JP6300436B2 - Testosterone-5α-reductase inhibitor - Google Patents

Description

  The present invention relates to a testosterone-5α-reductase inhibitor, a hair restorer, a prostatic hypertrophy inhibitor, an anti-acne agent, and a hair growth method.

  As one of the causes of male pattern hair loss, it is known that male hormones accumulate in large amounts in the metabolic system and increase the male hormone action. It is believed that testosterone is reduced to dihydrotestosterone (DHT) by 5α-reductase, and the hair growth period is shortened by the action of the reduced dihydrotestosterone. Therefore, it is considered that male pattern baldness caused by increased male hormone action can be prevented or reduced by inhibiting the reduction of testosterone to dihydrotestosterone, i.e., inhibiting testosterone-5α-reductase (Non-Patent Document). 1).

  In addition, it has been established that DHT is a major cause of prostatic hypertrophy, and it is known that 5α-reductase inhibitors are effective in treating prostatic hypertrophy (Non-patent Document 2).

  It is also known that sebum secretion ability increases due to increased production of DHT, and seborrheic hair loss and acne (acne vulgaris) develop.By inhibiting DHT production, seborrheic hair loss and It is thought that acne can be prevented or reduced.

Propolis is a glue-like substance made by mixing sap of trees collected by bees, plant shoots and exudates with beeswax, etc., and has antibacterial, antioxidant, anti-inflammatory, anti-tumor and anti-tumor effects. Allergic effects are known (Patent Documents 1 to 5).

  Since the components of propolis are affected by the type and mixing ratio of the source plant that is used as the material, it is known that the types and contents of active ingredients contained in propolis and their physiological activities are completely different depending on the country or region where they are collected. It has been.

  In recent years, research on the content of propolis by production area has been promoted. For example, cinnamic acid derivatives such as p-coumaric acid, artepilin C, dolpanin, and baccaline are detected as the main component of Brazilian propolis whose main plant is Baccaris dracuncrifolia. On the other hand, flavonoids such as chrysin and galangin are detected as main components of Chinese, European and Australian propolis originating from poplar. Thus, since the main components are different, Brazilian propolis can be classified into those having cinnamic acid derivatives as the main components, and Chinese propolis and the like can be classified into those having flavonoids as the main components.

  Patent Document 6 reports that an extract obtained by mixing a propolis from China and Brazil with a hydrophilic solvent or water has a strong inhibitory action on testosterone-5α-reductase.

  In addition, benzophenones such as nemorosone, guttiferone E, xanthochymol, etc., which do not belong to any of the aforementioned cinnamic acid derivatives and flavonoids as the main component, are the main components. Propolis is also confirmed. Examples of the propolis include Cuban, Panama, Venezuela, and Florida propolis. In Non-Patent Document 3, Clusia rosea (Copey tree) flower resin widely distributed in Cuba is a rich source of polyisoprenylated benzophenone, and Cuban propolis is the most abundant polyisoprenylated nemoloson. It is reported that it is contained as benzophenone, and nemoloson has effects such as antioxidant activity (Non-Patent Document 3), antibacterial activity (Non-Patent Document 4), and activation of endoplasmic reticulum stress response (Non-Patent Document 5). It has also been reported.

JP 2002-308830 A Japanese Unexamined Patent Publication No. 9-143179 JP 2004-159563 A JP-A-8-228701 JP 2008-214235 A JP 2000-53539 A

AL. Dallob et al., The Effect of Finasteride, a 5α-Reductase Inhibitor, on Scalp Skin Testosterone and Dihydrotestosterone Concentrations in Patients with Male Pattern Baldness.J Clin Endocrinol Metab, 79, 703-706 (1994) S. Tu-Yue et al., A Novel In Vitro Model to Screen Steroid 5α-Reductase Inhibitors Against Benign Prostatic Hyperplasia. Meth Find Exp Clin Pharmacol, 20 (4), 283-287 (1998) O. Cuesta-Rubio et al., Polyisoprenylated Benzophenones in Cuban Propolis; Biological Activity of Nemorosone. Z Naturforsch. 57e, 372-378 (2002) L. Monzote et al., Antimicrobial evaluation of the polyisoprenylated benzophenones nemorosone and guttiferone A. Phytother Res, 25 (3), 458-462 (2011) F. Holtrup et al., Microarray analysis of nemorosone-induced cytotoxic effects on pancreatic cancer cells reveals activation of the unfolded protein response (UPR). Br J Pharmacol, 162 (5), 1045-1059 (2011)

  The present invention provides a testosterone-5α-reductase inhibitor, a hair restorer, a prostatic hypertrophy inhibitor, an anti-acne agent, and a safe, natural product-derived substance, which are safe and have a substance derived from a natural product as an active ingredient. It aims at providing the hair-growth method by.

  Regarding propolis, the main component of which is benzophenone, there has been no known effect on prevention or reduction of male pattern baldness such as testosterone-5α-reductase inhibitory activity. The Brazilian propolis and Chinese propolis, which are known to have testosterone-5α-reductase inhibitory action, do not contain nemoloson.

  The present inventors have now found that propolis whose main component is benzophenones (Cuban propolis) has testosterone-5α-reductase inhibitory activity. Further, focusing on the testosterone-5α-reductase inhibitory action of propolis whose main component is benzophenones, the active ingredient was searched for and found that nemoloson has a strong physiological action.

