WO2007100376A2 - Compositions and methods for dermal delivery of drugs - Google Patents

Compositions and methods for dermal delivery of drugs Download PDF

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Publication number
WO2007100376A2
WO2007100376A2 PCT/US2006/048059 US2006048059W WO2007100376A2 WO 2007100376 A2 WO2007100376 A2 WO 2007100376A2 US 2006048059 W US2006048059 W US 2006048059W WO 2007100376 A2 WO2007100376 A2 WO 2007100376A2
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WO
WIPO (PCT)
Prior art keywords
formulation
volatile solvent
solidified layer
oil
skin
Prior art date
Application number
PCT/US2006/048059
Other languages
French (fr)
Other versions
WO2007100376A3 (en
Inventor
Jie Zhang
Kevin S. Warner
Sanjay Sharma
Original Assignee
Zars, 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 Zars, Inc. filed Critical Zars, Inc.
Priority to JP2008545866A priority Critical patent/JP2009519956A/en
Priority to CA002633464A priority patent/CA2633464A1/en
Priority to AU2006339350A priority patent/AU2006339350A1/en
Priority to EP06849969A priority patent/EP1968541A2/en
Priority to CN200680052642XA priority patent/CN101370453B/en
Publication of WO2007100376A2 publication Critical patent/WO2007100376A2/en
Publication of WO2007100376A3 publication Critical patent/WO2007100376A3/en

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Classifications

    • 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
    • A61K9/0014Skin, i.e. galenical aspects of topical compositions
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/08Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing oxygen, e.g. ethers, acetals, ketones, quinones, aldehydes, peroxides
    • A61K47/10Alcohols; Phenols; Salts thereof, e.g. glycerol; Polyethylene glycols [PEG]; Poloxamers; PEG/POE alkyl ethers
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/08Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing oxygen, e.g. ethers, acetals, ketones, quinones, aldehydes, peroxides
    • A61K47/12Carboxylic acids; Salts or anhydrides thereof
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/08Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing oxygen, e.g. ethers, acetals, ketones, quinones, aldehydes, peroxides
    • A61K47/14Esters of carboxylic acids, e.g. fatty acid monoglycerides, medium-chain triglycerides, parabens or PEG fatty acid esters
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/30Macromolecular organic or inorganic compounds, e.g. inorganic polyphosphates
    • A61K47/32Macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. carbomers, poly(meth)acrylates, or polyvinyl pyrrolidone
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/30Macromolecular organic or inorganic compounds, e.g. inorganic polyphosphates
    • A61K47/36Polysaccharides; Derivatives thereof, e.g. gums, starch, alginate, dextrin, hyaluronic acid, chitosan, inulin, agar or pectin
    • A61K47/38Cellulose; Derivatives thereof
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/44Oils, fats or waxes according to two or more groups of A61K47/02-A61K47/42; Natural or modified natural oils, fats or waxes, e.g. castor oil, polyethoxylated castor oil, montan wax, lignite, shellac, rosin, beeswax or lanolin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/70Web, sheet or filament bases ; Films; Fibres of the matrix type containing drug
    • A61K9/7015Drug-containing film-forming compositions, e.g. spray-on

