of the volumetric flow rate in Equations 1, 4 and 5 corresponds to a mammalian circulatory system in which there is only one pathway for the flow of liquid (e.g., blood) and injected indicator from the site of indicator injection (e.g., peripheral vein) to the ascending aorta exiting the left ventricle of the heart. Alternatively, two or more indicator/dilution curves result if there are two or more flow pathways having different transit times within the system which then converge at a single measurement site at a location downstream from the two or more pathways. By way of example, such a system with two pathways in which pathway 146 has a shorter transit time δ1 and pathway 152-154 has a longer transit time δ2 is shown in
As illustrated in
As seen in this hypothetical flow system illustrated in
where
COt=volumetric flow rate (e.g., milliliter/second);
D=amount of indicator injected (e.g. micrograms);
CCF=indicator concentration conversion factor to convert measured signal level (e.g. millivolts) into indicator concentration (e.g., micrograms/ml-millivolts);
At=total area under one or more indicator/dilution curves corresponding to one or more pathways for the flow of liquid in the system (e.g., millivolts-seconds);
A1=area under the indicator/dilution curve 165 for flow pathway 146 (e.g., millivolt-second); and
A2=area under the indicator/dilution curve 166 for flow pathway 152-154 (e.g., millivolt-second).
As illustrated in
where
CO1=volumetric flow rate in pathway 146 (e.g., milliliter/second);
Cot=total volumetric flow rate for both pathways 146 and 154 (e.g., milliliter/second);
A1=area under the indicator/dilution curve 165 for flow through pathway 146 (e.g., millivolt-second); and
A2=area under the indicator/dilution curve 166 for flow through pathway 152-154 (e.g., millivolt-second).
For the case of equal volumetric flow rates in pathways 146 and 152-154, the areas under the curves A1 and A2 will be equal. In this exemplary case, Eq. 7 can be written as follows (where A1=A2):
Alternatively, if the volumetric flow rate at pathway 146 is only one-tenth of the flow rate through pathway 154, then A2=10*A1 and Eq. 7 can be written in this exemplary case as follows (where A2=10*A1):
As illustrated in
where
COt=volumetric flow rate (e.g., milliliter/second);
D=amount of indicator injected (e.g. micrograms);
CCF=indicator concentration conversion factor to convert measured signal level (e.g. millivolts) into indicator concentration (e.g., micrograms/ml-millivolts);
At=total area under one or more indicator/dilution curves corresponding to one or more pathways for the flow of liquid in the system (e.g., millivolts-seconds);
A1=area under the indicator/dilution curve for flow pathway 192, curve 214 (e.g., millivolt-second);
A2=area under the indicator/dilution curve for flow pathway 204, curve 216, (e.g., millivolt-second); and
A3=area under the indicator/dilution for the primary pathway 200-202 through the lungs, curve 212 (e.g., millivolt-second).
As illustrated in
where
CO1=volumetric flow rate in pathway 1 (e.g., milliliter/second);
Cot=total volumetric flow rate for both pathways 1 and 2 (e.g., milliliter/second);
A1=area under the indicator/dilution curve for flow through pathway 192 (e.g., millivolt-second);
A2=area under the indicator/dilution curve for flow through pathway 204 (e.g., millivolt-second); and
A3=area under the indicator/dilution curve for flow through the main pathway 200-202 through lungs (e.g., millivolt-second).
For the case of equal volumetric flow rates in the three pathways, the areas under the curves A1, A2 and A3 will be equal based on the principles of the Steward-Hamilton equation for indicator/dilution based flow rate measurement as discussed with regard to Equations 4 and 5. Hence, Equation 11 can be written in this exemplary case as follows (where A1=A2=A3):
For the case of a flow system with two flow pathways the flow rate in any single pathway COi is giving by the general relationship:
where
COi=volumetric flow rate in pathway i (e.g., milliliter/second);
Cot=total volumetric flow rate for both pathways 1 and 2 (e.g., milliliter/second);
Ai=area under the indicator/dilution curve for flow through pathway i (e.g., millivolt-second);
A1=area under the indicator/dilution curve for flow through pathway 192 (e.g., millivolt-second);
A2=area under the indicator/dilution curve for flow through pathway 204 (e.g., millivolt-second); and
I=pathways 192 or 204.
For the case of a flow system with three flow pathways as illustrated in
where
COi=volumetric flow rate in pathway i (e.g., milliliter/second);
COt=total volumetric flow rate for all pathways (e.g., milliliter/second);
Ai=area under the indicator/dilution curve for flow through pathway i (e.g., millivolt-second);
A1=area under the indicator/dilution curve for flow through pathway 192 (e.g., millivolt-second);
A2=area under the indicator/dilution curve for flow through pathway 204 (e.g., millivolt-second);
A3=area under the principal indicator/dilution (e.g., millivolt-second); and
i=one of the three pathways.
