Patent Application
20080312579
The present invention relates generally to applicators for electrokinetic mass transfer of substances to live tissue and particularly relates to an apparatus for electrokinetically delivering substances, e.g., a medicament, to a treatment site on, in or under the skin of a human patient. In particular, this application is directed to electrokinetic delivery applicators for wide areas of skin to infuse medicament into a wide area treatment site and applicator for treatment sites having high resistances, such as a toenail or fingernail or area of hard skin.
Electrokinetic delivery of medicaments applies medication topically to the skin to reach a treatment site. One type of electrokinetic delivery mechanism is iontophoresis, which is the application of an electric current to the skin to enhance the permeability of the skin and thereby deliver ionic agents, e.g., ions of salts and other drugs, to the treatment site below the surface of the skin. Electrokinetic delivery methods include iontophoretic, transdermal, transmucosal cutaneous, electroosmosis, electroporation, and electromigration, any or all of which are more generally known as electrotransport, electromolecular transport or iontophoretic methods. These techniques are collectively referred to herein as electrokinetic delivery methods.
Electrokinetic delivery methods may be problematic when applied to, for example, large areas of skin, skin with highly variable impedances, or tissues with high intrinsic impedance such as toenails. Large skin treatment areas may be associated with skin conditions such as eczema, psoriasis and acne. To deliver medicament electrokinetically to a large skin treatment site, a relatively large medicament matrix is applied to the skin. A large electrical current is generally needed to electrokinetically drive sufficient medicament from the large area matrix into the skin. The matrix consists of a uniform solid phase within which is dispersed a uniform medicament formulation. Such a matrix is limited to delivering that medicament at one rate governed by the applied current from an electrode in general contact with the entire matrix. There is a need for a medicament matrix that is more responsive to the particular needs of tissues from one site to another beneath the matrix and that is capable of delivering one or more medicaments at various rates or dosages. Further, in lieu of a single electrode, an array of electrodes is superimposed on the matrix to establish electrical current through the medicament matrix and treatment site. Additionally, it is conventional for a counter electrode to be applied to the patient at a significant distance from the matrix. The current must flow through the patient from the delivery electrode adjacent the medicament matrix through the patient to the counter electrode. This resulting long current path through the skin may result in excessive voltage drop and poor control over spatial distribution of drug delivery.
Further, applying a large electrical current presents a risk of electrically sensitizing, irritating, or burning the skin, especially if the current is concentrated on a small skin area. A large area medicament matrix may be intended to contact a large area of skin. The uniformity of electrical impedance in a large area medicament matrix is not always maintainable due to factors such as patient movement, contact pressure, change of skin condition, development of skin lesion and liquid medicament migration. Area of low impedance may develop, and since current tends to follow the path of least resistance, the large current applied to the matrix as a whole may become concentrated on a localized area and may potentially cause tissue damage. In another example, the impedance of a toenail is high a relatively high voltage is applied to deliver medicament to the nail. The medicament matrix applied to the toenail may inadvertently touch the low impedance soft skin tissue next to the nail. There is a risk that a high current will flow and will be concentrated on the small area of soft skin that is inadvertently in contact with the medicament matrix. The high current concentration may cause a burn on the skin contact area adjacent the nail.
In other example, an electrokinetic applicator may be applied to a cold sore on a lip or the edge of the lip. The medicament matrix in the applicator is intended to contact the entire surface of the skin afflicted with the cold sore plus a surrounding area as a prophylactic measure. Due to the curvature of the lip and the edge of the lip, the applicator matrix may contact only a small skin area on the lip area rather than a larger skin area surrounding the cold sore. Current intended to be evenly distributed over the entire face on the applicator matrix may concentrate at the small skin contact area.
There is a long felt need for an electrokinetic device and method that delivers medicament and minimizes the potential for current concentration and associated burning of the skin contact area. In particular, there is a need for an electrokinetic device capable of delivering medicament using a high current applied to a large skin contact area, to a toenail or fingernail, or to a curved skin area without high density current being applied to soft tissue near the treatment site or a localized skin imperfection with relatively low impedance.
An electrokinetic apparatus has been developed to apply medicament to a treatment site of a mammalian user, the apparatus including: a segmented active electrode; a medicament matrix having one side abutting the segmented active electrode and another side adapted to contact a surface of skin over the treatment site, wherein the matrix includes at least one current direction barrier suppressing lateral and transverse current flow through the matrix.
