AU2004203072A1 - Composition to enhance permeation of topical skin agents - Google Patents

Description

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AUSTRALIA

PATENTS ACT 1990 COMPLETE SPECIFICATION FOR A STANDARD PATENT

ORIGINAL

Name of Applicant: Actual Inventors: Address for Service is: Johnson Johnson Consumer Companies, Inc.

John Kung and Jue-Chen Liu and Susan M. Niemiec SHELSTON IP Margaret Street SYDNEY NSW 2000 CCN: 3710000352 Attorney Code: SW Telephone No: Facsimile No.

(02) 9777 1111 (02) 9241 4666 Invention Title: COMPOSITION TO ENHANCE PERMEATION OF TOPICAL SKIN

AGENTS

Details of Original Application No. 53544/99 dated 08 October 1999 The following statement is a full description of this invention, including the best method of performing it known to us:- File: 25579AUP01 5003867601. DOC/5844 1A COMPOSITION TO ENHANCE PERMEATION OF TOPICAL SKIN

AGENTS

s 1. Field of the Invention This invention relates to compositions and methods for enhancing the penetration of topical skin agents into the epidermal and dermal layers of the skin.

More particularly, it relates to compositions containing at least one active ingredient, a to skin conditioner or nutrient that can be enhanced and regulated in penetrating the skin with a polymeric emulsifier, and, alternatively, a sugar or a polyoxyethylene alcohol.

2. Background of the Invention In the field of therapeutic skin care, topical agents are often applied to the skin.

is In order to ensure their therapeutic activity, these agents must be applied onto the skin and be allowed to penetrate the epidermis and dermis. Although conceptually simple, this has often proven to be a formidable task, because of the skin's intended function as a well-designed barrier to foreign matter from the ambient environment. The outermost layer of the skin is composed of the stratum canewn, or "horny layer", containing several layers of dead, keratinized and flattened skin cells. This layer is extremely difficult to penetrate. It contains approximately 15% water, 70% protein and lipid. The predominant protein is keratin. In the stratum comeum, a corified envelope forms around the keratin resulting in coreocytes. Between these corneocytes are the lipids that bind the corneocytes together. From this structure, two routes become available for active ingredients to enter the skin.

Hydrophobic active ingredient are generally expected to be more apt to penetrate the skin through the intercellular lipid spaces. Hydrophilic actives, however, are expected to penetrate the stratum corneum through a transcellular pathway, i.e., through the coreocyte. However, even though there are two routes of entry, most topical actives still have difficulty penetrating the stratum coreum. Furthermore, if a composition contains actives that are hydrophobic as well as hydrophilic, the known penetration enhancing agents for one type of active may not serve to assist the penetration of the other and, in fact, may be expected to inhibit such penetration.

Another problem arises when providing formulations that enhance the penetration of topical agents: increasing the amount of active agent in the skin often produces excessive skin irritAtion. This, of course, is extremely undesirable, particularly for patients who are suffering inflammatory skin diseases or conditions.

Therefore, an object of this invention is to provide a delivery system that enhances the skin penetration of topically active agents.

An additional object of this invention is to provide that such delivery system not only allows for enhancing the penetration of the active but regulating delivery of the topical active as well.

Yet another object of this invention is to provide a delivery system having a low irritation profile while enhancing the skin penetration of such active ingredients.

A novel composition that enhances the penetration of hydrophilic and/or hydrophobic topically active compounds through the outermost layer of the skin would be advantageous for delivering therapeutic agents to the skin. Surprisingly, we have found novel compositions that enhance and regulate the penetration of topical active ingredients. Moreover, the compositions of this invention are unexpectedly mild and non-irritating to the skin despite the increased penetration of topical active agents.

Summary of the Invention The novel composition of this invention may enhance the penetration of either hydrophobic or hydrophilic topical active agents. The compositions of this invention fiurther provide a method of enhancing the penetration of both hydrophobic and hydrophilic agents, as well as a method to regulate the penetration of such agents. The novel compositions of this invention that enhance the penetration of hydrophobic active agents contains at least one hydrophobic or hydrophilic active agent, and a polymeric emulsifier. This composition may more preferably contain a sugar.

3 The novel compositions of this invention that enhance the penetration of hydrophilic active agents may also contain at least one hydrophilic penetrationenhancing agent such as a polyoxyethylene alcohol. Additionally, other components that aid in enhancing and regulating the penetration of such topical active agent may be added to the compositions of this invention such as the following: a polymeric emulsifier, a sugar and a polyoxyethylene alcohol. Novel compositions of this invention that possess the property of enhanced penetration that contain a hydrophobic active agent may also contain at least one hydrophilic penetration-enhancing agent such as a sugar.

