CH656307A5 - PREPARATION FOR LOCAL ACNE TREATMENT. - Google Patents

Description

The invention relates to pharmaceutical preparations for the topical treatment of acne.

Acne is a well-known inflammatory disease in areas of the skin where the sebaceous glands are the largest, most numerous and most active. In its lighter forms, acne is a more or less superficial impairment, which manifests itself in slight spotty irritations, and normal skin hygiene is a satisfactory treatment. However, in the more inflammatory forms of acne, bacteria penetrate into and around the hair follicles and occur for the formation of

Pustules, infected pockets and, in extreme cases, inflamed, infected cysts appear. These inflammations can expand greatly and form permanent disfiguring scars.

Acne is very common during puberty and affects at least 80% of teenagers. It is known that facial rashes in many adolescents lead to such mental disorders that they have difficulty in contacting, consequently withdrawing and feeling sorry for themselves. Those affected can be constantly aware of the disfigurement. For these reasons, a medical preparation for the treatment of acne is extremely important and can eliminate the need for psychotherapeutic treatment.

To reduce the severity of acne, the skin has been subjected to various local medical treatments. For this, antibacterial soaps have been used as well as bactericidal agents, e.g. Sulfur and resorcinol. Other topical formulations included benzoyl peroxide, hexachlorophene, erythromycin, or neomycin sulfate, but none of these preparations were really effective.

US Pat. No. 3,535,422 describes a therapeutic preparation for the treatment of acne which contains a uniform dispersion of benzoyl peroxide in a flowable medium which has water and at least one emollient organic agent.

US Pat. No. 4,056,611 relates to a therapeutic preparation for the treatment of acne from a stable dispersion of finely divided benzoyl peroxide in an aqueous alcohol vehicle. This single phase preparation is non-lipoid and contains a nonionic surfactant that is soluble in the aqueous alcohol vehicle.

The US application Ser. No. 60 392 with the filing date of July 25, 1979 by the proprietor describes dioctyl sodium sulfosuccinate as a stabilizing agent for benzoyl peroxide formulations and the improved stability of benzoyl peroxide in finely divided form.

The known peroxide formulations, which contain only fine peroxide particles in an emulsion of water and certain selected emollients, have the disadvantage that when evaporation reduces the water content of the emulsion, the majority of the organic emollients and the large amounts -Zoyl peroxide particles close to the surface of the skin and in contact with the acne spots, which can cause irritation.

In addition, the use of large amounts of nonionic surfactants in these preparations, unless extremely fine peroxide particles are used, is very likely to cause irritation by the peroxide.

Furthermore, due to the strong oxidizing effect of the peroxide component when processed with conventional ointments or emulsions or with other active ingredients, inconsistent compositions are obtained which soon show an unacceptable loss of keratolytic activity.

It has now been found that a mixture of the peroxide of an organic acid other than benzoyl peroxide and erythromycin produces a synergistic effect on the skin. The peroxide inhibits the formation of free fatty acids in the skin, in particular by inactivating extracellular lipase (by oxidation), which is necessary in order to break down triglycerides into free fatty acids and glycerin. Erythromycin effectively reduces the concentration of Corynebacterium acnes, (i.e. P. acnes), normal anaerobic bacteria, which are the main source of lipase. As an example of the peroxide of an organic acid

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may be called lauroyl peroxide. Instead of erythromycin, which is preferred, erythromycin stearate or glu-coheptonate can be used.

The corresponding preparation in which the benzoyl peroxide is used as the peroxide of an organic acid forms the subject of Swiss Patent No. 647 147.

These two components can be applied to the skin as a mixture or separately. In the latter case, the erythromycin is preferably applied first to the skin and immediately or shortly afterwards the peroxide. The order of application can also be reversed. If a mixture is first made and then applied to the skin, it is best to make it at the time of application or to apply the mixture within 24 hours.

The reason for the direct use of the mixture is the relative intolerance of the two active ingredients, which is why it is also advisable to place the two ingredients in separate vials, vials or other containers. According to an advantageous embodiment of the invention, a new carrier is used for the active constituents, as a result of which the mixture of these constituents obtains a surprising stability and storage stability at temperatures which are usually used in the storage of erythromycin solutions. In addition, the new carrier leads to a more uniform dispersion of the active ingredients.