A method has been developed to electrokinetically deliver a medicament to a treatment site in a mammalian user, the method comprising: applying a first surface of a medicament matrix to a surface on the user; applying a segmented first electrode to a second surface of the medicament matrix; applying electrical current to an electrical current path extending through the first electrode segments, medicament matrix, at least partially through the user and to a second electrode; delivering medicament from the matrix into the treatment site by electrokinetically transporting the medicament along the current path, and blocking transverse current from one electrode segment of the first electrode to the surface on the user not aligned with the one electrode segment.
An electrokinetic apparatus has been developed to apply medicament to a treatment site of a mammalian user, the apparatus comprising: an active electrode including first and second active electrode segments; a counter electrode including first and second counter electrode segments; a medicament matrix having one side abutting the segments of the active electrode and another side adapted to contact a surface of the user over the treatment site, wherein the matrix includes at least one current direction barrier suppressing transverse current flow through the matrix; a first electrical circuit including the first active electrode segment and the first counter electrode segment, and a second electrical circuit including the second active electrode segment and the second counter electrode segment, wherein the first electrical circuit is galvanic-isolated from the second electrical circuit. This apparatus can also be expanded to include a multitude of active electrodes in addition to the first and second active electrodes.
An applicator panel has been developed for an electrokinetic delivery system including: an array of electrodes arranged on a flexible substrate and conductive pathways between each of the electrodes and a connector to receive a connection to a electronic control and power source circuit, wherein each electrode includes a center active electrode region and an outer return electrode region extending around the active electrode region, and at least one non-woven layer having a pattern of medicament cells and network of ribs between the cells, wherein the non-woven layer has a back surface laminated to the array of electrodes and the cells are each aligned with a respective one of the electrodes.
An applicator for an electrokinetic delivery system has been developed comprising: an array of electrodes arranged on a substrate and conductive pathways between each of the electrodes and a connector to receive a connection to a electronic control and power source circuit, wherein the electrodes are arranged in at least a first commonly connected group of electrodes and a second commonly connected group of electrodes; a first medicament layer having a pattern of first medicament cells, wherein the first medicament cells are aligned with the electrodes of the first commonly connected group of electrodes; a second medicament layer having a pattern of second medicament cells, wherein the second medicament cells are aligned with the electrodes of the second commonly connected group of electrodes, and an electronic controller controlling the electrokinetic delivery to a treatment site of a patient and underlying the first and second medicament layers, wherein medicament in the first medicament layer is delivered by electrically actuating the first commonly connected group of electrodes and medicament in the second medicament layer is delivered by electrically actuating the second commonly connected group of electrodes. The first and second groups of electrodes may or may not be of the same polarity. For example, an applicator pad with both anodic and cathodic electrodes would be well suited to deliver medicaments having both anionic and cationic actives to be delivered at the same time. Such an applicator having both anodic and cathodic electrodes may include a neutral polarity counterelectrode for each of the anodic and cathodic electrodes.
An applicator panel has been developed for an electrokinetic delivery system comprising: an array of electrodes arranged on a flexible substrate and conductive pathways between each of the electrodes and a connector to receive a connection to a electronic control and power source circuit; at least one non-woven layer having a pattern of medicament cells and ribs between the cells, wherein the cells are aligned with electrodes of the array; an adhesive matrix where the adhesive is aligned with the ribs, wherein the non-woven layer is sandwiched between the array of electrodes and the adhesive matrix.
A method has been developed to form an applicator panel for an electrokinetic delivery system comprising: embossing a pattern of medicament cells and ridges on a non-woven layer; infusing a medicament into the medicament cells; forming an electrode layer by applying an array of electrodes on a front side of an electrode layer substrate and forming an electrical distribution circuit on a back side of the electrode layer substrate, and securing the front side of the electrode layer substrate to a back side of the non-woven layer, wherein the electrodes are aligned with the medicament cells. The method may further include forming a first sub-layer and a second sub-layer of the non-woven layer, wherein each of the sub-layers includes a separate group of the medicament cells and the group of the medicament cells in the first sub-layer is non-overlapping with the group of the medicament cells in the second sub-layer.
An array of electrodes in an applicator panel has been developed for an electrokinetic delivery system including a medicament layer having an array of medicament cells, each of the electrodes comprising: a center electrode region aligned with one of the medicament cells; a non-conductive region surrounding the center electrode, and a neutral return electrode region encircling the annular adhesive seal. The center region in each of a first plurality of the electrodes is a cathodic center region coupled to a source of positive voltage and the center region in each of a second plurality of the electrodes is an anodic center region coupled to a source of negative voltage.
