JP2020023581A - External composition - Google Patents

Abstract

To provide a formulation technique regarding an external composition comprising a terpenoid compound, the technique making it possible to prevent the deposition of the terpenoid compound even when stored under a low temperature condition.SOLUTION: In the external composition, a terpenoid compound and a heparin analog are used in combination, so that it is possible to prevent the deposition of the terpenoid compound even when stored under a low temperature condition.SELECTED DRAWING: None

Description

  The present invention relates to an external composition containing a terpenoid compound. More specifically, the present invention relates to a composition for external use, in which precipitation of a terpenoid compound is suppressed even under low temperature conditions, and which has excellent formulation stability.

  Terpenoid compounds such as menthol cause mild perception by local cold sensation and exert an analgesic / pruritic effect. Therefore, terpenoid compounds have been widely used for many years and have been formulated in external compositions. On the other hand, terpenoid compounds have a disadvantage that they have poor dissolution stability and are liable to be precipitated when stored under low-temperature conditions even once dissolved. Such precipitation of the terpenoid compound not only causes deterioration of the appearance properties of the external use composition, but also decreases the intended medicinal effect of the terpenoid compound.Therefore, in the external use composition containing the terpenoid compound, There is a need for a formulation design that suppresses precipitation.

  Conventionally, various formulation techniques for suppressing the precipitation of terpenoid compounds have been studied. For example, Patent Document 1 discloses that in a water-containing ointment, precipitation of l-menthol can be suppressed by using 1% by weight or more of l-menthol and a specific ratio of camphor in combination. However, the technique of Patent Document 1 has a drawback that a large amount of camphor is required, there are many restrictions on the formulation design, and since the scent of camphor becomes dominant, there is also a limitation that fragrance is restricted. Patent Literature 2 discloses that in an oral composition, the precipitation of l-menthol can be suppressed by using l-menthol and propylene glycol, glycerin and / or sorbite in a specific ratio. ing. However, Patent Document 2 has a drawback that a sufficient effect of suppressing the precipitation of l-menthol cannot be obtained.

  Against such a background of the prior art, development of a new formulation technique for suppressing the precipitation of a terpenoid compound is desired.

JP-A-2002-154952 JP 2003-81798 A

  An object of the present invention is to provide a formulation technique which can suppress the precipitation of a terpenoid compound even when stored under a low temperature condition in an external composition containing the terpenoid compound.

  The present inventor has conducted intensive studies to solve the above problems, and found that, in a composition for external use, by using a terpenoid compound and a heparin-like substance in combination, the precipitation of a terpenoid compound can be suppressed even at a low temperature. .

In addition, the present inventor has found that an external composition containing a terpenoid compound and a heparin-like substance can suppress the precipitation of a terpenoid compound, but when stored under low-temperature conditions, insoluble aggregates (such as moya) thought to be derived from the heparin-like substance New insolubilities that are easily visible. Therefore, the present inventor further studied diligently and found that, in addition to the terpenoid compound and the heparin-like substance, by adding diphenhydramine, the precipitation of the terpenoid compound under low-temperature conditions was suppressed, and the insoluble aggregation described above was suppressed. It has been found that the formation of products can also be suppressed.

The present invention has been completed by further study based on these findings. That is, the present invention provides the following aspects of the invention.
Item 1. An external composition comprising a terpenoid compound and a heparin-like substance.
Item 2. Item 3. The external composition according to Item 1, further comprising diphenhydramine.
Item 3. Item 3. The external use composition according to Item 2, wherein the diphenhydramine is contained in an amount of 0.1 to 10 parts by weight per 1 part by weight of the heparin-like substance.
Item 4. Item 4. The composition for external use according to any one of Items 1 to 3, wherein the terpenoid compound is a monoterpene.
Item 5. A method for suppressing the precipitation of a terpenoid compound in an external composition containing a terpenoid compound, wherein a terpenoid compound and a heparin-like substance coexist in the external composition.
Item 6. A method for suppressing the formation of insoluble aggregates in an external composition containing a terpenoid compound and a heparin analog, wherein the external use composition comprises a terpenoid compound, a heparin analog, and diphenhydramine.

