WO2003070323A1 - Ultrasound cardiac stimulator - Google Patents

Ultrasound cardiac stimulator Download PDF

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Publication number
WO2003070323A1
WO2003070323A1 PCT/IL2003/000134 IL0300134W WO03070323A1 WO 2003070323 A1 WO2003070323 A1 WO 2003070323A1 IL 0300134 W IL0300134 W IL 0300134W WO 03070323 A1 WO03070323 A1 WO 03070323A1
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WO
WIPO (PCT)
Prior art keywords
heart
ultrasound
ulfrasound
cardiac
operative
Prior art date
Application number
PCT/IL2003/000134
Other languages
French (fr)
Inventor
Dan Adam
Original Assignee
Technion Research & Development Foundation Ltd.
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Technion Research & Development Foundation Ltd. filed Critical Technion Research & Development Foundation Ltd.
Priority to EP03706886A priority Critical patent/EP1480723A1/en
Priority to US10/505,630 priority patent/US7699778B2/en
Priority to AU2003208592A priority patent/AU2003208592A1/en
Publication of WO2003070323A1 publication Critical patent/WO2003070323A1/en
Priority to US12/762,389 priority patent/US20100204576A1/en

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Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N7/00Ultrasound therapy
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61BDIAGNOSIS; SURGERY; IDENTIFICATION
    • A61B17/00Surgical instruments, devices or methods, e.g. tourniquets
    • A61B17/00234Surgical instruments, devices or methods, e.g. tourniquets for minimally invasive surgery
    • A61B2017/00238Type of minimally invasive operation
    • A61B2017/00243Type of minimally invasive operation cardiac
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61BDIAGNOSIS; SURGERY; IDENTIFICATION
    • A61B17/00Surgical instruments, devices or methods, e.g. tourniquets
    • A61B2017/00681Aspects not otherwise provided for
    • A61B2017/00694Aspects not otherwise provided for with means correcting for movement of or for synchronisation with the body
    • A61B2017/00703Aspects not otherwise provided for with means correcting for movement of or for synchronisation with the body correcting for movement of heart, e.g. ECG-triggered
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/18Applying electric currents by contact electrodes
    • A61N1/32Applying electric currents by contact electrodes alternating or intermittent currents
    • A61N1/36Applying electric currents by contact electrodes alternating or intermittent currents for stimulation
    • A61N1/362Heart stimulators
    • A61N1/3629Heart stimulators in combination with non-electric therapy
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N7/00Ultrasound therapy
    • A61N2007/0078Ultrasound therapy with multiple treatment transducers

