JP2017178798A - Composition for external use - Google Patents

Abstract

PROBLEM TO BE SOLVED: To provide an external composition that can improve the skin moisture content and skin barrier function, and also has a good feeling in use.SOLUTION: An external composition uses γ-oryzanol and a heparin analog in combination, which can dramatically improve the skin moisture content and skin barrier function, and moreover, the external composition favorably spreads when applied on the skin and has a good feeling in use.SELECTED DRAWING: None

Description

  The present invention relates to a composition for external use that can improve skin moisture content and skin barrier function, and has an excellent feeling of use.

  Healthy and moist skin has sufficient moisture in the stratum corneum on the skin surface. However, if the secretion amount of sebum covering the skin surface decreases or the lipids between keratinocytes in the skin decrease, the water content of the stratum corneum decreases and so-called dry skin is formed. Dry skin involves various factors such as age, constitution, climate, environment, and lifestyle, and may also arise from systemic diseases such as nutritional disorders, renal failure, and myxedema.

  Conventionally, skin care products containing moisturizing ingredients have been used for the treatment of dry skin. Among the moisturizing components, γ-oryzanol is known to be useful as a component that improves dry skin diseases by activating the sebaceous glands. However, γ-oryzanol alone is not always sufficient for the treatment of dry skin, and development of a formulation technology that enhances the treatment effect is desired.

  In addition, when γ-oryzanol is contained in the composition for external use, it may be solubilized or emulsified, but once it is solubilized or emulsified and stored under low temperature conditions, the solubilized state or emulsified state cannot be maintained, There exists a tendency for the stability as a composition to fall. Conventionally, various preparation techniques for stabilizing a composition for external use containing γ-oryzanol have been studied. For example, Patent Document 1 discloses that stability is improved by combining a retinol derivative and / or a tocopherol derivative and urea together with γ-oryzanol. The formulation technique disclosed in Patent Document 1 is excellent not only in the stability of the composition containing γ-oryzanol but also in the barrier function of the skin. Development of a technique for stabilizing the composition by a method different from the formulation technique of 1 is desired.

  On the other hand, heparin-like substances are polysulfated mucopolysaccharides such as chondroitin polysulfate, which are known to have moisturizing action, anti-inflammatory action, blood circulation promoting action, etc., and have few side effects. (See, for example, Patent Document 2). However, the heparin-like substance alone is not expected to have a sufficient effect on the treatment of dry skin, and the composition for external use containing the heparin-like substance has a drawback that the spreadability when applied to the skin is poor and the feeling of use is inferior. There is. Conventionally, it has not been known at all about using a heparin-like substance in combination with γ-oryzanol, and it is not possible to analogize the effect obtained by using these in combination.

Japanese Patent Laid-Open No. 2006-23170 Japanese Examined Patent Publication No. 62-4362

  An object of the present invention is to provide a composition for external use that can improve the skin moisture content and the skin barrier function and that has an excellent feeling of use.

  The present inventor conducted intensive studies to solve the above problems and found that the skin moisture content and the skin barrier function can be drastically improved by using γ-oryzanol and a heparin-like substance in combination. It has also been found that the composition for external use has good spreadability when applied to the skin and can have an excellent feeling of use. Furthermore, even in the case where γ-oryzanol is present in a solubilized or emulsified state in the composition, it has been found that the state of the composition can be maintained under low temperature conditions, so that the properties of the composition can be stably maintained. . The present invention has been completed by further studies based on this finding.

That is, this invention provides the invention of the aspect hung up below.
Item 1. An external composition comprising γ-oryzanol and a heparin-like substance.
Item 2. Item 2. The external composition according to Item 1, wherein γ-oryzanol is solubilized.
Item 3. Item 2. The composition for external use according to Item 1, wherein γ-oryzanol is emulsified.
Item 4. Item 4. The composition for external use according to any one of Items 1 to 3, wherein the content of γ-oryzanol is 0.05% by weight or more.
Item 5. Item 5. The external composition according to any one of Items 1 to 4, wherein the heparin-like substance content is 0.1% by weight or more.
Item 6. The external composition in any one of claim | item 1 -5 used for prevention or improvement of dry skin.
Item 7. A method for stabilizing a solubilized or emulsified state of γ-oryzanol, wherein γ-oryzanol and a heparin-like substance are allowed to coexist in an external composition.

