EP1931421A1 - Transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist - Google Patents

Transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist

Info

Publication number
EP1931421A1
EP1931421A1 EP06816083A EP06816083A EP1931421A1 EP 1931421 A1 EP1931421 A1 EP 1931421A1 EP 06816083 A EP06816083 A EP 06816083A EP 06816083 A EP06816083 A EP 06816083A EP 1931421 A1 EP1931421 A1 EP 1931421A1
Authority
EP
European Patent Office
Prior art keywords
active agent
opioid antagonist
opioid
active
electrode assembly
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Withdrawn
Application number
EP06816083A
Other languages
German (de)
English (en)
French (fr)
Inventor
Darrick Carter
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
TTI Ellebeau Inc
Original Assignee
TTI Ellebeau Inc
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by TTI Ellebeau Inc filed Critical TTI Ellebeau Inc
Publication of EP1931421A1 publication Critical patent/EP1931421A1/en
Withdrawn legal-status Critical Current

Links

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/18Applying electric currents by contact electrodes
    • A61N1/20Applying electric currents by contact electrodes continuous direct currents
    • A61N1/30Apparatus for iontophoresis, i.e. transfer of media in ionic state by an electromotoric force into the body, or cataphoresis
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/02Details
    • A61N1/04Electrodes
    • A61N1/0404Electrodes for external use
    • A61N1/0408Use-related aspects
    • A61N1/0428Specially adapted for iontophoresis, e.g. AC, DC or including drug reservoirs
    • A61N1/0432Anode and cathode
    • A61N1/044Shape of the electrode
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/435Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
    • A61K31/44Non condensed pyridines; Hydrogenated derivatives thereof
    • A61K31/445Non condensed piperidines, e.g. piperocaine
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/435Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
    • A61K31/47Quinolines; Isoquinolines
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0002Galenical forms characterised by the drug release technique; Application systems commanded by energy
    • A61K9/0009Galenical forms characterised by the drug release technique; Application systems commanded by energy involving or responsive to electricity, magnetism or acoustic waves; Galenical aspects of sonophoresis, iontophoresis, electroporation or electroosmosis
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0012Galenical forms characterised by the site of application
    • A61K9/0019Injectable compositions; Intramuscular, intravenous, arterial, subcutaneous administration; Compositions to be administered through the skin in an invasive manner
    • A61K9/0021Intradermal administration, e.g. through microneedle arrays, needleless injectors
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/02Details
    • A61N1/04Electrodes
    • A61N1/0404Electrodes for external use
    • A61N1/0408Use-related aspects
    • A61N1/0428Specially adapted for iontophoresis, e.g. AC, DC or including drug reservoirs
    • A61N1/0432Anode and cathode
    • A61N1/0436Material of the electrode
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/02Details
    • A61N1/04Electrodes
    • A61N1/0404Electrodes for external use
    • A61N1/0408Use-related aspects
    • A61N1/0428Specially adapted for iontophoresis, e.g. AC, DC or including drug reservoirs
    • A61N1/0444Membrane
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/02Details
    • A61N1/04Electrodes
    • A61N1/0404Electrodes for external use
    • A61N1/0408Use-related aspects
    • A61N1/0428Specially adapted for iontophoresis, e.g. AC, DC or including drug reservoirs
    • A61N1/0448Drug reservoir
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/18Applying electric currents by contact electrodes
    • A61N1/20Applying electric currents by contact electrodes continuous direct currents
    • A61N1/30Apparatus for iontophoresis, i.e. transfer of media in ionic state by an electromotoric force into the body, or cataphoresis
    • A61N1/303Constructional details
    • A61N1/306Arrangements where at least part of the apparatus is introduced into the body
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N1/00Electrotherapy; Circuits therefor
    • A61N1/18Applying electric currents by contact electrodes
    • A61N1/32Applying electric currents by contact electrodes alternating or intermittent currents
    • A61N1/36Applying electric currents by contact electrodes alternating or intermittent currents for stimulation
    • A61N1/36014External stimulators, e.g. with patch electrodes
    • A61N1/36021External stimulators, e.g. with patch electrodes for treatment of pain