  According to the present invention, the terpenoid compound is excellent in dissolution stability, and even when stored under low-temperature conditions, the precipitation of the terpenoid compound can be suppressed, so that even in winter or cold regions, the intended medicinal effect of the terpenoid compound can be improved. It is possible to maintain stability.

  Furthermore, according to a preferred embodiment of the present invention, in an external composition containing a terpenoid compound and a heparin-like substance, the formation of insoluble aggregates considered to be derived from the heparin-like substance can be suppressed, so that the appearance properties are good, It has also become possible to provide significantly better formulation stability.

1. External composition The external composition of the present invention is characterized by containing a terpenoid compound and a heparin-like substance. Hereinafter, the composition for external use of the present invention will be described in detail.

Terpenoid compound The topical composition of the present invention contains a terpenoid compound. Terpenoid compounds, once dissolved, have the property of precipitating when stored under low-temperature conditions, but in the external composition of the present invention, terpenoids under low-temperature conditions are acted upon by the action of a heparin-like substance described below. It is possible to effectively suppress the precipitation of the compound.

  The terpenoid compound is also referred to as isoprenoid or terpene, and is usually a compound in which a plurality of isoprene units (5 carbon atoms) are bonded. The terpenoid compounds are monoterpenes (two isoprene units), sesquiterpenes (three isoprene units), diterpenes (four isoprene units), and triterpenes (six isoprene units, depending on the number of isoprene units included). ) Etc. In the external composition of the present invention, any of these terpenoid compounds may be used.

  Specific examples of the monoterpene include alcohol-based monoterpenes such as menthol, thymol, geraniol, linalool, borneol, cineol, and terpineol; aldehyde-based monoterpenes such as citral, citronellal, perillaldehyde, and safranal; camphor, menthon, and carbohydrate Mention is made of, for example, ketone monoterpenes such as mentone and yonone. Specific examples of sesquiterpenes include camazulene, santalen, patchulen, cedrol, cedrenol, farnesol, eugenol, α-bisabolol, β-caryophyllene alcohol, sclareol, geranyl linalool, isophytol, nerolidol, globulol, guaiol, α-Santa roll, catrol, farnesal, germacrone, cyperone, zerumbon, vetiven and the like. In addition, specific examples of diterpenes include retinal. These terpenoid compounds may have any of the d-form, l-form and dl-form when optical isomers are present. Further, these terpenoid compounds may be used alone or in combination of two or more.

  Among these terpenoid compounds, from the viewpoint of suppressing precipitation more effectively, preferably those terpenes, more preferably alcohol monoterpenes, ketone monoterpenes, particularly preferably menthol, borneol, camphor, most preferably Menthol is an example.

  These terpenoid compounds may be used in the form of essential oils containing monoterpenes. The essential oil containing monoterpene can be appropriately selected and used from known ones. For example, the essential oil containing menthol includes peppermint oil, peppermint oil, spearmint oil and the like.

  The content of the terpenoid compound in the composition for external use of the present invention may be appropriately set according to the medicinal properties to be provided in the composition for external use, for example, 0.1 to 10% by weight, preferably 0.1 to 5% by weight. % By weight, more preferably 0.5 to 5% by weight. In general, the higher the content of the terpenoid compound in the composition for external use, the more the precipitation due to storage under low temperature conditions tends to be remarkable. However, in the composition for external use of the present invention, the content of the terpenoid compound is 1% by weight or more. Even with the content, precipitation due to storage under low-temperature conditions can be effectively suppressed. In view of such effects of the present invention, the content of the terpenoid compound in the external composition of the present invention is more preferably 1 to 5% by weight, and particularly preferably 2 to 3% by weight.

Heparin analog The topical composition of the present invention further contains a heparin analog. Heparin-like substances play a role in suppressing the precipitation of terpenoid compounds caused by storage under low-temperature conditions.

  The heparin-like substance is a polysulfated mucopolysaccharide such as chondroitin polysulfate, and is a known drug known to have a moisturizing action, an anti-inflammatory action, a blood circulation promoting action, and the like.