The therapeutic gel according to the invention must contain sufficient peroxides to be therapeutically effective, but should not contain more peroxide than can be dispersed evenly in the carrier in order to obtain a smoothly spreadable preparation. These considerations require that the composition contain at least 1% and no more than 30% by weight peroxide. The peroxide content is preferably 2.5 to 15% by weight. The peroxide component of the composition should be of high purity and in the form of finely divided crystalline particles, preferably in the form of particles with an average average particle size of less than 35 microns. The use of such a finely divided peroxide gives greater stability and shelf life when used in combination with dioctyl sodium sulfosuccinate as a surface-active agent. The gel according to the invention can advantageously be a further wetting agent, e.g. Contain esters, of polyols and sugars, condensation products of ethylene oxide with fatty acids, fatty alcohols, long-chain alkylphenols, long-chain mercaptans, long-chain amides, polyethers of polyhydroxylated fatty alcohols and alkylpolyglycol ethers in an amount of about 3 to about 6% by weight.

Surprisingly, it has been found that the use of a peroxide and an erythromycin compound together with dioctyl sodium sulfosuccinate as a surfactant in an aqueous alcoholic gel vehicle results in a composition that is completely stable with respect to the peroxide component, even at temperatures higher than they normally are such products are used. Even after evaporation, the mixture according to the invention enables a uniform release of the peroxide, so that burning and redness, i.e. Appearances that occur with other sharp formulations are not observed.

The preferred aqueous gel contains 1 to 30 and preferably 5 to 15% by weight of peroxide, in particular very finely divided peroxide with a particle size below 150 microns and an average average particle size below 35 microns. The gel contains dioctyl sodium sulfosuccinate as a surface-active agent which improves the stability of the composition in an amount of 0.1 to 2% by weight of the composition. This can also advantageously contain a further wetting agent in an amount of 1.0 to 6.0% by weight and preferably 3 to 6% by weight.

Further advantages of the invention emerge from the attached drawings:

Figure 1 shows in perspective a package with two containers for the two active components.

Figure 2 shows a section along the line 2-2 of the figure

1,

3 shows a section along the line 3 - 3 of Figure 2 and

Figure 4 is a perspective view of a pack with a single container.

A mixture of the two active ingredients can be easily dusted on the affected area of the skin, as is done with an ordinary face powder. For this purpose, one can either use the mixture shown in FIG. 4 or apply the separate components in the two containers of FIG. 1 one after the other, or a mixture of the two components of FIG. However, the mixture can be stretched with a carrier that is a powder, a semi-solid carrier of creamy consistency or. a liquid, such as a water emulsion or an organic solvent, in particular an aqueous mixture which contains dioctyl sodium sulfosuccinate as surface-active agent.

On a weight basis, the selected erythromycin and peroxide are measured so that when applied to the skin, the latter is half to 30 times the weight of the former, and preferably 1 to 5 times the weight of the former. In an extender skin application mixture, erythromycin should be 0.5% to 5.0% w / w and peroxide 1.0% to 30% w / w. A preferred concentration is 2 to 3% of the selected erythromycin and 5 to 10% of the selected peroxide.

Since the solubility of erythromycin is limited,

are the preferred dermatological solvents alcohol or acetone, but the formulation according to the invention is not limited to these liquids. Erythromycin decomposes rapidly in solution, even at normal room temperature. Cooling slightly extends the shelf life of these solutions.

A preferred diluent or carrier is a hydroalcoholic gel system, but liquid suspensions and emulsions as well as creams, ointments and powders are also acceptable. The conventional pharmaceutical methods can be used to produce these customary locally applicable preparations. For example, a mixture can be filled in a closable conventional container 9 for an ointment or the like, as shown in Figure 4, since this reduces the stabilization problem. The patient should be advised to keep the preparation in the refrigerator. A small cardboard box or the like 10 is provided for the container 9.

The best for commercial purposes is a small cardboard box 5 with a lid 6 which contains two closable containers, as shown in FIGS. 1 to 3. Only the erythromycin is in one container, and it is large enough that all other components can be mixed in it later. The other container contains an aqueous gel with the peroxide, with or without solvent for the erythromycin, as well as the other ingredients for the preparation of the topical formulation. Surprisingly

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As already stated above, it has been found that the preparation is stable with dioctyl sodium sulfosuccinate as a surface-active agent.