  According to the composition for external use of the present invention, it is possible to improve the skin moisture content and the skin barrier function, which is effective for preventing or improving dry skin and exhibiting an excellent skin care effect. Moreover, the composition for external use of this invention is excellent in spreadability, and its usability | use_condition is also favorable. Furthermore, the composition for external use of the present invention is excellent in low-temperature stability and can retain the solubilized or emulsified state of γ-oryzanol even when stored under low-temperature conditions. The properties of the composition can be maintained stably.

1. External Composition The external composition of the present invention is characterized by containing γ-oryzanol and a heparin-like substance. By using both of these components in combination, the skin moisture content and the skin barrier function can be dramatically improved, excellent spreadability and good usability can be provided, and further γ-oryzanol can be solubilized or Even when it is present in the composition in an emulsified state, low temperature stability can be provided. Hereinafter, the external composition of the present invention will be described in detail.

γ-Oryzanol The composition for external use of the present invention contains γ-oryzanol. γ-Oryzanol is an ester of ferulic acid and triterpene alcohol or an ester of ferulic acid and sterol.

In the composition for external use of the present invention, as γ-oryzanol, either an ester of ferulic acid and triterpene alcohol or an ester of ferulic acid and sterol may be used alone or in combination. Also good. Preferred examples of γ-oryzanol used in the present invention include those containing cycloartenyl ferulate (C ₄₀ H ₅₈ O ₄ ), more preferably those containing 95 wt% or more of cycloartenyl ferulate, particularly preferably Include those containing 98% by weight or more of cycloartenyl ferulate.

  The CAS registration number of γ-oryzanol is represented by “11042-64-1”. The γ-oryzanol used in the present invention may include oryzanol A (CAS registration number [21238-33-5]) and oryzanol C (CAS registration number [469-36-3]).

  About the (gamma)-oryzanol used by this invention, the raw material, a manufacturing method, a refinement | purification method, etc. are not specifically limited, For example, what isolated and refine | purified itself from the rice bran etc. is mentioned.

  In addition, γ-oryzanol is produced and sold by, for example, Oriza Oil Co., Ltd., Tsukino Food Industry Co., Ltd., Wako Pure Chemical Industries, Ltd., Riken Vitamin Co., Ltd., Okayasu Shoten Co., Ltd., etc. In the composition, these commercially available products can also be used as γ-oryzanol.

  The content of γ-oryzanol in the composition for external use of the present invention is not particularly limited and may be appropriately set according to the preparation form, but is, for example, 0.05% by weight or more, preferably 0.05 to 2% by weight. %, More preferably 0.1 to 1% by weight, particularly preferably 0.5 to 1% by weight.

  In the composition for external use of the present invention, the state of γ-oryzanol is not particularly limited. For example, even when γ-oryzanol is present in a solubilized or emulsified state in the composition for external use, Since the state can be maintained, the properties of the composition can be stably maintained. Therefore, in the external composition of the present invention, a preferable example of the state of γ-oryzanol includes a solubilized or emulsified state. Here, the solubilization of γ-oryzanol means that γ-oryzanol dissolves transparently and uniformly by being taken into the micelle. The emulsification of γ-oryzanol means that an oil layer containing γ-oryzanol is dispersed as droplets with a surfactant to form an emulsion.

Heparin analog The external composition of the present invention contains a heparin analog. Heparin-like substances are polysulfated mucopolysaccharides such as chondroitin polysulfate and are known drugs known to have moisturizing action, anti-inflammatory action, blood circulation promoting action, and the like.

