TREA

Inhaler component

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Information

  • Patent Grant
  • 10045562
  • Patent Number
    10,045,562
  • Date Filed
    Friday, January 9, 2015
    9 years ago
  • Date Issued
    Tuesday, August 14, 2018
    6 years ago
Information
Abstract
This disclosure relates to an inhaler component for the formation of a vapor-air mixture and/or a condensation aerosol by evaporation of a liquid material and optionally the condensation of the formed vapor. In one example, the inhaler component includes an electrical heater to evaporate liquid, a capillary wick that together with the electrical heater defines a compound structure that supplies liquid to the electrical heater, and a carrier supporting the compound structure. The carrier makes electrical contact with the electrical heater, and at least partially defines a portion of a capillary gap. The capillary gap is in fluid communication with the wick and automatically supplies liquid to the compound structure. Internal and external sides or faces of the carrier (relative to the compound structure) can define portions of the capillary gap.
Description

The invention concerns an inhaler component for the formation of a vapor and air mixture and/or a condensation aerosol by evaporation of a liquid material and optionally by condensation of the resulting vapor, comprising:

    • a housing;
    • an electrical heating element to evaporate a portion of the liquid material;
    • a wick with a capillary structure, which wick forms a compound structure with the heating element and automatically supplies the heating element with the liquid material;
    • a carrier plate, preferably a circuit board, which carries the compound structure and on which the heating element makes electrical contact;
    • a capillary gap at least partly formed by the carrier plate for the automatic supplying of the compound structure with the liquid material in that an end segment of the wick protrudes into the capillary gap.


DEFINITION OF TERMS

In the present patent application, the term “inhaler” refers to medical as well as nonmedical inhalers. Moreover, the term refers to inhalers for administering of pharmaceuticals and substances that have not been declared to be pharmaceuticals. The term furthermore refers to smoking articles and cigarette replacement articles, such as are contained in the European patent class A24F47/00B, insofar as these are designed to provide the user with a mixture of vapor and air, and/or a condensation aerosol. The term “inhaler” should also make no limitations as to how the resulting mixture of vapor and air and/or condensation aerosol is supplied to the user or his body. The mixture of vapor and air and/or condensation aerosol can be inhaled into the lungs, or also only be taken to the oral cavity—without inhalation into the lungs.


A “capillary gap” is considered to be any gap that brings about a liquid transport simply by virtue of the capillary action of its bounding walls. Wicks, jacketed wicks, or channels filled with wick material are not capillary gaps.


The use of the singular “compound structure” does not preclude the presence of several compound structures. The invention explicitly includes arrangements with several compound structures.


WO 2010/045671 (Helmut Buchberger) specifies an inhaler component for the intermittent, inhalation, or draw-synchronized formation of a mixture of vapor and air and/or condensation aerosol, consisting of (FIG. 9-12 and FIG. 17-18) a housing 3, a chamber 21 arranged in the housing 3, an air inlet opening 26 for the supply of air from the surroundings into the chamber 21, an electrical heating element for evaporating a portion of a liquid material 16, whereupon the resulting vapor mixes in the chamber 21 with the air supplied by the air inlet opening 26, and the mixture of vapor and air and/or condensation aerosol is formed. The inhaler component furthermore comprises a wick with a capillary structure, which wick forms a sheetlike compound structure 22 with the heating element and automatically supplies the heating element with the liquid material 16 once again after an evaporation. The sheetlike compound structure 22 is mounted by two end segments on two electrically conducting platelike contacts 23, on whose surface the heating element at the same time makes electrical contact. The plate like contacts 23 can also be formed alternatively by circuit boards or one shared circuit board. At least one heated segment of the sheetlike compound structure 22 is arranged free of contact in the chamber 21, and the capillary structure of the wick lies in said segment for the most part free, at least on one side 24 of the sheetlike compound structure. The sheetlike compound structure 22 or its wick protrudes by one end into a capillary gap 41, which for its part is capillary coupled or can be coupled to a liquid container 4 containing the liquid material 16. The liquid container 4 has a closure 18 that can be opened, which is still closed prior to use. The closure 18 can be manually opened by the user, whereupon the liquid material 16 floods a reservoir 45 and wets the capillary gap 41. The capillary gap 41 draws the liquid material 16 from the liquid container 4 or reservoir 45 and transports it to the compound structure 22. The capillary gap 41 is formed basically by one of the two platelike contacts 23 and a top piece 42 placed on the surface of the latter, in that the two adjoining structural elements or their surfaces form boundary walls of the capillary gap 42. Furthermore, a ventilation channel 52 is worked into the platelike contact 23, which connects the reservoir 45 or the liquid container 4 to the chamber 21. The ventilation channel 52 produces a pressure equalization in that each portion of liquid material 16 arriving in the capillary gap 41 is immediately replaced by an equal-volume portion of air.


Finally, a storage buffer 53 is integrated in the top piece 42, which communicates with the capillary gap 41 and itself consists of capillaries—see FIG. 11 and FIG. 17. The storage buffer 53 has the ability to take up liquid material 16 from the capillary gap 41, store it temporarily, and return it to the capillary gap 41 when needed. In this way, the inhaler component can also be operated in an inverted position—the mouth piece 5 pointing downward—at least for as long as liquid material 16 is on hand in the storage buffer 53. The storage buffer 53 consists of parallel arranged slits 54 that are worked into the top piece 42. The slits 54 communicate, on the one hand, via openings 55 with the capillary gap 41 and on the other hand via a ventilation gap 56 with the chamber 21. The capillarity of the slits 54 has the effect that the liquid material 16 flows from the reservoir 45 via the capillary gap 41 and via the openings 55 into the slits 54, where it is temporarily stored, and it can be pulled back again by the capillary gap 41 as needed.


The design of the storage buffer 53 proves to be extremely bulky. The fabrication of the fine slits 54 and openings 55 worked into the top piece 42 is also relatively costly. Finally, it is a disadvantage that the openings 55 disturb the capillarity of the capillary gap 41, because otherwise wettable wall segments of the capillary gap 41 are lost by the openings 55. In the worst case, the disturbance of the capillarity can impair the supply of the sheetlike compound structure 22 with the liquid material 16.


The problem on which the invention is based is to eliminate the aforementioned drawbacks of the arrangement known from the prior art. In particular, the invention is based on the problem of configuring an inhaler component of the kind described above by simple design features so that sufficient quantities of liquid material can be buffered without requiring a substantial additional construction space. Furthermore, the reliability of supplying the compound structure with the liquid material should be enhanced.


The problem is solved by the characterizing features of patent claim 1. Accordingly, it is specified that both the front side and the back side of the carrier plate form boundary walls of the capillary gap, at least for a portion. Thus, the supplying of the compound structure with the liquid material occurs not merely on one side of the carrier plate, but on both sides. On both sides of the carrier plate there are provided capillary gaps or capillary gap segments that are bounded by the carrier plate. In this way, an additional capillary gap volume can be created in a simple and space-saving manner, serving at the same time as a buffer. Another beneficial effect is to be seen in the redundancy of the liquid supply; if the supply fails is one capillary gap segment—for whatever reason—the compound structure can still be supplied with/the liquid material at least via the capillary gap segment lying on the other side of the carrier plate.


In a modification of the invention, it is specified that the edge of the carrier plate also forms at least a portion of a boundary wall of the capillary gap. In this way, the buffer volume can be further increased. It is especially beneficial for the capillary gap to at least partly encloses the carrier plate. The enclosure has the effect that the capillary gap segments at the front and back side of the carrier plate communicate with each other via the edge of the carrier plate. Even if the capillary liquid flow were to be interrupted at several places of the capillary gap, there would be at least one alternative pathway to go around the affected places.


According to the invention, over 50 percent of the carrier plate surface form boundary walls of the capillary gap. Segments of the carrier plate sticking out from the housing are not counted in the calculation. Thanks to the large-scale usage of the carrier plate surface as a boundary wall for the capillary gap, the aforementioned effects as to the formation of an additional buffer volume and the enhancing of the supply reliability are maximized. Moreover, the supply capacity, which is the maximum delivered quantity of liquid material through the capillary gap per unit of time, can be increased.


It is especially advantageous when the capillary gap is formed at least partially by the carrier plate and an adjoining wall of the housing. In this case, the capillary gap is formed, at least partly, solely by components already available. Already present wall segments of the housing are used as boundary walls of the capillary gap. No additional construction space is required.