Definitions

  • This disclosure generally relates to the field of iontophoresis and, more particularly, to transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist.
  • Iontophoresis employs an electromotive force and/or current to transfer an active agent (e.g., a charged substance, an ionized compound, an ionic a drug, a therapeutic, a bioactive-agent, and the like), to a biological interface (e.g., skin, mucus membrane, and the like), by applying an electrical potential to an electrode proximate an iontophoretic chamber containing a similarly charged active agent and/or its vehicle.
  • an active agent e.g., a charged substance, an ionized compound, an ionic a drug, a therapeutic, a bioactive-agent, and the like
  • a biological interface e.g., skin, mucus membrane, and the like
  • Iontophoresis devices typically include an active electrode assembly and a counter electrode assembly, each coupled to opposite poles or terminals of a power source, for example a chemical battery or an external power source.
  • Each electrode assembly typically includes a respective electrode element to apply an electromotive force and/or current.
  • Such electrode elements often comprise a sacrificial element or compound, for example silver or silver chloride.
  • the active agent may be either cationic or anionic, and the power source may be configured to apply the appropriate voltage polarity based on the polarity of the active agent.
  • Iontophoresis may be advantageously used to enhance or control the delivery rate of the active agent.
  • the active agent may be stored in a reservoir such as a cavity. See e.g., U.S. Patent No. 5,395,310.
  • the active agent may be stored in a reservoir such as a porous structure or a gel.
  • An ion exchange membrane may be positioned to serve as a polarity selective barrier between the active agent reservoir and the biological interface.
  • the membrane typically only permeable with respect to one particular type of ion (e.g., a charged active agent), prevents the back flux of the oppositely charged ions from the skin or mucous membrane.
  • iontophoresis devices Commercial acceptance of iontophoresis devices is dependent on a variety of factors, such as cost to manufacture, shelf life, stability during storage, efficiency and/or timeliness of active agent delivery, biological capability, and/or disposal issues. Furthermore, an iontophoresis device that is able to deliver an active agent and is effective at inducing analgesia or aesthesia in a subject is likewise desirable.
  • the present disclosure is directed to overcome one or more of the shortcomings set forth above, and provide further related advantages.
  • the present disclosure is directed to a self- contained iontophoretic drug delivery system.
  • the system includes at least one active agent reservoir, an active electrode assembly including at least one active electrode element, a power source, and a biocompatible backing.
  • the system is configured for providing transdermal delivery of one or more therapeutic active agents to a biological interface of a subject and inducing analgesia or aesthesia in the subject for a limited period of time.
  • the at least one active agent reservoir includes a pharmaceutical composition for inducing analgesia or anesthesia in the subject.
  • the pharmaceutical composition for inducing analgesia or anesthesia in the subject may include at least one analgesic or anesthetic active agent in combination with at least one opioid antagonist.
  • the at least one active electrode element is operable to provide an electromotive force for driving the pharmaceutical composition (comprising the at least one analgesic or anesthetic active agent in combination with the at least one opioid antagonist) for inducing analgesia or anesthesia in the subject from the at least one active agent reservoir, to the biological interface of the subject.
  • the power source is electrically coupleable to the active electrode assembly, and is operable for supplying an electromotive force to the active electrode assembly.
  • the biocompatible backing is configured to encase the at least one active agent reservoir and the active electrode assembly.
  • the present disclosure is directed to a method for systemic treatment of at least one condition associated with pain, neuropathic pain, acute pain, chronic pain, or cancer pain.
  • the method includes contacting a location on a biological interface with an iontophoretic drug delivery device that includes an active electrode assembly having at least one active agent reservoir.
  • the at least one active agent reservoir includes a pharmaceutical composition including at least a therapeutically effective amount of at least one opioid agonist and at least one opioid antagonist.
  • the method further includes applying a sufficient amount of current to the active electrode assembly for transdermal ⁇ administering a therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the at least one opioid agonist and the at least one opioid antagonist.
  • the present disclosure is directed to a method of treating opiate dependency and/or eliciting a substantially opiate free state in a subject in need thereof.
  • the method includes contacting a location on a biological interface of the subject with an iontophoretic drug delivery operable for iontophoretically delivering a pharmaceutical composition comprising a therapeutically effective amount of at least one opioid antagonist.
  • the method further includes transdermal ⁇ delivering a therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the least one opioid antagonist.
  • the present disclosure is directed to a method of inducing anesthesia, analgesia, or anti-hyperalgesia in a subject.
  • the method includes positioning an active electrode and a counter electrode of an iontophoretic delivery device on a biological interface of the subject.
  • the iontophoretic drug delivery device is operable for iontophoretically delivering a pharmaceutical composition comprising an effective amount of at least one opioid agonist and at least one opioid antagonist.
  • the method further includes iontophoretically delivering an anesthesia inducing, an analgesia inducing, or an anti-hyperalgesia inducing synergistic amount of a pharmaceutical composition comprising at least one opioid agonist and at least one opioid antagonist.
  • the present disclosure is directed to a method of treating opiate agonist-induced narcotic/respiratory depression in a subject in need thereof.
  • the method includes contacting a location on a biological interface of the subject with an iontophoretic drug delivery device operable for iontophoretically delivering a pharmaceutical composition comprising a therapeutically effective amount of at least one opioid antagonist.
  • the method further includes transdermal ⁇ delivering a therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the least one opioid antagonist.
  • Figure 1A is a top, front view of a transdermal drug delivery system according to one illustrated embodiment.
  • Figure 1 B is a top, plan view of a transdermal drug delivery system according to one illustrated embodiment.
  • Figure 2A is a schematic diagram of the iontophoresis device of Figures 1A and 1 B comprising an active and counter electrode assemblies according to one illustrated embodiment.
  • Figure 2B is a schematic diagram of the iontophoresis device of Figure 2A positioned on a biological interface, with an optional outer release liner removed to expose the active agent, according to another illustrated embodiment.
  • Figure 2C is a schematic diagram of the iontophoresis device comprising an active and counter electrode assemblies and a plurality of microneedles according to one illustrated embodiment.
  • Figure 3A is a bottom, front view of a plurality of microneedles in the form of an array according to one illustrated embodiment.
  • Figure 3B is a bottom, front view of a plurality of microneedles in the form of one or more arrays according to another illustrated embodiment.
  • Figure 4 is a flow diagram of a method for systemic treatment of at least one condition associated with pain, neuropathic pain, acute pain, chronic pain, or cancer pain according to one illustrated embodiment.
  • Figure 5 is a flow diagram of a method of inducing anesthesia, analgesia, or anti-hyperalgesia in a subject according to one illustrated embodiment.
  • Figure 6 is a flow diagram of a method of treating opiate dependency and/or eliciting a substantially opiate free state in a subject in need thereof according to one illustrated embodiment.
  • Figure 7 is a flow diagram of a method of treating opiate agonist-induced narcotic/respiratory depression in a subject in need thereof according to one illustrated embodiment.
  • Figure 8 is a Time (min) vs. Drug Transported ( ⁇ g) plot for hydromorphone delivery across human skin according to one illustrated embodiment.
  • Figure 9 is a mass spectrum plot for hydromorphone in serum according to one illustrated embodiment.
  • Figure 10 is a Time (min) vs. Hydromorphone (ng/ml) plot showing hydromorphone levels in test animals following iontophoretic delivery according to one illustrated embodiment.
  • membrane means a boundary, a layer, barrier, or material, which may, or may not be permeable.
  • the term “membrane” may further refer to an interface. Unless specified otherwise, membranes may take the form a solid, liquid, or gel, and may or may not have a distinct lattice, non cross-linked structure, or cross-linked structure.
  • ion selective membrane means a membrane that is substantially selective to ions, passing certain ions while blocking passage of other ions.
  • An ion selective membrane for example, may take the form of a charge selective membrane, or may take the form of a semi-permeable membrane.
  • charge selective membrane means a membrane that substantially passes and/or substantially blocks ions based primarily on the polarity or charge carried by the ion.
  • Charge selective membranes are typically referred to as ion exchange membranes, and these terms are used interchangeably herein and in the claims.
  • Charge selective or ion exchange membranes may take the form of a cation exchange membrane, an anion exchange membrane, and/or a bipolar membrane.
  • a cation exchange membrane substantially permits the passage of cations and substantially blocks anions. Examples of commercially available cation exchange membranes include those available under the designators NEOSEPTA, CM-1 , CM-2, CMX, CMS, and CMB from Tokuyama Co., Ltd.
  • an anion exchange membrane substantially permits the passage of anions and substantially blocks cations.
  • examples of commercially available anion exchange membranes include those available under the designators NEOSEPTA, AM-1 , AM-3, AMX, AHA, ACH, and ACS also from Tokuyama Co., Ltd.
  • bipolar membrane means a membrane that is selective to two different charges or polarities.
  • a bipolar membrane may take the form of a unitary membrane structure, a multiple membrane structure, or a laminate.
  • the unitary membrane structure may include a first portion including cation ion exchange materials or groups and a second portion opposed to the first portion, including anion ion exchange materials or groups.
  • the multiple membrane structure e.g., two film structure
  • the cation and anion exchange membranes initially start as distinct structures, and may or may not retain their distinctiveness in the structure of the resulting bipolar membrane.
  • the term "semi-permeable membrane” means a membrane that is substantially selective based on a size or molecular weight of the ion.
  • a semi-permeable membrane substantially passes ions of a first molecular weight or size, while substantially blocking passage of ions of a second molecular weight or size, greater than the first molecular weight or size.
  • a semi-permeable membrane may permit the passage of some molecules at a first rate, and some other molecules at a second rate different from the first.
  • the "semi-permeable membrane” may take the form of a selectively permeable membrane allowing only certain selective molecules to pass through it.
  • porous membrane means a membrane that is not substantially selective with respect to ions at issue.
  • a porous membrane is one that is not substantially selective based on polarity, and not substantially selective based on the molecular weight or size of a subject element or compound.
  • the term "gel matrix" means a type of reservoir, which takes the form of a three dimensional network, a colloidal suspension of a liquid in a solid, a semi-solid, a cross-linked gel, a non cross-linked gel, a jelly-like state, and the like.
  • the gel matrix may result from a three dimensional network of entangled macromolecules (e.g., cylindrical micelles).
  • a gel matrix may include hydrogels, organogels, and the like.
  • Hydrogels refer to three-dimensional network of, for example, cross-linked hydrophilic polymers in the form of a gel and substantially composed of water. Hydrogels may have a net positive or negative charge, or may be neutral.