1 o The novel compositions of this invention that provide the regulation of delivery of hydrophilic and hydrophobic active agents in the same composition contain at least one hydrophobic active agent; at least one hydrophilic active agent, such hydrophilic active agent optionally being a sugar; a sugar; and polyoxyethylene alcohol.

Polymeric emulsifiers, particularly those which have been hydrophobicallymodified, are useful in the compositions of this invention. In both pharmaceutical and cosmetic compositions, lotions and creams have been used as popular delivery vehicles for applying topical actives. Emulsions are two-phase systems that contain two immiscible liquids, typically oil and water. In order to stabilize oil in water, ionic or non-ionic surfactants may be used to reduce interfacial surface tensions creating oil droplets dispersed in water. Unlike traditional emulsifiers, polymeric emulsifiers operate by creating gels around the oil droplets. When these droplets come near each other, they are repelled by the gel layers. Preferably, a nonionic polymeric emulsifier, more preferably a hydrophilic cross-polymer which has been hydrophobically modified and most preferably, a hydrophobically-modified polyacrylic acid emulsifier having from about 10 to about 30 carbon atoms is used in the products and compositions of this invention. Most preferably, the polymeric emulsifier should be Pemulen*, an acrylate/C10-30 alkyl acrylate crosspolymer commercially available from B.F. Goodrich Specialty Chemicals of Cleveland, Ohio. Surprisingly, delivery systems containing lipophilic topical active ingredients formulated in the compositions of this invention in -4 conjunction with Pemulen' provided enhanced penetration of the lipophilic topical active ingredient. Preferably, the polymeric emulsifier should be present in the compositions of this invention an amount of from about 0.01 to about 20% by weight of the composition. More preferably, they should be present in an amount of from about 0.1 to about 5 weight percent of the composition. Most preferably, they should be present in an amount of from about 0.1 to about 1 weight percent of the composition.

Sugars have also been commonly used in pharmaceutical and cosmetic compositions as humectants. Surprisingly, in the compositions of this invention, sugars 0o that were incorporated into such compositions for the purpose of improving the compositions' skin feel characteristics, served to enhance the penetration of hydrophobic topical active ingredients. We also found, surprisingly, that the combination of hydrophobically-modified polymeric emulsifiers and sugars enhanced the penetration of the hydrophobic active ingredients together to a greater degree than is either would if used separately. Moreover, sugars that assist in enhancing penetration may be hydrophilic topically active agents themselves. Sugars that may be useful in the compositions of this invention include, for example, ascorbic acid-2-glucoside, oligosaccharides such as lactose and melibiose and the like. Preferably, the sugar should be present in the compositions of this invention an amount of from about. 0.01 to about 20% by weight of the composition. More preferably, they should be present in an amount of from about 0.1 to about 10 weight percent of the composition. Most preferably, they should be present in an amount of from about 0.1 to about 7 weight percent of the composition.

In order to enhance the penetration of hydrophilic topical actives, a 2 5 polyoxyalkylene alcohol may be incorporated into the compositions of this invention.

More preferably, a polyoxyethylene alcohol may be incorporated into the compositions of this invention. More preferably, such alcohols as steareth-10-20 and the like may be incorporated into the compositions of this invention. Preferably, the polyoxyalkylene alcohol should be present in the compositions of this invention an amount of from about 0.01 to about 20% by weight of the composition. More preferably, they should be present in an amount of from about 0.01 to about 5 weight percent of, the composition. Most preferably, they should be present in an amount of from about 0.01 to about 2 weight percent of the composition.

s In a system that contains both the hydrophobically modified acrylic acid, sugar and polyoxyethylene alcohol, unexpectedly, the compositions not only increase permeation of the topical active ingredients, but can be used to regulate the penetration of the active ingredients as well. For example, by changing the ratios of the ingredients, either hydrophobic or hydrophilic active agent penetration may be up- or downregulated in order to enhance the therapeutic benefits of the formulations of this invention. By balancing the proportions of the elements of the compositions of the invention, proper concentrations of topical actives could be delivered, depending upon the type of benefit desired. For example, a retinoid such as retinol may be utilized in a composition to combat wrinkles and prevent photodamage while ascorbic acid-2glucoside may be utilized for the purpose of promoting even skin tone or preventing sun-induced erythema. Therefore, under some circumstances, the retinol benefit may be up-regulated in order to provide treatment of wrinkles while the penetration into the skin of another undesirable hydrophilic component that functions as a formulation excipient disodium EDTA that causes irritation) may be down-regulated to achieve maximum benefit. Surprisingly, although increased penetration of actives occurred, irritation was found to be minimal.