  The origin of the heparin-like substance used in the present invention is not particularly limited. For example, it is obtained by polysulfating mucopolysaccharides, tissues of edible animals (for example, tracheal cartilage such as cattle and pigs) And the like extracted from the lung including In the emulsified composition of the present invention, as the heparin-like substance, a heparin-like substance included in the Japanese Pharmacopoeia pharmaceutical standards is preferably used.

  The content of the heparin-like substance in the composition for external use of the present invention may be appropriately set according to the dosage form, for example, 0.1% by weight or more, preferably 0.1 to 1% by weight, more preferably Is 0.3 to 1% by weight.

  Further, in the composition for external use of the present invention, the ratio of the heparin-like substance to γ-oryzanol is not particularly limited, but skin moisture content, skin barrier function, feeling of use, and solubilization of γ-oryzanol under low temperature conditions From the viewpoint of further improving the stability of the state or emulsified state, 0.1 to 20 parts by weight, preferably 0.1 to 10 parts by weight, more preferably 0, of heparin-like substance per 1 part by weight of γ-oryzanol. 0.1 to 8 parts by weight, particularly preferably 0.1 to 5 parts by weight.

In the external composition of the water present invention, in the case of solubilizing or emulsifying γ- oryzanol, as the solvent, it preferably contains water.

  When water is contained in the composition for external use of the present invention, the content is not particularly limited, and for example, 30% by weight or more can be mentioned. Usually, the higher the water content, the more difficult it is to maintain the solubilized or emulsified state of γ-oryzanol by storage under low temperature conditions. However, in the composition for external use of the present invention, the water content is low. At most, the state can be kept stable. In view of the effects of the present invention, the water content in the external composition of the present invention is preferably 40 to 99.5% by weight, more preferably 50 to 99% by weight, and particularly preferably 60 to 95% by weight. It is done.

Surfactant In addition, the external composition of the present invention preferably contains a surfactant in order to solubilize or emulsify γ-oryzanol into a desired formulation. The surfactant is not particularly limited as long as it is pharmaceutically acceptable, and any of a nonionic surfactant, an anionic surfactant, a cationic surfactant, and an amphoteric surfactant can be used. A nonionic surfactant is preferably used.

  Specific examples of the surfactant include POE (10-50 mol) phytosterol ether, POE (10-50 mol) dihydrocholesterol ether, POE (10-50 mol) 2-octyldodecyl ether, POE (10-50 mol). Mol) decyltetradecyl ether, POE (10-50 mol) oleyl ether, POE (2-50 mol) cetyl ether, POE (5-50 mol) behenyl ether, POE (5-30 mol) polyoxypropylene (5-5 mol) 30 mol) Polyoxyethylene alkyl ethers such as 2-decyltetradecyl ether, POE (10 to 50 mol) polyoxypropylene (2 to 30 mol) cetyl ether, phosphoric acid / phosphate thereof (POE cetyl ether phosphoric acid) Sodium), POE (20-60 mol) sol Tan monooleate, POE (10-60 mol) sorbitan monoisostearate, POE (10-80 mol) glyceryl monoisostearate, POE (10-30 mol) glyceryl monostearate, POE (20-100 mol) Polyoxypropylene modified silicone, POE / alkyl modified silicone, polyethylene glycol monolaurate, polyethylene glycol monopalmitate, polyethylene glycol monostearate, polyethylene glycol dilaurate, polyethylene glycol dipalmitate, polyethylene glycol distearate, polyethylene glycol dioleate, Polyglycol diricinoleate, polyoxyethylene hydrogenated castor oil (5-100), polysorbate (20-85), grease Phosphorus fatty acid ester (glyceryl monostearate etc.), hydrogenated soybean phospholipid, hydrogenated lanolin alcohol. These surfactants may be used individually by 1 type, and may be used in combination of 2 or more type.

  When the surfactant is included in the external composition of the present invention, the content thereof may be appropriately set according to the formulation form and the like, for example, 0.1 to 30% by weight. More specifically, when the external composition of the present invention is a cream, the surfactant content is 0.1 to 15% by weight, preferably 0.5 to 10% by weight. Moreover, when the external composition of this invention is a liquid agent, 0.1-30 weight% is mentioned as content of surfactant, Preferably 0.5-15 weight% is mentioned.