  The origin of the heparin-like substance used in the present invention is not particularly limited, and examples thereof include those obtained by polysulfating mucopolysaccharides and tissues of edible animals (for example, tracheal cartilage such as cows and pigs). Extracted from the lungs). In the composition for external use of the present invention, a heparin-like substance listed in the Japanese Pharmacopoeia Non-Pharmaceutical Standards is suitably used as the heparin-like substance.

  The content of the heparin-like substance in the composition for external use of the present invention may be appropriately set according to the type and the content of the terpenoid compound to be used, for example, 0.05 to 3% by weight. From the viewpoint of more effectively suppressing the precipitation of the terpenoid compound due to storage under low-temperature conditions, the content of the heparin-like substance in the composition for external use of the present invention is preferably 0.1 to 1% by weight, and more preferably. Is from 0.3 to 1% by weight.

In the external composition of the present invention, the ratio between the terpenoid compound and the heparin-like substance is determined according to each of the above-mentioned contents, but the precipitation of the terpenoid compound due to storage under low-temperature conditions is more effectively suppressed. In view of the above, the heparin-like substance is at least 0.01 part by weight, preferably at least 0.05 part by weight, more preferably at least 0.1 part by weight, particularly preferably at least 0.3 part by weight, per part by weight of the terpenoid compound. The above is mentioned. The upper limit of the heparin-like substance per 1 part by weight of the terpenoid compound is not particularly limited, but is, for example, 20 parts by weight, preferably 10 parts by weight.

Diphenhydramine The topical composition of the present invention preferably contains diphenhydramine in addition to the terpenoid compound and the heparin-like substance. An external composition containing a terpenoid compound and a heparin-like substance can suppress the precipitation of the terpenoid compound by storage under low-temperature conditions, but there is a problem that insoluble aggregates likely to be caused by the heparin-like substance are easily generated, but diphenhydramine Can further overcome this problem and provide excellent formulation stability.

  Diphenhydramine is a drug known as an antihistamine. In addition, diphenhydramine can take the form of a salt such as diphenhydramine hydrochloride. However, diphenhydramine (diphenhydramine (non-salt form)) is used in the present invention because diphenhydramine cannot exert the above-described effect of suppressing the formation of insoluble aggregates. You.

  When diphenhydramine is contained in the composition for external use of the present invention, its content may be appropriately set according to the content of the heparin-like substance, and for example, 0.01 to 3% by weight. From the viewpoint of more effectively suppressing the formation of the insoluble aggregates described above, the content of diphenhydramine in the composition for external use of the present invention is preferably 0.1 to 1% by weight and 0.5 to 1% by weight. No.

  The ratio between the heparin-like substance and diphenhydramine is determined according to the above-mentioned contents. From the viewpoint of suppressing the formation of the above-mentioned insoluble aggregates more effectively, the ratio of diphenhydramine to 1 part by weight of the heparin-like substance is reduced. 0.1 parts by weight or more, preferably 0.3 parts by weight or more. The upper limit of diphenhydramine per 1 part by weight of the heparin-like substance is not particularly limited, but is, for example, 10 parts by weight, preferably 5 parts by weight, and more preferably 3 parts by weight.

Composition for external use of the water present invention, for the preparation or the like into the desired formulation, if necessary, may contain water. In a composition for external use containing a terpenoid compound, when water is contained, the precipitation of the terpenoid compound due to storage under low-temperature conditions tends to be remarkable, but the composition for external use of the present invention contains water. Also, the precipitation of the terpenoid compound due to storage under a low temperature condition can be effectively suppressed.

  When water is contained in the external composition of the present invention, the content is not particularly limited, and for example, 0.1% by weight or more. Usually, as the water content increases, the precipitation of the terpenoid compound due to storage under low-temperature conditions tends to be remarkable, but in the external composition of the present invention, even when the water content is high, the low-temperature conditions , The precipitation of the terpenoid compound due to storage in the above can be effectively suppressed. In view of the effects of the present invention, the water content in the external composition of the present invention is preferably 0.3% by weight or more, more preferably 1% by weight or more, and particularly preferably 5% by weight or more. The upper limit of the water content in the composition for external use of the present invention is not particularly limited, but may be, for example, 90% by weight, preferably 80% by weight, and more preferably 70% by weight.