The case of a flow system with two flow pathways exists in the human body when a right-to-left cardiac shunt or pulmonary is present. As described above, the most common form of a right-to-left cardiac shunt is known as a PFO.
Exemplary methods, apparatus and systems capable of determining the magnitude of the flow rate associated with a right-to-left cardiac or pulmonary shunt are hereafter disclosed. As previously described, a non-invasive optical sensor is initially positioned on the surface of a subject's skin at a location (e.g., the scaphoid fossa of the ear). A biocompatible indicator is next injected at a predetermined rate into a peripheral (e.g., antecubital) vein of the subject while the subject is directed to engage in a Valsalva maneuver that may result in the opening of a PFO and a flow of blood directly from the right atrium to the left atrium of the heart without passing through the longer pathway in the lungs.
The non-invasive optical sensor transcutaneously measures the concentration of the injected indicator as a function of time. As seen in
The situation in the human body where only one right-to-left shunt exists is illustrated schematically in
Still referring to
In the cases where there are either one or two right-to-left shunts, a much larger indicator/dilution curve also occurs and is associated with that amount of blood which normally flows through the much longer pathway in the lungs and back to the left atrium of the heart. This larger indicator/dilution curve is seen in
For the case of a human subject with a single right-to-left cardiac shunt as seen in
where the terms are the same as those defined for Equations 7 and 13.
Likewise, for the case of a human subject with two right-to-left shunts detected as seen in
where the terms are the same as those defined for Eq. 14.
As seen in Equations 15, 16 and 17, the areas A1, A2 and A3 are calculated parameters based on the measurement of indicator concentration as a function of time for each of the indicator/dilution curves that corresponds to the presence of a single right-to-left shunt (see A1 in
As seen in Equation 7 and
For the case of an adult human, the normal value of the Stroke Index, SI is known to be 46±5 ml/m2 (see Shoemaker, W. C., et al., “Textbook of Critical Care,” W.B. Saunders Company, Philadelphia 1995: pg. 263). As seen in the Shoemaker reference, Stroke Index, SI is related to Cardiac Index, CI and heart rate, HR as follows:
where
SI=Stroke Index (ml/m2);
CI=Cardiac Index (ml/second-m2); and
HR=heart rate (beats per second) determined by measuring beats per minute and dividing by 60 seconds/minute.
As seen in the cited Shoemaker reference, the Cardiac Index CI is equal to the Cardiac Output CO divided by the Body Surface Area BSA as follows:
where
CI=Cardiac Index (ml/m2);
CO=Cardiac Output (ml/second); and
BSA=Body Surface Area (square meters or m2).
The Body Surface Area (BSA) can be calculated by one of several algorithms incorporating the height and weight of the human subject. One of the recommended algorithms used to calculate the Body Surface Area, BSA is the algorithm known as the Mosteller Formula (see Mosteller, R. D., “Simplified Calculation of Body Surface Area,” New England Journal of Medicine 1987; 17[17]: 1098). The Mosteller Formula for Body Surface Area is given by the following equation:
BSA=((H*W)/3131)1/2 (Eq. 20)
where
BSA=Body Surface Area (m2);
H=Height of subject (inches); and
W=Weight of subject (pounds).
The normal value of the Cardiac Output for a human subject can then be calculated by solving Equations 18 and 19 for Cardiac Output CO as follows. First, rewriting Equation 19 in terms of Cardiac Output CO obtains:
CO═CI*BSA (Eq. 21)
Rewriting Equation 18 in terms of Cardiac Index CI obtains:
CI═SI*HR (Eq. 22)
Substituting formula for Cardiac Index CI (Equation 22) into the formula for Cardiac Output CO in Equation 21 obtains:
CO−CI*BSA=SI*HR*BSA (Eq. 23)
where:
a. the normal value for SI is known to be 46±5 ml/m2;
b. HR is measured using a heart rate monitor and averaged over the period of the measurement of the relative concentration of the indicator during the period from the indicator injection to the time of the peak of the normal indicator/dilution curve associated with blood flow through the lungs and back to the left atrium of the heart (beats/second); and
c. BSA is calculated using Mosteller Formula given in Equation 20 in units of m2.