  • a reservoir means any form of mechanism to retain an element, compound, pharmaceutical composition, active agent, and the like, in a liquid state, solid state, gaseous state, mixed state and/or transitional state.
  • a reservoir may include one or more cavities formed by a structure, and may include one or more ion exchange membranes, semipermeable membranes, porous membranes and/or gels if such are capable of at least temporarily retaining an element or compound.
  • a reservoir serves to retain a biologically active agent prior to the discharge of such agent by electromotive force and/or current into the biological interface.
  • a reservoir may also retain an electrolyte solution.
  • active agent refers to a compound, molecule, or treatment that elicits a biological response from any host, animal, vertebrate, or invertebrate, including for example fish, mammals, amphibians, reptiles, birds, and humans.
  • active agents include therapeutic agents, pharmaceutical agents, pharmaceuticals (e.g., a drug, a therapeutic compound, pharmaceutical salts, and the like) non-pharmaceuticals (e.g., cosmetic substance, and the like), a vaccine, an immunological agent, a local or general anesthetic or painkiller, an antigen or a protein or peptide such as insulin, a chemotherapy agent, an anti-tumor agent.
  • the term "active agent” further refers to the active agent, as well as its pharmacologically active salts, pharmaceutically acceptable salts, prodrugs, metabolites, analogs, and the like.
  • the active agent includes at least one ionic, cationic, ionizeable, and/or neutral therapeutic drug and/or pharmaceutical acceptable salts thereof.
  • the active agent may include one or more "cationic active agents" that are positively charged, and/or are capable of forming positive charges in aqueous media.
  • many biologically active agents have functional groups that are readily convertible to a positive ion or can dissociate into a positively charged ion and a counter ion in an aqueous medium.
  • active agents may be polarized or polarizable, that is exhibiting a polarity at one portion relative to another portion.
  • an active agent having an amino group can typically take the form an ammonium salt in solid state and dissociates into a free ammonium ion (NH4+) in an aqueous medium of appropriate pH.
  • active agent may also refer to electrically neutral agents, molecules, or compounds capable of being delivered via electro- osmotic flow.
  • the electrically neutral agents are typically carried by the flow of, for example, a solvent during electrophoresis. Selection of the suitable active agents is therefore within the knowledge of one skilled in the relevant art.
  • one or more active agents may be selected from analgesics, anesthetics, anesthetics vaccines, antibiotics, adjuvants, immunological adjuvants, immunogens, tolerogens, allergens, toll-like receptor agonists, toll-like receptor antagonists, immuno-adjuvants, immuno-modulators, immuno-response agents, immuno-stimulators, specific immuno-stimulators, non-specific immuno-stimulators, and immunosuppressants, or combinations thereof.
  • Non-limiting examples of such active agents include lidocaine, articaine, and others of the -caine class; morphine, hydromorphone, fentanyl, oxycodone, hydrocodone, buprenorphine, methadone, and similar opioid agonists; sumatriptan succinate, zolmitriptan, naratriptan HCI, rizatriptan benzoate, almotriptan malate, frovatriptan succinate and other 5- hydroxytryptaminei receptor subtype agonists; resiquimod, imiquidmod, and similar TLR 7 and 8 agonists and antagonists; domperidone, granisetron hydrochloride, ondansetron and such anti-emetic drugs; Zolpidem tartrate and similar sleep inducing agents; L-dopa and other anti-Parkinson's medications; aripiprazole, olanzapine, quetiapine, risperidone,
  • anesthetic active agents or pain killers include ambucaine, amethocaine, isobutyl p-aminobenzoate, amolanone, amoxecaine, amylocaine, aptocaine, azacaine, bencaine, benoxinate, benzocaine, N,N-dimethylalanylbenzocaine, N 1 N- dimethylglycylbenzocaine, glycylbenzocaine, beta-ad renoceptor antagonists betoxycaine, bumecaine, bupivicaine, levobupivicaine, butacaine, butamben, butanilicaine, butethamine, butoxycaine, metabutoxycaine, carbizocaine, carticaine, centbucridine, cepacaine, cetacaine, chloroprocaine, cocaethylene, cocaine, pseudococaine, cyclomethycaine, dibucaine, dimethisoquin
  • subject generally refers to any host, animal, vertebrate, or invertebrate, and includes fish, mammals, amphibians, reptiles, birds, and particularly humans.
  • agonist refers to a compound that can combine with a receptor (e.g., an opioid receptor, Toll- like receptor, and the like) to produce a cellular response.
  • a receptor e.g., an opioid receptor, Toll- like receptor, and the like
  • An agonist may be a ligand that directly binds to the receptor.
  • an agonist may combine with a receptor indirectly by forming a complex with another molecule that directly binds the receptor, or otherwise resulting in the modification of a compound so that it directly binds to the receptor.
  • an antagonist refers to a compound that can combine with a receptor (e.g., an opioid receptor, a Toll-like receptor, and the like) to inhibit a cellular response.
  • a receptor e.g., an opioid receptor, a Toll-like receptor, and the like
  • An antagonist may be a ligand that directly binds to the receptor.
  • an antagonist may combine with a receptor indirectly by forming a complex with another molecule that directly binds to the receptor, or otherwise results in the modification of a compound so that it directly binds to the receptor.
  • the term "effective amount” or “therapeutically effective amount” includes an amount effective at dosages and for periods of time necessary, to achieve the desired result.
  • the effective amount of a composition containing a pharmaceutical agent may vary according to factors such as the disease state, age, gender, and weight of the subject.
  • analgesic refers to an agent that lessens, alleviates, reduces, relieves, or extinguishes a neural sensation in an area of a subject's body.
  • the neural sensation relates to pain, in other aspects the neural sensation relates to discomfort, itching, burning, irritation, tingling, "crawling," tension, temperature fluctuations (such as fever), inflammation, aching, or other neural sensations.
  • the term "anesthetic” refers to an agent that produces a reversible loss of sensation in an area of a subject's body.
  • the anesthetic is considered to be a "local anesthetic" in that it produces a loss of sensation only in one particular area of a subject's body.
  • agents may act as both an analgesic and an anesthetic, depending on the circumstances and other variables including but not limited to dosage, method of delivery, medical condition or treatment, and an individual subject's genetic makeup. Additionally, agents that are typically used for other purposes may possess local anesthetic or membrane stabilizing properties under certain circumstances or under particular conditions.
  • immunogen refers to any agent that elicits an immune response.
  • immunogen include, but are not limited to natural or synthetic (including modified) peptides, proteins, lipids, oligonucleotides (RNA, DNA, etc.), chemicals, or other agents.
  • allergen refers to any agent that elicits an allergic response.
  • allergens include but are not limited to chemicals and plants, drugs (such as antibiotics, serums), foods (such as milk, wheat, eggs, etc), bacteria, viruses, other parasites, inhalants (dust, pollen, perfume, smoke), and/or physical agents (heat, light, friction, radiation).
  • drugs such as antibiotics, serums
  • foods such as milk, wheat, eggs, etc
  • bacteria viruses, other parasites
  • inhalants dust, pollen, perfume, smoke
  • physical agents heat, light, friction, radiation
  • the term "adjuvant” and any derivations thereof refers to an agent that modifies the effect of another agent while having few, if any, direct effect when given by itself.
  • an adjuvant may increase the potency or efficacy of a pharmaceutical, or an adjuvant may alter or affect an immune response.
  • opioid generally refers to any agent that binds to and/or interacts with opioid receptors.
  • opioid classes examples include endogenous opioid peptides, opium alkaloids (e.g., morphine, codeine, and the like), semi-synthetic opioids (e.g., heroin, oxycodone and the like), synthetic opioids (e.g., buprenorphinemeperidine, fentanyl, morphinan, benzomorphan derivatives, and the like), as well as opioids that have structures unrelated to the opium alkaioids (e.g., pethidine, methadone, and the like).
  • opioids include endogenous opioid peptides, opium alkaloids (e.g., morphine, codeine, and the like), semi-synthetic opioids (e.g., heroin, oxycodone and the like), synthetic opioids (e.g., buprenorphinemeperidine, fentanyl, morphinan, benzomorphan derivatives, and the like), as well as opioids that have structures unrelated to the
  • the terms "vehicle,” “carrier,” “pharmaceutically vehicle,” “pharmaceutically carrier,” “pharmaceutically acceptable vehicle,” or “pharmaceutically acceptable carrier” may be used interchangeably, and refer to pharmaceutically acceptable solid or liquid, diluting or encapsulating, filling or carrying agents, which are usually employed in pharmaceutical industry for making pharmaceutical compositions.
  • vehicles include any liquid, gel, salve, cream, solvent, diluent, fluid ointment base, vesicle, liposomes, nisomes, ethasomes, transfersomes, virosornes, non ionic surfactant vesicles, phospholipid surfactant vesicles, micelle, and the like, that is suitable for use in contacting a subject.
  • the pharmaceutical vehicle may refer to a composition that includes and/or delivers a pharmacologically active agent, but is generally considered to be otherwise pharmacologically inactive.
  • the pharmaceutical vehicle may have some therapeutic effect when applied to a site such as a mucous membrane or skin, by providing, for example, protection to the site of application from conditions such as injury, further injury, or exposure to elements. Accordingly, in some embodiments, the pharmaceutical vehicle may be used for protection without a pharmacological agent in the formulation.
  • FIGS 1A and 1 B show an exemplary iontophoretic drug delivery system 6 for delivering of one or more active agents to a subject.
  • the system 6 includes an iontophoresis device 8 including active and counter electrode assemblies 12, 14, respectively, and a power source 16.
  • the active and counter electrode assemblies 12, 14, are electrically coupleable to the power source 16 to supply an active agent contained in the active electrode assembly 12, via iontophoresis, to a biological interface 18 (e.g., a portion of skin or mucous membrane).
  • the iontophoresis device 8 may optionally include a biocompatible backing 19. In some embodiments, the biocompatible backing 19 encases the iontophoresis devices 8.
  • the biocompatible backing 19 physically couples the iontophoresis device 8 to the biological interface 18 of the subject.
  • the system 6 is configured for providing transdermal delivery of one or more therapeutic active agents to a biological interface of a subject and inducing analgesia or aesthesia in the subject for a limited period of time.
  • the active electrode assembly 12 may further comprise, from an interior 20 to an exterior 22 of the active electrode assembly 12: an active electrode element 24, an electrolyte reservoir 26 storing an electrolyte 28, an inner ion selective membrane 30, one or more inner active agent reservoirs 34, storing one or more active agents 36, an optional outermost ion selective membrane 38 that optionally caches additional active agents 40, and an optional further active agent 42 carried by an outer surface 44 of the outermost ion selective membrane 38.
  • the active electrode assembly 12 may further comprise an optional outer release liner 46.
  • the one or more active agent reservoirs 34 are loadable with a vehicle and/or pharmaceutical composition for transporting, delivering, encapsulating, and/or carrying the one or more active agents 36, 40, 42.
  • at least one active agent reservoir 34 includes a pharmaceutical composition for inducing analgesia or anesthesia in the subject.
  • the pharmaceutical composition for inducing analgesia or anesthesia in the subject may include at least one analgesic or anesthetic active agent in combination with at least one opioid antagonist.
  • the pharmaceutical composition includes at least a therapeutically effective one or more active agents 36, 40, 42 selected from one or more opioid agonist.
  • the pharmaceutical composition includes at least a therapeutically effective one or more active agents 36, 40, 42 selected from one or more opioid antagonist. In yet some further embodiments, the pharmaceutical composition includes a therapeutically effective amount of at least one opioid agonist and at least one opioid antagonist.
