Controlled removal of biological membrane by pyrotechnic charge for transmembrane transport

BACKGROUND OF THE INVENTION

This invention relates to transporting substances across a biological membrane of an animal, such as a human, and particularly to a device and method for forming openings in the biological membrane for delivering substances into the animal through the biological membrane for treatment applications, or extracting substances from the animal through the biological membrane for monitoring or other diagnosis applications.

There are many techniques known in the art for making openings or holes in biological membranes, such as skin, for drug delivery and monitoring applications. One well known example of the need in the art for less painful puncturing of a biological membrane is in the field of diabetes monitoring. Diabetes patients often must submit to painful finger sticks, sometimes several times a day, with lancets and micro-lancets in order to obtain an adequate quantity of fluid. Other than the relative size of the lancets decreasing, the use of lancets, and the resulting finger sensitivity and pain, has not changed for many years. Other techniques have been developed, such as the use of laser, hydraulic jets, or electroporation, with the purpose of minimizing the pain and invasiveness of the procedure. See, for example, commonly assigned U.S. Pat. No. 5,885,211 to Eppstein et al., which is directed to thermal microporation techniques and devices to form one or more micropores in a biological membrane.

Each of these technologies have their associated advantages and disadvantages, and accordingly, other techniques are being developed that may prove to have broad application in all transmembrane transport applications.

SUMMARY

Briefly, the present invention is directed to a method and apparatus for forming artificial openings in a selected area of a biological membrane using a pyrotechnic element that is triggered to explode in a controlled fashion so that the micro-explosion produces the artificial opening in the biological membrane to a desired depth and diameter. The method and apparatus of the present invention is suitable for use in connection with analyte monitoring whereby access to a biological fluid is gained through the at least one opening. Likewise, this technique is useful for transmembrane delivery applications where it is desirable to delivery substances through the membrane into the organism.

The above and other objects and advantages of the present invention will become more readily apparent when reference is made to the following description taken in conjunction with the accompanying drawings.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1

is a perspective view of a device comprising a pyrotechnic element connected to a trigger element disposed on a substrate that is placed in proximity with a biological membrane of an organism.

FIG. 2

is an exploded perspective view of the device shown in FIG.

1

.

FIG. 3

is a cross-sectional view of the device shown in FIG.

2

.

FIG. 4

is a cross-sectional view similar to FIG.

3

and showing the device and underlying biological membrane after the pyrotechnic element is detonated.

FIG. 5

is an exploded perspective view of device according to another embodiment of the invention.

FIG. 6

is a cross-sectional view of the device shown in FIG.

5

.

FIG. 7

is a partial cross-section view of a device according to another embodiment of the invention.

FIG. 8

is a partial cross-sectional view of the device shown in

FIG. 7

showing the formation of an opening in the biological membrane.

FIG. 9

is a partial cross-section view of a conductive network disposed on the upper surface of the substrate in contact with a plurality of pyrotechnic elements for triggering the detonation of a plurality of pyrotechnic elements to form a plurality of openings in the biological membrane.

FIG. 10

is a top view of a device having a conductive network disposed on the upper surface of the substrate in contact with a plurality of pyrotechnic elements for triggering the pyrotechnic elements to from a plurality of artificial openings.

FIG. 11

is a partial, top view of a device illustrating a detonating scheme employing traces of pyrotechnic compound disposed on the substrate between adjacent pyrotechnic elements.

FIG. 12

is a partial, cross-section view of a device showing the pyrotechnic element combined with one or more permeants or enhancers to be introduced into the organism during the explosive formation of the artificial opening.

FIG. 13

is a partial, cross-section view of a device featuring a reservoir for permeants or enhancers disposed between the pyrotechnic element and the biological membrane.

FIG. 14

is a partial, cross-section view of a device showing a cover film disposed on the pyrotechnic element.

FIG. 15

is a partial, cross-section view of a device featuring a reservoir cavity for permeants or enhancers disposed between a first film layer and a second film layer.

FIG. 16

is a partial, cross-section view of another device featuring a reservoir cavity for permeants or enhancers disposed between a first film layer and a second film layer.

FIG. 17

is a partial cross-section view of a device featuring angled orientation of the pyrotechnic element.

DETAILED DESCRIPTION OF THE INVENTION

It is to be understood that this invention is not limited to the particular configurations, process steps, and materials disclosed herein as such configurations, process steps, and materials may vary somewhat. It is also to be understood that the terminology employed herein is used for the purpose of describing particular embodiments only and is not intended to be limiting since the scope of the present invention will be limited only by the appended claims and equivalents thereof.

It is noted that, as used in this specification and the appended claims, the singular forms “a,” “an,” and “the” include plural referents unless the context clearly dictates otherwise. In describing and claiming the present invention, the following terminology will be used in accordance with the definitions set out below.

As used herein, the term “tissue” means an aggregate of cells of a particular kind, together with their intercellular substance, that forms a structural material. At least one surface of the tissue must be available for the present invention to be carried out. The preferred surface of the tissue is the skin.