Polyhydric alcohol The external composition of the present invention may contain a polyhydric alcohol, if necessary, for the purpose of further enhancing the effect of suppressing precipitation of the terpenoid compound by storage under low-temperature conditions.

  The polyhydric alcohol is not particularly limited as long as it is pharmaceutically or cosmetically acceptable. For example, propylene glycol, ethylene glycol, 1,3-butylene glycol, isoprene glycol, diethylene glycol, dipropylene glycol, Glycerin and the like. These polyhydric alcohols may be used alone or in combination of two or more. Among these polyhydric alcohols, propylene glycol, 1,3-butylene glycol, dipropylene glycol, and glycerin are preferred.

  When a polyhydric alcohol is contained in the composition for external use of the present invention, the content may be appropriately set according to the type of the polyhydric alcohol to be used, the formulation of the composition for external use, and the like. 1 to 50% by weight, preferably 1 to 30% by weight, more preferably 3 to 20% by weight.

Monohydric Lower Alcohol The topical composition of the present invention may contain a monohydric lower alcohol depending on the formulation form and the like.

  The monohydric lower alcohol is not particularly limited as long as it is pharmaceutically or cosmetologically acceptable. For example, the carbon number of ethanol, propanol, isopropanol, n-butanol, sec-butanol, tert-butanol, etc. 1-4 monohydric lower alcohols. These monohydric lower alcohols may be used alone or in a combination of two or more. Among these monohydric lower alcohols, preferred are ethanol and isopropanol.

  In the external composition of the present invention, when a monohydric lower alcohol is contained, the content thereof may be appropriately set according to the type of the monohydric lower alcohol to be used, the formulation of the external composition, and the like. 0.1 to 50% by weight, preferably 1 to 30% by weight.

Other Components In addition to the components described above, the externally applied composition of the present invention may contain other additives usually used in the externally used composition in order to obtain a desired formulation. Such additives include, for example, aqueous bases, oil bases, thickeners, pH adjusters, surfactants, emulsifiers, solubilizers, preservatives, preservatives, antioxidants, stabilizers, Chelating agents, fragrances, coloring agents and the like can be mentioned.

  In addition, the external composition of the present invention may contain other pharmacological components, if necessary, in addition to the components described above, as long as the effects of the present invention are not hindered. The pharmacological components that can be added to the composition for external use of the present invention are not particularly limited. Meprilcaine or a salt thereof, an alkyl benzoate (eg, diethylaminoethyl parabutylaminobenzoate hydrochloride), orthocaine, oxesazein, oxypolyentoxydecane, funnel extract, percaminpase, tesit decithin, etc., an anti-inflammatory agent (glycol salicylate, methyl salicylate, Indomethacin, felbinac, diclofenac sodium, loxoprofen sodium, etc.), fungicides (decalinium chloride, cetylpyridinium chloride, chlorhexidine hydrochloride, Chlorhexidine conate, aqueous ammonia, sulfadiazine, phenol, etc.), antipruritic (thiantol, etc.), skin protectant (castor oil, etc.), blood circulation promoting components (nonylate varnishylamide, nicotinic acid benzyl ester, capsaicin, capsicum extract, etc.), muco Polysaccharides (such as sodium chondroitin sulfate and glucosamine); and humectants (amphoteric surfactants such as trimethylglycine, methacryloyloxyethyl phosphorylcholine and copolymers thereof (eg, copolymers with alkyl methacrylate)), and the like. These medicinal components may be used alone or in combination of two or more. When these pharmacological components are contained in the composition for external use of the present invention, the contents thereof may be appropriately set according to the type of the pharmacological components used, the expected effects, and the like.

Formulation Form and Usage Aspect The external composition of the present invention is used as a transdermal formulation (external medicine, cosmetic, etc.), and is particularly suitably used as an external medicine.