  • the at least one opioid agonist may be selected from endogenous opioid peptides, opium alkaloids, semi-synthetic opioids, and fully synthetic opioids, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof.
  • the at least one opioid agonist is selected from (5 ⁇ ,7 ⁇ ,8 ⁇ -(-)-N-methyl-N-[7-(1-pyrrolidinyl)-1- oxaspiro(4, 5)dec-8-yl]-benzene-acetamide (U69,593)), [D-Ala2, N-Me- Phe4,Gly5-ol]enkephalin (DAMGO), delta-([D-Pen2,D-Pen5]-enkephalin (DPDPE)), buprenorphine, codeine, dextromoramide, dihydrocodeine, fentanyl, heroin, hydrocodone, hydromorphone, meperidine, methadone, morphine, nicomorph
  • the at least one opioid antagonist may be selected from [(-)- (1 R,5R,9R)-5,9-diethyl-2-(3-furyl-methyl)-2 l -hydroxy-6,7-benzomorphan] (MR2266), [allyl]2-tyr-alpha-amino-isobutyric acid (Aib)-Aib-Phe-Leu-OH (ICI-174864), 4-(3-hydroxyphenyl)-34-dimethyl-alpha-phenyl-1 - piperidinepropanol (LY117413), 6 ⁇ -Naltrexol, 7-Benzylidenenaltrexone (BNTX), b-funaltrexamine (b-FNA), cyclazocine, cyclorphan, dezocine, diprenorphine, levorphanol, meptazinol, methiodide, methylnaltrexone, nalide, nalmefene, nalmex
  • the at least one opioid antagonist is selected from hydromorphone, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof; and the at least one opioid antagonist is selected from naloxone, naltrexone, nalmefene, naloxonazine, NTI, nor-BNI, LY25506, LY9935, LY255582, and LY117413, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof.
  • the at least one opioid antagonist is selected from hydromorphone, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof; and the at least one opioid antagonist is selected from naloxone, naltrexone, 6 ⁇ -naltrexol, nalmefene, and naloxonazine, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof.
  • the at least one opioid antagonist is selected from palladone, Palladone® SR, Dilaudid® and hydromorphone hydrochloride; and the at least one opioid antagonist is selected from Narcan®, Trexan®, Revex®, Nubian®, nalaxone hydrochloride, naltrexone hydrochloride, nalmefene hydrochloride, and nulbuphine hydrochloride.
  • the least one opioid agonist and at least one opioid antagonist are present in synergistic anti- hyperalgesic effective amounts.
  • the pharmaceutical composition may further comprises at least one active agent selected from vaccines, antibiotics, adjuvants, immunological adjuvants, immunogens, tolerogens, allergens, toll-like receptor agonists, and toll-like receptor antagonists, immuno-adjuvants, immuno-modulators, immuno-response agents, immuno-stimulators, specific immuno-stimulators, non-specific immuno-stimulators, and immunosuppressants, or combinations thereof.
  • active agent selected from vaccines, antibiotics, adjuvants, immunological adjuvants, immunogens, tolerogens, allergens, toll-like receptor agonists, and toll-like receptor antagonists, immuno-adjuvants, immuno-modulators, immuno-response agents, immuno-stimulators, specific immuno-stimulators, non-specific immuno-stimulators, and immunosuppressants, or combinations thereof.
  • the pharmaceutical composition may include a therapeutically effective amount of at least one opioid agonist, at least one opioid antagonist, and at least one active agent selected from an antihistamine drug, a vasoconstrictor drug (e.g., epinephrine, adrenaline, norepinephrine, and the like), a steroid, and the like.
  • an antihistamine drug e.g., epinephrine, adrenaline, norepinephrine, and the like
  • a steroid e.g., a steroid, and the like.
  • the pharmaceutical composition may be useful for systemic treatment of at least one condition associated with pain, neuropathic pain, acute pain, chronic pain, or cancer pain.
  • the at least one condition associated with pain, neuropathic pain, acute pain, chronic pain, or cancer pain includes cancer; chemotherapy; alcoholism; amputation; a back, leg, or hip problem; diabetes; a facial nerve problem; an HIV infection or AIDS; multiple sclerosis; spinal surgery; opiate induced narcotic/respiratory depression; or detoxification of opiate-dependency.
  • nociceptors respond to a variety of stimuli including burns, cuts, infection, chemical changes, pressure, and many other sensations that are interpreted as pain by a biological subject.
  • nociceptors respond to a variety of stimuli including burns, cuts, infection, chemical changes, pressure, and many other sensations that are interpreted as pain by a biological subject.
  • the tenderness and pain associated with the injury or other stimulus typically dissipates.
  • neuropathic pain is certainly real, the cause may be difficult to determine.
  • Neuropathic pain is often described as shooting, stabbing, burning or searing. As used herein and in the appended claims, such pain is termed “neuropathic pain.” Conditions with which neuropathic pain may be commonly associated include, but are not limited to, shingles (herpes zoster virus infection; post-herpetic pain); cancer; chemotherapy; alcoholism; amputation (e.g., phantom limb syndrome); back, leg, and hip problems (sciatica); diabetes; facial nerve problems (trigeminal neuralgia); HIV infection or AIDS; multiple sclerosis; and spinal surgery. Chronic pain may also occur without any know injury or disease. For example, subjects may experience pain with no obvious injury or other stimulus.
  • a treatment may include chronic ongoing administration of drugs or other active agents that ameliorate the pain, such as analgesic active agents, anesthetic active agents and/or painkillers.
  • drugs or other active agents may be administered passively by application of one or more devices 8 to a biological interface 18 (e.g., skin or mucous membrane) at or near areas where a subject is experiencing neuropathic pain.
  • the one or more agents are deliverable from the device 8 onto or into the biological interface 18 to exert its effect in alleviating the pain.
  • one or more agents may advantageously be actively administered by a device 8 through a biological interface 18 and tissue into the systemic circulation. Accordingly, the agent may exert its therapeutic effect locally and more broadly.
  • one or more active agents are administered through area portion of a biological interface from which they may enter the blood stream and be carried systemically into a capillary bed or other vasculature of an area experiencing pain (e.g., neuropathic pain and the like).
  • the device for active administration of an anesthetic or painkiller is an iontophoretic device, as described in detail herein.
  • systemic circulation typically refers to movement of blood through the portion of a cardiovascular system and/or circulatory system that carries oxygenated blood from the heart to the body and oxygen-depleted blood from the body back to the heart.
  • blood may flow through vessels that include, but are not necessarily limited to, arteries, arterioles, capillaries, venules, and veins.
  • Systemic circulation as used herein and in the claims, may also refer to movement of fluids through a lymphatic system, which collects lymph from tissues and returns it to the cardiovascular circulatory system. Lymph typically originates from blood plasma that leaks from the cardiovascular system into spaces within tissue.
  • Systemic delivery refers to movement of compounds, such as active agents, from one location to another via systemic circulation.
  • the active electrode assembly 12 of the iontophoretic delivery device 8 may further comprise an optional inner sealing liner (not shown) between two layers of the active electrode assembly 12, for example, between the inner ion selective membrane 30 and the inner active agent reservoir 34.
  • the inner sealing liner if present, would be removed prior to application of the iontophoretic device to the biological surface 18.
  • the system 6 takes the form of a self- contained iontophoretic drug delivery system.
  • the system 6 includes at least one active agent reservoir 34, an active electrode assembly 12 including at least one active electrode element 24, and a power source 16.
  • the at least one active agent reservoir 34 includes a pharmaceutical composition for inducing analgesia or anesthesia in the subject.
  • the pharmaceutical composition for inducing analgesia or anesthesia in the subject may include at least one analgesic or anesthetic active agent in combination with at least one opioid antagonist.
  • the active electrode element 24 is electrically coupled to a first pole 16a of the power source 16 and positioned in the active electrode assembly 12 to apply an electromotive force to transport the active agent 36, 40, 42 via various other components of the active electrode assembly 12.
  • the magnitude of the applied electromotive force is generally that required to deliver the one or more active agents according to a therapeutic effective dosage protocol. In some embodiments, the magnitude is selected such that it meets or exceeds the ordinary use operating electrochemical potential of the iontophoresis delivery device 8.
  • the at least one active electrode element 24 is operable to provide an electromotive force for driving the pharmaceutical composition (comprising the at least one analgesic or anesthetic active agent in combination with the at least one opioid antagonist) for inducing analgesia or anesthesia in the subject from the at least one active agent reservoir 34, to the biological interface 18 of the subject.
  • the active electrode element 24 may take a variety of forms.
  • the active electrode element 24 may advantageously take the form of a carbon-based active electrode element.
  • a carbon-based active electrode element Such may, for example, comprise multiple layers, for example a polymer matrix comprising carbon and a conductive sheet comprising carbon fiber or carbon fiber paper, such as that described in commonly assigned pending Japanese patent application 2004/317317, filed October 29, 2004.
  • the carbon-based electrodes are inert electrodes in that they do not themselves undergo or participate in electrochemical reactions.
  • an inert electrode distributes current through the oxidation or reduction of a chemical species capable of accepting or donating an electron at the potential applied to the system, (e.g., generating ions by either reduction or oxidation of water).
  • Additional examples of inert electrodes include stainless steel, gold, platinum, capacitive carbon, or graphite.
  • an active electrode of sacrificial conductive material such as a chemical compound or amalgam, may also be used.
  • a sacrificial electrode does not cause electrolysis of water, but would itself be oxidized or reduced.
  • a metal/metal salt may be employed for an anode. In such case, the metal would oxidize to metal ions, which would then be precipitated as an insoluble salt.
  • An example of such anode includes an Ag/AgCI electrode. The reverse reaction takes place at the cathode in which the metal ion is reduced and the corresponding anion is released from the surface of the electrode.
  • the electrolyte reservoir 26 may take a variety of forms including any structure capable of retaining electrolyte 28, and in some embodiments may even be the electrolyte 28 itself, for example, where the electrolyte 28 is in a gel, semi-solid or solid form.
  • the electrolyte reservoir 26 may take the form of a pouch or other receptacle, a membrane with pores, cavities, or interstices, particularly where the electrolyte 28 is a liquid.
  • the electrolyte 28 comprises ionic or ionizable components in an aqueous medium, which can act to conduct current towards or away from the active electrode element.
  • Suitable electrolytes include, for example, aqueous solutions of salts.
  • the electrolyte 28 includes salts of physiological ions, such as, sodium, potassium, chloride, and phosphate.
  • the electrolyte 28 may further comprise an anti-oxidant.
  • the anti-oxidant is selected from anti-oxidants that have a lower potential than that of, for example, water. In such embodiments, the selected anti-oxidant is consumed rather than having the hydrolysis of water occur.
  • an oxidized form of the anti-oxidant is used at the cathode and a reduced form of the anti-oxidant is used at the anode.
  • biologically compatible anti-oxidants include, but are not limited to, ascorbic acid (vitamin C), tocopherol (vitamin E), or sodium citrate.
  • the electrolyte 28 may take the form of an aqueous solution housed within a reservoir 26, or in the form of a dispersion in a hydrogel or hydrophilic polymer capable of retaining substantial amount of water.
  • a suitable electrolyte may take the form of a solution of 0.5 M disodium fumarate: 0.5 M polyacrylic acid: 0.15 M anti-oxidant.
  • the inner ion selective membrane 30 is generally positioned to separate the electrolyte 28 and the inner active agent reservoir 34, if such a membrane is included within the device.
  • the inner ion selective membrane 30 may take the form of a charge selective membrane.
  • the inner ion selective membrane 30 may take the form of an anion exchange membrane, selective to substantially pass anions and substantially block cations.