Definitions

  • the present invention is related to the field of cardiac diagnosis and therapy.
  • BACKGROUND OF THE INVENTION The myocardium is susceptible to mechanical stimulation: case reports have detailed incidents of cardiac arrest due to a ball or a fist hitting the person's thorax.
  • Physiological studies have reported initiation of an action potential due to a mechanical stimulation such as tapping of the epicardium [Avitall, B., Levine, H. J., Naimi, S., Donahue, R. P., Pauker, S. G., and Adam, D. R., "Local effects of electrical and mechanical stimulation on the recovery properties of canine ventricle," Am. J. Cardiology 50, 263-270 (1982)], or due to stretch.
  • ultrasound pulses have been reported to shatter kidney stones, while also affecting inner cellular structures and membrane properties.
  • ultrasound pulses increase membrane permeability and specific ion flow.
  • Ultrasound transducers attached to cardiac catheters have been used to induce electrical activity locally in the heart, for diagnostic purposes.
  • External ultrasound transducers used for imaging have also been observed to induce action potentials in the heart, inadvertently, especially when contrast agents containing small bubbles are injected into the bloodstream. Because of the danger of inducing action potentials in the heart in an uncontrolled way, great care is taken during ultrasound imaging of the heart not to induce action potentials.
  • Direct electrical stimulation of the heart is done for cardiac pacing, usually via electrodes implanted during surgery.
  • Electrodes may be inserted by catheters via the venous or arterial system.
  • Catheters are also used to carry laser or RF or ultrasound energy to specific sites in the heart or elsewhere in the circulatory system, in order to ablate tissue for therapeutic purposes. All of these invasive procedures involve obvious risks and expenses.
  • Ultrasound energy from external transducer arrays has been focused on tumors in order to destroy them by heating.
  • An aspect of some embodiments of the invention relates to stimulating cardiac tissue, or any other excitable tissue such as muscles and nerves, using ultrasound, for diagnostic and/or therapeutic purposes, using transducers located outside the body, or in the esophagus or other non-invasive body channels, such as the nasal cavities.
  • ultrasound contrast agents for example microbubbles or liposomes, are used to enhance the procedure, for example by increasing the sensitivity of the cardiac tissue to stimulation.
  • an imaging system is used to track and observe the heart before, during, and/or after the cardiac tissue is stimulated. This is done, for example, in order to observe the local or global mechanical response of the heart to the stimulation, or to focus the ultrasound energy on the correct spot.
  • the imaging system is an ultrasound imaging system, using the same transducers as are used for stimulation. Alternatively or additionally, other ultrasound transducers may be used for imaging. Alternatively or additionally, a Computer Aided Tomography system using x-rays, a Magnetic Resonance Imaging system, or any imaging system known to the art may be used.
  • contrast agents are used to improve image quality, and/or to distinguish between perfused and non- perfused tissue.
  • the location and orientation of the heart, or a particular point on the heart are tracked in real time while ultrasound is used to stimulate the heart. Such tracking makes it possible to repeatedly focus ultrasound on the same spot in the heart, or to successively focus ultrasound on two or more spots with known relative positions.
  • ultrasound waves are focused on one small spot in the heart, to stimulate the tissue, and the response to stimulation is observed.
  • This stimulation spot can be deep inside the myocardium, as well as on the exterior or interior surface of the heart.
  • the ultrasound waves are focused on a different stimulation spot.
  • the ultrasound waves are focused on more than one stimulation spot simultaneously, or nearly simultaneously relative to the speed of propagation of signals in the heart.
  • measurements are optionally made of the intensity and duration of ultrasound needed to induce action potentials, either propagating or non-propagating, and the spatial distribution of the potential is optionally measured, as a function of time.
  • the mechanical response of tissue to action potentials is optionally measured as a function of time, for example by observing changes in thickness and motion of the cardiac wall, at the stimulation spot and at other spots.
  • the ultrasound source is aimed at a particular location in the heart and its firing is synchronized to the cardiac cycle, for example, using an ECG (which may provide local electrical information) or using an analysis of a series of images.
  • the analysis may be automatic or manual, for example.
  • the imager is also aimed at the particular location and/or at a location where an effect of the excitation is expected and/or is desired to be studied.
  • the imager is closely synchronized with the stimulating ultrasound, which may make it easier to detect the short-term mechanical response of the heart tissue to the ultrasound. It may also be possible to detect the motion of the heart wall due to the pressure of the ultrasound.
  • the imager can detect the exact location of excitation (even if the aiming is not precise), for example, by detecting non-linear effects at the location.
  • the imager can capture a development of mechanical response to the excitation, over a period of time, due to the action potential.
  • this detected response may be synchronized with a measurement of electrical activity from outside the body (e.g., using a high resolution ECG) or from inside the body (e.g., using a catheter). It should be noted that in this manner a map having a resolution better than the aiming ability can be created, by marking the map with the actual excitation signal location.
  • the analysis of the detected response and the ECG may be manual or automatic.
  • the mechanical response to the action potential is found automatically by using image analysis software to measure changes in wall thickness. When this measurement is synchronized to a local ECG, a delay in mechanical response is calculated.
  • results of these measurements are optionally used for identifying ischemic tissue that is permanently damaged, and distinguishing it from tissue that is stunned or hibernating but could be revived. Tissue that is overly sensitive to stimulation, and could give rise to arrhythmias, may also be identified.
  • Maps of the location of healthy and pathological tissue in the heart are used in some embodiments of the invention to design spatial and temporal sequences of stimulation that are optimal for pacemaking.
  • such sequences are tested and compared using ultrasound stimulation.
  • some tissue is ablated by ultrasound, or by other means as known in the art.
  • ultrasound is used to increase membrane permeability at particular locations in the heart and/or particular times in the cardiac cycle, in order to selectively increase the absorption or effect of drugs at those locations and/or times.
  • the drugs are delivered to specific locations by a cardiac catheter.
  • a phased array of transducers is used to generate the focused ultrasound pulses.
  • a single transducer with focusing is used.
  • the transducers are placed on the outside of the chest.
  • the transducers optionally are placed between the ribs.
  • the transducers are placed on the sternum, or below the rib cage.
  • the transducers are placed non-invasively inside the body, for example in the esophagus.
  • ultrasound pulses are used to provide temporary pacing of the heart, for example when a conventional pacemaker is temporarily not operating, or during bradycardia.
  • different temporal and spatial sequences of ultrasound pulses are tested and compared, in order to find the best sequence to use for pacing.
  • the different sequences are evaluated using, for example, electrocardiograph data, systolic pressure measurements, and/or images showing the mechanical response of the heart, including systolic and diastolic left ventricular volume and ejection fraction.
  • a cardiac catheter is used to provide direct electrical simulation of the heart, in addition to the stimulation by ultrasound.
  • Direct electrical stimulation may help to identify tissue pathologies by comparing its effects to the effects of mechanical stimulation by ultrasound. In one example, such a comparison is used to distinguish stunned from hibernating myocardium.
  • the ultrasound pulses are focused at a coarse, resolution, and used to produce a coarse map of pathological tissue, and a cardiac catheter is used to map certain regions more precisely.
  • the imaging system is optionally used to determine the precise location of the cardiac catheter.
  • the catheter optionally is used to ablate or otherwise kill cardiac tissue, optionally monitoring the process with the imaging system. This killing is done by any means known to the art.
  • the catheter brings electric power to an ohmic or inductive heating element, a refrigerating element, an ultrasound transducer or a radio frequency transmitter in the circulatory system, or the catheter carries laser light on a fiber optic cable, or carries a drug.
  • an ultrasound cardiac stimulation system comprising: a spatially selective ultrasound source comprising at least one ultrasound transducer located outside the circulatory system; and a controller; wherein the controller generates an electrical response in the heart by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.
  • an injector which injects cardiac drugs into the bloodstream, and the controller changes the rate at which cardiac tissue absorbs the drugs by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.
  • the controller is operative to choose the ultrasound power level.
  • the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ⁇ 20%.
  • the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ⁇ 10%.
  • the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ⁇ 3%.
  • an injector which injects one or both of drugs for treating the heart and contrast agents into the bloodstream.
  • the controller is operative to reduce the power level of ultrasound when the contrast agents are injected.
  • the controller is operative to choose the one or more locations to which the ultrasound is transmitted.
  • the controller controls the ultrasound source to direct ultrasound energy to a designated location, and the point of highest power flux density falls within an axial precision of 3 mm of said designated location.
  • the axial precision is 1.5 mm.
  • the point of highest power flux density remains within the axial precision of the designated location for at least 1 millisecond.
  • the point of highest power flux density remains within the axial precision of the designated location for at least 10 milliseconds.
  • the controller controls the ultrasound source to direct ultrasound energy to a designated location, and the point of highest power flux density falls within a transverse precision of 1 mm of said designated location.
  • the transverse precision is 0.5 mm.
  • the point of highest power flux density remains within the transverse precision of the designated location for at least 1 millisecond.
  • the point of highest power flux density remains within the transverse precision of the designated location for at least 10 milliseconds.
  • the controller controls the ultrasound source to direct a high enough power level of ultrasound to one or more locations in the heart to kill cardiac tissue by heating it.
  • the controller controls the ultrasound source to direct a high enough power level of ultrasound to one or more locations in the heart to kill cardiac tissue by cavitation.
  • an electrocardiograph which measures the timing of the cardiac cycle.
  • the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating in any one chamber of the heart, from the electrical response originating in any other chamber of the heart.
  • the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating in one side of any chamber of the heart, from the electrical response originating in the other side of said chamber of the heart.
  • the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one centimeter away from said location.
  • the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one millimeter away from said location.
  • the system uses feedback from the electrocardiograph to control the ultrasound power level.
  • the controller is operative to make a map of the heart, showing the ultrasound power flux required to generate the electrical response at each of several locations in the heart.
  • the controller is operative to direct the ultrasound source to transmit a first sequence of timed localized pulses of ultrasound energy to the heart, and a second such sequence which differs from the first sequence in one or both of timing and location of the pulses, and the controller is operative to collect a first data set showing the effects of the first sequence on the heart, and a second data set showing the effects of the second sequence on the heart.
  • the first data set and the second data set comprise data from the electrocardiogram.
  • a memory which is operative to store the first data set and the second data set, a data analyzer which is operative to analyze data and produce analysis results from the first data set and the second data set, and a display which displays the analysis results.
  • the first data set and the second data set comprise data on systolic pressure.
  • the first sequence and the second sequence differ in timing of the pulses.
  • the first sequence and the second sequence differ in location of the pulses.
  • the cardiac imaging system which produces images showing the position of one or more locations on the heart.
  • the first data set and the second data set comprise data from the cardiac imaging system.
  • an image analyzer which analyzes images produced by the cardiac imaging system for the first sequence and the second sequence, and calculates one or more of the systolic left ventricular volume for the first and second sequence, the diastolic left ventricular volume for the first and second sequence, and the ejection fraction for the first and second sequence.
  • the images produced by the imaging system show the mechanical response of the heart to stimulation produced by the ultrasound.
  • the imaging system is in a fixed position and orientation with respect to the ultrasound source.
  • sensors which determine the relative position and orientation of the imaging system and the ultrasound source.
  • the imaging system determines the relative position and orientation of the ultrasound source by imaging it.
  • the controller coordinates the timing of the imaging system with the timing of the ultrasound source.
  • the controller is operative to make a map of the heart, using data from the imaging system, showing the mechanical response of the heart at one or more locations to ultrasound energy transmitted to one or more locations.
  • the system uses feedback from the imaging system to control the ultrasound power level.
  • the imaging system uses ultrasound imaging.
  • the imaging system shares one or more ultrasound transducers with the ultrasound source used to generate the electric response in the heart.
  • the imaging system does not share any ultrasound transducers with the ultrasound source used to generate the electric response in the heart.
  • the imaging system comprises a computerized tomography x-ray imaging system.
  • the imaging system comprises a magnetic resonance imaging system.
  • image processing software which analyzes the images to determine the position of one or more locations on the heart.
  • the image processing software determines the position of one or more locations on the heart in real time during a cardiac cycle.
  • the confroller coordinates the timing of the transmission of ultrasound with the cardiac cycle.
  • a cardiac catheter which generates an electrical response in the heart
  • a calibration mode of the confroller wherein the controller, when it is in the caUbration mode, calibrates the ultrasound power transmitted to the heart by the ultrasound array, by comparing a physiological response induced by the ultrasound array to a physiological response induced by the catheter.
  • the physiological responses compared by the controller comprise electrical responses.
  • the physiological responses compared by the controller comprise mechanical responses.
  • the cardiac catheter generates an electrical response by direct electric stimulation.
  • the cardiac catheter comprises an internal ultrasound transducer, and the cardiac catheter generates an electrical response by transmitting ultrasound.
  • the cardiac catheter kills cardiac tissue.
  • the cardiac catheter comprises a light guide, and the light guide carries light from the laser, which light kills cardiac tissue.
  • the ultrasound source comprises a phased array of the ultrasound transducers.
  • at least one of the at least one ultrasound transducers is adapted for use on the surface of the body.
  • the at least one ultrasound transducers comprise at least two ulfrasound transducers, sized and spaced so that they can be placed between the ribs, in such a way as to avoid blocking of ultrasound by the ribs .
  • At least one of the at least one ultrasound transducers is adapted for use in the esophagus.
  • At least one of the at least one ultrasound transducers is adapted for use in a nasal cavity.
  • the ultrasound source and the controller are operative to direct the ultrasound energy with 90% of the power flux falling within 3 mm transversely of the point of highest power flux density.
  • the ultrasound source and the controller are operative to direct the ultrasound energy with 90% of the power flux falling within 1.5 mm transversely of the point of highest power flux density.
  • the ultrasound source and the confroller are operative to direct the ultrasound energy with 90% of the power flux falling within 1 mm transversely of the point of highest power flux density.
  • the ultrasound source and the confroller are operative to direct the ultrasound energy with the power flux spreading out to 50% of its highest density within 6 mm axially of the point of highest power flux density.
  • the ultrasound source and the controller are operative to direct the ultrasound energy with the power flux spreading out to 50% of its highest density within 3 mm axially of the point of highest power flux density.
  • the ultrasound source and the controller are operative to direct the ultrasound energy with the power flux spreading out to 50% of its highest density within 1.5 mm axially of the point of highest power flux density.
  • the ultrasound source and the controller are operative to direct the ultrasound energy with a power flux density greater than 30 watts per square centimeter at the point of highest power flux density.
  • the ultrasound source and the controller are operative to direct the ulfrasound energy with a power flux density greater than 100 watts per square centimeter at the point of highest power flux density.
  • the ultrasound source and the controller are operative to direct the ulfrasound energy with a power flux density greater than 300 watts per square centimeter at the point of highest power flux density.
  • the ultrasound source and the controller are operative to direct the ultrasound energy in a pulse lasting less than 10 milliseconds.
  • the ultrasound source and the controller are operative to direct the ultrasound energy in a pulse lasting less than 1 millisecond.
  • the ultrasound source and the controller are operative to direct the ultrasound energy in a pulse lasting for a duration within 10% of a duration for which the controller is directed to direct the energy.
  • the ultrasound source and the controller are operative to direct the ultrasound energy at a frequency greater than 0.5 megahertz and less than 6 megahertz.
  • a method of changing a cardiac stimulation sequence for a patient comprising: a) choosing a test sequence of locations in the heart of the patient, and a time in the cardiac cycle to stimulate each location; b) stimulating the test sequence of locations at the chosen times in the cardiac cycle, using an ultrasound cardiac stimulation system from outside the heart; c) evaluating a change in cardiac synchronization of the patient associated with the test sequence; d) choosing a stimulation sequence for a pacemaker, based at least partly on the change in cardiac synchronization that the test sequence produces; and e) changing a stimulation sequence of the heart to conform to the chosen stimulation sequence.
  • using an ultrasound cardiac stimulation system from outside the heart comprises using an ultrasound stimulation system from outside the body.
  • changing a stimulation sequence of the heart comprises installing a pacemaker.
  • changing a stimulation sequence of the heart comprises adjusting a pacemaker.
  • adjusting a pacemaker comprises programming a pacemaker.
  • adjusting a pacemaker comprises adjusting a pacemaker to obtain improved cardiac synchronization.
  • (a), (b) and (c) are performed a plurality of times for different test sequences, and choosing an optimal stimulation sequence is based at least partly on the change in a measure of cardiac performance that the different test sequences produce.
  • the measure of cardiac performance comprises cardiac output.
  • evaluating the change in the measure of cardiac performance comprises using systolic pressure measurements.
  • evaluating the change in the measure of cardiac performance comprises using images of a mechanical response of the heart to the stimulation.
  • at least one of the test sequences comprises a plurality of locations with the same chosen time.
  • evaluating the change in cardiac synchronization comprises using electrocardiograph data.
  • Fig. 1 is a schematic cross-sectional view of the chest and heart, showing ultrasound systems used for stimulating the heart, according to an exemplary embodiment of the invention
  • Fig. 2 is a flowchart illustrating how a map is made of the sensitivity of the heart to stimulation by ultrasound pulses;
  • Fig. 3 is a flowchart showing how the imaging system is used to track the location of different spots on the heart in real time; and Fig. 4 is a flowchart showing how cardiac tissue is destroyed, while the effects are monitored.
  • FIG. 1 schematically shows an ulfrasound system according to an exemplary embodiment of the invention.
  • a heart 10 is shown in a cross-section of a patient's chest 12.
  • a phased array 14 of ultrasound transducers focuses ultrasound waves 16 on a spot 18 in the wall of the heart, stimulating cardiac tissue at that spot and possibly inducing action potentials, detected by an electrocardiograph 20.
  • the ulfrasound can generally be focused on any desired spot 18.
  • any other method of focusing ultrasound known to the art is used to focus the ulfrasound waves on spot 18.
  • the diameter of the spot cannot be much smaller than one wavelength, assuming that it is in the far field of the transducers, i.e. at least several wavelengths away from the transducers.
  • the frequency of the ultrasound optionally has a frequency approximately 1 MHz or higher, which would have a wavelength in the body of about 1.5 mm or less.
  • Ultrasound transducers exist which can operate at frequencies as high as 10 MHz. If the frequency is too high, however, and the desired focused spot is not close enough to the transducers, then the ultrasound will be largely absorbed before reaching the desired spot, and higher fransducer power or more transducers will be needed to produce the same ultrasound power flux at the spot.
  • the focused spot is elliptical, 1 to 2 mm in diameter and 4 to 6 mm in length in the direction of propagation, with the acoustic pressure outside the spot significantly lower than the peak pressure.
  • Focused spots with dimensions greater or smaller than these values, for example 0.5 mm to 4 mm in diameter and 2 mm to 10 mm in length, are also optionally used.
  • Peak acoustic pressures are typically 2 to 4 MPa, corresponding to powers of 125 to 500 watts per square centimeter, and pulse lengths are typically 1 to 10 milliseconds long.