One preferred embodiment of the invention concerns an inhaler component with a liquid container containing the liquid material from which the capillary gap draws the liquid material, and it is specified that the capillary gap is at least partially formed by the carrier plate and an adjacent wall of the liquid container. The liquid container can either form an independent structural part, or be part of the housing. In the latter case, the liquid container is formed by walls of the housing. Especially favorable conditions result when the capillary gap communicates via a supply opening in the wall of the liquid container with the liquid material in the liquid container, in that the wall of the liquid container forms a shoulder at the edge of the supply opening and the carrier plate abuts against the shoulder with its edge. Accordingly, no additional means are needed to connect the capillary gap to the liquid container. Thanks to the shoulder, a wall segment of the supply opening is extended outwardly. If one assumes that the surfaces involved are readily wettable by the liquid material, the result is that a small quantity of liquid material is drawn out from the supply opening by the forces of adhesion acting at the lengthened wall segment. The effect is sufficient for the liquid material to also reach and wet the carrier plate abutting by its edge against the shoulder. Thus, the capillary gap is coupled to the liquid material in the liquid container and can become filled with the liquid material, driven by the capillary forces acting in it.


The invention furthermore involves an inhaler, comprising an inhaler component according to the invention as described above. The inhaler component can thus also be only a part, especially an interchangeable part, of an inhaler.





The invention will now be explained more closely by means of a sample embodiment according to the drawings. There are shown:



FIG. 1, an inhaler according to the invention in various views;



FIG. 2, the inhaler of FIG. 1 with a reusable inhaler part and an interchangeable inhaler component in the decoupled state;



FIG. 3a and FIG. 3b, the interchangeable inhaler component in various views;



FIG. 4a, FIG. 4b, FIG. 4c, FIG. 4d, FIG. 4e, FIG. 4f, FIG. 4g, sectional views of the interchangeable inhaler component along line A-A in FIG. 3b in various assembly states;



FIG. 5, detail a of FIG. 4a in a magnified view;



FIG. 6, detail b of FIG. 4b in a magnified view;



FIG. 7, a carrier plate configured as a multilayer circuit board;



FIG. 8, a sectional view of the interchangeable inhaler component along line B-B in FIG. 3b;



FIG. 9, detail c of FIG. 8 in a magnified view;



FIG. 10, a cross section of the interchangeable inhaler component at the level of the supply opening;



FIG. 11, a cross section of the interchangeable inhaler component at the level of the compound structures.



FIG. 12, an alternative configuration of detail c (see FIG. 9).






FIG. 1 shows an inhaler according to the invention, whose form and size are configured so that the inhaler can be easily and conveniently handled by the user. In terms of volume, the inhaler is only around half the size of a cigarette pack. The sample inhaler depicted consists essentially of two parts, namely, an inhaler part 1 and an inhaler component 2.


The inhaler component 2 consists of a housing 3, which forms a tobacco pipe-like mouthpiece 4 at one end face. The inhaler component 2 contains a liquid material, which is electrically evaporated inside the housing 3 and converted into an inhalable mixture of vapor and air and/or condensation aerosol. The resulting mixture of vapor and air and/or condensation aerosol is presented to the user via the mouthpiece 4. The liquid material can be any substance or preparation that evaporates largely free of residue under atmospheric conditions. This condition is already fulfilled when the particular substance or preparation is present in the diluted state, e.g., dissolved in water and/or ethanol, and the solution evaporates largely free of residue. Thanks to a sufficiently good dilution in an easily volatile solvent such as water and/or ethanol, even otherwise hard to evaporate substances can meet the above-given condition, and a thermal decomposition of the liquid material is avoided or substantially reduced.


The aerosol particles produced by condensation generally have a mass median aerodynamic diameter (MMAD) less than 2 μm and therefore also reach the alveoli. The inhaler of the invention is especially suitable for the administering of substances with systemic action—especially those active substances that deploy their main action in the central nervous system. As an example, one can mention nicotine, whose boiling point is 246° C. The nicotine-containing aerosol particles are deposited primarily in the bronchi and alveoli, where the active substance passes into the blood stream lightning-fast. A few seconds later the nicotine reaches the brain in concentrated form and can deploy the known effects there.


The inhaler part 1 consists of a main housing 5, which again is preferably made of plastic. The main housing 5 contains at least one battery 6 and as electrical circuit 7 (shown by broken line in FIG. 1) with switch 7a. The battery 6 and the electrical circuit 7 provide the electrical energy needed for the evaporation of the liquid material. The battery 6 consists preferably of a rechargeable battery, such as the type CGRI8650K from Panasonic, www.industrial.panasonic.com. This is a cylindrical lithium ion cell of size 18650 with a storage capacity of 1650 mAh and a current load capacity up to 30 A. Comparable cells are also manufactured by other manufacturer, such as Sony, Samsung, LG Chem, in large numbers.


As is shown by FIG. 2, the inhaler part 1 and the inhaler component 2 in the specific sample embodiment are detachable from each other. This arrangement makes the inhaler part 1 reusable, which is basically sensible if one considers that, first, the inhaler part 1 does not come into contact with the liquid material i.e., it is not contaminated with the liquid material, and secondly it contains components that are more long-lived than the components of the inhaler component 2. The inhaler component 2, after the liquid material is used up, is properly disposed of as a whole by the user, and replaced by a new inhaler component 2. In this respect, the inhaler component 2 constitutes an interchangeable, disposable article. A proper disposal is especially appropriate when the liquid material contains pharmaceuticals or poisons such as nicotine. Basically, of course, it would also be conceivable to make the inhaler part 1 and the inhaler component 2 as a single piece, i.e., not detachable from each other. However, this configuration would be less economical, because in this case all parts and components of the inhaler, i.e., the inhaler as a whole, would form a disposable article for onetime use. Of course, the present invention also includes this embodiment, but in this case the entire inhaler is to be understood as being the inhaler component.


The mechanical coupling between the interchangeable inhaler component 2 and the reusable inhaler part 1 occurs by insert tongues 8a and guide lugs 9a formed by the housing 3, which fit into corresponding insert sockets 8b and guide grooves 9b formed by the main housing 5 of the reusable inhaler part 1. The insert tongues 8a and insert sockets 8b serve at the same time to channel the electrical energy into the interchangeable inhaler component 2 for evaporation of the liquid material, as will be shown in further detail below.



FIG. 3a and FIG. 3b show different views of the interchangeable inhaler component 2. FIGS. 4-11 provide further insight into the internal construction of the inhaler component 2. Accordingly, the housing 3 of the inhaler component 2 has essentially a rectangular shape. Inside the rectangular housing 3 are the components important to the forming of a mixture of vapor and air and/or condensation aerosol. These include in particular the compound structures 10, which bring about the evaporation of the liquid material. In the specific sample embodiment, six compound structures 10 are arranged alongside each other, and the compound structures have a sheetlike shape. The sheetlike compound structures 10 each consist of a wick and an electrical heating element, which are joined together in sheet fashion or integrated with each other in sheet fashion. The sheetlike compound structures 10 can be formed, for example, by a metal foil with metal cloth layers sintered on it. Instead of the metal cloth, open-pore metal foams can also be used. The open-pore capillary structure of the cloth layers sintered on the metal foil or the metal foam form the wick, and the electrical resistance of the metal forms the heating element. Suitable metallic resistance materials are, for example, refined steels such as AISI 304 or AISI 316, as well as heat conducting alloys, especially NiCr alloys. The manufacture of such sheetlike compound structures 10 is prior art and disclosed in detail, for example in the already cited WO 2010/045671 (Helmut Buchberger). It should be noted that the sheetlike compound structures 10 need not have a flat configuration, but can also have a three-dimensional curvature.


As is best shown by FIG. 4b and FIG. 7, the sheetlike compound structures 10 are mounted by two end segments 10a, 10b on a carrier plate 11. The carrier plate 11 has a large cavity 12, across which the compound structures 10 stretch without contact. The carrier plate 11 in the specific sample embodiment is configured as a circuit board, especially a multilayer circuit board. Basically all known circuit board materials are suited as the material for the circuit board 11, especially materials of type FR1 to FR5. The sheetlike compound structures 10 are in electrical contact in the region of the end segments 10a, 10b on conductor tracks 13 of the circuit board 11. In FIG. 7, the conductor tracks 13 are shown as black areas. In the case of the aforementioned metal foil compound structures, the electrical contacting occurs preferably by a soldering at the foil side, possibly after prior treatment with a suitable flux agent. Refined steels of material grades AISI 304 and AISI 316 can be easily soldered, for example, with a solder concentrate commercially known as “5050S-Nirosta” from Stannol GmbH, www.stannol.de. Alternatively, the electrical contacting can consist of a glue connection by means of an electrically conductive adhesive, such as a silver-containing glue on an epoxy basis. The fitting of the circuit board 11 with the sheetlike compound structures 10 and the production of their contacts is done fully automatic, in which methods of the circuit board industry can be used, which methods moreover are also suited to a mass production.