  • the inner ion selective membrane 30 may advantageously prevent transfer of undesirable elements or compounds between the electrolyte 28 and the inner active agent reservoir 34.
  • the inner ion selective membrane 30 may prevent or inhibit the transfer of sodium (Na+) ions from the electrolyte 28, thereby increasing the transfer rate and/or biological compatibility of the iontophoresis device 8.
  • the inner active agent reservoir 34 is generally positioned between the inner ion selective membrane 30 and the outermost ion selective membrane 38.
  • the inner active agent reservoir 34 may take a variety of forms including any structure capable of temporarily retaining active agent 36.
  • the inner active agent reservoir 34 may take the form of a pouch or other receptacle, a membrane with pores, cavities, or interstices, particularly where the active agent 36 is a liquid.
  • the inner active agent reservoir 34 further may comprise a gel matrix.
  • an outermost ion selective membrane 38 is positioned generally opposed across the active electrode assembly 12 from the active electrode element 24.
  • the outermost membrane 38 may, as in the embodiment illustrated in Figures 2A and 2B, take the form of an ion exchange membrane having pores 48 (only one called out in Figures 2A and 2B for sake of clarity of illustration) of the ion selective membrane 38 including ion exchange material or groups 50 (only three called out in Figures 2A and 2B for sake of clarity of illustration).
  • the ion exchange material or groups 50 selectively substantially passes ions of the same polarity as active agent 36, 40, while substantially blocking ions of the opposite polarity.
  • the outermost ion exchange membrane 38 is charge selective.
  • the outermost ion selective membrane 38 may take the form of a cation exchange membrane, thus allowing the passage of the cationic active agent while blocking the back flux of the anions present in the biological interface, such as skin.
  • the outermost ion selective membrane 38 may optionally cache active agent 40.
  • the ion exchange groups or material 50 temporarily retains ions of the same polarity as the polarity of the active agent in the absence of electromotive force or current and substantially releases those ions when replaced with substitutive ions of like polarity or charge under the influence of an electromotive force or current.
  • the outermost ion selective membrane 38 may take the form of semi-permeable or microporous membrane which is selective by size.
  • such a semi-permeable membrane may advantageously cache active agent 40, for example by employing the removably releasable outer release liner to retain the active agent 40 until the outer release liner is removed prior to use.
  • the outermost ion selective membrane 38 may be optionally preloaded with the additional active agent 40, such as ionized or ionizable drugs or therapeutic agents and/or polarized or polarizable drugs or therapeutic agents. Where the outermost ion selective membrane 38 is an ion exchange membrane, a substantial amount of active agent 40 may bond to ion exchange groups 50 in the pores, cavities or interstices 48 of the outermost ion selective membrane 38.
  • active agent 40 such as ionized or ionizable drugs or therapeutic agents and/or polarized or polarizable drugs or therapeutic agents.
  • the active agent 42 that fails to bond to the ion exchange groups of material 50 may adhere to the outer surface 44 of the outermost ion selective membrane 38 as the further active agent 42.
  • the further active agent 42 may be positively deposited on and/or adhered to at least a portion of the outer surface 44 of the outermost ion selective membrane 38, for example, by spraying, flooding, coating, electrostatically, vapor deposition, and/or otherwise.
  • the further active agent 42 may sufficiently cover the outer surface 44 and/or be of sufficient thickness to form a distinct layer 52.
  • the further active agent 42 may not be sufficient in volume, thickness, or coverage as to constitute a layer in a conventional sense of such term.
  • the active agent 42 may be deposited in a variety of highly concentrated forms such as, for example, solid form, nearly saturated solution form, or gel form. If in solid form, a source of hydration may be provided, either integrated into the active electrode assembly 12, or applied from the exterior thereof just prior to use.
  • the active agent 36, additional active agent 40, and/or further active agent 42 may be identical or similar compositions or elements. In other embodiments, the active agent 36, additional active agent 40, and/or further active agent 42 may be different compositions or elements from one another.
  • a first type of active agent may be stored in the inner active agent reservoir 34, while a second type of active agent may be cached in the outermost ion selective membrane 38. In such an embodiment, either the first type or the second type of active agent may be deposited on the outer surface 44 of the outermost ion selective membrane 38 as the further active agent 42. Alternatively, a mix of the first and the second types of active agent may be deposited on the outer surface 44 of the outermost ion selective membrane 38 as the further active agent 42.
  • a third type of active agent composition or element may be deposited on the outer surface 44 of the outermost ion selective membrane 38 as the further active agent 42.
  • a first type of active agent may be stored in the inner active agent reservoir 34 as the active agent 36 and cached in the outermost ion selective membrane 38 as the additional active agent 40, while a second type of active agent may be deposited on the outer surface 44 of the outermost ion selective membrane 38 as the further active agent 42.
  • the active agents 36, 40, 42 will all be of common polarity to prevent the active agents 36, 40, 42 from competing with one another. Other combinations are possible.
  • the outer release liner may generally be positioned overlying or covering further active agent 42 carried by the outer surface 44 of the outermost ion selective membrane 38.
  • the outer release liner may protect the further active agent 42 and/or outermost ion selective membrane 38 during storage, prior to application of an electromotive force or current.
  • the outer release liner may be a selectively releasable liner made of waterproof material, such as release liners commonly associated with pressure sensitive adhesives.
  • An interface-coupling medium (not shown) may be employed between the electrode assembly and the biological interface 18.
  • the interface-coupling medium may take, for example, the form of an adhesive and/or gel.
  • the gel may take, for the form of a hydrating gel. Selection of suitable bioadhesive gels is within the knowledge of one skilled in the relevant art.
  • the counter electrode assembly 14 comprises, from an interior 64 to an exterior 66 of the counter electrode assembly 14: a counter electrode element 68, an electrolyte reservoir 70 storing an electrolyte 72, an inner ion selective membrane 74, an optional buffer reservoir 76 storing buffer material 78, an optional outermost ion selective membrane 80, and an optional outer release liner (not shown).
  • the counter electrode element 68 is electrically coupled to a second pole 16b of the power source 16, the second pole 16b having an opposite polarity to the first pole 16a.
  • the counter electrode element 68 is an inert electrode.
  • the counter electrode element 68 may take the form of the carbon-based electrode element discussed above.
  • the electrolyte reservoir 70 may take a variety of forms including any structure capable of retaining electrolyte 72, and in some embodiments may even be the electrolyte 72 itself, for example, where the electrolyte 72 is in a gel, semi-solid or solid form.
  • the electrolyte reservoir 70 may take the form of a pouch or other receptacle, or a membrane with pores, cavities, or interstices, particularly where the electrolyte 72 is a liquid.
  • the electrolyte 72 is generally positioned between the counter electrode element 68 and the outermost ion selective membrane 80, proximate the counter electrode element 68. As described above, the electrolyte 72 may provide ions or donate charges to prevent or inhibit the formation of gas bubbles (e.g., hydrogen or oxygen, depending on the polarity of the electrode) on the counter electrode element 68 and may prevent or inhibit the formation of acids or bases or neutralize the same, which may enhance efficiency and/or reduce the potential for irritation of the biological interface 18.
  • gas bubbles e.g., hydrogen or oxygen, depending on the polarity of the electrode
  • the inner ion selective membrane 74 is positioned between and/or to separate, the electrolyte 72 from the buffer material 78.
  • the inner ion selective membrane 74 may take the form of a charge selective membrane, such as the illustrated ion exchange membrane that substantially allows passage of ions of a first polarity or charge while substantially blocking passage of ions or charge of a second, opposite polarity.
  • the inner ion selective membrane 74 will typically pass ions of opposite polarity or charge to those passed by the outermost ion selective membrane 80 while substantially blocking ions of like polarity or charge.
  • the inner ion selective membrane 74 may take the form of a semi-permeable or microporous membrane that is selective based on size.
  • the inner ion selective membrane 74 may prevent transfer of undesirable elements or compounds into the buffer material 78.
  • the inner ion selective membrane 74 may prevent or inhibit the transfer of hydroxy (OH-) or chloride (Cl-) ions from the electrolyte 72 into the buffer material 78.
  • the optional buffer reservoir 76 is generally disposed between the electrolyte reservoir and the outermost ion selective membrane 80.
  • the buffer reservoir 76 may take a variety of forms capable of temporarily retaining the buffer material 78.
  • the buffer reservoir 76 may take the form of a cavity, a porous membrane, or a gel.
  • the buffer material 78 may supply ions for transfer through the outermost ion selective membrane 42 to the biological interface 18. Consequently, the buffer material 78 may comprise, for example, a salt (e.g., NaCI).
  • the outermost ion selective membrane 80 of the counter electrode assembly 14 may take a variety of forms.
  • the outermost ion selective membrane 80 may take the form of a charge selective ion exchange membrane.
  • the outermost ion selective membrane 80 of the counter electrode assembly 14 is selective to ions with a charge or polarity opposite to that of the outermost ion selective membrane 38 of the active electrode assembly 12.
  • the outermost ion selective membrane 80 is therefore an anion exchange membrane, which substantially passes anions and blocks cations, thereby prevents the back flux of the cations from the biological interface.
  • suitable ion exchange membranes include the previously discussed membranes.
  • the outermost ion selective membrane 80 may take the form of a semi-permeable membrane that substantially passes and/or blocks ions based on size or molecular weight of the ion.
  • the outer release liner (not shown) may generally be positioned overlying or covering an outer surface 84 of the outermost ion selective membrane 80.
  • the outer release liner may protect the outermost ion selective membrane 80 during storage, prior to application of an electromotive force or current.
  • the outer release liner may be a selectively releasable liner made of waterproof material, such as release liners commonly associated with pressure sensitive adhesives.
  • the outer release liner may be coextensive with the outer release liner (not shown) of the active electrode assembly 12.
  • the iontophoresis device 8 may further comprise an inert molding material 86 adjacent exposed sides of the various other structures forming the active and counter electrode assemblies 12, 14.
  • the molding material 86 may advantageously provide environmental protection to the various structures of the active and counter electrode assemblies 12, 14. Enveloping the active and counter electrode assemblies 12, 14 is a housing material 90.
  • the active and counter electrode assemblies 12, 14 are positioned on the biological interface 18. Positioning on the biological interface may close the circuit, allowing electromotive force to be applied and/or current to flow from one pole 16a of the power source 16 to the other pole 16b, via the active electrode assembly, biological interface 18 and counter electrode assembly 14.
  • the outermost active electrode ion selective membrane 38 may be placed directly in contact with the biological interface 18.
  • an interface-coupling medium (not shown) may be employed between the outermost active electrode ion selective membrane 22 and the biological interface 18.
  • the interface-coupling medium may take, for example, the form of an adhesive and/or gel.