  The present invention has been completed based on these findings and has been completed. The present invention provides the following testosterone-5α-reductase inhibitors, hair restorers, prostate hypertrophy inhibitors, anti-acne agents, and the like.

(I) Testosterone-5α-reductase inhibitor
(I-1) A testosterone-5α-reductase inhibitor comprising a benzophenone or a salt thereof as an active ingredient.
(I-2) The testosterone-5α-reductase inhibitor according to (I-1), wherein the benzophenones are nemoloson, isomers or derivatives thereof.
(I-3) The testosterone-5α-reductase inhibitor according to (I-2), comprising as an active ingredient a propolis containing nemoloson, an isomer or derivative thereof, or an extract thereof.
(I-4) The testosterone-5α-reductase inhibitor according to (I-3), wherein the propolis is a Cuban propolis.
(I-5) Plants belonging to Crucia Rosea, Crucia Grandiflora, Crucia Hilaryana, Crucia Insignis, Crucia Renguerios or Crucia Nemorosa or extracts thereof, or active ingredients thereof, as described in (I-2) Testosterone-5α-reductase inhibitor.

(II) Hair restorer
(II-1) A hair restorer comprising as an active ingredient the testosterone-5α-reductase inhibitor according to any one of (I-1) to (I-5).
(II-2) The hair restorer according to (II-1), which is an external preparation for hair growth.
(II-3) The hair restorer according to (II-1), which is an oral agent for hair growth.
(II-4) A cosmetic for hair containing the testosterone-5α-reductase inhibitor according to any one of (I-1) to (I-5) or the hair restorer according to (II-1).

(III) Hair growth method
(III-1) A hair growth method characterized by orally ingesting a benzophenone or a salt thereof (excluding medical practice for humans).
(III-2) The hair growth method according to (III-1), wherein the benzophenones are nemoloson, isomers or derivatives thereof.
(III-3) The hair-growth method according to (III-2), characterized by orally ingesting propolis containing nemoloson, an isomer or derivative thereof, or an extract thereof.
(III-4) The hair growth method according to (III-3), wherein the propolis is a Cuban propolis.
(III-5) It is characterized by orally ingesting a plant belonging to Crucia Rosea, Crucia Grandiflora, Crucia Hilariana, Crucia Insignis, Crucia Renguerios or Crucia Nemorosa or an extract thereof (III The hair-growth method as described in -2).

(IV) Prostatic hypertrophy inhibitor
(IV-1) A prostatic hypertrophy inhibitor comprising the testosterone-5α-reductase inhibitor according to any one of (I-1) to (I-5) as an active ingredient.
(IV-2) The prostatic hypertrophy inhibitor according to (IV-1), which is an oral preparation for suppressing prostatic hypertrophy.

(V) Anti-acne agent
(V-1) An anti-acne agent comprising the testosterone-5α-reductase inhibitor according to any one of (I-1) to (I-5) as an active ingredient.
(V-2) The anti-acne agent according to (V-1), which is an anti-acne external preparation.
(V-3) The anti-acne agent according to (V-1), which is an oral anti-acne agent.
(V-4) A skin cosmetic comprising the testosterone-5α-reductase inhibitor according to any one of (I-1) to (I-5) or the anti-acne agent according to (V-1).

  Propolis containing nemoloson, its isomers or its derivatives has excellent testosterone-5α-reductase inhibitory activity, so it is expected to have hair loss prevention, hair growth and hair growth action, prostate hypertrophy suppression action, and acne prevention or treatment effect Is done.

  Therefore, propolis containing nemoloson, its isomers or derivatives thereof is useful as an active ingredient for testosterone-5α-reductase inhibitors, hair restorers, prostate hypertrophy inhibitors, and anti-acne agents, and for hair or skin. It is useful as a component of cosmetics. In addition, propolis containing nemoloson, its isomers or derivatives thereof is particularly useful as a component of health foods, supplements and the like that are taken orally.

  Since the inhibitory effect of testosterone-5α-reductase is observed for propolis containing nemoloson, its isomers or derivatives thereof, nemoloson (benzophenones) itself, nemoloson, isomers or derivatives thereof, Kurusia genus Is useful as an active ingredient of a testosterone-5α-reductase inhibitor, a hair restorer, a prostatic hypertrophy inhibitor, and an anti-acne agent, and is also useful as an ingredient for cosmetics for hair or skin. In addition, benzophenones and plants belonging to the genus Kursia are particularly useful as components of health foods and supplements that are taken orally.

  Moreover, since propolis containing nemoloson, its isomer or its derivative has been conventionally used as a food material, it is highly safe.

  Hereinafter, the present invention will be described in detail.

(1) Benzophenones In the present invention, the benzophenones are preferably isoprenylated benzophenones. Examples of the isoprenylated benzophenones include garcinol, isogarcinol, xanthochymol, isoxanthochymol, gucciferon E, and plukenethion A. , Mucronulatol, Garcinielliptone I, Hyperibone B, Propolone A, Propolone B, Propolone C, Propolone D, Examples include Clusianone and Grandone. As the isoprenylated benzophenones, nemoloson, its isomer (preferably a stereoisomer), or a derivative thereof is particularly preferable. Derivatives of nemoloson include, for example, methyl nemoloson II (O-methyl nemorosone II) and hydroxynemoloson (Hidroxy-nemorosone), and isomers of nemoloson include, for example, nemoloson II (nemorosone II), 7-epinemoloson. (7-epi-nemorosone).