The ETS control unit 12 may be housed in a handheld device having an actuator switch to provide a manual trigger of the application of medicament by electrokinetic delivery. The ETS control unit may comprise a power system, such as batteries; a microcontroller for monitoring certain conditions, such as whether a valid cartridge is inserted in the device, and controlling the application of current to the active electrode, and conductive circuits connecting the power supply, microcontroller, actuator switch, active electrode and counter electrode. The ETS control unit, when actuated, applies current to each of the plurality of electrode segments of the active electrode. The current applied to the electrode segments may be, for example, on the order of 660 microAmps (uA). A current path includes the power connector 14, active electrode 18, medicament matrix 20 which is applied to the skin of a patient, e.g., a mammalian user, the patient, a counter electrode 21 that is applied to the patient, and the ETS control unit.
The active electrode power connector 14 may include a plurality contact pins 22, e.g., five pins, each having a current limiting device, such as a current limiting diodes (CLD) 24. The five diodes are arranged in electrical series with the contact pins. A conductive bus 26 provides a common connection between each pin 22 and diode 24 arrangements and the ETS control unit. The diodes each limit the current to a respective one of the contact pins 22 to, for example, 132 uA or about one fifth the total current applied by the entire electrode segments. The diodes may be selected to limit the current to each of the contact pins to a predetermined level, such as a current level determined by the total current applied to all electrodes divided by the number of contact pins 22.
The current limiting device 24 is preferably a simple, miniature current limiting device for each of the partition and/or sub-divided segments of the active electrode. The diodes 24 are one example of a current limiting device such as the generic current limiting diodes 1N5283 through 1N5314 and the CCLM0130 manufactured by Central Semiconductor Corporation. Other electronic circuit components that limit the current to each contact pin may be suitable. There are several types of current limiting diodes (CLD), such as a current regulator diode, constant current diode, and current limit diodes. Current regulating diodes regulate the current flowing through them to a maximum level and if current exceeds its current regulation point, it drops its terminal voltage. A constant current diode is similar to a junction field effect transistor (JFET) whose gate terminal is shorted to source. A constant current diode can automatically limit a current through a laser driver current limit diode over a wide range of power supply voltages. A laser driver current limit diode is a type of current limiting diode (CLD) that works on the principle of a quantum process whereby light is emitted due to transition of electrons from high-level to low-level energy states. Current limit diodes are employed to ensure that excessive current does not flow to any one of the active electrodes. The CLD is preferably arranged in the housing of the device (rather than in the cartridge), so that the CLD may be reused and is not discarded with the cartridge.
Current is distributed equally to each segment of the active electrode 18 in proportion to the number of electrodes and/or the size of the matrix corresponding to the corresponding electrode segment. The current is distributed, for example, by the bus 26 and the current limiting device 24 with each pogo pin 22. Because of the current limiting devices 22, the current flow through each segment 36 of the active electrode 18 is preferably limited and not excessive due to a small skin area or other condition that might lead to current concentration. The maximum current density applied to the matrix by each active electrode segment is generally equal to the current applied by the pogo pin 22 applied to the electrode segment divided by the area of the electrode segment.
The pins 22 may be spring biased, e.g., pogo pins, such that the pins are biased downward and can be deflected upwards, as shown by a double-headed arrow in
The cartridge 16 may have a generally cylindrical shape with an annular plastic wall 28 that defines a cylindrical recess 30 to receive the medicament matrix 20. The recess 30 may have an open face 32 which is applied to the surface of the skin or toenail to press the medicament matrix against the skin or nail. The cartridge may alternatively be embodied as an array of cartridges that are applied to various locations on the skin or nail.
The active electrode 18 may be mounted on a surface 34 (
If the skin contact area 40 is smaller than the matrix face 42, the current may become concentrated on the small skin contact area 40 as is illustrated by the arrows in
The foam structure of the matrix 44 may be provided by specialty foams that mimics a honeycomb structure and allows ion to flow only in one direction, i.e., parallel to axis 41. The structure of the matrix 44 effectively blocks transversal ionic flow and prevents current tunneling from neighboring segments of the active electrode. Current concentration is effectively avoided by the use of a current directional foam (or other medicament matrix that prevents lateral current flow transverse to the cartridge axis) in combination with a segmented electrode having current limiting devices. The foam structure minimizing transverse current flow augments the effect of current limiting diodes connected to a multi-electrode matrix and the intrinsic resistance to lateral current flow of the medicament and/or skin.