  • ultrasound pulses with frequencies, powers and pulse lengths of 1 to 5 MPa, corresponding to 30 to 800 watts per square centimeter, or even greater than or less than this range, are used.
  • Transducer array 14 is shown outside the chest in Fig. 1.
  • the transducers are optionally placed between the ribs, or below the rib cage. Alternatively, they are placed inside the chest, in the esophagus.
  • An imaging system 22 is used to determine the position and orientation of the heart, relative to transducer array 14, so that ultrasound energy can be accurately focused on a desired spot on the heart by transducer array 14.
  • Fig. 1 shows an imaging system that is separate from fransducer array 14, optionally transducer array 14 is used for an ultrasound imaging system, as well as for stimulating cardiac tissue.
  • ultrasound waves for imaging purposes are optionally transmitted alternately with ultrasound waves for cardiac stimulation. If the imaging waves and stimulating waves are transmitted close enough together in time, then the heart will not move very much, and the information from the imaging system can still be used to accurately focus the stimulating waves. Alternatively or additionally, the stimulating waves themselves are used for imaging.
  • the imaging system need not be an ultrasound imaging system. It could be an x-ray CAT system, or an MRI system, or any other medical imaging system known to the art.
  • imaging system 22 is not an ultrasound imaging system using the same transducer array 14 that is used for stimulation, then it may be desirable to know the relative position and orientation of imaging system 22 and transducer array 14. Ultrasound can then be used to stimulate a spot whose position is defined by imaging system 22, and imaging system 22 can image a spot that has been stimulated, observing the effects of the stimulation.
  • transducer array 14 is rigidly connected to imaging system 22, so that they always have the same relative position and orientation.
  • imaging system 22 determines the relative position and orientation of transducer array 14 by imagining it.
  • a computer 24 controls the phase, amplitude, and timing of ultrasound waves emitted by the transducers in transducer array 12, using input from the human operator, the imaging system, and the electrocardiograph. Details of how this is done, according to an embodiment of the invention, are given in Fig. 2.
  • Computer 24 could comprise an general purpose computer running appropriate software, or custom-designed control circuitry, or a combination of the two.
  • Fig. 1 schematically shows an intravenous tube 26, which is used to introduce contrast agents into the bloodstream, during ultrasound stimulation.
  • Contrast agents which are encapsulated small gas bubbles, significantly attenuate the propagating ultrasound energy, reflecting, scattering and absorbing it.
  • the contrast agent bubbles oscillate and sometimes burst, producing exfremely high pressures locally. This enhances the stimulating effect of ultrasound on cardiac tissue.
  • lower power transducers can be used to produce the same stimulation effect, and there may be less heating of tissue for the same stimulation effect.
  • Contrast agents are also useful in imaging, for example for showing the precise boundaries of tissue with normal perfusion of blood and regions with reduced or no perfusion.
  • intravenous tube 26 is used to introduce drugs into the bloodstream during ulfrasound stimulation of the heart. Since ultrasound stimulation can increase the permeability of cell membranes, certain locations in the heart will be induced to take up drugs from the bloodstream, more than other regions that are not stimulated. The uptake of drugs can also be timed to occur at certain times in the cardiac cycle, if the ultrasound stimulation is gated with an electrocardiograph. Alternatively or additionally, the contrast agents and/or the drugs can be introduced into the heart by a cardiac catheter, rather than intravenously, allowing additional control over the spatial and temporal distribution of the contrast agents and/or drugs.
  • Fig. 2 is a flowchart showing how the transducer array is used to map regions of healthy and pathological tissue in the heart, according to an exemplary embodiment of the invention.
  • Tissue is optionally classified as healthy or pathological according to one or more of several criteria, for example: • Ultrasound power level required to induce an action potential
  • the flowchart in Fig. 2 illustrates only how the first criterion, ultrasound power level required to induce an action potential, is mapped, but optionally any one or combination of these criteria are used to make a map.
  • the map identifies regions which are more susceptible than normal, or less susceptible than normal, to producing extra action potentials (beyond those associated with the regular heartbeat) when stimulated by ultrasound.
  • Such a map can reveal the location of ischemic tissue, which typically requires higher than normal ultrasound levels to produce an action potential, and/or tissue which is susceptible to arrhythmias, which may require a lower than normal ultrasound level to produce an action potential.
  • a region is chosen for mapping, either the whole heart or a part of the heart, and the range of ultrasound power levels is optionally chosen. This range starts at a level well below the power that would be needed to induce an action potential in normal tissue, and ends at a level above the power that would be needed to induce an action potential in normal tissue, but optionally not at such a high level that the tissue could be damaged by heating or cavitation.
  • the region for mapping is optionally chosen by the operator as a range of myocardial coordinates, defined in relation to the heart tissue, i.e.
  • a given point on the heart has constant myocardial coordinates even while its absolute position is changing because the heart is beating.
  • the range could be chosen by the operator by dragging a mouse across a 3-D displayed image of the heart (for example, a series of 2-D cross-sections) frozen at a particular phase in the cardiac cycle.
  • a phase in the cardiac cycle, or a set of phases is also chosen for mapping.
  • the response of tissue to stimulation generally depends on the phase in the cardiac cycle at which the stimulation is applied.
  • they are chosen or changed during the procedure.
  • the myocardial coordinates of the spot to be stimulated are set at the first point on the grid to be mapped, and the power is set at the bottom of the range.
  • the confroller waits for the desired phase in the cardiac cycle, using electrocardiograph data, for example, to determine at what time the desired phase occurs.
  • a quick image which need not have high resolution, is made of the heart, in order to locate the absolute position (relative to the transducers) of the spot to be stimulated. Making an error in location of the focused spot is potentially dangerous, since a high power ultrasound pulse intended for an insensitive spot could be focused by mistake on a very sensitive area and induce fibrillation.
  • the image made in 106 is used to determine the orientation and location of the heart, and this information is used to convert the myocardial coordinates of the point being stimulated to thoracic coordinates, defined relative to the chest cavity (and hence to the transducers, which are optionally pressed against the outside of the chest). Some details of how this calculation is done are given below in the description of Fig. 3. If the imaging and calculation could be done in less than 50 milliseconds, or better yet in less than 10 milliseconds, then the heart would move very little between the time it is imaged and the time the ultrasound energy is applied for stimulation.
  • the range of points to be mapped is directly defined in terms of thoracic coordinates at a particular phase in the cardiac cycle, and the ulfrasound energy is always applied at the same phase in the cycle.
  • a disadvantage of this alternative method is that there could be variations in position and orientation of the heart from one heartbeat to the next.
  • the ulfrasound transducers are located in the esophagus rather than on the outside of the chest, then it may not be sufficient just to define the position of the point to be mapped in thoracic coordinates. In addition, it may be necessary to take into account changes in position of the fransducers relative to the chest cavity. Optionally this is done by using an external imaging system to locate the position of the stimulating fransducers in the esophagus. Alternatively, if the same fransducers are used for stimulation and imaging, then those transducers can be used directly to find the location of the heart (or of the desired point on the heart) relative to the fransducers.
  • the stimulating ultrasound energy is focused on the desired spot on the heart. As described above in the description of Fig. 1, this is optionally done by first using a computer to calculate the phases and amplitudes of the fransducers in the array, needed to focus ultrasound energy on the desired spot.
  • a cine (moving) image is optionally made of the heart, in order to assess the mechanical response of the heart, if any, to the stimulation.
  • the image is processed to track only a limited set of points on the heart, sufficient to characterize the mechanical response of the heart, and only these results are stored.
  • the cine imaging optionally begins before the stimulation is applied, and continues while the stimulation is applied and for a given period afterwards. Even if the same transducers are used for imaging and stimulation, the cine imaging optionally begins before the stimulation, and is briefly interrupted while the transducers are used for stimulation, and resumed afterwards.
  • the cine image or a still image is precisely synchronized with the ultrasound stimulation, and is used to detect the short-term mechamcal response of the heart tissue to the ultrasound stimulation, which may provide more information about the exact location of the ultrasound stimulation.
  • the confroller examines data, for example from an electrocardiograph, to determine whether the ulfrasound stimulation induced an action potential, beyond the action potential that already existed as part of the natural cardiac cycle.
  • the electrocardiograph provides some information about the spatial distribution of action potentials, as well as their amplitude and time dependence.
  • the electrocardiograph is calibrated before it is used to measure induced action potentials, for example by comparing the induced action potentials to the regular action potential. If no extra action potential is observed, and if the power level is not yet at the top of the chosen range (118), then the power is raised to the next level (120), and the flow goes back to 105, in preparation for a new application of ultrasound energy at the same spot. If the power was already at the maximum level, then this spot is recorded as unresponsive (124), and the flow goes to 132.
  • the power starts at the middle of the range, at a level that has a 50% chance of exciting an action potential, according to some model. If an action potential is seen, then the power is lowered to a level that now has a 50% chance of eliciting an action potential, taking into account the previous results. If an action potential is not seen, then the power is raised to a level that now has a 50% chance of eliciting an action potential, taking into account the previous results. This procedure is continued until the exact threshold for eliciting an action potential is found, to the desired precision.
  • This "zeroing in” procedure has an advantage over the "one step at a time” procedure, in that the number of steps required scales as the logarithm of the desired precision, rather than scaling linearly with the desired precision.
  • a disadvantage of the "zeroing in” procedure is that it might overstimulate a very sensitive spot, causing fibrillation. Many other procedures are possible for determining the threshold for eliciting action potentials, which will be apparent to persons skilled in the art.
  • the data is examined to see whether the action potential is propagating, and how it propagates (126).
  • This information is recorded (128), and (130) any mechanical response is assessed (based on the cine image made in 114, for example), and recorded.
  • image processing software is used to assign one or more quantitative values to characterize the mechanical response.
  • the mechanical response could be characterized by the operator after viewing the cine image.
  • the cine image for each spot is stored, and the mechanical response is evaluated at leisure after the map of action potential threshold is completed.
  • the myocardial coordinates are set for the next spot in the grid, and the flow goes back to 104.
  • the procedure ends (136).
  • the recorded data on the ultrasound power threshold needed to induce an action potential at each point, and on the propagation of induced action potentials, are then used to create one or more maps, for example using postprocessing software.
  • the maps could show the propagation paths, as well as the action potential threshold at each spot. The accuracy of the map showing action potential thresholds will be confirmed if it is consistent with the map of propagation paths, for example if it shows that regions that are resistant to inducing action potentials are also regions that block propagation of action potentials induced elsewhere.
  • a map could be made for each of several phases.
  • the controller could change the phase and loop back to 102, until all desired phases were examined.
  • the phase could be changed in an inner loop.
  • ulfrasound stimulation could be done at each of several different phases.
  • the controller moves to the next spot. This procedure produces a map of the minimum power needed to induce an action potential at the most sensitive phase in the cardiac cycle.
  • the power threshold for inducing an action potential is measured for each of several phases at each spot.
  • corrections to the ultrasound power level are optionally made taking into account absorption of ulfrasound energy between the transducers and the focused spot.
  • the amount of abso ⁇ tion may be estimated by using known values for absorption lengths of ultrasound at the frequency used, in different types of tissue.
  • abso ⁇ tion may be measured by using data from the imaging system, if it is an ultrasound imaging system, or by detecting stimulating ulfrasound waves reflected back to the fransducers. For example, images can be compared at lower ultrasound frequency, where there is less abso ⁇ tion, and higher frequency where there is more abso ⁇ tion, in order to calibrate the amount of abso ⁇ tion at the frequency used for stimulation.
  • the ultrasound power flux focused on a given spot in the heart is controlled to within 10%, taking into account errors in the powers and phases of the transducers, and uncertainties in the amount of power that is absorbed between the transducers and the focused spot.
  • the power is controlled only to within 20%, or to within better than 3%.
  • Corrections are also optionally made to the map by taking into account the finite amplitude of ulfrasound at locations other than the focused spot, which can be calculated from the size, spacing, and number of transducers in the array, and by modeling reflections and refraction of ultrasound waves. Such a spatial distribution of the ultrasound intensity could stimulate action potentials first at those other locations, if the tissue there is much more sensitive than the tissue at the focused spot.
  • One way to calculate these corrections is to make a map of sensitivity initially ignoring these effects, and then seeing whether such effects would be important according to that map, and correcting for them, and making a new map. This procedure is repeated until the map changes very little from one iteration to the next.
  • information about the intensity of ultrasound energy at different locations is obtained by measuring the amplitude of higher harmonics .(integer multiples of the transmitted frequency) generated at those locations.
  • data on the induced action potentials from the electrocardiograph, and/or imaging data on the mechanical response to ulfrasound stimulation are used to control the power level of the ultrasound transducers using feedback in real time, instead of or in addition to using this data to make corrections to the applied ultrasound power when analyzing the data afterwards.
  • Fig. 3 is a flowchart showing how the controller analyzes the data from the imaging system and calculates the location (relative to the transducers) of the spot on the heart where the ultrasound energy is to be focused, according to an embodiment of the invention. This is done, for example, using the following steps.
  • a 3D image of the heart is recorded, using the imaging system.
  • image analysis software is used to locate in the image key landmarks on the heart, for example the centers of valves, certain branching points of the coronary artery, certain points at the edge of the septum, etc.
  • the coordinates (relative to the imaging system) of the landmarks are used to calculate the values of a finite set of parameters which substantially characterize the mechanical state of the heart.
  • the parameters comprise three parameters representing the 3D position of the center of the heart, three parameters representing the orientation of the heart in space, and four parameters describing the state of expansion of each chamber of the heart.
  • the values of the parameters are used to calculate the thoracic coordinates of the desired spot, whose location is defined in myocardial coordinates, according to a algorithm worked out in advance.
  • the algorithm is based on a mathematical model of where each point on the heart is located as a function of the different parameters, for example the state of expansion of each chamber.
  • This coordinate transformation algorithm can be verified for human hearts in general, and perhaps some free parameters are calibrated for individual patients. This verification and calibration is done by locating spots on the heart (other than the landmarks) on the image, and seeing whether their location is correctly predicted by the algorithm.
  • the image processing software determines the location (relative to the imaging system) of each point in a 3D grid of points defined in myocardial coordinates, and inte ⁇ olation is then used to find the location of the spot. In effect this procedure would use a much larger set of parameters, but a much simpler coordinate conversion algorithm, than the procedure outlined above.
  • the controller calculates the ultrasound wave phases and amplitudes of the transducers in the array required to direct the ultrasound energy to the spot.
  • the information is optionally used to develop and optimize sequences of cardiac stimulation for pacemaking.
  • Selected spatial and temporal sequences of stimulation are tested or modeled, using ultrasound pulses focused on the desired locations, at the desired times in the cardiac cycle, as determined by the electrocardiograph.
  • more than one location is stimulated at nearly the same instant.
  • the electrocardiograph, and/or the imaging system is used to measure the strength and regularity of the heartbeat, to assess the efficacy of a given sequence for pacemaking, and the sequence is compared to other sequences.
  • one or more other indices are used to evaluate a given sequence, including, for example, systolic pressure, systolic left ventricular volume, diastolic left ventricular volume, and/or ejection fraction.
  • indices are optionally measured by any conventional means, including the use of images or other data from the ultrasonic, or other, imaging system.
  • image analysis is used to calculate one or more of these indices from the images.
  • the indices are determined by a person viewing the images.
  • the ulfrasound system used for stimulating cardiac tissue can also be used to destroy cardiac tissue, for example diseased or arrhythmogenic tissue.
  • Fig. 4 is a flowchart showing the procedure by which tissue is destroyed, according to an exemplary embodiment of the invention.
  • the ultrasound power level, coordinates of the first spot, and phase in the cardiac cycle are chosen.
  • it is possible to track the spot continuously as the heart beats, and to keep ultrasound focused on it throughout the cardiac cycle there are advantages to applying ultrasound power for a time short compared to the cardiac period, and to repeat this at the same phase of the cardiac cycle over several heartbeats if necessary.
  • One advantage is that there may be less error in aiming the ultrasound, since the location of the spot relative to the chest does not vary by that much from one cardiac cycle to the next, at the same phase.
  • Another advantage is that the ultrasound power can be applied to the spot at a phase in the cardiac cycle when the surrounding cardiac tissue is not sensitive to stimulation by ulfrasound.
  • the controller waits for the right phase in the cardiac cycle. Then (304) the heart is imaged, and, as outlined in Fig. 3, the image is used to convert the myocardial coordinates of the chosen spot to thoracic coordinates (306).
  • a pulse of ultrasound energy is transmitted.
  • the power and duration of the pulse are optionally chosen so that it destroys a small amount of tissue, but not enough to do serious damage to the heart if the energy was not focused in exactly the right spot.
  • the heart is imaged again, and the image is examined (312) to verify the destruction of tissue at the intended spot.
  • an ultrasound stimulation sequence is optionally performed to verify that the destruction of tissue at that spot has the expected effect on electrical propagation paths.
  • One well known reason for destroying cardiac tissue, possibly even healthy tissue, is to prevent propagation of action potentials on undesired paths. If the imaging and stimulation test reveal that the goal was accomplished (316), the procedure ends (318).
  • the imaging and/or stimulation test reveal that the ulfrasound energy was not aimed correctly (320), or if the power was too high or too low, then appropriate adjustments are made (322), and the procedure returns to 302 to prepare for transmitting another pulse of ultrasound. If the imaging and/or stimulation test reveal that everything is proceeding as planned (320), but that more tissue needs to be destroyed at the same spot (324), then the procedure also returns to 302. If the procedure is proceeding as planned but the work on that spot is done, then the next spot is chosen, and the power level may be adjusted (322), and the procedure returns to 302.
  • tissue is destroyed by heating it, which can kill it or cause it to disintegrate.
  • tissue is killed by cavitation induced by ultrasound.
  • the tissue is killed directly, for example by ablating it, or indirectly, for example by inducing apoptosis.
  • ultrasound contrast agent is used to increase cavitation effects and/or energy abso ⁇ tion at the site of tissue being killed.
  • ulfrasound stimulation can be used to monitor the killing of cardiac tissue by other means known to the art, such as laser light, radio waves, or ultrasound waves brought to the heart by a cardiac catheter.
  • the words “locations on the heart” as used herein mean locations on the surface of the heart or inside the heart, including within the myocardium.
  • position and orientation when used herein with reference to an imaging system, mean position and orientation of the elements of the imaging system whose position and orientation affect the point of view of the images produced by the imaging system.
  • data analyzer and “image analyzer” as used herein mean any device which analyzes data, including software running on a general pu ⁇ ose computer, and specially designed digital or analog electronic circuits, whether or not it analyzes data in real time, and whether or not it is located in the vicinity or located remotely.
  • analysis results produced by a data analyzer from a data set can include a selection of any or all unchanged pieces of data in the data set, as well as the results of mathematical calculations using the pieces of data in the data set.