Definitions

  • the present invention relates generally to systems developed for dermal delivery of drugs. More particularly, the present invention relates to formulations including at least two non-volatile solvents, wherein the formulation as a whole has a viscosity suitable for application as a layer to a skin surface, and which forms a sustained drug-delivering adhesive solidified layer on the skin.
  • Semisolid formulations are available in a few different forms, including ointments, creams, foams, pastes, gels, or lotions and are applied topically to the skin.
  • transdermal patch dosage forms also are available in a few different forms, including matrix patch configurations and liquid reservoir patch configurations.
  • a matrix patch the active drug is mixed in an adhesive that is coated on a backing film.
  • the drug-laced adhesive layer is typically directly applied onto the skin and serves both as means for affixing the patch to the skin and as a reservoir or vehicle for facilitating delivery of the drug.
  • a liquid reservoir patch the drug is typically incorporated into a solvent system which is held by a thin bag, which can be a thin flexible container.
  • the thin bag can include a permeable or semi-permeable membrane surface that is coated with an adhesive for affixing the membrane to the skin.
  • the membrane is often referred to as a rate limiting membrane (although it may not actually be rate limiting in the delivery process in all cases) and can control transport of the drug from within the thin bag to the skin for dermal delivery.
  • patches and semisolid formulations are widely used to deliver drugs into and through the skin, they both have significant limitations.
  • most semisolid formulations usually contain solvent(s), such as water and ethanol, which are volatile and thus evaporate shortly after application. The evaporation of such solvents can cause a significant decrease or even termination of dermal drug delivery, which may not be desirable in many cases.
  • solvent(s) such as water and ethanol
  • semisolid formulations are often "rubbed into” the skin, which does not necessarily mean the drug formulation is actually delivered into the skin.
  • this phrase often means that a very thin layer of the drug formulation is applied onto the surface of the skin.
  • Such thin layers of traditional semisolid formulations applied to the skin may not contain sufficient quantity of active drug to achieve sustained delivery over long periods of time.
  • traditional semisolid formulations are often subject to unintentional removal due to contact with objects such as clothing, which may compromise the sustained delivery and/or undesirably soil clothing.
  • Drugs present in a semisolid formulation may also be unintentionally delivered to persons who come in contact with a subject undergoing treatment with a topical semisolid formulation.
  • a drug should have sufficient solubility in the adhesive, as primarily only dissolved drug contributes to the driving force required for skin permeation.
  • liquid reservoir patches even if a drug is compatible with a particular liquid or semisolid solvent system carried by the thin bag of the patch, the solvent system still has to be compatible to the adhesive layer coated on the permeable or semi-permeable membrane; otherwise the drug may be adversely affected by the adhesive layer or the drug/solvent system may reduce the tackiness of the adhesive layer.
  • reservoir patches are bulkier and usually are more expensive to manufacture than matrix patches.
  • dermal patches including transdermal patches
  • the backing film (in matrix patches) and the thin fluid bag (in reservoir patches) are typically made of polyethylene or polyester, both of which are relatively non-stretchable materials. If the patch is applied to a skin area that is significantly stretched during body movements, such as a joint, separation between the patch and skin may occur thereby compromising the delivery of the drug.
  • a patch present on a skin surface may hinder the expansion of the skin during body movements and cause discomfort.
  • patches are not ideal dosage forms for skin areas subject to expansion, flexing and stretching during body movements.
  • an adhesive formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and at least one solidifying agent.
  • the solvent vehicle can comprise a volatile solvent system including at least one volatile solvent and a non-volatile solvent system including at least one non-volatile solvents.
  • the at least two non-volatile solvents of the non-volatile solvent system can facilitate transdermal delivery of the drug at a therapeutically effective rate over a sustained period of time, even after the non-volatile solvent system is substantially evaporated from the solidified layer.
  • the formulation can have viscosity suitable for application to the skin surface prior to evaporation of at least one volatile solvent, and can further be formulated such that when applied to the skin surface, the formulation forms a solidified layer after at least a portion of the volatile solvent system is evaporated. Sustained drug delivery from the solidified layer can also occur.
  • the formulation is formulated such that it has at least two volatile solvents, at least two non-volatile solvents, at least two solidifying agents, or combinations thereof.
  • a method of dermally delivering a drug can comprise applying an adhesive formulation to a skin surface of a subject.
  • the formulation be any formulation as set forth above.
  • Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system, and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time.
  • a solidified layer for delivering a drug can comprise a drug, a non-volatile solvent system including at least one nonvolatile solvents, wherein the non-volatile solvent system is capable of facilitating the delivery of the drug at therapeutically effective rates over a sustained period of time, and at least one solidifying agent.
  • the solidified layer can be stretchable by 5% in one direction without cracking, breaking, or separating from a skin surface to which the layer is applied.
  • the formulation is formulated such that it has at least two non-volatile solvents, at least two solidifying agents, or combinations thereof.
  • FIG. 1 is a graphical representation of cumulative amount of testosterone delivered across a biological membrane in vitro over time from a solidified adhesive formulation and a marketed product (AndroGel) in accordance with embodiments of the present invention.
  • FIG. 2 is a graphical representation of the cumulative amount of acyclovir delivered transdermal ⁇ over time from two separate formulations in accordance with embodiments of the present invention compared to the marketed product Zovirax cream.
  • a drug includes reference to one or more of such compositions.
  • skin is defined to include human skin (intact, diseased, ulcerous, or broken), finger and toe nail surfaces, and mucosal surfaces that are usually at least partially exposed to air such as lips, genital and anal mucosa, and nasal and oral mucosa.
  • drug(s) refers to any bioactive agent that is applied to, into, or through the skin which is applied for achieving a therapeutic affect. This includes compositions that are traditionally identified as drugs, as well other bioactive agents that are not always considered to be “drugs” in the classic sense, e.g., peroxides, humectants, emollients, etc., but which can provide a therapeutic effect for certain conditions.
  • drug it is understood that there are various forms of a given drug, and those various forms are expressly included. In accordance with this, various drug forms include polymorphs, salts, hydrates, solvates, and cocrystals.
  • one physical form of a drug may possess better physical-chemical properties making it more amenable for getting to, into, or through the skin, and this particular form is defined as the "physical form favorable for dermal delivery.”
  • the steady state flux of diclofenac sodium from flux enabling nonvolatile solvents is much higher than the steady state flux of diclofenac acid from the same flux enabling non-volatile solvents. It is therefore desirable to evaluate the flux of the physical forms of a drug from non-volatile solvents to select a desirable physical form/non-volatile solvent combination.
  • transdermal drug delivery or “dermal delivery of drug(s)” shall include both transdermal and topical drug delivery, and includes the delivery of drug(s) to, through, or into the skin.
  • Transdermal delivery of drug can be targeted to skin tissues just under the skin, regional tissues or organs under the skin, systemic circulation, and/or the central nervous system.
  • Topical delivery includes delivery of a drug to a skin tissue, and subsequent absorption into deeper tissues that may occur.
  • flux such as in the context of "dermal flux” or “transdermal flux,” respectively, refers to the quantity of the drug permeated into or across skin per unit area per unit time. A typical unit of flux is microgram per square centimeter per hour.
  • One way to measure flux is to place the formulation on a known skin area of a human volunteer and measure how much drug can permeate into or across skin within certain time constraints.
  • Various methods in vivo methods might be used for the measurements as well.
  • the method described in Example 1 or other similar method in vitro methods can also be used to measure flux.
  • flux-enabling with respect to the non-volatile solvent system (or solidified layer including the same) refers to a non-volatile solvent system (including one or more non-volatile solvents) selected or formulated specifically to be able to provide therapeutically effective flux for a particular drug(s).
  • a flux enabling non-volatile solvent system is defined as a non-volatile solvent system which, alone without the help of any other ingredients, is capable of delivering therapeutic effective levels of the drug across, onto or into the subject's skin when the non-volatile solvent system is saturated with the drug.
  • a flux enabling non-volatile solvent system is a non-volatile solvent system that can provide therapeutically effective daily doses over 24 hours when the non-volatile solvent system is saturated with the drug and is in full contact with the subject's skin with no more than 500 cm 2 contact area.
  • the contact area for the non-volatile solvent system is no more than 100 cm 2 .
  • Testing using this saturated drug-in-solvent state can be used to measure the maximum flux- generating ability of a non-volatile solvent system.
  • the drug solvent mixture needs to be kept on the skin for a clinically effective amount of time. In reality, it may be difficult to keep a liquid solvent on the skin of a human volunteer for an extended period of time.
  • an alternative method to determine whether a solvent system is "flux-enabling" is to measure the in vitro drug permeation across the hairless mouse skin or human cadaver skin using the apparatus and method described in Example 1.
  • This and similar methods are commonly used by those skilled in the art to evaluate permeability and feasibility of formulations.
  • whether a non-volatile solvent system is flux-enabling can be tested on the skin of a live human subject with means to maintain the non-volatile solvent system with saturated drug on the skin, and such means may not be practical for a product.
  • the non-volatile solvent system with saturated drug can be soaked into an absorbent fabric material which is then applied on the skin and covered with a protective membrane.
  • Such a system is not practical as a pharmaceutical product, but is appropriate for testing whether a non-volatile solvent system has the intrinsic ability to provide effective drug flux, or whether it is flux-enabling.
  • the solidified layer can also be "flux enabling" for the drug while some of the nonvolatile solvents remain in the solidified layer, even after the volatile solvents (including water) have been substantially evaporated.
  • therapeutically effective rate(s), refers to sufficient amounts or delivery rates of a drug which achieves any appreciable level of therapeutic results in treating a condition for which the drug is being delivered. It is understood that "appreciable level of therapeutic results” may or may not meet any government agencies' efficacy standards for approving the commercialization of a product. It is understood that various biological factors may affect the ability of a substance to perform its intended task. Therefore, an "effective amount,” “therapeutically effective amount,” or “therapeutically effective rate(s)” may be dependent in some instances on such biological factors to some degree. However, for each drug, there is usually a consensus among those skilled in the art on the range of doses or fluxes that are sufficient in most subjects.
  • “Therapeutically effective flux” is defined as the permeation flux of the selected drug that delivers sufficient amount of drug into or across the skin to be clinically beneficial in that some of the patient population can obtain some degree of benefit from the drug flux. It does not necessarily mean that most of the patient population can obtain some degree of benefit or the benefit is high enough to be deemed “effective” by relevant government agencies or the medical profession. More specifically, for drugs that target skin or regional tissues or organs close to the skin surface (such as joints, certain muscles, or tissues/organs that are at least partially within 5 cm of the skin surface),
  • therapeutically effective flux refers to the drug flux that can deliver a sufficient amount of the drug into the target tissues within a clinically reasonable amount of time.
  • therapeutically effective flux refers to drug flux that, via clinically reasonable skin contact area, can deliver sufficient amounts of the selected drug to generate clinically beneficial plasma or blood drug concentrations within a clinically reasonable time.
  • Clinically reasonable skin contact area is defined as a size of skin application area that most subjects would accept. Typically, a skin contact area of 400 cm 2 or less is considered reasonable.
  • the flux needs to be at least 4000 mcg/400cm 2 /10 hour, which equals 1 mcg/cm 2 /hr.
  • different drugs have different "therapeutically effective flux.
  • Therapeutically effective flux may also be different in different subjects and or at different times for even the same subject. However, for each drug, there is usually a consensus among the skilled in the art on the range of doses or fluxes that are sufficient in most subjects at most times.
  • the therapeutically effective flux values in Table 1 represent the steady state flux values of marketed products through hairless mouse or human epidermal membrane in an in vitro system described in Example 1. These values are meant only to be estimates and to provide a basis of comparison for formulation development and optimization.
  • the therapeutically effective flux for a selected drug could be very different for different diseases to be treated for, different stages of diseases, different individual subjects, etc. It should be noted that the flux listed may be more than therapeutically effective.
  • Table 2 illustrate screening of a nonvolatile solvent's flux enabling ability for some of the drugs specifically studied. Experiments were carried out as described in Example 1 below and the results are further discussed in the subsequent Examples 2-9.
  • plasticizing in relation to flux-enabling non-volatile solvent(s) is defined as a flux-enabling non-volatile solvent that acts as a plasticizer for the solidifying agent.
  • a "plasticizer” is an agent which is capable of increasing the percentage elongation of the formulation after the volatile solvent system has at least substantially evaporated. Plasticizers also have the capability to reduce the brittleness of solidified formulation by making it more flexible and/or elastic.
  • propylene glycol is a "flux-enabling, plasticizing non-volatile solvent" for the drug ketoprofen with polyvinyl alcohol as the selected solidifying agent.
  • propylene glycol in a formulation of ketoprofen with Gantrez S- 97 or Avalure UR 405 as solidifying agents does not provide the same plasticizing effect.
  • the combination of propylene glycol and Gantrez S-97 or Avalure UR 405 is less compatible and results in less desirable formulation for topical applications. Therefore, whether a given non-volatile solvent is "plasticizing" depends on which solidifying agent(s) is selected.
  • flux-enabling non-volatile solvent can be a single chemical substance or a mixture of two or more chemical substances.
  • the steady state flux value for clobetasol propionate in Table 3 is a 9:1 for propylene glycol:isostearic acid mixture that generated much higher clobetasol flux than propylene glycol or ISA alone (see Table 2). Therefore, the 9:1 propylene glycol:isostearic acid mixture is a "high flux- enabling non-volatile solvent” but propylene glycol or isostearic acid alone is not.
  • adheresion or "adhesive” when referring to a solidified layer herein refers to sufficient adhesion between the solidified layer and the skin so that the layer does not fall off the skin during intended use on most subjects.
  • adheresive or the like when used to describe the solidified layer means the solidified layer is adhesive to the skin surface to which the initial formulation layer was originally applied (before the evaporation of the volatile solvent(s)). In one embodiment, it does not mean the solidified layer is adhesive on the opposing side.
  • whether a solidified layer can adhere to a skin surface for the desired extended period of time partially depends on the condition of the skin surface.
  • the adhesive solidified layer of the current invention may not be able to maintain perfect contact with the skin surface and deliver the drug over a sustained period of time for every subject under any conditions on the skin surface.
  • a standard is that it maintains good contact with most of the skin surface, e.g. 70% of the total area, over the specified period of time for most subjects under normal conditions of the skin surface and external environment.
  • the terms "flexible,” “elastic,” “elasticity,” or the like, as used herein refer to sufficient elasticity of the solidified layer so that it is not broken if it is stretched in at least one direction by up to about 5%,. and often to about 10% or even greater.
  • a solidified layer that exhibits acceptably elasticity and adhesion to skin can be attached to human skin over a flexible skin location, e.g., elbow, finger, wrist, neck, lower back, lips, knee, etc., and will remain substantially intact on the skin upon stretching of the skin.
  • a flexible skin location e.g., elbow, finger, wrist, neck, lower back, lips, knee, etc.
  • the solidified layers of the present invention do not necessarily have to have any elasticity in some embodiments.
  • peelable when used to describe the solidified layer, means the solidified layer can be lifted from the skin surface in one large piece or several large pieces, as opposed to many small pieces or crumbs.
  • sustained relates to therapeutically effective rates of dermal drug delivery for a continuous period of time of at least 30 minutes, and in some embodiments, periods of time of at least about 2 hours, 4 hours, 8 hours, 12 hours, 24 hours, or longer.
  • volatile solvent system can be a single solvent or a mixture of solvents that are volatile, including water and solvents that are more volatile than water.
  • Non-limiting examples of volatile solvents that can be used in the present invention include iso-amyl acetate, denatured alcohol, methanol, ethanol, isopropyl alcohol, water, propanol, C4-C6 hydrocarbons, butane, isobutene, pentane, hexane, acetone, chlorobutanol, ethyl acetate, fluro-chloro- hydrocarbons, turpentine, methyl ethyl ketone, methyl ether, hydrofluorocarbons, ethyl ether, 1 ,1,1,2 tetrafluorethane 1,1,1 ,2,3,3,3-heptafluoropropane, 1,1,1 ,3,3,3 hexafluoropropane, and combinations thereof.
  • Non-volatile solvent system in this invention is defined as a mixture of at least two solvents that are each less volatile than water.
  • a non-volatile solvent is defined as a solvent that is less volatile than water.
  • the non-volatile solvent system can also contain substances that are solid or liquid at room temperatures, such as pH or ion-pairing agents. After evaporation of the volatile solvent system, most of the non-volatile solvent system should remain in the solidified layer for a period of time sufficient to adequately dermally deliver a given drug to, into, or through the skin of a subject at a sufficient flux for a period of time to provide a therapeutic effect.
  • the non-volatile solvent system can also serve as a plasticizer of the solidified layer, so that the solidified layer is elastic and flexible.
  • the non-volatile solvent system provides better plasticizing effects for the solidifying agents than any single non-volatile solvent of the non-volatile solvent system alone.
  • Including multiple non-volatile solvents as part of the non-volatile solvent system can also provide various other benefits.
  • a single non-volatile solvent may not provide the formulation with adequate compatibility with other ingredients in the formulation, e.g. volatile solvent system or solidifying agent, and/or the ability to generate therapeutically effective flux of the drug.
  • the non-volatile solvent system provides better compatibility with the solidifying agent than any single non-volatile solvent of the non-volatile solvent system alone. In another aspect of the invention, the non-volatile solvent system provides higher flux than any single non-volatile solvent of the non-volatile solvent system alone.
  • the present invention allows for combinations of two or more non-volatile solvents which together are able to provide both therapeutically effective drug flux while maintaining formulation component compatibility.
  • solvent vehicle describes compositions that include both a volatile solvent system and non-volatile solvent system.
  • the volatile solvent system is chosen so as to evaporate from the adhesive formulation quickly to form a solidified layer, and the non-volatile solvent system is formulated or chosen to substantially remain as part of the solidified layer after volatile solvent system evaporation so as to provide continued delivery of the drug.
  • the drug can be partially or completely dissolved in the solvent vehicle or formulation as a whole.
  • the drug can also be partially or completely solubilizable in the non-volatile solvent system once the volatile solvent system is evaporated.
  • Formulations in which the drug is only partially dissolved in the non-volatile solvent system after the evaporation of the volatile solvent system have the potential to maintain longer duration of sustained delivery, as the undissolved drug can dissolve into the non-volatile solvent system as the dissolved drug is being depleted from the solidified layer during drug delivery.
  • “Adhesive solidifying formulation” or “solidifying formulation” refers to a composition that has a viscosity suitable for application to a skin surface prior to evaporation of its volatile solvent(s), and which can become a solidified layer after evaporation of at least a portion of the volatile solvent(s).
  • the solidified layer once formed, can be very durable. In one embodiment, once solidified on a skin surface, the formulation can form a peel.
  • the peel can be a soft, coherent solid that can be removed by peeling large pieces from the skin relative to the size of the applied formulation, and often, can be peeled from the skin as a single piece.
  • the application viscosity is typically more viscous than a water-like liquid, but less viscous than a soft solid.
  • preferred viscosities include materials that have consistencies similar to pastes, gels, ointments, and the like, e.g., viscous liquids that flow but are not subject to spilling.
  • a composition when a composition is said to have a viscosity "suitable for application" to a skin surface, this means the composition has a viscosity that is high enough so that the composition does not substantially run off the skin after being applied to skin, but also has a low enough viscosity so that it can be easily spread onto the skin.
  • a viscosity range that meets this definition can be from about 100 cP to about 3,000,000 cP (centipoises), and more preferably from about 1 ,000 cP to about 1 ,000,000 cP.
  • the additional adhesive agent or substance can be an additional non-volatile solvent or an additional solidifying agent.
  • Non-limiting examples of substances which might be used as additional adhesion enhancing agents include copolymers of methylvinyl ether and maleic anhydride (Gantrez polymers), polyethylene glycol and polyvinyl pyrrolidone, gelatin, low molecular weight polyisobutylene rubber, copolymer of acrylsan alkyl/octylacrylamido (Dermacryl 79), and/or various aliphatic resins and aromatic resins. .
  • washable when used with respect to the adhesive formulations of the present invention refers to the ability of the adhesive formulation to be removed by the application of a washing solvent using a normal or medium amount of washing force.
  • the required force to remove the formulations by washing should not cause significant skin irritation or abrasion.
  • gentle washing force accompanied by the application of an appropriate washing solvent is sufficient to remove the adhesive formulations disclosed herein.
  • the solvents which can be used for removing by washing the formulations of the present invention are numerous, but preferably are chosen from commonly acceptable solvents including the volatile solvents listed herein. Preferred washing solvents do not significantly irritate human skin and are generally available to the average subject.
  • washing solvents include but are not limited to water, ethanol, methanol, isopropyl alcohol, acetone, ethyl acetate, propanol, and combinations thereof.
  • the washing solvents can be selected from the group consisting of water, ethanol, isopropyl alcohol and combinations thereof.
  • Surfactants can also be used in some embodiments.
  • An acceptable length of time with respect to "drying time” refers to the time it takes for the formulation to form a non-messy solidified surface after application on skin under standard skin and ambient conditions, and with standard testing procedure. It is noted that the word "drying time” in this application does not mean the time it takes to completely evaporate off the volatile solvent(s). Instead, it means the time it takes to form the non-messy solidified surface as described above.
  • Standard skin is defined as dry, healthy human skin with a surface temperature of between about 30 0 C to about 36°C.
  • Standard ambient conditions are defined by the temperature range of from 20 0 C to 25°C and a relative humidity range of from 20% to 80%.
  • the term "standard skin” in no way limits the types of skin or skin conditions on which the formulations of the present invention can be used.
  • the formulations of the present invention can be used to treat all types of "skin,” including undamaged (standard skin), diseased skin, or damaged skin.
  • skin conditions having different characteristics can be treated using the formulations of the present invention, the use of the term "standard skin” is used merely as a standard to test the compositions of the varying embodiments of the present invention.
  • formulations that perform well e.g., solidify, provide therapeutically effective flux, etc.
  • Standard testing procedure or “standard testing condition” is as follows: To standard skin at standard ambient conditions is applied an approximately 0.1 mm layer of the adhesive solidifying formulation and the drying time is measured. The drying time is defined as the time it takes for the formulation to form a non-messy surface such that the formulation does not lose mass by adhesion to a piece of 100% cotton cloth pressed onto the formulation surface with a pressure of between about 5 and about 10 g/cm 2 for 5 seconds.
  • Solidified layer describes the solidified or dried layer of an adhesive solidifying formulation after at least a portion of the volatile solvent system has evaporated. The solidified layer remains adhered to the skin, and is preferably capable of maintaining good contact with the subject's skin for substantially the entire duration of application under standard skin and ambient conditions.
  • the solidified layer also preferably exhibits sufficient tensile strength so that it can be peeled off the skin at the end of the application in one piece or several large pieces (as opposed to a layer with weak tensile strength that breaks into many small pieces or crumbles when removed from the skin).
  • a plurality of drugs, compounds, and/or solvents may be presented in a common list for convenience. However, these lists should be construed as though each member of the list is individually identified as a separate and unique member. Thus, no individual member of such list should be construed as a de facto equivalent of any other member of the same list solely based on their presentation in a common group without indications to the contrary.
  • an adhesive formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and a solidifying agent.
  • the solvent vehicle can comprise a volatile solvent system including at least one volatile solvent and a non-volatile solvent system including at least two non-volatile solvents.
  • the at least two non-volatile solvents of the non-volatile solvent system can facilitate transdermal delivery of the drug at a therapeutically effective rate over a sustained period of time, even after the non-volatile solvent system is substantially evaporated.
  • the formulation can have viscosity suitable for application to the skin surface prior to evaporation of at least one volatile solvent, and can further be formulated such that when applied to the skin surface, the formulation forms a solidified layer after at least a portion of the volatile solvent system is evaporated. Sustained drug delivery from the solidified layer can also occur.
  • a method of dermally delivering a drug can comprise applying an adhesive solidifying formulation to a skin surface of a subject.
  • the formulation can comprise a drug, solvent vehicle, and a solidifying agent.
  • the solvent vehicle can comprise a volatile solvent system including at least one volatile solvent, and a non-volatile solvent system including at least two non-volatile solvents, wherein the non-volatile solvent system facilitates dermal delivery of the drug at a therapeutically effective rate over a sustained period of time.
  • the formulation can have a viscosity suitable for application and adhesion to the skin surface prior to evaporation of the volatile solvent system
  • Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system; and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time.
  • a solidified layer for delivering a drug can comprise a drug, a non-volatile solvent system including at least two non-volatile solvents, wherein the non-volatile solvent system is capable of facilitating the delivery of the drug at therapeutically effective rates over a sustained period of time, and a solidifying agent.
  • the solidified layer can be stretchable by 5% in at least one direction without cracking, breaking, or separating from a skin surface to which the layer is applied.
  • an adhesive formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and at least two solidifying agents.
  • the solvent vehicle can include a volatile solvent system including at least one volatile solvent, and a non-volatile solvent system including at least one nonvolatile solvent wherein the non-volatile solvent system can be flux-enabling for the drug such that the drug can be delivered in therapeutically effective amounts even after most of the volatile solvent(s) is(are) evaporated.
  • the formulation can have a viscosity suitable for application and adhesion to a skin surface prior to evaporation of the volatile solvent system, and can form a solidified layer after at least partial evaporation of the volatile solvent system after skin application.
  • a method of dermally delivering a drug can comprise applying an adhesive solidifying formulation to a skin surface of a subject.
  • the formulation can include a drug, a solvent vehicle, and at least two solidifying agents.
  • the solvent vehicle can comprise a volatile solvent system including at least one volatile solvent, and a non-volatile solvent system including at least one non-volatile solvent.
  • the formulation can have a viscosity suitable for application and adhesion to the skin surface prior to evaporation of the volatile solvent system.
  • Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system; and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time.
  • a solidified layer for delivering a drug can comprise a drug, a non-volatile solvent system comprising at least one nonvolatile solvent, and at least two polymeric solidifying agents.
  • a formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and a solidifying agent.
  • the solvent vehicle can comprise a volatile solvent system including at least two volatile solvents, and a non-volatile solvent system including at least one non-volatile solvent.
  • the formulation has a viscosity suitable for application and adhesion to a skin surface prior to evaporation of the volatile solvent system wherein the non-volatile solvent system can be flux-enabling for the drug such that the drug can be delivered at a therapeutically effective amount even after most of the volatile solvent(s) is(are) evaporated.
  • the formulation applied to the skin surface can form a solidified layer after at least partial evaporation of the volatile solvent system and can further be formulated such that when applied to the skin surface, the formulation forms a solidified layer after at least a portion of the volatile solvents is (are) evaporated, but yet continues to deliver drug after substantially solidifying. Additionally, the drug can continue to be delivered after the volatile solvent system is at least substantially evaporated.
  • a method of dermally delivering a drug can comprise applying an adhesive solidifying formulation to a skin surface of a subject.
  • the adhesive formulation can comprise a drug, a solvent vehicle, and a solidifying agent.
  • the solvent vehicle can comprise a volatile solvent system including at least two volatile solvent, and a non-volatile solvent system including at least one non-volatile solvent.
  • the formulation can have a viscosity suitable for application and adhesion to the skin surface prior to evaporation of the volatile solvent system.
  • Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system; and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time.
  • the formulations can also contain substances that are solid or liquid at room temperatures, such as pH or ion-pairing agents. After evaporation of the volatile solvent system, most of the non-volatile solvent system should remain in the solidified layer for a period of time sufficient to adequately dermally deliver a given drug to, into, or through the skin of a subject at a sufficient flux for a period of time to provide a therapeutic effect.
  • the nonvolatile solvent system can also serve as a plasticizer of the solidified layer, so that the solidified layer is elastic and flexible.
  • these embodiments exemplify the present invention which is related to novel formulations, methods, and solidified layers that are typically in the initial form of semi-solids (including creams, gels, pastes, ointments, and other viscous liquids), which can be easily applied onto the skin as a layer, and can quickly (from 15 seconds to about 4 minutes under standard skin and ambient conditions) to moderately quickly (from about 4 to about 15 minutes under standard skin and ambient conditions) change into a solidified layer, e.g., a coherent and soft solid layer which can be peelable, for drug delivery.
  • semi-solids including creams, gels, pastes, ointments, and other viscous liquids
  • a solidified layer thus formed is capable of delivering drug to the skin, into the skin, across the skin, etc., at substantially constant rates, over an sustained period of time, e.g., hours to tens of hours, so that most of the active drug is delivered after the solidified layer is formed.
  • a solid layer-forming formulation for dermal drug delivery can use a single solidifying agent
  • the use of two or more solidifying agents in the formulation herein can provide important advantages. This is because in addition to solidifying the formulations, the solidifying agent(s) in the formulation often impacts component compatibility as well as flexibility and skin adhesiveness of the solidified layer. Sometimes it takes two or more solidified agents to address all these needs.
  • the present invention is related to solidifying formulations that use two or more solidified agents to produce better formulation properties than any single solidifying agent alone within a given formulation could accomplish.
  • the solidified layer typically adheres to the skin, but has a solidified, minimally-adhering, outer surface which is formed relatively soon after application and which does not substantially transfer to or otherwise soil clothing or other objects that a subject is wearing or that the solidified layer may inadvertently contact.
  • the solidified layer can also be formulated such that it is highly flexible and stretchable, and thus capable of maintaining good contact with a skin surface, even if the skin is stretched during body movement, such as at a knee, finger, elbow, or other joints.
  • the volatile solvent system can be selected from pharmaceutically or cosmetically acceptable solvents known in the art.
  • the volatile solvent system can include ethanol, isopropyl alcohol, water, dimethyl ether, diethyl ether, butane, propane, isobutene, 1,1 , difluoroethane, 1,1,1,2 tetrafluorethane, 1,1,1,2,3,3,3-heptafluoropropane, 1 ,1 ,1 ,3,3,3 hexafluoropropane, ethyl acetate, acetone or combinations thereof.
  • the volatile solvent system can include iso-amyl acetate, denatured alcohol, methanol, propanol, isobutene, pentane, hexane, chlorobutanol, turpentine, cytopentasiloxane, cyclomethicone, methyl ethyl ketone, or combinations thereof.
  • the volatile solvent system can include a mixture or combination of any of the volatile solvents set forth in the embodiments above.
  • the volatile solvent system comprises at least one volatile solvent with a boiling point higher than 20 0 C (a liquid volatile solvent) and at least one volatile solvent with a boiling point lower than about 20 0 C (gaseous volatile solvents).
  • Boiling points refer to boiling points measured at normal atmospheric pressure.
  • Formulations of the present invention which have both liquid and gas volatile solvents can have significantly shorter drying times than those with only liquid volatile solvents.
  • concentration of the gas volatile solvent is below the formulations solubility. This allows the formulation to be stored in containers for conventional, un- pressurized semi-solid products. Alternatively, these solvents can be used as propellants for spray-on formulations.
  • gas volatile solvents which may be used in the present invention include but are not limited to ether, dimethyl ether, diethyl ether, propane, isobutene, diflouroethane, butane, 1,1 ,1 ,2 tetraflourethane, 1 ,1,1 ,2,3,3,3-heptaflouropropane, and 1,1,1,3,3,3, hexaflouropropane, and combinations thereof. Additionally, these volatile solvents should be chosen to be compatible with the rest of the formulation. It is desirable to use an appropriate weight percentage of the volatile solvent(s) in the formulation. Too much of the volatile solvent system prolongs the drying time. Too little of the volatile solvent system can make it difficult to spread the formulation on the skin.
  • the weight percentage of the volatile solvent(s) can be from about 10 wt% to about 85 wt%, and more preferably from about 20 wt% to about 50 wt%.
  • the volatile solvent system comprises at least 10 wt% of the formulation. In another embodiment, the volatile solvent system comprises at least about 20 wt% of the formulation.
  • the volatile solvent system can also be chosen to be compatible with the non-volatile solvent system, solidifying agent, drug, and any other excipients that may be present.
  • polyvinyl alcohol (PVA) is not soluble in ethanol. Therefore, a volatile solvent which will dissolve PVA needs to be formulated in the solidified layer. For instance, water will dissolve PVA and can be utilized as a volatile solvent in a formulation; however, the drying time in such a formulation may be too long to certain applications. Therefore, a second volatile solvent (e.g., ethanol) can be formulated into the formulation to reduce the water content but maintain a sufficient amount of water to keep PVA in solution and thereby reduce the drying time for the formulation.
  • a second volatile solvent e.g., ethanol
  • the volatile solvent system can be chosen to reduce drying time for the formulation.
  • a second volatile solvent e.g., ethanol
  • the volatile solvent can be chosen to improve solubility of a particular drug form utilized in the formulation. For example, ropivacaine HCI is not soluble in non-volatile solvents isostearic acid, triacetin, and Span 20.
  • one of the volatile solvents of the volatile solvent system can be less volatile than the other.
  • the less volatile solvent can have better compatibility with the solidifying agent as compared to a more volatile solvent in the solvent system.
  • volatile solvent retaining substances can include water, hygroscopic substances, honey, glycerol, propylene glycol, and the like.
  • the non-volatile solvent system can also be chosen or formulated to be compatible with the solidifying agent, the drug, the volatile solvent, and any other ingredients that may be present.
  • the solidifying agent can be chosen so that it is dispersible or soluble in the non-volatile solvent system. Most non-volatile solvent systems and solvent vehicles as a whole will be formulated appropriately after experimentation.
  • PEG 400 poly ethylene glycol
  • glycerol non-volatile solvent
  • water volatile solvent
  • PEG 400 cannot effectively dissolve poly vinyl alcohol (PVA), and thus, is not very compatible alone with PVA, a solidifying agent.
  • PVA poly vinyl alcohol
  • a non-solvent system including PEG 400 and glycerol (compatible with PVA) in an appropriate ratio can be formulated, achieving a compatibility compromise.
  • non-volatile solvent/solidifying agent incompatibility is observed when Span 20 is formulated into a formulation containing PVA. With this combination, Span 20 can separate out of the formulation and form an oily layer on the surface of the solidified layer. Thus, appropriate solidifying agent/nonvolatile solvent selections are desirable in developing a viable formulation and compatible combinations. It is not necessary that both the non-volatile solvents of the non-volatile solvent system be compatible with the solidifying agent. In some embodiments one of the non-volatile solvents of the non-volatile solvent system can be present to provide compatibility with the solidifying agent while a second non-volatile solvent can act as the flux enabling non-volatile solvent.
  • the at least two non-volatile solvents that can be used to form non-volatile solvent systems can be selected from a variety of pharmaceutically acceptable liquids.
  • the non-volatile solvent system can include glycerol, propylene glycol, isostearic acid, oleic acid, propylene glycol, trolamine, tromethamine, triacetin, sorbitan monolaurate, sorbitan monooleate, sorbitan monopalmitate, butanol, or combinations thereof.
  • the non-volatile solvent system can include benzoic acid, butyl alcohol, dibutyl sebecate, diglycerides, dipropylene glycol, eugenol, fatty acids such as coconut oil, fish oil, palm oil, grape seed oil, isopropyl myristate, mineral oil, oleyl alcohol, vitamin E, triglycerides, sorbitan fatty acid surfactants, triethyl citrate, or combinations thereof.
  • benzoic acid butyl alcohol, dibutyl sebecate, diglycerides, dipropylene glycol, eugenol, fatty acids such as coconut oil, fish oil, palm oil, grape seed oil, isopropyl myristate, mineral oil, oleyl alcohol, vitamin E, triglycerides, sorbitan fatty acid surfactants, triethyl citrate, or combinations thereof.
  • the non-volatile solvent system can include 1 ,2,6-hexanetriol, alkyltriols, alkyldiols, acetyl monoglycerides, tocopherol, alkyl dioxolanes, p-propenylanisole, anise oil, apricot oil, dimethyl isosorbide, alkyl glucoside, benzyl alcohol, bees wax, benzyl benzoate, butylene glycol, caprylic/capric triglyceride, caramel, cassia oil, castor oil, cinnamaldehyde, cinnamon oil, clove oil, coconut oil, cocoa butter, cocoglycerides, coriander oil, corn oil, coriander oil, corn syrup, cottonseed oil, cresol, cyclomethicone, diacetin, diacetylated monoglycerides, diethanolami ⁇ e, dietthylene glycol monoethyl ether, diglycer
  • non-volatile solvent system can include a combination or mixture of non-volatile solvents set forth in any of the above discussed embodiments.
  • the non-volatile solvent system or at least one of the non-volatile solvents in the non-volatile solvent system can also serve as plasticizer in the adhesive formulation so that when the solidified layer is formed, the layer is flexible, stretchable, and/or otherwise "skin friendly.”
  • Certain volatile and/or nonvolatile solvent(s) that are irritating to the skin may be desirable to use to achieve the desired solubility and/or permeability of the drug. It is also desirable to add compounds that are both capable of preventing or reducing skin irritation and are compatible with the formulation. For example, in a formulation where the volatile solvent is capable of irritating the skin, it would be helpful to use a non-volatile solvent that is capable of reducing skin irritation. Examples of solvents that are known to be capable of preventing or reducing skin irritation include, but are not limited to, glycerin, honey, and propylene glycol.
  • non-volatile solvents can provide advantageous benefits such as acting as a plasticizer, improve adhesion, reducing skin irritation, inhibiting phase separation, and the like.
  • at least on of the at least two non-volatile solvents present in the non-volatile solvent system can act to promote the flux of one of the drugs while the other non-volatile solvent promotes the flux of the other drug.
  • the two or more non-volatile solvents of the non-volatile solvent system of the present invention may be such that the non-volatile solvents used independently are not flux-enabling non-volatile solvents for a drug but when formulated together become a flux-enabling non-volatile solvent.
  • One possible reason for these initially non enabling non-volatile solvents to become enabling non-volatile solvents when formulated together may be due to the optimization of the ionization state of the drug to a physical form which has higher flux or the non-volatile solvents act in some other synergistic manner.
  • non-volatile solvents may optimize the pH of the formulation or the skin tissues under the formulation layer to minimize irritation.
  • suitable combinations of non-volatile solvents that result in an adequate non-volatile solvent system include but are not limited to isostearic acid /trolamine, isostearic acid /diisopropyl amine, oleic acid/trolamine, and propylene glycol /isostearic acid.
  • the selection of the solidifying agent can also be carried out in consideration of the other components present in the adhesive formulation.
  • the solidifying agent can be selected or formulated to be compatible to the drug and the solvent vehicle (including the volatile solvent(s) and the non-volatile solvent system), as well as to provide desired physical properties to the solidified layer once it is formed.
  • the solidifying agent can be selected from a variety of agents.
  • the solidifying agent can include polyvinyl alcohol with a MW range of 20,000-70,000 (Amresco), esters of polyvinylmethylether/maleic anhydride copolymer (ISP Gantrez ES-425 and Gantrez ES-225) with a MW range of 80,000-160,000, neutral copolymer of butyl methacrylate and methyl methacrylate (Degussa Plastoid B) with a MW range of 120,000-180,000, dimethylaminoethyl methacrylate-butyl methacrylate- methyl methacrylate copolymer (Degussa Eudragit E100) with a MW range of 100,000-200,000, ethyl acrylate-methyl methacrylate-trimethylammonioethyl methacrylate chloride copolymer with a MW greater than 5,000 or similar MW to Eudragit RLPO (Degussa), Zein (prolamine) with a MW greater than
  • the solidifying agent can include ethyl cellulose, hydroxy ethyl cellulose, hydroxy methyl cellulose, hydroxy propyl cellulose, hydroxypropyl methyl cellulose, carboxymethyl cellulose, methyl cellulose, polyether amides, corn starch, pregelatinized corn starch, polyether amides, shellac, polyvinyl pyrrolidone, polyisobutylene rubber, polyvinyl acetate phthalate, or combinations thereof.
  • the solidifying agent can include ammonia methacrylate, carrageenan, cellulose acetate phthalate aqueous such as CAPNF from Eastman, carboxy polymethylene, cellulose acetate (microcrystalline), cellulose polymers, divinyl benzene styrene, ethylene vinyl acetate, silicone, guar gum, guar rosin, gluten, casein, calcium caseinate, ammonium caseinate, sodium caseinate, potassium casei ⁇ ate, methyl acrylate, microcrystalline wax, polyvinyl acetate, PVP ethyl cellulose, acrylate, PEG/PVP, xantham gum, trimethyl siloxysilicate, maleic acid/anhydride colymers, polacrilin, poloxamer, polyethylene oxide, poly glactic acid/poly-l-lactic acid, turpene resin, locust bean gum, acrylic copolymers, polyurethane dispersions, dextrin, polyvinyl
  • the solidifying agent can include a combination of solidifying agents set forth in the any of the above discussed embodiments.
  • Other polymers may also be suitable as the solidifying agent, depending on the solvent vehicle components, the drug, and the specific functional requirements of the given formulation.
  • Other polymers may also be suitable as the solidifying agent, depending on the solvent vehicle components, the drug, and the specific functional requirements of the given formulation.
  • the non-volatile solvent system and the solidifying agent(s) should be compatible with each other.
  • Compatibility can be defined as i) the solidifying agent does not substantially negatively influence the function of the non-volatile solvent system, except for some reduction of flux; ii) the solidifying agent can hold the non-volatile solvent system in the solidified layer so that substantially no non-volatile solvent oozes out of the layer, and/or iii) the solidified layer formed with the selected non-volatile solvent system and the solidifying agent has acceptable flexibility, rigidity, tensile strength, elasticity, and adhesiveness.
  • the weight ratio of the non-volatile solvent system to the solidifying agent(s) can be from about 0.1 :1 to about 10:1. In another aspect, the ratio between the non-volatile solvent system and the solidifying agent can be from about 0.5:1 to about 2:1.
  • the use of at least two solidifying agents can provide superior peel characteristics. Desirable characteristics can include enhanced elasticity, enhanced skin adhesion, enhanced tensile strength, and the like.
  • the combination of the at least two solidifying agents can provide a more homogenous formulation with minimal if any phase separation.
  • polyvinyl alcohol (PVA) can be used as one of the solidifying agents in combination with Gantrez. In that combination, the PVA functions to provide enhanced elasticity while the Gantrez provides enhanced skin adhesion.
  • a formulation can be made which utilizes Eudgragit E-100 in combination with PVA as the solidifying agent. The formulation has quicker solidifying characteristics and results in a solidified layer with enhanced tensile strength.
  • the thickness of the formulation layer applied on the skin should also be appropriate for a given formulation and desired drug delivery considerations. If the layer is too thin, the amount of the drug may not be sufficient to support sustained delivery over the desired length of time. If the layer is too thick, it may take too long to form a non-messy outer surface of the solidified layer. If the drug is very potent and the solidified layer has very high tensile strength, a layer as thin as 0.01 mm may be sufficient. If the drug has rather low potency and the solidified layer has low tensile strength, a layer as thick as 2-3 mm may be desirable. Thus, for most drugs and formulations, the appropriate thickness can be from about 0.01 mm to about 3 mm, but more typically, from about 0.05 mm to about 1 mm.
  • the flexibility and stretchability of a solidified layer can be desirable in some applications.
  • the solidified layer is coherent, flexible, and continuous.
  • Such flexible and coherent nature can greatly enhance the ease of use of the formulation.
  • certain nonsteroidal anti-inflammatory agents NSAIDs
  • NSAIDs nonsteroidal anti-inflammatory agents
  • skin areas over joints and certain muscle groups are often significantly stretched during body movements. Such movement prevents non-stretchable patches from maintaining good skin contact.