Thus, for example, in a composition wherein a hydrophobic active ingredient is desired to be delivered to a great extent into the skin and the penetration of an irritating hydrophilic excipient is desired to be down-regulated, the ratio of the hydrophobically modified acrylic acid, sugar and polyoxyethylene alcohol present in such a composition should be from about 0.001 to about 1000. The ratio of the hydrophobically modified acrylic acid to the sugar should be from about 0.001 to about 1000. The ratio of the hydrophobically modified acrylic acid to the polyoxyalkylene alcohol should be from about 0.001 to about 1000. The ratio of the sugar to the polyoxyalkylene should be

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6 from about 0.001 to about 1000. More preferably, the ratios should be as follows: the ratio of the hydrophobically modified acrylic acid, sugar and polyoxyethylene alcohol present in such a composition should be from about 0.1 to about 10. The ratio of the hydrophobically modified acrylic acid to the sugar should be from about 0.1 to about 10. The ratio of the hydrophobically modified acrylic acid to the polyoxyalkylene alcohol should be from about 0.1 to about 10. The ratio of the sugar to the polyoxyalkylene should be from about 0.1 to about The compositions of this invention assist in enhancing skin penetration of hydrophobic, also known as lipophilic, compounds. More particularly, hydrophobic vitamins such as retinol and tocopherol and the like may be incorporated into the compositions of this invention as active agents. To maximize the delivery of a lipophilic agent, the composition contains at least one topical active agent and a hydrophilic polymer that has been hydrophobically modified. The use of a sugar in combination with the hydrophobically-modified hydrophilic polymer unexpectedly is further increases the delivery of the active agent.

The addition of polyoxyalkylene alcohol should increase the penetration and regulation of any hydrophilic ingredients in the composition. Despite the enhanced penetration of the topical agents, the composition is surprisingly non-irritating to the skin.

Any topical dosage form known to those of ordinary skill in the art, including, but not limited to, lotions, gels, sprays, aerosols and mousses.

The compositions of this invention should preferably contain: a topically active amount of a pharmaceutical or cosmetic active ingredient; from about 0.01% to about 20% of a non-ionic polymeric emulsifier; optionally, from about 0.01% to about 20% of a sugar; and optionally, from about 0.01% to about 20% of a polyoxyethylene alcohol.

Detailed Description of the Preferred Embodiments

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7 This invention provides compositions and methods to enhance and regulate the delivery of topical agents. The compositions of this invention comprises a pharmaceutical agent or cosmetic active ingredient, hydrophilic polymer that has been hydrophobically modified, optionally a sugar, optionally, polyoxyalkylene alcohol or any combination thereof. The pharmaceutical active includes any drug, hydrophobic or hydrophilic in nature, that would be appropriate for topical use. The cosmetic active includes any ingredient appropriate for cosmetics, nutrients or skin conditioners. These compositions are also non-irritating to the skin.

The pharmaceutical actives that can be used in the compositions of this invention, but not limited to, are antimicrobials, allergy inhibitors, anti-acne, analgesics, antitussives, antipruritics, anesthetics, antihistamines, anti-infective agents, inflammation inhibitors, anti-emetics, anticholinergics, vasoconstrictors, vasodilators, and wound healing promoters and the like.

The cosmetic active ingredients that can be used in the compositions of this is invention, but not limited to, are vitamins vitamin B complex; including thiamine, nicotinic acid, biotin, pantothenic acid, choline, riboflavin, vitamin B6, vitamin B12, pyridoxine, inositol, camitine; vitamins A, C, D, E, K and their derivatives, provitamins), amino acids and their derivatives, herbal extracts, retinoids, flavonoids, antioxidants, anti-inflammatory, skin conditioners, skin lighteners, chelating agents, cell turnover enhancers, coloring agents, fragrances, pigments and sunscreens and the like.

Preferably, the hydrophobically-modified hydrophilic polymeric emulsifiers used in the compositions of this invention are hydrophobically modified acrylic acids.

Such as akylacrylates and the esters. The akyl chain lengths ranges from C2-C30.

Sugars that can be used in the compositions of this invention may include, but are not limited to, glucose, oligosaccharides, more particularly disaccharides such as fructose, melibiose, xylose, sucrose, arbutin, maltose, glucosides glycosides and derivatives thereof and the like. Sugars function in the compositions of this invention to enhance penetration of both hydrophobic and hydrophilic active ingredients.

