Methods for iontophoretic delivery of antiviral agents

Description

BACKGROUND OF THE INVENTION

1. Field of the Invention

This invention relates generally to the transdermal electrokinetic mass transfer of medication into a diseased tissue, and, more specifically, to a portable apparatus for the iontophoretic delivery of medication across the skin and incorporation of the medication into diseased tissues and blood vessels adjacent to the delivery site. The apparatus provides a new method for treating and managing diseases presenting cutanoeus lesions.

2. Prior Art

Iontophoresis has been employed for several centuries as a means for applying medication locally through a patient's skin and for delivering medicaments to the eyes and ears. The application of an electric field to the skin is known to greatly enhance the skin's permeability to various ionic agents. The use of iontophoretic transdermal delivery techniques has obviated the need for hypodermic injection for many medicaments, thereby eliminating the concomitant problems of trauma, pain and risk of infection to the patient.

Iontophoresis involves the application of an electromotive force to drive or repel oppositely charged ions through the dermal layers into a target tissue. Particularly suitable target tissue include tissues adjacent to the delivery site for localized treatment or tissues remote therefrom in which case the medicament enters into the circulatory system and is transported to a tissue by the blood. Positively charged ions are driven into the skin at an anode while negatively charged ions are driven into the skin at a cathode. Studies have shown increased skin penetration of drugs at anodic or cathodic electrodes regardless of the predominant molecular ionic charge on the drug. This effect is medicated by polarization and osmotic effects.

Regardless of the charge of the medicament to be administered, a iontophoretic delivery device employs two electrodes (an anode and a cathode) in conjunction with the patient's skin to form a closed circuit between one of the electrodes (referred to herein alternatively as a “working” or “application” or “applicator” electrode) which is positioned at the delivered site of drug delivery and a passive or “grounding” electrode affixed to a second site on the skin to enhance the rate of penetration of the medicament into the skin adjacent to the applicator electrode.

Recent interest in the use of iontophoresis for delivering drugs through a patient's skin to a desired treatment site has stimulated a redesign of many of such drugs with concomitant increased efficacy of the drugs when delivered transdermally. As iontophoretic delivery of medicaments become more widely used, the opportunity for a consumer/patient to iontophoretically administer a transdermal dosage of medicaments simply and safely at non-medical or non-professional facilities would be desirable and practical. Similarly, when a consumer/patient travels, it would be desirable to have a personal, easily transportable apparatus available which is operable for the iontophoretic transdermal delivery of a medication packaged in a single dosage applicator. The present invention provides a portable iontophoretic medicament delivery apparatus and a unit-dosage medicament-containing applicator electrode which is disposable and adapted for use with the apparatus for self-administering medicament.

SUMMARY OF THE INVENTION

The present invention discloses a portable iontophoretic transdermal or transmucoscal medicament delivery apparatus and a unit dosage medicament applicator electrode adapted for use with the apparatus for the self-administration of a unit dose of a medicament into the skin. The apparatus is particularly suited for the localized treatment of herpes infections. Recurrent herpetic infections (fever blisters or herpes labialis) are very common and usually involve the mucocutaneous juncture. The established treatment for recurrent herpetic lesions (oral or genital) has been primarily supportive; including local topical application of anesthesia. Severe cases have been treated with systemic Acyclovir® (Zovirax Burroughs-Wellcome). Some cases the condition is managed with prophylactic long-term dosing administration with a suitable antiviral agent at great expense. Systemic treatment of acute herpetic flare-ups may reduce the normal 10-12 day course of cutaneous symptoms into a 6-8 day episode. Topical treatment of lesions with Acyclovir® has not been as effective as in vitro studies would suggest. A compound which is not presently available to clinicians but has demonstrated significant anti herpetic activity is 5-iodo-2 deoxyuridine (IUDR). Both of those agents have shown limited clinical efficacy when applied topically to the herpetic lesion. It is the present inventor's contention that the limited efficacy of topical administration previously observed is, at least in part, due to the poor skin penetration of these medicaments when applied topically. The present invention provides improved transdermal delivery of these medicaments and demonstrates improved clinical results in the case of Herpes.

Oral Herpes (most commonly Herpes simplex I infection) as well as genital Herpes (usually Herpes Simplex II infection) afflict many people, cause discomfort, shame, and may contribute to more severe and costly illnesses such as cervical cancer, prostate cancer, and perinatal blindness from herpetic conjunctivitis. The present invention discloses a portable, user-friendly transdermal delivery device and a method for using the device with Acyclovir® (or similar antiviral agent) to greatly benefit these afflicted patients. The present inventor has constructed embodiments of this device and conducted human clinical trials which clearly demonstrate improved therapeutic efficacy using iontophoretically administered antiviral agents when compared to unassisted topical application of the agent.

It is an object of the present invention to provide an iontophoretic medicament delivery apparatus which is portable and operable for self-administration of medicament into the skin of a person.

It is another object of the present invention to provide an improved iontophoretic transdermal drug delivery apparatus having a medicament-containing application electrode which disperses a single dosage and is disposable and non-reusable.

It is a feature of the present invention that the iontophoretic medicament delivery apparatus is easily maneuverable and operable when hand-held.

It is another feature of the present invention that the iontophoretic medicament delivery apparatus is battery powered and conveniently transported by a person.

It is a further feature of the present invention that the iontophoretic medicament delivery apparatus employs a tactile electrode which is in electrical contact with the skin of a user's hand when the apparatus is held in the user's hand, obviating the need for a separate grounding electrode connector or wire.