As used herein, “poration,” “microporation,” or any such similar term means the formation of a small hole or pore in or through the biological membrane, such as skin or mucous membrane, or the outer layer of an organism to lessen the barrier properties of this biological membrane the passage of biological fluids, such as analytes from below the biological membrane for analysis or the passage of active permeants or drugs from without the biological membrane for selected purposes. Preferably the hole or “micropore” so formed is approximately 1-1000 μm in diameter and will extend into the biological membrane sufficiently to break the barrier properties of this layer without adversely affecting the underlying tissues. It is to be understood that the term “micropore” is used in the singular form for simplicity, but that the device of the present invention may form multiple artificial openings.

As used herein “penetration” means the controlled removal of cells caused by the thermal and kinetic energy released when the pyrotechnic element explodes which causes cells of the biological membrane and possibly some adjacent cells to be “blown away” from the site.

As used herein, “penetration enhancement” or “permeation enhancement” means an increase in the permeability of the biological membrane to a drug, analyte, or other chemical molecule, compound or particle (also called “permeant”), i.e., so as to increase the rate at which a drug, analyte, or other chemical molecule, compound or particle permeates the biological membrane and facilitates the increase of flux across the biological membrane for the purpose of the withdrawal of analytes out through the biological membrane or the delivery of drugs across the biological membrane and into the underlying tissues.

As used herein, “enhancer”, “chemical enhancer,” “penetration enhancer,” “permeation enhancer,” and the like includes all enhancers that increase the flux of a permeant, analyte, or other molecule across the biological membrane, and is limited only by functionality. In other words, all cell envelope disordering compounds and solvents and any other chemical enhancement agents are intended to be included. Additionally, all active force enhancer technologies such as the application of sonic energy, mechanical suction, pressure, or local deformation of the tissues, iontophoresis or electroporation are included. For example, ammonia may be used as an enhancer for the device of the present invention. In this example, the ammonia may increase the permeability of selected tissue structures, such as the capillary walls, within the tissues proximate to, or extending some distance from, the formed micropore. One or more enhancer technologies may be combined sequentially or simultaneously. For example, the ammonia enhancer may first be applied to permealize the capillary walls and then an iontophoretic or sonic energy field may be applied to actively drive a permeant into those tissues surrounding and comprising the capillary bed. The shock wave generated by the detonation of the pyrotechnic element of the present invention is itself a sonic permeation enhancer.

As used herein, “transdermal” or “percutaneous” means passage of a permeant into and through the biological membrane to achieve effective therapeutic blood levels or local tissue levels of a permeant, or the passage of a molecule or fluid present in the body (“analyte”) out through the biological membrane so that the analyte molecule may be collected on the outside of the body.

As used herein, the term “permeant,” “drug,” or “pharmacologically active agent” or any other similar term means any chemical or biological material or compound suitable for transdermal administration by the methods previously known in the art and/or by the methods taught in the present invention, that induces a desired biological or pharmacological effect, which may include but is not limited to (1) having a prophylactic effect on the organism and preventing an undesired biological effect such as an infection, (2) alleviating a condition caused by a disease, for example, alleviating pain or inflammation caused as a result of disease, and/or (3) either alleviating, reducing, or completely eliminating the disease from the organism. The effect may be local, such as providing for a local anesthetic effect, or it may be systemic. Such substances include broad classes of compounds normally delivered into the body, including through body surfaces and membranes, including skin. In general, this includes but is not limited to: antiinfectives such as antibiotics and antiviral agents; analgesics and analgesic combinations; anorexics; antihelminthics; antiarthritics; antiasthmatic agents; anticonvulsants; antidepressants; antidiabetic agents; antidiarrheals; antihistamines; antiinflammatory agents; antimigraine preparations; antinauseants; antineoplastics; antiparkinsonism drugs; antipruritics; antipsychotics; antipyretics; antispasmodics; anticholinergics; sympathomimetics; xanthine derivatives; cardiovascular preparations including potassium and calcium channel blockers, beta-blockers, alpha-blockers, and antiarrhythmics; antihypertensives; diuretics and antidiuretics; vasodilators including general coronary, peripheral and cerebral; central nervous system stimulants; vasoconstrictors; cough and cold preparations, including decongestants; hormones such as estradiol and other steroids, including corticosteroids; hypnotics; immunosuppressives; muscle relaxants; parasympatholytics; psychostimulants; sedatives; and tranquilizers. By the method of the present invention, both ionized and nonionized drugs may be delivered, as can drugs of either high or low molecular weight. Additionally, microparticles, DNA, RNA, viral antigens or any combination of the permeants listed above may be deliver by the present invention.

As used herein, an “effective” amount of a pharmacologically active agent means a sufficient amount of a compound to provide the desired local or systemic effect and performance at a reasonable benefit/risk ratio attending any medical treatment. An “effective” amount of a permeation or chemical enhancer as used herein means an amount selected so as to provide the desired increase in biological membrane permeability, the desired depth of penetration, rate of administration, and amount of drug delivered.