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-8- Polyoxyethylene alcohols function in the compositions of this invention to enhance the penetration of hydrophilic active ingredients and can be used in the compositions of this invention. Such polyoxyethylene alcohols include, but are not limited to: ceteths, laureths, myreths, oleths, steareths and trideths. One particularly preferred example is steareth-10 or Brij 76 made by ICI Surfactants of Delaware, USA.

The delivery system and active ingredients are incorporated in a pharmaceutically or cosmetically acceptable vehicle. Preferably, the pH of the compositions of this invention should be from about 5 to about 9, more preferably from about 5 to about 7.

Of course, topical skin care agents known to those of ordinary skill in the art may be incorporated into the compositions of this invention, including mineral oils, animal oils, vegetable oils and silicones have all been used in cosmetic creams and lotions of the emulsion type. In addition to such oils, other emollients and surface active agents have been incorporated in the emulsions, including glyceryl trioleate, acetylated sucrose distearate, sorbitan trioleate, polyoxyethylene monostearate, glycerol monooleate, sucrose distearate, polyethylene glycol (50) monostearate, octylphenoxypoly (ethyleneoxy) ethanol, deacylerin penta-isostearate, sorbitan sesquioleate, hydroxylated lanolin, lanolin, triglyceryl diisostearate, polyoxyethylene oleyl ether, calcium stearoyl-2-lactylate, methyl glucoside sesquistearate, sorbitan monopalmitate, methoxy polyethylene glycol-22/dodecyl glycol copolymer (Elfacos E200), polyethylene glycol-45/dodecyl glycol copolymer (Elfacos ST99), polyethylene glycol 400 distearate and glyceryl stearate; alcohols, such as cetyl alcohol and lanolin alcohol; myristates, such as isopropyl myristate; cetyl palmitate; cholesterol; stearic acid; propylene glycol; glycerine, sorbitol and the like. Thickeners such as natural gums and synthetic polymers, as well as preservatives such as methylparaben, butyl paraben, propylparaben and phenyoxyethanol, coloring agents and fragrances also are commonly included in such compositions. Other active ingredients such as sunscreen materials and antimicrobial materials may be utilized in the compositions of the present invention provided that they are physically and chemically compatible with the other components of the compositions.

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9 The following examples illustrate, but do not serve to limit the scope of the compositions and methods of this invention.

Examples Example 1: Determination of Penetration and Regulation of Topical Agents Five formulations were made containing the following ingredients: Formulation A (Comparison formulation): Ingredient Weight Percent Water 73.86% Thickeners 1.35% Chelating agent 0.10% Panthenol 0.50% Glycerine 3.00% Whitening agent 3.00% PH adjustor 0.05% 1s C12-15 alkyl benzoate 4.00% Octyl hydroxy stearate 1.00% Dimethicone 1.00% Cetyl alcohol 2.50% Cetearyl glucoside 1.40% Tocopheryl acetate and Tocopherol 0.55% Sunscreen 4.00% Preservative .1.25% Stabilizers 1.10% Retinol 0.04% The following formulations B, C, D and E were made as set forth below: Formulation B: Ingredient Weight Percent 10 Water 78.04% Glycerin 3.00% D panthenol 0.50% Disodiuin EDTA 0.10% Preservative 0.73% Preservative 0.3 Acry lates/C1O-30A Ikyl 0.25% Acrylate Cross-Polymfer Carbomer 0.40% Ascorbic Acid .0.0 1% Dibutyhydroxyr-toluene 0.10% Cetyl Alcohol 2.00% C1- 1 alkyl benzoate 4.00% Octyl hydroxy stearate 1.00% Dimethicone 1.00% Di-aipha tocopheryl acetate 0.50% Octyl methoxy-cinnamate 4.00% Propyl paraben 0.17% Na hydroxide 2.60% Retinol 0c: 0.2 0% Tocopherol 0.05% Thea Sinesis Extract 1.00% Formulation C: Inrdet Weight Percent Water 73.39% Glycerin 3.00% 11 D panthenol .0.50% Disodiumn EDTA 0.10% Ascorbic Acid-2G 2.00% Phenoxyethanol 0.73% Methyl paraben 0.35% Xanthan gum 0.20% Hydroxyethylcellulose 1.15% Ascorbic Acid 0.01% Dibutyihydroxytolu ene 0.10% Cetearyl glucoside 1.40% Cetyl Alcohol 2.00%

