CA2463660C - Inhalation device - Google Patents
Inhalation device Download PDFInfo
- Publication number
- CA2463660C CA2463660C CA002463660A CA2463660A CA2463660C CA 2463660 C CA2463660 C CA 2463660C CA 002463660 A CA002463660 A CA 002463660A CA 2463660 A CA2463660 A CA 2463660A CA 2463660 C CA2463660 C CA 2463660C
- Authority
- CA
- Canada
- Prior art keywords
- dry powder
- powder inhaler
- inhaler according
- powder
- electronic circuitry
- Prior art date
- Legal status (The legal status 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 status listed.)
- Expired - Lifetime
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- 239000000843 powder Substances 0.000 claims abstract description 106
- 229940112141 dry powder inhaler Drugs 0.000 claims abstract description 26
- 230000006872 improvement Effects 0.000 claims abstract description 3
- 230000007613 environmental effect Effects 0.000 claims description 3
- 230000000670 limiting effect Effects 0.000 claims description 2
- 239000003814 drug Substances 0.000 description 107
- 229940079593 drug Drugs 0.000 description 89
- 239000002245 particle Substances 0.000 description 67
- 239000002775 capsule Substances 0.000 description 44
- 230000006870 function Effects 0.000 description 14
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- 238000004519 manufacturing process Methods 0.000 description 11
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- 230000008901 benefit Effects 0.000 description 4
- 239000000969 carrier Substances 0.000 description 4
- 238000007599 discharging Methods 0.000 description 4
- 239000012530 fluid Substances 0.000 description 4
- 230000003434 inspiratory effect Effects 0.000 description 4
- 238000002483 medication Methods 0.000 description 4
- 238000010521 absorption reaction Methods 0.000 description 3
- 238000012387 aerosolization Methods 0.000 description 3
- 230000007423 decrease Effects 0.000 description 3
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- 238000005516 engineering process Methods 0.000 description 3
- 230000000241 respiratory effect Effects 0.000 description 3
- 241000699670 Mus sp. Species 0.000 description 2
- 208000003251 Pruritus Diseases 0.000 description 2
- BUGBHKTXTAQXES-UHFFFAOYSA-N Selenium Chemical compound [Se] BUGBHKTXTAQXES-UHFFFAOYSA-N 0.000 description 2
- 239000000443 aerosol Substances 0.000 description 2
- 238000004220 aggregation Methods 0.000 description 2
- NDAUXUAQIAJITI-UHFFFAOYSA-N albuterol Chemical compound CC(C)(C)NCC(O)C1=CC=C(O)C(CO)=C1 NDAUXUAQIAJITI-UHFFFAOYSA-N 0.000 description 2
- 230000003444 anaesthetic effect Effects 0.000 description 2
- 208000006673 asthma Diseases 0.000 description 2
- 239000011324 bead Substances 0.000 description 2
- 238000001514 detection method Methods 0.000 description 2
- 238000011161 development Methods 0.000 description 2
- 201000010099 disease Diseases 0.000 description 2
- 208000037265 diseases, disorders, signs and symptoms Diseases 0.000 description 2
- 230000005686 electrostatic field Effects 0.000 description 2
- 239000000945 filler Substances 0.000 description 2
- 238000010884 ion-beam technique Methods 0.000 description 2
- 239000007788 liquid Substances 0.000 description 2
- 239000006199 nebulizer Substances 0.000 description 2
- 229960002052 salbutamol Drugs 0.000 description 2
- 229910052711 selenium Inorganic materials 0.000 description 2
- 239000011669 selenium Substances 0.000 description 2
- 239000000126 substance Substances 0.000 description 2
- 239000000758 substrate Substances 0.000 description 2
- 235000012431 wafers Nutrition 0.000 description 2
- 241000132092 Aster Species 0.000 description 1
- XUKUURHRXDUEBC-KAYWLYCHSA-N Atorvastatin Chemical compound C=1C=CC=CC=1C1=C(C=2C=CC(F)=CC=2)N(CC[C@@H](O)C[C@@H](O)CC(O)=O)C(C(C)C)=C1C(=O)NC1=CC=CC=C1 XUKUURHRXDUEBC-KAYWLYCHSA-N 0.000 description 1
- IVRMZWNICZWHMI-UHFFFAOYSA-N Azide Chemical compound [N-]=[N+]=[N-] IVRMZWNICZWHMI-UHFFFAOYSA-N 0.000 description 1
- GUBGYTABKSRVRQ-QKKXKWKRSA-N Lactose Natural products OC[C@H]1O[C@@H](O[C@H]2[C@H](O)[C@@H](O)C(O)O[C@@H]2CO)[C@H](O)[C@@H](O)[C@H]1O GUBGYTABKSRVRQ-QKKXKWKRSA-N 0.000 description 1
- 241000594011 Leuciscus leuciscus Species 0.000 description 1
- 241001465754 Metazoa Species 0.000 description 1
- 229920002472 Starch Polymers 0.000 description 1
- RTAQQCXQSZGOHL-UHFFFAOYSA-N Titanium Chemical compound [Ti] RTAQQCXQSZGOHL-UHFFFAOYSA-N 0.000 description 1
- 230000009471 action Effects 0.000 description 1
- 239000000654 additive Substances 0.000 description 1
- 230000000996 additive effect Effects 0.000 description 1
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- 230000002776 aggregation Effects 0.000 description 1
- 238000004458 analytical method Methods 0.000 description 1
- 238000013459 approach Methods 0.000 description 1
- DUPIXUINLCPYLU-UHFFFAOYSA-N barium lead Chemical compound [Ba].[Pb] DUPIXUINLCPYLU-UHFFFAOYSA-N 0.000 description 1
- 229910002113 barium titanate Inorganic materials 0.000 description 1
- JRPBQTZRNDNNOP-UHFFFAOYSA-N barium titanate Chemical compound [Ba+2].[Ba+2].[O-][Ti]([O-])([O-])[O-] JRPBQTZRNDNNOP-UHFFFAOYSA-N 0.000 description 1
- 239000011230 binding agent Substances 0.000 description 1
- 239000008280 blood Substances 0.000 description 1
- 210000004369 blood Anatomy 0.000 description 1
- 229940124630 bronchodilator Drugs 0.000 description 1
- 239000004067 bulking agent Substances 0.000 description 1
- 239000003990 capacitor Substances 0.000 description 1
- 230000015556 catabolic process Effects 0.000 description 1
- 229910010293 ceramic material Inorganic materials 0.000 description 1
- 230000008859 change Effects 0.000 description 1
- 239000003153 chemical reaction reagent Substances 0.000 description 1
- 239000003795 chemical substances by application Substances 0.000 description 1
- 230000003247 decreasing effect Effects 0.000 description 1
- 230000001419 dependent effect Effects 0.000 description 1
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- 230000005284 excitation Effects 0.000 description 1
- 238000002474 experimental method Methods 0.000 description 1
- 230000001939 inductive effect Effects 0.000 description 1
- 238000002347 injection Methods 0.000 description 1
- 239000007924 injection Substances 0.000 description 1
- 239000011810 insulating material Substances 0.000 description 1
- 239000012212 insulator Substances 0.000 description 1
- 230000007803 itching Effects 0.000 description 1
- 239000008101 lactose Substances 0.000 description 1
- 230000014759 maintenance of location Effects 0.000 description 1
- 230000013011 mating Effects 0.000 description 1
- 238000005259 measurement Methods 0.000 description 1
- 229910052751 metal Inorganic materials 0.000 description 1
- 239000002184 metal Substances 0.000 description 1
- 230000005012 migration Effects 0.000 description 1
- 238000013508 migration Methods 0.000 description 1
- 239000000203 mixture Substances 0.000 description 1
- 238000012544 monitoring process Methods 0.000 description 1
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- 108091008695 photoreceptors Proteins 0.000 description 1
- 239000012254 powdered material Substances 0.000 description 1
- 238000003825 pressing Methods 0.000 description 1
- 238000007639 printing Methods 0.000 description 1
- 239000003380 propellant Substances 0.000 description 1
- 230000001681 protective effect Effects 0.000 description 1
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- 210000002345 respiratory system Anatomy 0.000 description 1
- 238000007789 sealing Methods 0.000 description 1
- 239000004065 semiconductor Substances 0.000 description 1
- 230000035945 sensitivity Effects 0.000 description 1
- VYPSYNLAJGMNEJ-UHFFFAOYSA-N silicon dioxide Inorganic materials O=[Si]=O VYPSYNLAJGMNEJ-UHFFFAOYSA-N 0.000 description 1
- 239000008107 starch Substances 0.000 description 1
- 235000019698 starch Nutrition 0.000 description 1
- 150000003431 steroids Chemical class 0.000 description 1
- 238000003860 storage Methods 0.000 description 1
- 230000001360 synchronised effect Effects 0.000 description 1
- 229940124597 therapeutic agent Drugs 0.000 description 1
- 239000002699 waste material Substances 0.000 description 1
Classifications
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M15/00—Inhalators
- A61M15/0085—Inhalators using ultrasonics
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M15/00—Inhalators
- A61M15/0065—Inhalators with dosage or measuring devices
- A61M15/0068—Indicating or counting the number of dispensed doses or of remaining doses
- A61M15/008—Electronic counters
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M15/00—Inhalators
- A61M15/02—Inhalators with activated or ionised fluids, e.g. electrohydrodynamic [EHD] or electrostatic devices; Ozone-inhalators with radioactive tagged particles
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M16/00—Devices for influencing the respiratory system of patients by gas treatment, e.g. ventilators; Tracheal tubes
- A61M16/0003—Accessories therefor, e.g. sensors, vibrators, negative pressure
- A61M2016/0015—Accessories therefor, e.g. sensors, vibrators, negative pressure inhalation detectors
- A61M2016/0018—Accessories therefor, e.g. sensors, vibrators, negative pressure inhalation detectors electrical
- A61M2016/0021—Accessories therefor, e.g. sensors, vibrators, negative pressure inhalation detectors electrical with a proportional output signal, e.g. from a thermistor
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M2202/00—Special media to be introduced, removed or treated
- A61M2202/06—Solids
- A61M2202/064—Powder
Landscapes
- Health & Medical Sciences (AREA)
- Engineering & Computer Science (AREA)
- Life Sciences & Earth Sciences (AREA)
- Heart & Thoracic Surgery (AREA)
- Bioinformatics & Cheminformatics (AREA)
- Pulmonology (AREA)
- Anesthesiology (AREA)
- Biomedical Technology (AREA)
- Hematology (AREA)
- Animal Behavior & Ethology (AREA)
- General Health & Medical Sciences (AREA)
- Public Health (AREA)
- Veterinary Medicine (AREA)
- Biophysics (AREA)
- Medicinal Preparation (AREA)
- Infusion, Injection, And Reservoir Apparatuses (AREA)
Abstract
A dry powder inhaler comprises a chamber for holding a dry powder, having a vibrator operatively connected to the chamber for deaggregating the dry powder, whereupon the deaggregated dry powder may be picked up by an air stream generated by inhalation of a user, and carried for introduction into the user. The improvement of the invention lies in the presence of at least two vibrators designed to vibrate at different frequencies.
Description
WO 99164095 . ~ PCTNS99/13420 Inhalation Devise Field of the Invention 3 The present invention relates generally to the field of metering, packaging and delivery of pharmaceuticals and drugs. Particular utility for the present invention is found in the area of facilitating metering and 6 packaging of dn- powder medications and f or inhalation of powdered 7 medications, although other utilities are contemplated, including other medicament applications - g Related Art 9 'Certain diseases of the respirator~~ tract are kno«,~n to respond to treatment by the direct application of therapeutic agents. As these agents are 11 most readily available in dry powdered form, their application is most 12 conveniently accomplished by inhaling tile powdered material through the 13 nose or mouth. ~I-11IS powdered form results in the better utilization of the 1~ medicament in that the drug is deposited exactly at the site desired and where its action maybe required; hence, very nunute doses.of the drug are often 1b equally as efficacious as larger doses administered by other means, with a 17 consequent marked reduction in the incidence of undesired side effects and 18 IlledICa1'nellt cost., AlPternativelv, the drug in tl-Iis form may be used for '19 ~ treatment of diseases other than those of the respiratow svstem. When~he drug is deposited on the vem~ large surface areas of the lungs, it may be very 21 rapidlv_absorbed into the blood stream; hence, this method of application 22 may take the place of administration by injection, tablet, or other con~~entional 23 means.
24 It is the opinion of the pharmaceutical industry that the bioavailability of the drug is optimum when the drug particles delivered to the respiratory 26 tract are between l .to 5 microns in size: When the drug particles need to'be in 27 this size range the dry powder delivery sy stem needs to address a number of 28 issues:
29 (1) Small size particles develop an electrostatic charge on themselves during manufacturing and storage. This causes the particles to agglomerate y ' _. _ ~
WO 99/64095 ~ PCTIUS99113420 1 or aggregate, resulting in clusters of particles which have an effective size 2 greater than ~ microns. The probability of these large clusters making it to the 3 deep lungs then decreases. This in turn results in a lower percentage of the packaged drug being available to the patient for absorption. .
(2) The amount of active drug that needs to be delivered to the patient 6 may be of the order of 10s of micrograms. For example, albuterol, in the case 7 of a drug used in asthma, this is usually 25 to 50 micrograms. Current 8 manufacturing equipment can effectively deliver aliquots of drugs in 9 milligram dose range with acceptable accurac~~. So the standard practice is to 20 mix the active drug with a filler or bulking agent such as lactose, This 11 additive also makes the drug "easy to flow". This filler is also called a carrier 12 , since the drug particles also stick to 'these particles through electrostatic or 23 chemical bonds. These carrier particles are vert-~ much larger than the drug 1~ particles in size. The ability of the dry powder inhaler to sepaiate drug from , the carrier is an important performance parameter in the effectiveness of the 15 design.
17 (3) Active drug particles with sizes greater than ~ microns will be 18 deposited either in the mouth or throat. This introduces another level of 19 uncertainty since the bioavaiiability and-absorption of the drug in these a locations is different from the lungs. D-ry powder inhalers need to muumize 21 the drug deposited in these locations to reduce the uncertainty associated 22 with the bioavailability of the drug.
23 Prior art dry powder inhalers (DPIs) usually have a means for 24 introducing the drug (active drug plus carrier) .into a high velocity air stream.
The high velocity air-stream is used as the primary mechanism for br Baking , 26 up the cluster of micronized particles or separ sting the drug particles from 27 the carrier. Several inhalation devices useful for dispensing this powder form 28 of medicament are known in the prior art. For example, in U.S. Patent Nos.
29 3,507,277; 3,518,992; 3,635,219; 3,795,24; and 3,807,400, inhalation devices are J
' _.
WO 99!64095 r ' ~ ~ ~j'~ ~ PCTIUS99/13420 1 disclosed having means for piercing of a capsule containing a powdered 2 medicament, «which upon inhalation is drawn out of the pierced capsule and 3 into the user's mouth. Several.of these patents disclose propeller means, :l ~~hich upon inhalation aid in dispensing the powder out of the capsule, so that it is not necessary to rely solely on the inhaled air to suction powder from 6 the capsule: For example, in U.S. Patent No. 2,517,48?, a device i5 disclosed 7 hav ing a powder containing capsule placed in a Iower chamber before 8 inhalation, where it is pierced by manual depression of a piercing pin by the 9 user. Aster piercing, inhalation is beg~.m and the capsule is drawn into an upper chamber of the device where it mov es about in all directions to cause a 11 dispensing of powder through the pierced holes and into the inhaled air 12 stream. U.S. Patent No. 3,831,606 discloses an inhalation device having 13 multiple piercing pins, propeller means, and a self-contained power source 14 for operating the propeller means via external manual manipulation, so that upon inhalation the propeller means aids in dispensing the powder into the 16 stream of inhaled air. See also U.S. Patent No. 5,458,135.
17 These prior art devices present several problems and possess several 18 disadvantages which are remedied by the inhalation de~~ices of the present 19 invention. For instance, these prior art devices require that the user exert considerable effort in inhalation to effect dispensing or withdrawal of powder 21 from a pierced capsule into the inhaled air stream. With these prior art 22 devices, suction of powder through the pierced holes in the capsule caused by 23 inhalation generally does not withdraw all or even most of the powder out of 24 the capsule, thus causing a waste of the medicament. also, such prior art devices result in unr_ontroiled amounts or clumps of po~n~dered material being 26 inhaled into the user's mouth, rather than a constant inhalation of controlled 27 amounts of finely dispersed powder.