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Abstract

An ultrasound cardiac stimulation system comprising: a spatially selective ultrasound source comprising at least one ultrasound transducer located outside the circulatory system; and a controller; where the controller generates an electrical response in the heart by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.

Description

ULTRASOUNDCARDIAC STIMULATOR
FIELD OF THE INVENTION The present invention is related to the field of cardiac diagnosis and therapy. BACKGROUND OF THE INVENTION The myocardium is susceptible to mechanical stimulation: case reports have detailed incidents of cardiac arrest due to a ball or a fist hitting the person's thorax. Physiological studies have reported initiation of an action potential due to a mechanical stimulation such as tapping of the epicardium [Avitall, B., Levine, H. J., Naimi, S., Donahue, R. P., Pauker, S. G., and Adam, D. R., "Local effects of electrical and mechanical stimulation on the recovery properties of canine ventricle," Am. J. Cardiology 50, 263-270 (1982)], or due to stretch. Separately, high energy ultrasound pulses have been reported to shatter kidney stones, while also affecting inner cellular structures and membrane properties. In particular, it has been reported that ultrasound pulses increase membrane permeability and specific ion flow. Ultrasound transducers attached to cardiac catheters have been used to induce electrical activity locally in the heart, for diagnostic purposes. External ultrasound transducers used for imaging have also been observed to induce action potentials in the heart, inadvertently, especially when contrast agents containing small bubbles are injected into the bloodstream. Because of the danger of inducing action potentials in the heart in an uncontrolled way, great care is taken during ultrasound imaging of the heart not to induce action potentials. Direct electrical stimulation of the heart is done for cardiac pacing, usually via electrodes implanted during surgery. Electrical stimulation is also used to measure cardiac response, as a diagnostic, and for this purpose electrodes may be inserted by catheters via the venous or arterial system. Catheters are also used to carry laser or RF or ultrasound energy to specific sites in the heart or elsewhere in the circulatory system, in order to ablate tissue for therapeutic purposes. All of these invasive procedures involve obvious risks and expenses.
Ultrasound energy from external transducer arrays has been focused on tumors in order to destroy them by heating.
SUMMARY OF INVENTION
An aspect of some embodiments of the invention relates to stimulating cardiac tissue, or any other excitable tissue such as muscles and nerves, using ultrasound, for diagnostic and/or therapeutic purposes, using transducers located outside the body, or in the esophagus or other non-invasive body channels, such as the nasal cavities. Optionally, ultrasound contrast agents, for example microbubbles or liposomes, are used to enhance the procedure, for example by increasing the sensitivity of the cardiac tissue to stimulation.
In some embodiments of the invention, an imaging system is used to track and observe the heart before, during, and/or after the cardiac tissue is stimulated. This is done, for example, in order to observe the local or global mechanical response of the heart to the stimulation, or to focus the ultrasound energy on the correct spot. Optionally, the imaging system is an ultrasound imaging system, using the same transducers as are used for stimulation. Alternatively or additionally, other ultrasound transducers may be used for imaging. Alternatively or additionally, a Computer Aided Tomography system using x-rays, a Magnetic Resonance Imaging system, or any imaging system known to the art may be used. Optionally, contrast agents are used to improve image quality, and/or to distinguish between perfused and non- perfused tissue.
In some embodiments of the invention, the location and orientation of the heart, or a particular point on the heart, are tracked in real time while ultrasound is used to stimulate the heart. Such tracking makes it possible to repeatedly focus ultrasound on the same spot in the heart, or to successively focus ultrasound on two or more spots with known relative positions.
In some embodiments of the invention, ultrasound waves are focused on one small spot in the heart, to stimulate the tissue, and the response to stimulation is observed. This stimulation spot can be deep inside the myocardium, as well as on the exterior or interior surface of the heart. Optionally, after a period of time, the ultrasound waves are focused on a different stimulation spot. Alternatively or additionally, the ultrasound waves are focused on more than one stimulation spot simultaneously, or nearly simultaneously relative to the speed of propagation of signals in the heart. For each stimulation spot or set of stimulation spots, measurements are optionally made of the intensity and duration of ultrasound needed to induce action potentials, either propagating or non-propagating, and the spatial distribution of the potential is optionally measured, as a function of time. The mechanical response of tissue to action potentials is optionally measured as a function of time, for example by observing changes in thickness and motion of the cardiac wall, at the stimulation spot and at other spots.
In an exemplary embodiment of the invention, the following configuration is used. The ultrasound source is aimed at a particular location in the heart and its firing is synchronized to the cardiac cycle, for example, using an ECG (which may provide local electrical information) or using an analysis of a series of images. The analysis may be automatic or manual, for example. The imager is also aimed at the particular location and/or at a location where an effect of the excitation is expected and/or is desired to be studied. Optionally, the imager is closely synchronized with the stimulating ultrasound, which may make it easier to detect the short-term mechanical response of the heart tissue to the ultrasound. It may also be possible to detect the motion of the heart wall due to the pressure of the ultrasound. In operation, the imager can detect the exact location of excitation (even if the aiming is not precise), for example, by detecting non-linear effects at the location. In addition, the imager can capture a development of mechanical response to the excitation, over a period of time, due to the action potential. Further, this detected response may be synchronized with a measurement of electrical activity from outside the body (e.g., using a high resolution ECG) or from inside the body (e.g., using a catheter). It should be noted that in this manner a map having a resolution better than the aiming ability can be created, by marking the map with the actual excitation signal location. In any case, the analysis of the detected response and the ECG may be manual or automatic. For example, the mechanical response to the action potential is found automatically by using image analysis software to measure changes in wall thickness. When this measurement is synchronized to a local ECG, a delay in mechanical response is calculated.
The results of these measurements are optionally used for identifying ischemic tissue that is permanently damaged, and distinguishing it from tissue that is stunned or hibernating but could be revived. Tissue that is overly sensitive to stimulation, and could give rise to arrhythmias, may also be identified. Maps of the location of healthy and pathological tissue in the heart are used in some embodiments of the invention to design spatial and temporal sequences of stimulation that are optimal for pacemaking. Optionally, such sequences are tested and compared using ultrasound stimulation. Optionally, some tissue is ablated by ultrasound, or by other means as known in the art.
In some embodiments of the invention, ultrasound is used to increase membrane permeability at particular locations in the heart and/or particular times in the cardiac cycle, in order to selectively increase the absorption or effect of drugs at those locations and/or times. Optionally, the drugs are delivered to specific locations by a cardiac catheter.
In some embodiments of the invention, a phased array of transducers is used to generate the focused ultrasound pulses. Alternatively or additionally, a single transducer with focusing is used. Optionally, the transducers are placed on the outside of the chest. To avoid having the ultrasound energy blocked by the ribs, the transducers optionally are placed between the ribs. Additionally or alternatively, the transducers are placed on the sternum, or below the rib cage. Additionally or alternatively, the transducers are placed non-invasively inside the body, for example in the esophagus.
In some embodiments of the invention, ultrasound pulses are used to provide temporary pacing of the heart, for example when a conventional pacemaker is temporarily not operating, or during bradycardia. Optionally, different temporal and spatial sequences of ultrasound pulses are tested and compared, in order to find the best sequence to use for pacing. The different sequences are evaluated using, for example, electrocardiograph data, systolic pressure measurements, and/or images showing the mechanical response of the heart, including systolic and diastolic left ventricular volume and ejection fraction. In some embodiments of the invention, a cardiac catheter is used to provide direct electrical simulation of the heart, in addition to the stimulation by ultrasound. Direct electrical stimulation may help to identify tissue pathologies by comparing its effects to the effects of mechanical stimulation by ultrasound. In one example, such a comparison is used to distinguish stunned from hibernating myocardium. In another example, the ultrasound pulses are focused at a coarse, resolution, and used to produce a coarse map of pathological tissue, and a cardiac catheter is used to map certain regions more precisely. The imaging system is optionally used to determine the precise location of the cardiac catheter. In addition to or instead of electrically stimulating the heart, the catheter optionally is used to ablate or otherwise kill cardiac tissue, optionally monitoring the process with the imaging system. This killing is done by any means known to the art. For example the catheter brings electric power to an ohmic or inductive heating element, a refrigerating element, an ultrasound transducer or a radio frequency transmitter in the circulatory system, or the catheter carries laser light on a fiber optic cable, or carries a drug.
There is thus provided, in accordance with an embodiment of the invention, an ultrasound cardiac stimulation system comprising: a spatially selective ultrasound source comprising at least one ultrasound transducer located outside the circulatory system; and a controller; wherein the controller generates an electrical response in the heart by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.
Optionally, there is an injector which injects cardiac drugs into the bloodstream, and the controller changes the rate at which cardiac tissue absorbs the drugs by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.
Optionally, the controller is operative to choose the ultrasound power level.
In an embodiment of the invention, the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ±20%.
Optionally, the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ±10%.
Optionally, the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ±3%. In an embodiment of the invention, an injector which injects one or both of drugs for treating the heart and contrast agents into the bloodstream.
Optionally, the controller is operative to reduce the power level of ultrasound when the contrast agents are injected.
In an embodiment of the invention, the controller is operative to choose the one or more locations to which the ultrasound is transmitted.
Optionally, the controller controls the ultrasound source to direct ultrasound energy to a designated location, and the point of highest power flux density falls within an axial precision of 3 mm of said designated location.
Alternatively, the axial precision is 1.5 mm. Optionally, the point of highest power flux density remains within the axial precision of the designated location for at least 1 millisecond.
Optionally, the point of highest power flux density remains within the axial precision of the designated location for at least 10 milliseconds.
Optionally, the controller controls the ultrasound source to direct ultrasound energy to a designated location, and the point of highest power flux density falls within a transverse precision of 1 mm of said designated location.
Alternatively, the transverse precision is 0.5 mm.
Optionally, the point of highest power flux density remains within the transverse precision of the designated location for at least 1 millisecond. Optionally, the point of highest power flux density remains within the transverse precision of the designated location for at least 10 milliseconds. In an embodiment of the invention, the controller controls the ultrasound source to direct a high enough power level of ultrasound to one or more locations in the heart to kill cardiac tissue by heating it.
Alternatively or additionally, the controller controls the ultrasound source to direct a high enough power level of ultrasound to one or more locations in the heart to kill cardiac tissue by cavitation.
In an embodiment of the invention, there is an electrocardiograph which measures the timing of the cardiac cycle.
Optionally, the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating in any one chamber of the heart, from the electrical response originating in any other chamber of the heart.
Optionally, the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating in one side of any chamber of the heart, from the electrical response originating in the other side of said chamber of the heart. Optionally, the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one centimeter away from said location.
Optionally, the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one millimeter away from said location.
Optionally, the system uses feedback from the electrocardiograph to control the ultrasound power level.
In an embodiment of the invention, the controller is operative to make a map of the heart, showing the ultrasound power flux required to generate the electrical response at each of several locations in the heart.
Optionally, the controller is operative to direct the ultrasound source to transmit a first sequence of timed localized pulses of ultrasound energy to the heart, and a second such sequence which differs from the first sequence in one or both of timing and location of the pulses, and the controller is operative to collect a first data set showing the effects of the first sequence on the heart, and a second data set showing the effects of the second sequence on the heart.
Optionally, the first data set and the second data set comprise data from the electrocardiogram. Optionally, there is a memory which is operative to store the first data set and the second data set, a data analyzer which is operative to analyze data and produce analysis results from the first data set and the second data set, and a display which displays the analysis results.
Optionally, the first data set and the second data set comprise data on systolic pressure. Optionally, the first sequence and the second sequence differ in timing of the pulses.
Alternatively or additionally, the first sequence and the second sequence differ in location of the pulses.
In an embodiment of the invention, there is a cardiac imaging system which produces images showing the position of one or more locations on the heart. Optionally, the first data set and the second data set comprise data from the cardiac imaging system.
Optionally, there is an image analyzer which analyzes images produced by the cardiac imaging system for the first sequence and the second sequence, and calculates one or more of the systolic left ventricular volume for the first and second sequence, the diastolic left ventricular volume for the first and second sequence, and the ejection fraction for the first and second sequence.
Optionally, the images produced by the imaging system show the mechanical response of the heart to stimulation produced by the ultrasound.
Optionally, the imaging system is in a fixed position and orientation with respect to the ultrasound source.
Alternatively or additionally, there are sensors which determine the relative position and orientation of the imaging system and the ultrasound source.
Alternatively or additionally, the imaging system determines the relative position and orientation of the ultrasound source by imaging it. Optionally, the controller coordinates the timing of the imaging system with the timing of the ultrasound source.
Optionally, the controller is operative to make a map of the heart, using data from the imaging system, showing the mechanical response of the heart at one or more locations to ultrasound energy transmitted to one or more locations. Optionally, the system uses feedback from the imaging system to control the ultrasound power level.
Optionally, the imaging system uses ultrasound imaging. Optionally, the imaging system shares one or more ultrasound transducers with the ultrasound source used to generate the electric response in the heart.
Alternatively, the imaging system does not share any ultrasound transducers with the ultrasound source used to generate the electric response in the heart. Alternatively or additionally, the imaging system comprises a computerized tomography x-ray imaging system.
Alternatively or additionally, the imaging system comprises a magnetic resonance imaging system.
Optionally, there is image processing software which analyzes the images to determine the position of one or more locations on the heart.
Optionally, the image processing software determines the position of one or more locations on the heart in real time during a cardiac cycle.
Optionally, the confroller coordinates the timing of the transmission of ultrasound with the cardiac cycle. In an embodiment of the invention, there is a cardiac catheter which generates an electrical response in the heart, and a calibration mode of the confroller, wherein the controller, when it is in the caUbration mode, calibrates the ultrasound power transmitted to the heart by the ultrasound array, by comparing a physiological response induced by the ultrasound array to a physiological response induced by the catheter. Optionally, the physiological responses compared by the controller comprise electrical responses.
Alternatively or additionally, the physiological responses compared by the controller comprise mechanical responses.
Optionally, the cardiac catheter generates an electrical response by direct electric stimulation.
Alternatively or additionally, the cardiac catheter comprises an internal ultrasound transducer, and the cardiac catheter generates an electrical response by transmitting ultrasound.
In an embodiment of the invention, the cardiac catheter kills cardiac tissue.
Optionally, the cardiac catheter comprises a light guide, and the light guide carries light from the laser, which light kills cardiac tissue.
Optionally, the ultrasound source comprises a phased array of the ultrasound transducers. Optionally, at least one of the at least one ultrasound transducers is adapted for use on the surface of the body.
Optionally, the at least one ultrasound transducers comprise at least two ulfrasound transducers, sized and spaced so that they can be placed between the ribs, in such a way as to avoid blocking of ultrasound by the ribs .
Alternatively or additionally, at least one of the at least one ultrasound transducers is adapted for use in the esophagus.
Alternatively or additionally, at least one of the at least one ultrasound transducers is adapted for use in a nasal cavity. Optionally, the ultrasound source and the controller are operative to direct the ultrasound energy with 90% of the power flux falling within 3 mm transversely of the point of highest power flux density.
Alternatively or additionally, the ultrasound source and the controller are operative to direct the ultrasound energy with 90% of the power flux falling within 1.5 mm transversely of the point of highest power flux density.
Alternatively or additionally, the ultrasound source and the confroller are operative to direct the ultrasound energy with 90% of the power flux falling within 1 mm transversely of the point of highest power flux density.
Optionally, the ultrasound source and the confroller are operative to direct the ultrasound energy with the power flux spreading out to 50% of its highest density within 6 mm axially of the point of highest power flux density.
Alternatively or additionally, the ultrasound source and the controller are operative to direct the ultrasound energy with the power flux spreading out to 50% of its highest density within 3 mm axially of the point of highest power flux density. Alternatively or additionally, the ultrasound source and the controller are operative to direct the ultrasound energy with the power flux spreading out to 50% of its highest density within 1.5 mm axially of the point of highest power flux density.
Optionally, the ultrasound source and the controller are operative to direct the ultrasound energy with a power flux density greater than 30 watts per square centimeter at the point of highest power flux density.
Alternatively or additionally, the ultrasound source and the controller are operative to direct the ulfrasound energy with a power flux density greater than 100 watts per square centimeter at the point of highest power flux density. Alternatively or additionally, the ultrasound source and the controller are operative to direct the ulfrasound energy with a power flux density greater than 300 watts per square centimeter at the point of highest power flux density.
Optionally, the ultrasound source and the controller are operative to direct the ultrasound energy in a pulse lasting less than 10 milliseconds.
Alternatively or additionally, the ultrasound source and the controller are operative to direct the ultrasound energy in a pulse lasting less than 1 millisecond.
Optionally, the ultrasound source and the controller are operative to direct the ultrasound energy in a pulse lasting for a duration within 10% of a duration for which the controller is directed to direct the energy.
Optionally, the ultrasound source and the controller are operative to direct the ultrasound energy at a frequency greater than 0.5 megahertz and less than 6 megahertz.
There is thus also provided a method of changing a cardiac stimulation sequence for a patient, comprising: a) choosing a test sequence of locations in the heart of the patient, and a time in the cardiac cycle to stimulate each location; b) stimulating the test sequence of locations at the chosen times in the cardiac cycle, using an ultrasound cardiac stimulation system from outside the heart; c) evaluating a change in cardiac synchronization of the patient associated with the test sequence; d) choosing a stimulation sequence for a pacemaker, based at least partly on the change in cardiac synchronization that the test sequence produces; and e) changing a stimulation sequence of the heart to conform to the chosen stimulation sequence. In an embodiment of the invention, using an ultrasound cardiac stimulation system from outside the heart comprises using an ultrasound stimulation system from outside the body.
Optionally, changing a stimulation sequence of the heart comprises installing a pacemaker.
Alternatively or additionally, changing a stimulation sequence of the heart comprises adjusting a pacemaker.
Optionally, adjusting a pacemaker comprises programming a pacemaker. Optionally, adjusting a pacemaker comprises adjusting a pacemaker to obtain improved cardiac synchronization. In an embodiment of the invention, (a), (b) and (c) are performed a plurality of times for different test sequences, and choosing an optimal stimulation sequence is based at least partly on the change in a measure of cardiac performance that the different test sequences produce. Optionally, the measure of cardiac performance comprises cardiac output. Optionally, evaluating the change in the measure of cardiac performance comprises using systolic pressure measurements.
Alternatively or additionally, evaluating the change in the measure of cardiac performance comprises using images of a mechanical response of the heart to the stimulation. Optionally, at least one of the test sequences comprises a plurality of locations with the same chosen time.
Optionally, evaluating the change in cardiac synchronization comprises using electrocardiograph data.
BRIEF DESCRIPTION OF THE DRAWINGS
Exemplary embodiments of the invention are described in the following sections with respect to the drawings. The drawings are generally not to scale. The same or similar reference numbers are used for the same or related features on different drawings. Features found in one embodiment can also be used in other embodiments, even though all features are not shown in all drawings.
Fig. 1 is a schematic cross-sectional view of the chest and heart, showing ultrasound systems used for stimulating the heart, according to an exemplary embodiment of the invention; Fig. 2 is a flowchart illustrating how a map is made of the sensitivity of the heart to stimulation by ultrasound pulses;
Fig. 3 is a flowchart showing how the imaging system is used to track the location of different spots on the heart in real time; and Fig. 4 is a flowchart showing how cardiac tissue is destroyed, while the effects are monitored.
DETAILED DESCRIPTION OF EXEMPLARY EMBODIMENTS Fig. 1 schematically shows an ulfrasound system according to an exemplary embodiment of the invention. A heart 10 is shown in a cross-section of a patient's chest 12. A phased array 14 of ultrasound transducers focuses ultrasound waves 16 on a spot 18 in the wall of the heart, stimulating cardiac tissue at that spot and possibly inducing action potentials, detected by an electrocardiograph 20. By adjusting the relative phases and amplitudes of the different transducers in the array, the ulfrasound can generally be focused on any desired spot 18. Alternatively, any other method of focusing ultrasound known to the art is used to focus the ulfrasound waves on spot 18. The diameter of the spot cannot be much smaller than one wavelength, assuming that it is in the far field of the transducers, i.e. at least several wavelengths away from the transducers. If it is desired to focus the ultrasound on a region much smaller than the thickness of the myocardium, the frequency of the ultrasound optionally has a frequency approximately 1 MHz or higher, which would have a wavelength in the body of about 1.5 mm or less. Ultrasound transducers exist which can operate at frequencies as high as 10 MHz. If the frequency is too high, however, and the desired focused spot is not close enough to the transducers, then the ultrasound will be largely absorbed before reaching the desired spot, and higher fransducer power or more transducers will be needed to produce the same ultrasound power flux at the spot. Typically, frequencies between 0.5 and 6 MHz are used, and the focused spot is elliptical, 1 to 2 mm in diameter and 4 to 6 mm in length in the direction of propagation, with the acoustic pressure outside the spot significantly lower than the peak pressure. Focused spots with dimensions greater or smaller than these values, for example 0.5 mm to 4 mm in diameter and 2 mm to 10 mm in length, are also optionally used. Peak acoustic pressures are typically 2 to 4 MPa, corresponding to powers of 125 to 500 watts per square centimeter, and pulse lengths are typically 1 to 10 milliseconds long. However, optionally ultrasound pulses with frequencies, powers and pulse lengths of 1 to 5 MPa, corresponding to 30 to 800 watts per square centimeter, or even greater than or less than this range, are used.
