Inhaler that uses focused acoustic waves to deliver a pharmaceutical product

Information

  • Patent Grant
  • 8122880
  • Patent Number
    8,122,880
  • Date Filed
    Monday, December 18, 2000
    24 years ago
  • Date Issued
    Tuesday, February 28, 2012
    12 years ago
Abstract
An improved method and apparatus for delivering medication to the lungs is described. Acoustic ink printing technology is modified to operate as an inhaler that generates tiny droplets near a patient's nose or mouth. The tiny droplets are easily carried by air currents into the patient's lungs. The inhaler itself is preferably a battery operated portable device that can be easily carried and easily cleaned to avoid contaminating the medication.
Description

This application is related to issued U.S. Pat. No. 6,622,720 entitled “Using Capillary Wave Driven Droplets to Deliver a Pharmaceutical Product”, and patent application Ser. No. 09/739,989 entitled “A Method of Using Focused Acoustic Waves to Deliver a Pharmaceutical Product”. All Applications were filed on Dec. 18, 2000 and all Applications are assigned to the same Assignee.


BACKGROUND OF THE INVENTION

Many pharmaceutical products or drugs that provide relief from nasal or lung ailments are delivered through the respiratory system. In order to deliver these drugs, typically, the drug is compressed in a container. Users release the compressed pharmaceutical by opening a valve for a brief interval of time near the user's mouth or nose. Pump mechanisms may also be used to directly spray the pharmaceutical into the user's mouth or nose. The user may then draw a breath to further inhale the pharmaceutical product.


These techniques for delivering pharmaceuticals pose several problems. The first problem is that the droplet size produced is typically too large to be carried in an air stream generated by a normal intake of breath. Thus, in order to transport the larger droplets of pharmaceutical products, the product is propelled into the orifice. This may be done by using compressed air or by expelling the pharmaceutical product into the orifice at a high speed.


Unfortunately, a fast moving particle, defined as a particle that is moving much faster than the accompanying airstream, cannot easily travel around bends that occur in the human respiratory system. Thus, when the traditional means of injecting pharmaceuticals into the mouth are used, much of the pharmaceutical product is deposited on the back of the mouth or in the throat. The deposited pharmaceutical product may then be ingested into the digestive tract instead of the respiratory system. The ingested pharmaceutical product represents lost or wasted medication.


A second problem is that the varying amounts of lost pharmaceutical product makes it difficult to control dosages. Wasted droplets of medication that are deposited on the back of the throat makes it possible that the patient will receive insufficient medication. Determining the amount wasted and trying to compensate for the wasted medication is a difficult and inexact process.


Thus an improved method and apparatus of delivering pharmaceutical products to a patient's respiratory system is needed.


SUMMARY OF THE INVENTION

In order to more efficiently deliver pharmaceutical products, acoustic ink printing (AIP) technology has been adapted for use in delivering medications to a patient. In one embodiment of the invention, a liquid medication is distributed over several acoustic ejector drivers. The drivers are inserted into or placed in close proximity to an orifice of the patient such as the mouth or the nose. A power source provides energy to each driver. The drivers convert the energy into focused acoustic waves that cause small droplets of medication to be ejected into the orifice. Air currents distribute the medication throughout the patient's respiratory system.





BRIEF DESCRIPTION OF THE DRAWINGS


FIG. 1 shows a cross section of a droplet ejector in an array of droplet ejectors ejecting a droplet of pharmaceutical product.



FIG. 2 shows ejection of droplets using capillary action.



FIG. 3 shows one embodiment of forming an inhaler that uses a single transducer to drive multiple droplet sources.



FIG. 4 shows an example distribution of droplet ejectors on an inhaler head.



FIG. 5 shows a cross sectional side view of one embodiment of an inhaler designed for insertion into the mouth of a patient.



FIG. 6 shows the inhaler in use by a patient.