Oily Base The composition for external use of the present invention may contain an oily base as necessary for preparation into a desired preparation form. The oily base is not particularly limited as long as it is pharmaceutically acceptable, and examples include vegetable oil, animal oil, mineral oil, fatty acid alkyl ester, fatty acid, higher alcohol, silicone oil and the like.

  Examples of oily bases include olive oil, wheat germ oil, rice oil, safflower oil, soybean oil, camellia oil, corn oil, rapeseed oil, sesame oil, castor oil, sunflower oil, cottonseed oil, peanut oil, jojoba oil, hydrogenated Oil, avocado oil, fennel oil, clove oil, peppermint oil, eucalyptus oil, lemon oil, orange oil, carnauba wax, candelilla wax, rice bran wax, tree wax, etc .; animal oils such as lard, fish oil, squalane, beeswax; paraffin, Mineral oils such as hydrogenated polyisobutene, liquid paraffin, gelled hydrocarbon (plasty base, etc.), petrolatum, etc .; carbon number 4 such as diisopropyl adipate, isopropyl myristate, isopropyl palmitate, cetyl palmitate, diethyl sebacate, ethyl oleate ~ 30 fatty acids and C1-C34 alcohols Esters: fatty acids having 4 to 30 carbon atoms such as lauric acid, myristic acid, palmitic acid, sebacic acid, oleic acid, linoleic acid; myristyl alcohol, cetyl alcohol, oleyl alcohol, stearyl alcohol, isostearyl alcohol, behenyl alcohol, hexadecyl alcohol Monohydric higher alcohols having 6 to 34 carbon atoms such as lanolin alcohol; chilled polysiloxane, crosslinked methylpolysiloxane, cyclic silicone, alkyl-modified silicone, amino-modified silicone, polyether-modified silicone, polyglycerin-modified silicone, acrylic silicone, Examples include silicone oils such as phenyl-modified silicone. These oily bases may be used alone or in combination of two or more.

  When the oily base is contained in the composition for external use of the present invention, the content may be appropriately set according to the formulation form and the like. More specifically, when the composition for external use of the present invention is a cream, the content of the oily base is 0.1 to 60% by weight, preferably 1 to 40% by weight. Moreover, if the composition for external use of this invention is a liquid agent, 0.05-30 weight% as content of an oil-based base, Preferably 0.1-15 weight% is mentioned.

Polyhydric alcohol Furthermore, the composition for external use of the present invention may contain a polyhydric alcohol as necessary for improving the moisture retention.

  The polyhydric alcohol is not particularly limited as long as it is pharmaceutically acceptable. For example, ethylene glycol, 1,3-butylene glycol, propylene glycol, isoprene glycol, diethylene glycol, dipropylene glycol, polypropylene glycol, glycerin, etc. Is mentioned. These polyhydric alcohols may be used individually by 1 type, and may be used in combination of 2 or more type.

  When polyhydric alcohol is contained in the composition for external use of the present invention, the content may be appropriately set according to the formulation form and the like, for example, 0.05 to 30% by weight. More specifically, when the composition for external use of the present invention is a cream, the content of the polyhydric alcohol is 0.05 to 20% by weight, preferably 0.1 to 15% by weight. Moreover, if the composition for external use of this invention is a liquid agent, 0.05-30 weight% is mentioned as content of a polyhydric alcohol, Preferably 0.1-20 weight% is mentioned.