Hence, the normal value of the total Cardiac Output can be estimated within a narrow range based on the known normal value for Stroke Index SI (viz., 46±5 ml/m2), by measuring the subject's heart rate HR and calculating the Body Surface Area BSA based on the subject's height and weight. This estimated value for Cardiac Output, CO is equivalent to the total flow rate COt incorporated into Equations 7, 11, 13 and 14. By way of example and referring to Equation 7, Equation 23 and
where:
CO1=flow rate or Shunt Conductance through right-to-left shunt (ml/second);
SI=Stroke Index whose normal value is 46±5 ml/m2;
HR=Heart Rate which is measured using a heart rate monitor (beats/second);
BSA=Body Surface Area calculated using Mosteller Formula (m2);
A1=calculated area under measured indicator/dilution indicator concentration curve associated with right-to-left shunt as seen in
A2=calculated area under measured indicator/dilution indicator concentration curve associated with blood flow through the lungs and back to left atrium of the heart as seen in
Hence, Eq. 24 allows the equivalent flow rate or Shunt Conductance through a single right-to-left shunt to be calculated within a narrow range (based on normal range of Stroke Index of 46±5 ml/m2). Likewise, Equation 14 for the case of two co-existing right-to-left shunts can be re-written as follows:
where
CO1=flow rate or Shunt Conductance through a first right-to-left shunt (ml/second);
CO2=f low rate or Shunt Conductance through a second right-to-left shunt (ml/second);
SI=Stroke Index whose normal value is 46±5 ml/m2;
HR=Heart Rate which is measured using a heart rate monitor (beats/second);
BSA=Body Surface Area calculated using Mosteller Formula (m2);
A1=calculated area under a first measured indicator/dilution indicator concentration curve associated with right-to-left shunt (millivolt-second);
A2=calculated area under a second measured indicator/dilution indicator concentration curve associated with shunt flow through pulmonary arterial pathway (e.g., PAVM) and back to left atrium of the heart (millivolt-second); and
A3=calculated area under a third measured indicator/dilution indicator concentration curve associated with blood flow through lungs and back to left atrium of heart (millivolt-second).
As a result of the ratiometric approach specified in the present invention for calculating the flow rate or Shunt Conductance associated with one or two right-to-left shunts, several terms required for the calculation of the volumetric flow rate of a system are cancelled out and therefore do to have to be determined. Note that Eq. 6 for the case of calculating the flow rate in a system with two flow pathways includes the parameters for (a) the amount of the indicator injected D (e.g., grams) and (b) the factor for converting the measured signal level (in millivolts) into a concentration level CCF (e.g., grams/ml).
However, due to the ratiometric form of Equation 7 in the present invention, the terms D and CCF cancel out. Also, the units of measure for the fluorescence signal level (e.g., millivolts-seconds) cancel out. As a result, the exact amount of the indicator injected does not have to be accurately known. However, the amount of the indicator injected needs to be sufficiently large so that the much smaller indicator/dilution curves associated with one or two right-to-left shunts can be adequately resolved and their corresponding areas can be accurately calculated. In one embodiment of the present invention involving the use of ICG dye (supplied, for example, by Akorn, Inc., 2500 Millbrook Drive, Buffalo Grove, III. 60089) as the indicator, the preferred amount of ICG dye injected is 2.0 ml at an ICG dye concentration of 2.5 milligram/ml which is equivalent to an injected ICG dose of 5.0 milligrams. The chemical name for Indocyanine Green is 1H-benz(e)indolium, 2-[7-[1,3-dihydro-1,1-dimethyl-3-(4-sulfobutyl)-2H-benz[e]indo-2-ylidene]-1,3,5-heptatrienyl]-1,1-dimethyl-3-(4-sulfobutyl)-hydroxide, inner salt, sodium, or 2-[7-[1,1-dimethyl-3-(4-sulfobutyl)benz[e]indolin-2-ylidene]-1,3,5-heptatrienyl]-1,1-dimethyl-3-(4-sulfobutyl)-1H-benz[e]indolium hydroxide, inner salt, sodium salt.
A typical right-to-left shunt test procedure might involve a total of 3 to 5 tests which represents a total injected indicator dose of 15 to 25 milligrams. This cumulative dosage amount is well below the manufacturer's specified guideline which recommends a maximum ICG dose per day of 2 milligrams per kilogram of body weight. The recommended ICG dose for a human subject weighting 140 pounds or 63.6 kg is about 127 milligrams, a factor of 5 to 8.5 times higher than the amount of ICG dye required to perform multiple right-to-left shunt measurements on a single human subject weighing 140 pounds. This significant ratio of the actual to recommended dosage limit assures that method embodiments of the present invention can be safely employed.
This example involves the calculation of the flow rate or Shunt Conductance of a human subject with a single right-to-left shunt, as seen in
SI=Stroke Index for Normal Subject=46 ml/m2;
H=Height of subject=70 inches;
W=Weight of subject=160 pounds;
HR=measured average heart rate during period of measurement of indicator concentration as a function of time=1.0 beats/second (i.e., 60 beats/minute);
A1=calculated area under indicator/dilution curve derived from measured fluorescence signal level (in units of millivolts) vs. time (in seconds) associated with right-to-left shunt=40.5 millivolts-seconds; and
A2=calculated area under indicator/dilution curve derived from measured fluorescence signal level (in units of millivolts) vs. time (in seconds) associated with blood flow through lungs and back to left atrium of heart=3000 millivolts-seconds.