Unidirectional-aligned open cell foams and films suitable for use as a medicament matrix 44 are well known and include the Celgard™ microporous polypropylene film sold by Hoechst-Celanese Plastic Company of Newark, N.J. and is a flexible microporous film with a unidirectional structure. Unidirectional aligned polypropylene open cell foams have also been reported by BASF (Journal of Material.Science 41, 2006). These foam matrix materials may be applied as pharmaceutical grade, unidirectional current foams for use as medicament matrix.
The barrier walls 48 in the medicament matrix are aligned with axis of the cartridge. The barrier walls are dielectric and may comprise silicone rubber, air, or other dielectric material. The barrier walls are preferably aligned with the gaps 37 between the segments 36 (
The use of strategically positioned segmented electrodes, current limiting diodes, and unidirectional foam material (such as with honeycomb-like structure and as shown in
Onychomycosis is the invasion of a toenail plate by a dermatophyte, yeast or nondermatophyte mould. The medicament may be used to treat, for example, onychomycosis, which is a fungal invasion of the nail. The fungal infection may be due to a dermatophyte, yeast, or nondermatophyte mould. The medicament is intended to destroy the fungus or at least cause the fungal invasion to subside. For effective onychomycosis treatment, it is desirable to have the medicine, e.g., Terbinafine hydrochloride or Fluconazole, penetrates the nail and saturates the surrounding tissues. In view of the high electrical impedance of the nail plate, a high voltage, such as over one hundred volts, may be required to electrokinetically deliver the medicament to surrounding tissues in onychomycosis treatment. The toenail involved in onychomycosis treatment is often small and the matrix applied to the nail may touch the soft tissue adjacent the nail. Current concentration may occur due to the high current applied by the active electrode, especially if a portion of the matrix is in contact with the soft tissue adjacent the nail. Since current will seek the path of least resistance, current may traverse the medicament matrix to flow to the soft tissue. In this manner, severe current concentration can occur at the soft tissue in contact with the matrix.
The electrolytic layer of the counter electrode 66 may be a strip having an adhesive surface that adheres to the pad of the toe or finger. The active electrode segments 60 may be mounted on the medicament matrix 68, e.g., a porous sheet with an adhesive surface that adheres to the nail and upper skin tissue of the toe or finger. Each electrode segment 60 is in series with a current limiting device, e.g., a current limiting diode 24. The medicament matrix sheet 68 for onychomycosis treatment may include a thin hydrogel layer which may be a web applied to the nail. The medicament matrix 68 may extend beyond the nail and cover portions of the soft tissue of the toe or finger, as does the matrix below active electrode segment 60a.
The counter electrode segments 69 are each electrically coupled to a corresponding segment of the active electrode 60. An electrical circuit 71 is formed for each pair of active and counter electrode segments, wherein the circuit couples the pair to a power source and isolates the pair from current in the circuit 71 for other pairs of active and counter electrode segments. To safeguard against current concentration, each pair of active and counter electrode segments may be electrically isolated from the other pairs of electrode segments.
The current driver 72 may be a conventional transformer in which secondary voltage is determined by the ratio of primary to secondary transformer turns and controlled by a primary side oscillator driver power supply circuit (not shown). The current limiting diode 24 on each of the active electrode segments controls the current level applied by each active electrode segment to the matrix 68. The electrical circuit consisting of secondary winding 74, current diode 24, active and counter electrode segments 60 and 69, is intentionally simplified for clarity. Other active circuit elements can also be included to add more sophistications and features, if desired. Providing isolated pairs of electrode segments, minimizes current concentration in the presence of especially disparity in impedances between cuticle, nail folds, and nail plate. Use of segmented electrode pairs addresses the current concentration issue on the active and counter electrode side.
Using segmented active/counter electrodes for current concentration abatement has other benefits. By measuring the voltage drop across each electrode segment pair 60 and 69, and by dividing it with the current magnitude, the resistance of the current path can be determined and monitored either by analog or digital circuitry, or by a simple microprocessor operating within the same galvanic-isolated power loop.