As used herein, a “pyrotechnic element” means any chemical, matter or combination of chemicals and/or matters that have an explosive characteristic when suitably detonated. The pyrotechnic element of the present invention undergoes very rapid decomposition (as combustion) with the production of heat and the formation of more stable materials (as gases) which exert pressure as they expand at the high temperature produced thereby creating a shock wave with a high peak pressure lasting or a short period of time. Thus, the energy produced by the pyrotechnic element includes both high temperature and high pressure. One example of a pyrotechnic element suitable for the present invention includes a stoichiometric mixture of zirconium powder and potassium perchlorate combined with a nitrocellulose binder of 1-5 parts per 100 parts of the stoichiometric mixture as a suspension in an organic solvent. Another example would be a gelled form of nitroglycerin, which has the additional advantage of already being an approved drug for transdermal delivery applications.

As used herein, a “pyrotechnic ink” means any pyrotechnic element that is applied in a liquid form and which subsequently cures into the solid or gelled shape of the pyrotechnic element.

As used herein, the term “biological membrane” means the structure separating one area of an organism from another, such as a capillary wall, lining of the gut or the outer layer of an organism which separates the organism from it's external environment, such as epithelial tissue, skin, buccal mucosa or other mucous membrane. The stratum corneum of the skin may also be included as a biological membrane.

As used herein, “animal” or “organism” refers to humans and other living organisms including plants, to which the present invention may be applied.

As used herein, “analyte” means any chemical or biological material or compound suitable for passage through a biological membrane by the technology taught in this present invention, or by technology previously known in the art, of which an individual might want to know the concentration or activity inside the body. Glucose is a specific example of an analyte because it is a sugar suitable for passage through the skin, and individuals, for example those having diabetes, might want to know their blood glucose levels. Other examples of analytes include, but are not limited to, such compounds as sodium, potassium, bilirubin, urea, ammonia, calcium, lead, iron, lithium, salicylates, and the like.

As used herein, “transdermal flux rate” is the rate of passage of any analyte out through the skin of an individual, human or animal, or the rate of passage of any permeant, drug, pharmacologically active agent, dye, or pigment in and through the skin of an organism.

As used herein, “artificial opening” means any physical breach of the biological membrane of a suitable size for delivering or extraction fluid therethrough, including micropores.

The present invention is directed to a novel method and apparatus for creating microscopic holes, i.e. artificial openings

2

, in a biological membrane

4

, such as the stratum corneum of human skin, to increase the permeability of the biological membrane

4

with a minimal amount of sensation to the organism. Referring first to

FIG. 1

, the device of the present invention is shown generally at

10

. The device

10

comprises essentially three elements: a substrate

20

, a pyrotechnic element

30

, and a trigger device

40

. Generally, the function of the device

10

is to attach sufficiently to the surface of the biological membrane

4

and to make one or more artificial openings, or artificial openings

2

, therein. More particularly, upon the detonation and resulting micro-explosion of the pyrotechnic element

30

upon receipt of a detonation signal

42

from the trigger device

40

, high temperature gases in combination with high localized pressures are directed at the targeted tissues when the micro-explosion is created in proximity to the biological membrane

4

. This results in the thermal and kinetic energy removal of the targeted tissue and the resultant formation of an artificial opening

2

.

As one skilled in the art will appreciate, the formation of the artificial opening

2

by the micro-explosion produced by the present invention will cause the artificial openings

2

to be formed in a very short time, which allows the microporation process to be carried out with little or no sensation to the subject organism. Based on the combustion front propogation of some of the common pyrotechnic compounds, a micro-charge such as those being discussed in the context of this invention could be expected to completely detonate within a few microseconds. The present invention concentrates the thermal and pressure energy produced by the explosion to the targeted areas of the biological membrane. For example, if the complete detonation/poration cycle is completed within less than 0.010 seconds, it can be shown via finite element thermal analysis that the thermal energy introduced into the biological membrane falls off with such a steep gradient that the peak temperature within 100 microns of the poration area never exceeds ˜40° C., which is well below the human pain threshold for temperature if the targeted tissue is skin. More particularly, the present invention can create a pressure front which dissipates exponentially in the surrounding tissues after creating the desired pore, passing very little surplus energy into these adjacent tissues. In addition, the increased localized pressure produced by the micro-explosion of the pyrotechnic element

30

increases the combustion efficiency of the chemical reaction, which reduces the total amount of energy required to porate to a specific depth.