It is still another feature of the present invention that the iontophoretic medicament delivery apparatus is adapted to be operable with a disposable medicament containing applicator electrode which applicator electrode includes an absorbent, inert, non-corrosive portion containing a therapeutic agent.

It is yet another feature of the present invention to provide an embodiment of an iontophoretic transdermal delivery device wherein the disposable iontophoretic medicament-containing applicator electrode is adapted for releasable attachment to use with a hand-held base assembly housing a grounding electrode.

It is yet another feature of the present invention that the disposable iontophoretic medicament applicator electrode include indicator means operable for enabling a user to determine when the medicament within the removable applicator electrode has been released in delivery and/or depleted.

It is yet another feature of the present invention that the circuitry employed in the disposable iontophoretic medicament applicator include current limiting means operable for limiting the electrical current flowing between the surface of the applicator and the skin to less than about one milliampere per square centimeters of application electrode skin-contacting, surface.

It is another advantage of the present invention that the iontophoretic medicament delivery apparatus employs a disposable application electrode which conducts the electrical current to the tissue through the solution in which the medicament is dissolved.

It is still another advantage of the present invention that the improved disposable iontophoretic medicament applicator is inexpensive, safe to use, substantially unitary in construction and greatly increases the therapeutic efficacy of a medicament administered thereby.

The apparatus in accordance with the present invention provides a means for topically administering medicament directly and with, high efficiency into a diseased tissue thereby providing a novel method for treating clinical conditions presenting mucocutaneous symptoms and particularly mucocutaneous Herpes Simplex viral eruptions and sequelle associated therewith.

In one embodiment the electrode comprises a unitary flexible strip (such as SILASTIC®- by Dow Corning) having perforations dimensioned to accommodate a medicament placed therein. The perforations or “cells” can be made to store and dispense gels, ointments, fluids and other medicament vehicles without requiring the reformulation of the either the medicament or the vehicle.

The above objects, features and advantages of the invention are realized by the improved monopolar iontophoretic, medicament applicator which is easily transportable. The applicator employs a detachable medicament containing application electrode. The objects, features and advantages of the invention will become apparent upon consideration of the following detailed disclosure of the invention, especially when it is taken in conjunction with the accompanying drawings wherein:

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1

is a side elevational plan view of the iontophoretic medicament delivery apparatus showing the circumferential tactile ground electrode on the outer surface of the base housing and a disposable iontophoretic application electrode;

FIG. 2

is a side elevational view of the disposable non-reusable iontophoretic application electrode with a portion broken away to view the medicament dose packet;

FIG. 3

is a top view of a medicament dispensing electrode adapted for use with an iontophoresis handpiece.

FIG. 4

is a side elevational exploded view of the medicament dispensing electrode of FIG.

3

.

FIG. 5

is a perspective view illustrating the medicament dispensing electrode of

FIG. 3 and 4

attached to an iontophoresis handpiece in preparation for use.

FIG. 6

is a perspective view illustrating a patient preparing to self-administer medicament to lesions adjacent to the mouth employing the iontophoretic electrode/handpiece delivery system in accordance with the present invention.

DESCRIPTION OF THE PREFERRED EMBODIMENT

FIG. 1

shows, in side elevation, a preferred embodiment of the hand-held iontophoretic transdermal medicament delivery apparatus of the present invention. The apparatus, indicated generally by the numeral

10

, has an elongate base assembly

11

the major portion of which is preferably formed of plastic and shaped to conform to and comfortably fit with a user hand. An applicator electrode module

12

, containing a unit dose of medicament

23

, is releasably attached to a applicator electrode receptacle

14

on the distal end of the base assembly

11

. The application electrode

12

is preferably a “clip-on” type of electrode similar in configuration to an electrocardiogram electrode. In the drawing presented in

FIGS. 1 and 2

, electrically conductive elements such as wires and busses are presented as heavy lines. A wire

16

provides electrical connection between the applicator electrode receptacle

14

and wire

1

within the neck

15

of the base assembly

11

. Connecting wire

18

, in turn, provides electrical connection between the wire

16

and the current driver unit

19

housed within the base assembly

11

. A conductive tactile electrode

20

forms a portion of the exterior skin-contacting surface of the base assembly

11

preferably circumferentially enclosing a portion of the base housing or it may be interrupted or discontinuous on the outer surface. The tactile electrode

20

is in electrical communication with the cathode

24

C of battery

24

by means of a buss

17

and conductive urging spring

25

which secures the battery in position within the base assembly

11

. For the self-administration of medicament a user must have, skin contact with the tactile electrode

20

for the unit to operate. Current driver

19

underlies the cathodic (ground) tactile electrode

20

and is electrically connected via wire

21

to a voltage multiplier

22

. The voltage multiplier

22

receives low voltage power from the anode

24

a of the battery power source

24

and increases the available voltage for presentation to the application electrode

12

. The battery

24

is preferably a size AA or AAA. Battery

24

is held in place by an electrically conductive biasing spring

25

and ensures that electrical power is available at the application electrode

12

when the user grasps and holds the base housing

11

of the apparatus

10

thereby touching the cathodic tactile electrode

20

. The application electrode

12

and the tactile electrode

20

thus form a closed circuit in series with the user's skin.

When current flows across the user's skin to the application electrode in response to an applied voltage the current promotes and hastens the penetration of the medicament

23

contained in a reservoir

26

within the working electrode

12

into the skin. The polarity of the working electrode

12

is preferably unidirectional to promote the above described penetration without requiring a separate grounding electrode. The working application electrode

12

will be described in greater detail below.