In conducting electrokinetic transdermal drug delivery and onychomycosis treatment, an abnormal breach in the skin or nail may form such as a localized lesion, sore, pin hole or crack may develop in the skin or nail during treatment. Such an abnormal breach of the skin or nail barrier property can lead to a substantial reduction of local tissue impedance. Although the current of each segmented electrode pair is limited by the current limiting diode 24, the current density at the localized lesion can still be high enough to cause discomfort, burn, and tissue damage. This sudden impedance reduction can easily be detected by the microprocessor, and the current can either be reduced or switched off totally.
Since resistance of the current path for each individual segmented electrode pair can be measured, also since the current for each electrode pair can be separately controlled, a method of area mapping and current control for large skin area treatment is devised. As an exemplary case, consider large area facial eczema treatment using segmented electrodes and unidirectional medicinal foam matrix. Although the eczema afflicted area and topology may vary from patient to patient, a general purpose large area electrode containing a multitude of segmented active electrode can be used. In treatment, the medicament matrix is trimmed to cover the afflicted area. The flexible, segmented electrode sheet, being over-sized by design, is placed over the entire afflicted area. Since the resistance of each segmented pair can be measured, the afflicted area is identified as being with normal medicinal matrix resistance, whereas the un-afflicted area exhibits high resistance. Thus the afflicted area can be precisely mapped and treatment currents are switched on and delivered only to electrode pairs associated with the active area. There is no voltage being biased across un-used electrode pairs and there is no current flow to un-treated area. Impedance mapping allows for activation of active segments and de-activation of idle segments. It also allows for use of a universal active electrode design suitable for all patients.
Within the loop of each pair of segmented electrodes 1138, current flows from the active (positive) to the counter (negative) electrode through a medicament matrix, the treatment site and the body of the mammalian user. The current magnitude in each current loop is limited to a value controlled by the current limiting diode 1140 irrespective of the nail and tissue impedance. Although a high DC voltage is generated within each loop, this voltage is self regulating and it will drop entirely across the current limiting diode 1140, nail plate and the toe. Each current loop for each electrode pair maintains a pre-set current which is galvanic-isolated in so far as the coils are isolated. Because a sufficient amount of energy is transferred to the secondary side of the flyback transformer 1136 to obtain a sufficient high DC voltage, the full current allowed by each current diode is maintained. The nail and toe are effectively a short-circuit down stream from the current diode operating in the “limiting” mode.
The applicator panel is connected to a power source and computer controller 118 that may be mounted on the applicator panel or attached by electrical wires 120 to an electrode layer 122 on a side of the medicament layer opposite to the skin. Electrical current through the wires 120 from the power supply and controller to an electrical distribution circuit 124 that directs current to and from individual electrodes 126. The electrical power may be delivered through separate electric current channels to each electrode 126 such that the amount of current applied to each electrode may be separately controlled by the controller 18 or other circuits associated with the distribution circuit 124.
Each electrode 126 may include an active and neutral electrical terminal. There is a neutral electrode that is unique and local to each active electrode. The current path between the active and neutral electrical terminals of each electrode passes through the medicament layer and the treatment site. Accordingly, electrical power passing through each electrode causes medicament in the medicament layer to be delivered to the treatment site as the current in the power passes between the active and neutral terminals of the electrode.
The power supply may include batteries contained in a housing with the controller or may include an adapter that plugs into a conventional electrical current supply, such as an electrical wall socket. The housing 119 for the power supply and controller portion may be releasably coupled to the applicator panel 100, wherein the connection includes the wires 120 for providing electrical power and control signals between the housing and the applicator panel. The housing may also include user interface devices, such as an control switch(es) 121 and a liquid crystal (LCD) display. The control switch(es) 121 allows the user to input data and control signals into the controller, such as a medicament delivery signal or a code from a drug prescription order to indicate to the controller an amount, delivery rate and composition of medicament to be delivered to the patient. The display 117 may show to the user data generated by the controller identifying the medicament to be dispensed, application instructions, such as a location on the body to which the applicator panel is to be applied and a time period that the applicator panel is to remain on the body.
Medicament stored in the cells 128 (
The applicator panel 100 may be flexible to conform to the body in a manner that is comfortable to the user. The user may self-administer the medicament by applying the applicator panel to his or her skin and over the treatment site, which is the portion of the skin or body to receive the medicament. Before applying the applicator panel, the release liner is removed to expose the front surface 132 of the medicament layer 112. The release liner may be a sheet having a layer of impervious plastic to prevent seepage of the medicament while the applicator panel is in storage and an adhesive to adhere to the front surface of the medicament layer. The exposed front surface 132 of the medicament layer may include a microporation layer 134, such as an array of micro-needles that perforate an upper layer of the skin as the applicator panel is applied to the body. The micro-needles assist in the delivery of medicament to the treatment site. The microporation layer porates the stratum corneum of the skin, including a layer that applies alternating current (AC) or direct current (DC) electroporation, an ultrasound layer, a layer applying RF ablation from small RF electrodes, laser, and other mechanical and electromagnetic means that provide poration of the stratum corneum.