DETAILED DESCRIPTION OF THE INVENTION

An inhaler system that adapts acoustic ink printing technology to output small droplets of pharmaceutical product at a low velocity is described. The droplets are preferably less than 10 micrometers in diameter. Small droplet size and an output speed approximately matching the rate of airflow into the respiratory system maximizes the quantity of medication administered to a patient's lungs.



FIG. 1 shows an array 160 of droplet sources such as droplet sources 100, 101, 102, 103 for use in an inhaler 144. Each droplet source 100, 101, 102, 103 is capable of outputting droplets of pharmaceutical product. Inhaler 144 is designed such that the combined output of all droplets sources in array 160 over a predetermined period of time are sufficient to deliver a desired volume of pharmaceutical product to a patient. The pharmaceutical product is typically liquid that contains organic compounds for deposition in the lungs of the patient.



FIG. 1 includes a cross sectional view of one example droplet source 100 in array 160. The cross sectional view also shows a distribution of a reservoir of pharmaceutical product 108 shortly after ejection of a droplet 104 and before a mound 112 on a free surface 116 has relaxed. A radio frequency (RF) source 120 provides a RF drive energy to a driver element such as a transducer, typically a piezo-electric transducer 124, via bottom electrode 128 and top electrode 132. The acoustic energy from the transducer passes through base 136 into an acoustic lens 140. Acoustic lens 140 focuses the received acoustic energy into a focused acoustic beam 138 that terminates in a small focal area near free surface 116. In the illustrated embodiment, each droplet source in array 160 of droplet sources includes a corresponding acoustic lens and transducer to form an array of acoustic lenses and transducers.


Traditional acoustic ink printers usually use RF drives with frequencies of around 100 to 200 Megahertz (MHz). However, when droplet sources are used in inhalers, higher frequencies are preferred because higher frequencies generate smaller droplets that are more easily carried by air currents into the respiratory tract. Droplet sizes are typically on the order of the wavelength of the bulk acoustic wave propagating in the pharmaceutical product. This wavelength may be determined by dividing the velocity of sound for bulk wave propagation in the pharmaceutical product by the frequency of the bulk acoustic wave. Thus by increasing frequency, droplet size can be reduced A RF drive frequency exceeding 300 MHz typically results in the generation of droplets smaller than 5 micro-meters in diameter. Thus inhalers that directly eject droplets preferably operate in frequency ranges exceeding 300 MHz.


Higher frequencies used in inhaler droplet sources also result in higher power losses. Power losses in a droplet source are approximately proportional to the square of the frequency. Power losses in a droplet source are also proportional to the distance “d” from the top surface 141 of acoustic lens 140 to free surface 116 of the pharmaceutical product reservoir. In order to compensate for increased power losses due to the increased operating frequencies, distance “d” may be reduced compared to traditional AIP print heads. In inhaler applications, a distance “d” less than 150 micrometers may be used to conserve power.


A more detailed description of the droplet source or “droplet ejector” operation in a traditional AIP printhead is provided in U.S. Pat. No. 5,565,113 by Hadimioglu et al. entitled “Lithographically Defined Ejection Units” issued Oct. 15, 1996 and hereby incorporated by reference.



FIG. 1 uses focused acoustic energy to directly eject a droplet. FIG. 2 shows an alternative method of generating droplets using capillary action. When generating capillary wave-driven droplets, the principle mound 204 does not receive enough energy to eject a droplet. Instead, as the principle mound 204 decreases in size, the excess liquid is absorbed by surrounding capillary wave crests or side mounds 208, 212, 216, 220. These wave crests eject a mist corresponding to droplets 224, 228, 232, 236. In order to generate capillary action droplets instead of focused, single ejection droplets, each ejector transducer generates shorter pulse widths at a higher peak power. Example pulse widths are on the order of 5 microseconds or less when the transducer provides a peak power of approximately one watt or higher per ejector.