The base assembly

11

of apparatus

10

serves as a housing to the aforesaid components as a handle. The portion of the base assembly

11

exclusive of the tactile electrode, is preferably made of a plastic such as polyethylene, acrylonitrile, butadiene, styrene or similar durable plastic. The battery portion

24

is connected to a voltage multiplier

22

which steps up the voltage supplied by the battery

24

and applies the stepped up voltage to the current driver

19

. Current driver

19

presents a defined current and voltage output at the application electrode

12

the value of the current, which may be empirically determined being sufficient to drive the medicament through the porous, open-celled material

27

(

FIG. 2

) within the application electrode interposed between the skin contacting surface

13

and reservoir

26

containing the unit dose medicament and penetrate the patient's skin. The circuitry limits the maximum current available to the application electrode to preferably to less than about one milliampere per two square centimeters of the skin-contacting surface area

13

of the application electrode

12

. However, depending upon working electrode's

12

skin-contacting surface

13

configuration, the current level can vary from about 0.1 to about 1.2 milliamps. Currents ranging between 0.1 ma to 5 ma have been used clinically by the present inventor, but the higher currents caused the user minor discomfort and, with chronic use over time, may produce untoward effects.

FIG. 2

shows a preferred embodiment of the iontophoretic medicament-containing application electrode

12

. The application electrode

12

is preferably disposable and non-reusable and is suitable, for example, for transdermally delivering antiviral agents such as Acyclovir® for the treatment of cold sores or genital herpes. The size of the skin-contacting surface

13

or application electrode

12

may vary to accommodate specific clinical applications. The application electrode

12

is detachably housed within a recess within the receptacle

14

which recess presents an electrically conductive interior surface to complete the electrical flow path from the connecting wires

18

and

16

to a conductive element

29

within the application electrode. The electrical current from the current driver

19

is conducted through conductive inner surface of the application electrode receptacle

14

to the electrically conductive element

29

within the applicator electrode which element

29

is in electrical contact with the inner surface of the receptacle in contact therewith to drive the medicament

23

or treatment agent through the open-celled sponge-like matrix material

27

and through the user's skin (not shown). The medicament or treatment agent

23

is contained within a rupturable polymer reservoir

26

until dispensed during treatment. A slight exertion of pressure or squeezing of the reservoir

26

against reservoir puncture means

28

releases the medicament or treatment agent into an open-celled sponge-like material

27

within the application electrode for iontophoretic delivery into the patient's skin. Medicament

23

release can occur at the time of application or upon peruse compression of the electrode

12

. Application electrode

12

can be advantageously designed to include a stripping portion adapted to that upon removal of the application electrode

12

from the electrode receptacle

14

a protruding stripping portion (not shown) scrapingly strips the conductive coating from the conductive support arm

29

to prevent reuse of the disposable electrode

12

. Application electrode

12

in intentionally packaged with a single dose packet or reservoir

26

of treatment agent or medicament

23

. In addition to the medicament, the reservoir

26

can include a coloring agent, such as iodine, which turns dark blue upon contact with starch in the open-celled material to visibly indicate that the unit dose encapsulation has been used. Other suitable coloring agents can include pH indicators, wet saturation indicators or oxidizable pigments.

The open-celled sponge-like material

27

surrounding reservoir

26

should be inert to the medicament or treatment agent being employed, as well as being non-corrosive and stable when in contact with the treatment agent. Suitable materials include plastic pads, such as polyethylene, paper or cotton, porous ceramics, open-celled porous polytetrafluoroethylene, polyuethane and other inert plastics, and open-celled silicone rubber, such as may be employed with vertically aligned medicament-containing tubes. A typical medicament that can be contained within the rupturable polymer reservoir

26

is xylocaine or similar topical anesthetic.

The disposable electrode

12

possesses the advantages of preventing leaching or migration of the medicament from within the rupturable polymer reservoir, no attendant loss of efficacy, a long shelf life and little or no electrode corrosion. A suitable electrical control circuit for use in the iontophoretic medicament delivery apparatus

12

is shown in U.S. patent application Ser. No. 07/579,799, filed Sep. 10, 1990, now U.S. Pat. No. 5,160,316 and hereby specifically incorporated by reference herein in pertinent part.

FIG. 3

shows a particularly preferred embodiment of a disposable, one-time use electrode

30

for use with the iontophoresis handpiece

10

of the present invention.

FIG. 3

is a top view of the disposable electrode

30

with the upper release film

41

(

FIG. 4

) removed. A non-conductive substrate

31

is formed into a flat strip having a central portion A and two end portions B. The end portions B each have a cut-out therein containing an electrically conductive gel

32

. The gel

32

may be imbedded within a mesh or it may be constrained within the cut out by means of a porous, non-wicking and non-electrically conducing containment layer

34

and

35

much as tea is contained within a porous tea bag. The central portion A of the strip

31

has a medicament-containing reservoir

33

therewithin. The medicament-containing reservoir

33

may comprise a suitable medicament embedded within the mesh of a pharmacologically inert material. The medicament-containing reservoir

33

is positioned between die cuts

36

in the non-conductive substrate

31

which die cuts provide means for facilitating the predictable bending the electrode strip

30

to matingly conform to the shape of the exterior surface of an iontophoresis handpiece

10

(

FIG. 1

) Magnets

43

and

43

′ (shown in phantom in

FIG. 3

) disposed laterally to the central portion A provide means for magnetically activating a handpiece when the electrode is in position.

An exploded side view of the electrode

30

is shown in FIG.