Using subject's actual height and weight, the Body Surface Area BSA is calculated using Eq. 20 as follows:
BSA=((H*W)/3131)1/2=((70 inches*160 pounds)/3131)1/2=1.89 m2 (Eq. 27)
Substituting the measured and calculated parameters A1, A2 and heart rate as well as the normal Stroke Index value into Equation 24 provides the calculated value for the flow rate or Shunt Conductance, CO1 as follows:
This example involves the calculation of the flow rate or Shunt Conductance of a human subject with two right-to-left shunts, as seen in
SI=Stroke Index for Normal Subject=46 ml/m2;
H=Height of subject=72 inches;
W=Weight of subject=185 pounds;
HR=measured average heart rate during period of measurement of indicator concentration as a function of time=1.2 beats/second (i.e., 60 beats/minute);
A1=calculated area under indicator/dilution curve derived from measured fluorescence signal level (in units of millivolts) vs. time (in seconds) associated with a first right-to-left shunt=45.0 millivolts-seconds;
A2=calculated area under indicator/dilution curve derived from measured fluorescence signal level (in units of millivolts) vs. time (in seconds) associated with right-to-left shunt=65.7 millivolts-seconds;
A3=calculated area under indicator/dilution curve derived from measured fluorescence signal level (in units of millivolts) vs. time (in seconds) associated with blood flow through lungs and back to left atrium of heart=3100 millivolts-seconds;
Using subject's actual height and weight, the Body Surface Area, BSA is calculated using Eq. 20 as follows:
BSA=((H*W)/3131)1/2=((72 inches*185 pounds)/3131)1/2=2.06 m2 (Eq. 28)
Substituting the measured and calculated parameters A1, A2, A3 and heart rate as well as the normal Stroke Index value into Equation 25 provides the calculated value for the flow rate or Shunt Conductance for the first right-to-left shunt CO1 as follows:
Likewise, substituting the measured, calculated and assumed normal Stroke Index into Eq. 26 provides the calculated value for the flow rate or Shunt Conductance for the second right-to-left shunt, CO2 as follows:
In regard to
Referring now to
Along the exemplary display 98 are touch screen positions as well as visual cueing indicators. Region 268 is pressed by the nurse or clinician to initialize the overall procedure. Block 270 provides a cue to properly position the sensor described at 110 in
Referring to
The injected circulatory tracking reagent indicator passes through the earlier described flow sensor 126 which is controllably heated to 30° C., plus or minus 2° C., using resistance feedback control of serpentine copper adhesive material supported on a polyamide substrate, which is sometimes referred to as a “copper-on-Kapton”. When an injection of a liquid at room temperature occurs, the cooling effect causes an immediate decrease in the temperature of the heater component. This sudden decrease in temperature is used by the controller/monitor sensing circuitry to detect the precise time at which the injection has been initiated. This allows the monitoring unit to determine if the injections of the indicator from syringe 120 and isotonic saline flush from syringe 122 are initiated within a predetermined time period after the start and before the end of the Valsalva maneuver or test initiation. Flow sensor 126 is removably connected to a multi-lead connector 264 which in turn, is connected to earlier described cable 128 that extends to the controller/monitor 82. In regard to the former, an additional connector 286, compatible with the cable connector on controller/monitor 82 may be used.
Delivery tube 130 extends to connection with a relatively short catheter arrangement 132. Connection between delivery tube 130 and catheter arrangement 132 being made at a fitment 288. This relatively shorter catheter is employed to assure that there is no disturbance at the injected vein as a consequence of the manipulation of syringes 120 and 122 or the three way valve 124.
Referring to
Accordingly, region 298 is physically and thermally coupled to the outer surface of tube 294 to carry this out by employing a high thermal conductance, electrically insulative, transfer tape adhesive. One such transfer tape adhesive is 8805 manufactured by 3M of Minneapolis Minn.
Additionally shown in the figure is an enclosure half 306 having a tongue component 308 carrying a connector registration slot 310. A corresponding enclosure half is shown in general at 312 having a tongue 314 and registration slot 316. A back end connector represented generally at 318 is inserted and adhesively connected to one end of tube 294, while an oppositely disposed connector represented generally at 322 is adhesively coupled to the opposite end of tube 294. When assembled, the upper region 300 of the circuit 296 is glued over tongue 314 to result in the arrangement shown in
L10=0.8″ to 1.6″
L12=0.4″ to 0.7″
L14=0.4″ to 1.2
L16=0.3″ to 1.0″
L18=0.2″ to 0.5″
L20=0.6″ to 1.4″
L22=0.6″ to 1.4″
D10=0.10″ to 0.25″
D12=0.10″ to 0.25″
D14=0.100″ to 0.250″
D16=0.106″ to 0.260″
D20=0.35″ to 0.60″
D22=0.080″ to 0.120″
D24=0.35″ to 0.60″
D26=0.080″ to 0.120″
R10=0.110″ to 0.265″
W10=0.3″ to 1.0″
W12=0.030″ to 0.060″
W24=0.3″ to 1.0″
Width of heater serpentines=0.003″ to 0.010″; thickness of Kapton in flexible heater/lead circuit=0.001″ to 0.002″; thickness of copper in flexible heater/lead circuit=0.0003″ to 0.0010″; and thickness of high thermal conductance, electrically resistive transfer tape adhesives=0.002″ to 0.005″.