One advantage of using capillary action is the lower frequencies that can be used to create smaller droplets. The diameter of capillary generated droplets is similar in magnitude to the wavelength of capillary waves. The wavelength of capillary waves can be determined from the equation: wavelength=[2*Pi*T/(ro*f^2)]^(⅓) wherein T is the surface tension of the pharmaceutical fluid, ro is the density of the pharmaceutical fluid and f is the frequency output of the transducer. This equation and a more detailed explanation are provided on page 328 of Eisenmenger, Acoustica, 1959 which is hereby incorporated by reference. At typical densities and surface tensions, frequencies of below 15 MHz are typically used. Frequencies of 10 Megahertz (MHz) typically generate a capillary wavelength of 1.5 micrometers and a frequency of 1 MHz typically generates a capillary wavelength of 6.8 micrometers. Thus it is possible to generate approximately 5 micrometer diameter droplets at RF frequencies about two orders of magnitude smaller than the bulk waves used to generate “conventional” AIP droplets.


In capillary wave droplet systems, the lower frequencies used allows more flexibility in materials and tolerances used to fabricate transducers and acoustic lenses used to form the array of droplet sources. For example, plastics are not as lossy at the lower frequencies. The lower loss levels allow relatively inexpensive molded plastic spherical lenses to be used as acoustic lenses.


A second method of minimizing the cost of fabricating an array of droplet sources is to replace the plurality of transducers with a single transducer, the energy from the single transducer distributed to multiple lenses corresponding to multiple droplet sources. FIG. 3 shows an example of such a single transducer structure. In FIG. 3, each droplet source corresponds to an acoustic lens such as acoustic lenses 308, 312, 316. The acoustic lenses are positioned over a single large transducer 304. Each acoustic lens independently focuses a portion of the bulk planar wave produced by single large transducer 304 to create droplets across a free surface 320. Using a single transducer instead of the multiple transducers shown in FIG. 1 substantially reduces the cost associated with multiple transducers and the electronics to drive multiple transducers.


The number of droplet sources in an array of droplet sources may vary and typically depends on the dosages that will be administered. A typical five micron diameter drop of pharmaceutical product contains about 0.07 picoliters of fluid. Assuming a repetition rate of 200 KHz, a rate easily achievable with the typical ejector, each droplet source will deliver approximately 14 microliters per second. To administer medication at the rate of 100 milliliters per second, a typical number of ejectors may be around 7,000.



FIG. 4 shows a top view 404 of an example distribution of droplet sources 408. Typically, the droplet sources are mounted on a circular head 412 over a distance of approximately 10 centimeters to facilitate insertion into an oral cavity. Alternative configurations of droplet sources may be designed for insertion into a nasal cavity. Although a circular pattern of droplet sources best utilizes the surface area of circular head 412, in high viscosity pharmaceutical products, the flow of the product evenly across a circular pattern may prove difficult. Thus, in an alternate embodiment, a more linear pattern of droplet sources may be used.


Prevention of contamination, both from airborne particulate matter as well as organic matter such as bacteria is an important concern with the inhaler. Typically, openings 414 in circular head 412 are substantially larger than the droplet size ejected. For example, a typical opening size for ejection of a 10 micron diameter droplet may be approximately 100 microns. When droplet sources are not activated, the pharmaceutical product is maintained within the circular head 412 via surface tension across opening 414. The relatively large exposed surface area of opening 414 may allows dust and other particulate matter to enter the openings and contaminate the pharmaceutical product.


A cover 413 that fits over the circular head 412 helps minimize particulate contamination. In one embodiment opening and closing cover 413 may switch on and off the inhaler. An alternate method of avoiding contamination uses micro electromechanical structure (MEMS) covers 416 positioned over each opening. MEMS cover 416 may open for a short time interval allowing droplets to be ejected and remain closed during other time periods. In one embodiment, the cover, whether a large area cover or a MEMS covers, may be electronically controlled such that the ejection of droplets causes the cover to automatically retract out of the path of the ejected droplets. Such electronic control may be achieved by synchronizing a cover control with the electrical impulse driving the transducers.


Besides particulate contamination, bacterial contamination should also be minimized. One method of controlling bacterial contamination is to regularly sterilize the ejector head using UV radiation. However, may patients do not have the discipline to regularly sterilize the ejector head. One method of forcing a regular sterilization schedule is to automatically expose the ejector heads to UV radiation whenever the inhaler power supply is being recharged.