Other Components Further, the external composition of the present invention may contain a base material and additives other than the above-described components as necessary in order to obtain a desired formulation form. Such bases and additives are not particularly limited as long as they are pharmaceutically acceptable, but include, for example, cooling agents (menthol, camphor, borneol, mint water, mint oil, etc.), preservatives (methylparaben). , Propylparaben, benzoic acid, sodium benzoate, sorbic acid, etc.), flavoring agents (citral, 1,8-shionale, citronellal, farnesol, etc.), coloring agents (tar pigments (brown 201, blue 201, yellow 4) No., Yellow No. 403, etc.), cacao pigment, chlorophyll, aluminum oxide, etc.), thickener (polyvinylpyrrolidone, sodium alginate, ethyl cellulose, hydroxypropylmethylcellulose, sodium carboxymethylcellulose, xanthan gum, carrageenan, etc.), pH adjuster (phosphoric acid) , Hydrochloric acid, citric acid Sodium citrate, succinic acid, tartaric acid, sodium hydroxide, potassium hydroxide, triethanolamine, triisopropanolamine, etc.), wetting agent (sodium dl-pyrrolidonecarboxylate, D-sorbitol, macrogol, etc.), stabilization Agents (dibutylhydroxytoluene, butylhydroxyanisole, sodium edetate, sodium metaphosphate, L-arginine, L-aspartic acid, DL-alanine, glycine, sodium erythorbate, propyl gallate, sodium sulfite, sulfur dioxide, chlorogenic acid, Catechin, rosemary extract, etc.), antioxidants, ultraviolet absorbers, chelating agents, adhesives, buffers, solubilizers, solubilizers, preservatives and the like. These additives may be used individually by 1 type, and may be used in combination of 2 or more type. The content of these additives can be appropriately set according to the formulation form and the like.

  Furthermore, the composition for external use of the present invention may contain a pharmacological component other than γ-oryzanol and a heparin-like substance, if necessary, in addition to the components described above. Such pharmacological components include, for example, antihistamines (chlorpheniramine maleate, etc.), local anesthetics (procaine, tetracaine, bupipacaine, mepipacaine, chloroprocaine, proparacaine, meprilucaine or salts thereof, orthocaine, oxesasein, oxy Polyentoxydecane, funnel extract, percamine ase, tesit decite, etc.), anti-inflammatory agents (indomethacin, felbinac, diclofenac sodium, loxoprofen sodium, etc.), skin protectants (collodion, castor oil, etc.), blood circulation promoting ingredients (nonyl acid vanillylamide, nicotinic acid) Benzyl esters, capsaicin, pepper extract, etc.), refreshing agents (menthol, camphor, etc.), mucopolysaccharides (sodium chondroitin sulfate, glucosamine, etc.) It is below. These pharmacological components may be used alone or in combination of two or more. When these pharmacological components are contained, the content may be appropriately set according to the type of pharmacological component to be used, the expected effect, and the like.

Formulation Form / Usage Mode The composition for external use of the present invention is used as a preparation to be applied transdermally (external medicine, cosmetics, etc.), and particularly preferably used as an external medicine.

  The preparation form of the composition for external use of the present invention is not particularly limited as long as it can be applied transdermally. For example, liquid preparations (including lotions, sprays, aerosols, and emulsions), water-soluble ointments Agents, oily ointments, creams, foams, gels, patches and the like. Among these, Preferably, a liquid agent and a cream agent are mentioned.

  For preparation of these preparation forms, in accordance with a known method described in the 16th revised Japanese Pharmacopoeia General Rules for Preparation, etc., γ-oryzanol is solubilized or emulsified using additives according to the preparation form. Can be done. For example, in the case of a cream, an oil phase containing γ-oryzanol, an oily base, a surfactant, and other oily ingredients that are optionally added, a heparin-like substance, water, and if necessary It is manufactured by preparing an aqueous phase containing other water-soluble components to be added, and mixing and emulsifying these.

  The composition for external use of the invention can drastically improve the skin moisture content and the skin barrier function by the action of γ-oryzanol and heparin-like substances, and therefore can be used for the prevention or improvement of dry skin. Furthermore, the composition for external use of the invention can also be used for the prevention or treatment of diseases in which dry skin has deteriorated or skin diseases that can be caused by dry skin. Examples of such skin diseases include dry skin diseases (eg, sebum deficiency, sebum deficiency eczema, atopic dermatitis, progressive palmokeratoderma, foot keratoderma, childhood dry eczema), Examples include pore lichen, dry skin, pruritus, ichthyosis, shark skin, keratoses of elbows, knees, heels, and ankles, fingers, limbs / cracks, and childhood dry skin.