The type and amount of the gel-forming agent used according to the invention can be selected such that products with different viscosities are obtained. Preferred is a gel-forming agent that enables the formulation to be elegantly made to form a stable gel. A large number of gel-forming agents can be used for the purposes according to the invention. Preferred gel-forming agents are pure microcrystalline cellulose, colloidal magnesium aluminum silicate, hydroxypropylmethyl cellulose and the so-called hydroxylated vinyl polymers, in particular those described in US Pat. No. 2,798,053. Of these hydroxylated vinyl polymers, those of particular interest are those which are generally described as interpolymers of a monomeric monoolefinic acid with about 0.1 to about 10% by weight, based on the total monomers, of a monomeric polyether of an oligosaccharide in which the modified hydroxyl groups are etherified with allyl groups, the polyether containing at least two allyl ether groups per oligosaccharide molecule. Commercially available interpolymers of this type are sold under the trade name Carbopole®. These are described as polymers of acrylic acid which are crosslinked with about 1% of a polyallyl ether of sucrose with an average of about 5.8 allyl groups per sucrose molecule. These polymers have a molecular weight of the order of 1,000,000. They are available from B.F. Goodrich Chemical Company and are sold under the trademarks Carbopol® 934, Carbopol® 940 and Carbopol® 941.

The amount of the gel-forming agent in the compositions according to the invention can vary somewhat. Usually the compositions contain 0.1 to 15% and preferably 0.5 to 3% by weight of gelling agent based on the total weight of the finished composition. As already explained above, the simplest locally applicable preparation consists of a mixture of powdered peroxide and erythromycin without a diluent, which, however, should be applied carefully in small amounts to the skin. Instead of a mixture, one and then the other ingredient can be applied to the skin with gentle rubbing to mix the two on the skin. A suitable simple preparation is made as follows:

peroxide

Calcium phosphate erythromycin

Example 1 1 - 35% w / w. 63 - 98.5% w / w 0.5 - 5% w / w.

These ingredients are mixed intimately and dusted on the affected skin area one to four times a day. The mixture could be sold in container 9 of FIG. 4.

An example of a simple liquid preparation that can be applied to the skin one to four times like a conventional facial emulsion is given in the example below. It could be marketed in one of the bottles according to FIG. 1 with or without packaging 5.

Ethanol

Erythromycin

peroxide

Example 2 up to 100% w / w. 0.5 - 5% w / w. 1 - 30% w / w.

Further examples of preparations according to the invention are the following:

Example 3

lotion

The following components are placed in a first container 7:

5

100% by weight

Ethoxylated cetyl stearyl alcohol 7.00% by weight

Cetyl alcohol 0.75% by weight

Isopropyl myristate 5.00% by weight

io butylated hydroxyanisole 0.10% by weight

Polyoxy-40 stearate 0.25% by weight

Deionized or distilled water 68.80% by weight

Propylene glycol 3.00% by weight

Peroxide 5.00% by weight

15 acetone 10.00% by weight

Dioctyl sodium sulfosuccinate 0.10% by weight

The following constituent is placed in a container 8, the container being large enough to hold a quantity of solvent, preferably ethanol or acetone, in a ratio of 3 cm 3/20 g of the composition in the container 7.

Erythromycin 2% w / w. the contents of the container 7.

25 Both containers are placed in a pack 5 with the instruction that the contents of container 8 are placed in container 7 and mixed there carefully. Alternatively, 3 cm3 ethanol per 20 g of the material in container 7 can be added to the container with the erythromycin. The Ery-30 thromycin solution in ethanol is then placed in container 7 and mixed thoroughly. This could be done by the pharmacist or the patient. The patient applies the emulsion to the skin one to four times a day like a normal emulsion.

35 A modification of Example 3 is to dilute the contents of the container 8 with the same solvent and to apply some of the contents of the container 7 and then some of the contents of the container 8 to the skin so that the mixture occurs on the skin. This avoids the losses due to the limited shelf life of the mixture.

Example 4

cream

45 The following components are placed in a first container 7:

Ethoxylated cetyl-stearyl alcohol 15.00% by weight cetyl alcohol 1.25% by weight isopropyl myristate 5.00% by weight so butylated hydroxyanisole 0.10% by weight polyoxy-40 stearate 0.25% by weight

deionized or distilled water 60.60% by weight propylene glycol 3.00% by weight peroxide 5.00% by weight

55 acetone 10.00% by weight dioctyl sodium sulfosuccinate 0.10% by weight

The following constituent is placed in a second container 8, the container being large enough to hold a quantity of 60 solvent, preferably ethanol or acetone in a ratio of 3 cm 3/20 g of composition in container 7.