  • Lotions, ointments, creams, gels, foams, pastes, or the like also may not be suitable for use for the reasons cited above.
  • the solidifying formulations of the present invention can offer unique advantages and benefits. It should be pointed out that although good stretchability can be desirable in some applications.
  • the solidifying formulations of the present invention do not always need to be stretchable, as certain applications of the present invention do not necessarily benefit from this property. For instance, if the formulation is applied on a small facial area overnight for treating acne, a subject would experience minimal discomfort and formulation-skin separation even if the solidified layer is not stretchable, as facial skin usually is not stretched very much during a sleep cycle.
  • a further feature of a formulation prepared in accordance with embodiments of the present invention is related to drying time. If a formulation dries too quickly, the user may not have sufficient time to spread the formulation into a thin layer on the skin surface before the formulation is solidified, leading to poor skin contact. If the formulation dries too slowly, the subject may have to wait a long time before resuming normal activities (e.g. putting clothing on) that may remove un-solidified formulation. Thus, it is desirable for the drying time to be longer than about 15 seconds but shorter than about 15 minutes, and preferably from about 0.5 minutes to about 5 minutes.
  • Other benefits of the solidified layers of the present invention include the presence of a physical barrier that can be formed by the material itself.
  • local anesthetic agents and other agents such as clonidine may be delivered topically for treating pain related to neuropathy, such as diabetic neuropathic pain. Since many of such subjects feel tremendous pain, even when their skin area is only gently touched, the physical barrier of the solidified layer can prevent or minimize pain caused by accidental contact with objects or others.
  • the solidified layers of the present invention can be prepared in an initial form that is easy to apply as a semisolid dosage form. Additionally, upon volatile solvent system evaporation, the resulting solidified layer is relatively thick and can contain much more active drug than a typical layer of traditional cream, gel, lotion, ointment, paste, etc., and further, is not as subject to unintentional removal. Further, as the solidified layer remains adhesive and optionally peelable, easy removal of the solidified layer can occur, usually without the aid of a solvent or surfactant.
  • the adhesion to skin and elasticity of the material is such that the solidified layer will not separate from the skin upon skin stretching at highly stretchable skin areas, such as over joints and muscles.
  • the solidified layer can be stretched by 5%, or even 10% or greater, in at least one direction without cracking, breaking, and/or separating form a skin surface to which the solidified layer is applied.
  • the solidified layer can be formulated to advantageously deliver drug and protect sensitive skin areas without cracking or breaking.
  • the solidified layers made using the formulations of the present invention can be soft and coherent solids that are peelable from a skin surface as a single piece or as only a few large pieces relative to the application size.
  • the solidified layer can be removable by use of a solvent, such as water, alcohol, surfactant, or mixture thereof.
  • the solidified layers of the present invention can keep a substantial amount of the non-volatile solvent system, which is optimized for delivering the drug, on the skin surface.
  • This feature can provide unique advantages over existing products. For example, in some semi-solid formulations, upon application to a skin surface the volatile solvents quickly evaporate and the formulation layer solidifies into a hard lacquer-like layer. The drug molecules are immobilized in the hard lacquer layer and are substantially unavailable for delivery into the skin surface. As a result, it is believed that the delivery of the drug is not sustained over a long period of time. In contrast to this type of formulation, the solidified layers formed using the formulations of the present invention keep the drug molecules quite mobile in the non-volatile solvent system which is in contact with the skin surface, thus ensuring sustained delivery.
  • a solidified layer including bupivacaine, lidocaine, or ropivacaine can be formulated for treating diabetic and post herpetic neuralgia.
  • dibucanine and an alpha-2 agonist such as clonidine can be formulated in a solidified layer for treating the same disease.
  • retinoic acid and benzoyl peroxide can be combined in a solidified layer for treating acne, or alternatively, 1 wt% clindamycin and 5 wt% benzoyl peroxide can be combined in a solidified layer for treating acne.
  • a retinol solidifying formulation can be prepared for treating wrinkles, or a lidocaine solidifying formulation can be prepared for treating back pain.
  • a zinc oxide solidifying formulation (OTC) can be prepared for treating diaper rash, or an antihistamine solidified layer can be prepared for treating allergic rashes such as poison ivy.
  • Additional applications include delivering drugs for treating certain skin conditions, e.g., dermatitis, psoriasis, eczema, skin cancer, viral infections such as cold sore, genital herpes, shingles, etc., particularly those that occur over joints or muscles where a transdermal patch may not be practical.
  • drugs for treating certain skin conditions e.g., dermatitis, psoriasis, eczema
  • skin cancer e.g., dermatitis, psoriasis, eczema
  • viral infections such as cold sore, genital herpes, shingles, etc.
  • solidifying formulations containing imiquimod can be formulated for treating skin cancer, common and genital warts, and actinic keratosis.
  • Solidifying formulations containing antiviral drugs such as acyclovir, penciclovir, famciclovir, vaiacyclovir, steroids, behenyl alcohol can be formulated for treating herpes viral infections such as cold sores on the face and genital areas.
  • Solidifying formulations containing non-steroidal anti-inflammatory drugs (NSAIDs), capsaicin, alpha-2 agonists, and/or nerve growth factors can be formulated for treating soft tissue injury and muscle-skeletal pains such as joint and back pain of various causes. As discussed above, patches over these skin areas typically do not have good contact over sustained period of time, especially for a physically active subject, and may cause discomfort.
  • solidified adhesive formulations of the present invention address the shortcomings of both of these types of delivery systems.
  • a further embodiment involves a formulation containing at least one alpha-2 agonist drug, at least one tricyclic antidepressant agent, and/or at least one local anesthetic drug which is applied topically to treat neuropathic pain.
  • the drugs are gradually released from the formulation to provide pain relief over a sustained period of time.
  • the formulation can become a coherent, soft solid after 2-5 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
  • Another embodiment involves a formulation containing capsaicin which is applied topically to treat neuropathic pain.
  • the capsaicin is gradually released from the formulation for treating this pain over a sustained period of time.
  • the formulation can become a coherent, soft solid after 2-5 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
  • solidifying formulations containing tazorac for treating stretch marks, wrinkles, sebaceous hyperplasia, seborrheic keratosis.
  • solidifying formulations containing glycerol can be made so as to provide a protective barrier for fissuring on finger tips.
  • Still another embodiment can include a formulation containing a drug selected from the local anesthetic class such lidocaine and ropivacaine or the like, or NSAID class, such as ketoprofen, piroxicam, diclofenac, indomethacin, or the like, which is applied topically to treat symptoms of back pain, muscle tension, or myofascial pain or a combination thereof.
  • the local anesthetic and/or NSAID is gradually released from the formulation to provide pain relief over a sustained period of time.
  • the formulation can become a coherent, soft solid after about 2-5 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
  • a similar embodiment can include a formulation containing drugs capsaicin and a local anesthetic drug which is applied topically to the skin to provide pain relief.
  • Another embodiment can include a formulation containing the combination of a local anesthetic and a NSAID.
  • the drugs are gradually released from the formulation to provide pain relief over a sustained period of time.
  • the formulation can become a coherent, soft solid after 2-4 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
  • solidifying formulations for the delivery of drugs that treat the causes or symptoms of diseases involving joints and muscles can also benefit from the systems, formulations, and methods of the present invention.
  • diseases that may be applicable include, but not limited to, osteoarthritis (OA), rheumatoid arthritis (RA), joint and skeletal pain of various other causes, myofascial pain, muscular pain, and sports injuries.
  • Drugs or drug classes that can be used for such applications include, but are not limited to, non-steroidal anti-inflammatory drugs (NSAIDs) such as ketoprofen and diclofanec, COX-2 selective NSAIDs and agents. COX-3 selective NSAIDs and agents, local anesthetics such as lidocaine, bupivacaine, ropivacaine, and tetracaine, steroids such as dexamethasone.
  • NSAIDs non-steroidal anti-inflammatory drugs
  • COX-2 selective NSAIDs and agents COX-3 selective NSAIDs and agents, local anesthetics such as
  • Delivering drugs for the treatment of acne and other skin conditions can also benefit from principles of the present invention, especially when delivering drugs having low skin permeability.
  • topical retinoids, peroxides, and antibiotics for treating acne are mostly applied as traditional semisolid gels or creams.
  • sustained delivery over many hours is unlikely.
  • clindamycin, benzoyl peroxide, and erythromycin may be efficacious only if sufficient quantities are delivered into hair follicles.
  • a traditional semisolid formulation such as the popular acne medicine benzaclin gel, typically loses most of its solvent (water in the case of benzaclin) within a few minutes after the application.
  • the formulations of the present invention typically do not have this limitation.
  • the delivery of drugs for treating neuropathic pain can also benefit from the methods, systems, and formulations of the present invention.
  • a patch containing a local anesthetic agent, such as LidodermTM is widely used for treating neuropathic pain, such as pain caused by post-herpetic neuralgia and diabetes induced neuropathic pain. Due to the limitations of the patch as discussed above, the solidified layers prepared in accordance with the present invention provide some unique benefits, as well as provide a potentially less expensive alternative to the use of a patch.
  • Possible drugs delivered for such applications include, but are not limited to, local anesthetics such as lidocaine, prilocaine, tetracaine, bupivicaine, etidocaine; and other drugs including capsaicin and alpha-2 agonists such as clonidine, dissociative anesthetics such as ketamine, tricyclic antidepressants such as amitriptyline,.
  • local anesthetics such as lidocaine, prilocaine, tetracaine, bupivicaine, etidocaine
  • other drugs including capsaicin and alpha-2 agonists such as clonidine, dissociative anesthetics such as ketamine, tricyclic antidepressants such as amitriptyline,.
  • the solidifying formulations of the present invention can be formulated to treat a variety of conditions and disease such as musculoskeletal pain, neuropathic pain, alopecia, skin disease including dermatitis and psoriasis as well as skin restoration (cosmetic skin treatment), and infections including viral, bacterial, and fungal infection.
  • the formulations can deliver a wide ranging number and types of drugs and active agents.
  • the solidifying formulation can be formulated to include acyclovir, econazole, miconazole, terbinafine, lidocaine, bupivacaine, ropivacaine, and tetracaine, amitriptyline, ketanserin, betamethasone dipropionate, triamcinolone acetonide, clindamycin, benzoyl peroxide, tretinoin, Isotretinoin, clobetasol propionate, halobetasol propionate, ketoprofen, piroxicam, diclofenac, indomethacin, imiquimod, salicylic acid, benzoic acid, or combinations thereof
  • the formulation can include an antifungal drug such as amorolfine, butenafine, naftifine, terbinafine, fluconazole, itraconazole, ketoconazole, posaco ⁇ azole, ravuconazole, vori
  • the formulation can include an antifungal drug such as acyclovir, penciclovir, famciclovir, valacyclovir, behenyl alcohol, trifluridine, idoxuridine, cidofovir, gancyclovir, podofilox, podophyllotoxin.ribavirin, abacavir, delavirdine, didanosine, efavirenz, lamivudine, nevirapine, stavudine, zalcitabine, zidovudine, amprenavir, indinavir, nelfinavir, ritonavir, saquinavir, amantadine, interferon, oseltamivir, ribavirin, rimantadine, zanamivir, or combinations thereof.
  • an antifungal drug such as acyclovir, penciclovir, famciclovir, valacyclovir, behenyl alcohol
  • the formulation When the formulation is intended to provide antibacterial treatment it can be formulated to include an antibacterial drug such as erythromycin, clindamycin, tetracycline, bacitracin, neomycin, mupiroci ⁇ , polymyxin B, quinolones such as ciproflaxin, or combinations thereof.
  • an antibacterial drug such as erythromycin, clindamycin, tetracycline, bacitracin, neomycin, mupiroci ⁇ , polymyxin B, quinolones such as ciproflaxin, or combinations thereof.
  • the formulation when the formulation is intended to relieve pain, particularly neuropathic pain, can include a local anesthetic such as lidocaine, bupivacaine, ropivacaine, and tetracaine; an alpha-2 agonists such as clonidine.
  • a local anesthetic such as lidocaine, bupivacaine, ropivacaine, and tetracaine
  • an alpha-2 agonists such as clonidine.
  • the formulation when the formulation is intended to treat pain associated with inflammation it can be formulated to include an non-steroidal anti-inflammatory drug such as ketoprofen, piroxicam, diclofenac, indomethacin, COX inhibitors general COX inhibitors, COX-2 selective inhibitors, COX-3 selective inhibitors, or combinations thereof
  • the formulation can be formulated to treat skin disorders or blemishes by including active agents such as anti-acne drugs such as clindamycin and benzoyl peroxide, retinol, vitamin A derivatives such as tazarotene and isotretinoin, cyclosporin, anthralin, vitamin D3, cholecalciferol, calcitriol, calcipotriol, tacalcitol, calcipotriene, or combinations thereof.
  • active agents such as anti-acne drugs such as clindamycin and benzoyl peroxide, retinol, vitamin A derivatives such as tazarotene and isotretinoin, cyclosporin, anthralin, vitamin D3, cholecalciferol, calcitriol, calcipotriol, tacalcitol, calcipotriene, or combinations thereof.
  • the delivery of medication for treating warts and other skin conditions would also benefit from long periods of sustained drug delivery.
  • anti-wart compounds include but are not limited to:imiquimod, rosiquimod, keratolytic agents: salicylic acid, alpha hydroxy acids, sulfur, rescorcinol, urea, benzoyl peroxide, allantoin, tretinoin, trichloroacetic acid, lactic acid, benzoic acid, or combinations thereof.
  • a further embodiment involves the use of the solidifying formulations for the delivery of sex steroids including but not limited to progestagens consisting of progesterone, norethindrone, norethindroneacetate, desogestrel, drospirenone, ethynodiol diacetate, norelgestromin, norgestimate, levonorgestrel, dl-norgestrel, cyproterone acetate, dydrogesterone, medroxyprogesterone acetate, chlormadinone acetate, megestrol, promegestone, norethisterone, lynestrenol, gestodene, tibolene, androgens consisting of testosterone, methyl testosterone, oxandrolone, androstenedione, dihydrotestosterone.
  • estrogens consisting of estradiol, ethniyl estradiol, estiol, estrone, conjug
  • Non-sex steroids can also be delivered using the formulations of the present invention.
  • examples of such steroids include but are not limited to betamethasone dipropionate, halobetasol propionate, diflorasone diacetate, triamcinolone acetonide, desox ⁇ methasone, fluocinonide, halcinonide, mometasone furoate, betamethasone valerate, fluocinonide, fluticasone propionate, triamcinolone acetonide, fluocinolone acetonide, flurandrenolide, desonide, hydrocortisone butyrate, hydrocortisone valerate, alclometasone dipropionate, flumethasone pivolate, hydrocortisone, hydrocortisone acetate, or combinations thereof.
  • a further embodiment involves controlled delivery of nicotine for treating nicotine dependence among smokers and persons addicted to nicotine.
  • Formulations of the present invention would be a cost effective way of delivering
  • Another embodiment involves using the formulation to deliver antihistamine agents such as diphenhydramine and tripelennamine. These agents would reduce itching by blocking the histamine that causes the itch and also provide relief by providing topical analgesia.
  • antihistamine agents such as diphenhydramine and tripelennamine.
  • drugs which can be delivered using the solidifying formulations of the present invention include but are not limited to tricyclic anti-depressants such as amitriptyline; anticonvulsants such as carbamazepine and alprazolam; N-methyl-D-aspartate (NMDA) antagonists such as ketamine; 5-HT2A receptor antagonists such as ketanserin; and immune modulators such as tacrolimus and picrolimus.
  • tricyclic anti-depressants such as amitriptyline
  • anticonvulsants such as carbamazepine and alprazolam
  • N-methyl-D-aspartate (NMDA) antagonists such as ketamine
  • 5-HT2A receptor antagonists such as ketanserin
  • immune modulators such as tacrolimus and picrolimus.
  • Other drugs that can be delivered using the formulations and methods of the current invention include humectants, emollients, and other skin care compounds.
  • HMS Hairless mouse skin
  • HEM human epidermal membrane
  • SC stratum corneum
  • Skin flux ( ⁇ g/cm 2 /h) is determined from the steady-state slope of a plot of the cumulative amount of permeation versus time. It is to be noted that human cadaver skin can be used as the model membrane for the in vitro flux studies as well. The mounting of the skin and the sampling techniques used as the same as described above for the HMS studies.
  • Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 6-28 hours. If the experiment was continued it is anticipated the steady state would continue.
  • Adhesive formulations containing 0.05% (w/w) clobetasol propionate with propylene glycol and isostearic acid as non volatile solutions and various solidifying agents are prepared.
  • the formulations are prepared from the ingredients as shown in Table 5.
  • compositions shown above are studied for flux of clobetasol propionate as shown in Table 6 as follows:
  • Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 6-28 hours. If the experiment was continued it is anticipated the steady state would continue.
  • Example 3 As seen from Table 6 formulation described in Example 3 that contains polyvinyl alcohol as solidifying agent has high flux of clobetasol propionate.
  • Polyvinyl alcohol is known to form stretchable films and it is likely that this formulation will have acceptable wear properties.
  • the toughness of the resulting film can be modified by adding appropriate plasticizers if needed. Tackiness can also be modified by adding appropriate amounts of tackifier or by adding appropriate amounts of another solidifying agent such as Dermacryl 79.
  • a higher percentage of ethanol is needed to dissolve the polymer.
  • the solidifying agent used in Example 8 provides the highest flux of clobetasol propionate among the solidifying agents studied.
  • the wear properties of this formulation can be modified by adding appropriate levels of other ingredients including but not limited to plasticizers, tackifiers, non-volatile solvents and or solidifying agents.
  • Formulations of acyclovir in various non-volatile solvent systems are evaluated. Excess acyclovir is present. The permeation of acyclovir from the test formulations through HMS is presented in Table 7 below.
  • Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed, the steady-state delivery would likely continue well beyond 8 hours.
  • Steady state flux of acyclovir from the above non-volatile solvents are obtained by placing 200 mcL on the stratum corneum side (donor) of hairless mouse skin.
  • the in vitro studies are carried out as described in Example 1.
  • the surprising result showed the polyethylene glycol 400, span 80, ethyl oleate, or ethyl oleate plus trolamine are not flux-enabling solvents for acyclovir (e.g., steady state flux values significantly less than the steady state flux of acyclovir in the marketed product noted in Table 2, where the flux was about 3mcg/cm 2 /h).
  • Prototype solidifying formulations are prepared as follows. Several acyclovir solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 8, as follows:
  • compositions in Table 6 are prepared as follows. Eudragit RL-PO and ethanol are combined in a glass jar and heated with stirring until the RL-PO is dissolved. The isostearic acid and trolamine is added to the RL-PO/ethanol mixture and the mixture is vigorously stirred. Once a uniform mixture is obtained, acyclovir is added to the mixture and the formulation is vigorously mixed.
  • Prototype peel formulations are prepared as follows. Several acyclovir solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 9, as follows:
  • compositions of Examples 14 and 15 as shown in Table 8 are prepared as follows. Eudragit RL-PO and ethanol are combined in a glass jar and heated with stirring until the RL-PO is dissolved. The isostearic acid and diisopropanol amine or Neutrol TE Polyol (BASF) is added to the RL-PO/ethanol mixture and the mixture is vigorously stirred. Once a uniform mixture is obtained, acyclovir is added to the mixture and the formulation is vigorously mixed.
  • Prototype solidifying formulations are prepared as follows. Several acyclovir solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 10, as follows:
  • compositions in Table 10 are prepared as follows. Ethyl cellulose ECN7 or ethyl cellulose ECN 100 and ethanol are combined in a glass jar and heated with stirring until the solid cellulose is dissolved. The isostearic acid and trolamine is added to the cellulose/ethanol mixture and the mixture is vigorously stirred. Once a uniform mixture is obtained, acyclovir is added to the mixture and the formulation is vigorously mixed.
  • Example 10-17 The formulations of Examples 10-17 are tested in a hairless mouse skin (HMS) in vitro model described in Example 1.
  • Table 11 shows data obtained using the experimental process outlined above.
  • Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
  • the formulations of the invention shown above generally provide for significant penetration of the active ingredient, and further, the formulations of Examples 10-12 and 17 are found to be much greater in permeability than the marketed product Zovirax Cream.
  • the quantity of acyclovir that permeated across the HMS stratum corneum over time for Examples 10, 11 , and Zovirax Cream are shown in FIG. 2. Each value shown indicates the mean ⁇ SD of at least three experiments.
  • Examples 10-13 show the impact of the trolamine to isostearic acid (ISA) ratio on acyclovir flux enhancement.
  • the optimal ISA:trolamine ratio is 1 :1 to 2:1 and ratio greater than 4:1 show a significant decrease in the acyclovir skin flux.
  • Example 16 Additions of diisopropanol amine and Neutrol in place of trolamine (Examples 14 and 15 in the formulation show a significant decrease in acyclovir flux values. This may be due to a specific chemical interaction between trolamine and ISA creating an environment within the formulation which facilitates higher skin flux.
  • Examples 16 and 17 utilize a different solidifying agent to evaluate the impact of the solidifying agent on acyclovir flux. Surprisingly, Example 16 shows a significant decrease in acyclovir skin flux, but Example 17, which differed from Example 16 only by the molecular weight of the solidifying agent, shows no impact on acyclovir skin flux compared to a similar ISA:trolamine ratio in Example 10.
  • Examples 10 and 11 show sustained delivery of acyclovir up to 8 hours, it is reasonable to assume based on the drug load and the continued presence of the non volatile solvent that the delivery of acyclovir would continue at the reported flux values for as long as the subject desires to leave the solidifying formulation affixed to the skin.
  • Solidifying formulations are prepared as follows. Several solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 12, as follows:
  • Solidifying formulations of Examples 19-21 are prepared in the following manner:
  • the solidifying agents are dissolved in the volatile solvent (e.g., dissolve polyvinyl alcohol in water, Eudragit polymers in ethanol),
  • the non-volatile solvent is mixed with the solidifying agent/volatile solvent mixture.
  • the flux-enabling non-volatile solvent/solidifying agent/volatile solvent combination is compatible as evidenced by a homogeneous, single phase system that exhibited appropriate drying time, and provided a stretchable solidified layer and steady state flux for the drug (see Example 22 below).
  • HMS hairless mouse skin
  • HEM HEM in vitro model described in Example 1.
  • Table 13 shows data obtained using the experimental process outlined above.
  • Acyclovir, ropivacaine, and testosterone have surprisingly higher steady state flux values when the flux-enabling non-volatile solvent is incorporated into the solidifying formulation. It is speculated that the higher flux values may be the result of contributions of the volatile solvent or the solidifying agent impacting the chemical environment (e.g., increasing solubility) of the drug in the solidifying formulation resulting in higher flux values. Conversely, ketoprofen and diclofenac have lower steady state flux values when the enabling non- volatile solvent is incorporated into the solidifying formulation. This could be the result of the volatile solvent system or solidifying agent having the opposite impact on the chemical environment (e.g., decreasing solubility, physical interactions between drug and solidifying formulation) resulting in lower flux values. The steady state flux value for imiquimod is unchanged when comparing the solidifying formulation with the flux-enabling non-volatile solvent flux values.
  • a formulation with the following composition: 10.4% polyvinyl alcohol, 10.4% polyethylene glycol 400, 10.4% polyvinyl pyrrolidone K-90, 10.4% glycerol, 27.1 % water, and 31.3% ethanol was applied onto a human skin surface at an elbow joint and a finger joint, resulting in a thin, transparent, flexible, and stretchable solidified layer. After a few minutes of evaporation of the volatile solvents (ethanol and water), a solidified layer that was peelable was formed.
  • the non-volatile solvent system of polyethylene glycol and glycerol acts a plasticizer in the formulation.
  • the stretchable solidified layer had good adhesion to the skin and did not separate from the skin on joints when bent, and could easily be peeled away from the skin.
  • Example 27 Three formulations similar to the formulation in Example 27 (replacing ropivacaine base with ropivacaine HCI) are applied on the stratum corneum side of freshly separated hairless mouse skin.
  • the In vitro flux is determined for each formulation as outlined in Example 1.
  • the formulation compositions are noted in Table 14 below.
  • Flux values represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-9 hours. If the experiment was continued it is anticipated the steady state would continue.
  • a solidifying formulation for dermal delivery of imiquimod is prepared which includes a specified amount of imiquimod in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention.
  • the solidifying formulations contained the following components:
  • the flux values represent the mean and SD of three determinations ** Ratio to control calculated by dividing the flux value for each Example by the flux value for Aldara control flux.
  • formulation Examples 27 and 28 demonstrate the importance of the amount of non-volatile solvent in added to the formulation in dictating the flux-generating power of the entire formulation.
  • Formulation Examples 29-31 utilize a different solidifying agent which is compatible in a non-aqueous volatile solvent system (isopropanol).
  • the selection of non-volatile solvent system ISA/triacetin or ISA/Span 20/troIamine/triacetin combination showed no change in the in vitro flux.
  • the increase in vitro flux is shown to be influenced by an increase in the amount of imiquimod present in the formulation. At imiquimod levels above 4% the drug is saturated in the solidifying formulation.
  • Example 29 demonstrated comparable imiquimod flux to the other formulation Examples, but the importance of the non-volatile solvent system and solidifying agent compatibility necessitated the removal of trolamine because this non-volatile solvent negatively influenced the function of the Plastoid B polymer.
  • a solidifying formulation for dermal delivery of imiquimod is prepared which includes a specified amount of imiquimod in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention.
  • the solidifying formulations contained the following components: Table 17 - Imi uimod formulation ingredients
  • In vitro flux of Examples 32-35 is substantially increased compared to the Aldara control.
  • the reason for the improved in vitro flux values is attributed to the addition of salicylic acid.
  • Improved in vitro flux of imiquimod in Examples 32-35 is thought to be due to an ion pair interaction between imiquimod and salicylic acid.
  • the ion pair mechanism is thought that the lipophilicity of the counter ion (salicylic acid) improves the flux of imiquimod across the stratum corneum because it makes imiquimod less 'comfortable' in the formulation.
  • Comparison of the flux of Examples 32-34 show that the selection of the polymer and/or volatile solvents will impact the flux of imiquimod.
  • Example 32 contains PVA and water, one or both of these elements may contribute to an unfavorable medium in which the ion pair can form resulting in a negligible increase in imiquimod flux versus the Aldara control.
  • TEWL transepidermal water loss
  • Placebo Plastoid B formulation similar to the formulation described in Example 5 was applied to the top of the hand and the TEWL was measured on a side immediately adjacent to the solidified layer and on top of the solidified layer.
  • the TEWL measurement on the site covered by the solidified layer was 30% lower than the untreated skin site.
  • a solidifying formulation for dermal delivery of ropivacaine is prepared which includes a specified amount of ropivacaine in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention.
  • the solidifying formulations contained the following components:
  • the flux values represent the mean and SD of three determinations
  • ethanol is used as the volatile solvent
  • ISA, glycerol, trolamine, and PG mixture is used as the non-volatile solvent system.
  • ISA and propylene glycol used together to provide the appropriate solubility for the drug, while being compatible with the Eudragit RL-100 solidifying agent.
  • ISA, PG and glycerol serve as a plasticizer in the peelable formulation after the ethanol (volatile solvent) has evaporated.
  • the steady state flux of ropivacaine from formulation Examples 37 and 38 demonstrate the importance of the non-volatile solvent in dictating the flux- generating power of the entire formulation.
  • a formulation for dermal delivery of lidocaine is prepared which includes a saturated amount of lidocaine in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention.
  • the solidifying formulation is prepared from the ingredients as shown in Table 26. Table 21 - Lidocaine formulation com onents
  • lidocaine formulation in the present example has similar physical properties to the formulations in examples noted above.
  • the transdermal flux across hairless mouse skin is acceptable and steady-state delivery is maintained over 8 hours.
  • a formulation for dermal delivery of amitriptyline and a combination of amitripyline and ketamine is prepared which includes an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention.
  • the solidifying formulation is prepared from the ingredients as shown in Table 23.
  • the ingredients listed above are combined according to the following procedure.
  • the drug(s), water, and triisopropanolamine are combined in a glass jar and mixed until the drug is dissolved.
  • the isostearic acid, triacetin, Span 20, and isopropanol are added to the formulation and mixed well.
  • the polymer Plastoid B is added last and heated to about 60 0 C until the Plastoid B is completely dissolved. Once the polymer solution cooled to room temperature, the formulation is stirred vigorously for 2-3 minutes.
  • a formulation for dermal delivery of ropivacaine is prepared which includes an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention.
  • the solidifying formulation is prepared from the ingredients as shown in Table 25.
  • the ropivacaine HCI, water, and triisopropanolamine are combined in a glass jar and mixed until the drug is dissolved. Then the isostearic acid, triacetin, Span 20, and isopropanol are added to the formulation and mixed well.
  • the polymer Plastoid B is added last and heated to about 60 0 C until the Plastoid B is completely dissolved. Once the polymer solution cooled to room temperature, the formulation is stirred vigorously for 2-3 minutes.
  • Table 26 Steady-state flux of Ropivacaine HCI through hairless mouse skin from various adhesive formulations at 35 0 C
  • Example 44-47 shows the importance of the triacetin, isostearic acid, Span 20 combination in the formulation.
  • formulations were made without Span 20, triacetin, and isostearic acid respectively.
  • the in vitro flux of ropivacaine was impacted.
  • the synergistic combination of the flux-enabling non volatile solvent system is important in obtaining the maximum in vitro flux of ropivacaine.
  • This formulation has the following ingredients in the indicated weight parts:
  • polyvinyl alcohol (USP grade, from Amresco) is a solidifying agent
  • ethyl cellulose and Dermacryl 79 are auxiliary solidifying agents.
  • Isostearic acid and glycerol form the non-volatile solvent system while ethanol and water form the volatile solvent system.
  • Ropivacaine is the drug.
  • Ropvicaine is mixed with ISA.
  • Ethyl cellulose and Dermacryl 79 are dissolved in ethanol.
  • PVA is dissolved in water at temperature of about 60-70 C.
  • the resulting formulation is a viscous fluid.
  • a layer of about 0.1 mm thick is applied on skin, a non-tacky surface is formed in less than 2 minutes. Examples 49-50
  • Anti-fungal solidifying formulations are prepared and a qualitative assessment of the solidified layer's flexibility and viscosity are evaluated.
  • the formulation components are presented in Table 28 below.
  • the solidifying formulation in Example 49 has a low viscosity that was lower than may be desirable for application on a nail or skin surface.
  • the time to form a solidified layer with this formulation is longer than the desired drying time.
  • the formulation in Example 50 had an increase in the amount of solidifying agent (Eudgragit RL-PO) and decrease in amount of ethanol, which improves the viscosity and drying time.
  • Example 50 has a viscosity suitable for application and an improved drying time.
  • a solidifying formulation was prepared in accordance with Table 29, as follows:
  • the solidifying agent is dissolved in the volatile solvent (i.e. dissolve polyvinyl alcohol in water). • The flux enabling non-volatile solvent is mixed with the solidifying agent/volatile solvent mixture.
  • Example 51 The formulation prepared in Example 51 was tested for Skin Flux, as set forth in Table 30 below.
  • AndroGel currently marked product, is applied directly on the hairless mouse skin and the flux determinations are made as outlined in Example 1.
  • the steady state flux data is shown in FIG 1. It should be noted, the steady- state flux value reported in Table 3 is determined using the linear region between 2-6 hours.
  • the in vitro flux of testosterone from AndroGel substantially decreases beyond 6 hours. This may be due in part to the evaporation of the volatile solvent which may act as the main vehicle for delivery.
  • the formulation in Example 51 will deliver a steady-state amount of testosterone for at least g hours.
  • Example 53 A stretchable adhesive formulation for transdermal delivery of ketoprofen
  • the excipient mixture which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 31.
  • Example 53 The compositions of Example 53 were studied for flux of ketoprofen, as shown in Table 32, as follows:
  • Skin flux measurement represents the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
  • Example 53 ethanol and water formed the volatile solvent system, while a 1:1 mixture of glycerol and PEG 400 formed the non-volatile solvent system.
  • PEG 400 is a slightly better solvent than glycerol for ketoprofen, while glycerol is much more compatible with PVA than PEG 400.
  • the non-volatile solvent system of glycerol and PEG 400 are used together to provide a non-volatile solvent system for the drug, while being reasonably compatible with PVA.
  • PVA and PVP act as the solidifying agents.
  • glycerol and PEG 400 also serve as plasticizers in the adhesive formulation formed after the evaporation of the volatile solvents. Without the presence of glycerol and PEG 400, a solidified layer formed by PVA and PVP alone would be rigid and non- stretchable.
  • Example 53 composition A formulation similar to the formulation of Example 53 composition (with no ketoprofen) is applied onto a human skin surface at an elbow joint and a finger joint, resulting in a thin, transparent, flexible, and stretchable solidified layer. After a few minutes of evaporation of the volatile solvents (ethanol and water), a solidified layer is formed.
  • the stretchable solidified layer has good adhesion to the skin and does not separate from the skin on joints when bent, and can easily be peeled away from the skin.
  • a stretchable adhesive formulation for transdermal delivery of ketoprofen (which is suitable for delivery via skin on joints and muscles) is prepared which includes saturated amount of ketoprofen in an excipient mixture (more ketoprofen than that can be dissolved in the excipient mixture) to form an adhesive formulation, some of which are prepared in accordance with embodiments of the present invention.
  • the excipient mixture which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 33. Table 33
  • Formulations A and B are prepared in the following manner:
  • PVA solidifying agent
  • the flux adequate non-volatile solvent glycerol, PG
  • the flux adequate non-volatile solvent is mixed together with the solidifying agent/volatile solvent mixture.
  • Formulations A and B are placed on the skin of human volunteers. After a period of several hours, long enough for the volatile solvent to evaporate, the solidified layers were removed by the volunteers and the peelability properties were evaluated. In all instances the volunteers reported that formulation example A could not be removed in one or two pieces, but was removed in numerous small pieces. Formulation example B removed in one or two pieces.
  • the brittle nature of formulation A is attributed to the lower molecular weight PVA sample (Celvol). Low molecular weight PVA does not possess the same cohesive strength as higher molecular weight PVA material (Amresco) due to the reduced size of the polymer chain leading to a reduction in the degree of cross linking and physical interactions between individual PVA polymer chains. The reduced PVA chain interactions lead to a weakened solidified layer that is unable to withstand the mechanical forces the solidified layer is subjected to upon removal.
  • the excipient mixture which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 34.
  • Solidifying formulations in Examples 56 and 57 are prepared in the following manner:
  • PVA solidifying agent
  • the amount of water in the formulation did not significantly influence the time for the formulation to dry. However, it was noted during the study that the formulation was difficult to expel from the sample tube. After approximately 4 weeks after the formulation in Examples 56 and 57 were made the sample tubes were retrieved and were evaluated for ease of dispensing the formulation. It was noted that the formulation was impossible to expel from the tube. lnterpolymer complexation between Gantrez S-97 and PVA through electrostatic interactions, hydrophobic interactions, hydrogen bonding, or Van derWaals interactions is hypothesized to be the reason(s) for the observed thickening. Moreover, the extent of this interaction may be dependent on the stoichiometric ratio of the two polymers.
  • excipient mixture which will form an adhesive formulation, some of which are prepared in accordance with embodiments of the present invention.
  • the excipient mixture which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 36. Table 36
  • Solidifying formulations in Examples 58-61 are prepared in the following manner: • PVA (solidifying agent) is dissolved in water.
  • Formulations noted above were placed in laminate packaging tubes and stored at 25 C/60% RH and 40 C/ 75% RH conditions until pulled for testing. Physical testing was performed on each formulation. Examples 57-59 have been studied the longest and the resulting viscosity increase necessitated the desire to study the viscosity of Example 60. Table 37 summarizes the data generated on each formulation.
  • Examples 58 and 59 had the lowest water content of the four formulations and within 4 weeks of storage attained high viscosity values.
  • the only difference between Examples 58 and 59 is the amount of ethanol in the formulations. It was hypothesized that reducing the level of ethanol may reduce the physical thickening of the formulation due to an incompatibility between the PVA and ethanol.
  • the viscosity data show that the higher ethanol formulation (Example 58) had lower initial viscosity, but over the 4 weeks storage the viscosity of both Examples 58 and 59 attained viscosity values that were too high for a viable formulation.
  • Another hypothesis for the formulation thickening is that PVA is not compatible in high concentrations when dissolved in water. Additional formulations with higher water content were prepared to determine if an optimal water amount would keep the formulation from thickening up over time.
  • Example 60 viscosity after 16 weeks has not reached the viscosity values of the initial viscosity values of Examples 58 and 59.
  • Placebo versions of the formulations above were applied on study volunteers and the drying time was assessed by placing a piece of cotton to the application site and then applying a 5 gram weight on the cotton. The cotton and weight was removed after 5 seconds. This procedure was started approximately 3 - 4 minutes after application and at 10 to 60 second intervals thereafter until the cotton was removed without lifting the solidified layer or leaving residue behind.
  • Table 38 The results of the study are summarized in Table 38 below.
  • a stretchable adhesive formulation for transdermal delivery of ketoprofen (which is suitable for delivery via skin for treating inflammation or pain of joints and muscles) is prepared which includes ketoprofen in an exctpient mixture to form an adhesive formulation, some of which is prepared in accordance with embodiments of the present invention.
  • the solidifying formulation is prepared from the ingredients as shown in Table 39.
  • Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
  • Placebo formulations containing Gantrez ES 425 as an adhesive polymer were prepared for wear studies by volunteers.
  • the formulations are shown as examples in Table 41. All the formulations have polyvinyl alcohol as a solidifying agent to provide tensile strength to the solidifying formulation.
  • the amount of propylene glycol in the formulations was decreased from 19.6% (w/w) to 8.7% (w/w), and the amount of glycerol was increased by the same amount to keep the total non-volatile ratio constant. Keeping the non-volatile ratio constant is important as it determines the drying time and the duration of delivery.
  • the placebo formulations are worn on the palms of hand and percentage adherence of the solidified layer formed after evaporation of volatile solvents was observed after 5-6 hours.
  • clobetasol propionate 0.15% (w/w) clobetasol propionate with polyvinyl alcohol as solidifying polymer are prepared for in-vitro flux evaluation.
  • Propylene glycol and oleic acid are the non volatile solvents selected for facilitation of clobetasol propionate delivery.
  • glycerol is added as the non volatile solvent for its plasticizing properties. Ratios of ingredients used in the two formulations are shown in Table 42.
  • Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported are determined from the linear region of the cumulative amount versus time plots. The linear region are observed to be between 6-28 hours. If the experiment is continued, it is anticipated the steady state would continue.
  • Example 43 As seen from Table 43 formulation described in Example 67 that contained polyvinyl alcohol as a solidifying agent and 0.05% clobetasol propionate had 46% flux of clobetasol propionate when compared to the control formulation. Increasing the clobetasol propionate concentration drug concentration to 0.15% (w/w) increased the steady state flux and the flux values were 94% of the control formulation. It is expected that longer duration of application with the solidifying formulation would increase cumulative delivery in-vivo resulting in effective treatment of dermatitis.
  • Adhesive formulations containing 0.05% (w/w) clobetasol propionate with gelatin as solidifying agent are prepared for in-vitro flux evaluation.
  • Propylene glycol, isostearic acid, and oleic acid are used as non-volatile solvents to facilitate delivery of clobetasol.
  • Talc is added as a filler to reduce the drying time the formulation. Ratio of ingredients used in the formulation is shown in Table 44.
  • Table 44 Clobetasol Propionate formulations*
  • the fish gelatin based formulation shown in Example 44 is a water washable formulation and can be easily removed by subjects suffering from hand dermatitis. Steady state flux across human cadaver skin from 3 donors with formulation as described in Example 69 is compared to the commercial clobetasol ointment. The permeation results are shown in Table 45.
  • Skin flux measurements represent e mean and standard deviation of three determinations. Flux measurements reported are determined from the linear region of the cumulative amount versus time plots. The linear region are observed to be between 6-28 hours. If the experiment is continued, it is anticipated the steady state would continue.
  • Example 69 As seen from Table 45, formulation described in Example 69 has 62% higher steady state flux when compared to the commercial ointment. Higher steady state flux would result is expected to reduce inflammation in difficult to treat dermatitis and psoriasis cases.
  • Adhesive formulations containing 0.05% (w/w) clobetasol propionate with gelatin as solidifying polymer are prepared for in-vitro flux evaluation.
  • Propylene glycol, and isostearic acid are used as non-volatile solvents to facilitate delivery of clobetasol.
  • Fumed silica is added as a filler to reduce the drying time the formulation. Ratio of ingredients used in the formulation is shown in Table 46.
  • the fish gelatin based formulation shown in Example 70 is a water washable formulation and can be easily removed by subjects suffering from hand dermatitis. Steady state flux across human cadaver skin from 4 donors with formulation as described in Example 70 is compared to the commercial clobetasol ointment. The permeation results are shown in Table 47. Table 47 - Steady state flux of clobetasol propionate through human cadaver skin at 35 0 C
  • Example 70 has at-least similar or better steady state flux when to compared to the steady state flux with the commercial ointment.
  • fumed silica had a low density and is expected to have a less potential to separate from the formulation.
  • Solidifying formulations for dermal delivery of ropivacaine HCI are prepared which include excipient mixtures in accordance with embodiments of the present invention.
  • the formulations are prepared from the ingredients as shown in Table 48.
  • ingredients are noted as weight percent. ** from Degussa.
  • a prototype peel is prepared in accordance with Table 50 as follows:
  • Example 74 illustrates the necessity of an appropriate selection of a nonvolatile solvent and a solidifying agent. After mixing the formulation of Example 74 together, the formulation turned from a flowable solution into two distinct layers: a soft solid and a liquid layer. The formulation in this state is not spreadable on the skin surface. An incompatibility between trolamine and the Plastoid B polymer is suggested because of the hydrophilic nature of the trolamine and the hydrophobic nature of the polymer resulted in the trolamine being squeezed out of the formulation.
  • Prototype peel formulations are prepared as follows. Several peel formulations are prepared in accordance with embodiments of the present invention in accordance with Table 51 , as follows:
  • the solidifying agents are dissolved in the volatile solvent (e.g., dissolve polyvinyl alcohol in water, Eudragit polymers in ethanol),
  • the flux-enabling non-volatile solvent/solidifying agent/volatile solvent combination is compatible as evidenced by a homogeneous, single phase system that exhibited appropriate drying time, and provided a stretchable peel and steady state flux for the drug (see Example 78 below).
  • Example 78 The formulations of the Examples are tested in a hairless mouse skin
  • HMS human epidermal membrane
  • HEM human epidermal membrane
  • Prototype peels are prepared as follows. Several acyclovir peel formulations are prepared in accordance with embodiments of the present invention in accordance with Table 53 as follows:
  • the formulation was prepared by mixing Plastoid B in isopropyl alcohol until the polymer dissolved, then the remaining components were added and the mixture vigorously stirred until a uniform mixture was obtained.
  • Examples 80 and 81 show the importance of an additional polymer to solve the trolamine/polymer incompatibility.
  • Addition of ethylcellulose (N7 and N100) to the formulation reduced the amount of Plastoid B polymer to a level that is compatible with trolamine.
  • the resulting formulation produced a thickened, easily spreadable formulation.
  • the formulation in Example 82 exhibited precipitation, but the thickening due to addition of the N100 ethylcellulose will prevent the settling of the precipitation.
  • Example 80-72 The formulations of Examples 80-72 are tested in a hairless mouse skin (HMS) in vitro model described in Example 1.
  • Table 54 shows data obtained using the experimental process outlined above.
  • Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
  • Examples 71-82 show similar in vitro flux increase (based on ratio to control) over the Zovirax control. Addition of ethylcellulose to the formulations in Examples 81-83 may increase the occlusion due to the addition of the hydrophobic polymers.
  • Prototype peel formulations are prepared as follows. Several peel formulations are prepared in accordance with embodiments of the present invention in accordance with Table 55, as follows:
  • Example 84 The peel formulation of Example 84 is prepared in the following manner:
  • the solidifying agents are dissolved in the volatile solvent (e.g., dissolve polyvinyl alcohol in water, Eudragit polymers in ethanol),
  • the non-volatile solvent is mixed with the solidifying agents/volatile solvent mixture.
  • the flux-enabling non-volatile solvent/solidifying agents/volatile solvent combination is compatible as evidenced by a homogeneous, single phase system that exhibited appropriate drying time, and provided a stretchable peel and steady state flux for the drug (see Example 85 below).
  • Diclofenac have lower steady state flux values when the enabling non-volatile solvent is incorporated into the peel formulation. This could be the result of the volatile solvent system or the solidifying agents having the opposite impact on the chemical environment (e.g., decreasing solubility, physical interactions between drug and peel formulation) resulting in lower flux values.
  • the steady state flux value for imiquimod is unchanged when comparing the peel formulation with the flux-enabling non-volatile solvent flux values.