It may be recalled from
Ear 340 reappears in
In the lower region, the sensor 110 appears in phantom. In the phantom view, the sensor is seen to incorporate three paired laser/photodetectors 360a-360c. Turning to
Laser 362 reappears in
Referring now to the exemplary embodiment shown in
In the exemplary embodiment shown in
This sequential energizing of the laser and measuring the emitted fluorescence photons with the photodetector/filter in each pair of this three-pair array is repeated continuously throughout the 30 to 60 second period of measuring the concentration of the fluorescing indicator within the blood vessels within the ear in the region of the laser/photodetector pairs 360a-360c. The laser/photodetector pair which yields the highest measured peak fluorescence photon level during the 30 to 60 second measurement period will be selected to display the relative indicator concentration level as a function of time, as seen in
According to this method, the present invention allows the selection of that laser/photodetector pair which is in the closest proximity to the largest blood vessel or blood vessel array even though the blood vessels cannot be visually observed during the placement of the sensor or detector 110 at a fixed position at the skin surface of the patient (e.g., the pinna of the ear). As a result, the emitted photon signal level obtained from the fluorescing indicator within the blood stream can be maximized, thereby increasing the sensitivity of the method to detect smaller right-to-left shunts as well as increasing the accuracy of the quantification of the Shunt Conductance.
This use of an array of two or more sensors or detectors can also be applied to the detection of the concentration of indicators in the blood stream other than fluorescing indicators. For example, this same arrangement of two or more sensors or detectors can be applied to relative indicator concentration measurement methods involving (a) infrared spectroscopy, (b) radiation detection for the case of radio-labeled indicators, (c) radiographic detection of radio-opaque indicators, (d) magnetic resonance based detection involving magnetic resonance imaging contrast agents and/or (e) ultrasound detection methods involving ultrasound contrast agents.
In addition and still referring to
The sensor is embodied in a sensor apparatus comprising (a) an emitter-detector pair for monitoring the fluorescence of a fluorescing circulatory tracking reagent; b) an emitter providing a light source emitting a first wavelength for the transcutaneous excitation of an indicator within the bloodstream; and (c) a detector for measuring the intensity of the light emitted at a second wavelength from an indicator within the blood stream. The apparatus typically will be embodied with a plurality of emitter and detector pairs as disposed in a sensor array. The plurality of emitter and detector pairs allows the sensors to be sequentially queried in order to determine the emitter and detector pair providing a preferred sensor from the sensor array. Particularly, it is expected that one emitter/detector pair will be in a preferred proximity to the arterial blood flow of the sensor location. The sensor is a normally utilized as a transcutaneous sensor and the preferred sensor is determined by identifying the sensor in closest relationship a subcutaneous blood vessel in order to maximize the sensitivity of said sensor. The preferred sensor may be determined by one or more of signal to noise ratio, absolute signal level, and minimum background signal. As shown, the sensor apparatus is preferably utilized with an optical coupling agent at the skin/instrument interface. Moreover, the sensor apparatus can be queried for the reflectance of the emitter signal from the skin surface, and thereby used to determine the background radiation level and the absence of reflected signal from the skin triggers a no signal fault indication.
Referring to
The mouthpiece 385 is attached to a distal end of the tubing 386 with a fitment (not shown), such as a fitment employing a barbed mechanical attachment and/or gas-tight adhesive attachment. The proximal end of extension tubing 386 terminates at a quick-disconnect fitment 387, such as a Quick-Disconnect Insert Fitting with Hose Barb fitting for securing to extension tubing as supplied by Cole Parmer, Chicago, Ill., catalog No. K-06360-42. This quick-disconnect fitment 387 attaches to a mating quick disconnect port of controller/monitor 82 which, in turn, is connected to a pressure transducer within the controller/monitor to continuously measure exhalation pressure exerted by a patient into mouthpiece 385 during a Valsalva maneuver.
With respect to the Valsalva maneuver, it is noted that the display 98 as described in connection with
Referring now to
Power supply 390 receives input power via entry module 400, cable 402; an input power switch 404 is represented at cable 406. The opposite input from power switch 404 is at cable 408 which is directed to power supply 390. The output from power supply 390 is present at cables 410 and 412 extending respectively to control board 398 and driver board 392. Control board 328 is seen to incorporate a display driver; microprocessor; memory; clock; user interface; and USB interface. It is associated with the front panel display 98 as represented at lines 414 and 416. The control board 398 also is operationally associated via bi-directional bus 418 with a USB port 420, a volume control 422, a fan 424 and a speaker 426.