  • the gel may take, for example, the form of a hydrating gel or a hydrogel. If used, the interface- coupling medium should be permeable by the active agent 36, 40, 42.
  • the power source 16 is selected to provide sufficient voltage, current, and/or duration to ensure delivery of the one or more active agents 36, 40, 42 from the reservoir 34 and across a biological interface (e.g., a membrane) to impart the desired physiological effect.
  • the power source 16 may take the form of one or more chemical battery cells, super- or ultra-capacitors, fuel cells, secondary cells, thin film secondary cells, button cells, lithium ion cells, zinc air cells, nickel metal hydride cells, and the like.
  • the power source 16 may, for example, provide a voltage of 12.8 V DC, with tolerance of 0.8 V DC, and a current of 0.3 mA.
  • the power source 16 may be selectively, electrically coupled to the active and counter electrode assemblies 12, 14 via a control circuit, for example, via carbon fiber ribbons.
  • the iontophoresis device 8 may include discrete and/or integrated circuit elements to control the voltage, current, and/or power delivered to the electrode assemblies 12, 14.
  • the iontophoresis device 8 may include a diode to provide a constant current to the electrode elements 24, 68.
  • the one or more active agents 36, 40, 42 may take the form of one or more ionic, cationic, ionizeable, and/or neutral drugs or other therapeutic agents. Consequently, the poles or terminals of the power source 16 and the selectivity of the outermost ion selective membranes 38, 80 and inner ion selective membranes 30, 74 are selected accordingly.
  • the electromotive force across the electrode assemblies, as described leads to a migration of charged active agent molecules, as well as ions and other charged components, through the biological interface into the biological tissue. This migration may lead to an accumulation of active agents, ions, and/or other charged components within the biological tissue beyond the interface.
  • solvent e.g., water
  • the electroosmotic solvent flow enhances migration of both charged and uncharged molecules. Enhanced migration via electroosmotic solvent flow may occur particularly with increasing size of the molecule.
  • the active agent may be a higher molecular weight molecule.
  • the molecule may be a polar polyelectrolyte.
  • the molecule may be lipophilic.
  • such molecules may be charged, may have a low net charge, or may be uncharged under the conditions within the active electrode.
  • such active agents may migrate poorly under the iontophoretic repulsive forces, in contrast to the migration of small more highly charged active agents under the influence of these forces. These higher molecular weight active agents may thus be carried through the biological interface into the underlying tissues primarily via electroosmotic solvent flow.
  • the high molecular weight polyelectrolytic active agents may be proteins, polypeptides, or nucleic acids.
  • the active agent may be mixed with another agent to form a complex capable of being transported across the biological interface via one of the motive methods described above.
  • the transdermal drug delivery system 6 includes an iontophoretic drug delivery device 8 for providing transdermal delivery of one or more therapeutic active agents 36, 40, 42 to a biological interface 18.
  • the delivery device 8 includes active electrode assembly 12 including at least one active agent reservoir and at least one active electrode element operable to provide an electromotive force to drive an active agent from the at least one active agent reservoir.
  • the delivery device 8 may include a counter electrode assembly 14 including at least one counter electrode element 68, and a power source 16 electrically coupled to the at least one active and the at least one counter electrode elements 20, 68.
  • the iontophoretic drug delivery 8 may further include one or more active agents 36, 40, 42 loaded in the at least one active agent reservoir 34.
  • the delivery device 8 may further include a substrate 10 including a plurality of microneedles 17 in fluidic communication with the active electrode assembly 12, and positioned between the active electrode assembly 12 and the biological interface 18.
  • the substrate 10 may be positioned between the active electrode assembly 12 and the biological interface 18.
  • the at least one active electrode element 20 is operable to provide an electromotive force to drive an active agent 36, 40, 42 from the at least one active agent reservoir 34, through the plurality of microneedles 17, and to the biological interface 18.
  • the substrate 10 includes a first side 102 and a second side 104 opposing the first side 102.
  • the first side 102 of the substrate 10 includes a plurality of microneedles 17 projecting outwardly from the first side 102.
  • the microneedles 17 may be individually provided or formed as part of one or more arrays.
  • the microneedles 17 are integrally formed from the substrate 10.
  • the microneedles 17 may take a solid and permeable form, a solid and semi-permeable form, and/or a solid and non-permeable form.
  • solid, non-permeable, microneedles may further comprise grooves along their outer surfaces for aiding the transdermal delivery of one or more active agents.
  • the microneedles 17 may take the form of hollow microneedles.
  • the hollow microneedles may be filled with ion exchange material, ion selective materials, permeable materials, semi-permeable materials, solid materials, and the like.
  • the microneedles 17 are used, for example, to deliver a variety of pharmaceutical compositions, molecules, compounds, active agents, and the like to a living body via a biological interface, such as skin or mucous membrane.
  • pharmaceutical compositions, molecules, compounds, active agents, and the like may be delivered into or through the biological interface.
  • the length of the microneedle 17, either individually or in arrays 100a, 100b, and/or the depth of insertion may be used to control whether administration of a pharmaceutical compositions, molecules, compounds, active agents, and the like is only into the epidermis, through the epidermis to the dermis, or subcutaneous.
  • the microneedle 17 may be useful for delivering high-molecular weight active agents, such as those comprising proteins, peptides and/or nucleic acids, and corresponding compositions thereof.
  • the microneedles 17 can provide electrical continuity between the power source 16 and the tips of the microneedles 17.
  • the microneedles 17, either individually or in arrays 100a, 100b, may be used to dispense, deliver, and/or sample fluids through hollow apertures, through the solid permeable or semi permeable materials, or via external grooves.
  • the microneedles 17 may further be used to dispense, deliver, and/or sample pharmaceutical compositions, molecules, compounds, active agents, and the like by iontophoretic methods, as disclosed herein. Accordingly, in certain embodiments, for example, a plurality of microneedles 17 in an array 100a, 100b may advantageously be formed on an outermost biological interface-contacting surface of a transdermal drug delivery system 6.
  • the pharmaceutical compositions, molecules, compounds, active agents, and the like delivered or sampled by such a system 6 may comprise, for example, high-molecular weight active agents, such as proteins, peptides, and/or nucleic acids.
  • a plurality of microneedles 17 may take the form of a microneedle array 100a, 100b.
  • the microneedle array 100a, 100b may be arranged in a variety of configurations and patterns including, for example, a rectangle, a square, a circle (as shown in Figure 3A), a triangle, a polygon, a regular or irregular shapes, and the like.
  • the microneedles 17 and the microneedle arrays 100a, 100b may be manufactured from a variety of materials, including ceramics, elastomers, epoxy photoresist, glass, glass polymers, glass/polymer materials, metals (e.g., chromium, cobalt, gold, molybdenum, nickel, stainless steel, titanium, tungsten steel, and the like), molded plastics, polymers, biodegradable polymers, non-biodegradable polymers, organic polymers, inorganic polymers, silicon, silicon dioxide, polysilicon, silicon rubbers, silicon-based organic polymers, superconducting materials (e.g., superconductor wafers, and the like), and the like, as well as combinations, composites, and/or alloys thereof.
  • materials including ceramics, elastomers, epoxy photoresist, glass, glass polymers, glass/polymer materials, metals (e.g., chromium, cobalt, gold, molybdenum, nickel,
  • Techniques for fabricating the microneedles 17 are well known in the art and include, for example, electro-deposition, electro- deposition onto laser-drilled polymer molds, laser cutting and electro- polishing, laser micromachining, surface micro-machining, soft lithography, x-ray lithography, LIGA techniques (e.g., X-ray lithography, electroplating, and molding), injection molding, conventional silicon-based fabrication methods (e.g., inductively coupled plasma etching, wet etching, isotropic and anisotropic etching, isotropic silicon etching, anisotropic silicon etching, anisotropic GaAs etching, deep reactive ion etching, silicon isotropic etching, silicon bulk micromachining, and the like), complementary- symmetry/metal-oxide semiconductor (CMOS) technology, deep x-ray exposure techniques, and the like.
  • CMOS complementary- symmetry/metal-oxide semiconductor
  • the physical characteristics of the microneedles 17 depend on, for example, the anodization conditions (e.g., current density, etching time, HF concentration, temperature, bias settings, and the like) as well as substrate properties (e.g., doping density, doping orientation, and the like).
  • the anodization conditions e.g., current density, etching time, HF concentration, temperature, bias settings, and the like
  • substrate properties e.g., doping density, doping orientation, and the like.
  • the microneedles 17 may be sized and shaped to penetrate the outer layers of skin to increase its permeability and transdermal transport of pharmaceutical compositions, molecules, compounds, active agents, and the like.
  • the microneedles 17 are sized and shaped with an appropriate geometry and sufficient strength to insert into a biological interface (e.g., the skin or mucous membrane on a subject, and the like), and thereby increase a trans-interface (e.g., transdermal) transport of pharmaceutical compositions, molecules, compounds, active agents, and the like.
  • Figure 4 shows an exemplary method 400 for systemic treatment of at least one condition associated with pain, neuropathic pain, acute pain, chronic pain, or cancer pain.
  • the method includes contacting a location on a biological interface 18 with an iontophoretic drug delivery device 8 that includes an active electrode assembly 12 having at least one active agent reservoir 34.
  • the at least one active agent reservoir 34 includes a pharmaceutical composition including at least a therapeutically effective amount of at least one opioid agonist and at least one opioid antagonist.
  • the at least one opioid agonist is selected from endogenous opioid peptides, opium alkaloids, semi-synthetic opioids, and fully synthetic opioids, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof.
  • the at least one opioid agonist is selected from (5 ⁇ ,7 ⁇ ,8 ⁇ -(-)-N-methyl-N-[7-(1-pyrrolidinyl)-1-oxaspiro(4, 5)dec-8-yl]-benzene-acetamide (1169,593)), [D-AIa2,N-Me-Phe4,Gly5- oljenkephalin (DAMGO), delta-([D-Pen2,D-Pen5]-enkephalin (DPDPE)), buprenorphine, codeine, dextromoramide, dihydrocodeine, fentanyl, heroin, hydrocodone, hydromorphone, meperidine, methadone, morphine, nicomorphine, opium, oxycodone, oxymorphone, pentazocine, pethidine, propoxyphene, and tilidine, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof.
  • the at least one opioid antagonist is selected from [(-)-(1 R,5R,9R)-5,9-diethyl-2-(3-furyl-methyl)-2'-hydroxy-6,7- benzomorphan] (MR2266), [allyl]2-tyr-alpha-amino-isobutyric acid (Aib)-Aib- Phe-Leu-OH (ICI-174864), 4-(3-hydroxyphenyl)-34-dimethyl-alpha-phenyl-1- piperidinepropanol (LY117413), 6 ⁇ -Naltrexol, 7-Benzylidenenaltrexone (BNTX), b-funaltrexamine (b-FNA), cyclazocine, cyclorphan, dezocine, diprenorphine, levorphanol, meptazinol, methiodide, methylnaltrexone, nalide, nalmefene, nalm
  • the at least one opioid antagonist is selected from hydromorphone, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof; and the at least one opioid antagonist is selected from naloxone, naltrexone, nalmefene, naloxonazine, NTI, nor-BNI, LY25506, LY9935, LY255582, and LY117413, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof.
  • the at least one opioid antagonist is selected from hydromorphone, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof; and the at least one opioid antagonist is selected from naloxone, naltrexone, 6 ⁇ -naltrexol, nalmefene, and naloxonazine, or analogs or derivatives, or pharmaceutically acceptable salts or solvates thereof.