The substrate

20

of the device

10

has an upper surface

22

and a lower surface

24

. The pyrotechnic element

30

may be positioned on either the upper or the lower surface

22

,

24

of the substrate

20

but is shown disposed on the upper surface

22

of the substrate

20

. The trigger device

40

is operatively connected to the pyrotechnic element

30

and is preferably on the same surface of the substrate

20

that the pyrotechnic element is disposed. The lower surface of the substrate

20

is in physical contact with a selected surface area of the biological membrane

4

so that the pyrotechnic element

30

is fixed in relation to the biological membrane

4

. Fixing the pyrotechnic element

30

in relation to the surface of the biological membrane

4

allows for the controlled formation of artificial openings

2

having a shape within a predetermined range of both diameter and depth. To facilitate attachment of the device, a portion of the lower surface

24

of substrate

20

may have adhesive

25

attached thereto to facilitate attachment of the substrate

20

to the selected surface area of the biological membrane

4

and the energy transfer at this interface.

The substrate

20

of the device

10

is preferably formed from a non-conductive material. The substrate

20

may also preferably be chosen from material that chemically reacts and/or outgases in response to the thermal energy produced in the micro-explosion of the pyrotechnic element

30

to produce enhancer substances, such as ammonia, or other beneficial byproducts. Any suitably substrate-forming material may be used. Suitably materials include, for example, but are not limited to, natural and synthetic polymers and gels, paraffin, waxes, hydrogels, sol-gels, glass, fabric, ceramic or paper layers. Additionally, appropriate substrates

20

may include but are not limited to low-melting point polymers and polymers impregnated, coated or microencapsulated with enhancers. The substrate

20

may be designed to contain pigments to effect an instantaneous tattoo application upon detonation of the pyrotechnic charges suitable for veterinary or cosmetic tattoos.

The substrate

20

preferably has a thickness of approximately 10 microns to 1000 microns. More particularly, it is preferred that the substrate

20

has a thickness of approximately 10 to 500 microns. In the embodiment where the pyrotechnic element is disposed within a hole fabricated in the substrate

20

layer, the thickness of the substrate

20

may be used during the manufacturing process to control the amount of explosive material placed at each site, the shape of the resulting pressure front created when the charge is detonated, and the resulting geometries of the formed pore.

The trigger device

40

may be any means known to one skilled in the art for activating a pyrotechnic element

30

. These means include, but are not limited to, electrical triggers, percussive triggers, thermal triggers, optical triggers and the like. The only requirement for a suitable trigger device

40

for the present invention is the requirement that the trigger device

40

conduct a trigger signal

42

to the pyrotechnic element

30

capable of triggering the detonation of the pyrotechnic element

30

. The preferred trigger device

40

is an electrically conductive element

44

disposed in contact with the pyrotechnic element

30

which can conduct an electrical detonation signal

46

to the pyrotechnic element

30

. The source of the electrical detonation signal

46

may be any local or remote pulse source.

An example of an optical trigger is a laser beam emitted from a laser source, such as a laser diode. For example, pyrotechnic ink is screen printed in dots on a clear plastic film substrate. In use, the substrate is placed against the surface of the biological membrane with the ink dots facing the membrane. Detonation of the pyrotechnic ink is triggered by illuminating the dots with a laser beam through the clear plastic film substrate. Sufficient heat is achieved with a laser pulse of sufficient laser beam power and wavelength. Alternatively, the pyrotechnic ink is integrated with a photothermal material or dye that absorbs the laser beam energy to heat up and trigger detonation even faster. A laser beam trigger has an advantage of requiring no electrical connections to the pyrotechnic elements.

The same conductive elements

44

can also be used after the artificial opening formation process as electrodes for additional permeation enhancement techniques such as iontophoresis and/or electroporation, or even as the connections to a piezo-element placed within the device to provide a sonic energy source. A more detailed description of how all of these different enhancement techniques can be coupled with a pore formed in the skin is provided in the pending international patent application PCT W098/29134, “Microporation of Tissue for the Delivery of Bioactive Agents.” Similarly, the conductive elements that connect to the pyrotechnic elements are also useful, after the artificial openings are formed, as electrodes as part of a sensor, such as an electrochemical bio-sensor, for detecting an analyte in the biological fluid being collected from the artificial openings. Suitable materials for the conductive elements for use both as triggering elements and electrodes for electrochemical detection are platinum, platinum/carbon and carbon.

While the electrically conductive element

44

may be disposed on either the upper or the lower surface

22

,

24

of the substrate, the electrically conductive element

44

of the present invention is preferably disposed on the upper surface

22

of the substrate

20

. This advantageously results in the electrically conductive element

44

being separated from the surface of the biological membrane

4

by the interposing substrate

20

. This prevents the electrically conductive element

44

from contacting the surface of the biological membrane and resultantly being adversely affected by the undesirable effects of bodily fluids, such as sweat, body oil, and the like, which are present on the surface of most biological membranes

4

.