28 The above description of the prior art is taken largely from U,S. Pat.
29 No. 3,948,264 to Wilke et al, who disclose a device for facilitating inhalation of WO 99164095 p PCT/US99113420 1 a powdered medication that includes a body portion having primary and 2 secondary air inlet channels and an outlet channel. The secondary inlet 3 channel provides an enclosure for a capsule containing the powdered medication and the outlet channel is formed as a mouthpiece protruding from the body. A capsule piercing structure is provided, which upon rotation puts 6 one or more holes in the capsule so that upon vibration of the capsule by an 7 electro-mechanical vibrator, the powdered drug may be released froze the 8 capsule. The piercing means disclosed in Wilke et a1 includes three radially 9 mounted, spring-biased piercing needles mounted in a trochoidal chamber.
Upon hand rotation of the chamber,~simultaneaus inward radial motion of the I1 needles pierces the capsule. Further rotation of the chamber allows the 12 needles to be retracted by their spring mountings to their original positions to 13 withdraw the needles from the capsule. The electromechanical vibrator 14 includes, at its innermost end, a vibrating plunger rod which projects into the intersection of the inlet channel and the outlet channel. Connected to the 16 plunger rod is a mechanical solenoid buzzer for energizing the rod to vibrate.
17 The buzzer is powered by a high energy electric cell and is activated by an 18 external button switch. According to Wilke et al, upon inhalation through 19 outlet channel 3 and concurrent pressing of switch 10d to activate the electromechanical vibrating means 10, air is sucked through inlet channels 4 21 and 12 and the air stream through the secondary inlet channel ~ raises the 22 capsule up against the vibrating plunger rod 10a. The capsule is thus vibrated 23 rapidly c~~ith powder being tluidized and dispensed from the pierced holes 24 therein. (This technique is commonly used in .manufacturing for dispensing powder through a hopper where the hopper is vibrated to fluidize the , 26 powder and move it through the hopper outlet. The pierced holes in the 27 capsule represent the hopper outlet.) The air stream through inlet channel ~
28 and I2 aids in withdrawal of powder from the capsule and carries this 29 powder through the outlet channel 3 to the mouth of the user." (Wilke et al, .
24 It is the opinion of the pharmaceutical industry that the bioavailability of the drug is optimum when the drug particles delivered to the respiratory 26 tract are between l .to 5 microns in size: When the drug particles need to'be in 27 this size range the dry powder delivery sy stem needs to address a number of 28 issues:
29 (1) Small size particles develop an electrostatic charge on themselves during manufacturing and storage. This causes the particles to agglomerate y ' _. _ ~
WO 99/64095 ~ PCTIUS99113420 1 or aggregate, resulting in clusters of particles which have an effective size 2 greater than ~ microns. The probability of these large clusters making it to the 3 deep lungs then decreases. This in turn results in a lower percentage of the packaged drug being available to the patient for absorption. .
(2) The amount of active drug that needs to be delivered to the patient 6 may be of the order of 10s of micrograms. For example, albuterol, in the case 7 of a drug used in asthma, this is usually 25 to 50 micrograms. Current 8 manufacturing equipment can effectively deliver aliquots of drugs in 9 milligram dose range with acceptable accurac~~. So the standard practice is to 20 mix the active drug with a filler or bulking agent such as lactose, This 11 additive also makes the drug "easy to flow". This filler is also called a carrier 12 , since the drug particles also stick to 'these particles through electrostatic or 23 chemical bonds. These carrier particles are vert-~ much larger than the drug 1~ particles in size. The ability of the dry powder inhaler to sepaiate drug from , the carrier is an important performance parameter in the effectiveness of the 15 design.
17 (3) Active drug particles with sizes greater than ~ microns will be 18 deposited either in the mouth or throat. This introduces another level of 19 uncertainty since the bioavaiiability and-absorption of the drug in these a locations is different from the lungs. D-ry powder inhalers need to muumize 21 the drug deposited in these locations to reduce the uncertainty associated 22 with the bioavailability of the drug.
23 Prior art dry powder inhalers (DPIs) usually have a means for 24 introducing the drug (active drug plus carrier) .into a high velocity air stream.
The high velocity air-stream is used as the primary mechanism for br Baking , 26 up the cluster of micronized particles or separ sting the drug particles from 27 the carrier. Several inhalation devices useful for dispensing this powder form 28 of medicament are known in the prior art. For example, in U.S. Patent Nos.
29 3,507,277; 3,518,992; 3,635,219; 3,795,24; and 3,807,400, inhalation devices are J
' _.
WO 99!64095 r ' ~ ~ ~j'~ ~ PCTIUS99/13420 1 disclosed having means for piercing of a capsule containing a powdered 2 medicament, «which upon inhalation is drawn out of the pierced capsule and 3 into the user's mouth. Several.of these patents disclose propeller means, :l ~~hich upon inhalation aid in dispensing the powder out of the capsule, so that it is not necessary to rely solely on the inhaled air to suction powder from 6 the capsule: For example, in U.S. Patent No. 2,517,48?, a device i5 disclosed 7 hav ing a powder containing capsule placed in a Iower chamber before 8 inhalation, where it is pierced by manual depression of a piercing pin by the 9 user. Aster piercing, inhalation is beg~.m and the capsule is drawn into an upper chamber of the device where it mov es about in all directions to cause a 11 dispensing of powder through the pierced holes and into the inhaled air 12 stream. U.S. Patent No. 3,831,606 discloses an inhalation device having 13 multiple piercing pins, propeller means, and a self-contained power source 14 for operating the propeller means via external manual manipulation, so that upon inhalation the propeller means aids in dispensing the powder into the 16 stream of inhaled air. See also U.S. Patent No. 5,458,135.
17 These prior art devices present several problems and possess several 18 disadvantages which are remedied by the inhalation de~~ices of the present 19 invention. For instance, these prior art devices require that the user exert considerable effort in inhalation to effect dispensing or withdrawal of powder 21 from a pierced capsule into the inhaled air stream. With these prior art 22 devices, suction of powder through the pierced holes in the capsule caused by 23 inhalation generally does not withdraw all or even most of the powder out of 24 the capsule, thus causing a waste of the medicament. also, such prior art devices result in unr_ontroiled amounts or clumps of po~n~dered material being 26 inhaled into the user's mouth, rather than a constant inhalation of controlled 27 amounts of finely dispersed powder.
28 The above description of the prior art is taken largely from U,S. Pat.
29 No. 3,948,264 to Wilke et al, who disclose a device for facilitating inhalation of WO 99164095 p PCT/US99113420 1 a powdered medication that includes a body portion having primary and 2 secondary air inlet channels and an outlet channel. The secondary inlet 3 channel provides an enclosure for a capsule containing the powdered medication and the outlet channel is formed as a mouthpiece protruding from the body. A capsule piercing structure is provided, which upon rotation puts 6 one or more holes in the capsule so that upon vibration of the capsule by an 7 electro-mechanical vibrator, the powdered drug may be released froze the 8 capsule. The piercing means disclosed in Wilke et a1 includes three radially 9 mounted, spring-biased piercing needles mounted in a trochoidal chamber.
Upon hand rotation of the chamber,~simultaneaus inward radial motion of the I1 needles pierces the capsule. Further rotation of the chamber allows the 12 needles to be retracted by their spring mountings to their original positions to 13 withdraw the needles from the capsule. The electromechanical vibrator 14 includes, at its innermost end, a vibrating plunger rod which projects into the intersection of the inlet channel and the outlet channel. Connected to the 16 plunger rod is a mechanical solenoid buzzer for energizing the rod to vibrate.
17 The buzzer is powered by a high energy electric cell and is activated by an 18 external button switch. According to Wilke et al, upon inhalation through 19 outlet channel 3 and concurrent pressing of switch 10d to activate the electromechanical vibrating means 10, air is sucked through inlet channels 4 21 and 12 and the air stream through the secondary inlet channel ~ raises the 22 capsule up against the vibrating plunger rod 10a. The capsule is thus vibrated 23 rapidly c~~ith powder being tluidized and dispensed from the pierced holes 24 therein. (This technique is commonly used in .manufacturing for dispensing powder through a hopper where the hopper is vibrated to fluidize the , 26 powder and move it through the hopper outlet. The pierced holes in the 27 capsule represent the hopper outlet.) The air stream through inlet channel ~
28 and I2 aids in withdrawal of powder from the capsule and carries this 29 powder through the outlet channel 3 to the mouth of the user." (Wilke et al, .
WO 99164095 ' - , - ' PCTIUS99113420 1 column 3, lines ~5-55). Wilke et al further discloses that the electromechanical vibrator means may be placed at a right angle to the inlet chamber and that 3 the amplitude and frequency of vibration may be altered to regulate =1 dispensing characteristics of the inhaler.
Thus, as noted above, the vibrator in Wilke et al's disclosed inhaler is 6 an electromechanical device consisting of a rod driven by a solenoid buzzer.
7 (This electromechanical means may be a motor driving a cam [Col. ~, Line 8 ~0]}. A disadvantage of the inhaler implementation as disclosed by Wilke is 9 the relatively large mechanical movement required of the rod to effectively vibrate the capsules. The large movement of the rod, usually around 100s of 12 mice ons, is necessary due to the elasticity of the capsule walls and inertia of I2 the drug and capsule.
I3 Moreover, solenoid buzzers typically have operating frequencies less 14 than 5 Khz. This operating frequency tends to be noisy and therefore is not I5 desirable when incorporated into a dry powder inhaler from a patient's 16 perspective. A hirther disadvantage of the electrochemical achiators of Wilke I7 is the requirement for a high energy source {Wilke et al, CoI. 3, line 38), thus 18 requiring a lame battery source or frequent changes of the battery pack for 19 portable units. Both these features are not desirable from a patient safety and "ease of use" standpoint.
2I The inhaler of Wilke et al is primarily intended to reduce the amount of 22 powder Ieft behind in the capsule relative to other inhalers cited in the patent 24 disclosure. (~'~'ilke et al, Col. ~, Iines 59-68; Col. 5, lines I-48).
However, Wilke 24 et aI does not address the need to deaggregate the po~nrder into particle sizes or groups less than 6 microns in size as is required for effective delivery of the 26 medication to the lungs; rather Wilke et aI, like the prior art inhalers continues 27 to rely on the air stream velocity to deaggregate the powder ejected into the 28 air stream, into particle sizes suitable for delivery to the lungs.
Thus, as noted above, the vibrator in Wilke et al's disclosed inhaler is 6 an electromechanical device consisting of a rod driven by a solenoid buzzer.
7 (This electromechanical means may be a motor driving a cam [Col. ~, Line 8 ~0]}. A disadvantage of the inhaler implementation as disclosed by Wilke is 9 the relatively large mechanical movement required of the rod to effectively vibrate the capsules. The large movement of the rod, usually around 100s of 12 mice ons, is necessary due to the elasticity of the capsule walls and inertia of I2 the drug and capsule.
I3 Moreover, solenoid buzzers typically have operating frequencies less 14 than 5 Khz. This operating frequency tends to be noisy and therefore is not I5 desirable when incorporated into a dry powder inhaler from a patient's 16 perspective. A hirther disadvantage of the electrochemical achiators of Wilke I7 is the requirement for a high energy source {Wilke et al, CoI. 3, line 38), thus 18 requiring a lame battery source or frequent changes of the battery pack for 19 portable units. Both these features are not desirable from a patient safety and "ease of use" standpoint.
2I The inhaler of Wilke et al is primarily intended to reduce the amount of 22 powder Ieft behind in the capsule relative to other inhalers cited in the patent 24 disclosure. (~'~'ilke et al, Col. ~, Iines 59-68; Col. 5, lines I-48).
However, Wilke 24 et aI does not address the need to deaggregate the po~nrder into particle sizes or groups less than 6 microns in size as is required for effective delivery of the 26 medication to the lungs; rather Wilke et aI, like the prior art inhalers continues 27 to rely on the air stream velocity to deaggregate the powder ejected into the 28 air stream, into particle sizes suitable for delivery to the lungs.
. _.-_. , I ' 1 a WO 99/64095 ~ , PCTlUS99)1342U
1 ~ Another prior art inhalation device is disclosed in Burns et al U.S.
2 Patent No. 5,28,233. In this device, a liquid medication is atomized by an 3 ultrasonic device such as a piezo element (Burns et al, Col.10, lines 36-51). A
stream of air, usually at a high velocity, or a propellant then carries the atomized particles to the patient. The energy required to atomize the liquid 6 medication in the nebulizer is prohibitivelyT hi~,Yh, making.this approach for 7 the delivery of drugs to the lungs only feasible as a desk top unit.
The..high - 8 voltage requirements to drive the piezo, to produce the necessary mechanical 9 displacements, also sEwerely effects the weight and size of the device. It is also not obvious that the nebulizer operating principles can be applied to the 11 dry powder inhalers for delivery or powder medication to the lungs.
12 The prior art devices therefore have a number of disadvantages which 13 makes them less than desirable foi the delivery of dry powder to the lungs.
14 Some of these disadvantages are:
~ The performance of the prior art inhalers depends on the flowrate 16 generated by the user. Lower flowrate does not result in the 17 powder being totally deaggregated and hence adversely affects the 18 dose delivered to the patient.
19 ~ Inconsistency in the bioavailabilitv of the drugs from dose-to-dose because of lack of consistency in the deaggregation process.
21 ~ Lar4 a energ~T requirements for' driving the electromechanical based 22 inhalers which increases the size of the devices making them 23 unsuitable for portable use.
24 In our prior U.S. Patent No. 5,694,920, issued December 9,1997, ~~e provide an inhaler that utilizes vibration to facilitate suspension of powder 26 into a gas that overcomes the aforesaid and other disadvantages and 27 drawbacks of the above prior art. More particularly, the inhaler of our 28 aforesaid patent includes a piezoelectric vibrator for vibrating the powder. A
29 controller is provided for controlling supply (i.e., amplitude and/or t . z , _. _ WO 99164095 ' PCTIUS99/13420 1 frequency) of actuating electricity to the vibrator so as to cause vibration of 2 ' the powder that is adapted to optimally suspend at least a portion of the 3 powder into the gas. As described in our aforesaid patent, the controller may 4 include a user-actuable control for permitting the user to select the vibration frequencies and/or amplitudes for optimally suspending in the gas the type 6 of powder currently being used in the inhaler. The user-actuable control is 7 pre-calibrated with the controller to cause the controller to adjust the 8 Frequency and/or amplitude of actuating electricity supplied to the vibrator 9 to be that necessary far vibrating the type of po~~der selected by the user-actuablc~ control in such a way as to optimally suspend at least a portion of the 11 powder into the gas. The user-actuable control may include selection 12 gradations in terms at the average size of the powder particles to be 13 suspended iri the gas, and/or in terms of desired vibration frequencies and I4 amplitudes. Vibration frequency would be adjusted to at least about I2 ICHz, in order to optimally suspend such commonly used powdered medications in 16 the gas. Of course; vibration frequency and amplitude may be adjusted to 17 optimize suspension of the powdered medication being used.
18 An electrostatic field that is established across the air stream, whereby 19 by controlling the strength of the electrostatic field primarily only particle sizes of interest are introduced into the air steam, while larger size particles 21 are left behind in the container. This reduces the inconsistency associated 22 with the bioa~-ailability of the drug because of the large particles being 23 deposited into the mouth or throat as is common with devices described in prior art.
24 Summary of the Invention F
The present invention provides an improvement over prior art 26 inhalation de~~ices such as described in our aforesaid L:.S. Patent No.
27 5,694,920. In one embodiment of the invention, the inhaler contains two or 28 . more vibrator means or piezoelectric elements so that different drugs, i.e. of 29 different particle size, may be delivered from the same inhaler.
.
WO 99164095 ' PCT/US99li3420 1 In yet another embodiment of the invention, the piezoelectric elements 2 are switched between two. or more set frequencies, or frequencies swept so as 3 to avoid potentially setting up standing waves in the powder.
In yet another embodiment of the invention, the inhaler includes electronic circuitry for recording and/or controlling one or more functions 6 such as dose counting, patient compliance monitoring, and patient 7 compliance reminder. s. Also, the inhaler rnay be pr ogrammed according to a 8 delivery protocol, i.e. to alter the quantity of drug delivered over time.
If 9 desired, the inhaler also may include an environmental sensor and knockout control, for example,. to deactivate the inhaler in the event it is inadvertently 11 exposed to too high a temperature, a clock to deactivate the inhaler in the 12 event its shelf Iife is exceeded, and/or a security/safety lock-out.
13 Still vet another embodiment of the present invention provides aw air 14 flow sensor for controlling various components of an inhalation device.
Included in the preferred embodiment is an acoustic controller; the acoustic 16 controller including an acoustic element to sense air flow around the element 17 and for producing signals representative of a frequency and amplitude of the 18 , air t7ocl~, the signals being used to control (e.g., activated, deactiv ate, apply 19 , incremental i~oltage, etc.) certain components of the inhalation device.