4

. The conductive gel

32

filling the cut-outs may be contained within a mesh or may be contained within the cut-out by means of porous, non-wicking layers

34

and

35

. Similarly, the medicament-containing cut-out

33

may comprise the medicament embedded within a mesh, a gel, or similar substrate which releases the medicament in response to an electrical communication therewith. The upper containment layer

34

and the lower containment layer

35

serve to restrain the conductive gel within the medicament reservoir

33

to their respective cut-outs. An upper release film

41

is used to protect the adhesive surface (not shown) on the uppermost surface of the containment layer

34

. A lower release film

42

serves a similar function to protect the adhesive surface of the lower medicament containment layer

35

. The cut-outs

36

are shown to penetrate the strip of non-conductive material

31

adjacent to the medicament-containing reservoir

33

. It is particularly desirable to provide one or more activating magnetic bodies

43

and

43

′ within the strip

31

in order to properly position the electrode strip

30

and activate the handpiece

10

. Since it is anticipated that the handpiece/electrode assembly of the present invention will most likely be used in the bathroom, it is particularly desirable to hermetically seal the handpiece's internal operational mechanisms. The on/off switch within the handpiece can be in the form of a magnetically responsive switch which is turned “on” and “off” in response to the position of the electrode.

Turning now to

FIG. 5

, we see a disposable electrode

30

in the process of being applied to the terminal end of an iontophoresis handpiece

10

. The electrode

30

is applied to the active terminal

16

of the handpiece in such a manner that the medicament-containing reservoir

33

overlies and is in electrical contact with the active terminal

16

of the handpiece

10

. The conductive gel layers

32

are positioned on the handpiece to overly the ground electrode on the handpiece

10

. The ground electrode is indicated at

20

in FIG.

5

.

An alternate but equally effective embodiment of

FIG. 4

electrode can be manufactured from a mold injected soft, inert material, non-conductive and non-porous (such as SILASTIC®- by Dow Corning) in the shape embodied in FIG.

3

. The unit will contain vertically aligned open cells for containing and acting as reservoir for therapeutic medicaments as well as a conductive gel (if necessary). Such an embodiment is less costly to produce and avoids the process of assembling numerous layers.

The iontophoresis handpiece and electrode assembly in accordance with the preferred embodiment shown in

FIGS. 3 and 4

is shown being used by a patient

60

in FIG.

6

. The patient

60

grasps the handpiece by means of placing a finger

61

on at least one of the conductive gel ground electrodes thereby grounding the patient's body. The active electrode driver

19

of the handpiece is in electrical communication with the medicament-containing reservoir

33

. The medicament-containing reservoir

33

, thus positioned and grasped by the patient, is advanced to come in contact with a lesion

63

on the patient's skin. Upon contact, electrical current flows between the active electrode

19

in the handpiece to the ground electrode(s)

32

via passage through the medicament-containing reservoir

33

comprising the active electrode. The polarity of the current may be reversed to accommodate the charge on the medicament. The flow of an electrical current facilitates entry of the medicament within the reservoir

33

into the skin overlying the lesion

63

thereby locally delivering the medicament to the exact area to be treated.

EXPERIMENTAL CLINICAL TRIALS

The inventor has conducted a clinical study using a prototype iontophoretic device in accordance with the present invention for the treatment of cold sores. The clinical response was promising. A second independent, qualified investigator, a board-certified Urologist, conducted a study using the present apparatus and method for treating male genital herpes lesions with encouraging results. Table 1 summarizes data (discussed below) supporting the claim to unexpected clinical benefits treating disease with this novel method. The method and medicament application device when used together for treating these common embarrassing, and previously not easily-treatable ailments provide surprising advantages.

The embodiment of the device shown in FIG.

1

and described hereinabove is a improvement over the prototype used in the clinical study, which was a larger unit, not user friendly, which required physically connecting wires to the patient's body which created anxiety, and could not be used without attending personnel. Notwithstanding design, the apparatus used in the clinical study summarized in Table 1 employed electronics similar to the apparatus described herein and was used to optimize the clinical performance of the embodiment

12

of the device described herein.

TABLE 1

STAGE TREATMENT RESULTS

RESPONSE

IUDR

ACYCLOVIR ®

TOTALS

No response

1

1

2

Some response

1

3

4

Major response

26

42

68

The study included a control situation wherein seven patients were found who had simultaneous concurrent herpes lesions at separate locations on their bodies. In each case one lesion was treated with iontophoretic application of antiviral agent (Acyclovir® of IUDR) and the other lesion was treated in the standard method employed in the prior art comprising repeated topical application of the same antiviral comprising repeated topical application of the same antiviral agent. The iontophoretically enhanced treated lesion received a single 10-15 minute treatment. All iontophoretically treated lesions demonstrated resolution in 24 hours and none of the unassisted topically treated lesions demonstrated a similar response. The results for the control group are summarized in Table 2.

TABLE 2

CONTROL GROUP RESULTS

No response

Some resp.

Major resp.

IUDR

Treated lesion

0

0

7

Control lesion

5

2

0

ACYCLOVIR ®

Treated lesion

0

0

1

Control lesion

1

0

0

The clinical studies included patient volunteers with fill informed consent who suffered from recurrent cold sores. The study demonstrated greatest treatment efficacy if the herpes lesion received iontophoretic treatment within 36 hours of lesion onset. The treatment incorporated an electrode saturated with Acyclovir® ointment (ZOVIRAX®) or IUDR (STOXIL®) Ophthalmic drops as supplied by the manufacturer. Thus mounted Anodic electrode of the prototype system was used for a 10-15 minute application directly to the lesion with the average current setting of 0.2 ma-0.6 ma which was well tolerated by all patients.