Referring now to

FIGS. 2 and 3

, a conductive element

44

, such as a carbon trace, is applied to the upper surface

22

of the substrate

20

using techniques known to one skilled in the art. A pyrotechnic element

30

is then deposed on the conductive element

44

to complete the necessary connection of the pyrotechnic element

30

and the conductive element

44

. This step may be performed by disposing, such as by screening, a measure of pyrotechnic ink on the conductive element

44

. When the pyrotechnic ink cures, the pyrotechnic element

30

is in operative contact with the trigger device

40

. Because the substrate

20

is interposed between the surface of the biological membrane

4

and the pyrotechnic element

30

in this embodiment, it is preferred that the substrate

20

used for this embodiment be of a type that is readily volatized under the forces of the micro-explosion of the pyrotechnic element

30

so that sufficient energy is directed to the biological membrane

4

to form the desired artificial opening

2

. A artificial opening

2

formed using a device

10

of this embodiment would have the general shape shown in

FIG. 4

after the micro-explosion had occurred (assuming that the pyrotechnic element had a generally round cross-sectional shape). Enhancers may be preferably incorporated into the substrate

20

to enhance the resulting transdermal flux rate.

Referring now to

FIGS. 5-7

, devices according to second embodiment and third embodiments of the present invention are shown. In both embodiments, the substrate

20

has at least one aperture

26

extending through the substrate

20

. This aperture

26

has an aperture wall

28

of a predetermined shape so that a desired-shaped artificial opening

2

may be formed. As one skilled in the art will appreciate, by changing the shaped of the aperture wall, the form of the micropore may be altered. For example, a star shaped aperture wall of the aperture may be used to form a star shaped micropore. In a further example, a slot shaped aperture wall may be used to form a slot shaped micropore. Pores of a particular shape may have cosmetically preferable properties while still facilitating the desired transdermal flux rates. Preferably however, the aperture wall of the aperture has a square or round cross-sectional shape. These shapes allow for the ready determination, using calculations know to one skilled in the art, of the resulting depth and diameter of the formed micropore based upon the distance the pyrotechnic element is spaced from the biological surface and the known explosive power of the pyrotechnic element.

The conductive element

44

, which is exemplified by a carbon trace, is preferably applied to the upper surface

22

of the substrate

20

so that it is in contact with an aperture

26

of the substrate

20

. A pyrotechnic element

30

, preferably initially in the form of a pyrotechnic ink, is then deposed on each aperture

26

therein in contact with the conductive element

44

to complete the necessary connection of the pyrotechnic element

30

and the conductive element

44

of the trigger device

40

.

The primary difference between the second embodiment and third embodiment of the present invention is the disposition of the pyrotechnic element

30

within the aperture

26

in relation to the surface of the biological membrane

4

. In the second embodiment shown in

FIG. 6

, the pyrotechnic element

30

may substantially fill the aperture

26

of the substrate

20

so that the pyrotechnic element

30

is in close physical contact with the surface of the biological membrane

4

. In the third embodiment, as best shown in

FIG. 7

, the pyrotechnic element

30

extends only partially down inside the aperture

26

of the substrate

20

from the upper surface

22

so that the bottom surface

32

of the pyrotechnic element

30

is spaced a distance (d) from the lower surface

24

of the substrate

20

so that the aperture

26

is only partially filled.

If the pyrotechnic element

30

of the device

10

is in close physical contact with the selected surface area of the biological membrane

4

, as is shown in

FIGS. 5 and 6

, the explosive force is directed to the general surface of the biological membrane

4

on which the pyrotechnic element

30

is in contact. The resultant micropore

4

formed from the micro-explosion of the pyrotechnic element

30

is similar to that shown in FIG.

4

. This embodiment is efficient in that no portion of the force is wasted in volatilizing the substrate

20

. The temperature, pressure, and velocity of materials produced by the pyrotechnic element

30

and the resultant depth and diameter of the formed artificial opening

2

is dependent in this embodiment upon the nature (i.e., the physical properties and efficiency of the explosive pyrotechnic element

30

used per unit weight) of the pyrotechnic element and the quantity of pyrotechnic element

30

used.

Preferably however, and as shown in

FIG. 7

, the bottom surface of the pyrotechnic element

30

is spaced from the lower surface

24

of the substrate

20

. In this embodiment, it is preferred that pyrotechnic ink be used for the formation of the pyrotechnic element

30

so that a ready-formed shaped charged surface

34

is formed on the bottom surface

32

of the pyrotechnic element

30

when the pyrotechnic ink cures into the pyrotechnic element

30

. Due to surface tension acting on pyrotechnic ink when the ink cures from the fluid state, the bottom surface

32

of the pyrotechnic element

30

will arch toward the upper surface

22

of the substrate

20

and will have a generally parabolic shape in cross-section. This shaped charged surface

34

may be made by mechanical means after the pyrotechnic element

30

is disposed on and into the aperture

26

, but the use of surface tension acting on the pyrotechnic ink as it cures is the preferred means for forming a generally parabolic shaped charged surface

34

of the third embodiment of the present invention. When the pyrotechnic element

30

is detonated, the general parabolic shaped charge surface

34

causes the generation of high temperature, high pressure, and high velocity materials at the focus (F) of the shaped charge explosion. Spacing the pyrotechnic element

30

from the lower surface

24

of the substrate

20

, which in operation is coincident with the surface of the biological membrane

4

, allows the focus of the micro-explosion to be directed to the depth D desired within the biological membrane

4

. As shown in

FIG. 8

, this results in an artificial opening

2

extending therethrough the biological membrane

4

. Additionally, because the location of the focus of the shape charged surface

34

may be readily calculated from standard equations that consider the shape of the parabolic surface, the artificial opening

2

may be advantageously formed without damaging the underlying tissues, such as the epidermis of the skin when the stratum corneum of the skin is microporated.