  Here, nemoloson is a kind of isoprenylated benzophenones, and its structural formula is described in I Herna'ndez et al., Polyprenylated Benzophenone Derivatives from Cuban Propolis. J Nat Prod, 68, 931-934 (2005). Yes.

  Nemoloson is (1S) -1α-benzoyl-3,5α, 7β-triprenyl-4-hydroxy-8,8-dimethylbicyclo [3.3.1] non-3-ene-2,9-dione ((1S ) -1α-Benzoyl-3,5α, 7β-triprenyl-4-hydroxy-8,8-dimethylbicyclo [3.3.1] nona-3-ene-2,9-dione) Then, it is described as “nemoloson”.

  In the present invention, as the benzophenones or salts thereof, any of those not in an isolated or purified state (crude extract) and those isolated or purified can be used.

  Benzophenones can be used regardless of whether they are self-prepared products or commercially available products. Here, the method for self-preparing benzophenones is not particularly limited, and examples thereof include a method for extraction from plants and natural products containing benzophenones, and a method for chemical synthesis.

  Although it does not restrict | limit especially as a natural product and a plant containing benzophenone, For example, the propolis containing nemoloson, its isomer, or its derivative (s) and its origin plant are mentioned. Examples of propolis containing nemoloson, its isomers or derivatives thereof include, for example, propolis produced in Cuba, Panama, Venezuela, Florida and the like, and Cuban propolis is particularly preferable.

  The method for extracting benzophenones from propolis is not particularly limited. Propolis as a raw material is usually a propolis bulk or an alcohol-washed propolis bulk. These raw propolis ingots may be used as they are, but it is preferable to use a propolis that has been cut or pulverized to an appropriate size because the extraction efficiency is improved.

The solvent for obtaining the propolis extract is not particularly limited as long as benzophenones can be extracted. For example, water, CO ₂ , lower alcohol such as methanol, ethanol, n-propanol, isopropanol, n-butanol, ethyl acetate, etc. Esters, ketones such as acetone and methyl ethyl ketone, halogenated hydrocarbons such as methylene chloride and chloroform, aromatic hydrocarbons such as toluene and xylene, ethers such as tetrahydrofuran, diethyl ether and diisopropyl ether, ethylene glycol and propylene glycol And glycols such as glyme and diglyme, cellosolves such as methyl cellosolve and ethyl cellosolve, DMF, DMSO and the like.

  The extraction time is not particularly limited, and can be appropriately set depending on the form of propolis used as a raw material, the type and amount of a solvent used for extraction, the temperature at the time of extraction, stirring conditions, and the like. After completion of the extraction operation, the solid matter can be removed from the extraction mixture by a normal method, for example, filtration, and further, if necessary, a propolis solvent extraction fraction can be obtained by centrifugation or the like.

  The propolis solvent extract fraction thus obtained can be used as it is as an active ingredient of the present invention, but the form of the concentrate obtained by concentrating the extract fraction by a conventional method or the concentrate is sprayed. It can also be used in the form of a powder obtained by drying and freeze-drying. The propolis extract can be further purified by solvent extraction, column chromatography, recrystallization, liquid chromatography and the like.

  Examples of plants containing nemoloson, isomers or derivatives thereof include, for example, plants belonging to the genus Kursia, and plants belonging to the genus Kursia include Clusia rosea, Clusia grandiflora (Clusia grandiflora) , Plants belonging to Clusia hilariana, Clusia insignis, Clusia renggerioides, Clusia nemorosa and the like. The plant part to be used is not particularly limited as long as it contains a lot of nemoloson, its isomers or derivatives thereof, such as fruits (or seeds), flowers and leaves.

  When extracting benzophenone from a plant here, the method in particular is not restrict | limited, The method of extracting using the method of extracting using a polar solvent and the supercritical extraction method by a carbon dioxide etc. is mentioned. When extracting with a polar solvent, examples of the extraction solvent to be used include water, lower alcohols (methanol, ethanol, n-propanol, isopropanol, etc.), ketones (acetone, methyl ethyl ketone, methyl butyl ketone, etc.), esters (acetic acid, etc.). Methyl, ethyl acetate, etc.), glycols (ethylene glycol, propylene glycol), glycerin, tetrahydrofuran, acetonitrile, acetic acid, propionic acid, acetamide, dimethylformamide, dimethyl sulfoxide and the like.

  These extraction solvents can be used alone or in a combination of two or more. Preferably, water, lower alcohol (preferably ethanol) or a mixture thereof (hydrous alcohol, preferably hydrous ethanol). In the case where a hydrous alcohol (preferably hydrous ethanol) is used as the extraction solvent, the alcohol concentration is not limited, but preferably 20 to 99.9% by volume, particularly 50 to 99.9% by volume.

  Extraction is carried out by adding a part or all of the above plant to the solvent, extracting at 0 ° C. to the temperature at which the solvent boils, usually at a temperature of 100 ° C. or less, standing for 30 minutes to 3 days, soaking or soaking, and then insoluble. This can be done easily by removing the object. The solvent extract thus obtained is preferably further subjected to a process for isolating and purifying benzophenones. Such isolation and purification treatment can be performed by combining one or more conventional methods. Examples of such treatment include a precipitation method, a liquid-liquid countercurrent distribution method, an adsorption treatment with activated carbon, a resin, etc., a purification treatment with column chromatography, ion exchange chromatography, and the like.