Abstract

The present invention is drawn to adhesive formulations, methods of drug delivery, and solidified layers for dermal delivery of a drug. The formulation can include a drug, a solvent vehicle, and at least one solidifying agent. The solvent vehicle can have a volatile solvent system including at least one volatile solvent, and a non-volatile solvent system including at least one non-volatile solvent. The formulation can be formulated to contain at least two volatile solvents, at least two non-volatile solvents, or at least two solidifying agents. The formulation can have a viscosity suitable for application to a skin surface prior to evaporation of the volatile solvents system. When applied to the skin, the formulation can form a solidified layer after at least a portion of the volatile solvent system is evaporated.

Description

COMPOSITIONS AND METHODS FOR DERMAL DELIVERY OF DRUGS
FIELD OF THE INVENTION
The present invention relates generally to systems developed for dermal delivery of drugs. More particularly, the present invention relates to formulations including at least two non-volatile solvents, wherein the formulation as a whole has a viscosity suitable for application as a layer to a skin surface, and which forms a sustained drug-delivering adhesive solidified layer on the skin.
BACKGROUND OF THE INVENTION
Traditional dermal drug delivery systems can generally be classified into two forms: semisolid formulations and dermal patch dosage forms. Semisolid formulations are available in a few different forms, including ointments, creams, foams, pastes, gels, or lotions and are applied topically to the skin. Dermal
(including transdermal) patch dosage forms also are available in a few different forms, including matrix patch configurations and liquid reservoir patch configurations. In a matrix patch, the active drug is mixed in an adhesive that is coated on a backing film. The drug-laced adhesive layer is typically directly applied onto the skin and serves both as means for affixing the patch to the skin and as a reservoir or vehicle for facilitating delivery of the drug. Conversely, in a liquid reservoir patch, the drug is typically incorporated into a solvent system which is held by a thin bag, which can be a thin flexible container. The thin bag can include a permeable or semi-permeable membrane surface that is coated with an adhesive for affixing the membrane to the skin. The membrane is often referred to as a rate limiting membrane (although it may not actually be rate limiting in the delivery process in all cases) and can control transport of the drug from within the thin bag to the skin for dermal delivery.
While patches and semisolid formulations are widely used to deliver drugs into and through the skin, they both have significant limitations. For example, most semisolid formulations usually contain solvent(s), such as water and ethanol, which are volatile and thus evaporate shortly after application. The evaporation of such solvents can cause a significant decrease or even termination of dermal drug delivery, which may not be desirable in many cases. Additionally, semisolid formulations are often "rubbed into" the skin, which does not necessarily mean the drug formulation is actually delivered into the skin.
Instead, this phrase often means that a very thin layer of the drug formulation is applied onto the surface of the skin. Such thin layers of traditional semisolid formulations applied to the skin may not contain sufficient quantity of active drug to achieve sustained delivery over long periods of time. Additionally, traditional semisolid formulations are often subject to unintentional removal due to contact with objects such as clothing, which may compromise the sustained delivery and/or undesirably soil clothing. Drugs present in a semisolid formulation may also be unintentionally delivered to persons who come in contact with a subject undergoing treatment with a topical semisolid formulation. With respect to matrix patches, in order to be delivered appropriately, a drug should have sufficient solubility in the adhesive, as primarily only dissolved drug contributes to the driving force required for skin permeation. Unfortunately, solubility in adhesives that is too low does not generate adequate skin permeation driving force over sustained period of time. In addition, many ingredients, e.g., liquid solvents and permeation enhancers, which could be used to help dissolve the drug or increase the skin permeability, may not be able to be incorporated into many adhesive matrix systems in sufficient quantities to be effective. For example, at functional levels, most of these materials may adversely alter the wear properties of the adhesive. As such, the selection and allowable quantities of additives, enhancers, excipients, or the like in adhesive-based matrix patches can be limited. To illustrate, for many drugs, optimal transdermal flux can be achieved when the drug is dissolved in certain liquid solvent systems, but a thin layer of adhesive in a typical matrix patch often cannot hold enough appropriate drug and/or additives to be therapeutically effective. Further, the properties of the adhesives, such as coherence and tackiness, can also be significantly changed by the presence of liquid solvents or enhancers.
Regarding liquid reservoir patches, even if a drug is compatible with a particular liquid or semisolid solvent system carried by the thin bag of the patch, the solvent system still has to be compatible to the adhesive layer coated on the permeable or semi-permeable membrane; otherwise the drug may be adversely affected by the adhesive layer or the drug/solvent system may reduce the tackiness of the adhesive layer. In addition to these dosage form considerations, reservoir patches are bulkier and usually are more expensive to manufacture than matrix patches.
Another shortcoming of dermal (including transdermal) patches is that they are usually neither stretchable nor flexible, as the backing film (in matrix patches) and the thin fluid bag (in reservoir patches) are typically made of polyethylene or polyester, both of which are relatively non-stretchable materials. If the patch is applied to a skin area that is significantly stretched during body movements, such as a joint, separation between the patch and skin may occur thereby compromising the delivery of the drug. In addition, a patch present on a skin surface may hinder the expansion of the skin during body movements and cause discomfort. For these additional reasons, patches are not ideal dosage forms for skin areas subject to expansion, flexing and stretching during body movements. In view of the shortcomings of many of the current delivery systems, it would be desirable to provide systems, formulations, and/or methods that can i) provide sustained drug delivery over long periods of time; ii) are not vulnerable to unintentional removal by contact with clothing, other objects, or people for the duration of the application time; iii) can be applied to a skin area subject to stretching and expansion without causing discomfort or poor contact to skin; and/or iv) can be easily removed after application and use. SUMMARY OF THE INVENTION
Although film-forming technologies have been used in cosmetic and pharmaceutical preparations, typically, the solvents used in such systems evaporate shortly after application, and thus, are not optimal for sustained- release applications. In accordance with this, it has been recognized that the use of multiple non-volatile solvents, multiple volatile solvents, and/or multiple solidifying agents in the formulation can often optimize sustained drug delivery. In accordance with this, it would be advantageous to provide dermal delivery formulations, systems, and/or methods in the form of adhesive compositions or formulations having a viscosity suitable for application to the skin surface and which form a drug-delivering solidified layer on the skin that is optionally peelable or otherwise easily removable after use. As such, an adhesive formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and at least one solidifying agent. The solvent vehicle can comprise a volatile solvent system including at least one volatile solvent and a non-volatile solvent system including at least one non-volatile solvents. The at least two non-volatile solvents of the non-volatile solvent system can facilitate transdermal delivery of the drug at a therapeutically effective rate over a sustained period of time, even after the non-volatile solvent system is substantially evaporated from the solidified layer. The formulation can have viscosity suitable for application to the skin surface prior to evaporation of at least one volatile solvent, and can further be formulated such that when applied to the skin surface, the formulation forms a solidified layer after at least a portion of the volatile solvent system is evaporated. Sustained drug delivery from the solidified layer can also occur. The formulation is formulated such that it has at least two volatile solvents, at least two non-volatile solvents, at least two solidifying agents, or combinations thereof.
In an alternative embodiment, a method of dermally delivering a drug can comprise applying an adhesive formulation to a skin surface of a subject. The formulation be any formulation as set forth above. Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system, and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time.
In another embodiment, a solidified layer for delivering a drug can comprise a drug, a non-volatile solvent system including at least one nonvolatile solvents, wherein the non-volatile solvent system is capable of facilitating the delivery of the drug at therapeutically effective rates over a sustained period of time, and at least one solidifying agent. In one embodiment, the solidified layer can be stretchable by 5% in one direction without cracking, breaking, or separating from a skin surface to which the layer is applied. The formulation is formulated such that it has at least two non-volatile solvents, at least two solidifying agents, or combinations thereof.
Additional features and advantages of the invention will be apparent from the following detailed description and figures which illustrate, by way of example, features of the invention.
BRIEF DESCRIPTION OF THE DRAWINGS
FIG. 1 is a graphical representation of cumulative amount of testosterone delivered across a biological membrane in vitro over time from a solidified adhesive formulation and a marketed product (AndroGel) in accordance with embodiments of the present invention.
FIG. 2 is a graphical representation of the cumulative amount of acyclovir delivered transdermal^ over time from two separate formulations in accordance with embodiments of the present invention compared to the marketed product Zovirax cream.
DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENT(S)
Before particular embodiments of the present invention are disclosed and described, it is to be understood that this invention is not limited to the particular process and materials disclosed herein as such may vary to some degree. It is also to be understood that the terminology used herein is used for the purpose of describing particular embodiments only and is not intended to be limiting, as the scope of the present invention will be defined only by the appended claims and equivalents thereof. In describing and claiming the present invention, the following terminology will be used.
The singular forms "a," "an," and "the" include plural referents unless the context clearly dictates otherwise. Thus, for example, reference to "a drug" includes reference to one or more of such compositions. "Skin" is defined to include human skin (intact, diseased, ulcerous, or broken), finger and toe nail surfaces, and mucosal surfaces that are usually at least partially exposed to air such as lips, genital and anal mucosa, and nasal and oral mucosa.
The term "drug(s)" refers to any bioactive agent that is applied to, into, or through the skin which is applied for achieving a therapeutic affect. This includes compositions that are traditionally identified as drugs, as well other bioactive agents that are not always considered to be "drugs" in the classic sense, e.g., peroxides, humectants, emollients, etc., but which can provide a therapeutic effect for certain conditions. When referring generally to a "drug," it is understood that there are various forms of a given drug, and those various forms are expressly included. In accordance with this, various drug forms include polymorphs, salts, hydrates, solvates, and cocrystals. For some drugs, one physical form of a drug may possess better physical-chemical properties making it more amenable for getting to, into, or through the skin, and this particular form is defined as the "physical form favorable for dermal delivery." For example the steady state flux of diclofenac sodium from flux enabling nonvolatile solvents is much higher than the steady state flux of diclofenac acid from the same flux enabling non-volatile solvents. It is therefore desirable to evaluate the flux of the physical forms of a drug from non-volatile solvents to select a desirable physical form/non-volatile solvent combination.
The phrases "dermal drug delivery" or "dermal delivery of drug(s)" shall include both transdermal and topical drug delivery, and includes the delivery of drug(s) to, through, or into the skin. "Transdermal delivery" of drug can be targeted to skin tissues just under the skin, regional tissues or organs under the skin, systemic circulation, and/or the central nervous system. "Topical delivery" includes delivery of a drug to a skin tissue, and subsequent absorption into deeper tissues that may occur.
The term "flux" such as in the context of "dermal flux" or "transdermal flux," respectively, refers to the quantity of the drug permeated into or across skin per unit area per unit time. A typical unit of flux is microgram per square centimeter per hour. One way to measure flux is to place the formulation on a known skin area of a human volunteer and measure how much drug can permeate into or across skin within certain time constraints. Various methods (in vivo methods) might be used for the measurements as well. The method described in Example 1 or other similar method (in vitro methods) can also be used to measure flux. Although an in vitro method uses human epidermal membrane obtained from a cadaver, or freshly separated skin tissue from hairless mice rather than measure drug flux across the skin using human volunteers, it is generally accepted by those skilled in the art that results from a properly designed and executed in vitro test can be used to estimate or predict the results of an in vivo test with reasonable reliability. Therefore, "flux" values referenced herein can mean that measured by either in vivo or in vitro methods.
The term "flux-enabling" with respect to the non-volatile solvent system (or solidified layer including the same) refers to a non-volatile solvent system (including one or more non-volatile solvents) selected or formulated specifically to be able to provide therapeutically effective flux for a particular drug(s). For topically or regionally delivered drugs, a flux enabling non-volatile solvent system is defined as a non-volatile solvent system which, alone without the help of any other ingredients, is capable of delivering therapeutic effective levels of the drug across, onto or into the subject's skin when the non-volatile solvent system is saturated with the drug. For systemically targeted drugs, a flux enabling non-volatile solvent system is a non-volatile solvent system that can provide therapeutically effective daily doses over 24 hours when the non-volatile solvent system is saturated with the drug and is in full contact with the subject's skin with no more than 500 cm2 contact area. Preferably, the contact area for the non-volatile solvent system is no more than 100 cm2. Testing using this saturated drug-in-solvent state can be used to measure the maximum flux- generating ability of a non-volatile solvent system. To determine flux, the drug solvent mixture needs to be kept on the skin for a clinically effective amount of time. In reality, it may be difficult to keep a liquid solvent on the skin of a human volunteer for an extended period of time. Therefore, an alternative method to determine whether a solvent system is "flux-enabling" is to measure the in vitro drug permeation across the hairless mouse skin or human cadaver skin using the apparatus and method described in Example 1. This and similar methods are commonly used by those skilled in the art to evaluate permeability and feasibility of formulations. Alternatively, whether a non-volatile solvent system is flux-enabling can be tested on the skin of a live human subject with means to maintain the non-volatile solvent system with saturated drug on the skin, and such means may not be practical for a product. For example, the non-volatile solvent system with saturated drug can be soaked into an absorbent fabric material which is then applied on the skin and covered with a protective membrane. Such a system is not practical as a pharmaceutical product, but is appropriate for testing whether a non-volatile solvent system has the intrinsic ability to provide effective drug flux, or whether it is flux-enabling.
It is also noted that once the formulation forms a solidified layer, the solidified layer can also be "flux enabling" for the drug while some of the nonvolatile solvents remain in the solidified layer, even after the volatile solvents (including water) have been substantially evaporated. The phrase "effective amount," "therapeutically effective amount,"
"therapeutically effective rate(s)," or the like, as it relates to a drug, refers to sufficient amounts or delivery rates of a drug which achieves any appreciable level of therapeutic results in treating a condition for which the drug is being delivered. It is understood that "appreciable level of therapeutic results" may or may not meet any government agencies' efficacy standards for approving the commercialization of a product. It is understood that various biological factors may affect the ability of a substance to perform its intended task. Therefore, an "effective amount," "therapeutically effective amount," or "therapeutically effective rate(s)" may be dependent in some instances on such biological factors to some degree. However, for each drug, there is usually a consensus among those skilled in the art on the range of doses or fluxes that are sufficient in most subjects. Further, while the achievement of therapeutic effects may be measured by a physician or other qualified medical personnel using evaluations known in the art, it is recognized that individual variation and response to treatments may make the achievement of therapeutic effects a subjective decision. The determination of a therapeutically effective amount or delivery rate is well within the ordinary skill in the art of pharmaceutical sciences and medicine.
"Therapeutically effective flux" is defined as the permeation flux of the selected drug that delivers sufficient amount of drug into or across the skin to be clinically beneficial in that some of the patient population can obtain some degree of benefit from the drug flux. It does not necessarily mean that most of the patient population can obtain some degree of benefit or the benefit is high enough to be deemed "effective" by relevant government agencies or the medical profession. More specifically, for drugs that target skin or regional tissues or organs close to the skin surface (such as joints, certain muscles, or tissues/organs that are at least partially within 5 cm of the skin surface),
"therapeutically effective flux" refers to the drug flux that can deliver a sufficient amount of the drug into the target tissues within a clinically reasonable amount of time. For drugs that target the systemic circulation, "therapeutically effective flux" refers to drug flux that, via clinically reasonable skin contact area, can deliver sufficient amounts of the selected drug to generate clinically beneficial plasma or blood drug concentrations within a clinically reasonable time. Clinically reasonable skin contact area is defined as a size of skin application area that most subjects would accept. Typically, a skin contact area of 400 cm2 or less is considered reasonable. Therefore, in order to deliver 4000 meg of a drug to the systemic circulation via a 400 cm2 skin contact area over 10 hours, the flux needs to be at least 4000 mcg/400cm2/10 hour, which equals 1 mcg/cm2/hr. By this definition, different drugs have different "therapeutically effective flux. Therapeutically effective flux may also be different in different subjects and or at different times for even the same subject. However, for each drug, there is usually a consensus among the skilled in the art on the range of doses or fluxes that are sufficient in most subjects at most times.
The following are estimates of flux for some drugs that are therapeutically effective:
Table 1 - In vitro steady state flux values of various drugs
Figure imgf000011_0001
* Flux determined using an in vitro method described in Example 1. ** Estimated flux based on known potency relative to lidocaine.
The therapeutically effective flux values in Table 1 (with the exception of ropivacaine) represent the steady state flux values of marketed products through hairless mouse or human epidermal membrane in an in vitro system described in Example 1. These values are meant only to be estimates and to provide a basis of comparison for formulation development and optimization. The therapeutically effective flux for a selected drug could be very different for different diseases to be treated for, different stages of diseases, different individual subjects, etc. It should be noted that the flux listed may be more than therapeutically effective. The following examples listed in Table 2 illustrate screening of a nonvolatile solvent's flux enabling ability for some of the drugs specifically studied. Experiments were carried out as described in Example 1 below and the results are further discussed in the subsequent Examples 2-9.
Table 2 - In vitro steady state flux values of various drugs from non-volatile solvent systems
Figure imgf000012_0001
* Each value represents the mean and st. dev of three determinations. The in vitro steady state flux values in Table 2 from non-volatile solvents show surprising flux-enabling and non flux-enabling solvents. This information can be used to guide formulation development.
The term "plasticizing" in relation to flux-enabling non-volatile solvent(s) is defined as a flux-enabling non-volatile solvent that acts as a plasticizer for the solidifying agent. A "plasticizer" is an agent which is capable of increasing the percentage elongation of the formulation after the volatile solvent system has at least substantially evaporated. Plasticizers also have the capability to reduce the brittleness of solidified formulation by making it more flexible and/or elastic. For example, propylene glycol is a "flux-enabling, plasticizing non-volatile solvent" for the drug ketoprofen with polyvinyl alcohol as the selected solidifying agent. However, propylene glycol in a formulation of ketoprofen with Gantrez S- 97 or Avalure UR 405 as solidifying agents does not provide the same plasticizing effect. The combination of propylene glycol and Gantrez S-97 or Avalure UR 405 is less compatible and results in less desirable formulation for topical applications. Therefore, whether a given non-volatile solvent is "plasticizing" depends on which solidifying agent(s) is selected.
Different drugs often have different matching flux-enabling non-volatile solvent systems which provide particularly good results. Examples of such are noted in Table 3. Experiments were carried out as described in Example 1 below.
Table 3 - In vitro steady state flux values of various drugs from particularly high flux-enablin non-volatile solvent s stems
Figure imgf000013_0001
* Each value represents the mean.and st. dev of three determinations.
It should be noted that "flux-enabling non-volatile solvent," "flux-enabling, plasticizing non-volatile solvent," or "high flux-enabling non-volatile solvent" can be a single chemical substance or a mixture of two or more chemical substances. For example, the steady state flux value for clobetasol propionate in Table 3 is a 9:1 for propylene glycol:isostearic acid mixture that generated much higher clobetasol flux than propylene glycol or ISA alone (see Table 2). Therefore, the 9:1 propylene glycol:isostearic acid mixture is a "high flux- enabling non-volatile solvent" but propylene glycol or isostearic acid alone is not.
The term "adhesion" or "adhesive" when referring to a solidified layer herein refers to sufficient adhesion between the solidified layer and the skin so that the layer does not fall off the skin during intended use on most subjects. Thus, "adhesive" or the like when used to describe the solidified layer means the solidified layer is adhesive to the skin surface to which the initial formulation layer was originally applied (before the evaporation of the volatile solvent(s)). In one embodiment, it does not mean the solidified layer is adhesive on the opposing side. In addition, it should be noted that whether a solidified layer can adhere to a skin surface for the desired extended period of time partially depends on the condition of the skin surface. For example, excessively sweating or oily skin, or oily substances on the skin surface may make the solidified layer less adhesive to the skin. Therefore, the adhesive solidified layer of the current invention may not be able to maintain perfect contact with the skin surface and deliver the drug over a sustained period of time for every subject under any conditions on the skin surface. A standard is that it maintains good contact with most of the skin surface, e.g. 70% of the total area, over the specified period of time for most subjects under normal conditions of the skin surface and external environment. The terms "flexible," "elastic," "elasticity," or the like, as used herein refer to sufficient elasticity of the solidified layer so that it is not broken if it is stretched in at least one direction by up to about 5%,. and often to about 10% or even greater. For example, a solidified layer that exhibits acceptably elasticity and adhesion to skin can be attached to human skin over a flexible skin location, e.g., elbow, finger, wrist, neck, lower back, lips, knee, etc., and will remain substantially intact on the skin upon stretching of the skin. It should be noted that the solidified layers of the present invention do not necessarily have to have any elasticity in some embodiments.
The term "peelable," when used to describe the solidified layer, means the solidified layer can be lifted from the skin surface in one large piece or several large pieces, as opposed to many small pieces or crumbs.
The term "sustained" relates to therapeutically effective rates of dermal drug delivery for a continuous period of time of at least 30 minutes, and in some embodiments, periods of time of at least about 2 hours, 4 hours, 8 hours, 12 hours, 24 hours, or longer.
The use of the term "substantially" when referring to the evaporation of the volatile solvents means that a majority of the volatile solvents which were included in the initial formulation have evaporated. Similarly, when a solidified layer is said to be "substantially devoid" of volatile solvents, including water, the solidified layer has less than 10 wt%, and preferably less than 5 wt%, of the volatile solvents in the solidified layer as a whole. "Volatile solvent system" can be a single solvent or a mixture of solvents that are volatile, including water and solvents that are more volatile than water. Non-limiting examples of volatile solvents that can be used in the present invention include iso-amyl acetate, denatured alcohol, methanol, ethanol, isopropyl alcohol, water, propanol, C4-C6 hydrocarbons, butane, isobutene, pentane, hexane, acetone, chlorobutanol, ethyl acetate, fluro-chloro- hydrocarbons, turpentine, methyl ethyl ketone, methyl ether, hydrofluorocarbons, ethyl ether, 1 ,1,1,2 tetrafluorethane 1,1,1 ,2,3,3,3-heptafluoropropane, 1,1,1 ,3,3,3 hexafluoropropane, and combinations thereof. "Non-volatile solvent system" in this invention is defined as a mixture of at least two solvents that are each less volatile than water. Similarly, a non-volatile solvent is defined as a solvent that is less volatile than water. The non-volatile solvent system can also contain substances that are solid or liquid at room temperatures, such as pH or ion-pairing agents. After evaporation of the volatile solvent system, most of the non-volatile solvent system should remain in the solidified layer for a period of time sufficient to adequately dermally deliver a given drug to, into, or through the skin of a subject at a sufficient flux for a period of time to provide a therapeutic effect.
The non-volatile solvent system can also serve as a plasticizer of the solidified layer, so that the solidified layer is elastic and flexible. In one embodiment, the non-volatile solvent system provides better plasticizing effects for the solidifying agents than any single non-volatile solvent of the non-volatile solvent system alone. Including multiple non-volatile solvents as part of the non-volatile solvent system can also provide various other benefits. In some cases, a single non-volatile solvent may not provide the formulation with adequate compatibility with other ingredients in the formulation, e.g. volatile solvent system or solidifying agent, and/or the ability to generate therapeutically effective flux of the drug. In one aspect of the invention, the non-volatile solvent system provides better compatibility with the solidifying agent than any single non-volatile solvent of the non-volatile solvent system alone. In another aspect of the invention, the non-volatile solvent system provides higher flux than any single non-volatile solvent of the non-volatile solvent system alone. The present invention allows for combinations of two or more non-volatile solvents which together are able to provide both therapeutically effective drug flux while maintaining formulation component compatibility.
The term "solvent vehicle" describes compositions that include both a volatile solvent system and non-volatile solvent system. The volatile solvent system is chosen so as to evaporate from the adhesive formulation quickly to form a solidified layer, and the non-volatile solvent system is formulated or chosen to substantially remain as part of the solidified layer after volatile solvent system evaporation so as to provide continued delivery of the drug. Typically, the drug can be partially or completely dissolved in the solvent vehicle or formulation as a whole. Likewise, the drug can also be partially or completely solubilizable in the non-volatile solvent system once the volatile solvent system is evaporated. Formulations in which the drug is only partially dissolved in the non-volatile solvent system after the evaporation of the volatile solvent system have the potential to maintain longer duration of sustained delivery, as the undissolved drug can dissolve into the non-volatile solvent system as the dissolved drug is being depleted from the solidified layer during drug delivery. "Adhesive solidifying formulation" or "solidifying formulation" refers to a composition that has a viscosity suitable for application to a skin surface prior to evaporation of its volatile solvent(s), and which can become a solidified layer after evaporation of at least a portion of the volatile solvent(s). The solidified layer, once formed, can be very durable. In one embodiment, once solidified on a skin surface, the formulation can form a peel. The peel can be a soft, coherent solid that can be removed by peeling large pieces from the skin relative to the size of the applied formulation, and often, can be peeled from the skin as a single piece. The application viscosity is typically more viscous than a water-like liquid, but less viscous than a soft solid. Examples of preferred viscosities include materials that have consistencies similar to pastes, gels, ointments, and the like, e.g., viscous liquids that flow but are not subject to spilling. Thus, when a composition is said to have a viscosity "suitable for application" to a skin surface, this means the composition has a viscosity that is high enough so that the composition does not substantially run off the skin after being applied to skin, but also has a low enough viscosity so that it can be easily spread onto the skin. A viscosity range that meets this definition can be from about 100 cP to about 3,000,000 cP (centipoises), and more preferably from about 1 ,000 cP to about 1 ,000,000 cP. In some embodiments of the present invention, it may be desirable to add an additional agent or substance to the formulation so as to provide enhanced or increased adhesive characteristics. The additional adhesive agent or substance can be an additional non-volatile solvent or an additional solidifying agent. Non-limiting examples of substances which might be used as additional adhesion enhancing agents include copolymers of methylvinyl ether and maleic anhydride (Gantrez polymers), polyethylene glycol and polyvinyl pyrrolidone, gelatin, low molecular weight polyisobutylene rubber, copolymer of acrylsan alkyl/octylacrylamido (Dermacryl 79), and/or various aliphatic resins and aromatic resins. . The terms "washable," "washing" or "removed by washing" when used with respect to the adhesive formulations of the present invention refers to the ability of the adhesive formulation to be removed by the application of a washing solvent using a normal or medium amount of washing force. The required force to remove the formulations by washing should not cause significant skin irritation or abrasion. Generally, gentle washing force accompanied by the application of an appropriate washing solvent is sufficient to remove the adhesive formulations disclosed herein. The solvents which can be used for removing by washing the formulations of the present invention are numerous, but preferably are chosen from commonly acceptable solvents including the volatile solvents listed herein. Preferred washing solvents do not significantly irritate human skin and are generally available to the average subject. Examples of washing solvents include but are not limited to water, ethanol, methanol, isopropyl alcohol, acetone, ethyl acetate, propanol, and combinations thereof. In aspect of the invention the washing solvents can be selected from the group consisting of water, ethanol, isopropyl alcohol and combinations thereof. Surfactants can also be used in some embodiments. An acceptable length of time with respect to "drying time" refers to the time it takes for the formulation to form a non-messy solidified surface after application on skin under standard skin and ambient conditions, and with standard testing procedure. It is noted that the word "drying time" in this application does not mean the time it takes to completely evaporate off the volatile solvent(s). Instead, it means the time it takes to form the non-messy solidified surface as described above.
"Standard skin" is defined as dry, healthy human skin with a surface temperature of between about 300C to about 36°C. Standard ambient conditions are defined by the temperature range of from 200C to 25°C and a relative humidity range of from 20% to 80%. The term "standard skin" in no way limits the types of skin or skin conditions on which the formulations of the present invention can be used. The formulations of the present invention can be used to treat all types of "skin," including undamaged (standard skin), diseased skin, or damaged skin. Although skin conditions having different characteristics can be treated using the formulations of the present invention, the use of the term "standard skin" is used merely as a standard to test the compositions of the varying embodiments of the present invention. As a practical matter, formulations that perform well (e.g., solidify, provide therapeutically effective flux, etc.) on standard skin can also perform well diseased or damaged skin.