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2 15 alkyl benzoate 4.00% Octyl hydroxy stearate 1.00% Dimethicone 1.00% Di-alphatocopheryl 0.50%J acetate Octy methoxycinnamate 4.00% Propyl paraben 0.17% Na. hydroxide 2.45% Retinol 50c 0.20% Polyaczylanide laureth 0.70% 7 C13-C14 isoparafin Tocopherol 0.05% Thea Sinesis Extract 1.00% Formulation D: IngreientWeight Percent 12 Water 72.82% Glycerin 3.00% D panthenol 0.50% Disodium EDTA 0.10% Preservative 0.73% Preservative 0.35% Akl0.25% Acrylate Cross-Polymer Dimethicone 1.00% Cetyl Alcohol 2.00% Di-aipha tocopheryl acetate 0.50% Octyl methoxycinnamate 4.00% Propyl paraben 0.17% Na hydroxide 1.50% Retinol 50c 0.18% Ascorbic Adid-2G 6.35% Tocopherol 0.05% Thea Sinesis 1. 0 0%C Extract Formulation. E: IngreientWeight Percent' Water Glycerin D panthenol Disodium EDTA Ascorbic Acid-2G 71.59% 3.00% 0.50% 0.10% 2.00% 13 Preservative 0.73% Preservativ e 0.35% Acrylates/Co 30 Alkyl 0.25% Acrylate Cross-Polymer Carbomer 0.40% Ascorbic Acid 0.01% Dibutyhydroxy-toluene 0.10% Steareth-1O 2.00% Cetyl Alcohol 2.00%

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1 5 Akyl benzoate 4.00% Octyl hydroxy stearate, 1.00% Dixnethicone 1.00% Di-aipha. tocopheryl. 0.50% acetate Octyl 4.00% methoxycinnamate Preservative 0.17% Na hydroxide 5.05% Retinol. 50c 0.20% Tocopherol 0.05% Thea Sinesis Extract 1.00% Formuilation. F: Inmrdient Water Squalane Glycerin Macademia Nut Oil Pentae~ythitol Tetraoctanoate Weight Percent 49.484 15.000 10.000 -7.000 5.000 14 Butylene Glycol 4.000 Petrolatum 3.000 Quatemium 18 Hectorite 2.700 Polyglyceryl-2-Diisostearate 2.000 PEG 150 1.000 Retinol 0.166 Trisodium EDTA 0.100 Ascorbic Acid 0.100 Sodium Citrate 0.100 Tocopheryl Acetate 0.100 Preservative 0.100 Preservative 0.100 Butylated Hydroxytoluene (BHT) 0.050 Formulation B was made by adding water to a beaker and overcharging the beaker with 20 grams of water. The water was then purged with argon or nitrogen gas.

After 10-15 minutes, 20 grams of water was removed to check for oxygen content. If there was significant measurable oxygen in the sample, the purging was continued.

Once oxygen was purged from the water, glycerin, panthenol, disodium EDTA, a first preservative and ascorbic acid were added to the beaker. The acrylates/C10-30 alkyl acrylate and carbomer were then added to the water phase. The beaker was then transferred to a vacuum close kettle homogenizer under yellow lights and any residual oxygen removed. The beaker was then heated to 70 750C. A second preservative was added and mixing continued until it dissolved. The water phase was then neutralized with NaOH and the temperature held'at 70 750C for phasing. The remainder of the ingredients but for the Retinol, Tocopherol and Thea Sinesis Extract were combined in a separate beaker and heated to 70 750C. When both phases were at the same temperature and homogenous, the oil phase was added to the water phase under vacuum and homogenized together. The beaked was then cooled slowly. Retinol was added when the temperature reached 55°C and Tocopherol and Thea Sinesis extract 15 added at 45 0 C. Formulation C was made in a similar manner, except that AA-2G was added in addition to the ascorbic acid and, after the ascorbic acid was added, the xanthan gum, hydroxyethylene and glycerin were added to the water phase.

Formulation D was made similarly to Formulation B. Formulation E was made similarly to Formulation C except that Steareth 10 was added to the oil phase.

Formulation F was prepared by combining water, glycerin, PEG150, and butylene glycol in a beaker, and heating it to 75 0 C. At 75°C, Trisodium EDTA, ascorbic acid and sodium citrate was added. Combining squalene, Mac. Nut oil, pentaerythritol tetraoctanoate, petrolatum, quatemium 18 hectoriate, polyglyceryl-2diisostearate, and heating the mixture to 80 0 C while mixing. At 80 0 C, parabens and BHT were added to the mixture. The water phase was added to oil phase slowly and the heated was stopped. At 50 0 C, Vitamin E acetate and retinol were added. The whole process should be under argon and yellow light conditions.