Transducer array 14 is shown outside the chest in Fig. 1. To avoid the problem of ultrasound waves reflecting from the ribs, which have a very different acoustic impedance than the soft parts of the body, the transducers are optionally placed between the ribs, or below the rib cage. Alternatively, they are placed inside the chest, in the esophagus. An imaging system 22 is used to determine the position and orientation of the heart, relative to transducer array 14, so that ultrasound energy can be accurately focused on a desired spot on the heart by transducer array 14. Although Fig. 1 shows an imaging system that is separate from fransducer array 14, optionally transducer array 14 is used for an ultrasound imaging system, as well as for stimulating cardiac tissue. In this case, ultrasound waves for imaging purposes are optionally transmitted alternately with ultrasound waves for cardiac stimulation. If the imaging waves and stimulating waves are transmitted close enough together in time, then the heart will not move very much, and the information from the imaging system can still be used to accurately focus the stimulating waves. Alternatively or additionally, the stimulating waves themselves are used for imaging. The imaging system need not be an ultrasound imaging system. It could be an x-ray CAT system, or an MRI system, or any other medical imaging system known to the art.
If imaging system 22 is not an ultrasound imaging system using the same transducer array 14 that is used for stimulation, then it may be desirable to know the relative position and orientation of imaging system 22 and transducer array 14. Ultrasound can then be used to stimulate a spot whose position is defined by imaging system 22, and imaging system 22 can image a spot that has been stimulated, observing the effects of the stimulation. Optionally, transducer array 14 is rigidly connected to imaging system 22, so that they always have the same relative position and orientation. Alternatively, there are sensors mounted on transducer array 14, imaging system 22, or both of them, which sense the relative position and orientation of transducer array 14 and imaging system 22. Alternatively, imaging system 22 determines the relative position and orientation of transducer array 14 by imagining it. This option is especially useful when transducer array 14 is in the esophagus. A computer 24 controls the phase, amplitude, and timing of ultrasound waves emitted by the transducers in transducer array 12, using input from the human operator, the imaging system, and the electrocardiograph. Details of how this is done, according to an embodiment of the invention, are given in Fig. 2. Computer 24 could comprise an general purpose computer running appropriate software, or custom-designed control circuitry, or a combination of the two.
Fig. 1 schematically shows an intravenous tube 26, which is used to introduce contrast agents into the bloodstream, during ultrasound stimulation. Contrast agents, which are encapsulated small gas bubbles, significantly attenuate the propagating ultrasound energy, reflecting, scattering and absorbing it. The contrast agent bubbles oscillate and sometimes burst, producing exfremely high pressures locally. This enhances the stimulating effect of ultrasound on cardiac tissue. As a result, lower power transducers can be used to produce the same stimulation effect, and there may be less heating of tissue for the same stimulation effect. Contrast agents are also useful in imaging, for example for showing the precise boundaries of tissue with normal perfusion of blood and regions with reduced or no perfusion. Alternatively or additionally, intravenous tube 26 is used to introduce drugs into the bloodstream during ulfrasound stimulation of the heart. Since ultrasound stimulation can increase the permeability of cell membranes, certain locations in the heart will be induced to take up drugs from the bloodstream, more than other regions that are not stimulated. The uptake of drugs can also be timed to occur at certain times in the cardiac cycle, if the ultrasound stimulation is gated with an electrocardiograph. Alternatively or additionally, the contrast agents and/or the drugs can be introduced into the heart by a cardiac catheter, rather than intravenously, allowing additional control over the spatial and temporal distribution of the contrast agents and/or drugs.
Fig. 2 is a flowchart showing how the transducer array is used to map regions of healthy and pathological tissue in the heart, according to an exemplary embodiment of the invention. Tissue is optionally classified as healthy or pathological according to one or more of several criteria, for example: • Ultrasound power level required to induce an action potential
• Time delay after ultrasound energy is applied, before action potential appears
• Refractory period after action potential is induced, before another action potential can be induced
• Magnitude and delay of mechanical response to action potential • Amplitude and duration of action potential
The flowchart in Fig. 2 illustrates only how the first criterion, ultrasound power level required to induce an action potential, is mapped, but optionally any one or combination of these criteria are used to make a map. Using only the first criterion, the map identifies regions which are more susceptible than normal, or less susceptible than normal, to producing extra action potentials (beyond those associated with the regular heartbeat) when stimulated by ultrasound. Such a map can reveal the location of ischemic tissue, which typically requires higher than normal ultrasound levels to produce an action potential, and/or tissue which is susceptible to arrhythmias, which may require a lower than normal ultrasound level to produce an action potential. The steps shown in the flowchart in Fig. 2 are optionally performed by a controller, for example a computer with an interface to the human operator. At 100, the initial step in the flowchart, a region is chosen for mapping, either the whole heart or a part of the heart, and the range of ultrasound power levels is optionally chosen. This range starts at a level well below the power that would be needed to induce an action potential in normal tissue, and ends at a level above the power that would be needed to induce an action potential in normal tissue, but optionally not at such a high level that the tissue could be damaged by heating or cavitation. The region for mapping is optionally chosen by the operator as a range of myocardial coordinates, defined in relation to the heart tissue, i.e. a given point on the heart has constant myocardial coordinates even while its absolute position is changing because the heart is beating. Alternatively, the range could be chosen by the operator by dragging a mouse across a 3-D displayed image of the heart (for example, a series of 2-D cross-sections) frozen at a particular phase in the cardiac cycle. Optionally, in addition to choosing a range of positions and powers, a phase in the cardiac cycle, or a set of phases, is also chosen for mapping. The response of tissue to stimulation generally depends on the phase in the cardiac cycle at which the stimulation is applied. Optionally, instead of setting the range of positions, powers, and phase initially, they are chosen or changed during the procedure.
In 102 and 104, the myocardial coordinates of the spot to be stimulated are set at the first point on the grid to be mapped, and the power is set at the bottom of the range. In 105, the confroller waits for the desired phase in the cardiac cycle, using electrocardiograph data, for example, to determine at what time the desired phase occurs. In 106, a quick image, which need not have high resolution, is made of the heart, in order to locate the absolute position (relative to the transducers) of the spot to be stimulated. Making an error in location of the focused spot is potentially dangerous, since a high power ultrasound pulse intended for an insensitive spot could be focused by mistake on a very sensitive area and induce fibrillation. In 108 and 110, the image made in 106 is used to determine the orientation and location of the heart, and this information is used to convert the myocardial coordinates of the point being stimulated to thoracic coordinates, defined relative to the chest cavity (and hence to the transducers, which are optionally pressed against the outside of the chest). Some details of how this calculation is done are given below in the description of Fig. 3. If the imaging and calculation could be done in less than 50 milliseconds, or better yet in less than 10 milliseconds, then the heart would move very little between the time it is imaged and the time the ultrasound energy is applied for stimulation. Alternatively, instead of performing 106, 108 and 110, the range of points to be mapped is directly defined in terms of thoracic coordinates at a particular phase in the cardiac cycle, and the ulfrasound energy is always applied at the same phase in the cycle. A disadvantage of this alternative method is that there could be variations in position and orientation of the heart from one heartbeat to the next.
If the ulfrasound transducers are located in the esophagus rather than on the outside of the chest, then it may not be sufficient just to define the position of the point to be mapped in thoracic coordinates. In addition, it may be necessary to take into account changes in position of the fransducers relative to the chest cavity. Optionally this is done by using an external imaging system to locate the position of the stimulating fransducers in the esophagus. Alternatively, if the same fransducers are used for stimulation and imaging, then those transducers can be used directly to find the location of the heart (or of the desired point on the heart) relative to the fransducers.
In 112, the stimulating ultrasound energy is focused on the desired spot on the heart. As described above in the description of Fig. 1, this is optionally done by first using a computer to calculate the phases and amplitudes of the fransducers in the array, needed to focus ultrasound energy on the desired spot. In 114, a cine (moving) image is optionally made of the heart, in order to assess the mechanical response of the heart, if any, to the stimulation. Optionally, instead of storing the entire cine image, the image is processed to track only a limited set of points on the heart, sufficient to characterize the mechanical response of the heart, and only these results are stored. If the imaging system does not use the transducers used for stimulation, then the cine imaging optionally begins before the stimulation is applied, and continues while the stimulation is applied and for a given period afterwards. Even if the same transducers are used for imaging and stimulation, the cine imaging optionally begins before the stimulation, and is briefly interrupted while the transducers are used for stimulation, and resumed afterwards. Optionally the cine image or a still image is precisely synchronized with the ultrasound stimulation, and is used to detect the short-term mechamcal response of the heart tissue to the ultrasound stimulation, which may provide more information about the exact location of the ultrasound stimulation. At 116, the confroller examines data, for example from an electrocardiograph, to determine whether the ulfrasound stimulation induced an action potential, beyond the action potential that already existed as part of the natural cardiac cycle. The electrocardiograph provides some information about the spatial distribution of action potentials, as well as their amplitude and time dependence. Optionally, the electrocardiograph is calibrated before it is used to measure induced action potentials, for example by comparing the induced action potentials to the regular action potential. If no extra action potential is observed, and if the power level is not yet at the top of the chosen range (118), then the power is raised to the next level (120), and the flow goes back to 105, in preparation for a new application of ultrasound energy at the same spot. If the power was already at the maximum level, then this spot is recorded as unresponsive (124), and the flow goes to 132.
Optionally, instead of starting at the lowest power level and increasing the power one step at a time, the power starts at the middle of the range, at a level that has a 50% chance of exciting an action potential, according to some model. If an action potential is seen, then the power is lowered to a level that now has a 50% chance of eliciting an action potential, taking into account the previous results. If an action potential is not seen, then the power is raised to a level that now has a 50% chance of eliciting an action potential, taking into account the previous results. This procedure is continued until the exact threshold for eliciting an action potential is found, to the desired precision. This "zeroing in" procedure has an advantage over the "one step at a time" procedure, in that the number of steps required scales as the logarithm of the desired precision, rather than scaling linearly with the desired precision. A disadvantage of the "zeroing in" procedure is that it might overstimulate a very sensitive spot, causing fibrillation. Many other procedures are possible for determining the threshold for eliciting action potentials, which will be apparent to persons skilled in the art.
If an extra action potential was seen, then the data is examined to see whether the action potential is propagating, and how it propagates (126). This information is recorded (128), and (130) any mechanical response is assessed (based on the cine image made in 114, for example), and recorded. Optionally, image processing software is used to assign one or more quantitative values to characterize the mechanical response. Alternatively or additionally, the mechanical response could be characterized by the operator after viewing the cine image. Alternatively or additionally, the cine image for each spot is stored, and the mechanical response is evaluated at leisure after the map of action potential threshold is completed.
At 132, if all spots in the grid have not been examined, then (134) the myocardial coordinates are set for the next spot in the grid, and the flow goes back to 104. Once all spots in the grid have been examined, the procedure ends (136). The recorded data on the ultrasound power threshold needed to induce an action potential at each point, and on the propagation of induced action potentials, are then used to create one or more maps, for example using postprocessing software. The maps could show the propagation paths, as well as the action potential threshold at each spot. The accuracy of the map showing action potential thresholds will be confirmed if it is consistent with the map of propagation paths, for example if it shows that regions that are resistant to inducing action potentials are also regions that block propagation of action potentials induced elsewhere.
Although the flowchart in Fig. 2 assumes that ulfrasound stimulation is only applied at one phase in the cardiac cycle, optionally a map could be made for each of several phases. For example, instead of ending the procedure at 136, the controller could change the phase and loop back to 102, until all desired phases were examined. Alternatively, the phase could be changed in an inner loop. For example, at each power level, for each spot, ulfrasound stimulation could be done at each of several different phases. Optionally, once an action potential is observed, the controller moves to the next spot. This procedure produces a map of the minimum power needed to induce an action potential at the most sensitive phase in the cardiac cycle. Alternatively, the power threshold for inducing an action potential is measured for each of several phases at each spot.
In making the map, corrections to the ultrasound power level are optionally made taking into account absorption of ulfrasound energy between the transducers and the focused spot. The amount of absoφtion may be estimated by using known values for absorption lengths of ultrasound at the frequency used, in different types of tissue. Alternatively or additionally, absoφtion may be measured by using data from the imaging system, if it is an ultrasound imaging system, or by detecting stimulating ulfrasound waves reflected back to the fransducers. For example, images can be compared at lower ultrasound frequency, where there is less absoφtion, and higher frequency where there is more absoφtion, in order to calibrate the amount of absoφtion at the frequency used for stimulation. In some embodiments of the invention, the ultrasound power flux focused on a given spot in the heart is controlled to within 10%, taking into account errors in the powers and phases of the transducers, and uncertainties in the amount of power that is absorbed between the transducers and the focused spot. Alternatively, the power is controlled only to within 20%, or to within better than 3%.
Corrections are also optionally made to the map by taking into account the finite amplitude of ulfrasound at locations other than the focused spot, which can be calculated from the size, spacing, and number of transducers in the array, and by modeling reflections and refraction of ultrasound waves. Such a spatial distribution of the ultrasound intensity could stimulate action potentials first at those other locations, if the tissue there is much more sensitive than the tissue at the focused spot. One way to calculate these corrections is to make a map of sensitivity initially ignoring these effects, and then seeing whether such effects would be important according to that map, and correcting for them, and making a new map. This procedure is repeated until the map changes very little from one iteration to the next. Alternatively or additionally, information about the intensity of ultrasound energy at different locations is obtained by measuring the amplitude of higher harmonics .(integer multiples of the transmitted frequency) generated at those locations.
Optionally, data on the induced action potentials from the electrocardiograph, and/or imaging data on the mechanical response to ulfrasound stimulation, are used to control the power level of the ultrasound transducers using feedback in real time, instead of or in addition to using this data to make corrections to the applied ultrasound power when analyzing the data afterwards.
Fig. 3 is a flowchart showing how the controller analyzes the data from the imaging system and calculates the location (relative to the transducers) of the spot on the heart where the ultrasound energy is to be focused, according to an embodiment of the invention. This is done, for example, using the following steps. At 200, a 3D image of the heart is recorded, using the imaging system. At 202, image analysis software is used to locate in the image key landmarks on the heart, for example the centers of valves, certain branching points of the coronary artery, certain points at the edge of the septum, etc. At 204, the coordinates (relative to the imaging system) of the landmarks are used to calculate the values of a finite set of parameters which substantially characterize the mechanical state of the heart. For example, the parameters comprise three parameters representing the 3D position of the center of the heart, three parameters representing the orientation of the heart in space, and four parameters describing the state of expansion of each chamber of the heart. At 206, the values of the parameters are used to calculate the thoracic coordinates of the desired spot, whose location is defined in myocardial coordinates, according to a algorithm worked out in advance. The algorithm is based on a mathematical model of where each point on the heart is located as a function of the different parameters, for example the state of expansion of each chamber. This coordinate transformation algorithm can be verified for human hearts in general, and perhaps some free parameters are calibrated for individual patients. This verification and calibration is done by locating spots on the heart (other than the landmarks) on the image, and seeing whether their location is correctly predicted by the algorithm.
Other procedures may be used to accomplish the same result. For example, instead of only locating a small set of landmarks on the image, the image processing software determines the location (relative to the imaging system) of each point in a 3D grid of points defined in myocardial coordinates, and inteφolation is then used to find the location of the spot. In effect this procedure would use a much larger set of parameters, but a much simpler coordinate conversion algorithm, than the procedure outlined above.
Once the coordinates of the spot are known, the controller calculates the ultrasound wave phases and amplitudes of the transducers in the array required to direct the ultrasound energy to the spot.
Once a map has been made of the sensitivity of the cardiac tissue to stimulation, or of other properties such as delay time of action potentials or refractory time, the information is optionally used to develop and optimize sequences of cardiac stimulation for pacemaking. Selected spatial and temporal sequences of stimulation are tested or modeled, using ultrasound pulses focused on the desired locations, at the desired times in the cardiac cycle, as determined by the electrocardiograph. Optionally, more than one location is stimulated at nearly the same instant. Optionally, the electrocardiograph, and/or the imaging system, is used to measure the strength and regularity of the heartbeat, to assess the efficacy of a given sequence for pacemaking, and the sequence is compared to other sequences. Additionally or alternatively, one or more other indices are used to evaluate a given sequence, including, for example, systolic pressure, systolic left ventricular volume, diastolic left ventricular volume, and/or ejection fraction. (These indices are optionally measured by any conventional means, including the use of images or other data from the ultrasonic, or other, imaging system. Optionally, image analysis is used to calculate one or more of these indices from the images. Alternatively or additionally, the indices are determined by a person viewing the images.) Once an effective sequence is found, a pacemaker using direct electrical stimulation can be programmed and implanted to produce the most effective stimulation sequence.
The ulfrasound system used for stimulating cardiac tissue can also be used to destroy cardiac tissue, for example diseased or arrhythmogenic tissue. Fig. 4 is a flowchart showing the procedure by which tissue is destroyed, according to an exemplary embodiment of the invention. Initially, at 300, the ultrasound power level, coordinates of the first spot, and phase in the cardiac cycle are chosen. Although it is possible to track the spot continuously as the heart beats, and to keep ultrasound focused on it throughout the cardiac cycle, there are advantages to applying ultrasound power for a time short compared to the cardiac period, and to repeat this at the same phase of the cardiac cycle over several heartbeats if necessary. One advantage is that there may be less error in aiming the ultrasound, since the location of the spot relative to the chest does not vary by that much from one cardiac cycle to the next, at the same phase. Another advantage is that the ultrasound power can be applied to the spot at a phase in the cardiac cycle when the surrounding cardiac tissue is not sensitive to stimulation by ulfrasound. In 302, the controller waits for the right phase in the cardiac cycle. Then (304) the heart is imaged, and, as outlined in Fig. 3, the image is used to convert the myocardial coordinates of the chosen spot to thoracic coordinates (306). In 308 a pulse of ultrasound energy is transmitted. The power and duration of the pulse are optionally chosen so that it destroys a small amount of tissue, but not enough to do serious damage to the heart if the energy was not focused in exactly the right spot. In 310, the heart is imaged again, and the image is examined (312) to verify the destruction of tissue at the intended spot. In addition (314), an ultrasound stimulation sequence is optionally performed to verify that the destruction of tissue at that spot has the expected effect on electrical propagation paths. One well known reason for destroying cardiac tissue, possibly even healthy tissue, is to prevent propagation of action potentials on undesired paths. If the imaging and stimulation test reveal that the goal was accomplished (316), the procedure ends (318). If the imaging and/or stimulation test reveal that the ulfrasound energy was not aimed correctly (320), or if the power was too high or too low, then appropriate adjustments are made (322), and the procedure returns to 302 to prepare for transmitting another pulse of ultrasound. If the imaging and/or stimulation test reveal that everything is proceeding as planned (320), but that more tissue needs to be destroyed at the same spot (324), then the procedure also returns to 302. If the procedure is proceeding as planned but the work on that spot is done, then the next spot is chosen, and the power level may be adjusted (322), and the procedure returns to 302.
Optionally, tissue is destroyed by heating it, which can kill it or cause it to disintegrate. Alternatively or additionally, tissue is killed by cavitation induced by ultrasound. In either case, the tissue is killed directly, for example by ablating it, or indirectly, for example by inducing apoptosis. Optionally, ultrasound contrast agent is used to increase cavitation effects and/or energy absoφtion at the site of tissue being killed.
Instead of or in addition to using ulfrasound energy from external transducers to kill cardiac tissue, ulfrasound stimulation can be used to monitor the killing of cardiac tissue by other means known to the art, such as laser light, radio waves, or ultrasound waves brought to the heart by a cardiac catheter. The words "kill" and "destroy" and their conjugates, as used herein, mean "kill directly or indirectly," and includes, for example, ablation and inducing apoptosis. The words "locations on the heart" as used herein mean locations on the surface of the heart or inside the heart, including within the myocardium. The terms "position" and "orientation" when used herein with reference to an imaging system, mean position and orientation of the elements of the imaging system whose position and orientation affect the point of view of the images produced by the imaging system. The terms "data analyzer" and "image analyzer" as used herein mean any device which analyzes data, including software running on a general puφose computer, and specially designed digital or analog electronic circuits, whether or not it analyzes data in real time, and whether or not it is located in the vicinity or located remotely. The term "analysis results" produced by a data analyzer from a data set can include a selection of any or all unchanged pieces of data in the data set, as well as the results of mathematical calculations using the pieces of data in the data set. The words "comprise" and "include" and their conjugates as used herein mean "include but are not necessarily limited to." While the invention has been described with reference to certain exemplary embodiments, various modifications will be readily apparent to and may be readily accomplished by persons skilled in the art without departing from the spirit and scope of the above teachings.