The circuit board 11 protrudes from the housing 3 in the form of the already mentioned insert tongues 8a. The two insert tongues 8a serve to channel the electrical energy into the inhaler component 2. The electrical energy is supplied to the compound structures 10 via the conductor tracks 13. According to FIG. 7, the conductor tracks 13 are arranged on both the front side 11a and the back side 11b of the circuit board 11, while the front side 11a is the component mounting side, that is, the side on which the compound structures 10 make contact. Additional conductor tracks can also be arranged optionally in intermediate layers. The individual conductor track layers are advisedly joined together by means of so-called throughplatings of the prior art. FIG. 7, moreover, shows the current flow. Accordingly, in the specific example, every three compound structures 10 are hooked up in series with each other. In this way, the resulting heating resistance and thus the heating power and rate of evaporation can be influenced in certain limits. If can also be provided that the individual electrical resistances of the six compound structures 10 are of different size, for example, by appropriately varying the thickness of the metal foil. With this measure, the evaporation process can be made to depend on the location, as with a cigarette.


On the front side 11a of the circuit board 11 is placed an essentially platelike top piece 14, preferably made of plastic (see FIG. 4c and FIG. 8-10). The top piece 14 has a recess 15, which correlates in size and arrangement with the cavity 12 in the circuit board 11. In the most simple case, the top piece 14 is mounted directly on the end segments 10a, 10b of the sheetlike compound structures 10. In this way, the top piece 14 together with the circuit board 11 forms a first capillary gap segment 16a, whose clear width or gap width basically corresponds to the thickness of the sheetlike compound structures 10 (see FIG. 9 and FIG. 11). The gap width is typically 0.2 mm. In FIG. 4f, the two-dimensional extent of the first capillary gap segment 16a is shown as a black area. The top piece 14 is fastened to the circuit board 11 by a glue connection. The glue sites are shown as black areas in FIG. 4d. The circuit board 11 and the top piece 14 are preferably joined outside of the housing 3, i.e., they constitute a preassembled unit.


The circuit board 11 is mounted by its back side 11b at least partially on a rectangular liquid container 18 containing the liquid material 17 (see FIG. 4a/4b, FIG. 8-9 and FIG. 11). The liquid container 18 or its walls 18a are formed by the housing 3. The circuit board 11, however, is not mounted directly on the liquid container wall 18a, but rather on spacers 19. The spacers 19 are formed partly by the liquid container wall 18a and partly by other housing segments; they are shown in FIG. 4a as black areas. In this way, a second capillary gap segment 16b is formed. The back side 11b of the circuit board 11 and the adjacent liquid container wall 18a form the boundary walls of this second capillary gap segment 16b. In FIG. 4c the two-dimensional extent of the second capillary gap segment 16b is shown as a black area. The gap width is determined by the height of the spacers 19 and typically amounts to 0.3 mm. The circuit board 11 is fastened preferably by means of a glue connection to the spacers 19. The filling of the liquid container 18 with the liquid material 17 is done at the factory at the end of the manufacturing process, preferably through a small hole in the container wall 18a (not shown) in a fully automatic process using a cannula and a dispensing unit. After the filling, the hole is closed, for example, it is melted shut, and the entire inhaler component is packed air-tight.


The liquid container 18 has at its lower end a slitlike supply opening 20 (see FIG. 5-6, FIG. 9-10). The second capillary gap segment 16b draws all liquid material 17 through this supply opening 20. The capillary coupling occurs by a shoulder 21 formed by the liquid container wall 18a. Thanks to the shoulder 21, one wall segment of the supply opening 20 is lengthened outwardly (see FIG. 9). The forces of adhesion acting on the lengthened wall segment have the effect of a small quantity of liquid material 17 escaping from the supply opening 20. The effect is enough for the liquid material 17 to also reach the circuit board 11, which abuts by its edge 11c against the shoulder 21 (see FIG. 6 and FIG. 9). In an alternative embodiment, the circuit board 11 rests by its back side 11b on the shoulder 21 (see FIG. 12). As soon as the liquid material 17 wets the back side 11b of the circuit board 11, the second capillary gap segment 16b can produce its suction action and take up liquid material 17. For stiffness, the shoulder 21 thrusts against the housing 3 by a web 22.


The slitlike supply opening 20 has a widening, roughly in the middle. The widening forms a ventilation opening 23. The ventilation opening 23 communicates with a ventilation groove 24, worked into the circuit board 11 on its back side 11b, which in turn communicates via the cavity 12 with an interior space under atmospheric pressure. The ventilation opening 23 and the ventilation groove 24 bring about a pressure equalization, in that each portion of liquid material 17 that is taken up by the second capillary gap segment 16b is immediately replaced by an equal-volume portion of air.


As is best shown by FIGS. 10 and 11, the first capillary gap segment 16a and the second capillary gap segment 16b are joined together by a third capillary gap segment 16c. The third capillary gap segment 16c is formed by the circuit board edge 11c and an adjacent housing wall 3a. The platelike top piece 14 that is connected to the circuit board is used for the exact placement of the third capillary gap segment 16c. This adjoins the housing wall 3a and projects beyond the edge of the circuit board 11c by a precisely defined measure. The measure corresponds to the gap width of the third capillary gap segment 16c and typically amounts to 0.3 mm. The circuit board 11 and the platelike top piece 14, which as already mentioned form a preassembled unit, must thus be joined precisely.


The three capillary gap segments 16a, 16b, 16c together form the capillary gap 16. The capillary gap 16 thus consists of an extended, interconnected capillary gap system, which partly encloses the circuit board 11. Leaving out of consideration the segments of the circuit board 11 protruding from the housing 3, i.e., the insert tongues 8a, then in the specific sample embodiment distinctly more than 50% of the circuit board surface form boundary walls of the capillary gap 16. The resulting beneficial effects with regard to the buffering of the liquid material 17, as well as the supply reliability and supply capacity, have already been discussed. A basic requirement for achieving these favorable effects is that the liquid material 17 sufficiently wet all exposed surfaces. To make sure of this, the affected parts—namely the liquid container 18a, the circuit board 11 and compound structures 10, the top piece 14 and at least parts of the housing 3—should undergo hydrophilic treatment in a suitable process even prior to assembly. Suitable processes are hydrophilic treatment in oxygen plasma and hydrophilic treatment by means of plasma polymerization. Both processes are offered, for example, by the firm Diener electronic GmbH u. Co. KG, www.plasma.de, on a subcontract order basis. Furthermore, this firm is able to design and erect suitable plants for mass production according to the client's specifications.


Before going further into the mode of operation of the inhaler according to the invention, we shall now describe additional parts of the inhaler component 2. Even though these parts might not be directly relevant to the invention, their description still contributes to a better understanding of the function of the invented inhaler component as a whole, and to further assure the implementation of the invention: between the top piece 14 and the housing 3 there are arranged two open-pore, absorbent sponges 25a, 25b (see FIG. 4g and FIG. 11). The space between the sponges forms, together with the recess 15, a chamber 26 (also see FIG. 8), in which the actual formation of the mixture of vapor and air and/or condensation aerosol occurs. The sponges 25a, 25b take up condensate deposits formed from the vapor phase into their pores and prevent freely movable condensate accumulations from forming in the inhaler component 2, which might impair the function of the inhaler component. Such condensate accumulations can also be a problem from a hygiene standpoint, especially if they get into the user's oral cavity through the mouth piece 4. The sponges 25a, 25b preferably consist of a fine-pore fiber compound structure. The firm Filtrona Fibertee GmbH, www.filtronafibertec.com, specializes its the manufacture of such fiber compound structures, processing both cellulose acetate fibers bound by means of triacetin and also thermally bound polyolefin and polyester fibers.


The sponges 25a, 25b are mounted on angle profiles 27a, 27b formed from a U-beam 27 (see FIG. 4g and FIG. 11). The beam 27 is joined to the top piece 14 by a glue connection. The beam 27 and angle profiles 27a, 27b preferably consist of a hydrophobic plastic. The hydrophobic material acts like a moisture barrier and ensures that no liquid material 17 can get to the sponges 25a, 25b by capillary effects. In the legs 27c joining the angle profiles 27a, 27b, at the side facing the top piece 14, there is made a depression 28 which, together with the top piece 14, forms an air nozzle 29 (see FIG. 9 and FIG. 10). The air nozzle 29, as shall be discussed more closely hereafter, serves to bring ambient air into the chamber 26. So that condensate deposits do not block the air nozzle 29, it is recommended to cover the surface of the top piece 14 with a thin hydrophobic adhesive tape (not shown) is the region of the air nozzle 29.