The lesion was evaluated in 24 hours. In 92% of the iontophoretically treated cases (>70 lesions treated) a major response was noted. A major response was categorized by resolution of pain in >6 hours and lesion crusted and healing within 24 hours. The normal course of cold sores involves an average period of 10-12 days before resolution and healing occurs. The present apparatus and clinical method for treatment of mucocutaneous Herpes Simplex (type I and Type II) eruptions presented herein have been described and performed with excellent results. This novel user friendly apparatus in combination with the disclosed clinical treatment method presents a very effective new treatment for Herpes Simplex eruptions.

While the invention has been described above with references to specific embodiments thereof, it is apparent that many changes, modifications and variations in the materials, arrangements of parts and steps can be made without departing from the inventive concept disclosed herein. For example an impregnated conductive gel can also be used to as medicament containing medium to increase the physical stability and the tissue adhering characteristics of the electrode. Accordingly, the spirit and broad scope of the appended claims is intended to embrace all such changes, modifications and variations that may occur to one of skill in the art upon a reading of the disclosure. All patent applications, patents and other publication cited herein are incorporated by reference in their entirety.

Claims

1. A disposable medicament dispensing applicator electrode forand an iontophoretic drugmedicament delivery device adapted for the self-administration of a medicament into a person's skin at a localized treatment site, said device comprising a base assembly having an active terminal adapted to receive and make electrical contact with a detachablesaid medicament dispensing applicator electrode, wherein said base assembly comprises: a case having an elongate, substantially cylindrical outer surface having a size and shape adapted to be comfortably grasped within a person's hand, and wherein at least a portion of said outer surface is aincluding tactile electrode formed of an electrically conductive material;, and a bipolar electrical power means having a first pole and a second pole;, said electrical power means being enclosed within said case and wherein said first pole isbeing in electrical communication with said tactile electrode; wherein said medicament dispensing applicator electrode comprises:including a module containing a unit dose of medicament, an electrically conductive working electrode and means thereon adapted for releasably attaching said applicator electrode to said device in electrical contact with said second pole of said electrical power means, wherein said applicator electrode further comprisescomprising an elongate strip constructed of a substantially electrically non-conductive substrate material, said strip having a central portion containing athe medicament in an electrically conductive substratefor iontophoretic delivery of the medicament into the person's skin at the treatment site upon completion of an electrical circuit from said power means through said active terminal and said tactile electrode via the person's skin at the treatment site, and said strip having laterally symmetric end portions having cutouts therewithin.
2. The disposable medicament dispensing applicator electrode of claim 1 wherein said cutouts in said laterally symmetric end portions contain an electrically conductive material.
3. The disposable medicament dispensing applicator electrode of claim 2 wherein said electrically conductive material is a gel.
4. A disposable medicament dispensing applicator electrode for an iontophoretic drug delivery device adapted for the self-administration of a medicament into a person's skin, said device comprising a base assembly having an active terminal adapted to receive and make electrical contact with a detachable medicament dispensing applicator electrode wherein said base assembly comprises; a case having an elongate, substantially cylindrical outer surface having a size and shape adapted to be comfortably grasped within a person's hand and wherein at least a portion of said outer surface is a tactile electrode formed of an electrically conductive material; and a bipolar electrical power means having a first pole and a second pole; said electrical power means being enclosed within said case and wherein said first pole is in electrical communication with said tactile electrode; wherein said medicament dispensing applicator electrode comprises: a module containing a unit dose of medicament, an electrically conductive working electrode and means thereon adapted for releasably attaching applicator working electrode to said second pole of said electrical power means wherein said applicator electrode further comprises an elongate strip constructed of a substantially electrically non-conductive substrate material, said strip having a central portion containing a medicament in an electrically conductive substrate and said strip having laterally symmetric end portions having cutouts therewithin.
5. A combination disposable medicament dispensing applicator electrode and drug delivery device for electrokinetic self-administration of a medicament into an individual's skin at a localized treatment site, said device including a base assembly having an active terminal for receiving and making electrical contact with the medicament dispensing applicator electrode, said base assembly comprising a case including an outer surface having a size and shape for comfortably grasping within an individual's hand, a portion of said outer surface including a tactile electrode formed of an electrically conductive material and a bipolar electrical power means having a first pole and a second pole, said electrical power means being enclosed within said case, said first pole being in electrical contact with said tactile electrode, said medicament dispensing applicator electrode comprising an elongated strip containing a medicament, and means for releasably attaching said applicator electrode to said case in electrical contact with said second pole of said electrical power means, said strip being formed of a substantially electrically non-conductive strip material having a portion thereof containing a medicament, said device and said electrode being operable to electrokinetically effect delivery of the medicament in said strip to the individual's skin at the treatment site in contact with said substrate in response to completion of an electrical circuit between said second pole through said strip and via the individual's contacted skin at the treatment site and said first pole through said tactile electrode when the device is grasped by the individual.
6. A combination according to claim 5 wherein the medicament is charged.
7. A combination according to claim 5 wherein said non-conductive strip material portion contains a conductive gel to facilitate electrokinetic delivery of the medicament into the individual's skin at the treatment site.

REFERENCE TO RELATED APPLICATIONS

This application is a continuation-in-part of application Ser. No. 08/868,499 filed Jun. 4, 1997, now U.S. Pat. No. 5,879,323 issued Mar. 9, 1999, which is a divisional of allowed U.S. patent application Ser. No. 08/646,853 filed May 8, 1996 now U.S. Pat. No. 5,767,648.