As noted above the pyrotechnic element

30

is shaped to form a micropore of specified shape, diameter, and depth. The shape of the formed micropore of the present invention is preferably cone shaped as shown in

FIGS. 4 and 8

. The formed micropores preferably have a diameter in the range of 1-1000 μm and a depth in the range of 1-3000 μm. More particularly, the micropores preferably have a diameter in the range of 10-600 μm and a depth in the range of 10-1000 μm.

FIGS. 9 and 10

illustrate that the electrically conductive elements

44

are arranged in a network

46

. Specifically, the conductive elements

44

are connected to the respective apertures

26

are linked together in a conductive network

46

so that the plurality of pyrotechnic elements

30

disposed into the plurality of apertures

26

within the substrate

20

of the device

10

may be simultaneously or sequentially detonated upon receipt of the electrical detonation signal(s)

46

applied across the electrodes to the network

46

. For a sequential detonation, it may be desirable to isolate some circuits within the conductive network

46

and trigger the detonation sequence in a predetermined fashion programmed into the trigger device

40

. Alternatively, as described above, using slightly different length small traces of fuse material to connect each detonator to one or more pyrotechnic elements could be used to create a preset sequential detonation.

For an array of pyrotechnic elements disposed on a device, as shown in

FIG. 11

, it is also possible to use a conductive element

44

exemplified by the conductive carbon trace described herein to first detonate a single pyrotechnic element

30

and then by having placed within the array of pyrotechnic elements

30

a series of small traces

45

of a selected pyrotechnic substance which interconnects them, allow this first pyrotechnic element

30

detonation to initiate the subsequent detonation of all of the other elements

30

. This design simplifies the manufacture of the electrically activated trigger device

40

and can potentially result in a lower cost product.

The device

10

of the present invention may also be combined with permeants, chemical enhancers (E), therapeutic drugs (TD), or any combination of chemicals. Referring to

FIG. 12

, chemical enhancers E, therapeutic drugs TD, and/or other desired chemicals may be advantageously combined with the pyrotechnic element

30

. This allows the added chemical or compound to be forcefully introduced into the artificial opening

2

by the energy supplied by the detonation of the pyrotechnic element

30

. For example, the substrate

20

may be fabricated from powder of biodegradable polymer micro-particles which contain a permeant, e.g., a therapeutic compound such as a vaccine antigen, DNA, or protein. Upon detonation of the pyrotechnic element

30

, the bonds between the individual micro-particles forming the substrate

20

are broken and are subsequently driven at high velocity into the walls of the artificial opening

2

being formed. Some of these particles will penetrate through cell walls and come to rest within the interior of an intact and still viable cell. This momentary disruption of the cell wall by the shock wave and the kinetic impact of the particle have been shown to be an effective method for delivering macro-molecules and micro-particles.

Referring now to

FIG. 13

, an alternative embodiment of the device

10

of the present invention is shown. The device shown in

FIG. 13

comprises a thin walled membrane

50

attached to the lower surface

24

of the substrate

20

. As one skilled in the art will appreciate, a reservoir

52

is defined by the shaped charged surface

34

of portion of the pyrotechnic element

30

extending within the aperture

26

, the aperture walls

28

of the aperture

26

, and the thin walled membrane

50

. The reservoir

52

may contain chemical enhancers (E), therapeutic drugs (TD), or other beneficial substances. This reservoir

52

is explosively breached by the energy supplied by the detonation of the pyrotechnic element

30

which resultantly causes the stored substance to be forcefully delivered into the organism past the biological membrane

4

via the formed artificial opening

2

.

Referring now to

FIG. 14

, a cover film

60

overlays the top surface of the device of the present invention, covering at least the pyrotechnic element

30

and optionally the trigger device

40

. This cover film

60

helps to contain and focus the force of the micro-explosion of the pyrotechnic element

30

such that the heat and pressure generated by the micro-explosion is directed at the targeted tissue and is not vented to the surrounding atmosphere. Additionally, by containing the micro-explosion, the cover film

60

acts as a safety feature as any material that would be potentially ejected by the force of the micro-explosion would be contained. The cover film

60

is preferably formed from thermally non-conductive, high-melting point material, such as a suitable polymer, ceramic, metal and the like.

The aperture

26

in the configuration of

FIG. 14

is optional. For example, the substrate

20

is a matrix patch-like member that has indent areas on its upper surface, but otherwise is a contiguous element (without the aperture

26

as shown in FIG.