The "standard testing procedure" or "standard testing condition" is as follows: To standard skin at standard ambient conditions is applied an approximately 0.1 mm layer of the adhesive solidifying formulation and the drying time is measured. The drying time is defined as the time it takes for the formulation to form a non-messy surface such that the formulation does not lose mass by adhesion to a piece of 100% cotton cloth pressed onto the formulation surface with a pressure of between about 5 and about 10 g/cm2 for 5 seconds. "Solidified layer" describes the solidified or dried layer of an adhesive solidifying formulation after at least a portion of the volatile solvent system has evaporated. The solidified layer remains adhered to the skin, and is preferably capable of maintaining good contact with the subject's skin for substantially the entire duration of application under standard skin and ambient conditions. The solidified layer also preferably exhibits sufficient tensile strength so that it can be peeled off the skin at the end of the application in one piece or several large pieces (as opposed to a layer with weak tensile strength that breaks into many small pieces or crumbles when removed from the skin). As used herein, a plurality of drugs, compounds, and/or solvents may be presented in a common list for convenience. However, these lists should be construed as though each member of the list is individually identified as a separate and unique member. Thus, no individual member of such list should be construed as a de facto equivalent of any other member of the same list solely based on their presentation in a common group without indications to the contrary.
Concentrations, amounts, and other numerical data may be expressed or presented herein in a range format. It is to be understood that such a range format is used merely for convenience and brevity and thus should be interpreted flexibly to include not only the numerical values explicitly recited as the limits of the range, but also to include all the individual numerical values or sub-ranges encompassed within that range as if each numerical value and subrange is explicitly recited. As an illustration, a numerical range of "about 0.01 to 2.0 mm" should be interpreted to include not only the explicitly recited values of about 0.01 mm to about 2.0 mm, but also include individual values and subranges within the indicated range. Thus, included in this numerical range are individual values such as 0.5, 0.7, and 1.5, and sub-ranges such as from 0.5 to 1.7, 0.7 to 1.5, and from 1.0 to 1.5, etc. This same principle applies to ranges reciting only one numerical value. Furthermore, such an interpretation should apply regardless of the breadth of the range or the characteristics being described. With these definitions in mind, the present invention is drawn to an adhesive formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and a solidifying agent. The solvent vehicle can comprise a volatile solvent system including at least one volatile solvent and a non-volatile solvent system including at least two non-volatile solvents. The at least two non-volatile solvents of the non-volatile solvent system can facilitate transdermal delivery of the drug at a therapeutically effective rate over a sustained period of time, even after the non-volatile solvent system is substantially evaporated.. The formulation can have viscosity suitable for application to the skin surface prior to evaporation of at least one volatile solvent, and can further be formulated such that when applied to the skin surface, the formulation forms a solidified layer after at least a portion of the volatile solvent system is evaporated. Sustained drug delivery from the solidified layer can also occur.
In an alternative embodiment, a method of dermally delivering a drug can comprise applying an adhesive solidifying formulation to a skin surface of a subject. The formulation can comprise a drug, solvent vehicle, and a solidifying agent. The solvent vehicle can comprise a volatile solvent system including at least one volatile solvent, and a non-volatile solvent system including at least two non-volatile solvents, wherein the non-volatile solvent system facilitates dermal delivery of the drug at a therapeutically effective rate over a sustained period of time. The formulation can have a viscosity suitable for application and adhesion to the skin surface prior to evaporation of the volatile solvent system Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system; and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time.
In another embodiment, a solidified layer for delivering a drug can comprise a drug, a non-volatile solvent system including at least two non-volatile solvents, wherein the non-volatile solvent system is capable of facilitating the delivery of the drug at therapeutically effective rates over a sustained period of time, and a solidifying agent. The solidified layer can be stretchable by 5% in at least one direction without cracking, breaking, or separating from a skin surface to which the layer is applied.
In another embodiment, an adhesive formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and at least two solidifying agents. The solvent vehicle can include a volatile solvent system including at least one volatile solvent, and a non-volatile solvent system including at least one nonvolatile solvent wherein the non-volatile solvent system can be flux-enabling for the drug such that the drug can be delivered in therapeutically effective amounts even after most of the volatile solvent(s) is(are) evaporated. The formulation can have a viscosity suitable for application and adhesion to a skin surface prior to evaporation of the volatile solvent system, and can form a solidified layer after at least partial evaporation of the volatile solvent system after skin application. The drug can continue to be dermally delivered after the volatile solvent system is substantially evaporated. In another embodiment, a method of dermally delivering a drug can comprise applying an adhesive solidifying formulation to a skin surface of a subject. The formulation can include a drug, a solvent vehicle, and at least two solidifying agents. The solvent vehicle can comprise a volatile solvent system including at least one volatile solvent, and a non-volatile solvent system including at least one non-volatile solvent. The formulation can have a viscosity suitable for application and adhesion to the skin surface prior to evaporation of the volatile solvent system. Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system; and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time.
In another embodiment, a solidified layer for delivering a drug can comprise a drug, a non-volatile solvent system comprising at least one nonvolatile solvent, and at least two polymeric solidifying agents. In yet another embodiment, a formulation for dermal delivery of a drug can comprise a drug, a solvent vehicle, and a solidifying agent. The solvent vehicle can comprise a volatile solvent system including at least two volatile solvents, and a non-volatile solvent system including at least one non-volatile solvent. The formulation has a viscosity suitable for application and adhesion to a skin surface prior to evaporation of the volatile solvent system wherein the non-volatile solvent system can be flux-enabling for the drug such that the drug can be delivered at a therapeutically effective amount even after most of the volatile solvent(s) is(are) evaporated. The formulation applied to the skin surface can form a solidified layer after at least partial evaporation of the volatile solvent system and can further be formulated such that when applied to the skin surface, the formulation forms a solidified layer after at least a portion of the volatile solvents is (are) evaporated, but yet continues to deliver drug after substantially solidifying. Additionally, the drug can continue to be delivered after the volatile solvent system is at least substantially evaporated.
In another embodiment, a method of dermally delivering a drug can comprise applying an adhesive solidifying formulation to a skin surface of a subject. The adhesive formulation can comprise a drug, a solvent vehicle, and a solidifying agent. The solvent vehicle can comprise a volatile solvent system including at least two volatile solvent, and a non-volatile solvent system including at least one non-volatile solvent. The formulation can have a viscosity suitable for application and adhesion to the skin surface prior to evaporation of the volatile solvent system. Other steps include solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system; and dermally delivering the drug from the solidified layer to the skin surface at therapeutically effective rates over a sustained period of time. In further detail, the formulations can also contain substances that are solid or liquid at room temperatures, such as pH or ion-pairing agents. After evaporation of the volatile solvent system, most of the non-volatile solvent system should remain in the solidified layer for a period of time sufficient to adequately dermally deliver a given drug to, into, or through the skin of a subject at a sufficient flux for a period of time to provide a therapeutic effect. The nonvolatile solvent system can also serve as a plasticizer of the solidified layer, so that the solidified layer is elastic and flexible. Thus, these embodiments exemplify the present invention which is related to novel formulations, methods, and solidified layers that are typically in the initial form of semi-solids (including creams, gels, pastes, ointments, and other viscous liquids), which can be easily applied onto the skin as a layer, and can quickly (from 15 seconds to about 4 minutes under standard skin and ambient conditions) to moderately quickly (from about 4 to about 15 minutes under standard skin and ambient conditions) change into a solidified layer, e.g., a coherent and soft solid layer which can be peelable, for drug delivery. A solidified layer thus formed is capable of delivering drug to the skin, into the skin, across the skin, etc., at substantially constant rates, over an sustained period of time, e.g., hours to tens of hours, so that most of the active drug is delivered after the solidified layer is formed.
Although a solid layer-forming formulation for dermal drug delivery can use a single solidifying agent, the use of two or more solidifying agents in the formulation herein can provide important advantages. This is because in addition to solidifying the formulations, the solidifying agent(s) in the formulation often impacts component compatibility as well as flexibility and skin adhesiveness of the solidified layer. Sometimes it takes two or more solidified agents to address all these needs. The present invention is related to solidifying formulations that use two or more solidified agents to produce better formulation properties than any single solidifying agent alone within a given formulation could accomplish.
Additionally, the solidified layer typically adheres to the skin, but has a solidified, minimally-adhering, outer surface which is formed relatively soon after application and which does not substantially transfer to or otherwise soil clothing or other objects that a subject is wearing or that the solidified layer may inadvertently contact. The solidified layer can also be formulated such that it is highly flexible and stretchable, and thus capable of maintaining good contact with a skin surface, even if the skin is stretched during body movement, such as at a knee, finger, elbow, or other joints.
In selecting the various components that can be used, e.g., drug, solvent vehicle of volatile solvent system and non-volatile solvent system, solidifying agent(s), etc., various considerations can occur. For example, the volatile solvent system can be selected from pharmaceutically or cosmetically acceptable solvents known in the art. In one embodiment of the present invention, the volatile solvent system can include ethanol, isopropyl alcohol, water, dimethyl ether, diethyl ether, butane, propane, isobutene, 1,1 , difluoroethane, 1,1,1,2 tetrafluorethane, 1,1,1,2,3,3,3-heptafluoropropane, 1 ,1 ,1 ,3,3,3 hexafluoropropane, ethyl acetate, acetone or combinations thereof. In another embodiment of the present invention, the volatile solvent system can include iso-amyl acetate, denatured alcohol, methanol, propanol, isobutene, pentane, hexane, chlorobutanol, turpentine, cytopentasiloxane, cyclomethicone, methyl ethyl ketone, or combinations thereof. The volatile solvent system can include a mixture or combination of any of the volatile solvents set forth in the embodiments above.
In one embodiment, of the present invention the volatile solvent system comprises at least one volatile solvent with a boiling point higher than 20 0C (a liquid volatile solvent) and at least one volatile solvent with a boiling point lower than about 20 0C (gaseous volatile solvents). Boiling points refer to boiling points measured at normal atmospheric pressure. Formulations of the present invention which have both liquid and gas volatile solvents can have significantly shorter drying times than those with only liquid volatile solvents. When a gas volatile solvent is included in the volatile solvent system, it is often the case that concentration of the gas volatile solvent is below the formulations solubility. This allows the formulation to be stored in containers for conventional, un- pressurized semi-solid products. Alternatively, these solvents can be used as propellants for spray-on formulations. Examples of gas volatile solvents which may be used in the present invention include but are not limited to ether, dimethyl ether, diethyl ether, propane, isobutene, diflouroethane, butane, 1,1 ,1 ,2 tetraflourethane, 1 ,1,1 ,2,3,3,3-heptaflouropropane, and 1,1,1,3,3,3, hexaflouropropane, and combinations thereof. Additionally, these volatile solvents should be chosen to be compatible with the rest of the formulation. It is desirable to use an appropriate weight percentage of the volatile solvent(s) in the formulation. Too much of the volatile solvent system prolongs the drying time. Too little of the volatile solvent system can make it difficult to spread the formulation on the skin. For most formulations, the weight percentage of the volatile solvent(s) can be from about 10 wt% to about 85 wt%, and more preferably from about 20 wt% to about 50 wt%. In one aspect of the invention, the volatile solvent system comprises at least 10 wt% of the formulation. In another embodiment, the volatile solvent system comprises at least about 20 wt% of the formulation.
The volatile solvent system can also be chosen to be compatible with the non-volatile solvent system, solidifying agent, drug, and any other excipients that may be present. For example, polyvinyl alcohol (PVA) is not soluble in ethanol. Therefore, a volatile solvent which will dissolve PVA needs to be formulated in the solidified layer. For instance, water will dissolve PVA and can be utilized as a volatile solvent in a formulation; however, the drying time in such a formulation may be too long to certain applications. Therefore, a second volatile solvent (e.g., ethanol) can be formulated into the formulation to reduce the water content but maintain a sufficient amount of water to keep PVA in solution and thereby reduce the drying time for the formulation.
The volatile solvent system can be chosen to reduce drying time for the formulation. Returning to the PVA example above, the use of water to dissolve the PVA may result in the drying time in such a formulation may be too long to certain applications. Therefore, a second volatile solvent (e.g., ethanol) can be formulated into the formulation to reduce the water content but maintain a sufficient amount of water to keep PVA in solution and thereby reduce the drying time for the formulation. The volatile solvent can be chosen to improve solubility of a particular drug form utilized in the formulation. For example, ropivacaine HCI is not soluble in non-volatile solvents isostearic acid, triacetin, and Span 20. Therefore, addition of water to the formulation will aid in dissolving the ropivacaine HCl and with addition of a small amount of base to dissolve the remaining drug crystals. Complete dissolution of ropivacaine in the formulation is advantageous to having to avoid suspending the undissolved drug particles in a formulation with a relatively low viscosity that may result in drug settling. For a selected drug or a selected solidifying agent, some volatile solvents may be better solvents or more compatible than other volatile solvents. However, some times, the most suitable volatile solvent for a drug is not compatible with a solidifying agent, and vice versa. In some other situations, the most suitable volatile solvent for a drug and a solidifying agent evaporates to slowly resulting in a drying time that is unacceptable for the application. In the above situations, satisfactory compromises may be reached by using a specially formulated volatile solvent systems that contains two or more volatile solvents according to certain ratios (which are often experimentally determined). For example, one solvent can provide acceptable evaporation time, and another volatile solvent provides improved formulation compatibility.
In one embodiment of the present invention, one of the volatile solvents of the volatile solvent system can be less volatile than the other. The less volatile solvent can have better compatibility with the solidifying agent as compared to a more volatile solvent in the solvent system.
In another aspect of the present invention, it can be beneficial to retain or delay the volatilization of the volatile solvent system so that the solidifying formulation can maintain its desirable wear, and drug delivery properties. Such retention can be accomplished by including a volatile solvent retaining substance in the formulation. Volatile solvent retaining substances can include water, hygroscopic substances, honey, glycerol, propylene glycol, and the like. The non-volatile solvent system can also be chosen or formulated to be compatible with the solidifying agent, the drug, the volatile solvent, and any other ingredients that may be present. For example, the solidifying agent can be chosen so that it is dispersible or soluble in the non-volatile solvent system. Most non-volatile solvent systems and solvent vehicles as a whole will be formulated appropriately after experimentation. For instance, certain drugs have good solubility in poly ethylene glycol (PEG) having a molecular weight of 400 (PEG 400, non-volatile solvent) but poor solubility in glycerol (non-volatile solvent) and water (volatile solvent). However, PEG 400 cannot effectively dissolve poly vinyl alcohol (PVA), and thus, is not very compatible alone with PVA, a solidifying agent. In order to dissolve sufficient amount of an active drug and use PVA as a solidifying agent at the same time, a non-solvent system including PEG 400 and glycerol (compatible with PVA) in an appropriate ratio can be formulated, achieving a compatibility compromise. As a further example of compatibility, non-volatile solvent/solidifying agent incompatibility is observed when Span 20 is formulated into a formulation containing PVA. With this combination, Span 20 can separate out of the formulation and form an oily layer on the surface of the solidified layer. Thus, appropriate solidifying agent/nonvolatile solvent selections are desirable in developing a viable formulation and compatible combinations. It is not necessary that both the non-volatile solvents of the non-volatile solvent system be compatible with the solidifying agent. In some embodiments one of the non-volatile solvents of the non-volatile solvent system can be present to provide compatibility with the solidifying agent while a second non-volatile solvent can act as the flux enabling non-volatile solvent.
In further detail, the at least two non-volatile solvents that can be used to form non-volatile solvent systems can be selected from a variety of pharmaceutically acceptable liquids. In one embodiment of the present invention, the non-volatile solvent system can include glycerol, propylene glycol, isostearic acid, oleic acid, propylene glycol, trolamine, tromethamine, triacetin, sorbitan monolaurate, sorbitan monooleate, sorbitan monopalmitate, butanol, or combinations thereof. In another embodiment the non-volatile solvent system can include benzoic acid, butyl alcohol, dibutyl sebecate, diglycerides, dipropylene glycol, eugenol, fatty acids such as coconut oil, fish oil, palm oil, grape seed oil, isopropyl myristate, mineral oil, oleyl alcohol, vitamin E, triglycerides, sorbitan fatty acid surfactants, triethyl citrate, or combinations thereof. In a further embodiment the non-volatile solvent system can include 1 ,2,6-hexanetriol, alkyltriols, alkyldiols, acetyl monoglycerides, tocopherol, alkyl dioxolanes, p-propenylanisole, anise oil, apricot oil, dimethyl isosorbide, alkyl glucoside, benzyl alcohol, bees wax, benzyl benzoate, butylene glycol, caprylic/capric triglyceride, caramel, cassia oil, castor oil, cinnamaldehyde, cinnamon oil, clove oil, coconut oil, cocoa butter, cocoglycerides, coriander oil, corn oil, coriander oil, corn syrup, cottonseed oil, cresol, cyclomethicone, diacetin, diacetylated monoglycerides, diethanolamiπe, dietthylene glycol monoethyl ether, diglycerides, ethylene glycol, eucalyptus oil, fat, fatty alcohols, flavors, liquid sugars ginger extract, glycerin, high fructose corn syrup, hydrogenated castor oil, IP palmitate, lemon oil, lime oil, limonene, milk, monoacetin, monoglycerides, nutmeg oil, octyldodecanol, olive alcohol, orange oil, palm oil, peanut oil, PEG vegetable oil, peppermint oil, petrolatum, phenol, pine needle oil, polypropylene glycol, sesame oil, spearmint oil, soybean oil, vegetable oil, vegetable shortening, vinyl acetate, wax, 2-(2- (octadecyloxy)ethoxy)ethanol, benzyl benzoate, butylated hydroxyanisole, candelilla wax, carnauba wax, ceteareth-20, cetyl alcohol, polyglyceryl," dipolyhydroxy stearate, PEG-7 hydrogenated castor oil, diethyl phthalate, diethyl sebacate, dimethicone, dimethyl phthalate, PEG Fatty acid esters such as PEG- stearate, PEG - oleate, PEG- laurate, PEG fatty acid diesters such as PEG- dioleate, PEG- distearate, PEG-castor oil, glyceryl behenate, PEG glycerol fatty acid esters such as PEG glyceryl laurate, PEG glyceryl stearate, PEG glyceryl oleate, hexylene glycerol, lanolin, lauric diethanolamide, lauryl lactate, lauryl sulfate, medronic acid, methacrylic acid, multisterol extract, myristyl alcohol, neutral oil, PEG-octyl phenyl ether, PEG -alkyl ethers such as PEG-cetyl ether, PEG-stearyl ether, PEG- sorbitan fatty acid esters such as PEG-sorbitan diisosterate, PEG-sorbitan monostearate, propylene glycol fatty acid esters such as propylene glycol stearate, propylene glycol, caprylate/caprate, sodium pyrrolidone carboxylate, sorbitol, squalene, stear-o-wet, triglycerides, alkyl aryl polyether alcohols, polyoxyethylene derivatives of sorbitan-ethers, saturated polyglycolyzed C8-C10 glycerides, N-methyl pyrrolidone, honey, polyoxyethylated glycerides, dimethyl sulfoxide, azone and related compounds, dimethylformamide, N-methyl formamaide, fatty acid esters, fatty alcohol ethers, alkyl-amides (N.N-dimethylalkylamides), N-methyl pyrrolidone related compounds, ethyl oleate, polyglycerized fatty acids, glycerol monooleate, glyceryl monomyristate, glycerol esters of fatty acids, silk amino acids, PPG-3 benzyl ether myristate, Di-PPG2 myreth 10-adipate, honeyquat, sodium pyroglutamic acid, abyssinica oil, dimethicone, macadamia nut oil, limnanthes. alba seed oil, cetearyl alcohol, PEG-50 shea butter, shea butter, aloe vera juice, phenyl trimethicone, hydrolyzed wheat protein, or combinations thereof. In yet a further embodiment, the non-volatile solvent system can include a combination or mixture of non-volatile solvents set forth in any of the above discussed embodiments.
In addition to these and other considerations, the non-volatile solvent system, or at least one of the non-volatile solvents in the non-volatile solvent system can also serve as plasticizer in the adhesive formulation so that when the solidified layer is formed, the layer is flexible, stretchable, and/or otherwise "skin friendly."
Certain volatile and/or nonvolatile solvent(s) that are irritating to the skin may be desirable to use to achieve the desired solubility and/or permeability of the drug. It is also desirable to add compounds that are both capable of preventing or reducing skin irritation and are compatible with the formulation. For example, in a formulation where the volatile solvent is capable of irritating the skin, it would be helpful to use a non-volatile solvent that is capable of reducing skin irritation. Examples of solvents that are known to be capable of preventing or reducing skin irritation include, but are not limited to, glycerin, honey, and propylene glycol.
The feature of two non-volatile solvents in the non-volatile solvent system enhances the ability of the non-volatile solvent to provide therapeutically effective flux, while at the same time providing additional important characteristics which make the solidified formulations superior. As discussed in other areas of the application, non-volatile solvents can provide advantageous benefits such as acting as a plasticizer, improve adhesion, reducing skin irritation, inhibiting phase separation, and the like. In some embodiments it may be desirable to deliver two drugs which do not share a common flux-enabling non-volatile solvent. In such instances at least on of the at least two non-volatile solvents present in the non-volatile solvent system can act to promote the flux of one of the drugs while the other non-volatile solvent promotes the flux of the other drug. In such situations it may be desirable or necessary to include an additional non-volatile solvent which provides some of the other advantageous benefits discussed above. The two or more non-volatile solvents of the non-volatile solvent system of the present invention may be such that the non-volatile solvents used independently are not flux-enabling non-volatile solvents for a drug but when formulated together become a flux-enabling non-volatile solvent. One possible reason for these initially non enabling non-volatile solvents to become enabling non-volatile solvents when formulated together may be due to the optimization of the ionization state of the drug to a physical form which has higher flux or the non-volatile solvents act in some other synergistic manner. One further benefit of the mixing of the non-volatile solvents is that it may optimize the pH of the formulation or the skin tissues under the formulation layer to minimize irritation. Examples of suitable combinations of non-volatile solvents that result in an adequate non-volatile solvent system include but are not limited to isostearic acid /trolamine, isostearic acid /diisopropyl amine, oleic acid/trolamine, and propylene glycol /isostearic acid. The selection of the solidifying agent can also be carried out in consideration of the other components present in the adhesive formulation. The solidifying agent can be selected or formulated to be compatible to the drug and the solvent vehicle (including the volatile solvent(s) and the non-volatile solvent system), as well as to provide desired physical properties to the solidified layer once it is formed. Depending on the drug, solvent vehicle, and/or other components that may be present, the solidifying agent can be selected from a variety of agents. In one embodiment, the solidifying agent can include polyvinyl alcohol with a MW range of 20,000-70,000 (Amresco), esters of polyvinylmethylether/maleic anhydride copolymer (ISP Gantrez ES-425 and Gantrez ES-225) with a MW range of 80,000-160,000, neutral copolymer of butyl methacrylate and methyl methacrylate (Degussa Plastoid B) with a MW range of 120,000-180,000, dimethylaminoethyl methacrylate-butyl methacrylate- methyl methacrylate copolymer (Degussa Eudragit E100) with a MW range of 100,000-200,000, ethyl acrylate-methyl methacrylate-trimethylammonioethyl methacrylate chloride copolymer with a MW greater than 5,000 or similar MW to Eudragit RLPO (Degussa), Zein (prolamine) with a MW greater than 5,000 such as Zein with a MW around 35,000 (Freeman industries), pregelatinized starch having a MW similar to Instant Pure-Cote B793 (Grain Processing Corporation), ethyl cellulose MW greater than 5,000 or MW similar to Aqualon EC N7, N 10, N14, N22, N50 , or N100 (Hercules), fish gelatin having a MW 20,000-250,000 (Norland Products), gelatin, other animal sources with MW greater than 5,000, acrylates/octylacrylamide copolymer MW greater than 5,000 or MW similar to National Starch, Chemical Dermacryl 79, or combinations thereof.
In another embodiment, the solidifying agent can include ethyl cellulose, hydroxy ethyl cellulose, hydroxy methyl cellulose, hydroxy propyl cellulose, hydroxypropyl methyl cellulose, carboxymethyl cellulose, methyl cellulose, polyether amides, corn starch, pregelatinized corn starch, polyether amides, shellac, polyvinyl pyrrolidone, polyisobutylene rubber, polyvinyl acetate phthalate, or combinations thereof. In a further embodiment, the solidifying agent can include ammonia methacrylate, carrageenan, cellulose acetate phthalate aqueous such as CAPNF from Eastman, carboxy polymethylene, cellulose acetate (microcrystalline), cellulose polymers, divinyl benzene styrene, ethylene vinyl acetate, silicone, guar gum, guar rosin, gluten, casein, calcium caseinate, ammonium caseinate, sodium caseinate, potassium caseiπate, methyl acrylate, microcrystalline wax, polyvinyl acetate, PVP ethyl cellulose, acrylate, PEG/PVP, xantham gum, trimethyl siloxysilicate, maleic acid/anhydride colymers, polacrilin, poloxamer, polyethylene oxide, poly glactic acid/poly-l-lactic acid, turpene resin, locust bean gum, acrylic copolymers, polyurethane dispersions, dextrin, polyvinyl alcohol-polyethylene glycol co-polymers, methacrylic acid-ethyl acrylate copolymers such as BASF's Kollicoat polymers, methacrylic acid and methacrylate based polymers such as poly(methacrylic acid), or combinations thereof. In another embodiment, the solidifying agent can include a combination of solidifying agents set forth in the any of the above discussed embodiments. Other polymers may also be suitable as the solidifying agent, depending on the solvent vehicle components, the drug, and the specific functional requirements of the given formulation. Other polymers may also be suitable as the solidifying agent, depending on the solvent vehicle components, the drug, and the specific functional requirements of the given formulation. In one embodiment, the non-volatile solvent system and the solidifying agent(s) should be compatible with each other. Compatibility can be defined as i) the solidifying agent does not substantially negatively influence the function of the non-volatile solvent system, except for some reduction of flux; ii) the solidifying agent can hold the non-volatile solvent system in the solidified layer so that substantially no non-volatile solvent oozes out of the layer, and/or iii) the solidified layer formed with the selected non-volatile solvent system and the solidifying agent has acceptable flexibility, rigidity, tensile strength, elasticity, and adhesiveness. The weight ratio of the non-volatile solvent system to the solidifying agent(s) can be from about 0.1 :1 to about 10:1. In another aspect, the ratio between the non-volatile solvent system and the solidifying agent can be from about 0.5:1 to about 2:1.
The use of at least two solidifying agents can provide superior peel characteristics. Desirable characteristics can include enhanced elasticity, enhanced skin adhesion, enhanced tensile strength, and the like. In some embodiments, the combination of the at least two solidifying agents can provide a more homogenous formulation with minimal if any phase separation. For example, in one embodiment, polyvinyl alcohol (PVA) can be used as one of the solidifying agents in combination with Gantrez. In that combination, the PVA functions to provide enhanced elasticity while the Gantrez provides enhanced skin adhesion. In another embodiment, a formulation can be made which utilizes Eudgragit E-100 in combination with PVA as the solidifying agent. The formulation has quicker solidifying characteristics and results in a solidified layer with enhanced tensile strength. The thickness of the formulation layer applied on the skin should also be appropriate for a given formulation and desired drug delivery considerations. If the layer is too thin, the amount of the drug may not be sufficient to support sustained delivery over the desired length of time. If the layer is too thick, it may take too long to form a non-messy outer surface of the solidified layer. If the drug is very potent and the solidified layer has very high tensile strength, a layer as thin as 0.01 mm may be sufficient. If the drug has rather low potency and the solidified layer has low tensile strength, a layer as thick as 2-3 mm may be desirable. Thus, for most drugs and formulations, the appropriate thickness can be from about 0.01 mm to about 3 mm, but more typically, from about 0.05 mm to about 1 mm.
The flexibility and stretchability of a solidified layer can be desirable in some applications. In one aspect of the invention, the solidified layer is coherent, flexible, and continuous. Such flexible and coherent nature can greatly enhance the ease of use of the formulation. For instance, certain nonsteroidal anti-inflammatory agents (NSAIDs) can be applied directly over joints and muscles for transdermal delivery into joints and muscles. However, skin areas over joints and certain muscle groups are often significantly stretched during body movements. Such movement prevents non-stretchable patches from maintaining good skin contact. Lotions, ointments, creams, gels, foams, pastes, or the like also may not be suitable for use for the reasons cited above. As such, in transdermal delivery of NSAIDs into joints and/or muscles, the solidifying formulations of the present invention can offer unique advantages and benefits. It should be pointed out that although good stretchability can be desirable in some applications. The solidifying formulations of the present invention do not always need to be stretchable, as certain applications of the present invention do not necessarily benefit from this property. For instance, if the formulation is applied on a small facial area overnight for treating acne, a subject would experience minimal discomfort and formulation-skin separation even if the solidified layer is not stretchable, as facial skin usually is not stretched very much during a sleep cycle.
A further feature of a formulation prepared in accordance with embodiments of the present invention is related to drying time. If a formulation dries too quickly, the user may not have sufficient time to spread the formulation into a thin layer on the skin surface before the formulation is solidified, leading to poor skin contact. If the formulation dries too slowly, the subject may have to wait a long time before resuming normal activities (e.g. putting clothing on) that may remove un-solidified formulation. Thus, it is desirable for the drying time to be longer than about 15 seconds but shorter than about 15 minutes, and preferably from about 0.5 minutes to about 5 minutes. Other benefits of the solidified layers of the present invention include the presence of a physical barrier that can be formed by the material itself. For instance, local anesthetic agents and other agents such as clonidine may be delivered topically for treating pain related to neuropathy, such as diabetic neuropathic pain. Since many of such subjects feel tremendous pain, even when their skin area is only gently touched, the physical barrier of the solidified layer can prevent or minimize pain caused by accidental contact with objects or others.