  In the present invention, as benzophenones, natural products containing benzophenones and plants themselves may be used. For example, propolis containing nemoloson, its isomers or derivatives thereof, or plants belonging to the genus Kursia are active ingredients. May be used as

  Benzophenones may be used in a free state or in a salt state. Examples of the salt include a salt with an inorganic base such as sodium, potassium, magnesium, calcium, and aluminum; a salt with an organic base such as methylamine, ethylamine, and ethanolamine; and a basic amino acid such as lysine, ornithine, and arginine. Salts and ammonium salts. The salt may be an acid addition salt. Specific examples of the salt include hydrochloric acid, hydrobromic acid, hydroiodic acid, sulfuric acid, nitric acid, phosphoric acid and other mineral acids; formic acid, acetic acid, Organic acids such as propionic acid, oxalic acid, malonic acid, succinic acid, fumaric acid, maleic acid, lactic acid, malic acid, tartaric acid, citric acid, methanesulfonic acid, ethanesulfonic acid; and acidic amino acids such as aspartic acid, glutamic acid Examples include acid addition salts. Benzophenones also include hydrates, solvates and crystal polymorphs.

(2) Testosterone-5α-reductase inhibitor The testosterone-5α-reductase inhibitor of the present invention is characterized by containing a benzophenone or a salt thereof as an active ingredient.

  The testosterone-5α-reductase inhibitor of the present invention may contain additional components as long as the testosterone-5α-reductase inhibitory action of benzophenones is not hindered. Examples of the ratio of benzophenones or salts thereof in the testosterone-5α-reductase inhibitor when such additional components are included include 0.01 to 98% by weight.

  The testosterone-5α-reductase inhibitor of the present invention is not particularly limited in its form, and has, for example, a pharmaceutical form such as powder, granule, tablet, capsule, liquid, suspension, and emulsion. It may be.

  The testosterone-5α-reductase inhibitor of the present invention has an action of inhibiting the reduction of testosterone to dihydrotestosterone by 5α-reductase, so that it is used as an active ingredient in hair restorers, prostate hypertrophy inhibitors and anti-acne agents, and for hair It can be suitably used as a component of cosmetics and skin cosmetics.

  The testosterone-5α-reductase inhibitor of the present invention is a food or drink intended for health, health maintenance, promotion, etc., for example, health food, functional food, dietary supplement, supplement, food for specified health use, or functional nutrition food. The meaning is also included. In addition, the testosterone-5α-reductase inhibitor of the present invention includes the meaning of an additive that imparts a testosterone-5α-reductase inhibitory effect.

  For the above foods, excipients, brighteners, minerals, vitamins, flavonoids, quinones, polyphenols, amino acids, nucleic acids, essential fatty acids, refreshing agents, binders, sweeteners, disintegration as necessary Agents, lubricants, colorants, fragrances, stabilizers, preservatives, sustained release regulators, surfactants, solubilizers, wetting agents and the like can be blended.

  The dosage unit form for use as a supplement is not particularly limited and may be appropriately selected. Examples thereof include tablets, capsules, granules, liquids, and powders.

  The ratio of the benzophenone or its salt contained in said foodstuff can mention the density | concentration of 0.01 to 80 weight%, for example.

  The intake of the above food can be appropriately set according to various conditions such as the body weight, age, sex, and symptoms of the user.

(3) Hair Growth Agent The hair growth agent of the present invention is characterized by comprising the testosterone-5α-reductase inhibitor as an active ingredient.

  In the present invention, hair growth includes the concepts of hair growth, hair restoration, and hair loss prevention.

  The hair restorer of the present invention may contain an additional component as long as the hair restorer based on the testosterone-5α-reductase inhibitory action of benzophenones is not hindered. When such an additional component is included, the ratio of the testosterone-5α-reductase inhibitor in the hair restorer can be exemplified by 0.01 to 98% by weight in terms of the amount of benzophenones or salts thereof.

  The hair restorer of the present invention is not particularly limited in its form, and may have a pharmaceutical form such as powder, granule, tablet, capsule, liquid, suspension, or emulsion. Since the hair restorer of the present invention has a hair growth effect based on the testosterone-5α-reductase inhibitory action of benzophenones, it is preferably used as an external agent for hair growth or an oral agent for hair growth, and as a component of cosmetics for hair. be able to.

  When preparing as an external preparation for hair growth, it is possible to prepare a testosterone-5α-reductase inhibitor in the form of tonic, lotion, ointment and the like together with known ingredients to make an external preparation.

  In the external preparation for hair growth of the present invention, known additives used in the external preparation for hair growth, such as antibacterial agents, refreshing agents, salicylic acid, zinc and derivatives thereof, lactic acid and alkyl esters thereof, oils, surfactants, You may mix | blend 1 type, or 2 or more types selected from a fragrance | flavor, antioxidant, a ultraviolet absorber, a pigment | dye, ethanol, water, a moisturizer, a thickener, a solubilizer, etc.

  Moreover, you may mix | blend other components (minoxidil etc.) for improving the hair-growth effect in the external preparation for hair-growth of this invention.