The supplying of the inhaler component 2 with ambient air to form the mixture of vapor and air and/or condensation aerosol occurs via a suction snorkel 30 termed by the housing 3 (see FIG. 3a/3b and FIG. 8). The suction snorkel 30 is arranged at the end of the inhaler component 2 opposite the mouth piece 4. This position best protects against entry of rain water. In the connected state, the suction snorkel 30 of the inhaler component 2 projects through a hole 31 formed by the main housing 5 of the inhaler part 1 (see FIG. 2). There is a flow throttle 32 in the suction snorkel 30. The flow throttle 32 has the purpose of creating flow resistance, similar to that of a cigarette, so that the user feels a similar draw resistance to that when drawing on a cigarette. Specifically, the flow resistance should be in the range of 8-16 mbar for a flow rate of 1.05 L/min and have the most linear characteristic possible. The flow throttle 32 is required when the resulting mixture of vapor and air and/or condensation aerosol is to be supplied as with a cigarette, namely, by drawing into the oral cavity (draw volume around 20-80 mL), possibly followed by an inhalation into the lungs. This mode of operation is recommended primarily when the liquid material 17 contains nicotine. The flow throttle 32 is not needed, however, when the inhaler is to provide a direct lung inhalation in a single step, as is the case with most medical inhalers. The flow throttle 32 consists preferably of a fiber compound structure similar to a cigarette filter, wherein the density of the material should be attuned to the aforementioned flow characteristic. The material, in turn, can be ordered from the firm Filtrona Fibertec GmbH, www.filtronafibertec.com.


In the following, the function of the inhaler shall be described in detail: a user attaches a new inhaler component 2 to the reusable inhaler part 1. The electrical circuit 7 registers the connection and may order to carrying out of certain preparatory operations, such as one or more evaporation cycles with the aim of supplying the compound structures 10 with fresh liquid material 17 and/or bringing about stationary conditions. Once these operations are concluded, the electrical circuit 7 signals the readiness of the inhaler, for example, through a light-emitting diode. The user brings up the mouth piece 4 of the inhaler to his mouth and activates the switch 7a. At the same time, he begins to draw on the mouth piece 4. The partial vacuum produced in this way has the effect that air flows from the surroundings into the suction snorkel 30. After the air has passed through the flow throttle 32, the flow bends at a right angle (see arrows in FIG. 8 and FIG. 9) and emerges into a plenum chamber 33, where the air accumulates and is then supplied uniformly to the slitlike air nozzle 29. The air flow is accelerated in the air nozzle 29 and enters with a high exit velocity into the chamber 26.


Activating the switch 7a has the effect of turning on the heating current circuit 7. The heating current is preferably switched by means of a power MOSFET, and the supplied power can be adapted to the particular requirements by a duty cycle. This adapting can also be done in certain limits by the user via an interface, making it possible for him to influence the resulting quantity of aerosol or smoke. The heating current is switched on for a predetermined period of time (“heating period”), typically amounting to 1.0-1.8 seconds. The heating current is taken to the compound structures 10 via the insert tongues 8a and the conductor tracks 13 of the circuit board 11 and brings about a lightning-fast heating of the compound structures 10 and the liquid material 17 stored in the wicks, whereupon the liquid material 17 evaporates. The vapor is emitted into the chamber 26, where it mixes with the air flowing in through the air nozzle 29. The arrangement and dimensioning of the air nozzle 29 produces a fast and uniform flow across the compound structures 10. This makes sure that the vapor released by the compound structures 10 encounters approximately the same mixture conditions everywhere, and the mixture of vapor and air is intimate. The air brings about a cooling of the vapor, so that a condensation aerosol can also form, provided the evaporated liquid material 17 contains substances with sufficiently low vapor pressure—so-called aerosol-forming substances. A typical example of such aerosol-forming substances is glycerol.


The mixture of vapor and air and/or condensation aerosol formed in the chamber 26 finally flows through yet another cooler 34 in the sample embodiment, before if is presented to the user for inhaling via the mouth piece 4 (see FIG. 4g and FIG. 8). The cooler 34 can consist, for example, of a porous filler material, a fleecelike fiber material, or an open-cell foam material whose pores are flowed through by the resulting mixture of vapor and air and/or condensation aerosol. The cooler 34 can also be multistaged, wherein the individual cooler stages have different properties. If the material being evaporated contains nicotine. It may be advantageous to coat the cooler material of at least one cooler stage with a suitable absorbent, such as citric acid. The absorbent extracts volatile nicotine fractions from the flowing condensation aerosol, which would otherwise be deposited in the oral cavity and throat, which is neither pharmacokinetically nor organoleptically desirable. Moreover, fragrances such as menthol can be added to the cooler material.


Suitable fleecelike fiber materials can be ordered, for example, from the firm Freudenberg Vliesstoffe KG, www.freudenberg-filter.com. The material consisting of polyolefin fibers and marketed under the name Viledon® filter mats is prepared by customer specification, and the material properties can be attuned so that the end product is largely permeable to the fine particles of the resulting condensation aerosol. A suitable foam material can be ordered, for example, from the firm Dunlop Equipment, www.dunlop-equipment.com. This supplier offers Ni and NiCr foam under the product name Retimer® (Grade 80) with a porosity of 90-95% and a pore diameter of around 300 μm in slabs up to thickness of 15 mm. According to an oral communication from firm representatives, even somewhat more fine-pored foams can be produced from a technological standpoint. The metal foams, furthermore, can be additionally compacted by roll treatment. The slabs can be further processed by laser cutting or wire erosion. Ni foam and especially NiCr foam are characterized by high strength, as well as high temperature and oxidation resistance. These properties make advisable a recycling and reusing of the relatively expensive metal foams at the end of the useful life of the inhaler component 2. If the liquid material 17 contains nicotine, the inhaler component 2 should be provided to the consumer only in return for a suitable deposit. This makes sure that the majority of the coolers 34, sponges 25a, 25b and liquid containers 18 contaminated with nicotine residue will be properly disposed of and possibly recycled.


At the end of the heating period, the circuit 7 deactivates the switch 7a for a couple of seconds. The deactivation is reported to the user, for example, by a light-emitting diode, and is necessary so that the compound structures 10 can cool down, and the wicks can again take up new liquid material 17. The liquid transport is brought about by the capillarity of the compound structures 10 and their wicks. The wicks take up the liquid material 17 through the compound structure end segments 10a, 10b from the first capillary gap segment 16a (see FIG. 4b/4f and FIG. 11). Thus, the wicks are infiltrated from two sides. The uptake of liquid material 17 from the first capillary gap segment 16a induces a capillary pressure in the capillary gap 16 that works its way back to the liquid container 18. The capillary pressure has the consequence that liquid material 17 flows from the liquid container 18 across the slitlike supply opening 20 into the second capillary gap segment 16b (see arrows in FIG. 4a). From there, the liquid material 17 goes through the third capillary gap segment 16c into the first capillary gap segment 16a, where it finally replaces the quantity of liquid removed. If, for whatever reason, disturbances in the capillary flow occur at one or more places in the capillary gap system 16, in most instances an alternative pathway will be found to get around the affected sites.


The quantity of liquid material 17 removed from the liquid container 18 is replaced by an equivalent quantity of air in the course of a pressure equalization. The pressure equalization occurs via the ventilation groove 24 and the ventilation opening 23. Once the compound structures 10 and wicks have again been fully infiltrated with the liquid material 17, the inhaler is ready for another evaporation cycle.


In an inverted position of use of the inhaler component 2—the month piece 4 points downward—the capillary coupling between the capillary gap 16 and the liquid material 17 in the liquid container 18 is lost, because the air cushion 35 always present in the liquid container 18 always points upwards in every position on account of buoyancy, i.e., in the invested position of use it will come to lie in the region of the supply opening 20. An operation of the inhaler is still possible, at least for a certain number of draws or inhalations, because enough liquid material 17 has been buffered in the extended capillary gap system 16. Only when all capillary gap segments 16a, 16b, 16c are completely empty are the wicks liable to dry out. It is necessary, at latest at this time, to turn the inhaler component 2 back to a normal position of use, so that the capillary gap 16 can again fill with the liquid material 17, which process incidentally takes only a few seconds.


In conclusion, there shall be further disclosed, as an example, a nicotine-containing preparation of the liquid material 17, which has been evaporated in prototypes (see table 1). The condensation aerosol formed and given off in this case came very close to the smoke of a conventional cigarette in terms of pharmacological, pharmacokinetic and organoleptic effects. All of the listed ingredients are also found in cigarette smoke.













TABLE 1







Substance
CAS number
Wt. %




















Water
7732-18-5
52.88



Ethanol
64-17-5
4.14



glycerol (E422)
56-81-5
40.04



Nicotine
54-11-5
1.33



lactic acid (E270)
50-21-5
0.33



succinic acid (E363)
110-15-6
0.33



benzoic acid (E210)
65-85-0
0.24



acetic acid (E260)
64-19-7
0.71




Total:
100.00










It should also be pointed out that the invention of course is not limited to one or several sheetlike compound structures 10 according to the sample embodiment just described. Alternatively, the compound structures can also be linear or threadlike. Moreover, the compound structures can be electrically interconnected in any way desired. Finally, the invention also includes devices is which the liquid container 18 can be separated from the housing 3, so that the liquid container 18 can be replaced by a new liquid container as soon as it is empty.