' r Preferabhr, acoustic element is a microphone element or pressure 21 transducer positioned within the air passage of an inhalation device, (e.g., a 22 dry powder inhaler) that produces signals in response to the inhalation air 23 flow, these signals are used to control certain components of the inhaler;
e.g., 24 a high frequency vibrator, an electrostatic plate, timer, counter, etc.
Also preferably, these signals are used to activate/control certain components of 26 the inhalation device to maximize the inhalation effectiveness to obtain 27 maximum patient benefif from medicament.
28 Thus; the present invention provides a fully automated inhalation 29 device, that is breath activated, that perms .> optimal utilization of the ,._ 1 particular medication. For example, acoustic signals can be used to trigger 2 the high frequency vibrator and electrostatic plate only when the patient has 3 achieved optimum (e.g., maximum) inhalation effort, thereby ensuring that -1 the full (proper) dosage of medicament properly enter the patient's respiratory system. Alternatively, these signals (breath-activated signals) can 6 be used to progressively applyr increasing power to, or, sequentially .
.' activate/deactivate the various components of the inhalation device to S achieve optimal inllalatl011 dosage.
9 The present inventioiz also relates to the packagring of dry powders and particularly to the metering and packaging of precise quantities of 11 pharmaceuticals and drugs for medical uses.
12 The cer tification of new phar maceuticals is a lengthy and costly process 13 involving animal studies followed by chemical trails to establish both efficacy 2~ and safety. Because a pharmaceutical's characteristics may be affected by changes in manufacturing and/or packaging, the approval process limits the, 16 approval to a particular manufacturing and packaging process.
17 In our earlier U.S. Patent 5,699;69, granted December 23,1997, we I8 describe a method algid apparat~.is for packaging microgram quantities of fine 19 powders such as phar maceuticals using electrostatic phototechnology 2fl techniques. 1\~Iore particularly, as described in our aforesaid U:S.
Patent 21 5,699,b49, the ability of powders to acquire an electrical charge _ 22 advantageously is utilized for precisely measuring exact microgram 23 quantities of the pcJwder, whereupon these exact microgram quantities or a 2~ then placed in individual containers, and the containers sealed.
Electrostatic charge has been employed to attract a given quantity of 26 powder to a surface. An example of this is the laser printer or the electrostatic 27 copy devices where a drum is charged and toner particles are attracted and-28 held in position by the charge. The charge on the drum is neutralized by the 29 attracted toner powder, thus limiting the amount of toner in accordance with r . 1 .. . i~
1 the charge image on the drum. The charge on these printer drums is then 2 transferred to a sheet of paper or other carrier to give a final image. In our.
3 U.S. Patent 5,699,69, the same electrostatic charge technology is employed 4 for transfers ing a predetermined amount of a finely powdered pharmaceutical or drug to a carrier or an intermediate such as a drum, 6 carrying a charge of predetermined intensity and area, rotating the charged 7 drum surface; carrying the predetermined amount of powdered 8 pharmaceutical or drug on its surface, to a tr ansfer station where the charge is 9 overcome and tine dry powder is transferred to a package which is then sealed. In lieu of a drum, a belt, or other movable surface is charged to a 21 given potential in a localized area.
12 When a given amount of a powdered pharmaceutical or drug is to .be 13 packaged, the charge and. area ~of charge can be determined experimentally 14 for each dose of pharmaceutical or drug and each particle size distribution.
This can be done by controlling either the charged area for a given charge 16 density or the total electrostatic charge on any individual charged area:
These 17 conditions can be adjusted to provide essentiallv~the exact desired amount of 18 the particular pharmaceutical or drug to be transferred at the transfer station.
19 - In thepresent invention, the electrostatic charge technology described, "
in our aforesaid U.S: Patent 5,f99,649 is adopted to be used for measuring and 21 packaging unit doses of a pharmaceutical or drug in a readily ingestible form, 22 i.e. as a tablet or capsule. The technology thus described permits reproducible 23 precise measurement and packaging of a pharmaceutical or drug, and-which 24 may be scaled from laboratory to pilot plant to full scale production without the need for recertificadon.
26 Still other features and advantages of the present invention may be 2i seen from the follov~ring detailed description, taken in connection with the 28 attached drava~i.ngs, wherein like numerals depict like parts, and wherein:
. _.
2g ' Brief Description of Drawings Figure 1 is a perspective view of an inhaler of the prior art;
WO 99164095 - ~ . ~ PCT/US99/13420 1 Figure 2 is a rear plane view of the inhaler sho«-n in Figure 1;
2 Figure 3 is a longihidinal cross-sectional schematic view of the inhaler 3 of Figure 1;
4 Figure 4 is a functional block diagram of the vibration control system of one embodiment of Figure 1;
6 Figure ~ is a functional block diagram of the vibration control system 7 of another embodiment of the invention;
8 Figures 6-10 are .hmction block diagrams of the ~-ibration control 9 system in accordance with still yet other embodiments of the invention; and Figure I1 is a view, similar to Figi.ire 3 of vet another embodiment of I1 the invention.
12 Figure I' is a cross-sectional vie~.v of a typical inhalation device and the 13 acoustic controller of the present invention;
14 Figure 13 is an expanded cross-sectional view of Figure 12;
Figure I4 is a functional block diagram of a preferred embodiment of 16 the acoustic controller of the present invention;
I7 Figure l~ sho~nfs a schematic representation of the attraction of I8 negatively charged powder particles to a support haring a positive charge on 19 the surface thereof; r Figure I6 shows a block diagram of the various steps involved in 21 practicing the invention;
22 Figure I i is a schematic representation of one form of drum type 23 electrostatic device for transferring given small quantities of powdered drugs 24 from an electrostatic attraction station, where a given quantity of powdered drug is attracted to and neutralizes a given charge. on the drum, and a 26 subsequent transfer station where the drug is transferred from the drum to a 27 package therefor;
28 Figures 18 and 19 are schematic functional representations of preferred 29 components employed in the Fig. I7 type of apparatus;
_ _.. _._ WO 99/64095 '. , PCTlUS99/13420 1 ~ Figure 20 shows a different system wherein separate carriers, having 2 micronized drug particles electrostatically attached to their surface, are used 3 to carry the drug to the charged transfer surface;
Figures 2I and 22 show methods of aerosolizing the powdered drug and ionizing the~drug to give it a specific charge;
6 Figure ?3 shows a graph illustrating the percentage of suspended 7 particles as a function of time and size, permitting creation of a suspended 8 particle stream of any given desired size distribution;
9 Figur a 2~ showTs another embodiment of applying the aerosolized drug 20 to a drum carr~~ing charge "image";
11 Figure ?~ illustrates an ion projection system for creating the charge 12 "image" on a dielectric surface;
13 Figure 26 is a view similar to Fig. I6, and illustrating an alternative' 14 embodiment of the invention; .
Figure 27 is a view similar to Fig. 16, and illustrating another 16 alternative embodiment of the invention;
17 Figure 2S is a view similar to Fig. 16, and illustrating yet another 18 alternative embodiment of the invention; and 19 Figure 29 is a ~,~iew similar to Fia. 16, and illustrating still yet another alternative embodiment of the invention.
21 Figures 1-3 illustrate an embodiment 10 of inhaler made in accordance 22 with our aforesaid U.S. Patent No. 5,694,920. Inhaler 10 includes a hard 23 plastic or metal housing 18 having a generally L-shaped longitudinal cross-24 section. Housing 18 includes tour air flow openings 20, 28, 30, and 32..
Inhaler 10 includes a main air flow passage 26 wluch extends the length of the 26 housing 18 from the front 22 (at opening 20) to the rear 2=1 thereof (at opening 27 28) and has a generally square-shaped transver se cross-section, so as to permit 28 air flow therethrough (denoted by arrow F in Figure 1).
t~ _ _ WO 99/64095 n , . , . PCT/US99/13420 1 ~ Secondary air conduit 31 is generally L-shaped and runs longitudinally 2 from opening 30 in the rear 2~ surface of the housing 18 to main passage 26.
3 One-way t~lo«- valve 50 is mounted to the inner surface 33 of the main passage :l 26 via a conventional spring-biased hinge mechanism (not shown), which is adapted to cause the valve 50 to completely block air flow S through the 6 conduit 31 to the main passage 26 when the pressure of the air flow F in the 7 main passage 26 is blow a predetermined threshold indicative of inhalation 8 through the passage 26 by a user.
9 Powder dispensing chamber 54 is, formed in housing 18 for holding a capsule 34 of powder medication to be inhaled. Housing 18 includes a 12 moveable panel portion 32 in the rear 2~ for permitting the capsule 34 to be 12 introduced into the chamber 5~ and placed on the seating 52 of vibration 13 means 36 betcseen guiding means 60A, 60B. Preferably, means 36 comprises a 14 hard plastic or metallic protective shell 37 enclosing a piezoelectric vibrator , 90. (Figure ~). Preferably, vibrator 90 is inechanicaliy coupled through the 16 shell 37 via a disk (not shown) to the drug cartridge 3~ so as to permit x7 maximum vibratory energy to be tz~ansmitted from the vibrator 90 through 18 the shell 37 to the cartridge 3~. .Guiding means 60A, 60B includes two 19 surfaces which slant do~n~nwardlv toward the seating 52 so as to permit easy introduction and retention of the capsule on the seating 52 in the chamber 51.
21 Removable panel 32 includes another air inlet 3=1 for permitting additional air 22 flow S2 from the chamber 51 through conduit 61 into conduit 31 during 23 inhalation bt- the user. Preferably, panel 32 and housing 18 include 24 conventional mating mounting means {not shown) for permitting the panel 32 to be removable resecurable to the housing by the user between introduction 26 of fresh (i.e., completely full) capsules and removal of spent (i.e., empty) 27 capsules.
28 Inhaler 10 also includes a conventional miniature air stream velocity or 29 pressure sensor ~0 moiulted on the inner surface of the conduit 26 so as to _.
WO 99!64095 ~ ~ PCT/US99/13420 1 sense the speed and/or pressure of the air stream F. Preferably, sensor 40 2 comprises a cony entional spring-loaded flapper-yield switch which generates 3 electronic signals indicative of the speed and/or pressure of the air stream F
:1 in the conduit ?b, and transmits those signals via electrical connection 42 to .
electronic control circuitry 48 contained in housing 18 for controlling 6 actuation of the vibrator means based upon those signals.
7 Preferably, th~control circuitry 48 is embodied as an application 8 specific integrated circuit chip and/or some other type of very highly 9 integrated circuit chip. Alternatively, control circuitw ~8 may take the form of a microprocessor, or discrete electrical and electronic components. As will 11 he described more fully below; the control circuitry 48 determines the 12 amplitude and frequency of actuating power to be supplied from 13 conventional power source 46 (e.g., one or more D.C. batteries) to the 14 piezoelectric vibrator to thereby control vibration of the vibrator. The actuating po~n-er is supplied to the piezoelectric element 90 via electrical 16 connection 4~ between the vibrator and the circuitry 48.
17 Piezoelectric element 90 is made of a material that has a high-18 . frequency, and preferably, Ultrasonic resonant ~-ibratorv frequency (e.g., 19 about 15 to 100 MHz), and .is caused to vibrate with a particular frequency r and amplitude depending upon the frequency and/or amplitude of excitation 21 electricity applied to the piezoelectric element 90. Examples of materials that 22 can be used to comprise the piezoelectric element 90 include quartz and 23 polycrystalline ceramic materials (e.g., barium titanate and lead zirconate 24 titanate). Advantageously, by vibrating the piezoelectric element 90 at ultrasonic frequencies, the noise associated with vibrating the piezoelectric 26 element 90 at lower (i.e., non-ultrasonic) frequencies can be avoided.
27 Turning specifically to Figure :l, the various functional components 28 and operation of the control circuitry 48 will now be described. As ~~ill be 29 understood b~- Chase skilled in the art, although the functional components .
l , r , _ __ WO 99!64095 r PCT/US99/13420 1 sho~nTn in Figure ~ are directed to an analog realization of the control circuitry 2 48, the components of Figure ~ could be appropriately modified to realize 3 control circuitry ~8 in a digital embodiment without departing from this 4 embodiment 10 of the present invention.
Control circuitry ~8 preferably includes actuation controller 70 and 6 vibratory feedback control system 72. Actuation conti oiler 70 comprises a 7 conventional sc~~itching mechanism for permitting actuating power to be 8 supplied from the power source 46 to the control system 72 depending upon 9 the signals supplied to it from sensor =10 and the state of fihe power switch 12.
In other words, controller 70 permits actuating pokier to be supplied from the 12 source ~6 to the system 72 when the sliding indicator bar 1~ of switch 12 is set 12 to the "ON" position in channel track 16 and the inhalation sensor 40 supplies 13 signals to the controller 70 that indicate that the inhalation is occurring 14 through the main passage 26. F-~owever, controller 70 does not permit actuating pointer to flow from the source to the system i2 when either the 16 s~~itch 12 is Set to "OFF" or the signals supplied to the controller 70 from the 17 sensor ~0 indicate that inhalation is not taking place through the conduit 26.
28 When controller 70 first permits actuating power to be supplied from 19 the source ~6 to the feedback control system 72, the s~~stem'2 enters an initialization state wherein controllable means for supplying a predetermined 21 frequency and amplitude of actuating electricity 7~ is caused to generate 22 control signals for causing conventional pump circuit 80 to generate an initial 23 desired frequency and amplitude of actuating electricity based upon stored 24 values thereof stared in the .initialization memory means 82. Preferably, means 7~ comprises conventional frequency sweep generator and frequency 26 generator means 76 and 78, respectively. The signals generated by.means 74 27 are then supplied to charge pump circuit 80 to cause circuit 80 to supply the 28 piezoelectric element 90 with actuating electricity specified by the signals.
t t WO 99164095 ~ ~ PCTIUS99/13420 1 ~ Preferably, the initial frequency and amplitude of actuating electricity supplied to the piezoelectric element 90 is pre-calibrated to cause the 3 piezoelectric element 90 to vibrate at its resonance frequency when no :I powder cartridge or powder is placed on the means 36. As will be .
appreciated be those skilled in the art, maximum transfer of vibratory power 6 from the piezoelectric element to the powder in the container 34 takes place 7 when the piezoelectric element ~~ibrates at its resonant frequenc~.l. It has been S found that this results in maxin-tum de-aggregation and.suspension of the 9 powder from the container 3~ into the air to be inhaled by~ the user:
However, when the container 34 or powder is placed on the v ibrator means 36, the I1 weight and volume of the powder container, and the weight, volume, and 22 particular size of the powder to be suspended byr the piezoelectric element can .
13 change the vibration characteristics of the piezoelectric element, and cause the 1~ piezoelectric element to vibrate at other than its resonant frequency, Ihis can result in reduced vibratory energy transfer to the powder from the 16 piezoelectric element, and thereby, lessen the efficiency of the piezoelectric 17 element in de-aggregating and suspending the powder in the air inhaled by 18 the user.
19 ThE :feedback control system i2 overcomes this problem. In control system 7?, after the initial frequency, and amplitude of actuating electricity are 21 stlppl~ed to the piezoelectric element 90, the frequency generating means 22 svstematicalh- 'enerates control signals indicative of many~ different 23 amplitudes and freqeiencies of electricity for being supplied to the 2~ piezoelectric element 90 by the circuit 80. As the generating means 7~
"cycles through" the different freduencies and amplituades, the instantaneous power 26 transfer characteristics of the piezoelectric element 90 for each of these 27 different frequencies and amplitudes are determined by the detector 88, 28 which transmits this information to the peak power detector 86. Peak 29 detector 86 anahTzes the instantaneous power transfer. characteristics of the t.
WO 99/64095 ' ~ ~ PC1'/US99113420 1 piezoelectric element 90 and signals the sample and hold feedback contr oiler '_' 8~ when the power transfer characteristics are at local maxima. The controller 3 8=1 correlates these local maxima with tIze frequencies and amplitudes -1 commanded b~- the generator 7:1 to be supplied to the piezoelectric element 90.
6 After the frequency generator 7~ has finished its s~nreep through the 7 frequencies and amplitudes of power supplied to the piezoelectric element 90, 8 the controller 8-1 causes the generator 7=1 to cycle through the frequencies and 9 amplitudes of power that resulted in local maxima, and then determines which of these frequencies and amplitudes results in optimal power transfer 11 characteristics through the piezoelectric element 90.
12 Completing the controller 72 is a clock .a00 which is tripped when 13 actuating electricity is first supplied to the piezoelectric element 90.
Clock 500 1~ includes a counter which prevents a second activation of the piezoelectric element for a preset period of time. Thus, overuse and overdosing by the 1G, patient are pre~rented.