  The ratio of the testosterone-5α-reductase inhibitor contained in the external preparation for hair growth of the present invention is not particularly limited as long as the external preparation exhibits a hair growth action in terms of the amount of benzophenones or salts thereof. A concentration of 0.01 to 80% by weight can be mentioned.

  When prepared as an oral agent for hair growth, a testosterone-5α-reductase inhibitor is added to a tablet (plain tablet, sugar-coated tablet, effervescent tablet, film-coated tablet, non-toxic carrier, diluent or excipient acceptable in pharmaceuticals. (Including chewable tablets, troches, etc.), capsules, pills, powders (powder), fine granules, granules, liquids, suspensions, emulsions, syrups, pastes, etc. Oral preparations can be made.

  Moreover, you may mix | blend other components (finasteride etc.) for improving the hair-growth effect in the oral agent for hair-growth of this invention.

  The dosage of the oral agent for hair growth of the present invention can be appropriately determined according to various conditions such as the weight, age, sex, and symptoms of the patient.

  The ratio of the testosterone-5α-reductase inhibitor contained in the hair growth oral preparation of the present invention is not particularly limited as long as the oral preparation exhibits a hair growth action in terms of the amount of benzophenones or salts thereof. A concentration of 0.01 to 80% by weight can be mentioned.

  The dosage form of the hair cosmetic composition of the present invention is an aqueous solution system, a solubilization system, an emulsification system, a powder system, an oil liquid system, a gel system, an ointment system, an aerosol system, a water-oil two-layer system, a water-oil-powder. A wide range of dosage forms such as a three-layer system can be adopted.

  The use of the cosmetic for hair of the present invention is also optional, such as shampoo, rinse, hair treatment, hair conditioner, hair conditioner, hair nick, hair dye, hair manicure, pomade, hair liquid, hair cream, hair spray, etc. Can be mentioned.

  The hair cosmetic composition of the present invention includes known additives used in hair cosmetics, such as oily ingredients, moisturizers, thickeners, bactericides, antiseptics, ultraviolet absorbers, antioxidants, and pigments. In addition, one or more selected from a fragrance, a solvent, a pH adjuster, a blood circulation promoter and the like may be blended.

  The ratio of the testosterone-5α-reductase inhibitor or hair restorer contained in the hair cosmetic composition of the present invention is not particularly limited, but is, for example, 0.01 to 80% by weight in terms of the amount of benzophenones or salts thereof. The concentration can be mentioned.

  The hair cosmetic composition of the present invention can be expected to have effects of hair growth, hair growth and hair loss prevention.

  The hair restorer of the present invention also includes the meaning of foods and drinks for the purpose of health, health maintenance, enhancement, etc., for example, health foods, functional foods, dietary supplements, supplements, foods for specified health use, or nutritional functional foods It is. Moreover, the hair restorer of this invention includes the meaning about the additive which provides the hair restorer effect.

  For the above foods, excipients, brighteners, minerals, vitamins, flavonoids, quinones, polyphenols, amino acids, nucleic acids, essential fatty acids, refreshing agents, binders, sweeteners, disintegration as necessary Agents, lubricants, colorants, fragrances, stabilizers, preservatives, sustained release regulators, surfactants, solubilizers, wetting agents and the like can be blended.

  The dosage unit form for use as a supplement is not particularly limited and may be appropriately selected. Examples thereof include tablets, capsules, granules, liquids, and powders.

  The testosterone-5α-reductase inhibitor contained in the above food can include, for example, a concentration of 0.01 to 80% by weight in terms of the amount of benzophenones or salts thereof.

  The intake of the above food can be appropriately set according to various conditions such as the body weight, age, sex, and symptoms of the user.

(4) Prostatic hypertrophy inhibitor The prostatic hypertrophy inhibitor of the present invention is characterized by comprising the testosterone-5α-reductase inhibitor as an active ingredient.

  The prostatic hypertrophy inhibitor of the present invention may contain an additional component as long as the prostatic hypertrophy inhibitory action based on the testosterone-5α-reductase inhibitory action of benzophenones is not hindered. When such an additional component is included, the proportion of the testosterone-5α-reductase inhibitor in the prostate hypertrophy inhibitor can be exemplified by 0.01 to 98% by weight in terms of the amount of benzophenones or salts thereof.

  The form of the prostatic hypertrophy inhibitor of the present invention is not particularly limited, and for example, it may have a pharmaceutical form such as powder, granule, tablet, capsule, liquid, suspension, and emulsion. . Since the prostatic hypertrophy inhibitor of the present invention has a prostatic hypertrophy inhibitory action based on the testosterone-5α-reductase inhibitory action of benzophenones, it can be suitably used as an oral preparation for suppressing prostatic hypertrophy.

  When prepared as an oral preparation for suppressing prostate hypertrophy, a testosterone-5α-reductase inhibitor is added to a tablet (plain tablet, sugar-coated tablet, effervescent tablet, film coat) together with a non-toxic carrier, diluent or excipient acceptable in pharmaceuticals. Tablets, chewable tablets, troches, etc.), capsules, pills, powders (powder), fine granules, granules, solutions, suspensions, emulsions, syrups, pastes, etc. Thus, it is possible to prepare an oral preparation.

  The dose of the oral preparation for suppressing prostate hypertrophy according to the present invention can be appropriately determined according to various conditions such as the patient's weight, age, sex, and symptoms.