The heart rate monitor shown in
Tubing for carrying out the Valsalva maneuver has been described in
Cable 112 from optical sensor 110 couples with an earpiece connector as represented at block 470. Connector 470 is directed through a ferrite torroid 476 as represented at lines 472 and 474 and, as represented by lines 478 and 480, coupled to connector 482 which is associated with signal processing interface 484. It may be recalled that the analog signals from the photodetector are filtered and subjected to fast Fourier transform activity that involves A/D conversion as represented at block 486. Additionally, the laser diodes are driven by diode drivers represented at block 488, which perform in conjunction with such details as an auxiliary power supply 490 and auxiliary transformer 492. Also shown at the driver board 392 is an auxiliary transformer function 492, an isolation transformer function 494 and an opto-coupling function 496.
The present disclosure also describes exemplary methods for testing systems for monitoring cardiac output, circulatory behavior of blood fluids, and blood circulation, including circulation within peripheral tissues of a human body and organs, such as the heart, brain or liver. For example, a method is described for utilizing an experimental animal body for determining the efficacy of circulatory tracking systems by emplacing an injection catheter into the circulatory system or a chamber of the heart in a test animal with a functioning circulatory system and heart. Once the injection catheter is emplaced, a number of variables in a circulatory tracking system to be tested may be altered. For instance, a series of circulatory tracking reagents being tested with the method may be injected into the circulatory system of the test animal, and detector systems compatible with the circulatory tracking reagent can be activated at given locations on the body of the test animal. Then, the monitoring of the efficacy of a combination of given detectors, detector locations and circulatory tracking reagents to detect the presence of given circulatory tracking agents at a particular location on the test animal body allows the optimization of a given circulatory tracking system.
In a specific example directed to determining the efficacy of indicator dyes, a bolus of circulatory tracking reagent is injected into the circulatory system or chamber of the animal heart and the detector is emplaced on the body of the test animal such that the transit of the indicator dye may be traced.
With respect to animal testing, it should be understood that developing systems, apparatus and methods utilizable with an animal model to test the efficacy of the conceived shunt detection systems, apparatus and methods was not a trivial undertaking. For example, producing a right-to-left shunt within the cardiopulmonary system of a test animal was not practical, and emulating a Valsalva maneuver would not be effective on an animal (e.g., pig) maintained on or under general anesthesia.
Looking to
As represented at arrow 542, block 544 and arrow 546, a dosage indicator was controllably injected into the left ventricle of the animal heart during testing with a concentration and dosage that emulates a right-to-left cardiac shunt. To make this injection, a pigtail catheter 556 was utilized.
A pig heart is schematically illustrated and identified generally at 550 of
The general protocol for the in vivo animal experiments was as follows. Four female swine (pig), weighing 80-100 pounds were selected. Preoperative sedation was either telazol or xylazine, 1 g IM. Following sedation the animal was anesthetized via inhalation anesthesia (isoflurane 0.7-3%, initially) in oxygen via nose cone. Flurane was titrated to maintain a surgical plane of anesthesia (abolition of the lateral canthal reflex and lack of hypertension or tachycardia) throughout the procedure. A tracheostomy was performed and the animal was ventilated. Fluid filled catheters for pressure tracings and blood gases were placed by cutdown in the carotid artery and jugular vein to aid in maintaining homeostasis and monitoring adequacy of anesthesia and volume administration. Intravenous anesthesia such as fentanyl and/or pentothal was used as necessary.
Percutaneous access was established in a femoral artery using a 5 French, 90 cm pig-tail catheter (Cook Royal Flush Plus) fed retrograde into the left ventricle of the heart. Confirmation of catheter placement in the left ventricle was performed with fluoroscopic method and monitoring of pressure waveforms. Once left ventricle placement was confirmed, a transcutaneous fluoroscopic sensor unit was placed in contact with the skin surface at the ear. A syringe pump was used to deliver a range of doses of ICG ranging from approximately 0.016 ml to 2 ml of volume per injection at concentrations ranging from 0.4 to 1.6 mg/ml to allow for measurement of peak fluorescence signal as a function of injected ICG dose. This range of ICG dose levels was selected to simulate the range of magnitudes of right-to-left shunt “leakage rates” or fluid conductances.
A number of parameters were maintained at constant levels during the in vivo pig experiments. As a fluorescence detection system was utilized, excitation laser power level was at 100 milliwatts. The injection duration was approximately 1.1 seconds, and the ICG dye concentration: 400 micrograms/ml (or μg/ml), while the fluorescence probe was positioned proximal to either a blood vessel in the left ear or blood vessel in the right ear. An optical coupling agent, Aquasonic Gel, was utilized at the probe/skin interface.