14

). The substance for the pyrotechnic elements is screen printed on the substrate

20

into the indented areas. The detonation electrode material for the trigger device is applied to the surface above the pyrotechnic elements as shown in FIG.

14

. The cover film is then applied to the top surface of the device over the detonation electrode material of the trigger device. Consequently, the substrate

20

includes a region between the pyrotechnic elements

30

and the surface of the biological membrane that acts as a spacer. When the pyrotechnic elements are detonated, a shock wave is created through the substrate

20

forming the artificial opening(s). In addition, the substrate

20

is optionally treated with one or more enhancers or permeants, etc., so that upon detonation, the treated substrate matrix material is driven into the biological membrane with the micro-explosion.

In use, the device

10

of the present invention forms artificial openings

2

into a selected area of a biological membrane

4

for enhancing the permeability of the biological membrane

4

. The operator simply connects the lower surface

24

of the substrate

20

of the device

24

on the surface of a biological membrane

4

and then triggers the trigger device

40

of the device

10

. Triggering of the pyrotechnic element

30

(of sufficient energy to penetrate the biological membrane to a desired depth) causes an artificial opening

2

to form that extends into or through the biological membrane

4

.

A permeant, such as a therapeutic drug, may be applied to the formed artificial opening

2

for delivery of the therapeutic drug or compound from without the biological membrane

4

into the organism. In still another use for the formed artificial opening

2

, fluids or analytes may be withdrawn from the organism via the artificial opening

2

. In the absence of the barrier function normally attributable to the biological membrane

4

, such as the stratum corneum of the skin, the percutaneous transport of the therapeutic drug or the analytes is enhanced.

As shown in

FIG. 15

, a separate reservoir may be integrated into the device

10

for delivering the permeant to the formed micropore. A first film layer

70

is disposed on the upper surface

22

of the substrate

20

, and preferably over the pyrotechnic element

30

and the trigger element

44

. A second film layer

72

is secured to peripheral portions of the first film layer

70

to define a reservoir cavity

74

that contains one or more permeants. The reservoir cavity

74

, and more particularly the first film layer

72

, may be breached simultaneously with the pore forming detonation of the pyrotechnic element

30

.

Alternatively, as shown in

FIG. 16

, the first film layer

70

may be kept intact during the detonation of the pyrotechnic element

30

, and then opened up at a later time by either the detonation of a separate pyrotechnic element

75

placed on the first film layer

70

, or the activation of an optically or electrically heated element disposed on the first film layer

70

as disclosed in commonly assigned U.S. Pat. No. 5,885,211.

For some applications a plurality of separately addressable reservoirs

74

may be used to allow for the sequential administration of several different permeants which otherwise may not be compatible to be placed in the same formulation together. In this case it can be advantageous to isolate each permeant to a selected artificial opening

2

or set of artificial openings

2

thereby insuring that no mixing of the incompatible permeants occurs outside of the organism's body. One example of where this is useful is when a dilute ammonia (NH

3

) based permeation enhancer is being used to permealize the capillary walls for the delivery of a labile protein or peptide such as erythropoietin or parathyroid hormone. In this case the value of using the NH

3

compound has been shown dramatically in clinical studies, however the highly alkaline properties of the NH

3

are known to be detrimental to the integrity of the therapeutic permeant. By isolating each of these substances in separate reservoir cavities

74

, and then using separate pores to introduce them into the organism, the NH

3

enhancer can be given enough time to diffuse down to the capillary bed, perform its permealization function, and then be effectively neutralized by the huge buffering capacity of the organism's internal fluids. Then, with the pH in the tissue essentially back to normal, the therapeutic permeant can be introduced into a set of proximally adjacent pores

2

which allow diffusion to the very same capillaries permealized by the NH

3

. Various patterns can be used, for example a single pore

2

to deliver the NH

3

can be surrounded by a circle of pores

2

delivering the therapeutic permeant. Similarly, alternating rows of pores

2

could be used, or any pattern designed to deliver the appropriately effective amounts of the respective permeants which can be expected to vary from one application to the next.

The manufacture of this separate reservoir technology can be achieved using common die-stamping, printing, lithographic, and heat-bonding techniques. For example, the substrate

20

could first have the pyrotechnic elements

30

and the trigger device

40

placed on the upper surface of the substrate

20

via screen-printed or inkjet printing technologies. As described above, an enhancer may be combined with the pyrotechnic element

30

. Here, the NH

3

enhancer, exemplified by a solid form of ammonium carbonate, is deposited directly on those pyrotechnic elements

30

designated to deliver the NH

3

into the organism. The first film layer

70

is then placed over the entire assembly and thermally bonded with an indexed thermal die to form isolated pockets around the NH

3

active portions. This first film layer

70

is designed to withstand the detonation of the pyrotechnic elements

30

without rupturing in the areas of the NH

3

compound. When the pyrotechnic elements

30

that are combined with ammonium carbonate are detonated, the heat of the micro-explosion causes the ammonium carbonate to break down into NH

3

and H

2

O and delivers the enhancer into the walls of the pore

2

formed very efficiently. The second film layer

72

is then deposed on the first film layer to form at least one reservoir cavity

74

containing the desired therapeutic permeant. The initial pyrotechnic element

30

detonation may allow the rupture of this reservoir cavity

74

, or alternatively, separate thermal or PE detonations can be used to form openings in this reservoir cavity

74

to allow the stored therapeutic permeant access to the pores

2

formed beneath it in the organism.