2. TECHNICAL FIELD The present invention relates to a method for stabilizing a solubilized or emulsified state of γ-oryzanol in an external composition containing γ-oryzanol, wherein The method for stabilizing the solubilized or emulsified state of γ-oryzanol is characterized by coexisting γ-oryzanol and a heparin-like substance.

  In the stabilization method, γ-oryzanol, heparin-like substances, their contents, their ratios, types and contents of other ingredients to be blended, formulation forms of external compositions, etc. are described in “1. The same as in the case of the “composition”.

  EXAMPLES The present invention will be described more specifically with reference to the following examples, but the present invention is not limited to these examples.

Test Example 1: Evaluation of skin moisture content, skin barrier function and usability (extensibility)
1. Preparation of emulsion composition (cream agent) An emulsion composition (cream agent) having the composition shown in Table 1 was prepared. Specifically, each component of the aqueous phase shown in Table 1 was mixed, heated to 80 ° C., and stirred uniformly to prepare an aqueous phase. Separately, each component of the oil phase shown in Table 1 was heated to 80 ° C. and stirred uniformly to prepare an oil phase. In the preparation of the oil layer, polyoxyethylene (20) cetyl ether and polyoxyethylene (5) behenyl ether were preliminarily heated to 80 ° C. and mixed with other components. Next, the obtained water phase and oil phase were mixed and heated in the state heated to 80 ° C. to effect emulsification, and cooled to obtain an emulsified composition (cream agent).

2. Evaluation of Skin Moisture Content and Skin Barrier Function Each of the obtained emulsified compositions (0.3 g) was applied three times a day (morning, noon, evening) to the back of the hands of six subjects with dry skin. Skin water content and skin barrier function (transepidermal water transpiration; TEWL) were measured before application (initial stage) and 2 weeks after the start of application.

  The skin moisture content was measured using a skin surface horn layer moisture content measuring device SKICON-200EX (manufactured by IBI S Co., Ltd.), and the application part of the emulsion composition was measured 10 times. The average value of the skin surface horny layer moisture content was calculated, and according to the following formula, the skin moisture content increase rate (%) was calculated, and the 6 obtained “skin moisture content increase rate (%)” were averaged. The result of rounding off the first decimal place was taken as the evaluation result.

  Moreover, transepidermal water transpiration (TEWL) measured the application part of the emulsion composition 5 times using TEWL measuring apparatus VAPO SCAN AS-VT100RS (made by Asahi Technolab Co., Ltd.). The average value of transepidermal water transpiration was calculated, and the recovery rate (%) of the skin barrier function was calculated according to the following formula. The obtained 6 “skin barrier function recovery rate (%)” was averaged, and rounded off to the first decimal place. In addition, since the amount of transepidermal water transpiration becomes smaller as the skin barrier function is higher and the ability to retain skin moisture is larger, the amount of transepidermal water transpiration is used as an index of the skin barrier function.

3. Evaluation of Usability (Extendability) 0.1 g of each emulsified composition obtained was spread on the back of the subject's hand, and the extensibility at that time was evaluated. Specifically, the spreadability is evaluated based on the ease of spreading when water (good spreadability control) is spread on the back of the hand as “1”, and the JP Macrogol Ointment (poor spreadability control). The ease of spreading when spreading on the back of the hand was set to “10”, and the space between them was divided into 10 levels according to the ease of spreading and scored. The obtained 6 “scores” were averaged, and the result of rounding to the first decimal place was taken as the evaluation result.