These and other advantage can be summarized in the following non- limiting list of benefits, as follows. The solidified layers of the present invention can be prepared in an initial form that is easy to apply as a semisolid dosage form. Additionally, upon volatile solvent system evaporation, the resulting solidified layer is relatively thick and can contain much more active drug than a typical layer of traditional cream, gel, lotion, ointment, paste, etc., and further, is not as subject to unintentional removal. Further, as the solidified layer remains adhesive and optionally peelable, easy removal of the solidified layer can occur, usually without the aid of a solvent or surfactant. In some embodiments, the adhesion to skin and elasticity of the material is such that the solidified layer will not separate from the skin upon skin stretching at highly stretchable skin areas, such as over joints and muscles. For example, in one embodiment, the solidified layer can be stretched by 5%, or even 10% or greater, in at least one direction without cracking, breaking, and/or separating form a skin surface to which the solidified layer is applied. Still further, the solidified layer can be formulated to advantageously deliver drug and protect sensitive skin areas without cracking or breaking. Generally, the solidified layers made using the formulations of the present invention can be soft and coherent solids that are peelable from a skin surface as a single piece or as only a few large pieces relative to the application size. In other embodiments, the solidified layer can be removable by use of a solvent, such as water, alcohol, surfactant, or mixture thereof.
As a further note, it is a unique feature of the solidified layers of the present invention that they can keep a substantial amount of the non-volatile solvent system, which is optimized for delivering the drug, on the skin surface. This feature can provide unique advantages over existing products. For example, in some semi-solid formulations, upon application to a skin surface the volatile solvents quickly evaporate and the formulation layer solidifies into a hard lacquer-like layer. The drug molecules are immobilized in the hard lacquer layer and are substantially unavailable for delivery into the skin surface. As a result, it is believed that the delivery of the drug is not sustained over a long period of time. In contrast to this type of formulation, the solidified layers formed using the formulations of the present invention keep the drug molecules quite mobile in the non-volatile solvent system which is in contact with the skin surface, thus ensuring sustained delivery.
Specific examples of applications that can benefit from the systems, formulations, and methods of the present invention are as follows. In one embodiment, a solidified layer including bupivacaine, lidocaine, or ropivacaine, can be formulated for treating diabetic and post herpetic neuralgia.
Alternatively, dibucanine and an alpha-2 agonist such as clonidine can be formulated in a solidified layer for treating the same disease. In another embodiment, retinoic acid and benzoyl peroxide can be combined in a solidified layer for treating acne, or alternatively, 1 wt% clindamycin and 5 wt% benzoyl peroxide can be combined in a solidified layer for treating acne. In another embodiment, a retinol solidifying formulation (OTC) can be prepared for treating wrinkles, or a lidocaine solidifying formulation can be prepared for treating back pain. In another embodiment, a zinc oxide solidifying formulation (OTC) can be prepared for treating diaper rash, or an antihistamine solidified layer can be prepared for treating allergic rashes such as poison ivy.
Additional applications include delivering drugs for treating certain skin conditions, e.g., dermatitis, psoriasis, eczema, skin cancer, viral infections such as cold sore, genital herpes, shingles, etc., particularly those that occur over joints or muscles where a transdermal patch may not be practical. For example, solidifying formulations containing imiquimod can be formulated for treating skin cancer, common and genital warts, and actinic keratosis. Solidifying formulations containing antiviral drugs such as acyclovir, penciclovir, famciclovir, vaiacyclovir, steroids, behenyl alcohol can be formulated for treating herpes viral infections such as cold sores on the face and genital areas. Solidifying formulations containing non-steroidal anti-inflammatory drugs (NSAIDs), capsaicin, alpha-2 agonists, and/or nerve growth factors can be formulated for treating soft tissue injury and muscle-skeletal pains such as joint and back pain of various causes. As discussed above, patches over these skin areas typically do not have good contact over sustained period of time, especially for a physically active subject, and may cause discomfort. Likewise, traditional semisolid formulations such as creams, lotions, ointments, etc., may prematurely stop the delivery of a drug due to the evaporation of solvent and/or unintentional removal of the formulation. The solidified adhesive formulations of the present invention address the shortcomings of both of these types of delivery systems.
A further embodiment involves a formulation containing at least one alpha-2 agonist drug, at least one tricyclic antidepressant agent, and/or at least one local anesthetic drug which is applied topically to treat neuropathic pain.
The drugs are gradually released from the formulation to provide pain relief over a sustained period of time. The formulation can become a coherent, soft solid after 2-5 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
Another embodiment involves a formulation containing capsaicin which is applied topically to treat neuropathic pain. The capsaicin is gradually released from the formulation for treating this pain over a sustained period of time. The formulation can become a coherent, soft solid after 2-5 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
Another embodiment involves solidifying formulations containing tazorac for treating stretch marks, wrinkles, sebaceous hyperplasia, seborrheic keratosis. In another embodiment, solidifying formulations containing glycerol can be made so as to provide a protective barrier for fissuring on finger tips. Still another embodiment can include a formulation containing a drug selected from the local anesthetic class such lidocaine and ropivacaine or the like, or NSAID class, such as ketoprofen, piroxicam, diclofenac, indomethacin, or the like, which is applied topically to treat symptoms of back pain, muscle tension, or myofascial pain or a combination thereof. The local anesthetic and/or NSAID is gradually released from the formulation to provide pain relief over a sustained period of time. The formulation can become a coherent, soft solid after about 2-5 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
A similar embodiment can include a formulation containing drugs capsaicin and a local anesthetic drug which is applied topically to the skin to provide pain relief. Another embodiment can include a formulation containing the combination of a local anesthetic and a NSAID. In both of the above embodiments the drugs are gradually released from the formulation to provide pain relief over a sustained period of time. The formulation can become a coherent, soft solid after 2-4 minutes and remains adhered to the skin surface for the length of its application. It is easily removed any time after drying without leaving residual formulation on the skin surface.
In another embodiment, solidifying formulations for the delivery of drugs that treat the causes or symptoms of diseases involving joints and muscles can also benefit from the systems, formulations, and methods of the present invention. Such diseases that may be applicable include, but not limited to, osteoarthritis (OA), rheumatoid arthritis (RA), joint and skeletal pain of various other causes, myofascial pain, muscular pain, and sports injuries. Drugs or drug classes that can be used for such applications include, but are not limited to, non-steroidal anti-inflammatory drugs (NSAIDs) such as ketoprofen and diclofanec, COX-2 selective NSAIDs and agents. COX-3 selective NSAIDs and agents, local anesthetics such as lidocaine, bupivacaine, ropivacaine, and tetracaine, steroids such as dexamethasone.
Delivering drugs for the treatment of acne and other skin conditions can also benefit from principles of the present invention, especially when delivering drugs having low skin permeability. Currently, topical retinoids, peroxides, and antibiotics for treating acne are mostly applied as traditional semisolid gels or creams. However, due to the shortcomings as described above, sustained delivery over many hours is unlikely. For example, clindamycin, benzoyl peroxide, and erythromycin may be efficacious only if sufficient quantities are delivered into hair follicles. However, a traditional semisolid formulation, such as the popular acne medicine benzaclin gel, typically loses most of its solvent (water in the case of benzaclin) within a few minutes after the application. This short period of a few minutes likely substantially compromises the sustained delivery of the drug. The formulations of the present invention typically do not have this limitation. In another embodiment, the delivery of drugs for treating neuropathic pain can also benefit from the methods, systems, and formulations of the present invention. A patch containing a local anesthetic agent, such as Lidoderm™, is widely used for treating neuropathic pain, such as pain caused by post-herpetic neuralgia and diabetes induced neuropathic pain. Due to the limitations of the patch as discussed above, the solidified layers prepared in accordance with the present invention provide some unique benefits, as well as provide a potentially less expensive alternative to the use of a patch. Possible drugs delivered for such applications include, but are not limited to, local anesthetics such as lidocaine, prilocaine, tetracaine, bupivicaine, etidocaine; and other drugs including capsaicin and alpha-2 agonists such as clonidine, dissociative anesthetics such as ketamine, tricyclic antidepressants such as amitriptyline,.
As set forth in part above, the solidifying formulations of the present invention can be formulated to treat a variety of conditions and disease such as musculoskeletal pain, neuropathic pain, alopecia, skin disease including dermatitis and psoriasis as well as skin restoration (cosmetic skin treatment), and infections including viral, bacterial, and fungal infection. As such, the formulations can deliver a wide ranging number and types of drugs and active agents. In one embodiment, the solidifying formulation can be formulated to include acyclovir, econazole, miconazole, terbinafine, lidocaine, bupivacaine, ropivacaine, and tetracaine, amitriptyline, ketanserin, betamethasone dipropionate, triamcinolone acetonide, clindamycin, benzoyl peroxide, tretinoin, Isotretinoin, clobetasol propionate, halobetasol propionate, ketoprofen, piroxicam, diclofenac, indomethacin, imiquimod, salicylic acid, benzoic acid, or combinations thereof In another embodiment, the formulation can include an antifungal drug such as amorolfine, butenafine, naftifine, terbinafine, fluconazole, itraconazole, ketoconazole, posacoπazole, ravuconazole, voriconazole, clotrimazole, butoconazole , econazole, miconazole, oxiconazole, sulconazole, terconazole, tioconazole, caspofungin, micafungin, anidulafingin, amphotericin B, AmB, nystatin, pimaricin, griseofulvin, ciclopirox olamine, haloprogin, tolnaftate, and undecylenate, or combinations thereof.
In another embodiment, the formulation can include an antifungal drug such as acyclovir, penciclovir, famciclovir, valacyclovir, behenyl alcohol, trifluridine, idoxuridine, cidofovir, gancyclovir, podofilox, podophyllotoxin.ribavirin, abacavir, delavirdine, didanosine, efavirenz, lamivudine, nevirapine, stavudine, zalcitabine, zidovudine, amprenavir, indinavir, nelfinavir, ritonavir, saquinavir, amantadine, interferon, oseltamivir, ribavirin, rimantadine, zanamivir, or combinations thereof.
When the formulation is intended to provide antibacterial treatment it can be formulated to include an antibacterial drug such as erythromycin, clindamycin, tetracycline, bacitracin, neomycin, mupirociπ, polymyxin B, quinolones such as ciproflaxin, or combinations thereof.
When the formulation is intended to relieve pain, particularly neuropathic pain, the formulation can include a local anesthetic such as lidocaine, bupivacaine, ropivacaine, and tetracaine; an alpha-2 agonists such as clonidine. When the formulation is intended to treat pain associated with inflammation it can be formulated to include an non-steroidal anti-inflammatory drug such as ketoprofen, piroxicam, diclofenac, indomethacin, COX inhibitors general COX inhibitors, COX-2 selective inhibitors, COX-3 selective inhibitors, or combinations thereof
In another embodiment, the formulation can be formulated to treat skin disorders or blemishes by including active agents such as anti-acne drugs such as clindamycin and benzoyl peroxide, retinol, vitamin A derivatives such as tazarotene and isotretinoin, cyclosporin, anthralin, vitamin D3, cholecalciferol, calcitriol, calcipotriol, tacalcitol, calcipotriene, or combinations thereof.
In yet another embodiment, the delivery of medication for treating warts and other skin conditions would also benefit from long periods of sustained drug delivery. Examples of anti-wart compounds include but are not limited to:imiquimod, rosiquimod, keratolytic agents: salicylic acid, alpha hydroxy acids, sulfur, rescorcinol, urea, benzoyl peroxide, allantoin, tretinoin, trichloroacetic acid, lactic acid, benzoic acid, or combinations thereof. A further embodiment involves the use of the solidifying formulations for the delivery of sex steroids including but not limited to progestagens consisting of progesterone, norethindrone, norethindroneacetate, desogestrel, drospirenone, ethynodiol diacetate, norelgestromin, norgestimate, levonorgestrel, dl-norgestrel, cyproterone acetate, dydrogesterone, medroxyprogesterone acetate, chlormadinone acetate, megestrol, promegestone, norethisterone, lynestrenol, gestodene, tibolene, androgens consisting of testosterone, methyl testosterone, oxandrolone, androstenedione, dihydrotestosterone. estrogens consisting of estradiol, ethniyl estradiol, estiol, estrone, conjugated estrogens, esterified estrogens, estropipate, or combinations thereof.
Non-sex steroids can also be delivered using the formulations of the present invention. Examples of such steroids include but are not limited to betamethasone dipropionate, halobetasol propionate, diflorasone diacetate, triamcinolone acetonide, desoxϊmethasone, fluocinonide, halcinonide, mometasone furoate, betamethasone valerate, fluocinonide, fluticasone propionate, triamcinolone acetonide, fluocinolone acetonide, flurandrenolide, desonide, hydrocortisone butyrate, hydrocortisone valerate, alclometasone dipropionate, flumethasone pivolate, hydrocortisone, hydrocortisone acetate, or combinations thereof. A further embodiment involves controlled delivery of nicotine for treating nicotine dependence among smokers and persons addicted to nicotine. Formulations of the present invention would be a cost effective way of delivering therapeutic amounts of nicotine transdermally.
Another embodiment involves using the formulation to deliver antihistamine agents such as diphenhydramine and tripelennamine. These agents would reduce itching by blocking the histamine that causes the itch and also provide relief by providing topical analgesia.
Other drugs which can be delivered using the solidifying formulations of the present invention include but are not limited to tricyclic anti-depressants such as amitriptyline; anticonvulsants such as carbamazepine and alprazolam; N-methyl-D-aspartate (NMDA) antagonists such as ketamine; 5-HT2A receptor antagonists such as ketanserin; and immune modulators such as tacrolimus and picrolimus. Other drugs that can be delivered using the formulations and methods of the current invention include humectants, emollients, and other skin care compounds. EXAMPLES
The following examples illustrate the embodiments of the invention that are presently best known. However, it is to be understood that the following are only exemplary or illustrative of the application of the principles of the present invention. Numerous modifications and alternative compositions, methods, and systems may be devised by those skilled in the art without departing from the spirit and scope of the present invention. The appended claims are intended to cover such modifications and arrangements. Thus, while the present invention has been described above with particularity, the following examples provide further detail in connection with what are presently deemed to be the most practical and preferred embodiments of the invention.
Example 1
Hairless mouse skin (HMS) or human epidermal membrane (HEM) is used as the model membrane for the in vitro flux studies described in herein. Freshly separated epidermis removed from the abdomen of a hairless mouse is mounted carefully between the donor and receiver chambers of a Franz diffusion cell. The receiver chamber is filled with pH 7.4 phosphate buffered saline (PBS). The experiment is initiated by placing test formulations on the stratum corneum (SC) of the skin sample. Franz cells are placed in a heating block maintained at 370C and the HMS temperature is maintained at 35 °C. At predetermined time intervals, 800 μl_ aliquots are withdrawn and replaced with fresh PBS solution. Skin flux (μg/cm2/h) is determined from the steady-state slope of a plot of the cumulative amount of permeation versus time. It is to be noted that human cadaver skin can be used as the model membrane for the in vitro flux studies as well. The mounting of the skin and the sampling techniques used as the same as described above for the HMS studies.
Example 2
Human cadaver skin is used as a membrane to select a non-volatile solvent for clobetasol propionate. In vitro methodology is described in Example 1. About 200mcL of 0.1% (w/w) solution of clobetasol in various non-volatile solvents is added to the donor compartment of Franz cells. Results obtained after LC analysis are shown in Table 4.
Table 4 - Non volatile solvents for clobetasol propionate
Figure imgf000042_0001
* Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 6-28 hours. If the experiment was continued it is anticipated the steady state would continue.
All the neat non-volatile solutions studied have an average flux of less than 40 ng/cm2/hr over the 30 hour time period. Propylene glycol and glycerol have the lowest permeation for clobetasol propionate. A mixture of propylene glycol and isostearic acid at a weight ratio of 9:1 have significantly higher flux than either of the solvents alone or with the other solvents tested. The average flux is 20 times higher than that with light mineral oil which is the best non-mixed solvent. Hence, for clobetasol propionate, propylene glycol/isostearic acid combination is a good candidate for a non-volatile solvent system.
Examples 3-8
Adhesive formulations containing 0.05% (w/w) clobetasol propionate with propylene glycol and isostearic acid as non volatile solutions and various solidifying agents are prepared. The formulations are prepared from the ingredients as shown in Table 5.
Figure imgf000043_0001
Each of the compositions shown above are studied for flux of clobetasol propionate as shown in Table 6 as follows:
Table 6 - Steady state flux of Clobetasol propionate through human cadaver skin at 35 0C
Figure imgf000043_0002
* Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 6-28 hours. If the experiment was continued it is anticipated the steady state would continue.
As seen from Table 6 formulation described in Example 3 that contains polyvinyl alcohol as solidifying agent has high flux of clobetasol propionate. Polyvinyl alcohol is known to form stretchable films and it is likely that this formulation will have acceptable wear properties. The toughness of the resulting film can be modified by adding appropriate plasticizers if needed. Tackiness can also be modified by adding appropriate amounts of tackifier or by adding appropriate amounts of another solidifying agent such as Dermacryl 79. Regarding formulation described in Example 8, a higher percentage of ethanol is needed to dissolve the polymer. However, the solidifying agent used in Example 8 provides the highest flux of clobetasol propionate among the solidifying agents studied. The wear properties of this formulation can be modified by adding appropriate levels of other ingredients including but not limited to plasticizers, tackifiers, non-volatile solvents and or solidifying agents.
Example 9
Formulations of acyclovir in various non-volatile solvent systems are evaluated. Excess acyclovir is present. The permeation of acyclovir from the test formulations through HMS is presented in Table 7 below.
Table 7
Figure imgf000044_0001
* Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed, the steady-state delivery would likely continue well beyond 8 hours.
Steady state flux of acyclovir from the above non-volatile solvents are obtained by placing 200 mcL on the stratum corneum side (donor) of hairless mouse skin. The in vitro studies are carried out as described in Example 1. The surprising result showed the polyethylene glycol 400, span 80, ethyl oleate, or ethyl oleate plus trolamine are not flux-enabling solvents for acyclovir (e.g., steady state flux values significantly less than the steady state flux of acyclovir in the marketed product noted in Table 2, where the flux was about 3mcg/cm2/h). However, the combination of isostearic acid and trolamine or oleic acid and increasing amounts of trolamine are flux-enabling solvents for acyclovir. As can be seen, the highest flux was achieved using 30% trolamine with oleic acid as the non-volatile solvent system.
Examples 10-13
Prototype solidifying formulations are prepared as follows. Several acyclovir solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 8, as follows:
Table 8
Figure imgf000045_0001
In Examples 10-13, the compositions in Table 6 are prepared as follows. Eudragit RL-PO and ethanol are combined in a glass jar and heated with stirring until the RL-PO is dissolved. The isostearic acid and trolamine is added to the RL-PO/ethanol mixture and the mixture is vigorously stirred. Once a uniform mixture is obtained, acyclovir is added to the mixture and the formulation is vigorously mixed.
Examples 14-15
Prototype peel formulations are prepared as follows. Several acyclovir solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 9, as follows:
Table 9
Figure imgf000046_0001
The compositions of Examples 14 and 15 as shown in Table 8 are prepared as follows. Eudragit RL-PO and ethanol are combined in a glass jar and heated with stirring until the RL-PO is dissolved. The isostearic acid and diisopropanol amine or Neutrol TE Polyol (BASF) is added to the RL-PO/ethanol mixture and the mixture is vigorously stirred. Once a uniform mixture is obtained, acyclovir is added to the mixture and the formulation is vigorously mixed.
Examples 16-17
Prototype solidifying formulations are prepared as follows. Several acyclovir solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 10, as follows:
Table 10
Figure imgf000046_0002
In Examples 16-17 the compositions in Table 10 are prepared as follows. Ethyl cellulose ECN7 or ethyl cellulose ECN 100 and ethanol are combined in a glass jar and heated with stirring until the solid cellulose is dissolved. The isostearic acid and trolamine is added to the cellulose/ethanol mixture and the mixture is vigorously stirred. Once a uniform mixture is obtained, acyclovir is added to the mixture and the formulation is vigorously mixed.
Example 18
The formulations of Examples 10-17 are tested in a hairless mouse skin (HMS) in vitro model described in Example 1. Table 11 shows data obtained using the experimental process outlined above.
Table 11 - Steady-state flux (J) of Acyclovir through HMS
Formulation J* Ratio to (μg/cm2/h) Control
Example 10 12 ± 5 6
Example 1 1 19 ± 1 8
Example 12 8 + 1 4
Example 13 1 ± 1 0.5
Example 14 0.7 ± 0.3 0.35
Example 15 1 ± 0.9 0.5
Example 16 2 + 1 1
Example 17 19 ± 7 8
Zovirax Cream 2 ± 0.4 1
* Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
The formulations of the invention shown above generally provide for significant penetration of the active ingredient, and further, the formulations of Examples 10-12 and 17 are found to be much greater in permeability than the marketed product Zovirax Cream. The quantity of acyclovir that permeated across the HMS stratum corneum over time for Examples 10, 11 , and Zovirax Cream are shown in FIG. 2. Each value shown indicates the mean ± SD of at least three experiments. Examples 10-13 show the impact of the trolamine to isostearic acid (ISA) ratio on acyclovir flux enhancement. The optimal ISA:trolamine ratio is 1 :1 to 2:1 and ratio greater than 4:1 show a significant decrease in the acyclovir skin flux. Additions of diisopropanol amine and Neutrol in place of trolamine (Examples 14 and 15 in the formulation show a significant decrease in acyclovir flux values. This may be due to a specific chemical interaction between trolamine and ISA creating an environment within the formulation which facilitates higher skin flux. Examples 16 and 17 utilize a different solidifying agent to evaluate the impact of the solidifying agent on acyclovir flux. Surprisingly, Example 16 shows a significant decrease in acyclovir skin flux, but Example 17, which differed from Example 16 only by the molecular weight of the solidifying agent, shows no impact on acyclovir skin flux compared to a similar ISA:trolamine ratio in Example 10.
As can be seen from FIG. 2, Examples 10 and 11 show sustained delivery of acyclovir up to 8 hours, it is reasonable to assume based on the drug load and the continued presence of the non volatile solvent that the delivery of acyclovir would continue at the reported flux values for as long as the subject desires to leave the solidifying formulation affixed to the skin.
Examples 19-21
Prototype solidifying formulations are prepared as follows. Several solidifying formulations are prepared in accordance with embodiments of the present invention in accordance with Table 12, as follows:
Table 12
Figure imgf000048_0001
Figure imgf000049_0001
Solidifying formulations of Examples 19-21 are prepared in the following manner:
• The solidifying agents are dissolved in the volatile solvent (e.g., dissolve polyvinyl alcohol in water, Eudragit polymers in ethanol),
• The non-volatile solvent is mixed with the solidifying agent/volatile solvent mixture.
• The resulting solution is vigorously mixed well for several minutes.
• The drug is then added and the solidifying formulation is mixed again for several minutes.
In all the Examples noted above, the flux-enabling non-volatile solvent/solidifying agent/volatile solvent combination is compatible as evidenced by a homogeneous, single phase system that exhibited appropriate drying time, and provided a stretchable solidified layer and steady state flux for the drug (see Example 22 below).
Example 22
The formulations of the examples are tested in a hairless mouse skin (HMS) or HEM in vitro model described in Example 1. Table 13 shows data obtained using the experimental process outlined above.
Table 13 - Steady-state flux (J)
Figure imgf000049_0002
* Skin flux measurements represent the mean and standard deviation of three determinations.
** Data gathered using human epidermal membrane.
***Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed, the steady-state delivery would likely continue well beyond 8 hours.
****Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 6-28 hours. If the experiment was continued it is anticipated the steady state would continue.
Acyclovir, ropivacaine, and testosterone have surprisingly higher steady state flux values when the flux-enabling non-volatile solvent is incorporated into the solidifying formulation. It is speculated that the higher flux values may be the result of contributions of the volatile solvent or the solidifying agent impacting the chemical environment (e.g., increasing solubility) of the drug in the solidifying formulation resulting in higher flux values. Conversely, ketoprofen and diclofenac have lower steady state flux values when the enabling non- volatile solvent is incorporated into the solidifying formulation. This could be the result of the volatile solvent system or solidifying agent having the opposite impact on the chemical environment (e.g., decreasing solubility, physical interactions between drug and solidifying formulation) resulting in lower flux values. The steady state flux value for imiquimod is unchanged when comparing the solidifying formulation with the flux-enabling non-volatile solvent flux values.
Example 23
A formulation with the following composition: 10.4% polyvinyl alcohol, 10.4% polyethylene glycol 400, 10.4% polyvinyl pyrrolidone K-90, 10.4% glycerol, 27.1 % water, and 31.3% ethanol was applied onto a human skin surface at an elbow joint and a finger joint, resulting in a thin, transparent, flexible, and stretchable solidified layer. After a few minutes of evaporation of the volatile solvents (ethanol and water), a solidified layer that was peelable was formed. The non-volatile solvent system of polyethylene glycol and glycerol acts a plasticizer in the formulation. The stretchable solidified layer had good adhesion to the skin and did not separate from the skin on joints when bent, and could easily be peeled away from the skin.
Examples 24-26
Three formulations similar to the formulation in Example 27 (replacing ropivacaine base with ropivacaine HCI) are applied on the stratum corneum side of freshly separated hairless mouse skin. The In vitro flux is determined for each formulation as outlined in Example 1. The formulation compositions are noted in Table 14 below.
Table 14
Figure imgf000051_0001
Flux values represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-9 hours. If the experiment was continued it is anticipated the steady state would continue.
Since all three formulations have the exact same compositions of solidifying agent, volatile solvents, and flux-enabling non-volatile solvent. The only difference is which flux-enabling non-volatile solvent is used it is reasonable to conclude that for ropivacaine HCI that Span 20, polyethylene glycol 400, and Tween 40 qualify as flux-enabling non-volatile solvents.
Addition of tromethamine and Span 20 in example 30 produced a flexible coherent solid that was much less brittle than a formulation containing no nonvolatile solvents. Examples 27-31
A solidifying formulation for dermal delivery of imiquimod is prepared which includes a specified amount of imiquimod in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention. The solidifying formulations contained the following components:
Table 15 - Imi uimod eelable formulation in redients
Figure imgf000052_0001
* Ingredients are noted as weight percent. ** Polymer from Degussa
These formulations are applied to HMS skin as described in Example 1 , and the imiquimod flux is measured. A summary of the results from in vitro flux studies carried out with the formulations in Examples 27-31 are listed in Table 16.
Table 16 - Steady-state flux of imiquimod through hairless mouse skin from various adhesive formulations at 35 0C
Figure imgf000052_0002
The flux values represent the mean and SD of three determinations ** Ratio to control calculated by dividing the flux value for each Example by the flux value for Aldara control flux.
Regarding the formulation described in Examples 27 and 28, water is used as the volatile solvent, and the ISA, trolamine mixture is used as the non-volatile solvent system. Through experimentation, it is determined that ISA and Span 20 provide the appropriate solubility for the drug, however, these non-volatile solvents are hydrophobic and not compatible with the volatile solvent system used to dissolve the solidifying agent PVA. An emulsifier Pemulen TR-2 was used to emulsify the non-volatile solvents into the water phase. Further, in this embodiment, ISA and trolamine act as a plasticizer in the peelable formulation after the water (volatile solvent) has evaporated. The steady state flux of formulation Examples 27 and 28 demonstrate the importance of the amount of non-volatile solvent in added to the formulation in dictating the flux-generating power of the entire formulation. Formulation Examples 29-31 utilize a different solidifying agent which is compatible in a non-aqueous volatile solvent system (isopropanol). The selection of non-volatile solvent system ISA/triacetin or ISA/Span 20/troIamine/triacetin combination showed no change in the in vitro flux. The increase in vitro flux is shown to be influenced by an increase in the amount of imiquimod present in the formulation. At imiquimod levels above 4% the drug is saturated in the solidifying formulation. The increase in vitro flux as a function of increased drug addition (Examples 30 and 31) may be due to the increased solubility of drug in the solidified formulation once the volatile solvent is evaporated off. Example 29 demonstrated comparable imiquimod flux to the other formulation Examples, but the importance of the non-volatile solvent system and solidifying agent compatibility necessitated the removal of trolamine because this non-volatile solvent negatively influenced the function of the Plastoid B polymer.
Example 32-35
A solidifying formulation for dermal delivery of imiquimod is prepared which includes a specified amount of imiquimod in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention. The solidifying formulations contained the following components: Table 17 - Imi uimod formulation ingredients
Figure imgf000054_0001
Ingredients are noted as weight percent. ** Polymer from Degussa These formulations are applied to HMS skin as described in Example 1 , and the imiquimod flux is measured. A summary of the results from in vitro flux studies carried out with the formulations in Examples 32-35 are listed in Table 18.
Table 18 - Steady-state flux of Imiquimod through hairless mouse skin from various adhesive formulations at 35 0C
Figure imgf000054_0002
* The flux values represent the mean and SD of three determinations
** Ratio to control calculated by dividing the flux value for each Example by the flux value for Aldara control flux.
In vitro flux of Examples 32-35 is substantially increased compared to the Aldara control. The reason for the improved in vitro flux values is attributed to the addition of salicylic acid. Improved in vitro flux of imiquimod in Examples 32-35 is thought to be due to an ion pair interaction between imiquimod and salicylic acid. The ion pair mechanism is thought that the lipophilicity of the counter ion (salicylic acid) improves the flux of imiquimod across the stratum corneum because it makes imiquimod less 'comfortable' in the formulation. Comparison of the flux of Examples 32-34 show that the selection of the polymer and/or volatile solvents will impact the flux of imiquimod. Example 32 contains PVA and water, one or both of these elements may contribute to an unfavorable medium in which the ion pair can form resulting in a negligible increase in imiquimod flux versus the Aldara control.
Example 36
To demonstrate the ability of the solidified formulations to reduce the transepidermal water loss (TEWL) the following experiment was conducted. A placebo PVA formulation was applied to the top of the hand and the TEWL was measured on a site immediately adjacent to the solidified layer and on top of the solidified layer. The TEWL measurement of the site covered by the solidified layer was 33% lower than the untreated skin site.
Placebo Plastoid B formulation similar to the formulation described in Example 5 was applied to the top of the hand and the TEWL was measured on a side immediately adjacent to the solidified layer and on top of the solidified layer. The TEWL measurement on the site covered by the solidified layer was 30% lower than the untreated skin site.
Examples 37-38
A solidifying formulation for dermal delivery of ropivacaine is prepared which includes a specified amount of ropivacaine in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention. The solidifying formulations contained the following components:
Figure imgf000055_0001
Figure imgf000056_0001
* Ingredients are noted as weight percent.
These formulations are applied to HMS skin as described in Example 1 , and the ropivacaine flux is measured. A summary of the results from in vitro flux studies carried out with the formulations in Examples 37 and 38 is listed in Table 20.
Table 20 - Steady-state flux of Ropivacaine through hairless mouse skin from various adhesive formulations at 35 0C
Figure imgf000056_0002
The flux values represent the mean and SD of three determinations