  • the at least one opioid antagonist is selected from palladone, Palladone® SR, Dilaudid® and hydromorphone hydrochloride; and the at least one opioid antagonist is selected from Narcan®, Trexan®, Revex®, Nubian®, nalaxone hydrochloride, naltrexone hydrochloride, nalmefene hydrochloride, and nulbuphine hydrochloride.
  • the least one opioid agonist and at least one opioid antagonist are present in synergistic anti- hyperalgesic effective amounts.
  • the at least one condition associated with pain, neuropathic pain, acute pain, chronic pain, or cancer pain includes: cancer; chemotherapy; alcoholism; amputation (e.g., phantom limb syndrome); a back, leg, or hip problem (sciatica); diabetes; a facial nerve problem (trigeminal neuralgia); an HIV infection or AIDS; multiple sclerosis; spinal surgery; opiate induced narcotic/respiratory depression; or detoxification of opiate-dependency.
  • the pharmaceutical composition further comprises at least one active agent selected from vaccines, antibiotics, adjuvants, immunological adjuvants, immunogens, tolerogens, allergens, toll-like receptor agonists, and toll-like receptor antagonists, immuno- adjuvants, immuno-modulators, immuno-response agents, immuno- stimulators, specific immuno-stimulators, non-specific immuno-stimulators, and immuno-suppressants, or combinations thereof.
  • active agent selected from vaccines, antibiotics, adjuvants, immunological adjuvants, immunogens, tolerogens, allergens, toll-like receptor agonists, and toll-like receptor antagonists, immuno- adjuvants, immuno-modulators, immuno-response agents, immuno- stimulators, specific immuno-stimulators, non-specific immuno-stimulators, and immuno-suppressants, or combinations thereof.
  • the method further includes applying a sufficient amount of current to the active electrode assembly 12 for transdermal ⁇ administering a therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the at least one opioid agonist and the at least one opioid antagonist.
  • applying a sufficient amount of current to the active electrode assembly 12 comprises providing a sufficient voltage and current for a time interval, to the to the active electrode assembly 12, for delivering a therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the at least one opioid agonist and the at least one opioid antagonist, from the at least one active agent reservoir 34 to the location on the biological interface 18.
  • applying a sufficient amount of current comprises providing a sufficient voltage and current for a time interval to the active electrode assembly 12 to substantially achieve sustained-delivery or controlled- delivery of the pharmaceutical composition comprising the therapeutically effective amount of the at least one opioid agonist and the at least one opioid antagonist, over an extended period of time, so as to produce anesthesthetic, analgesic, or anti-hyperalgesic therapy in a subject.
  • Figure 5 shows an exemplary method 500 of inducing anesthesia, analgesia, or anti-hyperalgesia in a subject.
  • the method includes positioning an active electrode and a counter electrode of an iontophoretic delivery device on a biological interface of the subject.
  • the iontophoretic drug delivery device 8 is operable for iontophoretically delivering a pharmaceutical composition comprising an effective amount of at least one opioid agonist and at least one opioid antagonist.
  • the method further includes iontophoretically delivering an anesthesia inducing, an analgesia inducing, or an anti-hyperalgesia inducing synergistic amount of a pharmaceutical composition comprising at least one opioid agonist and at least one opioid antagonist.
  • Figure 6 shows an exemplary method 600 of treating opiate dependency and/or eliciting a substantially opiate free state in a subject in need thereof.
  • the method includes contacting a location on a biological interface 18 of the subject with an iontophoretic drug delivery 8 operable for iontophoretically delivering a pharmaceutical composition comprising a therapeutically effective amount of at least one opioid antagonist.
  • the method further includes transdermal ⁇ delivering a therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the least one opioid antagonist.
  • the method further includes providing sufficient voltage and current to deliver the therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the least one opioid antagonist to the location on the biological interface 18 of the subject, so as to eliciting the substantially opiate free state.
  • Figure 7 shows an exemplary method 600 of method of treating opiate agonist-induced narcotic/respiratory depression in a subject in need thereof.
  • the method includes contacting a location on a biological interface 18 of the subject with an iontophoretic drug delivery device 8 operable for iontophoretically delivering a pharmaceutical composition comprising a therapeutically effective amount of at least one opioid antagonist.
  • the method further includes transdermal ⁇ delivering a therapeutically effective amount of the pharmaceutical composition comprising the therapeutically effective amount of the least one opioid antagonist.
  • Figure 8 shows a Time (min) vs. Drug Transported ( ⁇ g) plot for hydromorphone delivery across human skin according to one illustrated embodiment.
  • a Franz cell setup using dermatomed human skin as the barrier to the center chamber was used to demonstrate transport across human skin in a benchtop setting.
  • Hydromorphone was diluted in water at 1 mg/ml and placed in contact with the anodal side of an iontophoresis delivery device 8.
  • a 0.33 mA/cm 2 current density was applied to the cell and time points taken as demonstrated in the Time (min) vs. Drug Transported ( ⁇ g) plot. Samples were analyzed for the presence of hydromorphone and plotted as a function of time.
  • mass spectrum analysis was performed on guinea pig serum samples following iontophoretic delivery of hydromorphone according to one illustrated embodiment.
  • SPE tubes (Varian Inc. Harbor City, CA) were prepared by washing with 2 ml of methanol followed by 2 ml of deionized water. The samples were applied and pulled through under vacuum.
  • HPLC-MS is an Agilent Technologies (Palo Alto, CA.) 1100 series including binary pump, degassing module, autosampler, column compartment, and mass spectrometer.
  • the column was a Zorbax SB-C18 150 mm x 2.1 mm x 5 ⁇ (Agilent Technologies, Palo Alto, CA.).
  • the column was maintained at 30 0 C.
  • the flow rate was 0.25 ml/min.
  • the mass spectrometer was operated in the ESI + mode using selected ion monitoring (SIM) for maximum sensitivity.
  • SIM selected ion monitoring
  • Ions monitored were m/z 286 for hydromorphone and m/z 292 for hydromorphone-de.
  • the lower limit of quantization of this assay is 0.2 ng/ml and the lower limit of detection is 0.1 ng/ml based upon a 0.25 ml sample size.
  • Figure 10 shows a Time (min) vs. Hydromorphone (ng/ml) plot of a Guinea pig in vivo experiment according to one illustrated embodiment.
  • the electrode a carbon on polyethylene film base was used.
  • the backing material of the patch was from 3M (polyolefin closed cell foam medical backing, product # 9773).
  • the reservoir material was polyester fabric (Textile Development Associates, #PETNF322.3030), 17 mm diameter, and 2 mm nominal thickness.
  • the disks were specially treated by saturating with a 2% wt/v solution of hydroxypropyl cellulose (Klucel, MF Pharm, Hercules Corp.) and dried in a convection oven.
  • the delivery solution was prepared by dissolving 21 mg of hydromorphone HCI (Sigma Chemical Co., Lot # 024K1167) into 10 ml_ of buffer solution containing 0.155 M Na Ascorbate, pH 4.55) to give a final concentration of 2.1 mg/mL.
  • the counter electrode solution was 0.5 M Disodium Fumarate (Fluka, Product # 47970, Lot # 443411/1). All buffer and drug solution were made on the same day of the experiment.
  • the patch was made by placing the screen-printed electrode (TTI) onto a backing of the backing material.
  • the patches were powered by 8-channel potentiostat/galvanostat (Solartron Analytical Model 1480) running Cell Test software (Solartron Analytical) for instrument control and data acquisition.
  • the drug delivery electrode was connected to the anode (+) and the counter electrode was connected to the cathode (-).
  • Current was delivered under a controlled current protocol at 1 mA (patch area 2.27 cm 2 , current density 0.44 mA/cm 2 ) for 45 min duration.
  • the instrument captured the total voltage drop across the patch reflecting the sum of the voltages (resistance to current passage) across each electrode, the skin at both interfaces and the underlying tissue. Samples were collected at the indicated time points and analyzed as shown in Figure 10.
  • some embodiments may include an interface layer interposed between the outermost active electrode ion selective membrane 22 and the biological interface 18.
  • Some embodiments may comprise additional ion selective membranes, ion exchange membranes, semi-permeable membranes and/or porous membranes, as well as additional reservoirs for electrolytes and/or buffers.
  • hydrogels have been known and used in the medical field to provide an electrical interface to the skin of a subject or within a device to couple electrical stimulus into the subject. Hydrogels hydrate the skin, thus protecting against burning due to electrical stimulation through the hydrogel, while swelling the skin and allowing more efficient transfer of an active component. Examples of such hydrogels are disclosed in U.S.
  • Further examples of such hydrogels are disclosed in U.S. Patent applications 2004/166147; 2004/105834; and 2004/247655, herein incorporated in their entirety by reference.
  • hydrogels and hydrogel sheets include CorplexTM by Corium, TegagelTM by 3M, PuraMatrixTM by BD; VigilonTM by Bard; ClearSiteTM by Conmed Corporation; FlexiGelTM by Smith & Nephew; Derma-GelTM by Medline; Nu-GeITM by Johnson & Johnson; and CuragelTM by Kendall, or acrylhydrogel films available from Sun Contact Lens Co., Ltd.
  • compounds or compositions can be delivered by an iontophoresis device comprising an active electrode assembly and a counter electrode assembly, electrically coupled to a power source to deliver an active agent to, into, or through a biological interface.
  • the active electrode assembly includes the following: a first electrode member connected to a positive electrode of the power source; an active agent reservoir having a drug solution that is in contact with the first electrode member and to which is applied a voltage via the first electrode member; a biological interface contact member, which may be a microneedle array and is placed against the forward surface of the active agent reservoir; and a first cover or container that accommodates these members.
  • the counter electrode assembly includes the following: a second electrode member connected to a negative electrode of the voltage source; a second electrolyte holding part that holds an electrolyte that is in contact with the second electrode member and to which voltage is applied via the second electrode member; and a second cover or container that accommodates these members.
  • compounds or compositions can be delivered by an iontophoresis device comprising an active electrode assembly and a counter electrode assembly, electrically coupled to a power source to deliver an active agent to, into, or through a biological interface.
  • the active electrode assembly includes the following: a first electrode member connected to a positive electrode of the voltage source; a first electrolyte reservoir having an electrolyte that is in contact with the first electrode member and to which is applied a voltage via the first electrode member; a first anion-exchange membrane that is placed on the forward surface of the first electrolyte holding part; an active agent reservoir that is placed against the forward surface of the first anion-exchange membrane; a biological interface contacting member, which may be a microneedle array and is placed against the forward surface of the active agent reservoir; and a first cover or container that accommodates these members.
  • the counter electrode assembly includes the following: a second electrode member connected to a negative electrode of the voltage source; a second electrolyte holding part having an electrolyte that is in contact with the second electrode member and to which is applied a voltage via the second electrode member; a cation-exchange membrane that is placed on the forward surface of the second electrolyte reservoir; a third electrolyte reservoir that is placed against the forward surface of the cation-exchange membrane and holds an electrolyte to which a voltage is applied from the second electrode member via the second electrolyte holding part and the cation-exchange membrane; a second anion-exchange membrane placed against the forward surface of the third electrolyte reservoir; and a second cover or container that accommodates these members.
  • the present disclosure comprises methods of treating a subject by any of the compositions and/or methods described herein.