I7 )'s1 operation of embodiment 10, the_drug-containing package 34 is 18 punctured and inserted .onto the surface 52 of vibe ator 36 in chamber 52 in the I9 manner described pi-e~riouslv.The power switch 12 is placed in tho "ON"
position and the user uZhales air through the conduit 26, air flow F is 2I generated through conduit 26. This causes one-w~ay ~~al~°e 50 to deflect to 22 , admit air flo~1- 5 through opening 30 into conduit 26, and also causes air flow 23 S2 through opening 3=~ and chamber 51 into conduit 26. The inhalation of air 2~ stream F is sensed by sensor 40 and is signaled to actuation controller 70, which causes po~ler to be supplied to the controller 72. The controller 72 then 26 adjusts the amplitude and frequency of actuating power supplied to the Z7 piezoelectric element until they are optimized for the best possible de- .
28 aggregation and suspension of the powder P from t?1e capsule into the air 29 stream F via air t7ows S and S2.
.
I ~ Figure ~ illustrates another embodiment of the invention: Figure 5 is 2 similar to Figure ~, except the clock 500 is replaced with a counter 502 which 3 counts the number of daces delivered by the device. Counter 502 is connected :I to a display 50-1 which displays the number of doses delivered, or, optionally, the number of doses remaining.
6 Figure 6 illustrates yet another embodiment of the invention. The 7 Figure 6 embodiment is similar to the Figure ~ embodiment, except the clock 8 500 is replaced by an internal monitor which contains a record of inhaler use.
9 - Completing the Figima 6 embodiment is a hatch 5I0 through which a 20 physician ma~-,access, road and/or download the data from monitor 508, 1I whereby to determine patient compliance.
12 Figure. ;' illustrates yet another embodiment of the invention. 'The L3 Figure 7 embodiment is similar to the Figure ~~ embodiment except in the 1~ Figure 7 embodiment-, clock 500 counts time for the purpose of reminding a patient to use the inhaler. Thus, clock 500 is connected to a tone generator 514:
16 Figure 8 illustrates yet another embodiment of the invention. The 17 Figure 8 embodiment is similar to the Figui a ~ embodiment, except that it 18 includes a clock or counter 516 which sends a signal to controller 84 to alter .
19 the acti~~ation time, i.e. to a shorter ox longer period, ~,vhoreby to alter the, quantitt.~ of drub delivered; e.g..to increase or decrease dosage over time.
_._ 22 Alternativelt-, clock 516 nzajr be prograrrtmed to disable the inhaler once a 22 certain date is gassed, i.e. so as to avoid possible use of out-of-date drugs.
23 Figure 9 illustrates yet another embodiment of the invention. Figure 9 2~ is similar to Figure ~, except the counter or clack 500 is replaced with a temperature sensor 518. Certain medications are heat sensitive, aild may be 26 deactivated, or.rendered potentially dangerous if exposed to high 27 temperatures, for example, as might occur if the inhaler is left in an 28 automobile on a sunny day. Temperature monitor 528 will deactivate 29 controller 72 zn the event a preset temperature is reached. If desired, monitor ( l . _.
WO 99164095 n > ~ PCT/US99113420 1 518 also could include a display warning the patient that a preset temperature ? has been. reached.
3 The Figure 10 embodiment is similar to the Figure 9 embodiment except in the Figure 10 embodiment, the temperature sensor is replaced with a "key" such as, for example, a three button keyboard by which the user's pin 6 code must be entered in order to activ ate the device. This will prevent, for 7 example, use of the irihale:r by someone other than the intended patient, and - F> would prevent, for example, controlled or dangerous drugs from being used 9 by children. Far ease of use, key 524 rnay permit the patient (or druggist) to program a specific pin code far the intended user.
11 Referring to Figure 11, which illustrates vet another embodiment of the 12 invention, in ~,-hich two piezoelectric vibrators 90A, 90B, are located side-by-13 side within the inhaler shell. In this embodiment, piezoelectric elements 1~ are designed to vibrate at different amplitudes and frequencies, i.e. so that, for example, two different drugs advantageously may be dispersed 16 simultaneously from the same inhaler, without compromising performance or 17 either drug. This permits delivery of two drugs which, nvhile active together, 18 may not readily be stored together. For example, an asthma inhaler may be 19 provided containing both a bronchodilator, such as albuterol, and a steroid .
which may require different peiza settings. The Figure 1I embodiment 21 includes a pre-calibrated controller 112 ~~hich includes a first and a second -22 pre-calibrated irequencv/amplitude control signal generator 110A,110B, 23 which supplies control signals to pump circuit A and pump circuit B, 24 respectiveh~. Of course, the pre-calibrated controller 112 may be replaced with a pair of feedback controllers similar to that shovs-n in Figure 4.
26 Referring to Figilres 12 and 13, a cross-sectional ~~ie~w of an airflow 27 passage 212 of an inhalation device 202 is depicted. It should be noted at the 28 outset that the airflow passage 212 depicted in Figure 12 is a generalized 29 airflo~~ passage of a typical inhalation device, such as those discussed above.
_. _. , WO 99/64095 , , PCT/US99/13420 f 1 However, the present invention is intended to be adapted to any inhalation device, regardless of the particular geometry of the airflow passage. At its 3 most basic Ie~~el, the present invention operates by providing an air flow :1 sensor 208 to detect air flow turbulence around the sensor 208 (i.e., inspiratory air flow rate of a user of the inhaler) and to control various components of the 6 inhalation device 202, as a function of the amplitude and/or frequency of the 7 detected airfl-o~i- h~rbulence, as described below.
8 As sho~,-n in Figure 1?; air 110 (or other fluid) enters the airflow 9 passageway 21'_. typically by the respiratory activity of a patient inhaling on the device 20~. As air 210 flow.~s through the passage 212, a portion thereof 11 flows through the opening 206 in the passage 202 into a cavity 204. Placed 12 within the cavity 204 is an air flow sensing device 208. Preferably, the air flow 13 sensing device 208 is an acoustic sensing device, e.g. a microphone. Also ~~
1~ preferably, microphone 208 is adapted to produce appropriate signals 248 in response to the airt~low detected within the cavity 204. The amplitude and 16 frequency of the airflow within the cavity 204 is a function of the airflow rate 17 210 within the air passage 212 of the device 202. Thus, output signals 248 18 from the microphone 208 v~~iil vary in both frequency and amplitude as a 19 function of air flow rate within the cavity (which is a function of flow rate within the passage 212), and thus, can be used to control various components 21 of the inhaler 202 as a function of frequency and/or amplitude, as described 22 below. Those skilled in the art will appreciate that the shape of the cavity 204 23 and the size of the opening 206 are chosen in accordance the particular 24 geometry of the air passage 212, the air flow rate 210 through the passage 212, and/or the frequency response and/or sensitivity of the microphone 208; and 26 all such variations are within the scope of the present invention.
Preferably, 27 as noted abo~,~e, the shape of the cavity 204 and tile size of the opening 206 are 28 chosento permit at least a portion of the air within the passage 202 to enter WO 99/64095 . -~ PCTIUS99/13420 1 the cavity 20~ with sufficient amplitude to induce a response from the ? mice ophone 20S.
3 Referring now to Figure 13, an expanded cross-sectional view of an -1 embodirrtent of the air flow sensor (described with. reference to Figure 12, above) in a dry- powder inhaler, such as disclosed in 'E.r'.S. Patent 5,69,920.
6 Depicted in Fi'rure 13 are the components of a typically dry powder inhaler 7 202. A mouthpiece 2=16 is provided for a user (i.e., patient) to inhale on the - $ device 202. A high-frequency vibratory mechanism 228 (e.g., piezoelectric 9 element, ultrasonic acoustic transducer, or other electromechanical vibratory mechanism, etc.) is provided to vibrate a container 220 (e.g., blister capsule) of 11 dry powdered medieament 250 to suspend particles of the medicament into 12 the air passage ?12. To further aid the suspension of particles, an elertrostadc 13 potential plate ?26 can be provided to draw particles of a certain charge (i.e., a 1~ charge opposite to that of the elects ostatic plate 226) into the air stream 210.
In this embodiment, a portion 210' of the air 210 drawn into the air passage 16 212 is induced into the cavity 20~, to be detected by the microphone element 17 208. Upon detection of airflow, the microphone element produces output 18 signals 248 proportional in amplitude and frequency of the air flow rate 19 within the air passage 212. The output signals 2:18 are used to control either the high-frequency vibrator 228 azid/or the electrostatic plate 226, or other 21 components of the inhaler, as described below.
22 ~ Figure 1~ is a block diagrariz representation of the acoustic control 23 system of the present invention for a dry powder inhaler. As described above, 2~ the microphone element 208 produces signals 2~8 in response to detected airflow 210'. These signals are processed by an amplitude/frequencv 26 processor 230 to condition the signals 248 arid to determW a the amplitude 2i and/or frequency of the output signals 2~8. The amplitude/frequency 28 processor produces output signals 248' to control the high-frequency vibrator 29 and/or electrostatic plate. To that end, output signals 2:18' are input into a _ ____ WO 99/64095 ~ , PCT/US99/13420 1 comparator circuit 240 and/or 232 and compared with a reference threshold 2 signal 242 and ~ or 234; respectively.
3 It should be understood that signals 24$ and 2.IS' are indicative of the airflow rate 210, described above. The present invention is intended to be controllable as a function of frequency and/or amplitude of signals 248, thus, 6 amplitude/frectuency processor can be adapted to condition the signals 248 in 7 terms of amplitude or. frequency are both. F-iigh frequency vibrator threshold 8 242 produces a signal 252 which represents the minimum voltage and/or 9 frequency required to activate the high frequency vibrator controller 244 (which, in turn, activates the high frequency vibrator ''?6): Comparator 240 11 compares signal 252 mith signal 248' and if the si~~mals have equal amplitude 12 and/or frequency (within some predetermined error margin), comparator I3 activates the high frequency vibrator controller 24=1, «which activates and 14 directly controls the high frequency vibrator 22b. Similarly, electrostatic plate deflector controller 236 is acfiivated by an equal match of signals 248' and 16 by the comparator 232. Electrostatic plate detector threshold 234 produces 17 signal 254 which represents the minimum voltage. and I or frequency reqtured 18 to activate the electrostatic plate 226.
19 Inspiratonr capacity processor 238 is provided to compute the peak inspiratory flow- 210 (represented by signals 248 and 2-18') of the patient.
21 Although not sho~r%n in the drawings, this information can be used to adjust 22 the threshold signals of the high frequency vibrator threshold 242 and/or 23 electrostatic plate detector threshold 23~. Of course, to accomplish this, the 24 high frequency- ~ribrator threshold 242 and/or electrostatic plate detector threshold 234 must be programmable, as is known in the art. in this way, the 26 microphone 20S can be programmed to trigger the various components of the 27 inhaler to adjust for varying inspiration flow rates from patient-to-patient or 28 individually . Thus, for example; the inspirator control scheme of the present 29 invention can be self-adjusting to account for a patient's decrease in r . ..
WO 99/64095 s . ' PCT/US99I13420 1 inspirafory flow rate caused by, for example, decreased lung capacity.
2 Alternatively, the processor 238 can be modified to seauentially turn on the J a 3 various components herein described {e.g., vibrator, electrostatic plate, etc.) at =1 optimal inhalation times {e.g., peak inhalation effort). Thus, for example, the processor 238 can be modified to activate the vibrator at a time just prior to 6 the user's peak inhalation effort, then to activate the electrostatic plate .' subsequently, thereby inducing the medicament into the airstream at a time 8 that produces optimal respiratory absorption of the medicament. Ivforeover, 9 processor 238 can be adapted ~w~ith appropriate memory to track a patient's inspiratorv flo~l~ rate which can be used to adjust the i~o«~dered medicament I1 250 to achieve maximum medication benefit.
12 Many modifications, alternatives and equivalents are possible. For 13 example, Processor 230, threshold signal generators t3-1 and 2~2, comparators 14 212 and 232 and can be any known digital (e.g., microprocessor) or analog circuitry and/or associated software to accomplish the functionality described 16 herein. Although the v arious components described in Figure 14 have been 17 described in a modular fashion, those skilled in the art will recognize that 18 each of these components can be discrete off-the-shelf or custom components, 19 or can be included in a single, unified system.
The present can be modified by permitting the microphone signals 248 21 and 248' to directly control activation of the high frequency vibrator 228 22 and/or electrostatic plate 226, thereby bypassing the comparators 240 and/or 23 232. In this ~-at-, microphone 208 can be adapted to activate these 24 components in a binary fashion that is not dependent upon flow rate. Also, it will be understood to those skilled in the art that the thresholding circuits 2& and 234, the amplitude/frequency processor 23Q aid the inspiratory capacitor 27 processor 238 can be adapted to permit user (patient) control and user-28 definable presets (i.e., minimum flow rate for activation, etc).
__. ' , .r ° , 1 ~ In addition, comparators 240 and 232 can be adapted to permit 2 generation of activation signals based differing signal strengths and/or 3 frequency. Thus, for example, the high frequency vibrator can be adapted to -1 activate only when a signal frequency of lKhz is achieved, while the electrostatic plate will only activate when a signal strength of 35mV. is 6 obtained.
7 Other modifications are also possible. For example, the microphone 8 208 can be positioned directly on the inner wall of the airflow passage 212 of 9 the device 202, instead of within the cavity 204. Also, as shown in Figure 12, a 20 . turbulence generator 214 can be provided to generator air turbulence within 11 the air passage ?12. This modification, for example, can be used in an.
12 inhalation device that woteld other~,vise not permit a portion 210' of the air 210 13 to enter the cavity 204. In addition, instead of a microphone 208, the acoustic 14 element can be any known fluid pressur a transducer (e.g., air pressure transducer) that will output appropriate signals as a function of fluid pressure 16 (ampl.itude) and/or frequency. Accordingly, the present invention can be 17 appropriately modified to operate in any fluid medium (other than air), to 18 provide automatic acoustic control.
19 Still other rnodifications are possible. Foy- example, although not , shown in the drawings, the present invention can be provided with a timer 21 that is controlled by siyals 248'. The timer can be appropriately modified to 22 control a schedule of ~n~hen the device may be activated, to avoid, for example, 23 an overdose. Thus, for example, the timer may be modified to only permit 24 activation of the components of the device at certain times of the day.
Moreover, the timer may be appropriately modified to permit downloading 26 of data related to usage (e.g., time of day used, dosage of medicament, 27 inhalation effort, etc.). Th'ts data can be particularly relevant for clinical trials 28 where it is important to track the recommended dosage and times of 29 medication. Of course, the previous description could be accomplished with, -- _ _ . ' WO 99/64095 ~ ' ' - PCT/US99/1342U
1 a counter, or the like, that simply counts the amount of times that the device 2 has been used.
3 Although the present invention has been dir ected to an acoustic. control :1 scheme for a dn- powder inhaler 202, the present invention is not so limited.
On the contrary, the present invention is intended to be adapted for any 6 inhalation device that would require a control mechanism (such as described 7 herein) based breath (inhalation} detection. For example, an anesthetic device 8 could be modified with the breath sensor and controller as provided herein to 9 monitor and control the amount of anesthetic a patient receives.
Additionally; the acoustic sensing element can be used to measure peak 11 inspiratory and l or expiratou~.~ flow of a particular patient, and record this 12 information for downloading and analysis.
13 Referring to Figure 15 there is illustrated a chamber 314 contaitung 14 aerosolized drv po~.rder particles of a pharmaceutical or drug 310. These particles 310 are suspended in air and carry a charge, for example a negative 16 charge. Also in the chamber is a support surf ace 312 hav ing a char ge opposite 17 to that an the particles. The support surface 312 will attract a number of 18 charged particles 310 sufficient to neutralize the charge on the surface of the 19 support 312. This support surface is one that can hold a discrete electrical charge on its surface, such as insulating material, e.g. plastic or a 21 semiconductor material, such as selenium, used in the photocopy industry.
22 The actual amount of pharmaceutical or drug powder transferred to 23 the carrier sheet is a function of the mass-to-charge ratio of the powdered 24 particles. If one assumes surface charge saturation, the amount of charge carried by the particles is directly related to the surface area. For spheriodal 2b particles, the charge z~aries as the square of the radius and the mass varies as 27 the cube. Thus, the amount of charged particles picked up by a given portion 28 of the surface of the char ge carrier will be a function the total charge on the 29 carrier. Thus, «kith a given surface charge density on the carrier, the amount -_ ._ WO 99164095 - . PCTlUS99J13420 1 of pharmaceutical or drug powder picked up is directly proportional to the 2 charged area. Thus, for doubling the amount of pharmaceutical or drug 3 powder to be picked up, and thus the dose amount, the area on which charge 4 is placed can be doubled. This can be used as a basic method to control the , amount of powder to be picked by the carrier. Thus, for any particular 6 powder or particle size distribution.of powder, the exact area and amount of 7 charge needed can be experimentally determined.