Experiments were conducted to determine the enhanced penetration and regulation effect of the delivery system. To determine transdermal penetration, in vio skin permeation studies were conducted using non-occluded Franz diffusion cells.

Human cadaver skin section were mounted in Franz diffusion cells containing a.

receptor medium composed of a phosphate buffer with 0.025% butylated hydroxytoluene and 1.5% oleth-20. The receptor capacity was 5 milliliters (ml) and the cell surface area was 0.636 cm 2 A 400 pmr dose of one of the following formulations was applied to the diffusion cell. After 24 hours, the surface of the cells were cleansed with a solution of methanol and ethyl acetate. The epidermis and dermis were separated, chopped and placed into vials containing a solution methanol and ethyl acetate and subjected to sonication to fragment the skin. After sonication, the skin fragments were analyzed using HPLC. Samples were taken at zero and 24-hour timepoints. Penetration of active ingredient was calculated based upon a percentage of applied dose. For these studies, the penetration of a lipophilic agent (retinol and a hydrophilic agent (ascorbic acid 2-glucoside, or "AA2G") were investigated.

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A

B err ern E H mao Sug

POC

The formulations investigated are set forth in Table 1 below: TABLE 1 :ipaitonIngredients 0 kOf applied Enhancement %A dose of retinol factor of reunol d( delivered into delivery di epdernis arventional Cetearyl Glucoside 0.175% 1.00N iuSifier (Control) rdrophobic.fl Acrylates/C1O.30 0.642% 3.67N dsfed acrylic acid afllo acryli culsifier .crosspolyrner knventional Ceteasyl glucoside and 0.241% 1-38N iulsifier and sugar AA-2G 'drophobically Acryiates/C1O-30 7.200.

dfied acrylc adid ak4 acryle saugar crosspoymar and AA-2G drphobicall An(ylaes/C1O.30 0-.4-64 01.0 dfied acrylic acid, 21171l acrylae a and crosspolyrnr, AA-2G yoxethylene and shol of -applied Efnanct ~se of AA-2G factor of AA-2G elivered into delivery dns 'A N/A A

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8B% 16%

N/A

5.65 From the. above data, it can be seen that a control formulation (Formulation A) containing only cetearyl glucoside delivered only 0. 175% of the applied dose of retinol into the epidermis. Surprisingly, however, when a formulation containing hydrophobically modified acrylic add emulsifier. was used -(Formulation the percentage of retinol delivered increased to 0.642%, a 3.669 fold increase in delivery.

When AA-2G and cetearyl glucoside were placed into. form ulation -with retinol (Formulation the retinol permeation surprisingly increased to 0.241%, a 1.38-fold increase over the control formulation A. Even more surprisingly, a formulation containing both hydrophobically modified acrylic acid and AA-2G (Formulation D), although an additive effect was expected, a total delivery of retinol of 1.26% or a 7.2 fold increase in retinol delivery to the epiderrmis.

The activity_ of Formulation E. demonstrates that the -addition of a, polyoxyethylene alcohol increased the penetration from 0.18% to 1.016%, or a 5.65fold increase of delivery of AA-2G. Surprisingly, the retinol permeation decreased from 1.25% to 0.464%, a 0.36-fold decrease. Thus, the compositions of this invention

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17 afford a method of regulating the delivery of both hydrophilic and lipophilic ingredients.

Example 2: Low Level of Irritation Demonstrated by Compositions of This Invention Those of ordinary skill in the art of formulating topical skin care compositions would expect an increase in skin irritation to accompany an increase in penetration of active ingredients. The compositions of this invention, however, were surprisingly nonirritating despite the improved penetration of active ingredients.

A standard test for skin irritation, called the "Modified Irritation Study" (MIS) was used to evaluate the delivery system using retinol as the topical agent. This test measures the irritation potential of compositions in human volunteers. Test formulations of this invention were applied to fifty test subjects three times per week for three weeks for a total of nine applications. An occlusive patch with 0.2 to 0.3 gm of each test composition was applied to the upper back of the human subject. The patches remained in place for an initial 24 hours. After 24 hours, the subject would remove the patch from the back. A 24-hour rest period, during which no test material was applied, followed the removal of a Monday and Wednesday patch application. A 48-hour rest period followed a Saturday patch removal.

After each rest period, the test areas were observed by a study coordinator and graded according to a scale of 0 to 4.0. Fresh test material and patches were applied to the identical test sites until nine induction patches were completed.