LIST OF REFERENCE NUMBERS




  • 1 reusable inhaler part


  • 2 interchangeable Inhaler component


  • 3 housing


  • 3
    a housing wall


  • 4 mouthpiece


  • 5 main housing


  • 6 battery


  • 7 electrical circuit


  • 7
    a switch


  • 8
    a insert tongues


  • 8
    b insert sockets


  • 9
    a guide lugs


  • 9
    b guide grooves


  • 10 sheetlike compound structures


  • 10
    a, 10b compound structure end segments


  • 11 carrier plate, circuit board, multilayer circuit board


  • 11
    a circuit board front side


  • 11
    b circuit board back side


  • 11
    c circuit board edge


  • 12 cavity


  • 13 conductor backs


  • 14 top piece


  • 15 recess


  • 16 capillary gap, capillary gap system


  • 16
    a first capillary gap segment


  • 16
    b second capillary gap segment


  • 16
    c third capillary gap segment


  • 17 liquid material


  • 18 liquid container


  • 18
    a liquid container wall


  • 19 spacer


  • 20 supply opening


  • 21 shoulder


  • 22 web


  • 23 ventilation opening


  • 24 ventilation groove


  • 25
    a, 23b open-pore, absorbent sponges


  • 26 chamber


  • 27 U-beam


  • 27
    a, 27b angle profiles


  • 27
    c leg


  • 28 depression


  • 29 air nozzle


  • 30 suction snorkel


  • 31 hole


  • 32 flow throttle


  • 33 plenum chamber


  • 34 cooler


  • 35 air cushion


Claims
  • 1. An apparatus, comprising: an inhaler component, the inhaler component including: an electrical heater configured to evaporate liquid;a capillary wick, the capillary wick and the electrical heater defining a compound structure configured to automatically supply liquid to the electrical heater;a carrier supporting the compound structure and making electrical contact with the electrical heater, the carrier at least partially defining a portion of a capillary gap, the capillary gap in fluid communication with the wick and configured to automatically supply liquid to the compound structure; anda liquid container, wherein a portion of a surface of the liquid container at least partially defines a portion of the capillary gap.
  • 2. The apparatus according to claim 1, wherein a portion of a surface of the carrier, distal relative to the compound structure, at least partially defines a portion of the capillary gap.
  • 3. The apparatus according to claim 2, wherein a portion of the surface of the carrier, proximal relative to the compound structure, at least partially defines a portion of the capillary gap.
  • 4. The apparatus according to claim 1, wherein the capillary gap at least partially surrounds a portion of the carrier.
  • 5. The apparatus according to claim 1, wherein more than half of the surface of the carrier at least partially defines a portion of the capillary gap.
  • 6. The apparatus according to claim 1, further including a housing.
  • 7. The apparatus according to claim 6, wherein a portion of the capillary gap is at least partially defined by a surface of the housing.
  • 8. The apparatus according to claim 1, wherein at least a portion of a surface defining a portion of the capillary gap is a hydrophilic surface.
  • 9. The apparatus of claim 8, wherein the hydrophilic surface is at least one of an oxygen-plasma treated hydrophilic surface and/or a plasma polymerization treated hydrophilic surface.
  • 10. The apparatus of claim 1, further comprising a flow throttle configured to, in use, provide flow resistance to air passing therethrough.
  • 11. The apparatus of claim 10, wherein the flow throttle is a fiber compound structure.
  • 12. The apparatus of claim 10, wherein the flow throttle is configured to provide flow resistance in the range of 8-16 mbar for a flow rate of 1.05 L/min.
  • 13. An inhaler component, comprising: a housing;an electrical heater configured to evaporate liquid;a capillary wick, the capillary wick and the electrical heater forming a compound structure configured to automatically supply liquid to the electrical heater;a carrier supporting the compound structure and making electrical contact with the electrical heater, the carrier at least partially defining a portion of a capillary gap and configured to automatically supply liquid to the compound structure via a portion of the capillary wick that extends into the capillary gap; anda liquid container, wherein a portion of a surface of the liquid container at least partially defines a portion of the capillary gap.
  • 14. The inhaler component according to claim 13, wherein a portion of a surface of the carrier and a wall of the housing together at least partially define a capillary gap portion.
  • 15. The inhaler component according to claim 14, wherein a portion of the surface of the carrier distal to the housing at least partially defines a capillary gap portion.
  • 16. The inhaler component according to claim 13, wherein at least a portion of a surface defining a capillary gap portion is a hydrophilic surface.
  • 17. The inhaler component of claim 13, further comprising: a suction snorkel at an end of the inhaler component opposite a mouthpiece end of the inhaler component; and a flow throttle disposed within the suction snorkel and configured to provide flow resistance to air passing through when the inhaler component is in use.
  • 18. The inhaler component of claim 17, wherein the flow resistance provided by the flow throttle is from 8 mbar to 16 mbar for a flow rate of 1.05 L/min.
Priority Claims (1)
Number Date Country Kind
A 1543/2011 Oct 2011 AT national
CLAIM FOR PRIORITY

This application is a continuation of U.S. patent application Ser. No. 14/353,256, filed Apr. 21, 2014, which is the National Stage of International Application No. PCT/EP2012/070647, filed Oct. 18, 2012, which in turn claims priority to and benefit of Austrian Patent Application No. AT A1543/2011, filed Oct. 21, 2011. The entire contents of the aforementioned applications are herein expressly incorporated by reference.