Often, even with sterilization and covers, some contamination of the ejector heads over time is inevitable. Furthermore, when Fresnel zone plates are used as acoustic lenses, the ejector may be hard to clean making it difficult to use the same ejector head with several different medications. Plastic spherical lenses are easier to clean and can be used at lower frequencies, such as are typically associated with a capillary action droplet ejector. In systems where several different medications are being administered or where the ejector becomes otherwise contaminated, the ejector head 420 detaches from a body of the inhaler and can be replaced by a replacement head or a disposable ejector head. A clip-on or other fastener mechanism attaches ejector head 420 to the body. In one embodiment of the invention, an ultraviolet (UV) radiation source 430 sterilizes ejector head 420.



FIG. 5 shows a cut away side view of one embodiment of inhaler 500 including ejector head 504 and body 508. Electrical conductors 512 connect each piezoelectric element 516 in ejector head 504 to a power source 520 when a switch 524 is closed. The power source may be a battery such as an alkaline or nickel/cadmium battery.


A typical ejector uses approximately two nanojoules of acoustic energy at the liquid surface per drop of liquid ejected. Multiplying the power needed at the liquid surface by the loss factor of the ejector results in an approximate power requirement of 20 nanojoules per ejector at the ejector head. The total power used is calculated by multiplying the power per ejector at the ejector head by the total number of ejectors. To deliver a 100 microliter dose five times a day, the total power requirement is approximately 140 joules which is well within the power capabilities of most batteries, including most rechargeable nickel/cadmium batteries.


In one embodiment of the invention, a handle 527 of the AIP inhaler includes a container that stores a reservoir 525 of medication. When the ejector head is attached to the inhaler body, a pipe 529, typically a hypodermic needle punctures a seal 531 that seals the reservoir 525 of medication. Typically, seal 531 is a rubber gasket that covers a section of the container of medication. A second pressurization needle 533 also punctures the rubber gasket and pumps gas into reservoir 525 slightly pressurizing the medication. The applied pressure should be sufficient to force the medication up pipe 529; however, the pressure should not be excessive such that it breaks the surface tension at the openings of the ejector head. Breaking the surface tension will prematurely force medication from the openings of the ejector head. Pressure detection system 535 monitors the pressure differential between the ambient surroundings and the pressure inside reservoir 525 and maintains the desired pressure to keep fluid in the ejector head without breaking the surface tension of each opening.


When drops are to be ejected, ejection switch 524 is closed. Closing ejection switch 524 activates the ejectors on ejector head 504 for a predetermined time interval. In one embodiment the invention, switch 524 is a trigger 526. After the droplet ejectors are placed in close proximity to an oral cavity, a patient presses trigger 526 closing of switch 524. Closing switch 524 cause the ejection of medication. In a second implementation of a switch control, an airspeed detector 527 controls the closing of switch 524. In particular, when an inhalation by the patient causes the speed of air around the ejectors to approximately match the expected speed of ejected droplets, the airspeed detector closes switch 524. The matched air speed provides an optimal air current for carrying droplets from the ejector into a patient's lungs.


Dosage setting switch 528 allows the user to adjust the dosage of medication provided by adjusting the duration of ejector operation after switch 524 is closed. In the illustrated embodiment, dosage setting switch 528 controls timer 532. Timer 532 determines a time duration over which power is provided to piezoelectric 516. The time interval is typically proportional to the dosage set on dosage setting switch 528. When all ejectors are fired, the time interval is typically the dosage divided by the total output of ejectors on ejector head 504 per unit time.