The applicator panel 100 may be used to electrokinetically transport a medicament into the skin and is particularly useful for applying medicament over large wide areas of an individual's face and body. The applicator panel 100 may be used to treat various dermatological conditions, such as eczema, psoriasis, acne, boils, and blemishes, provide anesthesia, or to provide dermal exfoliation. In general, iontophoresis is well suited to the targeted dermal delivery of medicaments, e.g., pharmaceutical drugs. The application of an electric field to the skin underlying the applicator panel enhances the ability of various ionic agents in the medicament or its transport materials to penetrate the skin barrier. Medicament from the medicament cells is delivered to the treatment site by forming an electrical path from the medicament cells, to the treatment site and to electrodes connected to a power supply. Electric current flows from the power supply to an electrode, into the medicament cells, to the skin and treatment site, to another electrode in contact with the skin and back to the power source. As the current flows from the medicament cells, through the skin and into the treatment site, medicament is delivered from the cells to the treatment site.
The medicament layer 112 may include an array of medicament cells 128, such as a honeycomb arrangement of cells. These cells may be each independently controlled or controlled in subset cell groups by the controller. Medicament, and optionally hydration and ion transport materials used in combination with the medicament to assist in electrokinetically delivering the medicament, may be stored in the cells by infusing the medicament in cells, such as the fibers that form the cells and medicament layer. The cells may be arranged in a two-dimensional array in the medicament layer. In this exemplary cellular array, each cell may have a dimension of approximately 2 mm (millimeters) for each edge. The cells may be shaped as squares (2 mm×2 mm), circular discs (2 mm diameter) or other shapes. The cells may be arranged in arrays formed of rows and columns in the layer 112, rows in which the cells are staggered with respect to cells in adjacent rows, concentric circles or in other arrangements.
The cells may be spaced apart from each other by about 2 mm. A network of ribs, e.g., ridges, 136 in the medicament layer 112 may separate the cells and provide a substrate for an adhesive to attach to the release liner and later to the skin. The adhesive may be a zone-coated adhesive applied in a pattern to conform to the network of ribs. The adhesive may form a seal between each cell and the skin and thereby assist in isolating the cell from each other when the applicator is applied to the skin. The network of ribs may be a network of rows and columns of material forming the medicament layer that extend between the cells. Further, the ribs may be embodied as ridges that protrude from the back side of the medicament layer that faces the electrode layer. The front side of the medicament layer may be relatively smooth. In one example, an array of cells 128 separated by a network of ribs 136 provide an open area (between the ribs) of about thirty percent (30%) of the area of the front face 132 of the medicament layer 112 is open area of the cells for drug delivery. The medicament layer(s) may be formed with a conventional flexible non-woven web of fibrous material, such as polyolefins, polyester, nylon, cotton or other synthetic or natural fibers and blends thereof. The layer 112 may have a material property of about 100 g/m2 (grams per meter squared) basis weight and a thickness of approximately 1.5 mm. By way of example, a one centimeter squared (1.0 cm2) pad for an applicator panel would provide about 0.3 cm2 open area of cells for medicament delivery and a volume of about 45 ul (micro liters). The actual liquid volume of medicament delivered by the cells may be about 25 ul.
The electrode layer 122 (Layer 01) may be formed of a flexible substrate 138. The electrode layer is a compliant electrode layer that provides current to discrete and isolated electrodes in the layer. The electrode layer may include as a polyimide film, such as Kapton® offered by DuPont or an equivalent high temperature resistant film. The polyimide film may be perforated to provide multi-axial electrical connections through the substrate between each of the electrodes, on one side of the film, to a distribution circuit, on an opposite side of the film. Alternately, a conductive distribution circuit may be screen printed in a desired pattern on flexible substrates such as textiles, nonwovens and films. By way of example, the film surface around each electrode in the electrode layer may be bordered by a heat seal layer comprised of ethylene vinylacetate, ethylene acrylic acid, or equivalent to which layer is thermally bonded to the electrode layer. On side of the film or substrate opposite to the electrodes, an array of conductive lines may be etched, printed or otherwise generated to form the electrical distribution array 130. On the opposite side of the substrate is formed the array of individual electrodes 126, wherein electrical contacts extend through the substrate to provide conductive contacts between the electrodes and the distribution array.