Claims

1. An ulfrasound cardiac stimulation system comprising: a spatially selective ultrasound source comprising at least one ulfrasound transducer located outside the circulatory system; and a controller; wherein the confroller generates an electrical response in the heart by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.
2. A system according to claim 1 and including an injector which injects cardiac drugs into the bloodstream, wherein the confroller changes the rate at which cardiac tissue absorbs the drugs by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.
3. A system according to claim 1, wherein the controller is operative to choose the ultrasound power level.
4. A system according to claim 3, wherein the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ±20%.
5. A system according to claim 4, wherein the system has sufficient precision to control the ulfrasound power level supplied to cardiac tissue to within ±10%.
6. A system according to claim 5, wherein the system has sufficient precision to control the ultrasound power level supplied to cardiac tissue to within ±3%.
7. A system according to any of claims 3-6, and including an injector which injects one or both of drugs for treating the heart and contrast agents into the bloodsfream.
8. A system according to claim 7 wherein the injector injects drugs into the bloodstream, and the controller changes the rate at which cardiac tissue absorbs the drugs by directing the ultrasound source to transmit a high enough power level of ultrasound to one or more locations in the heart.
9. A system according to claim 7 or claim 8, wherein the injector injects contrast agents into the bloodstream, and the controller is operative to reduce the power level of ultrasound when the contrast agents are injected.
10. A system according to any of claims 3-9 wherein the controller is operative to choose the one or more locations to which the ultrasound is transmitted.
11. A system according to claim 10, wherein the controller controls the ultrasound source to direct ulfrasound energy to a designated location, and the point of highest power flux density falls within an axial precision of 3 mm of said designated location.
12. A system according to claim 11, wherein the axial precision is 1.5 mm.
13. A system according to claim 11 or claim 12, wherein the point of highest power flux density remains within the axial precision of the designated location for at least 1 millisecond.
14. A system according to claim 13, wherein the point of highest power flux density remains within the axial precision of the designated location for at least 10 milliseconds.
15. A system according to any of claims 10-14, wherein the confroller controls the ultrasound source to direct ultrasound energy to a designated location, and the point of highest power flux density falls within a transverse precision of 1 mm of said designated location.
16. A system according to claim 15, wherein the transverse precision is 0.5 mm.
17. A system according to claim 15 or claim 16, wherein the point of highest power flux density remains within the transverse precision of the designated location for at least 1 millisecond.
18. A system according to claim 17, wherein the point of highest power flux density remains within the transverse precision of the designated location for at least 10 milliseconds.
19. A system according to any of claims 10-18, wherein the controller controls the ultrasound source to direct a high enough power level of ultrasound to one or more locations in the heart to kill cardiac tissue by heating it.
20. A system according to any of claims 10-19, wherein the confroller controls the ultrasound source to direct a high enough power level of ultrasound to one or more locations in the heart to kill cardiac tissue by cavitation.
21. A system according to any of claims 10-20, and including an electrocardiograph which measures the timing of the cardiac cycle.
22. A system according to claim 21, wherein the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating in any one chamber of the heart, from the electrical response originating in any other chamber of the heart.
23. A system according to claim 22, wherein the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating in one side of any chamber of the heart, from the electrical response originating in the other side of said chamber of the heart.
24. A system according to claim 23, wherein the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one centimeter away from said location.
25. A system according to claim 24, wherein the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one millimeter away from said location.
26. A system according to any of claims 21-25, which uses feedback from the electrocardiograph to control the ultrasound power level.
27. A system according to any of claims 21-26, wherein the controller is operative to make a map of the heart, showing the ulfrasound power flux required to generate the electrical response at each of several locations in the heart.
28. A system according to any of claims 21-27, wherein the controller is operative to direct the ultrasound source to transmit a first sequence of timed localized pulses of ultrasound energy to the heart, and a second such sequence which differs from the first sequence in one or both of timing and location of the pulses, and the controller is operative to collect a first data set showing the effects of the first sequence on the heart, and a second data set showing the effects of the second sequence on the heart.
29. A system according to claim 28 wherein the first data set and the second data set comprise data from the electrocardiogram.
30. A system according to any of claims 10-20, wherein the controller is operative to direct the ultrasound source to fransmit a first sequence of timed localized pulses of ulfrasound energy to the heart, and a second such sequence which differs from the first sequence in one or both of timing and location of the pulses, and the controller is operative to collect a first data set showing the effects of the first sequence on the heart, and a second data set showing the effects of the second sequence on the heart.
31. A system according to any of claims 28-30, and including a memory which is operative to store the first data set and the second data set, a data analyzer which is operative to analyze data and produce analysis results from the first data set and the second data set, and a display which displays the analysis results.
32. A system according to any of claims 28-31, wherein the first data set and the second data set comprise data on systolic pressure.
33. A system according to any of claims 28-32, wherein the first sequence and the second sequence differ in timing of the pulses.
34. A system according to any of claims 28-33, wherein the first sequence and the second sequence differ in location of the pulses.
35. A system according to any of claims 28-34, and including a cardiac imaging system which produces images showing the position of one or more locations on the heart.
36. A system according to claim 35, wherein the first data set and the second data set comprise data from the cardiac imaging system.
37. A system according to claim 36, and including an image analyzer which analyzes images produced by the cardiac imaging system for the first sequence and the second sequence, and calculates one or more of the systolic left ventricular volume for the first and second sequence, the diastolic left ventricular volume for the first and second sequence, and the ejection fraction for the first and second sequence.
38. A system according to any of claims 10-27, and including a cardiac imaging system which produces images showing the position of one or more locations on the heart.
39. A system according to any of claims 35-38, wherein the images produced by the imaging system show the mechanical response of the heart to stimulation produced by the ultrasound.
40. A system according to any of claims 35-39, wherein the imaging system is in a fixed position and orientation with respect to the ultrasound source.
41. A system according to any of claims 35-40, and including sensors which determine the relative position and orientation of the imaging system and the ultrasound source.
42. A system according to any of claims 35-41, wherein the imaging system determines the relative position and orientation of the ultrasound source by imaging it.
43. A system according to any of claims 35-42, wherein the confroller coordinates the timing of the imaging system with the timing of the ulfrasound source.
44. A system according to any of claims 35-43 wherein the controller is operative to make a map of the heart, using data from the imaging system, showing the mechanical response of the heart at one or more locations to ultrasound energy transmitted to one or more locations.
45. A system according to any of claims 35-44, which uses feedback from the imaging system to control the ultrasound power level.
46. A system according to any of claims 35-45, wherein the imaging system uses ultrasound imaging.
47. A system according to claim 46, wherein the imaging system shares one or more ultrasound transducers with the ultrasound source used to generate the electric response in the heart.
48. A system according to claim 46, wherein the imaging system does not share any ultrasound transducers with the ultrasound source used to generate the electric response in the heart.
49. A system according to any of claims 35-48, wherein the imaging system comprises a computerized tomography x-ray imaging system.
50. A system according to any of claims 35-49, wherein the imaging system comprises a magnetic resonance imaging system.
51. A system according to any of claims 35-50, and including image processing software which analyzes the images to determine the position of one or more locations on the heart.
52. A system according to claim 51, wherein the image processing software determines the position of one or more locations on the heart in real time during a cardiac cycle.
53. A system according to claim 1 or claim 2 wherein the controller is operative to choose the one or more locations to which the ulfrasound is transmitted.
54. A system according to claim 53, wherein the confroller controls the ulfrasound source to direct ultrasound energy to a designated location, and the point of highest power flux density falls within an axial precision of 3 mm of said designated location.
55. A system according to claim 54, wherein, when the axial precision is 1.5 mm.
56. A system according to claim 54 or claim 55, wherein the point of highest power flux density remains within the axial precision of the designated location for at least 1 millisecond.
57. A system according to claim 56, wherein the point of highest power flux density remains within the axial precision of the designated location for at least 10 milliseconds.
58. A system according to any of claims 53-57, wherein the confroller controls the ulfrasound source to direct ulfrasound energy to a designated location, and the point of highest power flux density falls within a fransverse precision of 1 mm of said designated location.
59. A system according to claim 58, wherein the transverse precision is 0.5 mm.
60. A system according to claim 58 or claim 59, wherein the point of highest power flux density remains within the fransverse precision of the designated location for at least 1 millisecond.
61. A system according to claim 60, wherein the point of highest power flux density remains within the transverse precision of the designated location for at least 10 milliseconds.
62. A system according to any of claims 53-61, and including an electrocardiograph which measures the timing of the cardiac cycle.
63. A system according to claim 62, wherein the electrocardiograph is operative to distinguish the electrical response to the ulfrasound, originating in any one chamber of the heart, from the electrical response originating in any other chamber of the heart.
64. A system according to claim 63, wherein the electrocardiograph is operative to distinguish the electrical response to the ulfrasound, originating in one side of any chamber of the heart, from the electrical response originating in the other side of said chamber of the heart.
65. A system according to claim 64, wherein the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one centimeter away from said location.
66. A system according to claim 65, wherein the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating at any location in the heart, from the electrical response originating one millimeter away from said location.
67. A system according to any of claims 1-9, and including an electrocardiograph which measures the timing of the cardiac cycle.
68. A system according to claim 67, wherein the electrocardiograph is operative to distinguish the electrical response to the ultrasound, originating in any one chamber of the heart, from the electrical response originating in any other chamber of the heart.
69. A system according to claim 68, wherein the electrocardiograph is operative to distinguish the electrical response to the ulfrasound, originating in one side of any chamber of the heart, from the electrical response originating in the other side of said chamber of the heart.
70. A system according to claim 69, wherein the electrocardiograph is operative to distinguish the electrical response to the ulfrasound, originating at any location in the heart, from the electrical response originating one centimeter away from said location.
71. A system according to claim 70, wherein the electrocardiograph is operative to distinguish the electrical response to the ulfrasound, originating at any location in the heart, from the electrical response originating one millimeter away from said location.
72. A system according to any of claims 1-9 and 53-71, and including a cardiac imaging system which produces images showing the position of one or more locations on the heart.
73. A system according to claims 72, wherein the imaging system is in a fixed position and orientation with respect to the ulfrasound source.
74. A system according to claim 72 or claim 73, and including sensors which determine the relative position and orientation of the imaging system and the ulfrasound source.
75. A system according to any of claims 72-74, wherein the imaging system determines the relative position and orientation of the ulfrasound source by imaging it.
76. A system according to any of claims 72-75, wherein the controller coordinates the timing of the imaging system with the timing of the ulfrasound source.
77. A system according to any of claims 72-76, wherein the imaging system uses ulfrasound imaging.
78. A system according to claim 77, wherein the imaging system shares one or more ultrasound fransducers with the ulfrasound source used to generate the electric response in the heart.
79. A system according to claim 77, wherein the imaging system does not share any ultrasound fransducers with the ulfrasound source used to generate the electric response in the heart.
80. A system according to any of claims 72-79, wherein the imaging system comprises a computerized tomography x-ray imaging system.
81. A system according to any of claims 72-80, wherein the imaging system comprises a magnetic resonance imaging system.
82. A system according to any of claims 72-81, and including image processing software which analyzes the images to determine the position of one or more locations on the heart.
83. A system according to claim 82, wherein the image processing software determines the position of one or more locations on the heart in real time during a cardiac cycle.
84. A system according to any of claims 21-52 and 62-83, wherein the controller coordinates the timing of the transmission of ulfrasound with the cardiac cycle.
85. A system according to any of claims 21-52 or 62-84, and including a cardiac catheter which generates an electrical response in the heart, and a calibration mode of the confroller, wherein the confroller, when it is in the calibration mode, calibrates the ulfrasound power fransmitted to the heart by the ulfrasound array, by comparing a physiological response induced by the ulfrasound array to a physiological response induced by the catheter.
86. A system according to claim 85 wherein the physiological responses compared by the confroller comprise electrical responses.
87. A system according to claim 85 or claim 86, wherein the physiological responses compared by the confroller comprise mechanical responses.
88. A system according to any of claims 85-87, wherein the cardiac catheter generates an electrical response by direct electric stimulation.
89. A system according to any of claims 85-88, wherein the cardiac catheter comprises an internal ulfrasound fransducer, and the cardiac catheter generates an electrical response by transmitting ulfrasound.
90. A system according to any of claims 85-88, wherein the cardiac catheter kills cardiac tissue.
91. A system according to claim 90, and including a laser, wherein the cardiac catheter comprises a light guide, and the light guide carries light from the laser, which light kills cardiac tissue.
92. A system according to any of the preceding claims, wherein the ulfrasound source comprises a phased array of the ulfrasound transducers.
93. A system according to any of the preceding claims, wherein at least one of the at least one ulfrasound transducers is adapted for use on the surface of the body.
94. A system according to claim 93, wherein the at least one ulfrasound fransducers comprise at least two ulfrasound fransducers, sized and spaced so that they can be placed between the ribs, in such a way as to avoid blocking of ulfrasound by the ribs.
95. A system according to any of the preceding claims, wherein at least one of the at least one ulfrasound fransducers is adapted for use in the esophagus.
96. A system according to any of the preceding claims, wherein at least one of the at least one ultrasound fransducers is adapted for use in a nasal cavity.
97. A system according to any of the preceding claims, wherein the ulfrasound source and the confroller are operative to direct the ultrasound energy with 90% of the power flux falling within 3 mm transversely of the point of highest power flux density.
98. A system according to claim 97, wherein the ulfrasound source and the confroller are operative to direct the ulfrasound energy with 90% of the power flux falling within 1.5 mm transversely of the point of highest power flux density.
99. A system according to claim 98, wherein the ultrasound source and the confroller are operative to direct the ulfrasound energy with 90% of the power flux falling within 1 mm transversely of the point of highest power flux density.
100. A system according to any of the preceding claims, wherein the ultrasound source and the confroller are operative to direct the ultrasound energy with the power flux spreading out to 50% of its highest density within 6 mm axially of the point of highest power flux density.
101. A system according to claim 100, wherein the ulfrasound source and the confroller are operative to direct the ulfrasound energy with the power flux spreading out to 50% of its highest density within 3 mm axially of the point of highest power flux density.
102. A system according to claim 101, wherein the ulfrasound source and the confroller are operative to direct the ulfrasound energy with the power flux spreading out to 50% of its highest density within 1.5 mm axially of the point of highest power flux density.
103. A system according to any of the preceding claims, wherein the ulfrasound source and the controller are operative to direct the ulfrasound energy with a power flux density greater than 30 watts per square centimeter at the point of highest power flux density.
104. A system according to claim 103, wherein the ultrasound source and the controller are operative to direct the ulfrasound energy with a power flux density greater than 100 watts per square centimeter at the point of highest power flux density.
105. A system according to claim 104, wherein the ulfrasound source and the confroller are operative to direct the ulfrasound energy with a power flux density greater than 300 watts per square centimeter at the point of highest power flux density.
106. A system according to any of the preceding claims, wherein the ulfrasound source and the controller are operative to direct the ulfrasound energy in a pulse lasting less than 10 milliseconds.
107. A system according to claim 106, wherein the ulfrasound source and the confroller are operative to direct the ulfrasound energy in a pulse lasting less than 1 millisecond.
108. A system according to any of the preceding claims, wherein the ulfrasound source and the confroller are operative to direct the ultrasound energy in a pulse lasting for a duration within 10% of a duration for which the confroller is directed to direct the energy.
109. A system according to any of the preceding claims, wherein the ulfrasound source and the confroller are operative to direct the ulfrasound energy at a frequency greater than 0.5 megahertz and less than 6 megahertz.
110. A method of changing a cardiac stimulation sequence for a patient, comprising: a) choosing a test sequence of locations in the heart of the patient, and a time in the cardiac cycle to stimulate each location; b) stimulating the test sequence of locations at the chosen times in the cardiac cycle, using an ulfrasound cardiac stimulation system from outside the heart; c) evaluating a change in cardiac synchronization of the patient associated with the test sequence; d) choosing a stimulation sequence for a pacemaker, based at least partly on the change in cardiac synchronization that the test sequence produces; and e) changing a stimulation sequence of the heart to conform to the chosen stimulation sequence.
111. A method according to claim 110, wherein using an ulfrasound cardiac stimulation system from outside the heart comprises using an ulfrasound stimulation system from outside the body.
112. A method according to claim 110 or claim 111, wherein changing a stimulation sequence of the heart comprises installing a pacemaker.
113. A method according to any of claims 110-112, wherein changing a stimulation sequence of the heart comprises adjusting a pacemaker.
114. A method according to claim 113, wherein adjusting a pacemaker comprises programming a pacemaker.
115. A method according to claim 113 or claim 114, wherein adjusting a pacemaker comprises adjusting a pacemaker to obtain improved cardiac synchronization.
116. A method according to any of claims 110-115, wherein (a), (b) and (c) are performed a plurality of times for different test sequences, and choosing an optimal stimulation sequence is based at least partly on the change in a measure of cardiac performance that the different test sequences produce.
117. A method according to claim 116, wherein the measure of cardiac performance comprises cardiac output.
118. A method according to claim 116 or claim 117, wherein evaluating the change in the measure of cardiac performance comprises using systolic pressure measurements.
119. A method according to any of claims 116-118, wherein evaluating the change in the measure of cardiac performance comprises using images of a mechanical response of the heart to the stimulation.
120. A method according to any of claims 116-119, wherein at least one of the test sequences comprises a plurality of locations with the same chosen time.
121. A method according to any of claims 110-120, wherein evaluating the change in cardiac synchronization comprises using electrocardiograph data.
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Cited By (54)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2004112886A2 (en) * 2003-06-17 2004-12-29 Ebr Systems, Inc. Methods and systems for vibrational treatment of cardiac arrhythmias
US7006864B2 (en) 2003-06-17 2006-02-28 Ebr Systems, Inc. Methods and systems for vibrational treatment of cardiac arrhythmias
US7050849B2 (en) 2003-11-06 2006-05-23 Ebr Systems, Inc. Vibrational therapy device used for resynchronization pacing in a treatment for heart failure
US7184830B2 (en) 2003-08-18 2007-02-27 Ebr Systems, Inc. Methods and systems for treating arrhythmias using a combination of vibrational and electrical energy
WO2007137671A2 (en) * 2006-05-26 2007-12-06 Christian Chaussy System for the stimulation of organs, e.g. the heart
US7558631B2 (en) 2004-12-21 2009-07-07 Ebr Systems, Inc. Leadless tissue stimulation systems and methods
US7606621B2 (en) 2004-12-21 2009-10-20 Ebr Systems, Inc. Implantable transducer devices
US7610092B2 (en) 2004-12-21 2009-10-27 Ebr Systems, Inc. Leadless tissue stimulation systems and methods
US7702392B2 (en) 2005-09-12 2010-04-20 Ebr Systems, Inc. Methods and apparatus for determining cardiac stimulation sites using hemodynamic data
US7699778B2 (en) 2002-02-21 2010-04-20 Technion Research & Development Foundation Ltd. Ultrasound cardiac stimulator
US7765001B2 (en) 2005-08-31 2010-07-27 Ebr Systems, Inc. Methods and systems for heart failure prevention and treatments using ultrasound and leadless implantable devices
US7953493B2 (en) 2007-12-27 2011-05-31 Ebr Systems, Inc. Optimizing size of implantable medical devices by isolating the power source
US8718773B2 (en) 2007-05-23 2014-05-06 Ebr Systems, Inc. Optimizing energy transmission in a leadless tissue stimulation system
US9283392B2 (en) 2008-03-25 2016-03-15 Ebr Systems, Inc. Temporary electrode connection for wireless pacing systems
WO2016123532A1 (en) * 2015-01-29 2016-08-04 Medtronic, Inc. Noninvasive assessment of cardiac resynchronization therapy
US9474457B2 (en) 2013-06-12 2016-10-25 Medtronic, Inc. Metrics of electrical dyssynchrony and electrical activation patterns from surface ECG electrodes
US9510763B2 (en) 2011-05-03 2016-12-06 Medtronic, Inc. Assessing intra-cardiac activation patterns and electrical dyssynchrony
US9586050B2 (en) 2014-08-15 2017-03-07 Medtronic, Inc. Systems and methods for configuration of atrioventricular interval
US9586052B2 (en) 2014-08-15 2017-03-07 Medtronic, Inc. Systems and methods for evaluating cardiac therapy
US9591982B2 (en) 2014-07-31 2017-03-14 Medtronic, Inc. Systems and methods for evaluating cardiac therapy
US9731139B2 (en) 2008-07-16 2017-08-15 Ebr Systems, Inc. Local lead to improve energy efficiency in implantable wireless acoustic stimulators
US9764143B2 (en) 2014-08-15 2017-09-19 Medtronic, Inc. Systems and methods for configuration of interventricular interval
US9776009B2 (en) 2014-03-20 2017-10-03 Medtronic, Inc. Non-invasive detection of phrenic nerve stimulation
US9877789B2 (en) 2013-06-12 2018-01-30 Medtronic, Inc. Implantable electrode location selection
US9924884B2 (en) 2013-04-30 2018-03-27 Medtronic, Inc. Systems, methods, and interfaces for identifying effective electrodes
US9986928B2 (en) 2013-12-09 2018-06-05 Medtronic, Inc. Noninvasive cardiac therapy evaluation
US10064567B2 (en) 2013-04-30 2018-09-04 Medtronic, Inc. Systems, methods, and interfaces for identifying optimal electrical vectors
US10251555B2 (en) 2013-06-12 2019-04-09 Medtronic, Inc. Implantable electrode location selection
US10433746B2 (en) 2017-12-22 2019-10-08 Regents Of The University Of Minnesota Systems and methods for anterior and posterior electrode signal analysis
US10492705B2 (en) 2017-12-22 2019-12-03 Regents Of The University Of Minnesota Anterior and posterior electrode signals
US10532213B2 (en) 2017-03-03 2020-01-14 Medtronic, Inc. Criteria for determination of local tissue latency near pacing electrode
US10617318B2 (en) 2018-02-27 2020-04-14 Medtronic, Inc. Mapping electrical activity on a model heart
US10668290B2 (en) 2018-03-01 2020-06-02 Medtronic, Inc. Delivery of pacing therapy by a cardiac pacing device
US10773085B2 (en) 2017-03-15 2020-09-15 Medtronic, Inc. QRS offset and onset determination
US10780279B2 (en) 2016-02-26 2020-09-22 Medtronic, Inc. Methods and systems of optimizing right ventricular only pacing for patients with respect to an atrial event and left ventricular event
US10780281B2 (en) 2018-03-23 2020-09-22 Medtronic, Inc. Evaluation of ventricle from atrium pacing therapy
US10786167B2 (en) 2017-12-22 2020-09-29 Medtronic, Inc. Ectopic beat-compensated electrical heterogeneity information
US10799703B2 (en) 2017-12-22 2020-10-13 Medtronic, Inc. Evaluation of his bundle pacing therapy
US10918870B2 (en) 2018-03-07 2021-02-16 Medtronic, Inc. Atrial lead placement for treatment of atrial dyssynchrony
US10918863B2 (en) 2017-07-28 2021-02-16 Medtronic, Inc. Generating activation times
US10940321B2 (en) 2018-06-01 2021-03-09 Medtronic, Inc. Systems, methods, and interfaces for use in cardiac evaluation
US11219769B2 (en) 2016-02-26 2022-01-11 Medtronic, Inc. Noninvasive methods and systems of determining the extent of tissue capture from cardiac pacing
US11253178B2 (en) 2015-01-29 2022-02-22 Medtronic, Inc. Noninvasive assessment of cardiac resynchronization therapy
US11285312B2 (en) 2018-03-29 2022-03-29 Medtronic, Inc. Left ventricular assist device adjustment and evaluation
US11304641B2 (en) 2018-06-01 2022-04-19 Medtronic, Inc. Systems, methods, and interfaces for use in cardiac evaluation
US11419539B2 (en) 2017-12-22 2022-08-23 Regents Of The University Of Minnesota QRS onset and offset times and cycle selection using anterior and posterior electrode signals
US11471678B2 (en) 2017-07-28 2022-10-18 Medtronic, Inc. Cardiac cycle selection
US11497431B2 (en) 2019-10-09 2022-11-15 Medtronic, Inc. Systems and methods for configuring cardiac therapy
US11547858B2 (en) 2019-03-29 2023-01-10 Medtronic, Inc. Systems, methods, and devices for adaptive cardiac therapy
US11642533B2 (en) 2019-11-04 2023-05-09 Medtronic, Inc. Systems and methods for evaluating cardiac therapy
US11697025B2 (en) 2019-03-29 2023-07-11 Medtronic, Inc. Cardiac conduction system capture
US11813464B2 (en) 2020-07-31 2023-11-14 Medtronic, Inc. Cardiac conduction system evaluation
US12023488B2 (en) 2020-08-17 2024-07-02 Ebr Systems, Inc. Implantable stimulation assemblies having tissue engagement mechanisms, and associated systems and methods
US12023503B2 (en) 2020-07-30 2024-07-02 Medtronic, Inc. ECG belt systems to interoperate with IMDs