Initially, measurements were taken following introduction of an ICG bolus of peak fluorescence signal amplitude compared with dose levels in order to determine proper positioning of the sensor probe. Peak signal amplitude was measured with a 100 μg dose delivered with a with 10 ml volume via syringe. Once it was determined that an operable sensor site was located, 20 repetitions at a 25 μg dose (0.063 ml injection volume) were performed at intervals of about 1 minute between injections. The injection and monitoring was repeated utilizing a 12.5 μg dose (0.0315 ml injection volume), and utilizing a 6.4 μg dose (0.0160 ml injection volume).
Next the effect of injection volume was investigated, by determining peak fluorescence signal amplitude with a fixed dose, and variable bolus volumes. Two different doses were repeatedly delivered in either a 1 ml volume or a 10 ml volume.
Following the animal testing protocol, euthanasia was performed with 40 mEq of potassium chloride via a central venous line.
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A parametric analysis of the test results was used to determine the ICG dose required for the high sensitivity detection of simulated right-to-left shunts of various sizes using the transcutaneous fluoroscopic sensor unit. Looking at Table 1 below, test data or test numbers 091 to 130 are set forth. Also shown in the table for each test is, for example, the area under the shunt curve in millivolt-seconds, as well as the ICG dose.
In Table 1, the column headings are abbreviated as follows: “Test” represents the individual test number; “Peak [mV]” is the measured peak amplitude in millivolts; “AUC [mVs]” represents the integrated area under the curve in millivolt-seconds; “ICG Dose [mg]” is the indocyanine green dose in milligrams; “Target Location” represents the location of detector placement (right ear at either a distal or proximal location); “Volume Injected [ml]” represents the volume of indicator injected in ml of 400 μg/ml ICG; “Inj. Rate ml/min” represents the measured injection rate of the indicator solution in milliliters/minute; “Inj. Dur. (s)” represents the measured duration of the injection in seconds; “Mean BP mm Hg” represents the mean diastolic blood pressure in millimeters of mercury; and “Heart Rate (BPM)” represents the measured heart rate in beats per minute.
The area under the dye dilution curve as well as peak signals were plotted for tests 091-110 and 111-130. The peak signals of test numbers 091-110 are plotted in
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As the data in Table 1 and associated
For example, additional fluorescent circulatory tracking reagents may be tested utilizing similar sensors to those shown in
Additional non-fluorescent circulatory tracking reagents may also be tested utilizing the described animal model. Spectrophotometric and or densitometric indicators may similarly be tested simply by altering the emitter and detector frequencies to utilize the known properties of such agents in blood. Radioactive isotopes, for instance, are also amenable for use as a circulatory tracking reagent, and effective use would rely on alteration of the sensor apparatus in order to detect such agents. A variety of radioactive detectors are known to those skilled in the art of radiology, as are rapidly metabolizable radioactive reagents that could be utilized with the disclosed systems, methods and apparatus. Previously, the ability to utilize the wide variety of potential circulatory tracking reagents has been severely limited by the inability to reproducibly invoke the opening of shunts, and even to perform such testing in humans at all.
A number of different animals in addition to pig may readily be utilized using the animal testing model demonstrated herein. Any mammal potentially could be utilized, although mammals with a heart of the approximate size of a human heart are preferred (e.g., primates such as the rhesus monkey and chimpanzee, as well as canines and felines). Large rodents are additionally predicted to be amenable to the testing technique, yet in the typical laboratory rodent, the small size of veins, heart and circulating blood volume may limit the ease of use of the technique for testing circulatory tracking reagents and compatible sensors.
The indicator ICG typically is provided to the practitioner in solid or particulate form. Accordingly, it is necessary to mix it with sterile water as represented at arrow 594 and block 596. The indicator solution is prepared by mixing a known weight of ICG dye with a predetermined volume of diluents such as sterile water or phosphate buffered saline. A predetermined volume of that indicator, for example, 2 ml is drawn into a first syringe as described at 120 in
The thus filled two syringes are connected to two ports on the three-way valve as identified at 124 in
The invention is embodied also in a kit providing a clinician with the disposable materials utilized when practicing the new method. A kit supplying consumable materials necessary for quantifying a circulatory anomaly typically would include a dose of circulatory indicator reagent as a shelf stable material; a diluent for preparing the dose of circulatory indicator reagent for injection; a syringe and needle apparatus for mixing the dose of circulatory indicator reagent and the diluent and for injecting the dose into an injection port; and a dose of nonreactive blood compatible clearing reagent for completing the injection.