Erythromycin 3% w / w. the contents of the container 7.

The same instructions apply here for the application as for the lotion of example 3. Because of the cream-like consistency, the containers 7 and 8 should have wide openings in order to facilitate the mixing and the removal of the cream.

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Example 5

gel

The following components are placed in the container 7:

Deionized or distilled water 54.65% by weight colloidal bentonite 2.50% by weight

Carboxyvinyl polymer (in the form of the acid) 1.00% by weight dioctyl sodium sulfosuccinate 1.00% by weight

Diisopropanolamine 0.75% by weight

Ethyl alcohol, 200 ° 35.00% by weight

Butylated hydroxyanisole 0.10% by weight

w.%

Peroxide, finely divided 5.00% by weight

In container 8, only erythromycin 3% w / w. the contents of the container 7 included.

The same instructions apply as in example 4 for mixing. Here too, containers with wide openings should be used.

Example 6

suspension

The following components are placed in the container 7:

Deionized or distilled water 56.97% by weight colloidal bentonite 1.50% by weight

Carboxyvinyl polymer (in the form of the acid) 0.25% by weight dioctyl sodium sulfosuccinate 1.00% by weight

Diisopropanolamine 0.18% by weight

Ethyl alcohol, 200 ° 35.00% by weight

Butylated hydroxyanisole 0.10% by weight

Peroxide (finely divided) 5.00% by weight

The container 8 contained only erythromycin in an amount of 2% w / w. the contents of the container 7.

The same instructions as in Example 3 apply to the application.

Example 7

The amounts of peroxide in Examples 3 to 6 can range from 1% to 30% w / w. the content in the container 7 can be reduced or increased, the amount of water being increased or decreased accordingly. The amount of erythromycin in container 8 should be up to 2 times the weight of the peroxide.

Example 8

In Examples 3 to 6, acetone and / or a lower alkanol such as methanol, ethanol and the like is used instead of the water.

Example 9

In the above examples, an erythromycin derivative is used instead of the erythromycin.

In the above examples illustrating the invention, certain components can be replaced by other components in a manner known to those skilled in the field of dermatological preparations. Within the scope of the invention, varying amounts of other constituents or alternative diluents can be added or exchanged, provided the person skilled in the art sees advantages therein. The acetone or the alcohols can also be changed according to the wishes of the person skilled in the art.

Example 10

(A) To 495.0 mg of purified water, 15.0 mg of Carbopol® 940 (a carboxyvinyl polymer in the acid form, manufactured by B.F. Goodrich Company) was added with stirring. After the mixture was stirred for 45 minutes, 4.095 mg of sodium hydroxide in 4.91 ml of purified water was added. The mixture was then stirred for a further 10 minutes, and 150.0 mg of ethyl alcohol, 0.050 mg of perfume and 0.50 mg of methyl salicylate were then added. To the mixture was added a mixture of 210.0 mg of wet-packed, finely divided peroxide (50% peroxide, 50% water), 2.0 mg of dioctyl sodium sulfosuccinate, 41.0 mg of alkyl polyglycol ether and 41.0 mg of purified water. The mixture was stirred for a further 30 min until a smooth gel was obtained.

(B) Three samples of this gel formulation A, each weighing about 20.0 g, were mixed with 0.8 g of erythromycin in 3.0 ml of absolute ethanol, so that a total of i5 23.25 g was obtained. Each gram of sample contained 34.40 mg erythromycin.

On the first day of the experiment (time 0), three 20.0 g gel samples of the active gel were mixed with the erythromycin ethanol solution for three minutes with a plastic spatula and then left to rest for about 15 minutes.

Duplicate samples of 1.0 g were taken from the three samples and subjected to a first addition of methanol and a second addition of 0.1 M pH 8.0 PO4 buffer to a total of 200 ml volume. This mixture was mixed at low speed for 3 minutes at room temperature on a mixer. The solution was then left to stand for 5 minutes to cause the foam to collapse, after which a 1.0 ml sample was taken and brought to 109 ml with 0.1 M pH 8.0 PO4 buffer.

30 These were placed in stainless steel cylinders that had previously been lowered onto inoculated agar plates. The top inoculated layer of 4 ml contained 1.5 ml inoculations with S. lutea (25% light transmission in a 1:40 dilution of the standard solution) per 100 ml of agar. 35 In other cylinders there were corresponding reference standards of (ig / ml erythromycin solutions.