The flexible substrate 138 may have an electrical distribution array 130 on one side of the substrate and electrodes 126 on the other side of the substrate. The distribution array 130 includes electrical connection contacts 140 to connect the array to the wires 130 leading to the power source and computer controller.
The medicament layer 112 (Layer 02) is attached to the electrode layer 122 by, for example, an adhesive. The medicament layer may be attached to the electrode layer such that the electrodes 126 are aligned with the cells 128 of the medicament layer 112. The medicament layer may be formed of a polyolefin non-woven material that has been thermally patterned through a conventional point-bonding process to create an array of medicament cells 128 and a network of ribs 136. The cells form discrete reservoirs containing medical drug formulations for delivery to the treatment site at the skin. The medicament layer may also be embossed to form the cells 128 and the ribs 136 between the cells.
An adhesive 144 (Layer 03) may be applied to the front surface 132 of the medicament layer to secure to the layer the release liner (Layer 04) 116 or optional microporation layer 134 (Layer 03a), e.g., microneedles. The adhesive may be applied to the portion of the front surface 132 corresponding to the ribs 136 to avoid the cells and potentially blocking the flow of the medicament from the cells to the skin. The adhesive may be a patterned, hypoallergenic adhesive applied through a hot-melt process to the front surface of the medicament layer and particularly to the ribs 136 between the cells of the front surface of the medicament layer. The adhesive 144 may be a high impedance material and, as such, may be used to electrically isolate the cells from one another. Further, the adhesive 144 may serve as a gasket seal between the skin and the cells. The adhesive may be a skin adhesive of variable tack and adhesion may be chosen depending upon the particular needs of the dermal substrate.
The microporation layer 134 is porous and may be applied directly to the front surface of the medicament layer. The medicament flows from the cells, through the microporation layer, e.g., a network of microneedles, and into the skin. The microporation layer 34 may be laminated to the front surface of the medicament layer. The microporation layer 134 may contain an array of microneedles or other microstructures that act to breach the stratum-corneum barrier of the skin and allow greater through-put of iontophoretically delivered actives. The microporation layer may be thermally fused to the overlying medicament layer, e.g., a polyolefin non-woven layer, to create a hermetic seal between the cells.
The layers of the applicator panel 100 are laminated together preferably in the sequence shown in
A combination of anodic and cathodic electrodes and associated medicament cells may be incorporated in an applicator panel to allow a combination of drugs to be included in the application and delivered simultaneously to the treatment site of a patient. The anodic electrodes 152 may be arranged in an outer border region 156 of the panel 150 and the cathodic electrodes 154 may be arranged in a center region 158 of the panel.
Each electrode 152, 154 may be separated from other electrodes in the electrode layer by an insulating, adhesive border. The anodic and cathodic delivery electrodes may be intermingled with anodic electrodes, surrounded by cathodic electrodes or (or the other way around) to provide localized delivery of two or more drugs from the same applicator panel.
From the electrodes and medicament layer, the drug delivery path follows lines of electromagnetic flux from the delivery electrode to the return electrode. The farther away the return electrode is placed from the delivery electrode, the deeper the drug penetrates into the skin. Furthermore, discrete and electrically isolated cells allow the power supply to provide both current polarities to the cells enabling anodic and cathodic delivery at the same time. This in turn allows the delivery of cationic and anionic actives from the same applicator panel and at the same time.
Differing drugs may be best suited for delivery by electrodes having different polarities, e.g., cathodic or anodic. The delivery of the medicaments requiring differing polarity for iontophoretic delivery is addressed by providing cathodic and anodic electrodes in electrode layer as is appropriate for the medicaments to be delivered. The counter electrode may be ‘neutral’ with a positive supply coupled to the cathodic electrodes 154 for those cationic drugs requiring a positive active electrode and a negative supply coupled to anodic electrodes 152 for those anionic drugs requiring a negative electrode.
Electrical current flows from the cathodic or anodic electrode 154, 152, into the skin and returns to the surrounding neutral electrode 162. An annular insulation ring 66 separates the outer neutral 162 and the inner active electrode 164. The depth into the skin to which the current flows and correspondingly to which medicament is delivered into the skin depends primarily on the width of the insulation ring 64. In designing the electrode layer, the width of the insulation ring 64 may be selected to achieve a desired depth of medicament delivery, such as to deliver the medicament to the treatment site.