Families Citing this family (42)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US7846096B2 (en) 2001-05-29 2010-12-07 Ethicon Endo-Surgery, Inc. Method for monitoring of medical treatment using pulse-echo ultrasound
US20030092988A1 (en) 2001-05-29 2003-05-15 Makin Inder Raj S. Staging medical treatment using ultrasound
US20130281897A1 (en) * 2003-09-04 2013-10-24 Ahof Biophysical Systems Inc. Non-invasive reperfusion system by deformation of remote, superficial arteries at a frequency much greater than the pulse rate
US20050228286A1 (en) * 2004-04-07 2005-10-13 Messerly Jeffrey D Medical system having a rotatable ultrasound source and a piercing tip
US20050240123A1 (en) * 2004-04-14 2005-10-27 Mast T D Ultrasound medical treatment system and method
US20050240124A1 (en) * 2004-04-15 2005-10-27 Mast T D Ultrasound medical treatment system and method
US7883468B2 (en) * 2004-05-18 2011-02-08 Ethicon Endo-Surgery, Inc. Medical system having an ultrasound source and an acoustic coupling medium
US7951095B2 (en) * 2004-05-20 2011-05-31 Ethicon Endo-Surgery, Inc. Ultrasound medical system
US7695436B2 (en) * 2004-05-21 2010-04-13 Ethicon Endo-Surgery, Inc. Transmit apodization of an ultrasound transducer array
US7473250B2 (en) * 2004-05-21 2009-01-06 Ethicon Endo-Surgery, Inc. Ultrasound medical system and method
US7632265B2 (en) * 2004-05-28 2009-12-15 St. Jude Medical, Atrial Fibrillation Division, Inc. Radio frequency ablation servo catheter and method
US8528565B2 (en) 2004-05-28 2013-09-10 St. Jude Medical, Atrial Fibrillation Division, Inc. Robotic surgical system and method for automated therapy delivery
US7974674B2 (en) * 2004-05-28 2011-07-05 St. Jude Medical, Atrial Fibrillation Division, Inc. Robotic surgical system and method for surface modeling
US8755864B2 (en) 2004-05-28 2014-06-17 St. Jude Medical, Atrial Fibrillation Division, Inc. Robotic surgical system and method for diagnostic data mapping
US9782130B2 (en) * 2004-05-28 2017-10-10 St. Jude Medical, Atrial Fibrillation Division, Inc. Robotic surgical system
US10258285B2 (en) 2004-05-28 2019-04-16 St. Jude Medical, Atrial Fibrillation Division, Inc. Robotic surgical system and method for automated creation of ablation lesions
US10863945B2 (en) * 2004-05-28 2020-12-15 St. Jude Medical, Atrial Fibrillation Division, Inc. Robotic surgical system with contact sensing feature
US7806839B2 (en) 2004-06-14 2010-10-05 Ethicon Endo-Surgery, Inc. System and method for ultrasound therapy using grating lobes
US8155910B2 (en) 2005-05-27 2012-04-10 St. Jude Medical, Atrial Fibrillation Divison, Inc. Robotically controlled catheter and method of its calibration
US20070016184A1 (en) * 2005-07-14 2007-01-18 Ethicon Endo-Surgery, Inc. Medical-treatment electrode assembly and method for medical treatment
WO2007136566A2 (en) 2006-05-19 2007-11-29 Prorhythm, Inc. Ablation device with optimized input power profile and method of using the same
US20080071173A1 (en) * 2006-09-18 2008-03-20 Aldrich William N Visualizing Formation of Ablation Lesions
US10035027B2 (en) * 2007-10-31 2018-07-31 The Board Of Trustees Of The Leland Stanford Junior University Device and method for ultrasonic neuromodulation via stereotactic frame based technique
EP3586923B1 (en) 2008-07-14 2021-06-16 Arizona Board Of Regents For And On Behalf Of Arizona State University Devices for modulating cellular activity using ultrasound
US11998266B2 (en) 2009-10-12 2024-06-04 Otsuka Medical Devices Co., Ltd Intravascular energy delivery
DE102011109037A1 (en) 2011-07-30 2013-01-31 Universität Zu Lübeck Method for finding the position of a transducer
WO2013059833A1 (en) 2011-10-21 2013-04-25 Neurotrek, Inc. Method and system for direct communication
WO2014036170A1 (en) 2012-08-29 2014-03-06 Thync, Inc. Systems and devices for coupling ultrasound energy to a body
WO2014071386A1 (en) * 2012-11-05 2014-05-08 Regents Of The University Of Minnesota Non-invasive lung pacing
US10456605B2 (en) 2013-03-14 2019-10-29 Recor Medical, Inc. Ultrasound-based neuromodulation system
US10124185B2 (en) 2013-09-27 2018-11-13 Zoll Medical Corporation Portable defibrillator used for display, hardcopy, and control for other devices
EP3086837B1 (en) * 2013-12-24 2023-06-14 RGB Medical Devices S.A. Monitoring a neuromuscular blockade status
RU2689172C2 (en) * 2014-05-09 2019-05-24 Конинклейке Филипс Н.В. Visualization systems and methods for arrangement of three-dimensional ultrasonic volume in required orientation
FR3025112A1 (en) * 2014-09-02 2016-03-04 Univ Bordeaux METHOD FOR CONTROLLING TARGET AREA OF HEART, METHOD FOR ABLATION OF TARGET AREA OF HEART, ASSOCIATED SYSTEMS
FR3025111A1 (en) * 2014-09-02 2016-03-04 Univ Bordeaux METHOD FOR CONTROLLING THE CALIBRATION OF A FOCUSED ULTRASONIC BEAM FOR CARDIAC STIMULATION, METHOD FOR CARDIAC STIMULATION, SYSTEMS AND DEVICES THEREFOR
WO2016075586A1 (en) * 2014-11-14 2016-05-19 Koninklijke Philips N.V. Ultrasound device for sonothrombolysis therapy
US11179581B2 (en) 2015-03-09 2021-11-23 The Research Foundation For The State University Of New York Systems and methods for promoting cellular activities for tissue maintenance, repair, and regeneration
US20170290561A1 (en) * 2016-04-06 2017-10-12 Covidien Lp Medical device imagable by ultrasound
EP3451933B1 (en) * 2016-05-03 2021-12-15 University Of Virginia Patent Foundation Systems and computer readable media for ischemic injury protective ultrasound
WO2019083863A1 (en) 2017-10-23 2019-05-02 Patent Holding Company 001, Llc Communication devices, methods, and systems
WO2021225994A1 (en) * 2020-05-02 2021-11-11 Datafeel Inc. Communication devices, methods, and systems
WO2022094439A1 (en) 2020-10-30 2022-05-05 Datafeel Inc. Wearable data communication apparatus, kits, methods, and systems