US Referenced Citations (116)

Number	Name	Date	Kind
279524	Beaty	Jun 1883	A
484522	McBride	Oct 1892	A
600290	Muir	Mar 1898	A
2129070	Wappler	Aug 1938	A
2834344	Kanai	May 1958	A
3019787	Simmons	Jan 1962	A
3048170	Lemos	Aug 1962	A
3107672	Hofmann	Oct 1963	A
3163166	Brant et al.	Dec 1964	A
3298368	Charos	Jan 1967	A
3520297	Bechtold	Jul 1970	A
3645260	Cinotti et al.	Feb 1972	A
3716054	Porter et al.	Feb 1973	A
3831598	Tice	Aug 1974	A
4325367	Tapper	Apr 1982	A
4383529	Webster	May 1983	A
4474570	Ariura et al.	Oct 1984	A
4510939	Brenman et al.	Apr 1985	A
4665921	Teranishi et al.	May 1987	A
4689039	Masaki	Aug 1987	A
4702732	Powers et al.	Oct 1987	A
4747819	Phipps et al.	May 1988	A
4787888	Fox	Nov 1988	A
4838273	Cartmell	Jun 1989	A
4913148	Diethelm	Apr 1990	A
4919648	Sibalis	Apr 1990	A
4953565	Tachibana et al.	Sep 1990	A
4957480	Morenings	Sep 1990	A
4979938	Stephen et al.	Dec 1990	A
4997418	DeMartini	Mar 1991	A
5037381	Bock et al.	Aug 1991	A
5042975	Chien et al.	Aug 1991	A
5090402	Bazin et al.	Feb 1992	A
5133352	Lathrop et al.	Jul 1992	A
5160316	Henley	Nov 1992	A
5162042	Gyory et al.	Nov 1992	A
5169384	Bosniak et al.	Dec 1992	A
5203768	Haak et al.	Apr 1993	A
5250022	Chien et al.	Oct 1993	A
5279543	Glikfeld et al.	Jan 1994	A
5284471	Sage, Jr.	Feb 1994	A
5298017	Theeuwes et al.	Mar 1994	A
5312326	Myers et al.	May 1994	A
5314502	McNichols et al.	May 1994	A
5331979	Henley	Jul 1994	A
5354321	Berger	Oct 1994	A
5360440	Andersen	Nov 1994	A
5362307	Guy et al.	Nov 1994	A
5362308	Chien et al.	Nov 1994	A
5374241	Lloyd et al.	Dec 1994	A
5374242	Haak et al.	Dec 1994	A
5376107	Inagi et al.	Dec 1994	A
5391195	Van Groningen	Feb 1995	A
5395310	Untereker et al.	Mar 1995	A
5413590	Williamson	May 1995	A
5415629	Henley	May 1995	A
5421816	Lipkovker	Jun 1995	A
5441936	Houghten et al.	Aug 1995	A
5443441	De Claviere	Aug 1995	A
5458569	Kirk et al.	Oct 1995	A
5464387	Haak et al.	Nov 1995	A
5466217	Myers et al.	Nov 1995	A
5470349	Kleditsch et al.	Nov 1995	A
5494679	Sage, Jr. et al.	Feb 1996	A
5501705	Fakhri	Mar 1996	A
5514167	Smith et al.	May 1996	A
5558632	Lloyd et al.	Sep 1996	A
5562607	Gyory	Oct 1996	A
5589563	Ward et al.	Dec 1996	A
5603693	Frenket et al.	Feb 1997	A
5607461	Lathrop	Mar 1997	A
5607691	Hale et al.	Mar 1997	A
5618275	Bock	Apr 1997	A
5658247	Henley	Aug 1997	A
5667487	Henley	Sep 1997	A
5668170	Gyory	Sep 1997	A
5676648	Henley	Oct 1997	A
5688233	Hofmann et al.	Nov 1997	A
5697896	McNichols et al.	Dec 1997	A
5700457	Dixon	Dec 1997	A
5711761	Untereker et al.	Jan 1998	A
5713846	Bernhard et al.	Feb 1998	A
5722397	Eppstein	Mar 1998	A
5725817	Milder	Mar 1998	A
5733255	Dinh et al.	Mar 1998	A
5755750	Petruska et al.	May 1998	A
5788666	Atanasoska	Aug 1998	A
5795321	McArthur et al.	Aug 1998	A
5797867	Guerrara et al.	Aug 1998	A
5830175	Flower	Nov 1998	A
5840057	Alosi	Nov 1998	A
5846217	Beck et al.	Dec 1998	A
5879323	Henley	Mar 1999	A
5882676	Lee et al.	Mar 1999	A
5908401	Henley	Jun 1999	A
5919155	Lattin et al.	Jul 1999	A
5931859	Burke	Aug 1999	A
5935598	Sage et al.	Aug 1999	A
5961482	Chien et al.	Oct 1999	A
5961483	Sage et al.	Oct 1999	A
5968005	Tu	Oct 1999	A
5968006	Hofmann	Oct 1999	A
5983130	Phipps et al.	Nov 1999	A
6004309	Phipps	Dec 1999	A
6004547	Rowe et al.	Dec 1999	A
6006130	Higo et al.	Dec 1999	A
6018679	Dinh et al.	Jan 2000	A
6023639	Hakky et al.	Feb 2000	A
6032073	Effenhauser	Feb 2000	A
6038485	Axelgaard	Mar 2000	A
6041252	Walker et al.	Mar 2000	A
6041253	Kost et al.	Mar 2000	A
6048545	Keller et al.	Apr 2000	A
6057374	Huntington et al.	May 2000	A
6101411	Newsome	Aug 2000	A
6167302	Millot	Dec 2000	A

Foreign Referenced Citations (4)