8 Referring now to Figuie l6, there is a schematic flow diagram of the 9 various items of equipment needed to perform in the total process from powder supply to packaged pharmaceutical or drug, i.e. in capsule form, 11 containing a specified amount of pharmaceutical or drug powder in the 12 package. At 316 is indicated the pharmaceutical or drug powder supply I3 which is fed into a device 3I8 for creating an aerosol of the powder. Next the 14 powder particles are ionized at 320. As will be indicated later, a number of I5 these steps and pieces of equipment can be combined. At 324 is indicated a 16 carrier surface capable of maintaining a space charge on its surface. This can 17 be a plastic belt, for example, or a selenium drum of the type used in Xerox TM
18 photocopiers. This carrier surface 324 is passed through a charging station 19 325 where a predetermined electrostatic charge 325A (an electrostatic "irilage"~ is created on a predetermined area of the transfer surface. This 21 charged surface 325A then passes through a step 326 ~s~~ herein powder is 22 deposited on the carrier surface in a sufficient amount 326A to neutralize the 23 charge carried by the carrier surface. Thereafterr the carrier surface, carrying 24 the predetermined amount 326A of powder on its surface, is passed to a powder discharging device 330 which discharges the powder 326A from the 26 surface 324 into the open end of a capsule 329, w-hicl~ capsule is carried on a 27 conveyor belt 3?8. A carrier 324 and conveyor belt 32$ are indexed and 28 synchronized in a predetermined manner so that the electrostatic "image"
29 aligns directly over the open end of capsule 329 and powder discharging v WO 99/64095 ~ ' PCTIL3S99l13420 1 device 330 during the discharge sequence. At that time powder discharging 2 device 330 is activated whereupon the predetermined amount 326A of 3 powder is released from surface 325A, and falls into capsule 329. The capsule =1 329 containing its charge of powder 326A, then passes through a capsule sealing step 332 wherein the capsule is capped.
6 As mentioned previously in discussing pigure 15, the carrier surface 7 with the electrostatic charge carries a known amount of charge on its surface 8 and the polarity of this charge is opposite to that of the powder particles 9 suspended in the chamber. The charged particles migrate to the charged surface because of the attraction by the opposite nature of the charges. This 11 migration of the particles continues until the charge on the carrier surface is 12 neutralized.
I3 The actual amount of powder mass transferred to the carrier sur fae'e is 14 a function of the mass-to-charge ratio of the charged particles. Although it is difficult to achieve a linear relationship between the mass and the actual 16 charge; it is possible to establish a fixed relationship between the surface area 17 of the powder particles and the charge the powder particle is carrying at 18 charge saturation. However, the surface area of a mixed group of powder 19 particles of different sizes and shapes can be exti°emeh- difficult to calculate P
mathernaticalle, particularly when the shapes are it r eguiar, (e.g. non-21 spherical, microcxvstalline, etc.) As mentioned earlier, the simplest method 22 of determining the amount and area of charge to attract a a yen weight of 23 particles is to estimate the correct area and charge and then apply the 24 estimated charge to the estimated area on the carrier surface 324 and expose this selectiveh~ charged area to a mass of powder which has been ionized in 26 the ionizing step. The amount of powder deposited can then be readily 27 measured at the discharge step. Thereafter, eithei° the size of the charged area 28 or the amount of charge applied to the area at the charging station 325 can be 29 adjusted upwardly or downwardly to provide the correct amount of charge, 2?
_. , Hr0 99154095 - , , ~ PCTIUS99113420 1 both in area and charge intensity, for picking up a desired weight of 2 oppositely charged powder.
3 Referring now to Figures 17,18 and 19, one preferred apparatus for 4 accomplishing the invention is illustrated schematicaih,~ in Figure 17, with .
details of the components thereof being shown in Figures 18 and 19. The 6 charge carrying surface is illustrated as a photo sensitit>e drum 324A which 7 rotates between the charge "image" exposure 325 which creates a charge 8 "image" 325A on the surface of the drum 324A. (see Figure 18) This "image"
9 exposure can be a light source e.g., a laser beam (or other controllable photon source), which is capable of creating an electrostatic "image" 325A on the 11 surface of the drum of a desired size and charge densiri~. The charge "image"
12 325A is then rotated to the image development station containing an ionized 13 cloud of drug powder which is attracted to the charge "image" 325 to 14 neutralize charge in the "image", thus, forming a powder "image"- 326A
containing a predetermined amount of powder. (see Figures 18 and 19) This 16 powder "image" 326A is rotated to a drug transfer station 330 where it is 27 released into the open ended capsule 329 carried on belt 328. This transfer to 18 the capsules 329 is accomplished, in one preferred embodiment, b~T the use of 19 high voltage plate 356 (see Figure 19) which overcomes;the attraction of the charged "image" 325A on the surface of the drum, thus releasing the powder 21 "image" 326A into the capsule 329. The pocket containing the predetermined 22 quantity of drug is then passed through the capsule capping step 332.
23 Figure 20 shows another embodiment of the im-ention wherein the 24 micronized drug particles 310 are carried on the surface of discrete carriers 360 which can be: for example; small plastic beads, for example. When these 26 plastic beads are contacted with an image 325A, the micronized particles 27 are transferred to the charge "image" 325A on the surface of the drum 324A
28 from the.discrete carriers 360. To accomplish this, the positive charge ort the _ -..
WO 99/64095 ' ' PCT/US99113420 1 image 325A should be higher than the positive charge on the surface of the 2 individual carriers 360.
3 Figures 21 and 22 show additional details of means for both handling =1 drugs and providing aerosolization and ionization to provide a suspended stream of fine drug powders having a predeterrruned size and charge. In 6 Figures 21 and 22, elements 316A, 318A and 320A and 316B, 318B-and 320B
7 correspond to the equivalent elements in Figures 16,17 and 18.
- 8 Since repeatability is important for drug metering it is necessary to 9 effectively address the issue of charge-to-mass variation with particle size.
One method of over-coming this problem is to control the particle size 21 distribution in the drug powder. Figure 22 shows one implementation to I2 achieve this contz-oI of particle size. The voltage on the electrostatic deflector 13 is adjusted to control the pa~,ticle sizes to be suspended in the holding 14 chamber for delivery to the ionization chamber. Once the desired particle sizes are suspended they are drawn into the ionization chamber to ensure 16 surface charge saturation on the particles. This will give a known charge to 17 the mass ratio.
18 Figure 21 shows an alternative means for controlling the size 19 distribution. A high velocity air stream is used to deaggregate the powder.
S
The deaggregated powder is then contained in holding chamber 318A. The 21 purpose of the holding chamber is to allov,r the larger size particles to settle, 22 thereby producing a factorable particle size distribution. The particle size 23 distribution is a function of the holding time as shown in Fig. 23. The 2~ suspended particles are then ionized and exposed to the charge image as sho~Tn at 326 in Figure 17.
26 Fig. 23 sho~,Ts the percentage of particles sizes suspended in a holding 27 chamber as a function of time. Such a chamber may be provided with a slow 28 upward flowing air current to maintain the aerosol suspension. As can be 29 seen, the percentage of suspended particles is very largely determined by __ _ WO 99/64095 ~ . PCT/US99/13420 1 particle size. Through experiment one can select a time slot that will give the 2 desired particle size distribution for any particle drug dosage.
Additionally, 3 or in place of settling time, one or more filters can be used for obtaining a :l given particle size range.
Fig. 24 is similar to Figure 18 except that the Image Development 6 Station 326A izz this figure is replaced with a stationan.~ electrode 3268 and an 7 air passagewa~~ 350 for carrying the aerosolized powder. The rotating drum 8 has a dielectric or photoreceptor surface 324 on to which is deposited the 9 latent image. As an.example the aerosolization chamber would be similar to IO that shown in Figure 2_l. The metering chamber in Figure 21 is then the air-11 ' passageway 325 between the dielectric surface 32~ and the stationary I2 electrode 3268. The undeposited powder then exits at the right side of this I3 air-passagewat- to be collected for later use or recirculated back into the .
14 aerosolization chamber.
Figure ?~ above shows an ion projection print head where. an ion beam 16 is used to produce a charge "image" on a dielectric surface. The corona wire 17 352 has a high voltage applied to it which causes the air to breakdown and 18 produces the ions 352A necessary for the operation of the ion projection I9 printers. The remainder of the ion projection print head includes the usual control electrode 354, screen electrode 356 and insulator 358. The relative 21 potential that is applied to the control and screen electrodes then regulates the 22 amount of ioru 325C that will be metered and deposited on to the dielectric 23 surface 324 these ions being deposited on the surface to form the latent image 24 325A. Both the intensity and size of the ion beam can be adjusted as will be apparent to one of ordinary skill in the art. The advantage of tlus system is 26 that it does not require a photosensitive surface and can therefore be rugged 27 making it suitable for the manufacturing environment.
28 The in~~ention is susceptible to modification. For example, .the 29 invention advantageously may be employed to form tablets each containing a a . . -.
WO 99164095 ' ' PCT/US99/1342U
1 precise amount of pharmaceutical or drug. Figure 26 is similar to Figure 16.
2 However, in the Figure 26 embodiment, tablet binder material 360 is 3 deposited in wells 362 of belt 364 at a first depositing station 366. The belt 364 4 carrying the partially filled wells 362 is then passed into powder discharging device 330, where the belt is indexed, as before, in coordination with carrier 6 surface 324. The predetermined amount 326A of powder is then discharged 7 from surface 32-1 into well 362, whereupon the belt is then moved to a well 8 filling station 368 where the wells 362 are filled. Well filling station 368 may 9 include a doctor blade (not shown) or the Like, for topping the wells 362.
Thereafter the filled wells pass through a tablet hardening station 370 wherein 11 the tablets are formed into unitary masses in known manner.
12 Figure 27 illustrates another alternative embodiment of the invention, 13 in which the surface of the drum 324 bearing th.e charged "image" 32~A is 14 passed through a powder bath or fluidized bed 380 containing the powder I5 par ticles: As before, the powder particles will stick only to the charged area 16 on the surface of the dr um.
17 Referring to Figure 28, in yet another embodiment of the invention, a I8 transport belt 382 carries a plurality of spaced edible wafers 384 or the like 19 upon which the predetermined amount of powder 386 may then be °' S
discharged onto the individual wafers.
21 Referring to Figure 29, in yet another embodiment of the invention, 22 transport belt 382 carries tape or sheet 388 formed of an edible substrate such 23 as starch. The powder particles 390 are deposited uniformly on the sheet 388, 24 which is then stripped from the belt 382, and cut i~zta specific sizes to determine the dose.
26 As can be seen from the foregoing description, the present invention 27 permits metering and packaging of dry powder pharmaceuticals and drugs, 28 in a highly precise, reproducible manner. Moreover, the invention readily 29 may be scaled from laboratory, i.e desk tap size, to pilot plant to full scale _.- _...._.
WO 99/64095 - ~ PCT/US991I3420 1 production capacity by simply changing size and/or handling speed. Since all 2 units operate according to identical processes, the drug used for clinical trials 3 would have the same manufacturing process as in full scale production.
Thus, production certification may be simplified.
Another advantage of the present invention is that the system may be 6 employed to meter and deposit different drugs and/or different dosages by 7 simply changing the "image". Alternatively, dosages may be changed, e.g.
8 larger doses made, by advancing the belt in a step-wise manner so that two or 9 more printed "dots" or a printed line may be deposited at one site on the belt.
The belt may then be advanced, and the process continued. Still other 11 modifications are possible. For example, the invention advantageously may 12 be used for "printing" diagnostic reagents or the like on a carrier or substrate.
13 Still other modifications and variations of the invention described I4 herein may be made and are intended to come within the scope of the appended claims.
1 ~ Another prior art inhalation device is disclosed in Burns et al U.S.
2 Patent No. 5,28,233. In this device, a liquid medication is atomized by an 3 ultrasonic device such as a piezo element (Burns et al, Col.10, lines 36-51). A
stream of air, usually at a high velocity, or a propellant then carries the atomized particles to the patient. The energy required to atomize the liquid 6 medication in the nebulizer is prohibitivelyT hi~,Yh, making.this approach for 7 the delivery of drugs to the lungs only feasible as a desk top unit.
The..high - 8 voltage requirements to drive the piezo, to produce the necessary mechanical 9 displacements, also sEwerely effects the weight and size of the device. It is also not obvious that the nebulizer operating principles can be applied to the 11 dry powder inhalers for delivery or powder medication to the lungs.
12 The prior art devices therefore have a number of disadvantages which 13 makes them less than desirable foi the delivery of dry powder to the lungs.
14 Some of these disadvantages are:
~ The performance of the prior art inhalers depends on the flowrate 16 generated by the user. Lower flowrate does not result in the 17 powder being totally deaggregated and hence adversely affects the 18 dose delivered to the patient.
19 ~ Inconsistency in the bioavailabilitv of the drugs from dose-to-dose because of lack of consistency in the deaggregation process.
21 ~ Lar4 a energ~T requirements for' driving the electromechanical based 22 inhalers which increases the size of the devices making them 23 unsuitable for portable use.
24 In our prior U.S. Patent No. 5,694,920, issued December 9,1997, ~~e provide an inhaler that utilizes vibration to facilitate suspension of powder 26 into a gas that overcomes the aforesaid and other disadvantages and 27 drawbacks of the above prior art. More particularly, the inhaler of our 28 aforesaid patent includes a piezoelectric vibrator for vibrating the powder. A
29 controller is provided for controlling supply (i.e., amplitude and/or t . z , _. _ WO 99164095 ' PCTIUS99/13420 1 frequency) of actuating electricity to the vibrator so as to cause vibration of 2 ' the powder that is adapted to optimally suspend at least a portion of the 3 powder into the gas. As described in our aforesaid patent, the controller may 4 include a user-actuable control for permitting the user to select the vibration frequencies and/or amplitudes for optimally suspending in the gas the type 6 of powder currently being used in the inhaler. The user-actuable control is 7 pre-calibrated with the controller to cause the controller to adjust the 8 Frequency and/or amplitude of actuating electricity supplied to the vibrator 9 to be that necessary far vibrating the type of po~~der selected by the user-actuablc~ control in such a way as to optimally suspend at least a portion of the 11 powder into the gas. The user-actuable control may include selection 12 gradations in terms at the average size of the powder particles to be 13 suspended iri the gas, and/or in terms of desired vibration frequencies and I4 amplitudes. Vibration frequency would be adjusted to at least about I2 ICHz, in order to optimally suspend such commonly used powdered medications in 16 the gas. Of course; vibration frequency and amplitude may be adjusted to 17 optimize suspension of the powdered medication being used.
18 An electrostatic field that is established across the air stream, whereby 19 by controlling the strength of the electrostatic field primarily only particle sizes of interest are introduced into the air steam, while larger size particles 21 are left behind in the container. This reduces the inconsistency associated 22 with the bioa~-ailability of the drug because of the large particles being 23 deposited into the mouth or throat as is common with devices described in prior art.
24 Summary of the Invention F
The present invention provides an improvement over prior art 26 inhalation de~~ices such as described in our aforesaid L:.S. Patent No.
27 5,694,920. In one embodiment of the invention, the inhaler contains two or 28 . more vibrator means or piezoelectric elements so that different drugs, i.e. of 29 different particle size, may be delivered from the same inhaler.
.
WO 99164095 ' PCT/US99li3420 1 In yet another embodiment of the invention, the piezoelectric elements 2 are switched between two. or more set frequencies, or frequencies swept so as 3 to avoid potentially setting up standing waves in the powder.
In yet another embodiment of the invention, the inhaler includes electronic circuitry for recording and/or controlling one or more functions 6 such as dose counting, patient compliance monitoring, and patient 7 compliance reminder. s. Also, the inhaler rnay be pr ogrammed according to a 8 delivery protocol, i.e. to alter the quantity of drug delivered over time.
If 9 desired, the inhaler also may include an environmental sensor and knockout control, for example,. to deactivate the inhaler in the event it is inadvertently 11 exposed to too high a temperature, a clock to deactivate the inhaler in the 12 event its shelf Iife is exceeded, and/or a security/safety lock-out.
13 Still vet another embodiment of the present invention provides aw air 14 flow sensor for controlling various components of an inhalation device.
Included in the preferred embodiment is an acoustic controller; the acoustic 16 controller including an acoustic element to sense air flow around the element 17 and for producing signals representative of a frequency and amplitude of the 18 , air t7ocl~, the signals being used to control (e.g., activated, deactiv ate, apply 19 , incremental i~oltage, etc.) certain components of the inhalation device.