As represented at arrow 614 and block 616, a determination is made as to whether the test at hand will be performed with a Valsalva maneuver. In the event that such maneuver will not be used, then the method diverts as represented at arrow 618. Where the Valsalva maneuver is to be used, then as represented at arrow 620 and block 622, the mouthpiece of the pressure transducer or manometer is set in the mouth of the patient as shown at 106 in
Next, the patient as represented at arrow 632 and block 634, is instructed to begin the Valsalva maneuver by exhaling into the mouthpiece to reach and continue a minimum level of 40 mmHg of pressure. The patient will have been instructed that this breathing maneuver will be continuous for about 15-20 seconds. Meanwhile, the patient as well as the practitioner may observe the dynamic bar graph at the display of the controller/monitor 82. This continuous measurement is represented at arrow 636 and block 638.
The system carries out this continuous monitoring looking for the noted minimum exhalation pressure as represented at arrow 640 and block 642. In the event that minimum pressure falls below the threshold, that event is then represented at arrow 644 and block 646. An audible alarm is sounded and a visual error message published instructing the patient to increase pressure. PFLAG is set to zero and the program reverts as represented at arrow 648 to arrow 632 where the system responds leading to the recommencement of the timing of the Valsalva maneuver.
Where the exhalation pressure is maintained at an appropriate level, then as represented at arrow 650 and block 652 PFLAG is set to one and the program continues as represented at arrow 654. Returning momentarily to
Arrow 662 reappears in
The three-way valve will be manipulated during these injections. Also during the injections, the fluid flow sensor 126 will be active as represented at arrow 676 and block 678. The start and end of injection is measured with the flow sensor.
A check is made as represented at arrow 680 and block 682 determining whether the start time less the end time is greater than the time of injection. Where it is not, then as represented at arrow 684 and block 686, a negative response causes the operator to be audibly alarmed and presented with a visual error message indicating that the injection was not completed in the allowed time interval. It is restarted as represented at arrow 688 leading to node A. Node A reappears in
Where the determination at block 682 is that the injection took place in a proper time frame, the program continues as represented at arrow 692. Arrow 692 reappears in
Next, as represented at arrow 706 and block 708, a determination is made as to whether the elapsed time is greater than or equal to the completion time. In the event it is not, then the program dwells as represented at arrow 710 extending to arrow 706. Where the elapsed time has reached the time of completion, then as represented at arrow 712 and block 714, average heart rate over the elapsed time is computed and the program continues as represented at arrow 716. Arrow 716 reappears in
Next, as represented at arrow 720 and block 722, the area A under the normal indicator dilution curve is calculated (AUC). This is the curve representing blood and indicator flowing through the lungs. Next, as represented at arrow 724 and block 726, a query posed at block 726 determines whether the calculated normal area is greater than or equal to a minimum under curve area. In the event that it is not, then as represented at arrow 728 and block 730, the operator is alerted with an audible alarm and visual error message that insufficient coupling exists between the sensor and blood-borne indicator in tissue. Where a query at block 726 results in an affirmative determination, then the area under any premature indicator/dilution curve or curves associated with a right-to-left shunt is/are calculated. The parameter Ai is the area under premature indicator dilution/curve i, where i is either one or two.
Next, as represented at arrow 736 and block 738, if Ai is non-zero, then the conductance associated with right-to-left shunts is calculated as described herein. Then, as represented at arrow 740 and block 742, a query is made as to whether another test is required for this patient. In the event of an affirmative determination, then as represented at arrow 744, node A reappearing in
While exemplary embodiments of the invention have been described herein, those skilled in the art will understand that various changes may be made and equivalents may be substituted for elements thereof without departing from the scope of the invention. In addition, many modifications may be made to adapt a particular situation or material to the teachings of the invention without departing from the essential scope thereof. Since certain changes may be made in the above compositions and methods without departing from the scope of the invention herein involved, it is intended that all matter contained in the above descriptions and examples or shown in the accompanying drawings shall be interpreted as illustrative and not in a limiting sense.
In this application all units are in the metric system or English system for the case of dimensions of the flow sensor 126 and its components and all amounts and percentages are by weight, unless otherwise expressly indicated. Also, all citations referred herein are expressly incorporated herein by reference. All terms not specifically defined herein are considered to be defined according to Dorland's Medical Dictionary, and if not defined therein according to Webster's New Twentieth Century Dictionary Unabridged, Second Edition. The disclosures of all of the citations provided are being expressly incorporated herein by reference.
This application is a continuation of U.S. application Ser. No. 12/418,866 filed on Apr. 6, 2009, which claims the benefit of Provisional Application No. 61/156,723 filed on Mar. 2, 2009 and Provisional Application No. 61/080,724 filed on Jul. 15, 2008, all of which are hereby incorporated by reference herein.
Number | Date | Country | |
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61156723 | Mar 2009 | US | |
61080724 | Jul 2008 | US |
Number | Date | Country | |
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Parent | 12418866 | Apr 2009 | US |
Child | 14100724 | US |