US Referenced Citations (277)
Number Name Date Kind
228598 Buckley Jun 1880 A
353327 Randolph Nov 1886 A
576653 Bowlby Feb 1897 A
595070 Oldenbusch Dec 1897 A
744074 Hiering Nov 1903 A
799844 Fuller Sep 1905 A
885374 Pohlig Apr 1908 A
1163183 Stoll Dec 1915 A
D53386 Thomas May 1919 S
1436157 Fazio Nov 1922 A
1807936 Saunders Jun 1931 A
1815069 Petro Jul 1931 A
1937120 Lagerholm Nov 1933 A
1937987 Sexton Dec 1933 A
2057353 Whittemore, Jr. Oct 1936 A
2262318 Fox Nov 1941 A
2411946 Vogel Dec 1946 A
2467923 Allen Apr 1949 A
2483304 Vogel Sep 1949 A
2522952 Krohn Sep 1950 A
2658368 Siegal Nov 1953 A
2782910 Liebow Feb 1957 A
2809634 Murai Oct 1957 A
3111396 Ball Nov 1963 A
3165225 Reitzel Jan 1965 A
3402724 Blount Sep 1968 A
3431393 Katsuda Mar 1969 A
3433632 Elbert et al. Mar 1969 A
3521643 Toth Jul 1970 A
3722742 Wertz Mar 1973 A
3743136 Chambers Jul 1973 A
3804100 Fariello Apr 1974 A
3861523 Fountain et al. Jan 1975 A
3863803 Valcic Feb 1975 A
3964902 Fletcher Jun 1976 A
4009713 Simmons et al. Mar 1977 A
4031906 Knapp Jun 1977 A
4094119 Sullivan Jun 1978 A
4145001 Weyenberg et al. Mar 1979 A
4161283 Hyman Jul 1979 A
4190412 Tokai Feb 1980 A
4193513 Bull Mar 1980 A
4214658 Crow Jul 1980 A
4503851 Braqunroth et al. Mar 1985 A
D279508 Bauer et al. Jul 1985 S
4588976 Jaselli May 1986 A
4676237 Wood et al. Jun 1987 A
4733794 Kent Mar 1988 A
4735217 Gerth et al. Apr 1988 A
4753383 Focke et al. Jun 1988 A
4793478 Tudor Dec 1988 A
4830028 Lawson May 1989 A
4848374 Chard et al. Jul 1989 A
4885129 Leonard Dec 1989 A
4917301 Munteanu Apr 1990 A
4922901 Brooks et al. May 1990 A
4923059 Evers et al. May 1990 A
4947874 Brooks et al. Aug 1990 A
4947875 Brooks et al. Aug 1990 A
4978814 Honour Dec 1990 A
5027837 Clearman Jul 1991 A
5044550 Lamm Sep 1991 A
5046514 Bolt Sep 1991 A
5060671 Counts et al. Oct 1991 A
D322687 Tschudin Dec 1991 S
5095647 Zobele Mar 1992 A
5095921 Losee et al. Mar 1992 A
5099861 Clearman Mar 1992 A
5121881 Lembeck Jun 1992 A
5167242 Turner et al. Dec 1992 A
5179966 Losee et al. Jan 1993 A
5247947 Clearman et al. Sep 1993 A
D346878 Gee et al. May 1994 S
5322075 Deevi et al. Jun 1994 A
5388574 Ingebrethsen Feb 1995 A
5390864 Alexander Feb 1995 A
5448317 Huang Sep 1995 A
5479948 Counts Jan 1996 A
5497792 Prasad et al. Mar 1996 A
5501236 Hill et al. Mar 1996 A
5505214 Collins Apr 1996 A
5540241 Kim Jul 1996 A
5553791 Alexander Sep 1996 A
5636787 Gowhari Jun 1997 A
5649554 Sprinkel et al. Jul 1997 A
5666977 Higgins et al. Sep 1997 A
5692291 Deevi Dec 1997 A
D392069 Rowland Mar 1998 S
5743251 Howell Apr 1998 A
D404201 Wennerstrom Jan 1999 S
5865185 Collins Feb 1999 A
5896984 Focke Apr 1999 A
D414892 Chen Oct 1999 S
5967312 Jacobs Oct 1999 A
6065592 Wik May 2000 A
6095505 Miller Aug 2000 A
D432263 Issa Oct 2000 S
D434217 Packard et al. Nov 2000 S
D434979 Liu Dec 2000 S
6155268 Takeuchi Dec 2000 A
D436725 Rogers Jan 2001 S
D438003 Minagawa et al. Feb 2001 S
D441133 Emery Apr 2001 S
6275650 Lambert Aug 2001 B1
D449521 Pinkus et al. Oct 2001 S
6321757 McCutcheon Nov 2001 B1
6446793 Layshock Sep 2002 B1
D466012 Baker Nov 2002 S
D470765 Baker Feb 2003 S
D471804 Staples Mar 2003 S
D472012 South Mar 2003 S
6527166 Focke et al. Mar 2003 B1
6530495 Joseph Mar 2003 B1
6561391 Baker May 2003 B1
6652804 Neumann et al. Nov 2003 B1
6681998 Sharpe Jan 2004 B2
6701921 Sprinkel Mar 2004 B2
6715605 Manservigi et al. Apr 2004 B1
D493617 Armato Aug 2004 S
6790496 Levander Sep 2004 B1
D509732 Staples Sep 2005 S
7100618 Dominguez Sep 2006 B2
7112712 Ancell Sep 2006 B1
D545186 Liebe et al. Jun 2007 S
D549573 Liebe et al. Aug 2007 S
7263282 Meyer Aug 2007 B2
D550455 Barnhart Sep 2007 S
D566329 Bagaric et al. Apr 2008 S
D566890 Bagaric et al. Apr 2008 S
7389878 Torrico Jun 2008 B1
D573889 Short et al. Jul 2008 S
7400940 McRae et al. Jul 2008 B2
D575451 Jones et al. Aug 2008 S
7455176 Focke et al. Nov 2008 B2
7540286 Cross et al. Jun 2009 B2
7565969 He Jul 2009 B2
D606854 Greenhalgh Dec 2009 S
D610983 Wai et al. Mar 2010 S
D611806 Bried Mar 2010 S
D613903 Wu Apr 2010 S
D613904 Wu Apr 2010 S
D616753 Beam et al. Jun 2010 S
7767698 Warchol Aug 2010 B2
7832410 Hon Nov 2010 B2
D628469 Taylor et al. Dec 2010 S
D631838 Cheng Feb 2011 S
D636257 Bougoulas et al. Apr 2011 S
7992554 Radomski Aug 2011 B2
D649658 Belfrance et al. Nov 2011 S
D650738 Leung Dec 2011 S
8113343 Akerlind Feb 2012 B2
D656094 Wu Mar 2012 S
8156944 Hon Apr 2012 B2
D661016 Borges et al. May 2012 S
D671677 Wu Nov 2012 S
D671678 Wu Nov 2012 S
8307834 Palmerino, Sr. et al. Nov 2012 B1
D672642 Supranowicz Dec 2012 S
D674539 Wu Jan 2013 S
8365742 Hon Feb 2013 B2
8375957 Hon Feb 2013 B2
8393331 Hon Mar 2013 B2
8430106 Potter Apr 2013 B2
8448783 Vecchi May 2013 B2
8490628 Hon Jul 2013 B2
8511318 Hon Aug 2013 B2
D693055 Manca et al. Oct 2013 S
D700397 Manca et al. Feb 2014 S
8752545 Buchberger Jun 2014 B2
8689805 Hon Aug 2014 B2
8794245 Scatterday Aug 2014 B1
8833364 Buchberger Sep 2014 B2
D715760 Kim et al. Oct 2014 S
D716267 Kim et al. Oct 2014 S
D720884 Liu Jan 2015 S
8948578 Buchberger Feb 2015 B2
D723738 Liu Mar 2015 S
D736460 McKeon et al. Aug 2015 S
D737507 Liu Aug 2015 S
9623205 Buchberger Apr 2017 B2
20010042546 Umeda Nov 2001 A1
20020016370 Shytle Feb 2002 A1
20020079309 Cox et al. Jun 2002 A1
20030005620 Ananth Jan 2003 A1
20030049025 Neumann et al. Mar 2003 A1
20030106552 Sprinkel, Jr. et al. Jun 2003 A1
20030200964 Blakley et al. Oct 2003 A1
20040031485 Rustad Feb 2004 A1
20040056651 Marietta Mar 2004 A1
20040129793 Nguyen et al. Jul 2004 A1
20050087460 Bruhm et al. Apr 2005 A1
20050204799 Koch Sep 2005 A1
20050211243 Esser Sep 2005 A1
20050224375 Focke et al. Oct 2005 A1
20050268911 Cross et al. Dec 2005 A1
20060078477 Althouse Apr 2006 A1
20070014549 Demarest Jan 2007 A1
20070062548 Horstmann Mar 2007 A1
20070102013 Adams et al. May 2007 A1
20070107879 Radomski et al. May 2007 A1
20070155255 Galauner et al. Jul 2007 A1
20070193895 Weiss et al. Aug 2007 A1
20080017204 Braunshteyn Jan 2008 A1
20080092912 Robinson et al. Apr 2008 A1
20080216828 Wensley et al. Sep 2008 A1
20080223382 Zeanah Sep 2008 A1
20090095311 Han Apr 2009 A1
20090188490 Han Jul 2009 A1
20090266837 Gelardi et al. Oct 2009 A1
20090272379 Thorens et al. Nov 2009 A1
20090288966 Minarelli et al. Nov 2009 A1
20090293892 Williams Dec 2009 A1
20100059070 Potter Mar 2010 A1
20100065653 Wingo Mar 2010 A1
20100083959 Siller Apr 2010 A1
20100108059 Axelson May 2010 A1
20100236546 Yamada Sep 2010 A1
20100313901 Fernando et al. Dec 2010 A1
20110011396 Fang Jan 2011 A1
20110036363 Urtsev et al. Feb 2011 A1
20110126848 Zuber et al. Jun 2011 A1
20110180433 Rennecamp Jul 2011 A1
20110226236 Buchberger Sep 2011 A1
20110290267 Yamada et al. Dec 2011 A1
20110297166 Takeuchi et al. Dec 2011 A1
20110303231 Li et al. Dec 2011 A1
20120145169 Wu Jun 2012 A1
20120199146 Marangos Aug 2012 A1
20120227752 Alelov Sep 2012 A1
20120227753 Newton Sep 2012 A1
20120260927 Liu Oct 2012 A1
20120285476 Hon Nov 2012 A1
20130074857 Buchberger Mar 2013 A1
20130081623 Buchberger Apr 2013 A1
20130098786 Collins Apr 2013 A1
20130192615 Tucker et al. Aug 2013 A1
20130192621 Li Aug 2013 A1
20130192623 Tucker Aug 2013 A1