Number	Date	Country
0232642	Mar 1964	AT
617979	Oct 1994	EP
1445703	Jun 1966	FR
0299553	Nov 1928	GB

Non-Patent Literature Citations (56)

Entry
“Iontophoretic Treatment of Oral Herpes,” Henley et al.; Laryngoscope, vol. 94, No. 1, pp. 118-121, Jan. 1984.
“Iontophoretic Application of Idoxuridine for Recurrent Herpes Labialis: Report of Preliminary Chemical Trials,” Gangarosa et al.; Meth. And Find. Exptl. Clin. Pharmacol. 1(2), pp. 105-109 (1979).
“Iontophoresis of Vidarabine Monophosphate for Herpes Orolabialis,” Gangarosa et al.; The Journal of Infectious Diseases, vol. 154, No. 6, pp. 930-934, Dec. 1986.
“The Natural History of Recurrent Herpes Simplex Labialis,” Spruance et al.; The New England Journal of Medicine, vol. 297, No. 2, pp. 69-75, Jul. 14, 1977.
“Infection with Herpes-Simplex Viruses 1 and 2,” Nahmias et al.; The New England Journal of Medicine, pp. 667-674, Sep. 27, 1973.
“Anesthesia of the Human Tympanic Membrane by Iontophoresis of a Local Anesthetic,” Comeau et al.; The Laryngoscope, 88:1978, pp. 277-285.
“Iontophoretic Application of Drugs,” Waud, J. Appl. Physiol. 23(1), 1967, pp. 128-130.
“Antibiotic Iontophoresis in the Treatment of Ear Chondritis,” LaForest et al., Physical Therapy, vol. 58, No. 1, Jan. 1978, pp. 32-34.
“The Quantity and Distribution of Radiolabeled Dexamethasone Delivered to Tissue by Iontophoresis,” Glass et al.; International Journal of Dermatololgy, vol. 19, Nov. 1980, 519-525.
“Iontophoretic Application of Antiviral Chemotherapeutic Agents,” Hill et al., Annals New York Academy of Sciences, pp. 604-612.
“Ocular lontophoresis,” Hill et al. Paper, Louisiana State University Medical Center, School of Medicine, New Orleans, Louisiana, pp. 331-354.
“Iontophoretic Application of Adenine Arabinoside Monophosphate to Herpes Simplex Virus Type 1-Infected Hairless Mouse Skin,” Park et al.; Antimicrobial Agentsand Chemotherapy, vol. 14, No. 4, Oct.; 1978, pp. 605-608.
“Iontophoresis: Applications in Transdermal Medication Delivery,” Costello et al.; Physical Therapy, vol. 75, No. 6, pp. 104/554-113/563, Jun. 1995.
Physical Enhancement of Dermatologic Drug Delivery: Iontophoresis and Phonophoresis,: Kassan et al.; Journal of the American Academy of Dermatology, Apr. 1996, pp. 657-666.
“Iontophoresis and Herpes Labialis,” Boxhall et al.; The Medical Journal of Australia, May 26, 1984, pp. 686-687.
“A Method of Antibiotic Administration in the Burn Patient,” Rapperport et al.; Plastic and Reconstructive Surgery, vol. 36, No. 5, pp. 547-552.
“Iontophoresis for Enhancing Penetration of Dermatologic and Antiviral Drugs,” Gangarosa et al., Journal of Dermatology, vol. 22, No. 11, pp. 865-875, Nov. 1995.
“Iontophoretic Treatment of Herpetic Whitlow,” Gangarosa et al., Arch. Phys. Med. Rehabil., vol. 70, Apr. 1989.
“Iontophoretic Application of Antiviral Drugs,” Gangarosa et al., Proceedings of an International Symposium held in Tokushima City, Japan, pp. 200-204, Jul. 27-30, 1981.
“Iontophoretic Application of Adenine Arabinoside Monophosphate for the Treatment of Herpes Simplex Virus Type 2 Skin Infections in Hairless Mice,” Gangarosa, The Journal of Infectious Diseases, vol. 140, No. 6, pp. 1014, Dec. 1979.
“Effect of Iontophoretic and Topical Application of Antiviral Agents in Treatment of Experimental HSV-1 Keratitis in Rabbits,” Kwon et al., Investigative Ophthalmology & Visual Science, vol. 18, No. 9, pp. 984-988, Sep., 1979.
“Acyclovir and Vidarabine Monophosphate: Comparison of Iontophoretic and Intravenous Administration for the Treatment of HSV-1 Stromal Keratitis,” Hill et al., The American Journal of Medicine, Acyclovir Symposium, pp. 300-304.
“Thymine Arabinoside (Ara-T) Topical and Iontophoretic Applications for Herpes Simplex Virus Type 1 and Type 2 Skin Infections in Hairless Mice,” Hill et al., Meth. And Find. Exptl. Clin. Pharmacol. 6(1), pp. 17-20, 1984.
“Iontophoresis Enhances the Transport of Acyclovir Through Nude Mouse Skin by Electrorepulsion and Electroosmosis,” Volpato et al., Pharmaceutical Research, vol. 12, No. 11, pp. 1623-1627, 1995.
“Early Application of Topical 15% Idoxuridine n Dimethyl Sulfoxide Shortens the Course of Herpes Simplex Labialis: A Multicenter Placebo-Controlled Trial,” Spruance et al., The Journal of Infectious Diseases, 1990; vol. 161; pp. 191-197.
“Iontophoresis for Surface Local Anesthesia,” Gangarosa, JADA, vol. 88, pp. 125-128, Jan. 1974.
