1. Field of the Invention
The stimulation of cardiac tissue using an acoustic transducer, referred to as a controller-transmitter, and one or more implanted receiver-stimulator devices has recently been proposed by the inventors herein in the patent applications referred to above. The controller-transmitter produces an acoustic signal which is received by the receiver-stimulator, and the receiver-stimulator in turn generates an electrical signal which is delivered to cardiac or other tissue through coupled tissue electrodes. The controller-transmitter may be external, but will usually be implanted, requiring that the controller-transmitter have a reasonable size, similar to that of implantable pacemakers, and that the controller-transmitter be capable of operating from batteries for a lengthy period, typically three or more years. The relatively small size and relatively long operational period require that the receiver-stimulators efficiently utilize the acoustic energy from the controller-transmitters.
For those reasons, it would be desirable to provide implantable transducer devices which are able to efficiently receive acoustic energy from implanted or external acoustic transmitters. It would be particularly desirable if the transducers could operate in an isotropic or nearly isotropic fashion where they could efficiently receive acoustic energy from an acoustic transmitter regardless of the relative orientation between the transmitter and the implanted transducer. At least some of these objectives will be met by the inventions described hereinafter.
2. Description of the Background Art
The following patents and patent publications describe various implantable transducers capable of converting applied acoustic energy into an electrical output: U.S. Pat. Nos. 3,659,615; 3,735,756; 5,193,539; 6,654,638; 6,628,989; and 6,764,446; U.S. Patent Application Publications 2002/0077673; 2004/0172083; and 2004/0204744; and published German application DE 4330680.
Systems and methods are provided for delivering electrical energy to body tissues for a variety of purposes. The energy will typically be delivered in order to stimulate cardiac tissue, for example in cardiac pacing for bradycardia, for termination of tachyarrhythmia, for bi-ventricular resynchronization therapy for heart failure, or the like. The systems and methods of the present invention, however, could be used in a variety of other applications, including applications for nerve stimulation, brain stimulation, voluntary muscle stimulation, gastric stimulation, bone growth stimulation, pain amelioration, and the like.
In a first aspect, the present invention provides an implantable receiver-stimulator device which is capable of receiving acoustic energy delivered from an acoustic source (physically separate from the receiver-stimulator device) and converting that acoustic energy to an electrical signal. The receiver-stimulator of the present invention will usually be very sensitive and will usually be able to receive and convert low levels of acoustic energy to produce electrical signals which are able to stimulate myocardial tissue. Typically, with devices of the present invention with cross sectional areas on the order of 3 mm2, an acoustic wave having a pressure level in the range from 0.2 to 0.4 mega Pascals (an intensity level of 1.3 to 5.6 W/cm2), can be converted to electrical signals in the range from 1.0 to 2.0_Volts. Thus, the devices of the present invention will usually be very efficient and capable of converting a large portion of the received acoustic energy into electrical energy, typically with a conversion efficiency of at least 25%, often being at least 50%. In addition to such high sensitivity and efficiency, the implantable receiver-stimulators of the present invention are also capable of functioning at least substantially isotropically. That is, the device sensitivity will be isotropic. By “isotropic,” it is meant that the receiver-stimulator will have a transducer assembly capable of receiving acoustic energy in a manner which is substantially insensitive to the relative orientation of the device to the acoustic source. The electric signal produced by the receiver-stimulator device in response to incident acoustic energy will vary by no more than ±6 dB as the orientation of the device varies relative to the acoustic source, often varying by no more than ±3 dB, preferably varying by no more than ±1 dB.
In a first specific embodiment, an implantable receiver-stimulator comprises a transducer assembly, typically being capable of isotropic operation as noted above, which receives acoustic energy from an acoustic source and which produces an electrical signal in response to the acoustic energy. The device further comprises demodulator circuitry which receives the electrical signal and which produces a biologically stimulating electrical output, e.g., suitable for cardiac pacing, nerve stimulation, brain stimulation, voluntary muscle stimulation, pain amelioration, or the like. The device will further include at least two tissue-contacting electrodes which are coupled to the demodulator circuitry to receive the stimulating electrical output and deliver said output to the tissue. Either or both of the electrodes may be mounted directly on the device, in some instances forming a portion of the device casing, or may alternatively be connected to the device by wires, cables, or the like, for placement.
The transducer assembly may comprise a cylindrical piezoelectric transducer having a pair of electrodes formed over opposed surfaces thereof. The incident acoustic energy will cause the piezoelectric transducer to vibrate and generate electrical charge which is collected by the electrodes and available for delivery to the demodulator circuitry. In a first exemplary embodiment, the piezoelectric transducer may be composed of a polycrystalline ceramic piezoelectric material. When the ceramic piezoelectric material is formed in the shape of a tube, the opposed electrodes may typically be formed over the outer and inner cylindrical surfaces of the transducer although electrodes over the opposing flat end surfaces may also be used.