  The formulation of the composition for external use of the present invention is not particularly limited as long as it can be applied transdermally. For example, a liquid preparation (including a lotion, a spray, an aerosol, and an emulsion), a water-soluble ointment Agents, oily ointments, creams, foams, gels, patches and the like. Among these, liquid preparations, ointments and creams are preferred. Preparation into these dosage forms can be carried out by formulating with an additive according to the dosage form according to a known method described in the 16th Revised Japanese Pharmacopoeia General Rules for Preparations and the like.

  The externally applied composition of the present invention can exert a cooling effect by a terpenoid compound, an analgesic / pruritic effect by local cooling stimulus, and the like, and is used by being applied to skin where cooling, analgesic / pruritus is required. In addition, since the composition for external use of the present invention can exhibit a moisturizing action, an anti-inflammatory action, a blood circulation promoting action, and the like by a heparin-like substance, it can be used by applying it to the skin where these actions are required.

2. The present invention relates to a method for suppressing the precipitation of a terpenoid compound in an external composition containing a terpenoid compound, wherein the terpenoid compound and a heparin-like substance coexist in the external composition. To provide a method for suppressing the precipitation of a terpenoid compound.

  In the method for suppressing precipitation, the types and contents of the terpenoid compound and the heparin-like substance to be used, the types and contents of other components to be blended, the formulation of the composition for external use, and the like are described in “1. Is the same as

3. The present invention relates to a method for suppressing the formation of insoluble aggregates in an external composition containing a terpenoid compound and a heparin-like substance. Disclosed is a method for suppressing the formation of insoluble aggregates, characterized in that a terpenoid compound, a heparin-like substance, and diphenhydramine coexist in a substance.

  In the production suppression method, the terpenoid compound, the heparin-like substance, the type and content of diphenhydramine, the type and content of other components to be blended, the formulation of the composition for external use, and the like are described in “1. It is the same as the case of "thing".

  Hereinafter, the present invention will be described more specifically with reference to Examples, but the present invention is not limited thereto.

Test Example 1: Evaluation of Precipitation Inhibiting Effect of Menthol An external composition having the composition shown in Table 1 was produced, and the precipitation inhibiting effect of menthol was evaluated. The specific test method is as follows.

  First, a heparin-like substance was mixed and dissolved in purified water to prepare a first solution. Separately, 1-menthol and polyoxyethylene hydrogenated castor oil 40 preheated to 60 ° C. were added to propylene glycol and mixed to prepare a second solution. Next, the first solution and the second solution were mixed and stirred to produce a liquid external composition. In each of the obtained external compositions, l-menthol was completely dissolved.

  15 g of the obtained composition for external use was placed in a vial bottle having a diameter of 2.7 cm and a height of 5.5 cm (excluding the lid), sealed tightly, and allowed to stand at 4 ° C. for 5 hours under light-shielding conditions. Thereafter, the external appearance of the composition for external use was observed, and the state of precipitation of l-menthol was evaluated. The evaluation of the state of l-menthol precipitation was made such that the amount of l-menthol precipitate (needle-shaped crystals) observed in Comparative Example 1 was “1”, and that the l-menthol precipitate (needle-shaped crystals) was The evaluation was performed by assigning a score of "10" to the case where no test was recognized at all and dividing the score into 10 stages according to the amount of the precipitates.

  Table 1 shows the obtained results. In the composition for external use containing no heparin-like substance, a large amount of l-menthol was observed (Comparative Example 1). On the other hand, in the composition for external use containing the heparin-like substance, the precipitation of l-menthol could be effectively suppressed (Examples 1 to 9). In particular, when the heparin-like substance was contained at a ratio of 0.15 to 15 parts by weight with respect to 1 part by weight of l-menthol, the effect of suppressing precipitation of l-menthol was remarkably recognized (Examples 1 to 7). ). Furthermore, it was confirmed that even when l-menthol had a high content of 1% by weight or more, the precipitation of l-menthol could be effectively suppressed by containing a heparin-like substance (Examples 6 to 9). .