When small dosages are desired, the dosage setting switch 528 may be programmed to reduce the number of ejectors fired on ejector head 504 by adjusting a control signal. The control signal switches ejectors in drive circuit 536. Reducing the number of ejectors fired reduces the output of pharmaceutical product per unit time. The duration of ejector firing may also be selected based on the droplet ejector switching mechanism. When an airspeed detector 527 is used, extension of the pharmaceutical discharge time may be undesirable. Instead, it may be desirable to maximize the ejection of droplets during a very short time interval to take advantage of the optimal air speed, thus typically all ejectors will fire for a fraction of a second. However, in trigger based or manual operation, it may be desirable to extend the time interval slightly to allow for imprecise synchronization between ejection of droplets and inhalation.


Drive circuit 536 provides the drive signal to the ejectors on ejector head 504. In a simple implementation of drive circuit 536, all ejectors are simultaneously activated. Thus, in one embodiment of the invention, all ejectors may be connected in parallel such that closing switch 524 results in simultaneous ejection of droplets from all ejectors. However, circumstances may dictate that all ejectors not be fired at once. For example, when power source 520 is low on energy and needs recharging, the electric current provided may be insufficient to fire all ejectors simultaneously. In such cases, the drive circuit may detect the lower power output and fire different ejectors at different times or switch some ejectors off altogether with a corresponding increase in time duration to allow dispensing of the recommended dosage. As previously described, a request for a very low dosage may also result in firing of less than all of the ejectors at once. System design my also dictate that not all ejectors are fired at once. Typically, RF power is power is switched on to a group of ejectors for a time duration, on the order of microseconds, and then switched off for several microseconds. In order to minimize the peak power requirements of the inhale when the RF power is switched off to the group of ejectors, a second group of ejectors may receive RF power. Thus in one embodiment, the drive circuit 536 includes a multiplexing circuit that may alternately switch groups of ejectors on and off and avoid overlapping firing times.



FIG. 6 illustrates the use of the inhaler by a human subject. In the illustrated embodiment, the patient 600 inserts the applicator or ejector head 604 of the inhaler 608 into an oral cavity 612. After insertion of inhaler 608, a finger such as a pointer or trigger finger 616 applies pressure to a switch 620. Alternately, the inhalation of air causes an airspeed indicator to detect the airspeed in aperture 624 and trigger a switch when the airspeed reaches a desired value. Under either implementation, the switch closes at a particular point in time causing power to be provided to the ejectors for a preset time duration and the ejection of a mist of medication into oral cavity 612.


As the mist of medication is produced, the patient deeply inhales. The inhalation causes air currents 628 to carry the droplets 632 of pharmaceutical product to the patient's lungs 636 where the pharmaceutical product is absorbed. The matching of the ejection speed of droplets 632 with the speed of air currents 628 and the small size of droplets 632 maximizes the percentage of pharmaceutical product that reaches lungs 636 and minimizes the percentage of pharmaceutical product deposited on the back of the throat 640.


While the preceding invention has been described in terms of a number of specific embodiments, it will be evident to those skilled in the art that many alternatives, modifications and variations may be performed while still remaining within the scope of the teachings contained herein. For example, specific power consumption of ejectors, ejector arrangements, methods of switching on the ejectors and methods of maintaining sterility of the inhaler have been described. However, such details should not be used to limit the scope of the invention and are merely provided to serve as examples for performing the claimed invention and lend clarity to the description. Accordingly, the present invention should not be limited by the embodiments used to exemplify it, but rather should be considered to be within the spirit and scope of the following claims and its equivalents, including all such alternative, modifications and variations.