The nine application scores for each test site for each subject were summed to yield a total score for 21 days. A grand total score for a test sample was obtained by adding the 21-day totals for all subjects. The grand total scores were normalized against the positive control (Formulation F below) which received a normalized score of 100 to obtain a Normalized Irritation Score. The results of these tests are set forth in Table 2 below.

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18

A

B

C

D

TABLE 2 Composition Ingredients Retinol Concentration Convention emulsifier Certeayl Glucoside 0.04% (Control) Hydrophobically Acrylates/C10-30 0.075% modified acrylic acid alkyl acraylae emulsifier crosspolymer Convenrional Ceteiyl glucoside and 0.075% emulsifier and sugar AA-2G Hydrophobically Acrylaes/C10-30 0.075% modified acrylic acid alkyl acrylate and sugar crosspolymer and AA-2G Water-in-oil emulsifier Polyglyceryl-2- 0.15% diisostearate and PEG I ln Totl amount of Normalized retnol delivered Irritation Score 0.21 9.88.

1.44 68.4 Ratio of total retinol delivered-Norma lized Irritation Score 2.1 1.2 13.5 .0.54 2.84 46.5 21

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N/A 100 N/A An increase in retinol penetration would generally be expected to result in higher skin irritancy, or a lower ratio of Total Retinol Delivered:Normalized Irritation Score. Ratios of the amount of retinol delivered to the irritation score were calculated to compare the formulations, they represent the amount of retinol delivered per each unit of irritation. As can be seen from the data set forth in Table 2, Formulations A, B and C are all comparable to each other. Formulation is a commercial product known to be mildly irritating. From these results with respect to Formulations A, B and C, it would appear that neither the hydrophobically modified acrylic acid emulsifier nor the sugar have an effect upon irritation mitigation.

However, surprisingly, Formulation D evidences a dramatic increase in retinol delivery per unit of irritation, and, therefore, is considerably less irritating than Formulations A, B and C. We would also expect that the therapeutic index of Formulation D would be greater than that of Formulations A, B or C in light of the increased amount of retinol delivered at a lower extent of irritation. We conclude that the irritation mitigation effect is unexpectedly greater in compositions containing both hydrophobically'modified acrylic acid and sugar.

19 Delivery of hydrqphilic active ingredients using the copstos f this invention and the concomitant irrtation mitigation effectmay. be seen exemplified below in Table 3.

TABLE 3 omoiin Ingredients -AA-2G T_-otal Amountc Njormalzed Ltio of Concentraton AA-2G Inritation Score AA-2G delivered (ug) delivered: Nonnalia Lhritation S D Hdrophobicaly Aaylsees/C17-0. 2% 1.08 21 0.05 modified 2aylic adid amkj acrylare and sugar crosspoyne and AA-2G, E Hydrophobically. Acylates/C10-30. 2% 6.09 26 0.3 modified acrylic add. aly 2aylate sugar anmd awospolymer, AApolyoxyeehylene 2G and serh-lo alcohol F Water-in-oil emnuliqfier Polycyceryl.2- 0% N-/A 100 N/A diisostearate andy 150 59 As set forth above in Table 3, one unit of irritation results in the delivery of 0.05% AA- 2G. With the addition of a polyoxyethylene alcohol, however, this number unexpectedly increases to 0.23%, meaning that more AA-2G is delivered to the skin with a lower irritation, generating a greater efficacy or therapeutic index.

Example 3: Additional Formulations of the Invention The compositions of this invention may be made by traditional preparation method. The following Table 4 illustrates compositionfs of this invention which we believe would -serve to enhance the delivery of hydrophobic and hydrophilic active ingredients to the epidermis and dermis of the skin with relatively low levels of irrtation.

TABLE 4 IneietFunction FOrmltOn I Forultion 2 Formulation 3 atrVehicle s. loco/ 100% a. 100%,, G enHumectant AboutO0- aboutl0o% About 0 -about io% AboutO0- aboui DioanEDTA Chelator About 0- about 1% About 0- about 1% Abou 0-abu Preserv-ative Preservative About 0. 1 to about 2 Abt .1 to abu but01t b Cabmer Thicener About 0 1tao1 -buOlobul AbouI-1 Ibc Peue Hdrophobically About 0.1 to about 1% About -0.25% About 0.25% modified polymer emulsifier Ascorbic Acd. 2- Sugar 0% About 0.1% to about Abot a0.1% t c .lcsie5% 5% Butylated Stab-lze Abou 0to about I% About 0-about i% About0- about I Holuene alcohol Emollient About 0 about 10% About0- about 10% A bout 0 -wabout C12-15 benzoate Emollient About 0 -about 10% About 0- about 10% About 0 -about Dimetsicoane S readin ent About 0to-about 10% About 0Oto about 5% About 2% 10% Neutralizer s. H 5-8 H5-8 pH5-8 SteiretM-O Po0o et~ene alcohol About 0 to about 5% About 0t bu Aot0t bu Emulsifier .Oobu5 bu~obu SncenSunscreen About 0 to about 10% About 0 to about 10% About 0 to about The compositions of this' Ivention may be administered topically,; but may also be utilized in delivery of oral and parenteral formulations.