Citations (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0504881A2 (en) * 1991-03-22 1992-09-23 Katsuro Tachibana Booster for therapy of diseases with ultrasound and pharmaceutical liquid composition containing the same
US5817021A (en) 1993-04-15 1998-10-06 Siemens Aktiengesellschaft Therapy apparatus for treating conditions of the heart and heart-proximate vessels
WO1999061058A1 (en) 1998-05-23 1999-12-02 Quadrant Healthcare (Uk) Limited Method of altering heartbeat
WO2001030397A2 (en) * 1999-10-25 2001-05-03 Board Of Regents Of The University Of Nebraska Ultrasound inducement of artial and ventricular rhythms
US6330475B1 (en) * 1996-12-18 2001-12-11 Medtronic Inc. System and a corresponding method for treating defibrillation in a heart

Family Cites Families (39)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3951140A (en) 1974-11-13 1976-04-20 Indianapolis Center For Advanced Research Ultrasonic therapy apparatus and method
US4265228A (en) 1978-09-14 1981-05-05 Zoll Paul M Mechanical pacemaker
US4303075A (en) 1980-02-11 1981-12-01 Mieczyslaw Mirowski Method and apparatus for maximizing stroke volume through atrioventricular pacing using implanted cardioverter/pacer
CA1199371A (en) * 1982-12-03 1986-01-14 Orest Z. Roy Ultrasonic enhancement of cardiac contractility synchronised with ecg event or defibrillation pulse
US4549535A (en) 1982-12-06 1985-10-29 Wing Thomas W Linear motor massage apparatus
US4637397A (en) 1985-05-30 1987-01-20 Case Western Reserve University Triphasic wave defibrillation
US4928672A (en) 1987-07-31 1990-05-29 Siemens Aktiengesellschaft Shockwave source having a centrally disposed ultrasound locating system
US4974461A (en) 1988-10-13 1990-12-04 The United States Of America As Represented By Department Of Health And Human Services Anthropomorphic cardiac ultrasound phantom
US5562608A (en) * 1989-08-28 1996-10-08 Biopulmonics, Inc. Apparatus for pulmonary delivery of drugs with simultaneous liquid lavage and ventilation
US5156154A (en) 1991-03-08 1992-10-20 Telectronics Pacing Systems, Inc. Monitoring the hemodynamic state of a patient from measurements of myocardial contractility using doppler ultrasound techniques
US5183040A (en) 1991-03-08 1993-02-02 Telectronics Pacing Systems, Inc. Apparatus and method for detecting abnormal cardiac rhythms using an ultrasound sensor in an arrhythmia control system
US5213098A (en) 1991-07-26 1993-05-25 Medtronic, Inc. Post-extrasystolic potentiation stimulation with physiologic sensor feedback
US5307816A (en) * 1991-08-21 1994-05-03 Kabushiki Kaisha Toshiba Thrombus resolving treatment apparatus
US5295484A (en) * 1992-05-19 1994-03-22 Arizona Board Of Regents For And On Behalf Of The University Of Arizona Apparatus and method for intra-cardiac ablation of arrhythmias
US5727556A (en) 1993-02-10 1998-03-17 Weth; Gosbert Method for pain therapy and/or for influencing the vegetative nervous system
DK0693924T4 (en) * 1993-02-22 2008-08-04 Abraxis Bioscience Inc Process for (in vivo) delivery of biological materials and compositions suitable therefor
SE9301055D0 (en) 1993-03-29 1993-03-29 Siemens-Elema Ab MECHANICAL DEFIBRILLATION
DE69432148T2 (en) 1993-07-01 2003-10-16 Boston Scientific Ltd., St. Michael CATHETER FOR IMAGE DISPLAY, DISPLAY OF ELECTRICAL SIGNALS AND ABLATION
US6983179B2 (en) * 1993-07-20 2006-01-03 Biosense, Inc. Method for mapping a heart using catheters having ultrasonic position sensors
EP0735842B1 (en) 1993-12-22 1999-03-31 Sulzer Osypka GmbH Ultrasonic marked cardiac ablation catheter
US5573012A (en) 1994-08-09 1996-11-12 The Regents Of The University Of California Body monitoring and imaging apparatus and method
US6690963B2 (en) * 1995-01-24 2004-02-10 Biosense, Inc. System for determining the location and orientation of an invasive medical instrument
SE9603066D0 (en) 1996-08-23 1996-08-23 Pacesetter Ab Electrode for tissue stimulation
US6840936B2 (en) * 1996-10-22 2005-01-11 Epicor Medical, Inc. Methods and devices for ablation
US5848969A (en) 1996-10-28 1998-12-15 Ep Technologies, Inc. Systems and methods for visualizing interior tissue regions using expandable imaging structures
US5846200A (en) * 1996-11-08 1998-12-08 Advanced Technology Laboratories, Inc. Ultrasonic diagnostic imaging system for analysis of left ventricular function
US6029518A (en) * 1997-09-17 2000-02-29 The United States Of America As Represented By The Administrator Of The National Aeronautics And Space Administration Manipulation of liquids using phased array generation of acoustic radiation pressure
US5991660A (en) 1997-09-18 1999-11-23 The Regents Of The University Of Michigan Cardiac pacing methods
US5968085A (en) 1998-04-20 1999-10-19 Medtronic, Inc. Pacing lead with integral guidance using ultrasound
US6141588A (en) * 1998-07-24 2000-10-31 Intermedics Inc. Cardiac simulation system having multiple stimulators for anti-arrhythmia therapy
EP1875960A3 (en) * 1998-10-28 2008-01-30 Covaris, Inc. Controlling sonic treatment
US6152882A (en) 1999-01-26 2000-11-28 Impulse Dynamics N.V. Apparatus and method for chronic measurement of monophasic action potentials
US6298269B1 (en) 1999-04-19 2001-10-02 Cardiac Pacemakers, Inc. Cardiac rhythm management system with ultrasound for autocapture or other applications
JP2003526403A (en) * 1999-06-14 2003-09-09 エクソジェン インコーポレイテッド Method and kit for cavitation induced tissue treatment with low intensity ultrasound
US6719694B2 (en) * 1999-12-23 2004-04-13 Therus Corporation Ultrasound transducers for imaging and therapy
US20020091339A1 (en) * 2000-08-24 2002-07-11 Timi 3 Systems, Inc. Systems and methods for applying ultrasound energy to stimulating circulatory activity in a targeted body region of an individual
CA2428872C (en) * 2000-11-28 2013-01-08 Allez Physionix Limited Systems and methods for making non-invasive physiological assessments
US6704600B2 (en) * 2001-07-13 2004-03-09 Cardiac Pacemakers, Inc. Device programmer with enclosed imaging capability
IL148299A (en) 2002-02-21 2014-04-30 Technion Res & Dev Foundation Ultrasound cardiac stimulator

Patent Citations (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0504881A2 (en) * 1991-03-22 1992-09-23 Katsuro Tachibana Booster for therapy of diseases with ultrasound and pharmaceutical liquid composition containing the same
US5817021A (en) 1993-04-15 1998-10-06 Siemens Aktiengesellschaft Therapy apparatus for treating conditions of the heart and heart-proximate vessels
US6330475B1 (en) * 1996-12-18 2001-12-11 Medtronic Inc. System and a corresponding method for treating defibrillation in a heart
WO1999061058A1 (en) 1998-05-23 1999-12-02 Quadrant Healthcare (Uk) Limited Method of altering heartbeat
WO2001030397A2 (en) * 1999-10-25 2001-05-03 Board Of Regents Of The University Of Nebraska Ultrasound inducement of artial and ventricular rhythms

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
AVITALL, B. ET AL.: "Local effects of electrical and mechanical stimulation on the recovery properties of canine ventricle", AM. J CARDIOLOGY, vol. 50, 1982, pages 263 - 270, XP023196842, DOI: doi:10.1016/0002-9149(82)90175-8

Cited By (80)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US7699778B2 (en) 2002-02-21 2010-04-20 Technion Research & Development Foundation Ltd. Ultrasound cardiac stimulator
WO2004112886A3 (en) * 2003-06-17 2005-09-29 Ebr Systems Inc Methods and systems for vibrational treatment of cardiac arrhythmias
US7006864B2 (en) 2003-06-17 2006-02-28 Ebr Systems, Inc. Methods and systems for vibrational treatment of cardiac arrhythmias
WO2004112886A2 (en) * 2003-06-17 2004-12-29 Ebr Systems, Inc. Methods and systems for vibrational treatment of cardiac arrhythmias
US7184830B2 (en) 2003-08-18 2007-02-27 Ebr Systems, Inc. Methods and systems for treating arrhythmias using a combination of vibrational and electrical energy
US7809438B2 (en) 2003-08-18 2010-10-05 Ebr Systems, Inc. Methods and systems for treating arrhythmias using a combination of vibrational and electrical energy
US7050849B2 (en) 2003-11-06 2006-05-23 Ebr Systems, Inc. Vibrational therapy device used for resynchronization pacing in a treatment for heart failure
US9333364B2 (en) 2004-06-15 2016-05-10 Ebr Systems, Inc. Methods and systems for heart failure treatments using ultrasound and leadless implantable devices
US9008776B2 (en) 2004-12-21 2015-04-14 Ebr Systems, Inc. Leadless tissue stimulation systems and methods
US7996087B2 (en) 2004-12-21 2011-08-09 Ebr Systems, Inc. Leadless tissue stimulation systems and methods
US8315701B2 (en) 2004-12-21 2012-11-20 Ebr Systems, Inc. Leadless tissue stimulation systems and methods
US7558631B2 (en) 2004-12-21 2009-07-07 Ebr Systems, Inc. Leadless tissue stimulation systems and methods
US7606621B2 (en) 2004-12-21 2009-10-20 Ebr Systems, Inc. Implantable transducer devices
US7610092B2 (en) 2004-12-21 2009-10-27 Ebr Systems, Inc. Leadless tissue stimulation systems and methods
US7848815B2 (en) 2004-12-21 2010-12-07 Ebr Systems, Inc. Implantable transducer devices
US7890173B2 (en) 2004-12-21 2011-02-15 Ebr Systems, Inc. Implantable transducer devices
US11376439B2 (en) 2005-08-31 2022-07-05 Ebr Systems, Inc. Methods and systems for heart failure prevention and treatments using ultrasound and leadless implantable devices
US7765001B2 (en) 2005-08-31 2010-07-27 Ebr Systems, Inc. Methods and systems for heart failure prevention and treatments using ultrasound and leadless implantable devices
US10207115B2 (en) 2005-08-31 2019-02-19 Ebr Systems, Inc. Method and systems for heart failure prevention and treatments using ultrasound and leadless implantable devices
US7702392B2 (en) 2005-09-12 2010-04-20 Ebr Systems, Inc. Methods and apparatus for determining cardiac stimulation sites using hemodynamic data
WO2007137671A2 (en) * 2006-05-26 2007-12-06 Christian Chaussy System for the stimulation of organs, e.g. the heart
WO2007137671A3 (en) * 2006-05-26 2008-02-21 Christian Chaussy System for the stimulation of organs, e.g. the heart
US11452879B2 (en) 2007-05-23 2022-09-27 Ebr Systems, Inc. Optimizing energy transmission in a leadless tissue stimulation system
US10080903B2 (en) 2007-05-23 2018-09-25 Ebr Systems, Inc. Optimizing energy transmission in a leadless tissue stimulation system
US10456588B2 (en) 2007-05-23 2019-10-29 Ebr Systems, Inc. Optimizing energy transmission in a leadless tissue stimulation system
US8718773B2 (en) 2007-05-23 2014-05-06 Ebr Systems, Inc. Optimizing energy transmission in a leadless tissue stimulation system
US7953493B2 (en) 2007-12-27 2011-05-31 Ebr Systems, Inc. Optimizing size of implantable medical devices by isolating the power source
US11752352B2 (en) 2008-03-25 2023-09-12 Ebr Systems, Inc. Temporary electrode connection for wireless pacing systems
US10688307B2 (en) 2008-03-25 2020-06-23 Ebr Systems, Inc. Temporary electrode connection for wireless pacing systems
US9283392B2 (en) 2008-03-25 2016-03-15 Ebr Systems, Inc. Temporary electrode connection for wireless pacing systems
US9907968B2 (en) 2008-03-25 2018-03-06 Ebr Systems, Inc. Temporary electrode connection for wireless pacing systems
US9731139B2 (en) 2008-07-16 2017-08-15 Ebr Systems, Inc. Local lead to improve energy efficiency in implantable wireless acoustic stimulators
US9510763B2 (en) 2011-05-03 2016-12-06 Medtronic, Inc. Assessing intra-cardiac activation patterns and electrical dyssynchrony
US11027135B2 (en) 2011-05-03 2021-06-08 Medtronic, Inc. Assessing intra-cardiac activation patterns
US9962097B2 (en) 2011-05-03 2018-05-08 Medtronic, Inc. Assessing intra-cardiac activation patterns and electrical dyssynchrony
US9974457B2 (en) 2011-05-03 2018-05-22 Medtronic, Inc. Assessing intra-cardiac activation patterns
US9924884B2 (en) 2013-04-30 2018-03-27 Medtronic, Inc. Systems, methods, and interfaces for identifying effective electrodes
US9931048B2 (en) 2013-04-30 2018-04-03 Medtronic, Inc. Systems, methods, and interfaces for identifying effective electrodes
US11648406B2 (en) 2013-04-30 2023-05-16 Medtronic, Inc. Systems, methods, and interfaces for identifying effective electrodes
US10064567B2 (en) 2013-04-30 2018-09-04 Medtronic, Inc. Systems, methods, and interfaces for identifying optimal electrical vectors
US9877789B2 (en) 2013-06-12 2018-01-30 Medtronic, Inc. Implantable electrode location selection
US9486151B2 (en) 2013-06-12 2016-11-08 Medtronic, Inc. Metrics of electrical dyssynchrony and electrical activation patterns from surface ECG electrodes
US9474457B2 (en) 2013-06-12 2016-10-25 Medtronic, Inc. Metrics of electrical dyssynchrony and electrical activation patterns from surface ECG electrodes
US10251555B2 (en) 2013-06-12 2019-04-09 Medtronic, Inc. Implantable electrode location selection
US9986928B2 (en) 2013-12-09 2018-06-05 Medtronic, Inc. Noninvasive cardiac therapy evaluation
US10206601B2 (en) 2013-12-09 2019-02-19 Medtronic, Inc. Noninvasive cardiac therapy evaluation
US9993172B2 (en) 2013-12-09 2018-06-12 Medtronic, Inc. Noninvasive cardiac therapy evaluation
US11456062B2 (en) 2013-12-09 2022-09-27 Medtronic, Inc. Noninvasive cardiac therapy evaluation
US9776009B2 (en) 2014-03-20 2017-10-03 Medtronic, Inc. Non-invasive detection of phrenic nerve stimulation
US9591982B2 (en) 2014-07-31 2017-03-14 Medtronic, Inc. Systems and methods for evaluating cardiac therapy
US9586052B2 (en) 2014-08-15 2017-03-07 Medtronic, Inc. Systems and methods for evaluating cardiac therapy
US9586050B2 (en) 2014-08-15 2017-03-07 Medtronic, Inc. Systems and methods for configuration of atrioventricular interval
US9764143B2 (en) 2014-08-15 2017-09-19 Medtronic, Inc. Systems and methods for configuration of interventricular interval
WO2016123532A1 (en) * 2015-01-29 2016-08-04 Medtronic, Inc. Noninvasive assessment of cardiac resynchronization therapy
US11253178B2 (en) 2015-01-29 2022-02-22 Medtronic, Inc. Noninvasive assessment of cardiac resynchronization therapy
US10780279B2 (en) 2016-02-26 2020-09-22 Medtronic, Inc. Methods and systems of optimizing right ventricular only pacing for patients with respect to an atrial event and left ventricular event
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US7699778B2 (en) 2010-04-20
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US20100204576A1 (en) 2010-08-12

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