' r Preferabhr, acoustic element is a microphone element or pressure 21 transducer positioned within the air passage of an inhalation device, (e.g., a 22 dry powder inhaler) that produces signals in response to the inhalation air 23 flow, these signals are used to control certain components of the inhaler;
e.g., 24 a high frequency vibrator, an electrostatic plate, timer, counter, etc.
Also preferably, these signals are used to activate/control certain components of 26 the inhalation device to maximize the inhalation effectiveness to obtain 27 maximum patient benefif from medicament.
28 Thus; the present invention provides a fully automated inhalation 29 device, that is breath activated, that perms .> optimal utilization of the ,._ 1 particular medication. For example, acoustic signals can be used to trigger 2 the high frequency vibrator and electrostatic plate only when the patient has 3 achieved optimum (e.g., maximum) inhalation effort, thereby ensuring that -1 the full (proper) dosage of medicament properly enter the patient's respiratory system. Alternatively, these signals (breath-activated signals) can 6 be used to progressively applyr increasing power to, or, sequentially .
.' activate/deactivate the various components of the inhalation device to S achieve optimal inllalatl011 dosage.
9 The present inventioiz also relates to the packagring of dry powders and particularly to the metering and packaging of precise quantities of 11 pharmaceuticals and drugs for medical uses.
12 The cer tification of new phar maceuticals is a lengthy and costly process 13 involving animal studies followed by chemical trails to establish both efficacy 2~ and safety. Because a pharmaceutical's characteristics may be affected by changes in manufacturing and/or packaging, the approval process limits the, 16 approval to a particular manufacturing and packaging process.
17 In our earlier U.S. Patent 5,699;69, granted December 23,1997, we I8 describe a method algid apparat~.is for packaging microgram quantities of fine 19 powders such as phar maceuticals using electrostatic phototechnology 2fl techniques. 1\~Iore particularly, as described in our aforesaid U:S.
Patent 21 5,699,b49, the ability of powders to acquire an electrical charge _ 22 advantageously is utilized for precisely measuring exact microgram 23 quantities of the pcJwder, whereupon these exact microgram quantities or a 2~ then placed in individual containers, and the containers sealed.
Electrostatic charge has been employed to attract a given quantity of 26 powder to a surface. An example of this is the laser printer or the electrostatic 27 copy devices where a drum is charged and toner particles are attracted and-28 held in position by the charge. The charge on the drum is neutralized by the 29 attracted toner powder, thus limiting the amount of toner in accordance with r . 1 .. . i~
1 the charge image on the drum. The charge on these printer drums is then 2 transferred to a sheet of paper or other carrier to give a final image. In our.
3 U.S. Patent 5,699,69, the same electrostatic charge technology is employed 4 for transfers ing a predetermined amount of a finely powdered pharmaceutical or drug to a carrier or an intermediate such as a drum, 6 carrying a charge of predetermined intensity and area, rotating the charged 7 drum surface; carrying the predetermined amount of powdered 8 pharmaceutical or drug on its surface, to a tr ansfer station where the charge is 9 overcome and tine dry powder is transferred to a package which is then sealed. In lieu of a drum, a belt, or other movable surface is charged to a 21 given potential in a localized area.
12 When a given amount of a powdered pharmaceutical or drug is to .be 13 packaged, the charge and. area ~of charge can be determined experimentally 14 for each dose of pharmaceutical or drug and each particle size distribution.
This can be done by controlling either the charged area for a given charge 16 density or the total electrostatic charge on any individual charged area:
These 17 conditions can be adjusted to provide essentiallv~the exact desired amount of 18 the particular pharmaceutical or drug to be transferred at the transfer station.
19 - In thepresent invention, the electrostatic charge technology described, "
in our aforesaid U.S: Patent 5,f99,649 is adopted to be used for measuring and 21 packaging unit doses of a pharmaceutical or drug in a readily ingestible form, 22 i.e. as a tablet or capsule. The technology thus described permits reproducible 23 precise measurement and packaging of a pharmaceutical or drug, and-which 24 may be scaled from laboratory to pilot plant to full scale production without the need for recertificadon.
26 Still other features and advantages of the present invention may be 2i seen from the follov~ring detailed description, taken in connection with the 28 attached drava~i.ngs, wherein like numerals depict like parts, and wherein:
. _.
2g ' Brief Description of Drawings Figure 1 is a perspective view of an inhaler of the prior art;
WO 99164095 - ~ . ~ PCT/US99/13420 1 Figure 2 is a rear plane view of the inhaler sho«-n in Figure 1;
2 Figure 3 is a longihidinal cross-sectional schematic view of the inhaler 3 of Figure 1;
4 Figure 4 is a functional block diagram of the vibration control system of one embodiment of Figure 1;
6 Figure ~ is a functional block diagram of the vibration control system 7 of another embodiment of the invention;
8 Figures 6-10 are .hmction block diagrams of the ~-ibration control 9 system in accordance with still yet other embodiments of the invention; and Figure I1 is a view, similar to Figi.ire 3 of vet another embodiment of I1 the invention.
12 Figure I' is a cross-sectional vie~.v of a typical inhalation device and the 13 acoustic controller of the present invention;
14 Figure 13 is an expanded cross-sectional view of Figure 12;
Figure I4 is a functional block diagram of a preferred embodiment of 16 the acoustic controller of the present invention;
I7 Figure l~ sho~nfs a schematic representation of the attraction of I8 negatively charged powder particles to a support haring a positive charge on 19 the surface thereof; r Figure I6 shows a block diagram of the various steps involved in 21 practicing the invention;
22 Figure I i is a schematic representation of one form of drum type 23 electrostatic device for transferring given small quantities of powdered drugs 24 from an electrostatic attraction station, where a given quantity of powdered drug is attracted to and neutralizes a given charge. on the drum, and a 26 subsequent transfer station where the drug is transferred from the drum to a 27 package therefor;
28 Figures 18 and 19 are schematic functional representations of preferred 29 components employed in the Fig. I7 type of apparatus;
_ _.. _._ WO 99/64095 '. , PCTlUS99/13420 1 ~ Figure 20 shows a different system wherein separate carriers, having 2 micronized drug particles electrostatically attached to their surface, are used 3 to carry the drug to the charged transfer surface;
Figures 2I and 22 show methods of aerosolizing the powdered drug and ionizing the~drug to give it a specific charge;
6 Figure ?3 shows a graph illustrating the percentage of suspended 7 particles as a function of time and size, permitting creation of a suspended 8 particle stream of any given desired size distribution;
9 Figur a 2~ showTs another embodiment of applying the aerosolized drug 20 to a drum carr~~ing charge "image";
11 Figure ?~ illustrates an ion projection system for creating the charge 12 "image" on a dielectric surface;
13 Figure 26 is a view similar to Fig. I6, and illustrating an alternative' 14 embodiment of the invention; .
Figure 27 is a view similar to Fig. 16, and illustrating another 16 alternative embodiment of the invention;
17 Figure 2S is a view similar to Fig. 16, and illustrating yet another 18 alternative embodiment of the invention; and 19 Figure 29 is a ~,~iew similar to Fia. 16, and illustrating still yet another alternative embodiment of the invention.
21 Figures 1-3 illustrate an embodiment 10 of inhaler made in accordance 22 with our aforesaid U.S. Patent No. 5,694,920. Inhaler 10 includes a hard 23 plastic or metal housing 18 having a generally L-shaped longitudinal cross-24 section. Housing 18 includes tour air flow openings 20, 28, 30, and 32..
Inhaler 10 includes a main air flow passage 26 wluch extends the length of the 26 housing 18 from the front 22 (at opening 20) to the rear 2=1 thereof (at opening 27 28) and has a generally square-shaped transver se cross-section, so as to permit 28 air flow therethrough (denoted by arrow F in Figure 1).
t~ _ _ WO 99/64095 n , . , . PCT/US99/13420 1 ~ Secondary air conduit 31 is generally L-shaped and runs longitudinally 2 from opening 30 in the rear 2~ surface of the housing 18 to main passage 26.
3 One-way t~lo«- valve 50 is mounted to the inner surface 33 of the main passage :l 26 via a conventional spring-biased hinge mechanism (not shown), which is adapted to cause the valve 50 to completely block air flow S through the 6 conduit 31 to the main passage 26 when the pressure of the air flow F in the 7 main passage 26 is blow a predetermined threshold indicative of inhalation 8 through the passage 26 by a user.
9 Powder dispensing chamber 54 is, formed in housing 18 for holding a capsule 34 of powder medication to be inhaled. Housing 18 includes a 12 moveable panel portion 32 in the rear 2~ for permitting the capsule 34 to be 12 introduced into the chamber 5~ and placed on the seating 52 of vibration 13 means 36 betcseen guiding means 60A, 60B. Preferably, means 36 comprises a 14 hard plastic or metallic protective shell 37 enclosing a piezoelectric vibrator , 90. (Figure ~). Preferably, vibrator 90 is inechanicaliy coupled through the 16 shell 37 via a disk (not shown) to the drug cartridge 3~ so as to permit x7 maximum vibratory energy to be tz~ansmitted from the vibrator 90 through 18 the shell 37 to the cartridge 3~. .Guiding means 60A, 60B includes two 19 surfaces which slant do~n~nwardlv toward the seating 52 so as to permit easy introduction and retention of the capsule on the seating 52 in the chamber 51.
21 Removable panel 32 includes another air inlet 3=1 for permitting additional air 22 flow S2 from the chamber 51 through conduit 61 into conduit 31 during 23 inhalation bt- the user. Preferably, panel 32 and housing 18 include 24 conventional mating mounting means {not shown) for permitting the panel 32 to be removable resecurable to the housing by the user between introduction 26 of fresh (i.e., completely full) capsules and removal of spent (i.e., empty) 27 capsules.
28 Inhaler 10 also includes a conventional miniature air stream velocity or 29 pressure sensor ~0 moiulted on the inner surface of the conduit 26 so as to _.
WO 99!64095 ~ ~ PCT/US99/13420 1 sense the speed and/or pressure of the air stream F. Preferably, sensor 40 2 comprises a cony entional spring-loaded flapper-yield switch which generates 3 electronic signals indicative of the speed and/or pressure of the air stream F
:1 in the conduit ?b, and transmits those signals via electrical connection 42 to .
electronic control circuitry 48 contained in housing 18 for controlling 6 actuation of the vibrator means based upon those signals.
7 Preferably, th~control circuitry 48 is embodied as an application 8 specific integrated circuit chip and/or some other type of very highly 9 integrated circuit chip. Alternatively, control circuitw ~8 may take the form of a microprocessor, or discrete electrical and electronic components. As will 11 he described more fully below; the control circuitry 48 determines the 12 amplitude and frequency of actuating power to be supplied from 13 conventional power source 46 (e.g., one or more D.C. batteries) to the 14 piezoelectric vibrator to thereby control vibration of the vibrator. The actuating po~n-er is supplied to the piezoelectric element 90 via electrical 16 connection 4~ between the vibrator and the circuitry 48.
17 Piezoelectric element 90 is made of a material that has a high-18 . frequency, and preferably, Ultrasonic resonant ~-ibratorv frequency (e.g., 19 about 15 to 100 MHz), and .is caused to vibrate with a particular frequency r and amplitude depending upon the frequency and/or amplitude of excitation 21 electricity applied to the piezoelectric element 90. Examples of materials that 22 can be used to comprise the piezoelectric element 90 include quartz and 23 polycrystalline ceramic materials (e.g., barium titanate and lead zirconate 24 titanate). Advantageously, by vibrating the piezoelectric element 90 at ultrasonic frequencies, the noise associated with vibrating the piezoelectric 26 element 90 at lower (i.e., non-ultrasonic) frequencies can be avoided.
27 Turning specifically to Figure :l, the various functional components 28 and operation of the control circuitry 48 will now be described. As ~~ill be 29 understood b~- Chase skilled in the art, although the functional components .
l , r , _ __ WO 99!64095 r PCT/US99/13420 1 sho~nTn in Figure ~ are directed to an analog realization of the control circuitry 2 48, the components of Figure ~ could be appropriately modified to realize 3 control circuitry ~8 in a digital embodiment without departing from this 4 embodiment 10 of the present invention.
Control circuitry ~8 preferably includes actuation controller 70 and 6 vibratory feedback control system 72. Actuation conti oiler 70 comprises a 7 conventional sc~~itching mechanism for permitting actuating power to be 8 supplied from the power source 46 to the control system 72 depending upon 9 the signals supplied to it from sensor =10 and the state of fihe power switch 12.
In other words, controller 70 permits actuating pokier to be supplied from the 12 source ~6 to the system 72 when the sliding indicator bar 1~ of switch 12 is set 12 to the "ON" position in channel track 16 and the inhalation sensor 40 supplies 13 signals to the controller 70 that indicate that the inhalation is occurring 14 through the main passage 26. F-~owever, controller 70 does not permit actuating pointer to flow from the source to the system i2 when either the 16 s~~itch 12 is Set to "OFF" or the signals supplied to the controller 70 from the 17 sensor ~0 indicate that inhalation is not taking place through the conduit 26.
28 When controller 70 first permits actuating power to be supplied from 19 the source ~6 to the feedback control system 72, the s~~stem'2 enters an initialization state wherein controllable means for supplying a predetermined 21 frequency and amplitude of actuating electricity 7~ is caused to generate 22 control signals for causing conventional pump circuit 80 to generate an initial 23 desired frequency and amplitude of actuating electricity based upon stored 24 values thereof stared in the .initialization memory means 82. Preferably, means 7~ comprises conventional frequency sweep generator and frequency 26 generator means 76 and 78, respectively. The signals generated by.means 74 27 are then supplied to charge pump circuit 80 to cause circuit 80 to supply the 28 piezoelectric element 90 with actuating electricity specified by the signals.
t t WO 99164095 ~ ~ PCTIUS99/13420 1 ~ Preferably, the initial frequency and amplitude of actuating electricity supplied to the piezoelectric element 90 is pre-calibrated to cause the 3 piezoelectric element 90 to vibrate at its resonance frequency when no :I powder cartridge or powder is placed on the means 36. As will be .
appreciated be those skilled in the art, maximum transfer of vibratory power 6 from the piezoelectric element to the powder in the container 34 takes place 7 when the piezoelectric element ~~ibrates at its resonant frequenc~.l. It has been S found that this results in maxin-tum de-aggregation and.suspension of the 9 powder from the container 3~ into the air to be inhaled by~ the user:
However, when the container 34 or powder is placed on the v ibrator means 36, the I1 weight and volume of the powder container, and the weight, volume, and 22 particular size of the powder to be suspended byr the piezoelectric element can .
13 change the vibration characteristics of the piezoelectric element, and cause the 1~ piezoelectric element to vibrate at other than its resonant frequency, Ihis can result in reduced vibratory energy transfer to the powder from the 16 piezoelectric element, and thereby, lessen the efficiency of the piezoelectric 17 element in de-aggregating and suspending the powder in the air inhaled by 18 the user.
19 ThE :feedback control system i2 overcomes this problem. In control system 7?, after the initial frequency, and amplitude of actuating electricity are 21 stlppl~ed to the piezoelectric element 90, the frequency generating means 22 svstematicalh- 'enerates control signals indicative of many~ different 23 amplitudes and freqeiencies of electricity for being supplied to the 2~ piezoelectric element 90 by the circuit 80. As the generating means 7~
"cycles through" the different freduencies and amplituades, the instantaneous power 26 transfer characteristics of the piezoelectric element 90 for each of these 27 different frequencies and amplitudes are determined by the detector 88, 28 which transmits this information to the peak power detector 86. Peak 29 detector 86 anahTzes the instantaneous power transfer. characteristics of the t.
WO 99/64095 ' ~ ~ PC1'/US99113420 1 piezoelectric element 90 and signals the sample and hold feedback contr oiler '_' 8~ when the power transfer characteristics are at local maxima. The controller 3 8=1 correlates these local maxima with tIze frequencies and amplitudes -1 commanded b~- the generator 7:1 to be supplied to the piezoelectric element 90.
6 After the frequency generator 7~ has finished its s~nreep through the 7 frequencies and amplitudes of power supplied to the piezoelectric element 90, 8 the controller 8-1 causes the generator 7=1 to cycle through the frequencies and 9 amplitudes of power that resulted in local maxima, and then determines which of these frequencies and amplitudes results in optimal power transfer 11 characteristics through the piezoelectric element 90.
12 Completing the controller 72 is a clock .a00 which is tripped when 13 actuating electricity is first supplied to the piezoelectric element 90.
Clock 500 1~ includes a counter which prevents a second activation of the piezoelectric element for a preset period of time. Thus, overuse and overdosing by the 1G, patient are pre~rented.