Regarding the formulation described in Examples 37 and 38, ethanol is used as the volatile solvent, and the ISA, glycerol, trolamine, and PG mixture is used as the non-volatile solvent system. Through experimentation, it is determined that ISA and propylene glycol used together to provide the appropriate solubility for the drug, while being compatible with the Eudragit RL-100 solidifying agent. Further, in this embodiment, ISA, PG and glycerol serve as a plasticizer in the peelable formulation after the ethanol (volatile solvent) has evaporated. The steady state flux of ropivacaine from formulation Examples 37 and 38 demonstrate the importance of the non-volatile solvent in dictating the flux- generating power of the entire formulation.
Example 39
A formulation for dermal delivery of lidocaine is prepared which includes a saturated amount of lidocaine in an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention. The solidifying formulation is prepared from the ingredients as shown in Table 26. Table 21 - Lidocaine formulation com onents
Figure imgf000057_0001
*lngredients are noted as weight percent. ** from Rohm & Haas.
Table 22 Steady-state flux of Lidocaine through hairless mouse skin from various adhesive formulations at 35 0C
Figure imgf000057_0002
The adhesive formulation of lidocaine formulation in the present example has similar physical properties to the formulations in examples noted above. The transdermal flux across hairless mouse skin is acceptable and steady-state delivery is maintained over 8 hours.
Examples 40-43
A formulation for dermal delivery of amitriptyline and a combination of amitripyline and ketamine is prepared which includes an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention. The solidifying formulation is prepared from the ingredients as shown in Table 23.
Figure imgf000057_0003
Figure imgf000058_0001
*lngredients are noted as weight percent. ** from DeGussa.
The ingredients listed above are combined according to the following procedure. The drug(s), water, and triisopropanolamine are combined in a glass jar and mixed until the drug is dissolved. Then the isostearic acid, triacetin, Span 20, and isopropanol are added to the formulation and mixed well. The polymer Plastoid B is added last and heated to about 600C until the Plastoid B is completely dissolved. Once the polymer solution cooled to room temperature, the formulation is stirred vigorously for 2-3 minutes.
The formulations in Table 10 are applied to HMS according to Example 1 , and the flux of amitriptyline and/or ketamine was measured. The results are summarized in Table 24:
Table 24 - Steady-state flux of Amitriptyline and Amitriptyline/Ketamine through hairless mouse skin from various adhesive formulations at 35 0C
Figure imgf000058_0002
The non-volatile solvent systems in the adhesive formulations of amitriptyline and amitriptyline/ketamine were found to exhibit the best compatibility when triacetin was used as the plastizing solvent. For example, when propylene glycol was used in place of triacetin the examples noted above the formulation turned into a soft solid in the storage container in about 12 hours. Replacing propylene glycol with trolamine resulted in a clear, flowable formulation with viscosity low enough so that is can be spread on a skin surface.. Examples 44-47
A formulation for dermal delivery of ropivacaine is prepared which includes an excipient mixture to form an adhesive formulation in accordance with embodiments of the present invention. The solidifying formulation is prepared from the ingredients as shown in Table 25.
Figure imgf000059_0001
* Ilngredients are noted as parts by weight. from Degussa. The ingredients listed above are combined according to the following procedure.
The ropivacaine HCI, water, and triisopropanolamine are combined in a glass jar and mixed until the drug is dissolved. Then the isostearic acid, triacetin, Span 20, and isopropanol are added to the formulation and mixed well. The polymer Plastoid B is added last and heated to about 60 0C until the Plastoid B is completely dissolved. Once the polymer solution cooled to room temperature, the formulation is stirred vigorously for 2-3 minutes.
The formulations in Table 25 are applied to HMS according to Example 1, and the flux of ropivacaine was measured. The results are summarized in Table 26: Table 26 - Steady-state flux of Ropivacaine HCI through hairless mouse skin from various adhesive formulations at 35 0C
Figure imgf000059_0002
The flux in each of Examples 44-47 shows the importance of the triacetin, isostearic acid, Span 20 combination in the formulation. In Examples 45-47 formulations were made without Span 20, triacetin, and isostearic acid respectively. The in vitro flux of ropivacaine was impacted. The synergistic combination of the flux-enabling non volatile solvent system is important in obtaining the maximum in vitro flux of ropivacaine.
Example 48
This formulation has the following ingredients in the indicated weight parts:
Table 27
Figure imgf000060_0001
In this formulation, polyvinyl alcohol (USP grade, from Amresco) is a solidifying agent, ethyl cellulose and Dermacryl 79 are auxiliary solidifying agents. Isostearic acid and glycerol form the non-volatile solvent system while ethanol and water form the volatile solvent system. Ropivacaine is the drug.
Procedures of making the formulation:
1. Ropvicaine is mixed with ISA.
2. Ethyl cellulose and Dermacryl 79 are dissolved in ethanol. 3. PVA is dissolved in water at temperature of about 60-70 C.
4. All of the above mixtures are combined together in one container and glycerol is added and the whole mixture is mixed well.
The resulting formulation is a viscous fluid. When a layer of about 0.1 mm thick is applied on skin, a non-tacky surface is formed in less than 2 minutes. Examples 49-50
Anti-fungal solidifying formulations are prepared and a qualitative assessment of the solidified layer's flexibility and viscosity are evaluated. The formulation components are presented in Table 28 below.
Table 28
Figure imgf000061_0001
The solidifying formulation in Example 49 has a low viscosity that was lower than may be desirable for application on a nail or skin surface. The time to form a solidified layer with this formulation is longer than the desired drying time. The formulation in Example 50 had an increase in the amount of solidifying agent (Eudgragit RL-PO) and decrease in amount of ethanol, which improves the viscosity and drying time. Example 50 has a viscosity suitable for application and an improved drying time.
Example 51
A solidifying formulation was prepared in accordance with Table 29, as follows:
Table 29 - Solidif in formulation for sex steroids
Figure imgf000061_0002
The ingredients of Table 29 were combined as follows:
The solidifying agent is dissolved in the volatile solvent (i.e. dissolve polyvinyl alcohol in water). • The flux enabling non-volatile solvent is mixed with the solidifying agent/volatile solvent mixture.
• The resulting solution is vigorously mixed well for several minutes.
• Drug is then added and the solidifying formulation is mixed again for several minutes.
Example 52
The formulation prepared in Example 51 was tested for Skin Flux, as set forth in Table 30 below.
Table 30 - Peel-forming formulation for sex steroids
Figure imgf000062_0001
*Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed, the steady-state delivery would likely continue well beyond 8 hours.
AndroGel, currently marked product, is applied directly on the hairless mouse skin and the flux determinations are made as outlined in Example 1. The steady state flux data is shown in FIG 1. It should be noted, the steady- state flux value reported in Table 3 is determined using the linear region between 2-6 hours. As can be seen from FIG. 1 , the in vitro flux of testosterone from AndroGel substantially decreases beyond 6 hours. This may be due in part to the evaporation of the volatile solvent which may act as the main vehicle for delivery. The formulation in Example 51 will deliver a steady-state amount of testosterone for at least g hours.
Example 53 A stretchable adhesive formulation for transdermal delivery of ketoprofen
(which is suitable for delivery via skin for treating inflammation or pain of joints and muscles) is prepared which includes saturated amount of ketoprofen in an excipient mixture (more ketoprofen than that can be dissolved in the exctpient mixture) to form an adhesive formulation, some of which is prepared in accordance with embodiments of the present invention. The excipient mixture, which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 31.
Table 31 - Keto rofen formulation com onents
Figure imgf000063_0001
* Ingredients are noted as % by weight.
The compositions of Example 53 were studied for flux of ketoprofen, as shown in Table 32, as follows:
Table 32 - Steady-state flux of Ketoprofen through hairless mouse skin from the adhesive formulation of Exam le 52 at 35 0C
Figure imgf000063_0002
* Skin flux measurement represents the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
Regarding formulation described in Example 53, ethanol and water formed the volatile solvent system, while a 1:1 mixture of glycerol and PEG 400 formed the non-volatile solvent system. Through experimentation, it is determined that PEG 400 is a slightly better solvent than glycerol for ketoprofen, while glycerol is much more compatible with PVA than PEG 400. Thus, the non-volatile solvent system of glycerol and PEG 400 are used together to provide a non-volatile solvent system for the drug, while being reasonably compatible with PVA. In additional detail with respect to the formulation in Example 53, PVA and PVP act as the solidifying agents. Further, in this embodiment, glycerol and PEG 400 also serve as plasticizers in the adhesive formulation formed after the evaporation of the volatile solvents. Without the presence of glycerol and PEG 400, a solidified layer formed by PVA and PVP alone would be rigid and non- stretchable.
Example 54
A formulation similar to the formulation of Example 53 composition (with no ketoprofen) is applied onto a human skin surface at an elbow joint and a finger joint, resulting in a thin, transparent, flexible, and stretchable solidified layer. After a few minutes of evaporation of the volatile solvents (ethanol and water), a solidified layer is formed. The stretchable solidified layer has good adhesion to the skin and does not separate from the skin on joints when bent, and can easily be peeled away from the skin.
Example 55
A stretchable adhesive formulation for transdermal delivery of ketoprofen (which is suitable for delivery via skin on joints and muscles) is prepared which includes saturated amount of ketoprofen in an excipient mixture (more ketoprofen than that can be dissolved in the excipient mixture) to form an adhesive formulation, some of which are prepared in accordance with embodiments of the present invention. The excipient mixture, which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 33. Table 33
Figure imgf000065_0001
* Ingredients are noted in weight percent. Formulations A and B are prepared in the following manner:
• PVA (solidifying agent) is dissolved in water. • The flux adequate non-volatile solvent (glycerol, PG) is mixed together with the solidifying agent/volatile solvent mixture.
• Then ethanol, and Gantrez ES 425 is added to the mixture.
• The resulting solution is vigorously mixed for several minutes. Preparation of the PVA in water solution in Formulation C was not feasible for this molecular weight of PVA at the percentages noted. Formulation C demonstrates that the correct polymer molecular weight for PVA is important to obtain the desired formulation properties.
Formulations A and B are placed on the skin of human volunteers. After a period of several hours, long enough for the volatile solvent to evaporate, the solidified layers were removed by the volunteers and the peelability properties were evaluated. In all instances the volunteers reported that formulation example A could not be removed in one or two pieces, but was removed in numerous small pieces. Formulation example B removed in one or two pieces. The brittle nature of formulation A is attributed to the lower molecular weight PVA sample (Celvol). Low molecular weight PVA does not possess the same cohesive strength as higher molecular weight PVA material (Amresco) due to the reduced size of the polymer chain leading to a reduction in the degree of cross linking and physical interactions between individual PVA polymer chains. The reduced PVA chain interactions lead to a weakened solidified layer that is unable to withstand the mechanical forces the solidified layer is subjected to upon removal.
Example 56-57
A stretchable adhesive formulation for transdermal delivery of ketoprofen
(which is suitable for delivery via skin on joints and muscles) was evaluated which includes a placebo excipient mixture which will form an adhesive formulation, some of which are prepared in accordance with embodiments of the present invention. The excipient mixture, which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 34.
Table 34
Figure imgf000066_0001
* Ingredients are noted in weight percent.
Solidifying formulations in Examples 56 and 57 are prepared in the following manner:
• PVA (solidifying agent) is dissolved in water.
• The flux adequate non-volatile solvent (glycerol, PG) is mixed together with the solidifying agent/volatile solvent mixture.
• Then ethanol, and Gantrez S97 is added to the mixture.
• The resulting solution is vigorously mixed for several minutes. Formulations above were applied on the forearms of study volunteers and the drying time was assessed by placing a piece of cotton to the application site and then applying a 5 gram weight on the cotton. The cotton and weight was removed after 5 seconds. This procedure was started approximately 3 - 4 minutes after application and at 10 to 60 second intervals thereafter until the cotton was removed without lifting the solidified layer from the skin or leaving residue behind. The time when this observation is made is defined as the drying time for the solidifying formulation. The results of the study are summarized in Table 35 below.
Table 35
Figure imgf000067_0001
The amount of water in the formulation did not significantly influence the time for the formulation to dry. However, it was noted during the study that the formulation was difficult to expel from the sample tube. After approximately 4 weeks after the formulation in Examples 56 and 57 were made the sample tubes were retrieved and were evaluated for ease of dispensing the formulation. It was noted that the formulation was impossible to expel from the tube. lnterpolymer complexation between Gantrez S-97 and PVA through electrostatic interactions, hydrophobic interactions, hydrogen bonding, or Van derWaals interactions is hypothesized to be the reason(s) for the observed thickening. Moreover, the extent of this interaction may be dependent on the stoichiometric ratio of the two polymers.
Example 58-61
A stretchable adhesive formulation for transdermal delivery of ketoprofen
(which is suitable for delivery via skin on joints and muscles) was evaluated which includes an excipient mixture which will form an adhesive formulation, some of which are prepared in accordance with embodiments of the present invention. The excipient mixture, which is a viscous and transparent fluid, is prepared using the ingredients as shown in Table 36. Table 36
Figure imgf000068_0001
* Ingredients are noted in weight percent.
Solidifying formulations in Examples 58-61 are prepared in the following manner: • PVA (solidifying agent) is dissolved in water.
• The flux adequate non-volatile solvent (glycerol, PG) is mixed together with the solidifying agent/volatile solvent mixture.
• Then ethanol, and Gantrez ES 425 is added to the mixture.
• The resulting solution is vigorously mixed for several minutes. • After mixing, ketoprofen is added and the final mixture is vigorously mixed again for several minutes.
Formulations noted above were placed in laminate packaging tubes and stored at 25 C/60% RH and 40 C/ 75% RH conditions until pulled for testing. Physical testing was performed on each formulation. Examples 57-59 have been studied the longest and the resulting viscosity increase necessitated the desire to study the viscosity of Example 60. Table 37 summarizes the data generated on each formulation.
Table 37
Figure imgf000068_0002
Figure imgf000069_0001
* Viscosity measured using a RVDV 1+ viscometer at 0.5 rpm.
Examples 58 and 59 had the lowest water content of the four formulations and within 4 weeks of storage attained high viscosity values. The only difference between Examples 58 and 59 is the amount of ethanol in the formulations. It was hypothesized that reducing the level of ethanol may reduce the physical thickening of the formulation due to an incompatibility between the PVA and ethanol. The viscosity data show that the higher ethanol formulation (Example 58) had lower initial viscosity, but over the 4 weeks storage the viscosity of both Examples 58 and 59 attained viscosity values that were too high for a viable formulation. Another hypothesis for the formulation thickening is that PVA is not compatible in high concentrations when dissolved in water. Additional formulations with higher water content were prepared to determine if an optimal water amount would keep the formulation from thickening up over time. Example 60 viscosity after 16 weeks has not reached the viscosity values of the initial viscosity values of Examples 58 and 59.
Placebo versions of the formulations above were applied on study volunteers and the drying time was assessed by placing a piece of cotton to the application site and then applying a 5 gram weight on the cotton. The cotton and weight was removed after 5 seconds. This procedure was started approximately 3 - 4 minutes after application and at 10 to 60 second intervals thereafter until the cotton was removed without lifting the solidified layer or leaving residue behind. The results of the study are summarized in Table 38 below. Table 38
Figure imgf000070_0001
average dry time value from 12 study subjects.
The presence of ethanol as a second volatile solvent appears to significantly reduce the time to dry. In data not shown a local anesthetic formulation containing only water as the volatile solvent and a ratio of water to PVA of 2:1 has a drying time of >15 minutes. Optimizing the ratio and the presence of an additional volatile solvent in formulations containing water significantly reduce the drying time. It is hypothesized that the additional volatile solvent, in this case ethanol, will hydrogen bond with the water and water will escape with the ethanol when evaporating off the skin thereby forming a solidified layer.
Example 62-63
A stretchable adhesive formulation for transdermal delivery of ketoprofen (which is suitable for delivery via skin for treating inflammation or pain of joints and muscles) is prepared which includes ketoprofen in an exctpient mixture to form an adhesive formulation, some of which is prepared in accordance with embodiments of the present invention. The solidifying formulation is prepared from the ingredients as shown in Table 39.
Table 39 - Ketoprofen solidif in formulation com onents
Figure imgf000070_0002
'Ingredients are noted as weight percent. Table 40 - Steady-state flux of ketoprofen through hairless mouse skin from an adhesive solidif in formulations at 35 0C
Figure imgf000071_0001
* Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
Example 64-66
Placebo formulations containing Gantrez ES 425 as an adhesive polymer were prepared for wear studies by volunteers. The formulations are shown as examples in Table 41. All the formulations have polyvinyl alcohol as a solidifying agent to provide tensile strength to the solidifying formulation. The amount of propylene glycol in the formulations was decreased from 19.6% (w/w) to 8.7% (w/w), and the amount of glycerol was increased by the same amount to keep the total non-volatile ratio constant. Keeping the non-volatile ratio constant is important as it determines the drying time and the duration of delivery. The placebo formulations are worn on the palms of hand and percentage adherence of the solidified layer formed after evaporation of volatile solvents was observed after 5-6 hours.
Table 41: Placebo formulations (%w/w ingredients)
Figure imgf000071_0002
Wear study results on 3 volunteers show that 70-80% of solidified layer as described in Example 64 stayed on palms after a duration of 5-6 hours. However, greater than 90% of solidified layer as shown in Example 66 stayed on palms of the volunteers. These examples demonstrate that glycerol is a better plasticizer that propylene glycol for the polyvinyl alcohol polymer. It also shows that the ratio of non-volatile solvent is critical in selecting the formulation for treatment of hand dermatitis.
Examples 67-68 Adhesive formulations containing 0.05% (w/w) clobetasol propionate and
0.15% (w/w) clobetasol propionate with polyvinyl alcohol as solidifying polymer are prepared for in-vitro flux evaluation. Propylene glycol and oleic acid are the non volatile solvents selected for facilitation of clobetasol propionate delivery. As shown in Example 66, glycerol is added as the non volatile solvent for its plasticizing properties. Ratios of ingredients used in the two formulations are shown in Table 42.
Table 42: Clobetasol Propionate solidifying formulations*
Figure imgf000072_0001
Numbers do not add to 100% because of rounding in the second decimal.
Both of the compositions shown above are studied for flux of clobetasol propionate on cadaver skin from three donors. The permeation results are as shown in Table 43. Commercial clobetasol ointment (0.05% w/w) was used as a control formulation. Table 43 - Steady state flux of clobetasol propionate through human cadaver skin at 35 0C
Figure imgf000073_0001
* Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported are determined from the linear region of the cumulative amount versus time plots. The linear region are observed to be between 6-28 hours. If the experiment is continued, it is anticipated the steady state would continue.
As seen from Table 43 formulation described in Example 67 that contained polyvinyl alcohol as a solidifying agent and 0.05% clobetasol propionate had 46% flux of clobetasol propionate when compared to the control formulation. Increasing the clobetasol propionate concentration drug concentration to 0.15% (w/w) increased the steady state flux and the flux values were 94% of the control formulation. It is expected that longer duration of application with the solidifying formulation would increase cumulative delivery in-vivo resulting in effective treatment of dermatitis.
Example 69
Adhesive formulations containing 0.05% (w/w) clobetasol propionate with gelatin as solidifying agent are prepared for in-vitro flux evaluation. Propylene glycol, isostearic acid, and oleic acid are used as non-volatile solvents to facilitate delivery of clobetasol. Talc is added as a filler to reduce the drying time the formulation. Ratio of ingredients used in the formulation is shown in Table 44. Table 44: Clobetasol Propionate formulations*
Figure imgf000074_0001
Numbers do not add to 100% because of rounding in the second decimal.
Unlike the polyvinyl based formulations shown in previous examples, the fish gelatin based formulation shown in Example 44 is a water washable formulation and can be easily removed by subjects suffering from hand dermatitis. Steady state flux across human cadaver skin from 3 donors with formulation as described in Example 69 is compared to the commercial clobetasol ointment. The permeation results are shown in Table 45.
Table 45 - Steady state flux of clobetasol propionate through human cadaver skin at 35 0C
Figure imgf000074_0002
"Skin flux measurements represent e mean and standard deviation of three determinations. Flux measurements reported are determined from the linear region of the cumulative amount versus time plots. The linear region are observed to be between 6-28 hours. If the experiment is continued, it is anticipated the steady state would continue.
As seen from Table 45, formulation described in Example 69 has 62% higher steady state flux when compared to the commercial ointment. Higher steady state flux would result is expected to reduce inflammation in difficult to treat dermatitis and psoriasis cases.
Example 70
Adhesive formulations containing 0.05% (w/w) clobetasol propionate with gelatin as solidifying polymer are prepared for in-vitro flux evaluation. Propylene glycol, and isostearic acid are used as non-volatile solvents to facilitate delivery of clobetasol. Fumed silica is added as a filler to reduce the drying time the formulation. Ratio of ingredients used in the formulation is shown in Table 46.
Table 46: Clobetasol Propionate formulations*
Figure imgf000075_0001
Numbers do not add to 100% because of rounding in the second decimal.
The fish gelatin based formulation shown in Example 70 is a water washable formulation and can be easily removed by subjects suffering from hand dermatitis. Steady state flux across human cadaver skin from 4 donors with formulation as described in Example 70 is compared to the commercial clobetasol ointment. The permeation results are shown in Table 47. Table 47 - Steady state flux of clobetasol propionate through human cadaver skin at 35 0C
Figure imgf000076_0001
*Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported are determined from the linear region of the cumulative amount versus time plots. The linear region are observed to be between 6-28 hours. If the experiment is continued, it is anticipated the steady state would continue.
As seen from Table 47, on an average, formulation described in Example 70 has at-least similar or better steady state flux when to compared to the steady state flux with the commercial ointment. Unlike talc used in Example 69, fumed silica had a low density and is expected to have a less potential to separate from the formulation.
Examples 71-73
Solidifying formulations for dermal delivery of ropivacaine HCI are prepared which include excipient mixtures in accordance with embodiments of the present invention. The formulations are prepared from the ingredients as shown in Table 48.
Table 48 - Ro ivacaine HCI solidif in formulation com onents.
Figure imgf000076_0002
ingredients are noted as weight percent. ** from Degussa.
The ingredients listed above are combined according to the following procedure. The ropivacaine HCI, water, and the amine base (triethylamine or diisopropanolamine) are combined in a glass jar and mixed until the drug is dissolved. Then the isostearic acid, triacetin, Span 20, and cetyl alcohol (Examples 72 and 73) or isopropanol (Example 71) is added to the formulation and mixed well. The polymer Plastoid B is added last and heated to about 60 0C until the Piastoid B is completely dissolved. Once the polymer solution cooled to room temperature, the formulation is stirred vigorously for 2-3 minutes. The formulations in Table 48 are applied to HMS according to Example 1 , and the flux of ropivacaine was measured. The results are summarized in Table 49:
Table 49 - Steady-state flux of ropivacaine hcl through hairless mouse skin from various adhesive solidif in formulations at 35 0C
Figure imgf000077_0001
Example 74
A prototype peel is prepared in accordance with Table 50 as follows:
Table 50
Figure imgf000077_0002
The formulation was prepared by mixing Plastoid B in isopropyl alcohol until the polymer dissolved, then the remaining components were added and the mixture vigorously stirred until a uniform mixture was obtained. Example 74 illustrates the necessity of an appropriate selection of a nonvolatile solvent and a solidifying agent. After mixing the formulation of Example 74 together, the formulation turned from a flowable solution into two distinct layers: a soft solid and a liquid layer. The formulation in this state is not spreadable on the skin surface. An incompatibility between trolamine and the Plastoid B polymer is suggested because of the hydrophilic nature of the trolamine and the hydrophobic nature of the polymer resulted in the trolamine being squeezed out of the formulation.
Examples 75-77
Prototype peel formulations are prepared as follows. Several peel formulations are prepared in accordance with embodiments of the present invention in accordance with Table 51 , as follows:
Table 51
Figure imgf000078_0001
Peel formulations of Examples 75-77 are prepared in the following manner:
• The solidifying agents are dissolved in the volatile solvent (e.g., dissolve polyvinyl alcohol in water, Eudragit polymers in ethanol),
• The non-volatile solvent is mixed with the solidifying agent/volatile solvent mixture. • The resulting solution is vigorously mixed well for several minutes.
• The drug is then added and the peel formulation is mixed again for several minutes.
In all the Examples noted above, the flux-enabling non-volatile solvent/solidifying agent/volatile solvent combination is compatible as evidenced by a homogeneous, single phase system that exhibited appropriate drying time, and provided a stretchable peel and steady state flux for the drug (see Example 78 below).
The use of a volatile solvent system of water and ethanol at the percentages in Examples 75-77 is an attempt to achieve a balance between drying time and compatibility with the other ingredients (namely PVA in these examples) in the formulations. Addition of ethanol is thought to reduce the drying time for the formulation due to ethanol/water interactions resulting in an increased evaporation rate of the volatile solvents, and enough water is present to ensure compatibility of PVA in the formulations. This is an example of using a two-member solvent system to successfully achieve an acceptable compromise between compatibility with the solidifying agent and the drying time.
Example 78 The formulations of the Examples are tested in a hairless mouse skin
(HMS) or human epidermal membrane (HEM) in vitro model described in Example 1. Table 52 shows data obtained using the experimental process outlined above.
Table 52 - Steady-state flux J
Figure imgf000079_0001
* Skin flux measurements represent the mean and standard deviation of three determinations.
** Data gathered using human epidermal membrane. ***Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed, the steady-state delivery would likely continue well beyond 8 hours.
****Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 6-28 hours. If the experiment was continued it is anticipated the steady state would continue.
In all cases in Table 52, the flux enabling non-volatile solvents in the formulation resulted in therapeutically effective flux for each of the formulations studied.
Example 79
A placebo formulation with the following composition: 10.4% polyvinyl alcohol, 10.4% polyethylene glycol 400, 10.4% polyvinyl pyrrolidone K-90, 10.4% glycerol, 27.1 % water, and 31.3% ethanol was applied onto a human skin surface at an elbow joint and a finger joint, resulting in a thin, transparent, flexible, and stretchable film. After a few minutes of evaporation of the volatile solvents (ethanol and water), a solidified layer that was peelable was formed. The stretchable solidified layer had good adhesion to the skin and did not separate from the skin on joints when bent, and could easily be peeled away from the skin.
Examples 80-82
Prototype peels are prepared as follows. Several acyclovir peel formulations are prepared in accordance with embodiments of the present invention in accordance with Table 53 as follows:
Table 53
Figure imgf000080_0001
The formulation was prepared by mixing Plastoid B in isopropyl alcohol until the polymer dissolved, then the remaining components were added and the mixture vigorously stirred until a uniform mixture was obtained.
Examples 80 and 81 show the importance of an additional polymer to solve the trolamine/polymer incompatibility. Addition of ethylcellulose (N7 and N100) to the formulation reduced the amount of Plastoid B polymer to a level that is compatible with trolamine. The resulting formulation produced a thickened, easily spreadable formulation. The formulation in Example 82 exhibited precipitation, but the thickening due to addition of the N100 ethylcellulose will prevent the settling of the precipitation.
Example 83
The formulations of Examples 80-72 are tested in a hairless mouse skin (HMS) in vitro model described in Example 1. Table 54 shows data obtained using the experimental process outlined above.
Table 54 - Steady-state flux (J) of Acyclovir through HMS
Figure imgf000081_0001
* Skin flux measurements represent the mean and standard deviation of three determinations. Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 4-8 hours. If experimental conditions allowed the steady state flux would extend beyond the 8 hours measured.
Steady-state flux variations of acyclovir through HMS from various lots of mice are expected. For this reason a control (Zovirax cream) is run with each Example formulation. The ratio to control column in Tables 53 and 54 can be compared to evaluate the improvement of the Example formulation over the control. The formulations of the invention shown above generally provide for significant penetration of the active ingredient, and further, the formulations of Examples 80-82 are found to be much greater in permeability than the marketed product Zovirax Cream.
Examples 71-82 show similar in vitro flux increase (based on ratio to control) over the Zovirax control. Addition of ethylcellulose to the formulations in Examples 81-83 may increase the occlusion due to the addition of the hydrophobic polymers.
Examples 84
Prototype peel formulations are prepared as follows. Several peel formulations are prepared in accordance with embodiments of the present invention in accordance with Table 55, as follows:
Table 55
Figure imgf000082_0001
The peel formulation of Example 84 is prepared in the following manner:
• The solidifying agents are dissolved in the volatile solvent (e.g., dissolve polyvinyl alcohol in water, Eudragit polymers in ethanol),
• The non-volatile solvent is mixed with the solidifying agents/volatile solvent mixture.
• The resulting solution is vigorously mixed well for several minutes.
• The drug is then added and the peel formulation is mixed again for several minutes. In the example noted above, the flux-enabling non-volatile solvent/solidifying agents/volatile solvent combination is compatible as evidenced by a homogeneous, single phase system that exhibited appropriate drying time, and provided a stretchable peel and steady state flux for the drug (see Example 85 below).
Addition of Eudragit E-100 polymer into the formulation in Example 84 increases adhesion to the skin surface prior to the evaporation of its volatile solvent(s). The PVA polymer in the formulation provides a solidified layer with high tensile strength that allows it to remain in one piece on the skin surface during the intended time of application. The combination of these two polymers provides a solidified layer with flexibility and adhesion to the skin that does not separate from the skin (sites include skin covering joints) and can easily be peeled away from the skin
Example 85
The formulations of the Examples are tested in a hairless mouse skin (HMS) or HEM in vitro model described in Example 1. Table 56 shows data obtained using the experimental process outlined above.
Table 56 - Steady-state flux (J)
Figure imgf000083_0001
* Skin flux measurements represent the mean and standard deviation of three determinations.
** Data gathered using human epidermal membrane.
***Flux measurements reported were determined from the linear region of the cumulative amount versus time plots. The linear region was observed to be between 6-28 hours. If the experiment was continued it is anticipated the steady state would continue.
Diclofenac have lower steady state flux values when the enabling non-volatile solvent is incorporated into the peel formulation. This could be the result of the volatile solvent system or the solidifying agents having the opposite impact on the chemical environment (e.g., decreasing solubility, physical interactions between drug and peel formulation) resulting in lower flux values. The steady state flux value for imiquimod is unchanged when comparing the peel formulation with the flux-enabling non-volatile solvent flux values.
While the invention has been described with reference to certain preferred embodiments, those skilled in the art will appreciate that various modifications, changes, omissions, and substitutions can be made without departing from the spirit of the invention. It is therefore intended that the invention be limited only by the scope of the appended claims.