Test Example 2: Evaluation of Preventive Effect of Menthol on Precipitation and Effect of Preventing Formation of Insoluble Aggregate An external composition having the composition shown in Table 2 was produced, and the effect of suppressing the precipitation of menthol and the effect of suppressing formation of insoluble aggregates were evaluated. The specific test method is as follows.

  First, a heparin-like substance was mixed and dissolved in purified water to prepare a first solution. When diphenhydramine hydrochloride was contained, diphenhydramine hydrochloride was dissolved in the first solution. Separately, propylene glycol, l-menthol, dl-camphor or d-borneol, ethanol (95 vol%), and polyoxyethylene hydrogenated castor oil 60 preheated to 60 ° C are added and mixed. Two solutions were prepared. When diphenhydramine was contained, diphenhydramine was dissolved in the second solution. Next, the first solution and the second solution were mixed and stirred to produce a liquid external composition. In each of the obtained external compositions, l-menthol, dl-camphor and d-borneol were all dissolved.

  15 g of the obtained composition for external use was placed in a vial bottle having a diameter of 2.7 cm and a height of 5.5 cm (excluding the lid), sealed, and allowed to stand for 6 hours under a light-shielding condition of -20 ° C, and then over 11 hours The temperature was raised to 5 ° C., and left at 5 ° C. for 1 hour.

  The appearance of each composition for external use after storage under the above conditions was observed, and the state of precipitation of l-menthol was evaluated. The evaluation of the state of l-menthol precipitation was made such that the amount of the l-menthol precipitate (needle-shaped crystals) observed in Comparative Example 2 was “1”, and the l-menthol precipitate (needle-shaped crystals) was The evaluation was performed by assigning a score of "10" to the case where no test was recognized at all and dividing the score into 10 stages according to the amount of the precipitates.

Furthermore, the external appearance of each composition for external use after storage under the above conditions is visually observed, the presence or absence of insoluble aggregates (insolubilized products that look like haze) is observed, and the formation of insoluble aggregates is performed according to the following criteria. The degree was evaluated.
：: No insoluble aggregates were observed.
Δ: Insoluble aggregates were slightly observed.
X: Insoluble aggregates are clearly observed.

  Table 2 shows the obtained results. In the composition for external use containing no heparin-like substance, a large amount of l-menthol was observed (Comparative Example 2). On the other hand, in the composition for external use containing the heparin-like substance, the precipitation of monoterpene could be effectively suppressed (Examples 10 to 22).

  On the other hand, in the case of a composition for external use containing l-menthol and a heparin-like substance without containing diphenhydramine, formation of insoluble aggregates was observed (Examples 10 and 11). Since the insoluble aggregate was not observed in the composition for external use containing no heparin analog (Comparative Example 2), it is considered that the insoluble aggregate was derived from the heparin analog. On the other hand, in the topical composition containing diphenhydramine together with the monoterpene and the heparin-like substance, insoluble aggregates could be suppressed (Examples 12, 13, 15 to 19, and 21). In particular, when 1 to 10 parts by weight of diphenhydramine was contained with respect to 1 part by weight of the heparin-like substance, the formation of insoluble aggregates was significantly suppressed (Examples 12, 13, 15 to 17, 19, and 21). ). In addition, it was confirmed that the addition of diphenhydramine also improved the effect of suppressing the precipitation of l-menthol (Examples 10 and 12).

Formulation Examples Ointments having the composition shown in Table 3 (Formulation Examples 1 to 10), creams having the composition shown in Table 4 (Formulation Examples 11 to 19), gels having the composition shown in Table 5 (Formulation Examples 20 to 25), And emulsions (Formulation Examples 21 to 31) having the compositions shown in Table 6 were prepared according to a conventional method. Each of the obtained preparations was superior in the effect of suppressing the precipitation of monoterpene and the formation of insoluble aggregates under low-temperature conditions, as compared with the case where heparin-like substance and diphenhydramine were not contained.

Claims (1)

  A method for suppressing the precipitation of monoperten in an external composition containing a monoterpene, wherein a monoperten and a heparin-like substance coexist in the external composition.