In a preferred exemplary embodiment, however, the piezoelectric transducer will be composed of a single crystal material, typically being cut in the <001> orientation. A preferred single crystal material comprises PMN-xPT material, where x is in the range from 5% to 50% by weight. Other single crystal materials may be of the composition PZN-xPT, or Relaxor-PT materials. When the piezoelectric transducer is composed of a single crystal, the opposed electrodes are preferably formed over the opposed flat end surfaces of the cylinder, not the cylindrical surfaces. Alternatively, for alternate crystal planes, electrodes formed on cylindrical surfaces or cylindrical surfaces on sectioned and composite crystal assemblies, may be preferred.
In a still further embodiment of the implantable receiver-stimulator of the present invention, the transducer assembly comprises a plurality of individual transducer elements. The demodulator circuitry similarly comprises a plurality of individual demodulator circuits, and each of the transducer elements is attached to one of the individual demodulator circuits. The transducer elements themselves will typically have a maximum dimension which is approximately one-half wavelength of the expected acoustic transmission, but the cumulative lateral dimensions of the individual transducer elements will preferably be much greater than a single wavelength. On the output of the demodulator circuitry there will be provisions for summing the electrical signals from each of the individual demodulator circuits to produce the biologically stimulating electrical output. Electrical signals may be summed in parallel, in series, or in a series-parallel combination.
In a second aspect of the present invention, methods for delivering energy to an implanted receiver-stimulator comprise implanting a receiver-stimulator, typically formed as an assembly having a transducer or transducers, being substantially isotropic as described above in connection with the devices of the present invention. Acoustic energy is directed to the implanted receiver-stimulator assembly from an acoustic source, which may be implanted or located externally, and the transducers produce electrical signals which vary by no more than ±6 dB as the orientation of the transducers vary relative to that of the acoustic source. The electrical signal is demodulated to produce a biologically stimulating electrical output, and the electrical output is delivered to tissue. The acoustic energy may be delivered to the receiver-stimulator from an external source, but will preferably be delivered from an implanted acoustic source. The electrical output flowing between stimulating electrodes which are in contact with tissue may possess specific characteristics of voltage, current, waveform, and the like. These electrical characteristics will be selected to stimulate the target cardiac tissue, nerve tissue, brain tissue, voluntary muscle tissue, bone tissue, or the like.
d illustrate various single crystal orientations and respective sensitivity profiles of transducer in the present invention.
As illustrated in
A first nearly isotropic transducer assembly 29 useful in the present invention is illustrated in
While the transducer assembly 29 of
Devices of the type depicted in
With respect to sensitivity, Table 1 below summarizes device sensitivity in a plane normal to the cylindrical axes of the devices. The devices were exposed to long bursts of ultrasound, in the general range of 340 kHz and 600 kHz. With no electrical load on the devices, the generated peak-to-peak voltage was measured by a high input impedance digital oscilloscope, with the results tabulated below with respect to the ultrasound field strength in MI (Mechanical Index, defined as rarefactional pressure in mega Pascals divided by the square root of the frequency in mega Hertz). Subsequently, in each test, the devices were electrically loaded with a 500 ohm resistor, with the results next tabulated below with respect to field strength. The electrical impedance of 500 ohms was used and was representative of the impedance between electrodes in contact with various human tissue types. And lastly, the devices were near optimally impedance matched with a transformer, connected to a full wave rectifier with a 0.1 micro Farad capacitor, and loaded with 500 ohms. The peak amplitude of the resulting DC (direct current) voltage envelope with respect to the field strength is reported below.
In the above Table, device 2199 was a PZT-5H ceramic tube, 0.070 inches long, 0.070 inches in outside diameter, and 0.045 inches on inner diameter. The tube was polarized with electrodes on the inner and outer cylindrical surface. Device 2216A was a PMN-32% PT single crystal tube, with the same dimensions as device 2199. However, the device was cut from a plate perpendicular to the <001> crystal orientation axis. The electrodes were on the flat faces with polarization between the electrodes. Device 2195 was a ceramic tube in all aspects the same as device 2199, with the exception of a 0.040 inch length.
In an open circuit mode, the single crystal devices are vastly superior to the ceramic devices. However, this represents an unrealistic situation in that sufficient current needs to be derived from the devices to stimulate tissue. While the single crystal materials still enjoy a substantial advantage when loaded with a representative tissue impedance, the performance gap has lessened. And lastly, when driving impedance matching, rectifier, filter, and representative tissue loaded circuits, there was still a good performance gap, but with slight variations.