Claims
  • 1. An apparatus for delivering a pharmaceutical product comprising: a first driver element to generate acoustic energy, the first driver element generating acoustic energy in pulses that are of a short duration and low frequency such that a droplet of pharmaceutical product is output from a capillary wave;a first acoustic lens positioned between the first driver element and the capillary wave to focus the acoustic energy generated by the first driver element;a delivery system to maintain the pharmaceutical product in a position to receive the acoustic energy from the first acoustic lens and cause ejection of the droplet of pharmaceutical product;a portable energy source to provide energy to the first driver element; anda second driver element coupled to the portable energy source to provide drive signal to ejectors that eject droplets of the pharmaceutical product, wherein the second driver element includes a multiplexing circuit that directs RF energy from the portable energy source to alternately switch groups of the ejectors on and off.
  • 2. The apparatus of claim 1 wherein the first acoustic lens is a fresnel lens.
  • 3. The apparatus of claim 1 wherein the first acoustic lens is a plastic lens.
  • 4. The apparatus of claim 1 further comprising: a second acoustic lens to focus the energy generated by the first driver element and cause ejection of a second droplet of pharmaceutical product.
  • 5. The apparatus of claim 1 further comprising: a MEMS cover to that protects the driver element from contamination when the driver element is not outputting acoustic energy.
  • 6. The apparatus of claim 1 wherein the delivery system includes a section for insertion into a human orifice, the section for insertion into the human orifice to increase an amount of the pharmaceutical product delivered to a patient.
  • 7. The apparatus of claim 1 wherein the capillary wave is generated by relaxation of a principle mound.
  • 8. An apparatus for delivering a pharmaceutical product comprising: a first driver element to generate acoustic energy, the first driver element designed to generate acoustic energy in pulses that are of a short duration and low frequency such that a plurality of droplets of pharmaceutical product is output from a capillary wave wherein the first driver element is programmed to output acoustic energy at a frequency below 15 MHz;an acoustic lens positioned between the first driver element and the capillary wave to focus the acoustic energy generated by the first driver element;a delivery system to maintain the pharmaceutical product in a position to receive the acoustic energy from the acoustic lens and cause ejection of the droplets of pharmaceutical product;an energy source to provide energy to the first driver element; anda second driver element coupled to the energy source to provide drive signal to ejectors that eject the plurality of droplets of the pharmaceutical product, wherein the second driver element includes a multiplexing circuit that directs RF energy from the energy source to switch one or more groups of the ejectors on and off.
  • 9. The apparatus of claim 8 wherein the droplets of pharmaceutical product output due to capillary action are less than 10 micrometers in diameter.
  • 10. An apparatus for delivering a pharmaceutical product comprising: a first driver element to generate acoustic energy below 15 Mhz directed to a capillary wave;an acoustic lens positioned between the first driver element and the capillary wave to focus the acoustic energy generated by the first driver element;a delivery system to maintain the pharmaceutical product in a position to receive the acoustic energy from the acoustic lens and cause ejection of a droplet of pharmaceutical product, the delivery system including a pressurization system that controls pressure of the pharmaceutical product;an energy source to provide energy to the first driver element; anda second driver element coupled to the energy source to provide drive signal to ejectors that droplets of the pharmaceutical product, wherein the second driver element includes a multiplexing circuit that directs RF energy from the energy source to switch one or more groups of the ejectors on and off.
  • 11. The apparatus of claim 10 further comprising: an ejector head to cover the acoustic lens, the ejector head being sterilized by an ultraviolet radiation source.