The panels of electrodes 176, 178 may be segmented into zones of electrodes, wherein each zone activates medicament cells having a different type of medicament than the cells corresponding to the other zones of electrodes. For example, each electrode panel may be segmented into triangular zones 180, 182, 184 and 186 of different grouping of electrodes. The electrodes in each zone are grouped together and are activated as a group. The electrodes of each group/zone are electrically isolated from the electrodes from other zones/groups. Each of the zones of electrodes is superimposed over a corresponding medicament sub-layer of the medicament layer. Each sub-layer may have cells with a drug or other medicine that is different than the drug or medicine in the other sub-layers. When the electrode panel is laminated with a medicament layer 172 having multiple sub-layers, one group of electrodes 180 may be aligned with active medicament cells 174 on a first medicament sub-layer, a second electrode group 182 may aligned with active medicament cells on a second medicament sub-layer, a third electrode group 184 may be aligned with active medicament cells on a third medicament sub-layer, and a fourth electrode group 186 may be aligned with active medicament cells on a fourth medicament sub-layer.
Each zone of electrodes 180, 182, 184 and 186 covers a relatively small surface area on the skin, e.g., about 1 cm2. The current flowing to each zone may be influenced by the contact area between the zone and the skin and the impedance of the contacted skin, e.g., psoriatic skin tissue has lower impedance than does normal skin tissue. A low impedance area of the skin could result in an excessive flow of current that could burn the skin. A current limiting circuit 1000, such as a current limiting diode or constant current source, prevents excessive levels of current flowing to any one of the zones of an electrode panel. Each individual diode or constant current source 1000 may be interrogated by the controller by measuring the voltage at the source resistor. The controller may adjust the current applied to different zones of the electrodes based upon the measured voltages that indicate areas of low impedance.
Each sub-layer 1112, 1114 and 1116 is “addressable” each by a different group of electrodes in the electrode layer. By addressing the sub-layers, medicament may be selectively delivered to the treatment site from just one sub-layer, multiple sub-layers or all sub-layers. Further, the addressing scheme may allow the delivery of medicament to be over a period of time by sequentially addressing the sub-layers over the period of time. The controller may be programmed such that the device delivers one or more the different drugs in the medicament sub-layers, depending on a selection made by the user of drugs to be delivered or depending on an electronically readable prescription prepared by a physician. The housing for the power supply and controller may include a user input (see applicator switch 121 in
The electrodes of the electrode array laminated over the medicament layer 1118 may be connected such that a first group of electrodes are aligned with the first group of cells 1122, a second group of electrodes are aligned with a second group of cells 1126 and a third group of electrodes are aligned with the third group of cells 1128. Each group of electrodes is separately controlled by the controller. The controller may be programmed to apply current to the electrodes corresponding to in just one of the sub-layers 1112, 1114 and 1116, to a plurality but less than all of the sub-layers or to all of the sub-layers. The user may enter through a user input device personal information, such as gender and weight. With that information, the controller may automatically determine the proper dosage of the drug and which of the medicament sub-layers should be activated to deliver the appropriate dosage.
The number of medicament sub-layers in the medicament layer and the number of electrode panels and zones of electrodes in each applicator pad is a matter of design choice. While an applicator pad may be designed such that each electrode and its corresponding medicament cell may be individually controlled by arranging an appropriate distribution circuit. However, the quantity of cells and electrodes in an applicator pad having an area of 120 cm2, such as in a partial facemask applicator, would need to be rather large and may provide an unnecessarily level of fine control over the deliver of medicament. The usage of sub-layers, electrode pads smaller than the applicator pad and electrode zones in each electrode pad allows for a reasonably quantity of control circuits while maintaining a reasonable resolution for managing areas of localized high current density.
While the invention has been described in connection with what is presently considered to be the most practical and preferred embodiment, it is to be understood that the invention is not to be limited to the disclosed embodiment, but on the contrary, is intended to cover various modifications and equivalent arrangements included within the spirit and scope of the appended claims.
This application claims the benefit of U.S. Provisional Patent Application Ser. Nos. 60/944,134 filed Jun. 15, 2007, and 61/033,608, filed Mar. 4, 2008.
| Number | Date | Country | |
|---|---|---|---|
| 61033608 | Mar 2008 | US | |
| 60944134 | Jun 2007 | US |