  The ratio of the testosterone-5α-reductase inhibitor contained in the oral preparation for suppressing prostate hypertrophy according to the present invention is not particularly limited as long as the oral agent exhibits the action for suppressing prostate hypertrophy, but it is converted into the amount of benzophenones or salts thereof. For example, a concentration of 0.01 to 80% by weight can be mentioned.

  The agent for suppressing prostate hypertrophy according to the present invention includes meanings of foods and drinks for the purpose of health, health maintenance, enhancement, etc., such as health foods, functional foods, dietary supplements, supplements, foods for specified health use, or foods with functional nutrition To do. Moreover, the prostatic hypertrophy inhibitor of the present invention includes the meaning of an additive that imparts an effect of suppressing prostatic hypertrophy.

  For the above foods, excipients, brighteners, minerals, vitamins, flavonoids, quinones, polyphenols, amino acids, nucleic acids, essential fatty acids, refreshing agents, binders, sweeteners, disintegration as necessary Agents, lubricants, colorants, fragrances, stabilizers, preservatives, sustained release regulators, surfactants, solubilizers, wetting agents and the like can be blended.

  The dosage unit form for use as a supplement is not particularly limited and may be appropriately selected. Examples thereof include tablets, capsules, granules, liquids, and powders.

  The testosterone-5α-reductase inhibitor contained in the above food can include, for example, a concentration of 0.01 to 80% by weight in terms of the amount of benzophenones or salts thereof.

  The intake of the above food can be appropriately set according to various conditions such as the body weight, age, sex, and symptoms of the user.

(5) Anti-acne Agent The anti-acne agent of the present invention is characterized by comprising the testosterone-5α-reductase inhibitor as an active ingredient.

  The anti-acne agent of the present invention may contain an additional component as long as the sebum secretion suppressing action based on the testosterone-5α-reductase inhibitory action of benzophenones is not hindered. When such an additional component is included, the proportion of the testosterone-5α-reductase inhibitor in the anti-acne agent can be exemplified by 0.01 to 98% by weight in terms of the amount of benzophenones or salts thereof.

  The anti-acne agent of the present invention is not particularly limited in its form, and may have a pharmaceutical form such as powder, granule, tablet, capsule, liquid, suspension, or emulsion. Since the anti-acne agent of the present invention has a sebum secretion inhibitory action based on the testosterone-5α-reductase inhibitory action of benzophenones, it is used as an anti-acne external agent or an anti-acne oral agent, and as a component of skin cosmetics. Can be preferably used.

  When preparing as an anti-acne external preparation, the testosterone-5α-reductase inhibitor can be prepared in the form of cream, gel, lotion, ointment and the like together with known ingredients to make an external preparation.

  The anti-acne external preparation of the present invention includes known additives used for anti-acne external preparations, such as antibacterial agents, oils, surfactants, fragrances, antioxidants, ultraviolet absorbers, dyes, ethanol, You may mix | blend the 1 type (s) or 2 or more types selected from water, a moisturizer, a thickener, a solubilizer, etc.

  The ratio of the testosterone-5α-reductase inhibitor contained in the anti-acne external preparation of the present invention is not particularly limited as long as the external preparation exhibits an acne prevention or treatment action, but is converted into the amount of benzophenones or salts thereof. For example, a concentration of 0.01 to 80% by weight can be mentioned.

  When prepared as an oral anti-acne preparation, testosterone-5α-reductase inhibitor is added to a tablet (plain tablet, sugar-coated tablet, effervescent tablet, film-coated tablet) together with a non-toxic carrier, diluent or excipient acceptable in pharmaceuticals. (Including chewable tablets, troches, etc.), capsules, pills, powders (powder), fine granules, granules, liquids, suspensions, emulsions, syrups, pastes, etc. Oral preparations are possible.

  The dose of the oral anti-acne preparation of the present invention can be appropriately determined according to various conditions such as the patient's weight, age, sex, and symptoms.

  The testosterone-5α-reductase inhibitor contained in the anti-acne oral preparation of the present invention is not particularly limited as long as the oral agent exhibits an acne prevention or treatment action, but in terms of the amount of benzophenones or salts thereof, For example, a concentration of 0.01 to 80% by weight can be mentioned.

  The skin cosmetic preparation of the present invention has an aqueous solution system, a solubilization system, an emulsification system, a powder system, an oil liquid system, a gel system, an ointment system, an aerosol system, a water-oil two-layer system, and a water-oil-powder. A wide range of dosage forms such as a three-layer system can be adopted.

  The use of the skin cosmetics of the present invention is also arbitrary, for example, lotion, milky lotion, cream, gel, essence, serum, pack, mask, face wash, massage agent, cleansing agent, after shave lotion, pre shave lotion , Shaving cream, body soap, soap and the like.

  The skin cosmetics of the present invention include known additives used in skin cosmetics, such as oily ingredients, moisturizers, thickeners, bactericides, preservatives, ultraviolet absorbers, antioxidants, and pigments. In addition, one or more selected from a fragrance, a solvent, a pH adjuster and the like may be blended.

  The ratio of the testosterone-5α-reductase inhibitor or the anti-acne agent contained in the skin cosmetic of the present invention is not particularly limited, but in terms of the amount of benzophenones or salts thereof, for example, 0.01 to 80% by weight Can be mentioned.

  The skin cosmetic of the present invention can be expected to be effective in preventing or treating acne.