Claims

CLAIMSWhat Is Claimed Is:
1. An adhesive solid formulation for dermal delivery of a drug, comprising: a) a drug; b) a solvent vehicle, comprising: i) a volatile solvent system including at least one volatile solvent, and ii) a non-volatile solvent system including at least one non-volatile solvent, and c) a solidifying agent, wherein the formulation has a viscosity suitable for application and adhesion to a skin surface prior to evaporation of the volatile solvent system, wherein the formulation applied to the skin surface forms a solidified layer after at least partial evaporation of the volatile solvent system, and wherein the drug continues to be dermally delivered after the volatile solvent system is at least substantially evaporated, with the proviso that there are at least two volatile solvents, two nonvolatile solvents, or two solidifying agents.
2. A formulation as in claim 1 , wherein the non-volatile solvent system acts as a plasticizer for the solidified agent.
3. A formulation as in claim 1 , wherein the formulation further comprises an additional agent that is added to increase adhesion of the formulation when applied to a skin surface.
4. A formulation as in claim 3, wherein the additional agent includes a member selected from the group consisting of copolymers of methylvinyl ether and maleic anhydride, polyethylene glycol and polyvinyl pyrrolidone, gelatin, low molecular weight polyisobutylene rubber, copolymer of acrylsan alkyl/octylacrylamido, aliphatic resins, aromatic resins, and combinations thereof.
5. A formulation as in claim 1 , wherein the volatile solvent system comprises water.
6. A formulation as in claim 1, wherein the solvent vehicle is substantially free of water.
7. A formulation as in claim 1 , wherein the formulation includes a first volatile solvent and a second volatile solvent, wherein the first volatile solvent is more volatile than the second volatile solvent, and wherein the second volatile solvent has better compatibility with the solidifying agent than the first volatile solvent.
8. A formulation as in claim 1 , wherein the formulation includes a first volatile solvent and a second volatile solvent, wherein the first volatile solvent is more volatile than the second volatile solvent, and wherein the second volatile solvent has better solubility for the drug than the first volatile solvent.
9. A formulation as in claim 1 , wherein the formulation has better solubility for the drug than a formulation that contains the same ingredients except only one of the volatile solvents.
10. A formulation as in claim 1, wherein the formulation includes at least two volatile solvents and has better solubility for the solidifying agent than a formulation that contains the same ingredients except only one of the volatile solvents.
11. A formulation as in claim 1 , wherein at least one of the volatile solvents has a boiling point greater than 20 0C and at least one of the volatile solvents having boiling point lower than 20 0C.
12. A formulation as in claim 1 , wherein at least one of the volatile solvents is selected from the group consisting of a hydrofluorocarbon, dimethyl ether, diethyl ether, propane, isobutane, difluoroethane, butane, 1 ,1 ,1,2 tetrafluorethane, 1 ,1 ,1 ,2,3,3,3-heptafluoropropane, 1 ,1 ,1,3,3,3 hexafluoropropane, and combinations thereof.
13. A formulation as in claim 1 , wherein the volatile solvent system includes at least one solvent more volatile than water, and includes at least one member selected from the group consisting of ethanol, isopropyl alcohol, water, dimethyl ether, diethyl ether, butane, propane, isobutene, 1 ,1 , difluoroethane, 1 ,1 ,1 ,2 tetrafluorethane, 1 ,1 ,1,2,3,3,3-heptafluoropropane, 1 ,1 ,1 ,3,3,3 hexafluoropropane, ethyl acetate, acetone, and combinations thereof.
14. A formulation as in claim 1, wherein the volatile solvent system includes at least one solvent more volatile than water, and includes at least one member selected from the group consisting of iso-amyl acetate, denatured alcohol, methanol, propanol, isobutene, peπtaπe, hexane, chlorobutanol, turpentine, cytopentasiloxane, cyclomethicone, methyl ethyl ketone, and combinations thereof.
15. A formulation as in claim 1 , wherein the non-volatile solvent system includes at least one member selected from the group consisting of glycerol, propylene glycol, isostearic acid, oleic acid, propylene glycol, trolamine, tromethamine, triacetin, sorbitan monolaurate, sorbitan monooleate, sorbitan monopalmitate, butanol, and combinations thereof.
16. A formulation as in claim 1, wherein the volatile solvent system includes at least one member selected from the group consisting of ethanol, iso- propyl alcohol, and combinations thereof.
17. A formulation as in claim 1 , wherein the non-volatile solvent system includes at least one member selected from the group consisting of benzoic acid, butyl alcohol, dibutyl sebecate, diglycerides, dipropylene glycol, eugenol, fatty acids, isopropyl myristate, mineral oil, oleyl alcohol, vitamin E, triglycerides, sorbitan fatty acid surfactants, triethyl citrate, and combinations thereof.
18. A formulation as in claim 1 , wherein the non-volatile solvent system includes at least one member selected from the group consisting of 1 ,2,6- hexanetriol, alkyltriols, alkyldiols, acetyl monoglycerides, tocopherol, alkyl dioxolanes, p-propenylanisole, anise oil, apricot oil, dimethyl isosorbide, alkyl glucoside, benzyl alcohol, bees wax, benzyl benzoate, butylene glycol, caprylic/capric triglyceride, caramel, cassia oil, castor oil, cinnamaldehyde, cinnamon oil, clove oil, coconut oil, cocoa butter, cocoglycerides, coriander oil, corn oil, coriander oil, corn syrup, cottonseed oil, cresol, cyclomethicone, diacetin, diacetylated monoglycerides, diethanolamine, dietthylene glycol monoethyl ether, diglycerides, ethylene glycol, eucalyptus oil, fat, fatty alcohols, flavors, liquid sugarsm ginger extract, glycerin, high fructose corn syrup, hydrogenated castor oil, IP palmitate, lemon oil, lime oil, limonene, milk, monoacetin, monoglycerides, nutmeg oil, octyldodecanol, olive alcohol, orange oil, palm oil, peanut oil, PEG vegetable oil, peppermint oil, petrolatum, phenol, pine needle oil, polypropylene glycol, sesame oil, spearmint oil, soybean oil, vegetable oil, vegetable shortening, vinyl acetate, wax, 2-(2- (octadecyloxy)ethoxy)ethanol, benzyl benzoate, butylated hydroxyanisole, candelilla wax, carnauba wax, ceteareth-20, cetyl alcohol, polyglyceryl, dipolyhydroxy stearate, PEG-7 hydrogenated castor oil, diethyl phthalate, diethyl sebacate, dimethicone, dimethyl phthalate, PEG fatty acid esters, PEG- stearate, PEG-oleate, PEG laurate, PEG fatty acid diesters, PEG- dioleate, PEG-distearate, PEG-castor oil, glyceryl behenate, PEG glycerol fatty acid esters, PEG glyceryl laurate, PEG glyceryl stearate, PEG glyceryl oleate, hexylene glycerol, lanolin, lauric diethanolamide, lauryl lactate, lauryl sulfate, medronic acid, methacrylic acid, multisterol extract, myristyl alcohol, neutral oil, PEG-octyl phenyl ether, PEG-alkyl ethers, PEG-cety] ether, PEG-stearyl ether, PEG-sorbitan fatty acid esters, PEG-sorbitan diisosterate, PEG-sorbitan monostearate, propylene glycol fatty acid esters, propylene glycol stearate, propylene glycol, caprylate/caprate, sodium pyrroltdone carboxylate, sorbitol, squalene, stear-o-wet, triglycerides, alkyl aryl polyether alcohols, polyoxyethylene derivatives of sorbitan-ethers, saturated polyglycolyzed C8-C10 glycerides, N-methyl pyrrolidone, honey, polyoxyethylated glycerides, dimethyl sulfoxide, azone and related compounds, dimethylformamide, N-methyl formamaide, fatty acid esters, fatty alcohol ethers, alkyl-amides (N1N- dimethylalkylamides), N-methyl pyrrolidone related compounds, ethyl oleate, polyglycerized fatty acids, glycerol monooleate, glyceryl monomyristate, glycerol esters of fatty acids, silk amino acids, PPG-3 benzyl ether myristate, Di-PPG2 myreth 10-adipate, honeyquat, sodium pyroglutamic acid, abyssinica oil, dimethicone, macadamia nut oil, limnanthes alba seed oil, cetearyl alcohol, PEG-50 shea butter, shea butter, aloe vera juice, phenyl trimethicone, hydrolyzed wheat protein, and combinations thereof.
19. A formulation as in claim 1, wherein the solidifying agent includes at least one member selected from the group consisting of polyvinyl alcohol, esters of polyvinylmethylether/maleic anhydride copolymer, neutral copolymers of butyl methacrylate and methyl methacrylate, dimethylaminoethyl methacryiate-butyl methacrylate-methyl methacrylate copolymers, ethyl acrylate-methyl methacrylate-trimethylammonioethyl methacrylate chloride copolymers, prolamine (Zein), pregelatinized starch, ethyl cellulose, fish gelatin, gelatin, acrylates/octylacrylamide copolymers, and combinations thereof.
20. A formulation as in claim 1, wherein the solidifying agent includes at least one member selected from the group consisting of ethyl cellulose, hydroxy ethyl cellulose, hydroxy methyl cellulose, hydroxy propyl cellulose, hydroxypropyl methyl cellulose, carboxymethyl cellulose, methyl cellulose, polyether amides, corn starch, pregelatinized corn starch, polyether amides, shellac, polyvinyl pyrrolidone, polyisobutylene rubber, polyvinyl acetate phthalate and combinations thereof.
21. A formulation as in claim 1, wherein the solidifying agent includes at least one member selected from the group consisting of ammonia methacrylate, carrageenan, cellulose acetate phthalate aqueous, carboxy polymethylene, cellulose acetate (microcrystalline), cellulose polymers, divinyl benzene styrene, ethylene vinyl acetate, silicone, guar gum, guar rosin, gluten, casein, calcium caseinate, ammonium casemate, sodium caseinate, potassium caseinate, methyl acrylate, microcrystalline wax, polyvinyl acetate, PVP ethyl cellulose, acrylate, PEG/PVP, xantham gum, trimethyl siloxysilicate, maleic acid/anhydride colymers, polacrilin, poloxamer, polyethylene oxide, poly glactic acid/poly-l-lactic acid, turpene resin, locust bean gum, acrylic copolymers, polyurethane dispersions, dextrin, polyvinyl alcohol-polyethylene glycol copolymers, methyacrylic acid-ethyl acrylate copolymers, methacrylic acid and methacrylate based polymers such as poly(methacrylic acid), and combinations thereof.
22. A formulation as in claim 1, wherein the formulation includes at least two solidifying agents which together are capable of generating a higher flux in the solidified layer than either of the solidifying agents alone.
23. A formulation as in claim 1 , wherein the formulation includes at least two solidifying agents which together provide enhanced physical stability of the formulation greater than either of the at least two solidifying agents alone.
24. A formulation as in claim 1, wherein the formulation includes at least two solidifying agents and at least one of the at least two solidifying agents is an acrylate/octylacrylamide copolymer or a polymethyl vinyl ather/maleic anhydride copolymer.
25. A formulation as in claim 1 , wherein the drug includes multiple pharmaceutically active agents.
26. A formulation as in claim 1 , wherein the drug Includes at least one member selected from the group consisting of acyclovir, econazole, miconazole, terbinafine, lidocaine, bupivacaine, ropivacaine, and tetracaine, amitriptyline, ketanserin, betamethasone dipropionate, triamcinolone acetonide, clindamycin, benzoyl peroxide, tretinoin, isotretinoin, clobetasol propionate, halobetasol propionate, ketoprofen, piroxicam, diclofenac, indomethacin, imiquimod, salicylic acid, benzoic acid, and combinations thereof.
27. A formulation as in claim 1 , wherein the drug includes at least one member selected from the group consisting of amorolfine, butenafine, naftifine, terbinafine, fluconazole, itraconazole, ketoconazole, posaconazole, ravuconazole, voriconazole, clotrimazole, butoconazole , econazole, miconazole, oxiconazoie, sulconazole, terconazole, tioconazole, caspofungin, micafungin, anidulafingin, amphotericin B1 AmB, nystatin, pimaricin, griseofulvin, ciclopirox olamine, haloprogin, tolnaftate, undecylenate, penciclovir, famciclovir, valacyclovir, behenyl alcohol, trifluridine, idoxuridine, cidofovir, gancyclovir, podofilox, podophyllotoxin, ribavirin, abacavir, delavirdine, didanosine, efavirenz, lamivudine, nevirapine, stavudine, zalcitabine, zidovudine, amprenavir, indinavir, nelfinavir, ritonavir, saquinavir, amantadine, interferon, oseltamivir, ribavirin, rimantadine, zanamivir, erythromycin, clindamycin, tetracycline, bacitracin, neomycin, mupirocin, polymyxin B, quinolones, ciproflaxin, bupivacaine, alpha-2 agonists, clonidine, amitriptyline, carbamazepine, alprazolam, ketamine, ketanserin, betamethasone dipropionate, halobetasol propionate, diflorasone diacetate, triamcinolone acetonide, desoximethasone, fluocinonide, halcinonide, mometasone furoate, betamethasone valerate, fluocinonide, fluticasone propionate, triamcinolone acetonide, fluocinolone acetonide, flurandrenolide, desonide, hydrocortisone butyrate, hydrocortisone valerate, alclometasone dipropionate, flumethasone pivolate, hydrocortisone, hydrocortisone acetate, tacrolimus, picrolimus, tazarotene, isotretinoin, cyclosporin, anthralin, vitamin D3, cholecalciferol, calcitriol, calcipotriol, tacalcitol, calcipotriene, piroxicam, diclofenac, indomethacin, imiquimod, rosiquimod, salicylic acid, alpha hydroxy acids, sulfur, rescorcinol, urea, benzoyl peroxide, allantoin, tretinoin, trichloroacetic acid, lactic acid, benzoic acid, progesterone, norethindrone, norethindroneacetate, desogestrel, drospirenone, ethynodiol diacetate, norelgestromin, norgestimate, levonorgestrel, dl-norgestrel, cyproterone acetate, dydrogesterone, medroxyprogesterone acetate, chlormadinone acetate, megestrol, promegestone, norethisterone, lynestrenol, gestodene, tibolene, testosterone, methyl testosterone, oxandrolone, androstenedione, dihydrotestosterone, estradiol, ethniyl estradiol, estiol, estrone, conjugated estrogens, esterified estrogens, estropipate, and combinations thereof.
28. A formulation as in claim 1, wherein the solidified layer is sufficiently flexible and adhesive to the skin such that when applied to the skin at a human joint, the solidified layer will remain substantially intact on the skin upon bending of the joint.
29. A formulation as in claim 1 , wherein the solidified layer is sufficiently flexible and adhesive to the skin such that when applied to a curved skin surface or weight bearing surface on the body, the solidified layer will remain substantially intact on the skin upon bending or stretching of the skin surface or weight bearing surface.
30. A formulation as in claim 1, wherein the formulation is formulated to deliver the drug at a therapeutically effective rate for at least about 2 hours following the formation of the solidified layer.
31. A formulation as in claim 1 , wherein the formulation is formulated to deliver the drug at a therapeutically effective rate for at least about 4 hours following the formation of the solidified layer.
32. A formulation as in claim 1 , wherein the formulation is formulated to deliver the drug at a therapeutically effective rate for at least about 8 hours following the formation of the solidified layer.
33. A formulation as in claim 1 , wherein the formulation is formulated to deliver the drug at a therapeutically effective rate for at least about 12 hours following the formation of the solidified layer.
34. A formulation as in claim 1 , wherein the weight ratio of the nonvolatile solvent system to the solidifying agent is from about 0.1 :1 to about 10:1.
35. A formulation as in claim 1 , wherein the weight ratio of the nonvolatile solvent system to the solidifying agent is from about 0.5:1 to about 2:1.
36. A formulation as in claim 1, wherein the volatile solvent system or the non-volatile solvent system is capable of causing human skin irritation and at least one of the at least two non-volatile solvents of the non-volatile solvent system reduces skin irritation.
37. A formulation as in claim 36, wherein the non-volatile solvent capable of reducing skin irritation includes a member selected from the group consisting of glycerin, propylene glycol, honey, and combinations thereof.
38. A formulation as in claim 1, wherein the solidified layer is formed within about 15 minutes of application to the skin surface under standard skin and ambient conditions.
39. A formulation as in claim 1, wherein the solidified layer is formed within about 5 minutes of the application to the skin surface under standard skin and ambient conditions.
40. A formulation as in claim 1 , wherein the formulation has an initial viscosity prior to skin application from about 100 cP to about 3,000,000 cP.
41. A formulation as in claim 1, wherein the formulation has an initial viscosity prior to skin application from about 1 ,000 cP to about 1 ,000,000 cP.
42. A formulation as in claim 1 , wherein the volatile solvent system comprises a volatile solvent retaining substance.
43. A formulation as in claim 42, wherein the volatile solvent retaining substance is water.
44. A formulation as in claim 42, wherein the volatile solvent retaining substance is hygroscopic.
45. A formulation as in claim 42, wherein the volatile solvent retaining substance is honey, glycerol, or propylene glycol.
46. A formulation as in claim 1, wherein the weight percentage of the volatile solvent system is from about 10 wt% to about 85 wt%.
47. A formulation as in claim 1, wherein the weight percentage of the volatile solvent system is from about 20 wt% to about 50 wt%.
48. A formulation as in claim 1, wherein at least one of the at least two non-volatile solvents is included to improve compatibility with the solidifying agent.
49. A formulation as in claim 1, wherein the non-volatile solvent system is capable of generating higher flux than any single non-volatile solvent in the non-volatile solvent system alone.
50. A formulation as in claim 1 , wherein the non-volatile solvent system provides better plasticizing effect to the solidifying agent than any single nonvolatile solvent in the non-volatile solvent system alone.
51. A formulation as in claim 1 , wherein the solidified layer is coherent, flexible, and continuous.
52. A formulation as in claim 1 , wherein the solidified layer, upon formation, is a soft, coherent solid that is peelable from a skin surface as a single piece or as only a few large pieces relative to the application size.
53. A formulation as in claim 1 , wherein the non-volatile solvent system has better compatibility with the solidifying agent than any single non-volatile solvent in the non-volatile solvent system alone.
54. A formulation as in claim 1 , wherein the solidified layer delivers the drug transdermally.
55. A formulation as in claim 1 , wherein the solidifying agent includes polyvinyl alcohol, the volatile solvent system includes water and an alcohol solvent, and the water to polyvinyl alcohol weight ratio is from about 4:1 to about 1 :1 , and the water to alcohol solvent weight ratio is from about 0.33:1 to about 6:1.
56. A method of dermally delivering a drug, comprising: a) applying an adhesive formulation as set forth in any of claims 1-53 b) solidifying the formulation to form a solidified layer on the skin surface by at least partial evaporation of the volatile solvent system; and c) dermally delivering the drug from the solidified layer to the skin surface at a therapeutically effective rate over a sustained period of time.
57. A method as in claim 56, wherein the step of applying includes applying the adhesive solidifying formulation at a thickness from about 0.01 mm to about 3 mm.
58. A method as in claim 56, wherein the step of applying includes applying the adhesive formulation at a thickness from about 0.05 mm to about 1 mm.
59. A method as in claim 56, wherein the solidified layer is kept on the skin for at least about 2 hours.
60. A method as in claim 56, wherein the solidified layer is kept on the skin for at least about 4 hours.
61. A method as in claim 56, wherein the solidified layer is kept on the skin for at least about 8 hours.
62. A method as in claim 56, wherein the solidified layer is kept on the skin for at least about 12 hours.
63. A method as in claim 56, further comprising the step of peeling the solidified layer from the skin after the sustained period of time to remove the solidified layer.
64. A method as in claim 56, further comprising the step of washing the solidified layer form the skin using a solvent after the sustained period of time to remove the solidified layer.
65. A solidified layer for delivering a drug, comprising: a) a drug; b) a non-volatile solvent system including at least one non-volatile solvent, wherein the non-volatile solvent system is capable of facilitating the delivery of the drug at therapeutically effective rates over a sustained period of time; and c) a solidifying agent, wherein the solidified layer is stretchable by 5% in one direction without cracking, breaking, or separating from a skin surface to which the layer is applied, with the proviso that the solidified layer include at least two non-volatile solvents or at least solidifying agents.
66. A solidified layer as in claim 65, wherein at least one non-volatile solvent in the non-volatile solvent system acts as a plasticizer for the solidifying agent.
67. A solidified layer as in claim 65, wherein solidified layer is sufficiently adhesive and flexible to remain substantially intact on a skin surface adjacent to a joint or muscle group where regular skin stretching occurs.
68. A solidified layer as in claim 65, wherein the weight ratio of the nonvolatile solvent system to the solidifying agent is from about 0.1:1 to about 10:1.
69. A solidified layer as in claim 65, wherein the solidified layer is formed within 15 minutes of the application to the skin surface under standard skin and ambient conditions.
70. A solidified layer as in claim 65, wherein the solidified layer has a thickness from about 0.01 mm to about 3 mm.
71. A solidified layer as in claim 65, wherein the non-volatile solvent system includes at least two solvents selected from the group consisting of 1 ,2,6-hexanetriol, alkyltriols, alkyldiols, acetyl monoglycerides, tocopherol, alkyl dioxolanes, p-propenylanisole, anise oil, apricot oil, dimethyl isosorbide, alkyl glucosides, benzoic acid, benzyl alcohol, butyl alcohol, bees wax, benzyl benzoate, butylene glycol, caprylic/capric triglyceride, caramel, cassia oil, castor oil, cinnamaldehyde, cinnamon oil, clove oil, coconut oil, cocoa butter, cocoglycerides, coriander oil, corn oil, coriander oil, corn syrup, cottonseed oil, cresol, cyclomethicone, diacetin, diacetylated monoglycerides, dibutyl subecate, diethanolamine, dietthylene glycol monoethyl ether, diglycerides, dipropylene glycol, ethylene glycol, eucalyptus oil, eugenol, fat, fatty acid (esters glycerides), fatty alcohols, liquid sugars, ginger extract, glycerin, high fructose corn syrup, hydrogenated castor oil, IPM, IP palmttate, isostearic acid, lemon oil, lime oil, limonene, milk, mineral oil, monoacetin, monoglycerides, nutmeg oil, oleic acid, octyldodecanol, oleyl alcohol, olive alcohol, orange oil, palm oil, polyethylene glycol (PEG), peanut oil, PEG vegetable oil, peppermint oil, petrolatum, phenol, pine needle oil, polypropylene glycol, propylene glycol, sesame oil, spearmint oil, soybean oil, trolamine, tromethemine, vegetable oil, vegetable shortening, vinyl acetate, vitamin E, wax, 2-(2-(octadecyloxy)ethoxy)ethanol, benzyl benzoate, butylated hydroxyanisole, candelilla wax, carnauba wax, ceteareth- 20, cetyl alcohol, polyglyceryl, dipolyhydroxy stearate, PEG-7 hydrogenated castor oil, diethyl phthalate, diethyl sebacate, dimethicone, dimethyl phthalate, PEG fatty acid esters including PEG stearates, PEG oleates, PEG laurates, PEG fatty acid diesters including PEG dioleates, PEG distearates, PEG castor oils, glyceryl behenate, PEG glycerol fatty acid esters including PEG glyceryl laurate, PEG glyceryl stearate, PEG glyceryl oleate, hexylene glycerol, lanolin, lauric diethanolamide, lauryl lactate, lauryl sulfate, medronic acid, methacrylic acid multisterol extract, myristyl alcohol, neutral oil, PEG octyl phenyl ethers, PEG alkyl ethers including PEG cetyl ethers, PEG stearyl ethers, PEG sorbitan fatty acid esters including PEG sorbitan diisosterates, PEG sorbitan monostearates, propylene glycol fatty acid esters including propylene glycol stearate, propylene glycol caprylate/caprate, sodium pyrrolidone carboxylate, sorbitol, squalene, stear-o-wet, triacetin, triglycerides, alkyl aryl polyether alcohols, polyoxyethylene derivatives of sorbitan-ethers, saturated polyglycolyzed C8-C10 glycerides, N-methyl pyrrolidone, honey, polyoxyethylated glycerides, dimethyl sulfoxide, azone and related compounds, dimethylformamide, N-methyl formamaide, fatty alcohol ethers, alkyl-amides (N.N-dimethylalkylamides), N-methyl pyrrolidone related compounds, sorbitan fatty acid surfactants including sorbitan monooleate, sorbitan trioleate, sorbitan monopalmitate, ethyl oleate, polyglycerized fatty acids, glycerol monooleate, glyceryl monomyristate, glycerol esters of fatty acids, and combinations thereof.
72. A solidified layer as in claim 65, wherein the solidifying agent includes at least one member selected from the group consisting of ammonia methacrylate, carrageenan, cellulose, cellulose derivatives including cellulose acetate phthalate aqueous, carboxymethylcellulose, methyl cellulose, hydroxyethylcellulose, ethylcellulose, hydroxypropylcellulose, cellulose acetate (microcrystalline), and cellulose polymers, carboxy polymethylene, xantham gum, divinyl benzene styrene, ethylene vinyl acetate, silicone, polyisobutylene, Shellac (FMC BioPolymer), guar gum, guar rosin, hypromellose phthalate, methyl acrylate, microcrystalline wax, polyvinyl alcohol, polyvinyl acetate, polyvinyl acetate phthalate, PVP ethyl cellulose, polyvinyl pyrrolidone (PVP), acrylate, polyethylene glycol/polyvinyl pyrrolidone copolymers, trimethyl siloxysilicate, maleic acid/anhydride copolymers, polacrilin, poloxamer, polyethylene oxide, poly glactic acid /poly-l-lactic acid, turpene resin, locust bean gum, prolamine (Zein), acrylic copolymers, polyurethane dispersions, gelatin, dextrin, starch, polyvinyl alcohol/polyethylene glycol copolymers, methyacrylic acid/ethyl acrylate copolymers, methacrylic acid and methacrylate based polymers including poly(methacrylic acid) copolymers and methylmethacrylate copolymers, esters of polyvinylmethylether/maleic anhydride copolymers, methyacrylic acid-ethyl acrylate copolymers, copolymers of methyl vinyl ether and maleic anhydride, aminoalkyl methacrylate copolymers, ammonioalkyl methacrylate copolymers, and combinations thereof.
73. A solidified layer as in claim 65, wherein the solidified layer is formulated to deliver the drug at a therapeutically effective rate for at least about 2 hours.
74. A solidified layer as in claim 65, wherein the solidified layer is formulated to deliver the drug at a therapeutically effective rate for from 2 to 12 hours.
75. A solidified layer as in claim 65, wherein the formulation is formulated to deliver the drug at a therapeutically effective rate for at least about 12 hours.
76. A solidified layer as in claim 65, wherein the solidified layer is a soft, coherent solid that is peelable from a skin surface as a single piece or as only a few large pieces relative to the application size.
77. A solidified layer as in claim 65, wherein the solidified layer is at least substantially devoid of volatile solvents, including water and any solvent less volatile than water.
78. A solidified layer as in claim 65, wherein the solidified layer is substantially devoid of water and solvents more volatile than water when the solidified layer contains no more than 10 wt% of water and solvents more volatile than water.
79. A solidified layer as in claim 65, wherein the solidified layer is substantially devoid of water and solvents more volatile than water when the solidified layer contains no more than 5 wt% of water and solvents more volatile than water.
80. A solidified layer as in claim 65, wherein the solidified layer is adhesive to the skin surface on one surface, and is non-adhesive on an opposing surface.
81. A solidified layer as in claim 65, wherein the solidified layer is flux- enabling for the drug.
PCT/US2006/048059 2005-12-14 2006-12-14 Compositions and methods for dermal delivery of drugs WO2007100376A2 (en)

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CA002633464A CA2633464A1 (en) 2005-12-14 2006-12-14 Compositions and methods for dermal delivery of drugs
AU2006339350A AU2006339350A1 (en) 2005-12-14 2006-12-14 Compositions and methods for dermal delivery of drugs
EP06849969A EP1968541A2 (en) 2005-12-14 2006-12-14 Compositions and methods for dermal delivery of drugs
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JP2012149097A (en) * 2008-10-08 2012-08-09 Takada Seiyaku Kk Tacrolimus preparation for external application
US11213587B2 (en) 2010-11-22 2022-01-04 Bausch Health Ireland Limited Pharmaceutical formulations containing corticosteroids for topical administration
US11839656B2 (en) 2010-11-22 2023-12-12 Bausch Health Ireland Limited Pharmaceutical formulations containing corticosteroids for topical administration
AU2012261693B2 (en) * 2011-10-31 2013-10-03 Beiersdorf Ag Fixing of perfume on wet skin
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EP3610891A1 (en) * 2013-11-14 2020-02-19 Lipidor AB Sprayable topical carrier and composition
EP3068437A4 (en) * 2013-11-14 2017-04-05 Lipidor AB Sprayable topical carrier and composition comprising phosphatidylcholine
EP3068437A1 (en) * 2013-11-14 2016-09-21 Lipidor AB Sprayable topical carrier and composition comprising phosphatidylcholine
US11090265B2 (en) 2015-01-30 2021-08-17 Medrx Co., Ltd. Aqueous preparation for external use
US11648256B2 (en) 2015-06-18 2023-05-16 Bausch Health Ireland Limited Topical compositions and methods for treating psoriasis
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US11679116B2 (en) 2015-06-18 2023-06-20 Bausch Health Ireland Limited Topical compositions and methods for treating psoriasis
US11957753B2 (en) 2018-04-30 2024-04-16 Bausch Health Ireland Limited Pharmaceutical formulations containing corticosteroids for topical administration

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CA2633464A1 (en) 2007-09-07
EP1968541A2 (en) 2008-09-17

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