The primary reason for the excellent performance of the single crystal material was the low frequency constant which results in a resonance at approximately 340 kHz, as seen in
In comparing the performance of the single crystal at its resonance of 340 kHz with the ceramics at their lowest frequency resonances at 550 to 600 kHz, the single crystal device was still on average more than 10 dB more sensitive, fully loaded, than the ceramic devices. Comparing the single crystal at its off resonance frequency with the ceramics at their off resonance frequencies, the single crystal device was more than 17 dB more sensitive. The single crystal material was thus seen to offer significant improvement over the ceramic material as a source of electrical energy in an acoustic field for the tissue stimulator.
The present invention has detailed the implementation of single crystal piezoelectric tubes cut in the <001> orientation for use in implantable receiver-stimulator devices, where the sensitivity normal to the crystal axis is circumferentially uniform in all directions, as depicted in
A further embodiment of the implantable receiver-stimulators of the present invention utilizes a transducer assembly which includes multiple transducer elements at least some of which have a size (equal to or less than one-half wavelength) selected to enhance the isotropic nature of the individual elements. Generally if the piezoelectric transducer size exceeds one half wavelength of the acoustic signal, directional variations in sensitivity will begin to dominate performance, whereas with device sizes less than one half wavelength, device sensitivity approaches isotropy, being almost uniform in all directions. Hydrophones, which are devices to sample acoustic fields, typically have upper operational limits corresponding to a sensor size of one half wavelength. Larger sizes would be preferred for hydrophone elements as the output is directly proportional to the cross sectional area of the device. Thus, for the receiver-stimulator, multiple elements are added specifically to increase the cross sectional area of the device to increase sensitivity. The implantable devices must have near isotropic responses, as the orientation of a device with respect to the acoustic excitation field may not coincide with the orientation of the device as it is implanted in the tissue which requires stimulation.
As depicted in
In order to overcome this deficit and yet to use multiple elements for greater output power, and to reduce or eliminate constructive and destructive interference between the elements, a separate detector/filter for each element is provided. The combination of a single transducer element and a single detector/filter may be referred to as a channel. As depicted in
Alternatively, as depicted in
Further, it is also possible to combine series and parallel connections on the outputs of the individual channels to achieve at least partially specific impedance matching between the individual piezoelectric elements and a target tissue mass.
To demonstrate this concept, a multi-element section 142 was fabricated as depicted in
In
When looking at the output of the detector/filter circuit under a no load condition, the output voltage falls off very slowly as compared to the voltage rise due to the input signal from the transducer element. This is seen in the lower four traces of
Lastly, in
It has thus been demonstrated experimentally that summation in the RF domain (transducer element output) will result in constructive and destructive interference, dependent on the phase relationship between the elements. Alternatively, by providing summation after detection and filtering, a phase independent environment is established, with only constructive interference.
The detector circuits discussed for this application might include half wave rectifiers, full wave rectifiers, voltage doublers, charge-pump devices, and the like. Filters may include series inductors, parallel capacitors, combinations of the same, and the like. Impedance matching may be accomplished through transformer devices, active or passive circuit components, or may be incorporated into the design of the detector/filter circuits. Further details on the detector/filter circuits are provided in co-pending application.
With the requirement for isotropic transducers in the receiver-stimulator, transducer size (in all lateral dimensions) should not exceed approximately 0.5 wavelengths, subject only to the amount of variation tolerated in signal strength at various elevation angles. Given a velocity of sound in normal tissue of approximately 1.5 millimeters per microseconds, at 1 MHz device sizes shall not exceed approximately 0.75 millimeters, at 0.5 MHz 1.5 millimeters, and at 250 kHz 3.0 millimeters.
Transducers in the receiver-stimulator can be positioned and located in any orientation, with respect to the axis of the transmitted acoustic beam. Transducers can be mounted in a linear manner as depicted in
While the above is a complete description of the preferred embodiments of the invention, various alternatives, modifications, and equivalents may be used. Therefore, the above description should not be taken as limiting the scope of the invention which is defined by the appended claims.
This application is a divisional of U.S. patent application Ser. No. 11/315,524, filed on Dec. 21, 2005, which claimed the benefit of the following provisional applications: 60/639,027, filed on Dec. 21, 2004; 60/689,606, filed on Jun. 9, 2005; and 60/639,056, filed on Dec. 21, 2004. The full disclosures of each of these prior filings are incorporated herein by reference. The subject matter of this application is related to that of the following commonly owned patent applications: Ser. No. 10/869,242; Ser. No. 10/869,776; and Ser. No. 10/869,705. The full disclosures of each of these prior filings are incorporated herein by reference but the benefit of the filing dates is not being claimed.
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