  The anti-acne agent of the present invention also includes the meaning of foods and drinks for the purpose of health, health maintenance, promotion, etc., such as health foods, functional foods, dietary supplements, supplements, foods for specified health use, or nutritional functional foods. Is. Further, the anti-acne agent of the present invention also includes the meaning of an additive that imparts an acne prevention or treatment effect.

  For the above foods, excipients, brighteners, minerals, vitamins, flavonoids, quinones, polyphenols, amino acids, nucleic acids, essential fatty acids, refreshing agents, binders, sweeteners, disintegration as necessary Agents, lubricants, colorants, fragrances, stabilizers, preservatives, sustained release regulators, surfactants, solubilizers, wetting agents and the like can be blended.

  The dosage unit form for use as a supplement is not particularly limited and may be appropriately selected. Examples thereof include tablets, capsules, granules, liquids, and powders.

  The ratio of the benzophenone or its salt contained in said foodstuff can give the density | concentration of 0.01 to 80 weight%, for example in conversion of the quantity of benzophenone or its salt.

  The intake of the above food can be appropriately set according to various conditions such as the body weight, age, sex, and symptoms of the user.

  The testosterone-5α-reductase inhibitor, hair restorer, prostate hypertrophy inhibitor, anti-acne agent, hair cosmetic, and skin cosmetic of the present invention described above are applied to mammals including humans. It is.

  Examples are given below to illustrate the present invention in more detail. However, the present invention is not limited to these examples.

Example 1 (Cuban propolis)
0, 10, 30, 50, 60, 70, 80, 90, 100 volume% ethanol (200 ml) was added to 4 g of the crushed propolis ingot from Cuba, and the mixture was extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.), and then concentrated under reduced pressure using an evaporator. The concentrated solution was subjected to lyophilization to obtain 0.26, 0.24, 0.16, 0.30, 0.64, 0.74, 1.08, 1.56, 1.87 g of propolis extract whose main component is benzophenones.

Example 2 (nemoloson)
Nemoloson was isolated according to the following method.

  (i) Ethanol extract of brown propolis bulk (Cuba) was concentrated with a rotary evaporator. When the viscosity increased, it was switched to a vacuum drying method and dried overnight at room temperature.

(ii) 1.4 g of the propolis extract obtained above was subjected to column chromatography (gel type: silica gel 60N (Kanto Chemical), column size: φ20 × 440 mm), and 100% by volume of chloroform was used as the eluent. (800 mL of each eluent was poured and 100 mL was collected). When each component obtained was confirmed by high performance liquid chromatography (HPLC) under the following conditions, it was confirmed that nemoloson was eluted at 300-400 mL.
<HPLC conditions>
Column: Cosmosil 5C-18-AR-II manufactured by Nacalai Tesque, 4.6 x 250 mm,
Moving bed: A liquid: 0.1 vol% TFA-containing water, B liquid: methanol
Gradient condition: 0 minute → 5 minutes: A: B = 40: 60 (v / v), 5 minutes → 50 minutes: A: B = 40: 60 (v / v) → 0: 100 (v / v) 50 minutes → 60 minutes: A: B = 0: 100 (v / v), 60 minutes → 70 minutes: A: B = 40: 60 (v / v), flow rate: 1 ml / min, detection wavelength: 280 nm,
Nemoloson retention time: 42 minutes

(iii) After concentrating the above fractions, the fractions were sequentially eluted by medium pressure column chromatography under the following conditions.
<Medium pressure column chromatography conditions>
Gel type: Silica gel, Hi-Flash colum ODS (Yamazen),
Column size: φ26 × 100 mm,
Detection wavelength: 280 nm,
Moving bed: A liquid: ultrapure water, B liquid: methanol,
Gradient condition: 0 minutes → 80 minutes: A: B = 40: 60 (v / v) → 0: 100 (v / v), 80 minutes → 100 minutes: A: B = 0: 100 (v / v) , Flow rate: 10 ml / min.

  The eluate was collected 20 mL at a time, and the 41st and 42nd fractions, which showed an absorption peak at a detection wavelength of 280 nm, were concentrated by an evaporator, and 18 mg (purity 99%) and 11 mg (purity 97%), respectively. Got the nemoloson.

  The identification results of nemoloson are shown below.

measuring device
NMR; AVANCE 300 manufactured by Bruker BioSpin
MS; Waters Quattro Premier XE
(i) Nemoloson
ESI-MS m / z: 502.7
1H-NMR (300 MHz, CDCl3) δHfrom TMS: H-9,13 (7.64 + 7.48, d 7.8), 7.23 (t 7,8), H-11 (7.39, t 7,8), H2-14 ( 2.40 to 2.70, complex), H-15 (-5.10, m), H3-17 (1.70 + 1.74, s / s), H3-18 (1.66 + 1.67, s / s), H2-19 (3.10 to 3.30 , complex), H-20 (5.10, m), H3-22 (1.66 + 1.70, s / s), H3-23 (1.62 + 1.67, s / s), H2-24 (2.05 to 2.70, complex), H-25 (not observed), H3-27 (1.17 + 1.13, s / s), H3-28 (1.35 + 1.40, s / s), H2-29 (2.06 to 2.20, complex), H-30 (4.98 , m), H3-32 (1.66 + 1.70, s / s) and H3-33 (1.56 + 1.58, s / s)
13C NMR (75 MHz, CDCl3) δC from TMS: C-1 (64.81 + 57.33), C-2 (207.32 + 206.59), C-3 (71.96 + 78.63), C-4 (194.64 + 170.20), C-5 (119.40 + 118.24), C-6 (167.19 + 191.92), C-7 (193.02), C-8 (137.67+ 136.74), C-9,13 (128.14), C-10,12 (127.59), C -11 (131.94 + 131.76), C-14 (29.50 + 29.20), C-15 (119.48 + 119.96), C-16 (136.96 + 136.27), C-17,22,32 (25.79, 25.67, 25.58), C-18,23,33 (17.94,17.74, 17.69), C-19 (23.86 + 22.49), C-20 (118.09 + 118.24), C-21 (134.08 + 135.59), C-24 (42.28 + 39.82) , C-25 (42.57 + 43.15), C-26 (47.18 + 48.24), C-27 (24.22 + 23.25), C-28 (13.93 + 15.70), C-29 (27.47 + 26.72), C-30 ( 122.30 +122.35) and C-31 (133.07)