Landscapes

  • Health & Medical Sciences (AREA)
  • Animal Behavior & Ethology (AREA)
  • Veterinary Medicine (AREA)
  • Public Health (AREA)
  • General Health & Medical Sciences (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Engineering & Computer Science (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Epidemiology (AREA)
  • Medicinal Chemistry (AREA)
  • Chemical & Material Sciences (AREA)
  • Biomedical Technology (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • Radiology & Medical Imaging (AREA)
  • Dermatology (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Medicines That Contain Protein Lipid Enzymes And Other Medicines (AREA)
  • Electrotherapy Devices (AREA)
EP06816083A 2005-09-30 2006-09-29 Transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist Withdrawn EP1931421A1 (en)

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US72213605P 2005-09-30 2005-09-30
PCT/US2006/038549 WO2007041544A1 (en) 2005-09-30 2006-09-29 Transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist

Publications (1)

Publication Number Publication Date
EP1931421A1 true EP1931421A1 (en) 2008-06-18

Family

ID=37696075

Family Applications (1)

Application Number Title Priority Date Filing Date
EP06816083A Withdrawn EP1931421A1 (en) 2005-09-30 2006-09-29 Transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist

Country Status (10)

Country Link
EP (1) EP1931421A1 (enExample)
JP (1) JP2009509692A (enExample)
KR (1) KR20080058433A (enExample)
CN (2) CN101321554A (enExample)
AU (1) AU2006299521A1 (enExample)
BR (1) BRPI0616788A2 (enExample)
CA (1) CA2622684A1 (enExample)
IL (1) IL190245A0 (enExample)
RU (1) RU2008117168A (enExample)
WO (1) WO2007041544A1 (enExample)

Families Citing this family (14)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20100239523A1 (en) * 2007-10-30 2010-09-23 The Regents Of The University Of Colorado Tlr modulators and methods for using the same
AU2009225434B2 (en) 2008-03-21 2014-05-22 The University Of Chicago Treatment with opioid antagonists and mTOR inhibitors
EP2303016A4 (en) 2008-05-01 2011-11-30 Univ California METHOD AND USE FOR THE USE OF SELECTIVE DELTA OPIOID RECEPTOR 1 AGONISTS, DELTA OPIOID RECEPTOR 2 AGONISTS AND / OR MU OPIOID RECEPTOR ANTAGONISTS FOR THE TREATMENT OF ACTIVE SUBSTANCES
WO2010110397A1 (ja) * 2009-03-25 2010-09-30 国立大学法人 香川大学 マイクロニードルおよびその製造方法と金型
CA2841785A1 (en) 2011-07-06 2013-01-10 The Parkinson's Institute Compositions and methods for treatment of symptoms in parkinson's disease patients
JP2018511355A (ja) 2015-01-28 2018-04-26 クロノ セラピューティクス インコーポレイテッドChrono Therapeutics Inc. 薬剤送達方法及びシステム
AU2016228779A1 (en) 2015-03-12 2017-09-07 Chrono Therapeutics Inc. Craving input and support system
CN106730311B (zh) * 2016-12-27 2019-10-29 潍坊大地医疗器械有限公司 经络综合治疗仪电极触头装置
JP2020503950A (ja) 2017-01-06 2020-02-06 クロノ セラピューティクス インコーポレイテッドChrono Therapeutics Inc. 経皮薬剤送達の装置及び方法
GB201704909D0 (en) 2017-03-28 2017-05-10 Ldn Pharma Ltd Cancer therapy
WO2019090125A2 (en) * 2017-11-02 2019-05-09 Chrono Therapeutics Inc. Smart abuse-deterrent transdermal drug delivery system
JP7420797B2 (ja) 2018-05-29 2024-01-23 モーニングサイド ベンチャー インベストメンツ リミテッド 薬剤送達の方法及びシステム
CA3119992A1 (en) 2018-11-16 2020-05-22 Morningside Venture Investments Limited Thermally regulated transdermal drug delivery system
ES3011582T3 (en) 2019-02-21 2025-04-07 Pharmaceutical Productions Inc Naloxone formulations for sublingual and/or buccal administration

Family Cites Families (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4626539A (en) * 1984-08-10 1986-12-02 E. I. Dupont De Nemours And Company Trandermal delivery of opioids
US4722726A (en) * 1986-02-12 1988-02-02 Key Pharmaceuticals, Inc. Method and apparatus for iontophoretic drug delivery
US4879297A (en) * 1987-06-01 1989-11-07 Warner-Lambert Company Fatty acids and their small chain esters as penetration enhancers in aqueous systems
US5312326A (en) * 1992-06-02 1994-05-17 Alza Corporation Iontophoretic drug delivery apparatus
EA009921B1 (ru) * 2003-07-25 2008-04-28 Еуро-Селтик С.А. Способ лечения синдрома отвыкания от зависимости у беременных женщин
TW200640526A (en) * 2005-02-24 2006-12-01 Alza Corp Transdermal electrotransport drug delivery systems with reduced abuse potential

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
See references of WO2007041544A1 *

Also Published As

Publication number Publication date
AU2006299521A1 (en) 2007-04-12
BRPI0616788A2 (pt) 2011-07-05
WO2007041544A1 (en) 2007-04-12
CN101321554A (zh) 2008-12-10
CA2622684A1 (en) 2007-04-12
KR20080058433A (ko) 2008-06-25
JP2009509692A (ja) 2009-03-12
CN101316623A (zh) 2008-12-03
RU2008117168A (ru) 2009-11-10
IL190245A0 (en) 2008-11-03

Similar Documents

Publication Publication Date Title
US7848801B2 (en) Iontophoretic systems, devices, and methods of delivery of active agents to biological interface
US20070093789A1 (en) Iontophoresis apparatus and method for delivery of angiogenic factors to enhance healing of injured tissue
US20070093788A1 (en) Iontophoresis method and apparatus for systemic delivery of active agents
US20080058701A1 (en) Delivery device having self-assembling dendritic polymers and method of use thereof
US20070093787A1 (en) Iontophoresis device to deliver multiple active agents to biological interfaces
US20070110810A1 (en) Transdermal drug delivery systems, devices, and methods employing hydrogels
US20070078376A1 (en) Functionalized microneedles transdermal drug delivery systems, devices, and methods
US7574256B2 (en) Iontophoretic device and method of delivery of active agents to biological interface
US20080033398A1 (en) Device and method for enhancing immune response by electrical stimulation
EP1931417A2 (en) Transdermal drug delivery systems, devices, and methods employing novel pharmaceutical vehicles
EP1931421A1 (en) Transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist
US20070081944A1 (en) Iontophoresis apparatus and method for the diagnosis of tuberculosis
MX2008004223A (en) Transdermal drug delivery systems, devices, andmethods employing opioid agonist and/or opioid antagonist
HK1125876A (en) Transdermal drug delivery systems, devices, and methods employing opioid agonist and/or opioid antagonist
MX2008004224A (es) Metodo y aparato de iontoforesis para el suministro sistemico de agentes activos
HK1125875A (en) Iontophoresis method and apparatus for systemic delivery of active agents

Legal Events

Date Code Title Description
PUAI Public reference made under article 153(3) epc to a published international application that has entered the european phase

Free format text: ORIGINAL CODE: 0009012

17P Request for examination filed

Effective date: 20080328

AK Designated contracting states

Kind code of ref document: A1

Designated state(s): AT BE BG CH CY CZ DE DK EE ES FI FR GB GR HU IE IS IT LI LT LU LV MC NL PL PT RO SE SI SK TR

17Q First examination report despatched

Effective date: 20090518

STAA Information on the status of an ep patent application or granted ep patent

Free format text: STATUS: THE APPLICATION IS DEEMED TO BE WITHDRAWN

18D Application deemed to be withdrawn

Effective date: 20110802