20130213419 Tucker et al. Aug 2013 A1
20130284192 Peleg et al. Oct 2013 A1
20130333700 Buchberger Dec 2013 A1
20130340779 Liu Dec 2013 A1
20130341218 Liu Dec 2013 A1
20130342157 Liu Dec 2013 A1
20140000638 Sebastian et al. Jan 2014 A1
20140007892 Liu Jan 2014 A1
20140020697 Liu Jan 2014 A1
20140048086 Zhanghua Feb 2014 A1
20140060528 Liu et al. Mar 2014 A1
20140060554 Collett et al. Mar 2014 A1
20140060555 Chang et al. Mar 2014 A1
20140196717 Liu Jul 2014 A1
20140196731 Scatterday Jul 2014 A1
20140202454 Buchberger Jul 2014 A1
20140238396 Buchberger Aug 2014 A1
20140238423 Tucker et al. Aug 2014 A1
20140238424 MacKo et al. Aug 2014 A1
20140261490 Kane Sep 2014 A1
20140261495 Novak Sep 2014 A1
20140270730 Depiano et al. Sep 2014 A1
20140283825 Buchberger Sep 2014 A1
20140286630 Buchberger Sep 2014 A1
20140299125 Buchberger Oct 2014 A1
20140209105 Sears et al. Nov 2014 A1
20140338680 Abramov Nov 2014 A1
20150114411 Buchberger Apr 2015 A1
20150208728 Lord Jul 2015 A1
20160073693 Reevell Mar 2016 A1
20160101909 Schennum et al. Apr 2016 A1
20160106154 Lord Apr 2016 A1
20160106155 Reevell Apr 2016 A1
20160120218 Schennum et al. May 2016 A1
20170042245 Buchberger Feb 2017 A1
20170188629 Dickens et al. Jul 2017 A1
20170197043 Buchberger Jul 2017 A1
20170197044 Buchberger Jul 2017 A1
20170197046 Buchberger Jul 2017 A1
Foreign Referenced Citations (187)
Number Date Country
507 187 Mar 2010 AT
507187 Mar 2010 AT
508244 Dec 2010 AT
510 405 Apr 2012 AT
6393173 Jun 1975 AU
6402132 Jul 1986 BR
2309376 Nov 2000 CA
698603 Sep 2009 CH
698603 Sep 2009 CH
2092880 Jan 1992 CN
2220168 Feb 1996 CN
1312730 Dec 2001 CN
1329567 Jan 2002 CN
2485265 Apr 2002 CN
2660914 Dec 2004 CN
2719043 Aug 2005 CN
1703279 Nov 2005 CN
2904674 May 2007 CN
101115901 Jan 2008 CN
201023852 Feb 2008 CN
201238609 May 2009 CN
201240612 May 2009 CN
201375023 Jan 2010 CN
201430913 Mar 2010 CN
201592850 Sep 2010 CN
101878958 Nov 2010 CN
201657770 Dec 2010 CN
102014677 Apr 2011 CN
201830900 May 2011 CN
201860753 Jun 2011 CN
102264420 Nov 2011 CN
202122096 Jan 2012 CN
202172846 Mar 2012 CN
102655773 Sep 2012 CN
202 722 498 Feb 2013 CN
202 750 708 Feb 2013 CN
202722498 Feb 2013 CN
106102863 Nov 2016 CN
594585 Mar 1934 DE
1950439 Apr 1971 DE
2940797 Apr 1981 DE
3148335 Jul 1983 DE
3218760 Dec 1983 DE
3936687 May 1990 DE
19630619 Feb 1998 DE
19654945 Mar 1998 DE
10330681 Jun 2004 DE
202006013439 Oct 2006 DE
202013100606 Feb 2013 DE
202013100606 Feb 2013 DE
0 280262 Aug 1988 EP
0295122 Dec 1988 EP
0358002 Mar 1990 EP
0358114 Mar 1990 EP
0488488 Jan 1991 EP
0444553 Sep 1991 EP
0845220 Jun 1998 EP
0893071 Jan 1999 EP
1166814 Jan 2002 EP
1166847 Jan 2002 EP
1736065 Dec 2006 EP
1820748 Aug 2007 EP
1847671 Oct 2007 EP
1950439 Jul 2008 EP
2018886 Jan 2009 EP
2022349 Feb 2009 EP
2113178 Nov 2009 EP
2340729 Jul 2011 EP
2340729 Jul 2011 EP
2 698 070 Feb 2014 EP
2698070 Feb 2014 EP
2762019 Aug 2014 EP
2762019 Aug 2014 EP
2835062 Feb 2015 EP
2835062 Feb 2015 EP
472030 Nov 1914 FR
960469 Apr 1950 FR
1292446 May 1962 FR
25575 Jan 1912 GB
30472 Dec 1909 GB
191100628 Nov 1911 GB
25575 Mar 1912 GB
191311086 Sep 1913 GB
110216 Oct 1917 GB
111454 Nov 1917 GB
120016 Oct 1918 GB
160493 Mar 1921 GB
163124 May 1921 GB
215992 May 1924 GB
268967 Apr 1927 GB
402064 Nov 1933 GB
507955 Jun 1939 GB
544329 Apr 1942 GB
565574 Nov 1944 GB
611596 Nov 1948 GB
626888 Jul 1949 GB
871869 Jul 1961 GB
1313525 Apr 1973 GB
1046183 Jul 1988 GB
2275464 Aug 1994 GB
2068034 Nov 1997 GB
2369108 May 2002 GB
4000273 Dec 2006 GB
4006615 Oct 2008 GB
220229 Aug 2014 GB
S5289386 Jul 1977 JP
S57-052456 Mar 1982 JP
57S-140354 Aug 1982 JP
S59-106340 Jan 1986 JP
S61-096763 May 1986 JP
61-096765 Jan 1988 JP
H08-299862 Nov 1996 JP
11-503912 Apr 1999 JP
H1189551 Apr 1999 JP
3093201 Apr 2003 JP
2004332069 Nov 2004 JP
2005-013092 Jan 2005 JP
2005-138773 Jun 2005 JP
2007-297124 Nov 2007 JP
2009-526714 Jul 2009 JP
2011-087569 May 2011 JP
6617184 Jun 1967 NL
2311859 Dec 2007 RU
2336001 Oct 2008 RU
2360583 Jul 2009 RU
89927 Dec 2009 RU
94815 Jun 2010 RU
103281 Apr 2011 RU
115629 May 2012 RU
121706 Nov 2012 RU
122000 Nov 2012 RU
124120 Jan 2013 RU
78167 Mar 2013 UA
WO 9527412 Oct 1995 WO
WO9632854 Oct 1996 WO
WO9748293 Dec 1997 WO
WO0009188 Feb 2000 WO
WO0021598 Apr 2000 WO
WO2002058747 Aug 2002 WO
WO2002060769 Aug 2002 WO
03028409 Apr 2003 WO
WO03028409 Apr 2003 WO
WO2003028409 Apr 2003 WO
WO03050405 Jun 2003 WO
WO2003083283 Oct 2003 WO
WO2003101454 Dec 2003 WO
WO2004022242 Mar 2004 WO
WO2004022243 Mar 2004 WO
WO2005106350 Nov 2005 WO
WO2006082571 Aug 2006 WO
WO2007042941 Apr 2007 WO
WO2007131449 Nov 2007 WO
WO2008006048 Jan 2008 WO
WO2008104870 Sep 2008 WO
WO2009015410 Feb 2009 WO
WO2009092419 Sep 2009 WO
WO 2009132793 Nov 2009 WO
WO2009132793 Nov 2009 WO
2010045670 Apr 2010 WO
2010045671 Apr 2010 WO
WO2010045670 Apr 2010 WO
WO2010045671 Apr 2010 WO
WO 2011109849 Sep 2011 WO
WO2011109849 Sep 2011 WO
WO2011137453 Nov 2011 WO
WO2012025496 Mar 2012 WO
WO 2012065310 May 2012 WO
WO2012065754 May 2012 WO
WO2012114082 Aug 2012 WO
WO2013034453 Mar 2013 WO
WO2013034460 Mar 2013 WO
WO2013045942 Apr 2013 WO
WO2013057185 Apr 2013 WO
WO2013098395 Jul 2013 WO
WO 2013116558 Aug 2013 WO
WO 2014130695 Aug 2013 WO
WO2013116558 Aug 2013 WO
WO2014130695 Aug 2013 WO
WO2013142671 Sep 2013 WO
WO2013189050 Dec 2013 WO
WO2013189052 Dec 2013 WO
WO2014005275 Jan 2014 WO
WO2014015463 Jan 2014 WO
WO2014061477 Apr 2014 WO
WO2014140320 Sep 2014 WO
WO2014150131 Sep 2014 WO
WO 2013082173 Oct 2014 WO
Non-Patent Literature Citations (84)
Entry
International Search Report and Written Opinion, dated Feb. 6, 2013 for PCT/EP2012/070647, filed Oct. 18, 2012 [Previously submitted to USPTO in U.S. Appl. No. 14/353,256, filed Apr. 21, 2014].
International Search Report and Written Opinion for PCT/GB2014/051333 dated Jul. 17, 2014.
IPRP dated Aug. 5, 2015 for International Application No. PCT/GB2014/051333.
International Search Report and Written Opinion, International Application No. PCT/GB2014/051334 dated Jul. 21, 2014.
International Search Report and Written Opinion, International Application No. PCT/GB2014/051332 dated Jul. 21, 2014.
International Search Report and Written Opinion for International Application No. PCT/EP2012/003103 dated Nov. 26, 2012.
International Search Report for corresponding International Application No. PCT/GB2015/051213 dated Jul. 16, 2015; 5 pages.
Written Opinion of the International Searching Authority for corresponding International Application No. PCT/GB2015/051213 dated Jul. 16, 2015; 9 pages.
IPRP for corresponding International Application No. PCT/GB2015/051213 dated Jul. 14, 2016; 21 pages.
International Search Report and Written Opinion for PCT/AT2012/000017 dated Jul. 3, 2012.
Translation of IPRP for PCT/AT2012/000017 dated Aug. 13, 2013.
Application and File History for U.S. Appl. No. 14/235,210, filed Mar. 4, 2014 inventor Buchberger.
Application and File History for U.S. Appl. No. 14/888,514, filed Nov. 2, 2015, inventor Reevell.
Application and File History for U.S. Patent Application No. 14/888,517 filed Nov. 2, 2015, inventor Reevell.
Application and File History for U.S. Appl. No. 13/125,343, filed Apr. 21, 2011 inventor Buchberger.