I7 )'s1 operation of embodiment 10, the_drug-containing package 34 is 18 punctured and inserted .onto the surface 52 of vibe ator 36 in chamber 52 in the I9 manner described pi-e~riouslv.The power switch 12 is placed in tho "ON"
position and the user uZhales air through the conduit 26, air flow F is 2I generated through conduit 26. This causes one-w~ay ~~al~°e 50 to deflect to 22 , admit air flo~1- 5 through opening 30 into conduit 26, and also causes air flow 23 S2 through opening 3=~ and chamber 51 into conduit 26. The inhalation of air 2~ stream F is sensed by sensor 40 and is signaled to actuation controller 70, which causes po~ler to be supplied to the controller 72. The controller 72 then 26 adjusts the amplitude and frequency of actuating power supplied to the Z7 piezoelectric element until they are optimized for the best possible de- .
28 aggregation and suspension of the powder P from t?1e capsule into the air 29 stream F via air t7ows S and S2.
.
I ~ Figure ~ illustrates another embodiment of the invention: Figure 5 is 2 similar to Figure ~, except the clock 500 is replaced with a counter 502 which 3 counts the number of daces delivered by the device. Counter 502 is connected :I to a display 50-1 which displays the number of doses delivered, or, optionally, the number of doses remaining.
6 Figure 6 illustrates yet another embodiment of the invention. The 7 Figure 6 embodiment is similar to the Figure ~ embodiment, except the clock 8 500 is replaced by an internal monitor which contains a record of inhaler use.
9 - Completing the Figima 6 embodiment is a hatch 5I0 through which a 20 physician ma~-,access, road and/or download the data from monitor 508, 1I whereby to determine patient compliance.
12 Figure. ;' illustrates yet another embodiment of the invention. 'The L3 Figure 7 embodiment is similar to the Figure ~~ embodiment except in the 1~ Figure 7 embodiment-, clock 500 counts time for the purpose of reminding a patient to use the inhaler. Thus, clock 500 is connected to a tone generator 514:
16 Figure 8 illustrates yet another embodiment of the invention. The 17 Figure 8 embodiment is similar to the Figui a ~ embodiment, except that it 18 includes a clock or counter 516 which sends a signal to controller 84 to alter .
19 the acti~~ation time, i.e. to a shorter ox longer period, ~,vhoreby to alter the, quantitt.~ of drub delivered; e.g..to increase or decrease dosage over time.
_._ 22 Alternativelt-, clock 516 nzajr be prograrrtmed to disable the inhaler once a 22 certain date is gassed, i.e. so as to avoid possible use of out-of-date drugs.
23 Figure 9 illustrates yet another embodiment of the invention. Figure 9 2~ is similar to Figure ~, except the counter or clack 500 is replaced with a temperature sensor 518. Certain medications are heat sensitive, aild may be 26 deactivated, or.rendered potentially dangerous if exposed to high 27 temperatures, for example, as might occur if the inhaler is left in an 28 automobile on a sunny day. Temperature monitor 528 will deactivate 29 controller 72 zn the event a preset temperature is reached. If desired, monitor ( l . _.
WO 99164095 n > ~ PCT/US99113420 1 518 also could include a display warning the patient that a preset temperature ? has been. reached.
3 The Figure 10 embodiment is similar to the Figure 9 embodiment except in the Figure 10 embodiment, the temperature sensor is replaced with a "key" such as, for example, a three button keyboard by which the user's pin 6 code must be entered in order to activ ate the device. This will prevent, for 7 example, use of the irihale:r by someone other than the intended patient, and - F> would prevent, for example, controlled or dangerous drugs from being used 9 by children. Far ease of use, key 524 rnay permit the patient (or druggist) to program a specific pin code far the intended user.
11 Referring to Figure 11, which illustrates vet another embodiment of the 12 invention, in ~,-hich two piezoelectric vibrators 90A, 90B, are located side-by-13 side within the inhaler shell. In this embodiment, piezoelectric elements 1~ are designed to vibrate at different amplitudes and frequencies, i.e. so that, for example, two different drugs advantageously may be dispersed 16 simultaneously from the same inhaler, without compromising performance or 17 either drug. This permits delivery of two drugs which, nvhile active together, 18 may not readily be stored together. For example, an asthma inhaler may be 19 provided containing both a bronchodilator, such as albuterol, and a steroid .
which may require different peiza settings. The Figure 1I embodiment 21 includes a pre-calibrated controller 112 ~~hich includes a first and a second -22 pre-calibrated irequencv/amplitude control signal generator 110A,110B, 23 which supplies control signals to pump circuit A and pump circuit B, 24 respectiveh~. Of course, the pre-calibrated controller 112 may be replaced with a pair of feedback controllers similar to that shovs-n in Figure 4.
26 Referring to Figilres 12 and 13, a cross-sectional ~~ie~w of an airflow 27 passage 212 of an inhalation device 202 is depicted. It should be noted at the 28 outset that the airflow passage 212 depicted in Figure 12 is a generalized 29 airflo~~ passage of a typical inhalation device, such as those discussed above.
_. _. , WO 99/64095 , , PCT/US99/13420 f 1 However, the present invention is intended to be adapted to any inhalation device, regardless of the particular geometry of the airflow passage. At its 3 most basic Ie~~el, the present invention operates by providing an air flow :1 sensor 208 to detect air flow turbulence around the sensor 208 (i.e., inspiratory air flow rate of a user of the inhaler) and to control various components of the 6 inhalation device 202, as a function of the amplitude and/or frequency of the 7 detected airfl-o~i- h~rbulence, as described below.
8 As sho~,-n in Figure 1?; air 110 (or other fluid) enters the airflow 9 passageway 21'_. typically by the respiratory activity of a patient inhaling on the device 20~. As air 210 flow.~s through the passage 212, a portion thereof 11 flows through the opening 206 in the passage 202 into a cavity 204. Placed 12 within the cavity 204 is an air flow sensing device 208. Preferably, the air flow 13 sensing device 208 is an acoustic sensing device, e.g. a microphone. Also ~~
1~ preferably, microphone 208 is adapted to produce appropriate signals 248 in response to the airt~low detected within the cavity 204. The amplitude and 16 frequency of the airflow within the cavity 204 is a function of the airflow rate 17 210 within the air passage 212 of the device 202. Thus, output signals 248 18 from the microphone 208 v~~iil vary in both frequency and amplitude as a 19 function of air flow rate within the cavity (which is a function of flow rate within the passage 212), and thus, can be used to control various components 21 of the inhaler 202 as a function of frequency and/or amplitude, as described 22 below. Those skilled in the art will appreciate that the shape of the cavity 204 23 and the size of the opening 206 are chosen in accordance the particular 24 geometry of the air passage 212, the air flow rate 210 through the passage 212, and/or the frequency response and/or sensitivity of the microphone 208; and 26 all such variations are within the scope of the present invention.
Preferably, 27 as noted abo~,~e, the shape of the cavity 204 and tile size of the opening 206 are 28 chosento permit at least a portion of the air within the passage 202 to enter WO 99/64095 . -~ PCTIUS99/13420 1 the cavity 20~ with sufficient amplitude to induce a response from the ? mice ophone 20S.
3 Referring now to Figure 13, an expanded cross-sectional view of an -1 embodirrtent of the air flow sensor (described with. reference to Figure 12, above) in a dry- powder inhaler, such as disclosed in 'E.r'.S. Patent 5,69,920.
6 Depicted in Fi'rure 13 are the components of a typically dry powder inhaler 7 202. A mouthpiece 2=16 is provided for a user (i.e., patient) to inhale on the - $ device 202. A high-frequency vibratory mechanism 228 (e.g., piezoelectric 9 element, ultrasonic acoustic transducer, or other electromechanical vibratory mechanism, etc.) is provided to vibrate a container 220 (e.g., blister capsule) of 11 dry powdered medieament 250 to suspend particles of the medicament into 12 the air passage ?12. To further aid the suspension of particles, an elertrostadc 13 potential plate ?26 can be provided to draw particles of a certain charge (i.e., a 1~ charge opposite to that of the elects ostatic plate 226) into the air stream 210.
In this embodiment, a portion 210' of the air 210 drawn into the air passage 16 212 is induced into the cavity 20~, to be detected by the microphone element 17 208. Upon detection of airflow, the microphone element produces output 18 signals 248 proportional in amplitude and frequency of the air flow rate 19 within the air passage 212. The output signals 2:18 are used to control either the high-frequency vibrator 228 azid/or the electrostatic plate 226, or other 21 components of the inhaler, as described below.
22 ~ Figure 1~ is a block diagrariz representation of the acoustic control 23 system of the present invention for a dry powder inhaler. As described above, 2~ the microphone element 208 produces signals 2~8 in response to detected airflow 210'. These signals are processed by an amplitude/frequencv 26 processor 230 to condition the signals 248 arid to determW a the amplitude 2i and/or frequency of the output signals 2~8. The amplitude/frequency 28 processor produces output signals 248' to control the high-frequency vibrator 29 and/or electrostatic plate. To that end, output signals 2:18' are input into a _ ____ WO 99/64095 ~ , PCT/US99/13420 1 comparator circuit 240 and/or 232 and compared with a reference threshold 2 signal 242 and ~ or 234; respectively.
3 It should be understood that signals 24$ and 2.IS' are indicative of the airflow rate 210, described above. The present invention is intended to be controllable as a function of frequency and/or amplitude of signals 248, thus, 6 amplitude/frectuency processor can be adapted to condition the signals 248 in 7 terms of amplitude or. frequency are both. F-iigh frequency vibrator threshold 8 242 produces a signal 252 which represents the minimum voltage and/or 9 frequency required to activate the high frequency vibrator controller 244 (which, in turn, activates the high frequency vibrator ''?6): Comparator 240 11 compares signal 252 mith signal 248' and if the si~~mals have equal amplitude 12 and/or frequency (within some predetermined error margin), comparator I3 activates the high frequency vibrator controller 24=1, «which activates and 14 directly controls the high frequency vibrator 22b. Similarly, electrostatic plate deflector controller 236 is acfiivated by an equal match of signals 248' and 16 by the comparator 232. Electrostatic plate detector threshold 234 produces 17 signal 254 which represents the minimum voltage. and I or frequency reqtured 18 to activate the electrostatic plate 226.
19 Inspiratonr capacity processor 238 is provided to compute the peak inspiratory flow- 210 (represented by signals 248 and 2-18') of the patient.
21 Although not sho~r%n in the drawings, this information can be used to adjust 22 the threshold signals of the high frequency vibrator threshold 242 and/or 23 electrostatic plate detector threshold 23~. Of course, to accomplish this, the 24 high frequency- ~ribrator threshold 242 and/or electrostatic plate detector threshold 234 must be programmable, as is known in the art. in this way, the 26 microphone 20S can be programmed to trigger the various components of the 27 inhaler to adjust for varying inspiration flow rates from patient-to-patient or 28 individually . Thus, for example; the inspirator control scheme of the present 29 invention can be self-adjusting to account for a patient's decrease in r . ..
WO 99/64095 s . ' PCT/US99I13420 1 inspirafory flow rate caused by, for example, decreased lung capacity.
2 Alternatively, the processor 238 can be modified to seauentially turn on the J a 3 various components herein described {e.g., vibrator, electrostatic plate, etc.) at =1 optimal inhalation times {e.g., peak inhalation effort). Thus, for example, the processor 238 can be modified to activate the vibrator at a time just prior to 6 the user's peak inhalation effort, then to activate the electrostatic plate .' subsequently, thereby inducing the medicament into the airstream at a time 8 that produces optimal respiratory absorption of the medicament. Ivforeover, 9 processor 238 can be adapted ~w~ith appropriate memory to track a patient's inspiratorv flo~l~ rate which can be used to adjust the i~o«~dered medicament I1 250 to achieve maximum medication benefit.
12 Many modifications, alternatives and equivalents are possible. For 13 example, Processor 230, threshold signal generators t3-1 and 2~2, comparators 14 212 and 232 and can be any known digital (e.g., microprocessor) or analog circuitry and/or associated software to accomplish the functionality described 16 herein. Although the v arious components described in Figure 14 have been 17 described in a modular fashion, those skilled in the art will recognize that 18 each of these components can be discrete off-the-shelf or custom components, 19 or can be included in a single, unified system.
The present can be modified by permitting the microphone signals 248 21 and 248' to directly control activation of the high frequency vibrator 228 22 and/or electrostatic plate 226, thereby bypassing the comparators 240 and/or 23 232. In this ~-at-, microphone 208 can be adapted to activate these 24 components in a binary fashion that is not dependent upon flow rate. Also, it will be understood to those skilled in the art that the thresholding circuits 2& and 234, the amplitude/frequency processor 23Q aid the inspiratory capacitor 27 processor 238 can be adapted to permit user (patient) control and user-28 definable presets (i.e., minimum flow rate for activation, etc).
__. ' , .r ° , 1 ~ In addition, comparators 240 and 232 can be adapted to permit 2 generation of activation signals based differing signal strengths and/or 3 frequency. Thus, for example, the high frequency vibrator can be adapted to -1 activate only when a signal frequency of lKhz is achieved, while the electrostatic plate will only activate when a signal strength of 35mV. is 6 obtained.
7 Other modifications are also possible. For example, the microphone 8 208 can be positioned directly on the inner wall of the airflow passage 212 of 9 the device 202, instead of within the cavity 204. Also, as shown in Figure 12, a 20 . turbulence generator 214 can be provided to generator air turbulence within 11 the air passage ?12. This modification, for example, can be used in an.
12 inhalation device that woteld other~,vise not permit a portion 210' of the air 210 13 to enter the cavity 204. In addition, instead of a microphone 208, the acoustic 14 element can be any known fluid pressur a transducer (e.g., air pressure transducer) that will output appropriate signals as a function of fluid pressure 16 (ampl.itude) and/or frequency. Accordingly, the present invention can be 17 appropriately modified to operate in any fluid medium (other than air), to 18 provide automatic acoustic control.
19 Still other rnodifications are possible. Foy- example, although not , shown in the drawings, the present invention can be provided with a timer 21 that is controlled by siyals 248'. The timer can be appropriately modified to 22 control a schedule of ~n~hen the device may be activated, to avoid, for example, 23 an overdose. Thus, for example, the timer may be modified to only permit 24 activation of the components of the device at certain times of the day.
Moreover, the timer may be appropriately modified to permit downloading 26 of data related to usage (e.g., time of day used, dosage of medicament, 27 inhalation effort, etc.). Th'ts data can be particularly relevant for clinical trials 28 where it is important to track the recommended dosage and times of 29 medication. Of course, the previous description could be accomplished with, -- _ _ . ' WO 99/64095 ~ ' ' - PCT/US99/1342U
1 a counter, or the like, that simply counts the amount of times that the device 2 has been used.
3 Although the present invention has been dir ected to an acoustic. control :1 scheme for a dn- powder inhaler 202, the present invention is not so limited.
On the contrary, the present invention is intended to be adapted for any 6 inhalation device that would require a control mechanism (such as described 7 herein) based breath (inhalation} detection. For example, an anesthetic device 8 could be modified with the breath sensor and controller as provided herein to 9 monitor and control the amount of anesthetic a patient receives.
Additionally; the acoustic sensing element can be used to measure peak 11 inspiratory and l or expiratou~.~ flow of a particular patient, and record this 12 information for downloading and analysis.
13 Referring to Figure 15 there is illustrated a chamber 314 contaitung 14 aerosolized drv po~.rder particles of a pharmaceutical or drug 310. These particles 310 are suspended in air and carry a charge, for example a negative 16 charge. Also in the chamber is a support surf ace 312 hav ing a char ge opposite 17 to that an the particles. The support surface 312 will attract a number of 18 charged particles 310 sufficient to neutralize the charge on the surface of the 19 support 312. This support surface is one that can hold a discrete electrical charge on its surface, such as insulating material, e.g. plastic or a 21 semiconductor material, such as selenium, used in the photocopy industry.
22 The actual amount of pharmaceutical or drug powder transferred to 23 the carrier sheet is a function of the mass-to-charge ratio of the powdered 24 particles. If one assumes surface charge saturation, the amount of charge carried by the particles is directly related to the surface area. For spheriodal 2b particles, the charge z~aries as the square of the radius and the mass varies as 27 the cube. Thus, the amount of charged particles picked up by a given portion 28 of the surface of the char ge carrier will be a function the total charge on the 29 carrier. Thus, «kith a given surface charge density on the carrier, the amount -_ ._ WO 99164095 - . PCTlUS99J13420 1 of pharmaceutical or drug powder picked up is directly proportional to the 2 charged area. Thus, for doubling the amount of pharmaceutical or drug 3 powder to be picked up, and thus the dose amount, the area on which charge 4 is placed can be doubled. This can be used as a basic method to control the , amount of powder to be picked by the carrier. Thus, for any particular 6 powder or particle size distribution.of powder, the exact area and amount of 7 charge needed can be experimentally determined.