Similarly, separately assessable reservoir cavities

74

, which can be sequentially opened, are useful to tailor the pharmacokinetics of a permeant to the desired values over time. For example, the device

10

could be set up to be responsive to the measurement of some analyte withdrawn from one or more artificial openings

2

, such as glucose, and when indicated, to open up a reservoir cavity

74

containing insulin to deliver a preset unit dosage of insulin in a closed loop fashion. Another application could be the periodic administration of flux enhancers designed to facilitate the extraction of fluids or analytes over extended periods of time, where each new dose of the enhancer would be tailored to act for some predetermined duration, allowing a long term monitoring system to utilize the same artificial opening, while still getting the benefits of an enhancer technology which in itself may be relatively short acting.

FIG. 17

illustrates still another embodiment of the invention wherein the angular position of the pyrotechnic element is controlled to affect the shape of the artificial opening so formed. As explained above, positioning the pyrotechnic element at some specified distance from the surface of the biological membrane may be used advantageously as one way of controlling the amount of energy presented to the surface of the biological membrane. In the case where a shaped charge pyrotechnic element is utilized, this spacing may be selected to place the focal point of the peak pressure precisely where desired in reference to the surface of the biological membrane.

Similarly, angular positioning of the shaped charge pyrotechnic element to the surface of the biological membrane can be used to control the shape of the pore formed and the amount of energy coupled into the targeted and adjacent tissues.

FIG. 17

shows a narrowly focused shaped charge pyrotechnic element

500

positioned in a cavity or channel

504

of a substrate member

502

at an angular position with respect to a lower surface of the substrate member

502

, and consequently of the surface of the biological membrane. The trigger or detonator element

540

detonates the pyrotechnic element

500

, so that the direction of the focused pressure wave is brought to the surface of the biological membrane at a shallow angle

510

. This configuration will produce a trench-like opening

520

, literally blowing the targeted tissue away while coupling very little energy into the adjacent tissues. An escape port or channel

530

is also optionally provided to assist in the removal of the waste gases and tissue fragments. The shape of the channel

504

in which the pyrotechnic element

500

resides and the shape of the escape channel

530

also contribute to forming a desired pressure focal points and assist in the extraction process of the material. These same channels can also be used to either extract a fluid from or deliver a permeant into the organism.

It should be understood the device comprising one or more pyrotechnic elements may also include structures to collect biological fluid and manage its movement to a sensor that is responsive to one or more analytes.

Although the present invention has been described with reference to specific details of certain embodiments thereof, it is not intended that such details should be regarded as limitations upon the scope of the invention except as and to the extent they are included in the accompanying claims.

Number	Name	Date	Kind
5224928	Sibalis et al.	Jul 1993	A
5380272	Gross	Jan 1995	A
5423803	Tankovich et al.	Jun 1995	A
5651768	Sibalis	Jul 1997	A
5713845	Tankovich	Feb 1998	A
5722397	Eppstein	Mar 1998	A
5752949	Tankovich et al.	May 1998	A
5817089	Tankovich et al.	Oct 1998	A
5885211	Eppstein et al.	Mar 1999	A
5925035	Tankovich	Jul 1999	A
6022316	Eppstein et al.	Feb 2000	A
6056738	Marchitto et al.	May 2000	A
6173202	Eppstein	Jan 2001	B1

Number	Date	Country
WO 9641657	Dec 1996	WO
WO 9707734	Mar 1997	WO
WO 9800193	Jan 1998	WO
WO 9822719	May 1998	WO
WO 9829134	Jul 1998	WO
WO 9929364	Jun 1999	WO
WO 9944507	Sep 1999	WO
WO 9944508	Sep 1999	WO
WO 9944637	Sep 1999	WO
WO 9944638	Sep 1999	WO
WO 9944678	Sep 1999	WO
WO 0003758	Jan 2000	WO
WO 0027473	May 2000	WO

	Number	Date	Country
	60/092731	Jul 1998	US
	60/138050	Jun 1999	US

Controlled removal of biological membrane by pyrotechnic charge for transmembrane transport

Information

Patent Number

Date Filed

Date Issued

Inventors

Original Assignees

Examiners

Agents

CPC

US Classifications

Field of Search

US

International Classifications

Abstract

Description

Claims

Parent Case Info

US Referenced Citations (13)

Foreign Referenced Citations (13)

Provisional Applications (2)