“Conductivity of Drugs Used for Iontophoresis,” Gangarosa et al., Journal of Phamaceutical Sciences, vol. 67, No. 10, pp. 1439-1434, Oct., 1978.
“A Pilot Study of Iontophoretic Cisplatin Chemotherapy of Basal and Squamous Cell Carcinomas of the Skin,” Chang et al., Arch. Dermatol., vol. 129, pp. 425-427, Apr. 1993.
“How Modern Iontophoresis Can Improve Your Practice,” Gangarosa et al.; Oral Surgery, No. 10, Report 2135, Oct. 1982, pp. 1027-1038.
“Postherpetic Neuralgia,” Baron et al.; Brain (1993), 116, pp. 1477-1496.
“Iontophoretic Assistance of 5-Iodo-2′-Deoxyuridine Penetration into Neonatal Mouse Skin and Effects of DNA Synthesis,” Gangarosa et al., Society for Experimental Biology and Medicine, pp. 439-443, 1977.
“Electrophoretic Evaluation of the Mobility of Drugs Suitable for lontophoresis,” Kamath et al., Meth. Find., Exp. Clin. Phamacol., 1995, 17(4): pp. 227-232.
“Passive versus Electrotransport-Facilitated Transdermal Absorption of Ketorolac,” Park et al.; Clinical Pharmacology & Therapeutics, vol. 63, No. 3, pp. 303-315.
“Transdermal Drug Delivery by Passive Diffusion and Iontophoresis: A Review,” Singh et al.; Medicinal Research Reviews, vol. 13, No. 5, 1993, pp. 570-621.
“Iontophoresis: Electrorepulsion and Electroosmosis,” Guy et al., Journal of Controlled Release 64 (2000) 129-132.
“Treatment of Common Cutaneous Herpes Simplex Virus Infections,” Emmert, American Family Physician, vol. 61, No. 6, Mar. 15, 2000, pp. 1697-1704.
“Gelatin-stabilised Microemulsion-Based Oranogels: Rheology and Application in Iontophoretic Transdermal Drug Delivery,” Kantaria et al., Journal of Controlled Release 60 (1999) 355-365.
“Electrotepulsion Versus Electroosmosis: Effect of pH on the Iontophoretic Flux of 5-Fluorouracil,” Merino at al., Pharmaceutical Research, vol. 16, No. 6 (1999).
“Azelaic Acid: Potential as a General Antitumoural Agent,” Breathnach, Medical Hypotheses (1999) 52(3) 221-226.
“Treatment of Mucocutaneous Herpes Simplex Virus Infections Unresponsive to Acyclovir with Topical Foscarnet Cream in AIDS Patients: A Phase I/II Study,” Javaly et al., Journal of Acquired Immune Deficiency Syndromes 21:301-306.
“Efficacy and Safety of Azelaic Acid and Glycolic Acid Combination Therapy Compared with Tretinoin Therapy for Acne,” Spellman et al., Clinical Therapeutics, vol. 20, No. 4, 1998.
“Passive Versis Electrotransport-Facilitated Transdermal Absorption of Ketorolac,” Park et al., Clinical Pharmacology & Therapeutics, vol. 63, No. 3, pp. 303-315.
“Soriudine Versus Acyclovir for Treatment of Dermatomal Herpes Zoster in Human Immunodeficiency Virus-Infected Patients: Results from a Randomized, Controlled Clinical Trial,” Gnann et al., Antimicrobial Agents and Chemotherapy, vol. 42, No. 5, May 1998, pp. 1139-1145.
“Azelaic Acid 20% Cream (AZELEX®) and the Medical Management of Acne Vulgaris,” Gibson, Dermatology Nursing, vol. 9, No. 5, pp. 339-344.
“Sorivudine: A Promising Drug for the Treatment of Varicella-Zoster Virus Infection,” Whitley, Neurology 1995; 45 (Supp. 8), pp. S73-S75.
“Transdermal Drug Delivery by Passive Diffusion and Iontophoresis: A Review,” Singh et al., Medicinal Research Reviews, vol. 13, No. 5, pp. 569-61 (1993).
“Antiherpesviral and Anticellular Effects of 1-β-D-Arabinofuranosy-E-5-(2-Halogenovinyl) Uracils,” Machinda et al., Antimicrobial Agents and Chemotherapy, Jul. 1981, pp. 47-52.
“Herpes Simplex,” American Academy of Dermatology.
“Common Cold” Virus is Near, Haney, The Associated Press, Jan. 15, 2000.
“New Medicines Move to Eradicate Acne,” Hemphill, The New York Times, Feb. 29, 2000.
“Warts,” American Academy of Dermatology, American Academy of Dermatology, 1997, Revised 1991, 1993.
“Psoriasis,” American Academy of Dermatology, 1994.
“Eczema/Atopic Dermatitis,” American Academy of Dermatology, 1987, Revised 1991, 1993, 1995.
“Skin Cancer: An Undeclared Epidemic,” American Academy of Dermatology, 1988, Revised 1989, 1993, 1994.
File History of U.S. Pat. No. 5,676,648 to Henley.
File History of U.S. Pat. No. 5,879,323 to Henley.

Divisions (1)

	Number	Date	Country
Parent	08/991827	Dec 1997	US
Child	09/654583		US

Reissues (1)

	Number	Date	Country
Parent	08/991827	Dec 1997	US
Child	09/654583		US

Methods for iontophoretic delivery of antiviral agents

Information

Patent Number

Date Filed

Date Issued

Inventors

Original Assignees

Examiners

Agents

US Classifications

Field of Search

US

International Classifications

Abstract