4). The results obtained are shown in Table 1. The increase in skin moisture was 205% for heparin-like substance alone (Comparative Example 1) and 31% for γ-oryzanol alone (Comparative Example 2), but 347 when these were used together (Example 1). It was revealed that the skin water content was improved by the synergistic action of the heparin analog and γ-oryzanol. Further, the recovery rate of the skin barrier function was 41% for the heparin-like substance alone (Comparative Example 1) and 8% for γ-oryzanol alone (Comparative Example 2), but when these were used in combination (Example 1). ) Was 61%, and it was confirmed that the skin barrier function was improved by the synergistic action of the heparin analog and γ-oryzanol. Furthermore, it is clear that the feeling of use (extensibility) is better when heparin-like substance and γ-oryzanol are used together (Example 1) than when these are used alone (Comparative Examples 1 and 2). It became.

Test Example 2: Evaluation of low-temperature stability
1. Preparation of Solution A solution having the composition shown in Table 2 was prepared. Specifically, first, a phase A in which a heparin-like substance and water were mixed and dissolved was prepared. Separately, γ-oryzanol is dissolved in sebacic acid diester, and polyoxyethylene (50) hydrogenated castor oil previously heated and dissolved at 60 ° C. is added and stirred to uniformly mix B phase. Got ready. Subsequently, A phase and B phase were heated and mixed at 80 degreeC, and after stirring uniformly, the liquid agent was prepared by cooling to room temperature. Among the obtained liquid agents, Examples 2 to 10, and Comparative Examples 3 to 5 and Reference Example 1 are all in a state where γ-oryzanol is solubilized, and Comparative Example 6 is in a cloudy state. there were.

2. Evaluation of stability under low temperature conditions 25 g of each solubilized solution thus obtained was filled in a vial (inner diameter: 35 mm, height: 78 mm), and the sample was covered. Each specimen is placed in a thermostat whose temperature can be controlled in the range of −20 ° C. to 5 ° C., (i) left at −20 ° C. for 11 hours, (ii) raised to 5 ° C. over 1 hour, (iii) 5 A total of 5 cycles of low-temperature load tests were conducted with the temperature being left at 11 ° C. for 11 hours, and (iv) the temperature was lowered to −20 ° C. over 1 hour.

  Then, after returning the temperature of each specimen to room temperature, the appearance was observed and the solubilized state of γ-oryzanol was evaluated. Specifically, the solubilized state was evaluated by setting the transparent state as “1” and the white turbid state of the liquid preparation of Comparative Example 6 containing no heparin-like substance (control of the cloudy state) as “10”. Was scored by dividing it into 10 stages according to the degree of cloudiness.

  The obtained results are shown in Table 2. As a result, in the case of γ-oryzanol alone (Comparative Examples 3 to 5), white turbidity due to destabilization of the solubilized state of γ-oryzanol was observed after the low temperature load test, but γ-oryzanol and heparin were observed. In the case of containing a similar substance (Examples 2 to 10), the solubilized state of γ-oryzanol was maintained and a transparent state could be maintained. On the contrary, in Examples 2 to 10, the solubilized state was even better after the low temperature load test.

Formulation Example External composition (O / W emulsion type cream) having the composition shown in Table 3, External composition (W / O emulsion type cream) having the composition shown in Table 4, and External composition having the composition shown in Table 5 ( (Emulsion), an external composition (gel agent) having the composition shown in Table 6 was prepared. When the obtained compositions for external use were evaluated in the same manner as described above, the skin moisture content and the skin barrier function were better than those of Comparative Examples 1 and 2, and γ-oryzanol was allowed to exist in a solubilized or emulsified state. In this case, the preparation stability under low temperature conditions was excellent.

Claims (7)

  An external composition comprising γ-oryzanol and a heparin-like substance.   The composition for external use according to claim 1, wherein γ-oryzanol is solubilized.   The external composition according to claim 1, wherein γ-oryzanol is emulsified.   The external composition in any one of Claims 1-3 whose content of (gamma)-oryzanol is 0.05 weight% or more.   The composition for external use in any one of Claims 1-4 whose content of a heparin analog is 0.1 weight% or more.   The external composition in any one of Claims 1-5 used for prevention or improvement of dry skin.   A method for stabilizing a solubilized or emulsified state of γ-oryzanol, wherein γ-oryzanol and a heparin-like substance are allowed to coexist in an external composition.