Kynol, Standard Specifications of Kynol Activated Carbon Fiber Products, published by Kynol. Date unknown.
Application and File History for U.S. Appl. No. 14/268,909, filed May 2, 2014 inventor Buchberger.
International Search Report dated Jan. 26, 2010 for International Application No. PCT/AT2009/000414.
Japanese Notice of Reasons for Rejection for Japanese Application No. 2015-137361 dated May 31, 2016.
Translation of IPRP dated May 1, 2014 for International Patent Application No. PCT/EP2012/070647 filed Oct. 18, 2012.
International Search Report and Written Opinion dated Feb. 6, 2013 for PCT/EP2012/070647 filed Oct. 18, 2012.
IPRP, International Application No. PCT/GB2014/051334 dated Nov. 12, 2015.
IPRP, International Application No. PCT/GB2014/051332 dated Nov. 12, 2015.
European Search Report for European Application No. 15178588 dated Apr. 14, 2016.
Chinese Office Action for Chinese Application No. 201480024978.X dated Jan. 18, 2017.
Russian Search Report for Russian Application No. 2015146843/12 (072088) date completed Apr. 24, 2017.
Application and File History for U.S. Appl. No. 14/787,946, filed Oct. 29, 2015, inventor Lord.
Application and File History for U.S. Appl. No. 14/353,256, filed Apr. 21, 2014, inventor Buchberger.
Application and File History for U.S. Appl. No. 15/454,156, filed Mar. 9, 2017, inventor Buchberger.
Application and File History for U.S. Appl. No. 15/307,095, filed Oct. 27, 2016, inventor Buchberger.
International Preliminary Report on Patentability for International Application No. PCT/GB2014/051688 dated Dec. 8, 2015.
International Search Report or International Application No. PCT/GB2014/051688 dated Aug. 26, 2014.
Written Opinion for International Application No. PCT/GB2014/051688 dated Aug. 26, 2014.
International Search Report of the International Searching Authority for International Application No. PCT/GB2014/051633 dated Dec. 4, 2014.
Written Opinion of the International Searching Authority for International Application No. PCT/GB2014/051633 dated Dec. 4, 2014.
Notification of Transmittal of IPRP for International Application No. PCT/GB2014/051633 dated Oct. 23, 2015.
International Preliminary Report on Patentability and Written Opinion dated Nov. 3, 2015 for International Application No. PCT/GB2014/051332.
International Search Report dated Jul. 21, 2014 for International Application No. PCT/GB2014/051332.
Office Action dated Sep. 3, 2014, for Russian Application No. 2013504605.
International Preliminary Report on Patentability, dated Apr. 26, 2011, for International Application No. PCT/AT2009/000414, 7 pages.
Written Opinion, dated Jan. 26, 2010 , for International Application No. PCT/AT2009/000414, 14 pages (with translation).
Russian Decision to Grant, Application No. 2015146845, dated Apr. 27, 2017, 8 pages.
International Preliminary Report on Patentability dated Aug. 13, 2013 for International Application No. PCT/AT2012/000017.
IPRP dated Apr. 22, 2014 for International Patent Application No. PCT/EP2012/070647 filed Oct. 18, 2012.
Great Britain Examination Report, Application No. GB1405720.2, dated Jun. 27, 2017, 3 pages.
GB Intention to Grant, Application No. GB1405720.2, dated Sep. 26, 2017, 2 pages.
International Search Report, International Application No. PCT/GB2014/051334 dated Jul. 21, 2014.
Russian Office Action, Application No. 2015146847, dated Sep. 22, 2017, 11 pages.
Application and File History for U.S. Appl. No. 13/984,512, filed Aug. 29, 2013, inventor Buchberger.
Decision to Grant in Russian Application No. 120267, dated Oct. 26, 2016. No English translation available.
International Search Report and Written Opinion for International Application No. PCT/GB2014/051333 dated Jul. 17, 2014.
IPRP for International Application No. PCT/GB2014/051333 dated Aug. 5, 2015.
Translation of Search Report for JP2016517671 dated Feb. 1, 2017.
Chinese Office Action for Chinese Application No. 201480031296.1 dated Mar. 27, 2017.
Chinese Notification of First Office Action for Chinese Application No. 2014800319265 dated Apr. 21, 2017.
Korean Office Action, Korean Application No. 10-2015-7034538, dated May 12, 2017, 5 pages.
Chinese Office Action for Chinese Application No. 201480024988.3 dated Dec. 30, 2016.
Chinese Office Action for Chinese Application No. 201480024988.3 dated Sep. 11, 2017.
Hong Kong Publication, Application No. 16113324.2, published Oct. 6, 2017, 1 page.
Hong Kong Publication, Application No. 14110165.2, published Dec. 19, 2014, 1 page.
Application and File History for U.S. Appl. No. 14/296,803, filed Jun. 5, 2014, inventor Buchberger.
European Search Report for European Application No. 16166656 dated Oct. 11, 2016.
Notice of Opposition Letter from EPO. Opposition against EP2358418 dated Mar. 1, 2017.
Rudolph G, BAT Cigarettenfabriken GmbH, 1987, The Influence of CO2 on the Sensory Characteristics of the Favor-System, http://legacy.library.ucsf.edu/tid/sla51f00.
Application and File History for U.S. Appl. No. 15/470,078, filed Mar. 27, 2017, inventor Buchberger.
Application and File History for U.S. Appl. No. 15/470,089, filed Mar. 27, 2017, inventor Buchberger.
Application and File History for U.S. Appl. No. 15/470,095, filed Mar. 27, 2017, inventor Buchberger.
Dunn et al., “Heat Pipes”, Fourth Edition, Pergamon, 1994, 14 pages, ISBN 0080419038.
International Search Report for International Application No. PCT/AT2009/000413 dated Jan. 25, 2010.
Japanese Notice of Reasons for Refusal, dated Oct. 7, 2013 and dated Oct. 15, 2013 for Japanese Application No. 2011532464, 6 pages.
Japanese Notice of Reasons for Rejection dated Sep. 8, 2015 for Japanese Application No. 2014179732.
Japanese Office Action for Application No. 2016-134648 dated May 23, 2017.
Pulmonary Pharmacology: Delivery Devices and Medications, accessed at www.cdeu.org/cecourses/z98207/ch4.htm.
Chinese First Office Action for Chinese Application no. 200980152395.4 dated Dec. 3, 2012, 6 pages (16 pages with translation).
Chinese Second Office Action for Chinese Application No. 200980152395.4 dated Aug. 20, 2013, 6 pages (16 pages with translation).
Written Opinion of the International Preliminary Examining Authority for corresponding International Application No. PCT/GB2015/051213 dated Jul. 16, 2015.
Japanese Office Action, Application No. 2016-564977 , dated Dec. 5, 2017, 3 pages. (6 pages with translation).
European Extended Search Report, Application No. 17189951.1, dated Jan. 4, 2018, 8 pages.
Russian Office Action, Application No. 2016142584, dated Nov. 21, 2017, 6 pages (8 pages with translation).
Decision to Grant, Russian Application No. 2011120430, dated Apr. 1, 2014, 10 pages.
Japanese Search Report, Application No. 2016-134648, dated Mar. 28, 2017, 11 pages.
Japanese Search Report, Application No. 2014-179732, dated Aug. 25, 2015, 5 pages.
Japanese Search Report, Application No. 2011-532464, dated Sep. 18, 2013, 73 pages.
Japanese Decision to Grant, application No. 2011-532464 Aug. 5, 2014, 3 pages.
Related Publications (1)
Number Date Country
20150114411 A1 Apr 2015 US
Continuations (1)
Number Date Country
Parent 14353256 US
Child 14594065 US