The plates of the standard curve and the test plates were incubated at 35 ° C. for 18 hours. The cylinders were removed and the zone areas read and compared to standard 40 zone areas.

Example 11

(A) 15.0 mg of Carbopol® 940 (a carboxyvinyl polymer in the acid form from B.F. Goodrich Company) were

45 ter stirring mixed with 536.0 mg of purified water. After stirring for 45 minutes, 4.095 mg of sodium hydroxide in 4.91 ml of purified water was added. The mixture was then stirred for 10 minutes, after which 150.0 mg of ethyl alcohol, 0.50 mg of perfume and 0.50 mg of Me-50 ethyl salicylate were added. To the mixture was added a mixture of 210.0 mg of moist-packed, finely divided peroxide (50% peroxide, 50% water), 2.0 mg of dioctyl sodium sulfosuccinate and 41.0 mg of purified water. The mixture was stirred for a further 30 minutes until a 55 smooth gel mixture was obtained.

(B) Samples of gel formulation A weighing about 20.0 g were mixed with 0.5 g erythromycin in 3.0 ml ethanol. The samples, now 22.87 g, were placed in containers. Each gram of the sample contained approximately

60 21.85 mg erythromycin. The product obtained was suitable for the treatment of acne.

Example 12

The following 65 gel formulation was prepared using the procedure of Example 11:

Peroxide (finely divided) 5.46% by weight

Erythromycin 2.00% by weight

Ethyl alcohol 44.10% by weight

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Polyoxyethylene lauryl ether 6.00% by weight

Colloidal magnesium aluminum silicate 2.50% by weight

Hydroxypropyl methyl cellulose 1.00% by weight

Citric acid 0.02% by weight

Dioctyl sodium sulfosuccinate 0.02% by weight

Water to fill up

The product obtained showed good stability and effectiveness for the treatment of acne.

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Claims (12)

656307 PATENT CLAIMS 1. Topical preparation for the treatment of acne, characterized in that it contains, in admixture, the peroxide of an organic acid, with the exception of benzoyl peroxide, and erythromycin, erythromycin stearate or erythromycinglucoheptonate, the peroxide being half to 30 times the weight of the erythromycin compound, based on erythromycin. 2. Preparation according to claim 1, characterized in that the peroxide consists of lauroyl peroxide. 3. Preparation according to claim 1 or 2, characterized in that it contains a pharmaceutically acceptable carrier. 4. Preparation according to claim 3, characterized in that it consists of a gel and contains dioctyl sodium sulfosuccinate as a surface-active and stabilizing agent. 5. Preparation according to one of claims 1 to 3, characterized in that the peroxide makes up 1.0 to 30% by weight and the erythromycin compound makes up 0.5 to 5% by weight of the composition. 6. Preparation according to claim 5, characterized in that the peroxide makes up 5 to 10% by weight and the erythromycin compound makes up 2 to 3% by weight of the composition. 7. Preparation according to claim 1, characterized in that the peroxide is present in the composition in the form of very finely divided crystalline particles, preferably in the form of particles with an average average particle size of less than 35 microns. 8. A preparation according to claim 7, characterized in that it is in the form of an aqueous gel and in addition to the erythromycin compound a) 1 to 30 wt.%, Preferably 5 to 15 wt.%, Peroxide with a particle size of less than 150 microns with a medium average particle size of less than 35 microns and b) contains 0.1 to 2% by weight of dioctyl sodium sulfosuccinate. 9. A preparation according to claim 8, characterized in that it further contains a further wetting agent in an amount of 1.0 to 6.0% by weight and preferably 3 to 6% by weight. 10. A preparation according to claim 8, characterized in that the gel-forming agent consists of colloidal magnesium aluminum silicate, hydroxypropylmethyl cellulose, microcrystalline cellulose or hydroxylated vinyl polymers. 11. A preparation for topical treatment of acne, characterized in that it contains an organic acid peroxide other than benzoyl peroxide and erythromycin, erythromycin stearate or erythromycinglucoheptonate, the peroxide being from half to 30 times the weight of the erythromycin compound, based on erythromycin , and is present separately from the erythromycin compound. 12. A preparation according to claim 11, characterized in that it contains dioctyl sodium sulfosuccinate as a surface-active and stabilizing agent.