Claims (27)

1. A composition comprising an active agent selected from the group consisting of hydrophobic active agents and hydrophilic active agents and a combination thereof and a polymeric emulsifier.

2. A composition according to claim 1 wherein said composition further comprises a hydrophobically-modified hydrophilic polymer.

3. A composition according to claim 1 wherein said composition further comprises a sugar.

4. A composition according to claim 2 wherein said hydrophobic and hydrophilic active agents are selected from the group consisting of one or more of the following: antimicrobials, allergy inhibitors, anti-acne, analgesics, antitussives, antipruritics, anesthetics, antihistamines, anti-infective agents, inflammation inhibitors, anti-emetics, anticholinergics, vasoconstrictors, vasodilators, wound healing promoters, vitamin B complex, thiamine, nicotinic acid, biotin, pantothenic acid, choline, riboflavin, vitamin B6, vitamin B12, pyridoxine, inositol, carnitine; vitamins A, C, D, E, K and their derivatives, pro-vitamins, amino acids and their derivatives, herbal extracts, retinoids, flavanoids, anti-oxidants, anti-inflammatory, skin conditioners, skin lighteners, chelating agents, cell turnover enhancers, coloring agents, fragrances, pigments and sunscreens.

5. A composition according to claim 2 wherein said active agent is hydrophobic.

6. A composition according to claim 5 wherein said composition further comprises a hydrophobically-modified hydrophilic polymer.

7. A composition according to claim 6 wherein said hydrophobically-modified hydrophilic polymer is a hydrophobically modified acrylate.

8. A composition according to claim 7 wherein said hydrophobically modified acrylate is acrylates/C10-30 alkyl acrylate cross-polymer.

9. A composition according to claim 5 wherein said composition further comprises a polyoxyalkylene alcohol.

A composition according to claim 9 wherein said polyoxyalkylene alcohol is a polyoxyethylene alcohol.

11. A composition according to claim 10 wherein said polyoxyethylene alcohol is a stearethl0-20. -22-

12. A composition according to claim 5 wherein said composition further comprises a sugar.

13. A composition according to claim 12 wherein said sugar is selected from the group consisting of: ascorbic acid-2-glucoside, oligosaccharides such as lactose and melibiose and combinations thereof.

14. A composition according to claim 13 wherein said sugar is ascorbic acid-2- glucoside.

A composition according to claim 2 wherein said active agent is hydrophilic.

16. A composition according to claim 15 wherein said active agent is ascorbic acid-2- glucoside.

17. A composition according to claim 15 wherein said composition further comprises a hydrophobically-modified hydrophilic polymer.

18. A composition according to claim 17 wherein said hydrophobically-modified hydrophilic polymer is a hydrophobically modified acrylate.

19. A composition according to claim 18 wherein said hydrophobically modified acrylate is acrylates/C10-30 alkyl acryalte cross-polymer.

A composition according to claim 15 wherein said composition further comprises a polyoxyalkylene alcohol.

21. A composition according to claim 20 wherein polyoxyalkylene alcohol is a polyoxyethylene alcohol.

22. A composition according to claim 21 wherein said polyoxyethylene alcohol is steareth10-20.

23. A method of mitigating retinoid irritation of human skin in a composition containing a retinoid comprising applying to said skin a sugar selected from the group consisting of: ascorbic acid-2-glucoside, oligosaccharides such as lactose and melibiose and combinations thereof.

24. A method according to claim 23 wherein said sugar is ascorbic acid-2-glucoside.

A method of controlling the administration of hydrophilic or hydrophobic active ingredients using a-composition of claim 1.

26. A composition for enhancing the penetration of a topical skin agent substantially as herein described with reference to any one of the embodiments of the invention illustrated in the accompanying examples but excluding any comparative examples. I -23-

:27. A method of mitigating retinoid irritation of human skin substantially as herein described with reference to any one of the embodiments of the invention illustrated in the accompanying examples. DATED this 7 th Day of July 2004 Shelston IP Attorneys for: Johnson Johnson Consumer Companies, Inc.