  • 12. An apparatus to output pharmaceutical product for inhalation into the respiratory system of a patient, the apparatus comprising: a portable energy supply;at least one transducer coupled to the portable energy supply, the at least one transducer to output acoustic energy below 15 Mhz and directed to a capillary wave;a plurality of lenses positioned between the at least one transducer and the capillary wave to receive and focus energy from the at least one transducer;a delivery system to maintain a reservoir of pharmaceutical product, a distance from a top surface of a lens and a surface of the reservoir of pharmaceutical product being less than 150 micro meters, the reservoir of pharmaceutical product to receive energy from the plurality of lenses, the received energy to cause ejection of a plurality of droplets; anda drive circuit coupled to the portable energy source to provide drive signal to ejectors that eject droplets of the pharmaceutical product, wherein the second driver element includes a multiplexing circuit that directs RF energy from the portable energy source to alternately switch groups of the ejectors on and off.
  • 13. The apparatus of claim 12 wherein each lens in the plurality of lenses is a Fresnel lens.
  • 14. The apparatus of claim 12 wherein each lens in the plurality of lenses is a plastic lens.
  • 15. The apparatus of claim 12 further comprising: a circuit that detects a flow of air going into a patient's lungs and couples the transducer to the portable energy supply when a critical air speed is reached.
  • 16. The apparatus of claim 12 wherein a diameter of at least one droplet in the plurality of droplets is less than 5 micrometers.
  • 17. A method of delivering pharmaceutical product comprising: generating a pulse of acoustic energy, the pulse having a short duration and low frequency such that the pulse of acoustic energy generates capillary waves, at least one capillary wave ejecting at least one droplet of pharmaceutical product;generating a drive signal to ejectors that eject droplets of the pharmaceutical product, wherein generating the drive signal includes multiplexing RF energy from an energy source to alternately switch groups of the ejectors on and off;focusing the acoustic energy between the pulse of acoustic energy and the capillary waves; and,positioning the droplet near a human orifice for inhalation into a respiratory system.
  • 18. The method of claim 17 wherein the at least one capillary wave is formed by the relaxation of at least one principal mound of pharmaceutical product.
  • 19. The method of claim 18 wherein the at least one principal mound is generated by focusing the pulse of acoustic energy.
  • 20. An apparatus comprising: a pharmaceutical product;a first driver element to generate acoustic energy, the first driver element generating acoustic energy in pulses that are of a short duration and low frequency such that a droplet of the pharmaceutical product is output from a capillary wave;an acoustic lens positioned between the driver element and the capillary wave to focus the acoustic energy generated by the first driver element;a delivery system to maintain the pharmaceutical product in a position to receive the acoustic energy from the acoustic lens and cause ejection of the droplet of the pharmaceutical product; anda second driver element coupled to a portable energy source to provide drive signal to ejectors that eject droplets of the pharmaceutical product, wherein the second driver element includes a multiplexing circuit that directs RF energy from the portable energy source to alternately switch groups of the ejectors on and off.
US Referenced Citations (43)
Number Name Date Kind
3387607 Gauthier et al. Jun 1968 A
3433461 Scarpa Mar 1969 A
4001650 Romain Jan 1977 A
4044273 Kanda et al. Aug 1977 A
4319155 Nakai et al. Mar 1982 A
4424465 Ohigashi et al. Jan 1984 A
4719480 Elrod et al. Jan 1988 A
4748461 Elrod May 1988 A
4751530 Elrod et al. Jun 1988 A
4976259 Higson et al. Dec 1990 A
5028937 Khuri-Yakub et al. Jul 1991 A
5063922 Hakkinen Nov 1991 A
5122818 Elrod et al. Jun 1992 A
5231426 Sweet Jul 1993 A
5268610 Hadimioglu et al. Dec 1993 A
5339101 Rawson et al. Aug 1994 A
5372126 Blau Dec 1994 A
5415161 Ryder May 1995 A
5485828 Hauser Jan 1996 A
5485928 Hauser Jan 1996 A
5497763 Lloyd et al. Mar 1996 A
5565113 Hadimioglu et al. Oct 1996 A
5722479 Oeftering Mar 1998 A
5803099 Sakuta et al. Sep 1998 A
5823428 Humberstone et al. Oct 1998 A
5855203 Matter Jan 1999 A
5894841 Voges Apr 1999 A
5912679 Takayama et al. Jun 1999 A
5996903 Asai et al. Dec 1999 A
6012454 Hodson et al. Jan 2000 A
6014970 Ivri et al. Jan 2000 A
6045208 Hirahara et al. Apr 2000 A
6120449 Snyder et al. Sep 2000 A
6136210 Biegelsen et al. Oct 2000 A
6182655 Keller et al. Feb 2001 B1
6200491 Zesch et al. Mar 2001 B1
6205999 Ivri et al. Mar 2001 B1
6302524 Roy Oct 2001 B1
6328421 Kojima et al. Dec 2001 B1
6601581 Babaev Aug 2003 B1
6622720 Hadimioglu Sep 2003 B2
6740530 Bruce et al. May 2004 B1
6861034 Elrod et al. Mar 2005 B1
Related Publications (1)
Number Date Country
20020073990 A1 Jun 2002 US