8 Referring now to Figuie l6, there is a schematic flow diagram of the 9 various items of equipment needed to perform in the total process from powder supply to packaged pharmaceutical or drug, i.e. in capsule form, 11 containing a specified amount of pharmaceutical or drug powder in the 12 package. At 316 is indicated the pharmaceutical or drug powder supply I3 which is fed into a device 3I8 for creating an aerosol of the powder. Next the 14 powder particles are ionized at 320. As will be indicated later, a number of I5 these steps and pieces of equipment can be combined. At 324 is indicated a 16 carrier surface capable of maintaining a space charge on its surface. This can 17 be a plastic belt, for example, or a selenium drum of the type used in Xerox TM
18 photocopiers. This carrier surface 324 is passed through a charging station 19 325 where a predetermined electrostatic charge 325A (an electrostatic "irilage"~ is created on a predetermined area of the transfer surface. This 21 charged surface 325A then passes through a step 326 ~s~~ herein powder is 22 deposited on the carrier surface in a sufficient amount 326A to neutralize the 23 charge carried by the carrier surface. Thereafterr the carrier surface, carrying 24 the predetermined amount 326A of powder on its surface, is passed to a powder discharging device 330 which discharges the powder 326A from the 26 surface 324 into the open end of a capsule 329, w-hicl~ capsule is carried on a 27 conveyor belt 3?8. A carrier 324 and conveyor belt 32$ are indexed and 28 synchronized in a predetermined manner so that the electrostatic "image"
29 aligns directly over the open end of capsule 329 and powder discharging v WO 99/64095 ~ ' PCTIL3S99l13420 1 device 330 during the discharge sequence. At that time powder discharging 2 device 330 is activated whereupon the predetermined amount 326A of 3 powder is released from surface 325A, and falls into capsule 329. The capsule =1 329 containing its charge of powder 326A, then passes through a capsule sealing step 332 wherein the capsule is capped.
6 As mentioned previously in discussing pigure 15, the carrier surface 7 with the electrostatic charge carries a known amount of charge on its surface 8 and the polarity of this charge is opposite to that of the powder particles 9 suspended in the chamber. The charged particles migrate to the charged surface because of the attraction by the opposite nature of the charges. This 11 migration of the particles continues until the charge on the carrier surface is 12 neutralized.
I3 The actual amount of powder mass transferred to the carrier sur fae'e is 14 a function of the mass-to-charge ratio of the charged particles. Although it is difficult to achieve a linear relationship between the mass and the actual 16 charge; it is possible to establish a fixed relationship between the surface area 17 of the powder particles and the charge the powder particle is carrying at 18 charge saturation. However, the surface area of a mixed group of powder 19 particles of different sizes and shapes can be exti°emeh- difficult to calculate P
mathernaticalle, particularly when the shapes are it r eguiar, (e.g. non-21 spherical, microcxvstalline, etc.) As mentioned earlier, the simplest method 22 of determining the amount and area of charge to attract a a yen weight of 23 particles is to estimate the correct area and charge and then apply the 24 estimated charge to the estimated area on the carrier surface 324 and expose this selectiveh~ charged area to a mass of powder which has been ionized in 26 the ionizing step. The amount of powder deposited can then be readily 27 measured at the discharge step. Thereafter, eithei° the size of the charged area 28 or the amount of charge applied to the area at the charging station 325 can be 29 adjusted upwardly or downwardly to provide the correct amount of charge, 2?
_. , Hr0 99154095 - , , ~ PCTIUS99113420 1 both in area and charge intensity, for picking up a desired weight of 2 oppositely charged powder.
3 Referring now to Figures 17,18 and 19, one preferred apparatus for 4 accomplishing the invention is illustrated schematicaih,~ in Figure 17, with .
details of the components thereof being shown in Figures 18 and 19. The 6 charge carrying surface is illustrated as a photo sensitit>e drum 324A which 7 rotates between the charge "image" exposure 325 which creates a charge 8 "image" 325A on the surface of the drum 324A. (see Figure 18) This "image"
9 exposure can be a light source e.g., a laser beam (or other controllable photon source), which is capable of creating an electrostatic "image" 325A on the 11 surface of the drum of a desired size and charge densiri~. The charge "image"
12 325A is then rotated to the image development station containing an ionized 13 cloud of drug powder which is attracted to the charge "image" 325 to 14 neutralize charge in the "image", thus, forming a powder "image"- 326A
containing a predetermined amount of powder. (see Figures 18 and 19) This 16 powder "image" 326A is rotated to a drug transfer station 330 where it is 27 released into the open ended capsule 329 carried on belt 328. This transfer to 18 the capsules 329 is accomplished, in one preferred embodiment, b~T the use of 19 high voltage plate 356 (see Figure 19) which overcomes;the attraction of the charged "image" 325A on the surface of the drum, thus releasing the powder 21 "image" 326A into the capsule 329. The pocket containing the predetermined 22 quantity of drug is then passed through the capsule capping step 332.
23 Figure 20 shows another embodiment of the im-ention wherein the 24 micronized drug particles 310 are carried on the surface of discrete carriers 360 which can be: for example; small plastic beads, for example. When these 26 plastic beads are contacted with an image 325A, the micronized particles 27 are transferred to the charge "image" 325A on the surface of the drum 324A
28 from the.discrete carriers 360. To accomplish this, the positive charge ort the _ -..
WO 99/64095 ' ' PCT/US99113420 1 image 325A should be higher than the positive charge on the surface of the 2 individual carriers 360.
3 Figures 21 and 22 show additional details of means for both handling =1 drugs and providing aerosolization and ionization to provide a suspended stream of fine drug powders having a predeterrruned size and charge. In 6 Figures 21 and 22, elements 316A, 318A and 320A and 316B, 318B-and 320B
7 correspond to the equivalent elements in Figures 16,17 and 18.
- 8 Since repeatability is important for drug metering it is necessary to 9 effectively address the issue of charge-to-mass variation with particle size.
One method of over-coming this problem is to control the particle size 21 distribution in the drug powder. Figure 22 shows one implementation to I2 achieve this contz-oI of particle size. The voltage on the electrostatic deflector 13 is adjusted to control the pa~,ticle sizes to be suspended in the holding 14 chamber for delivery to the ionization chamber. Once the desired particle sizes are suspended they are drawn into the ionization chamber to ensure 16 surface charge saturation on the particles. This will give a known charge to 17 the mass ratio.
18 Figure 21 shows an alternative means for controlling the size 19 distribution. A high velocity air stream is used to deaggregate the powder.
S
The deaggregated powder is then contained in holding chamber 318A. The 21 purpose of the holding chamber is to allov,r the larger size particles to settle, 22 thereby producing a factorable particle size distribution. The particle size 23 distribution is a function of the holding time as shown in Fig. 23. The 2~ suspended particles are then ionized and exposed to the charge image as sho~Tn at 326 in Figure 17.
26 Fig. 23 sho~,Ts the percentage of particles sizes suspended in a holding 27 chamber as a function of time. Such a chamber may be provided with a slow 28 upward flowing air current to maintain the aerosol suspension. As can be 29 seen, the percentage of suspended particles is very largely determined by __ _ WO 99/64095 ~ . PCT/US99/13420 1 particle size. Through experiment one can select a time slot that will give the 2 desired particle size distribution for any particle drug dosage.
Additionally, 3 or in place of settling time, one or more filters can be used for obtaining a :l given particle size range.
Fig. 24 is similar to Figure 18 except that the Image Development 6 Station 326A izz this figure is replaced with a stationan.~ electrode 3268 and an 7 air passagewa~~ 350 for carrying the aerosolized powder. The rotating drum 8 has a dielectric or photoreceptor surface 324 on to which is deposited the 9 latent image. As an.example the aerosolization chamber would be similar to IO that shown in Figure 2_l. The metering chamber in Figure 21 is then the air-11 ' passageway 325 between the dielectric surface 32~ and the stationary I2 electrode 3268. The undeposited powder then exits at the right side of this I3 air-passagewat- to be collected for later use or recirculated back into the .
14 aerosolization chamber.
Figure ?~ above shows an ion projection print head where. an ion beam 16 is used to produce a charge "image" on a dielectric surface. The corona wire 17 352 has a high voltage applied to it which causes the air to breakdown and 18 produces the ions 352A necessary for the operation of the ion projection I9 printers. The remainder of the ion projection print head includes the usual control electrode 354, screen electrode 356 and insulator 358. The relative 21 potential that is applied to the control and screen electrodes then regulates the 22 amount of ioru 325C that will be metered and deposited on to the dielectric 23 surface 324 these ions being deposited on the surface to form the latent image 24 325A. Both the intensity and size of the ion beam can be adjusted as will be apparent to one of ordinary skill in the art. The advantage of tlus system is 26 that it does not require a photosensitive surface and can therefore be rugged 27 making it suitable for the manufacturing environment.
28 The in~~ention is susceptible to modification. For example, .the 29 invention advantageously may be employed to form tablets each containing a a . . -.
WO 99164095 ' ' PCT/US99/1342U
1 precise amount of pharmaceutical or drug. Figure 26 is similar to Figure 16.
2 However, in the Figure 26 embodiment, tablet binder material 360 is 3 deposited in wells 362 of belt 364 at a first depositing station 366. The belt 364 4 carrying the partially filled wells 362 is then passed into powder discharging device 330, where the belt is indexed, as before, in coordination with carrier 6 surface 324. The predetermined amount 326A of powder is then discharged 7 from surface 32-1 into well 362, whereupon the belt is then moved to a well 8 filling station 368 where the wells 362 are filled. Well filling station 368 may 9 include a doctor blade (not shown) or the Like, for topping the wells 362.
Thereafter the filled wells pass through a tablet hardening station 370 wherein 11 the tablets are formed into unitary masses in known manner.
12 Figure 27 illustrates another alternative embodiment of the invention, 13 in which the surface of the drum 324 bearing th.e charged "image" 32~A is 14 passed through a powder bath or fluidized bed 380 containing the powder I5 par ticles: As before, the powder particles will stick only to the charged area 16 on the surface of the dr um.
17 Referring to Figure 28, in yet another embodiment of the invention, a I8 transport belt 382 carries a plurality of spaced edible wafers 384 or the like 19 upon which the predetermined amount of powder 386 may then be °' S
discharged onto the individual wafers.
21 Referring to Figure 29, in yet another embodiment of the invention, 22 transport belt 382 carries tape or sheet 388 formed of an edible substrate such 23 as starch. The powder particles 390 are deposited uniformly on the sheet 388, 24 which is then stripped from the belt 382, and cut i~zta specific sizes to determine the dose.
26 As can be seen from the foregoing description, the present invention 27 permits metering and packaging of dry powder pharmaceuticals and drugs, 28 in a highly precise, reproducible manner. Moreover, the invention readily 29 may be scaled from laboratory, i.e desk tap size, to pilot plant to full scale _.- _...._.
WO 99/64095 - ~ PCT/US991I3420 1 production capacity by simply changing size and/or handling speed. Since all 2 units operate according to identical processes, the drug used for clinical trials 3 would have the same manufacturing process as in full scale production.
Thus, production certification may be simplified.
Another advantage of the present invention is that the system may be 6 employed to meter and deposit different drugs and/or different dosages by 7 simply changing the "image". Alternatively, dosages may be changed, e.g.
8 larger doses made, by advancing the belt in a step-wise manner so that two or 9 more printed "dots" or a printed line may be deposited at one site on the belt.
The belt may then be advanced, and the process continued. Still other 11 modifications are possible. For example, the invention advantageously may 12 be used for "printing" diagnostic reagents or the like on a carrier or substrate.
13 Still other modifications and variations of the invention described I4 herein may be made and are intended to come within the scope of the appended claims.
Claims (19)
1. In a dry powder inhaler comprising a chamber for holding a dry powder, a vibrator operatively connected to said chamber for deaggregating said dry powder, and a passageway in which the deaggregated dry powder is picked up and carried by an air stream generated by inhalation of a user, the improvement wherein said chamber contains at least two vibrators designed to vibrate at different frequencies.
2. In a dry powder inhaler according to claim 1, further comprising electronic control circuitry which includes a controller for controlling dosing according to a pre-determined delivery protocol.
3. In a dry powder inhaler according to claim 2, wherein said electronic circuitry includes a controller for controlling the quantity of said powder delivered over time.
4. In a dry powder inhaler according to claim 3, wherein the controller varies quantity delivered with time.
5. In a dry powder inhaler according to claim 2, wherein said electronic circuitry counts doses delivered.
6. In a dry powder inhaler according to claim 2, wherein said electronic circuitry monitors patient compliance.
7. In a dry powder inhaler according to claim 6, further including means for recording patient usage, and for downloading the resulting record to a reader.
8. In a dry powder inhaler according to claim 2, wherein said electronic circuitry includes a clock.
9. In a dry powder inhaler according to claim 8, further including means associated with said clock for reminding a user.
10. In a dry powder inhaler according to claim 9, wherein said means for reminding comprises a tone generator.
11. In a dry powder inhaler according to claim 8, further comprising a lockout device associated with said clock for limiting frequency of use of said inhaler.
12. In a dry powder inhaler according to claim 2, wherein said electronic circuitry further comprises a lockout device for preventing unauthorized use of said inhaler.
13. In a dry powder inhaler according to claim 2, further comprising an environmental sensor associated with said electronic circuitry for deactivating the inhaler in the event the inhaler is exposed to ambient temperature conditions outside a predetermined range.
14. In a dry powder inhaler according to claim 13, further comprising a warning display activated by said environmental sensor when said inhaler is exposed to ambient temperature conditions outside said predetermined range.
15. In a dry powder inhaler according to claim 2, wherein said electronic circuitry further comprises a clock and lockout device for deactivating said inhaler at the expiration of a predetermined shelf life.
16. In a dry powder inhaler according to claim 2, wherein said electronic circuitry includes a controller for controlling operation of at least one of said vibrators over a plurality of frequencies.
17. In a dry powder inhaler according to claim 2, wherein said electronic circuitry comprises a microprocessor.
18. In a dry powder inhaler according to claim 2, wherein said electronic circuitry comprises a custom integrated circuit.
19. In a dry powder inhaler according to claim 2, wherein said electronic circuitry comprises discrete electrical and electronic components.
Applications Claiming Priority (7)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US09/097,105 | 1998-06-12 | ||
| US09/097,105 US6142146A (en) | 1998-06-12 | 1998-06-12 | Inhalation device |
| US09/097,104 US5960609A (en) | 1998-06-12 | 1998-06-12 | Metering and packaging method and device for pharmaceuticals and drugs |
| US09/097,104 | 1998-06-12 | ||
| US09/097,106 | 1998-06-12 | ||
| US09/097,106 US6152130A (en) | 1998-06-12 | 1998-06-12 | Inhalation device with acoustic control |
| CA002334590A CA2334590C (en) | 1998-06-12 | 1999-06-14 | Inhalation device |
Related Parent Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA002334590A Division CA2334590C (en) | 1998-06-12 | 1999-06-14 | Inhalation device |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| CA2463660A1 CA2463660A1 (en) | 1999-12-16 |
| CA2463660C true CA2463660C (en) | 2007-09-11 |
Family
ID=32512377
Family Applications (3)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA002463660A Expired - Lifetime CA2463660C (en) | 1998-06-12 | 1999-06-14 | Inhalation device |
| CA002463665A Expired - Lifetime CA2463665C (en) | 1998-06-12 | 1999-06-14 | Inhalation device |
| CA002463663A Expired - Lifetime CA2463663C (en) | 1998-06-12 | 1999-06-14 | Inhalation device with acoustic control |
Family Applications After (2)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA002463665A Expired - Lifetime CA2463665C (en) | 1998-06-12 | 1999-06-14 | Inhalation device |
| CA002463663A Expired - Lifetime CA2463663C (en) | 1998-06-12 | 1999-06-14 | Inhalation device with acoustic control |
Country Status (1)
| Country | Link |
|---|---|
| CA (3) | CA2463660C (en) |
-
1999
- 1999-06-14 CA CA002463660A patent/CA2463660C/en not_active Expired - Lifetime
- 1999-06-14 CA CA002463665A patent/CA2463665C/en not_active Expired - Lifetime
- 1999-06-14 CA CA002463663A patent/CA2463663C/en not_active Expired - Lifetime
Also Published As
| Publication number | Publication date |
|---|---|
| CA2463663A1 (en) | 1999-12-16 |
| CA2463660A1 (en) | 1999-12-16 |
| CA2463665A1 (en) | 1999-12-16 |
| CA2463665C (en) | 2008-12-30 |
| CA2463663C (en) | 2008-10-14 |
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Legal Events
| Date | Code | Title | Description |
|---|---|---|---|
| EEER | Examination request | ||
| MKEX | Expiry |
Effective date: 20190614 |