Example 3 (Crucia Rosea)
To 4 g of the pulverized product of Kursia rosea, 200 ml of 70 vol% ethanol was added, and the mixture was extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.) and then concentrated under reduced pressure using an evaporator to obtain a Kursia-Rosea extract. The extract contained 3 w / w% nemoloson and 30 w / w% nemoloson II.

Example 4 (Crucia Grandiflora)
200 g of 50% ethanol by volume was added to 4 g of the ground product of Kursia grandiflora and extracted by stirring at room temperature for 24 hours. The extract with stirring was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.) and then concentrated under reduced pressure using an evaporator to obtain a Crucia grandiflora extract. The extract contained 18 w / w% nemoloson.

Example 5 (Crucia Hilaryana)
To 4 g of the pulverized product of Kursia hirariana, 200 ml of 80% ethanol by volume was added, and the mixture was extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.) and then concentrated under reduced pressure using an evaporator to obtain a Kursia / Hilariana extract. The extract contained 2.5 w / w% nemoloson.

Example 6 (Crucia Insignis)
To 4 g of the crushed Crucia insignis, 200 ml of 90% ethanol was added, and the mixture was extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.) and then concentrated under reduced pressure using an evaporator to obtain a Kursia insignis extract. The extract contained 26.4 w / w% of 7-epi-nemoloson.

Example 7 (Crucia Rengelios)
To 4 g of the crushed crucia rengelioizu, 200 ml of 100% ethanol by volume was added, and the mixture was extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.) and then concentrated under reduced pressure using an evaporator to obtain a Kursia rengelioizu extract. The extract contained 15.4 w / w% 7-epi-nemoloson and 10.2 w / w% nemoloson II.

Example 8 (Crucia Nemoroso)
To 4 g of the pulverized product of Kursia rosea, 200 ml of 70 vol% ethanol was added, and the mixture was extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.) and then concentrated under reduced pressure using an evaporator to obtain a Kursia-Rosea extract. The extract contained 19.6 w / w% nemoloson and 5.6 w / w% 7-epi-nemoloson.

Comparative Example 1 (Propolis from Brazil)
To 4 g of pulverized propolis ingot from Southeast Brazil, 200 ml of 70% ethanol was added and extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.), and then concentrated under reduced pressure using an evaporator. Next, the concentrated solution was freeze-dried to obtain 2.11 g of a propolis extract whose main component is a cinnamic acid derivative.

Comparative Example 2 (Chinese propolis)
To 4 g of pulverized Chinese propolis ingot, 200 ml of 70% ethanol was added and extracted by stirring at room temperature for 24 hours. The extract was filtered through a filter paper (No. 2 manufactured by Advantech Toyo Co., Ltd.), and then concentrated under reduced pressure using an evaporator. Subsequently, the concentrated solution was subjected to lyophilization to obtain 1.75 g of a propolis extract whose main component is flavonoids.

Test example 1
Testosterone-5α-reductase isolated from the liver of Wistar rats by conventional centrifugation was used. The propolis extracts of Examples 1 and 2 were diluted with DMSO to final concentrations of 1000, 100, 10, 1, 0.1, and 0.01 μg / ml, respectively, and 0.9 μM testosterone in DTT buffer (pH 6.5). And 20 μg / ml testosterone-5α-reductase solution containing 50 μM NADPH and incubated at 37 ° C. for 30 minutes. The reaction was quenched by the addition of 1N HCl and neutralized with 1N NaOH. Testosterone was quantified using the Testosterone EIA Kit. DMSO, which is a sample diluent, was used as a control, and the inhibition rate was calculated by the following calculation method. A 50% inhibitory activity concentration (IC ₅₀ : μg / ml) was calculated from the obtained inhibition rate and action concentration.

Inhibition rate (%) = [(Control Absorption Intensity−Sample Absorption Intensity) / Control Absorption Intensity] × 100
The obtained results are shown in Tables 1 and 2.
The contribution ratio of nemoloson in Table 2 was obtained by the following formula.
Contribution ratio = (Propolis IC ₅₀ × nemoloson content / nemoloson IC ₅₀ ) × 100

※１：プロポリスペースト中にネモロソンは12.17(w/w%)含まれる。
※２：寄与率が計算上100%以上となるため、100%と記載している(試験の誤差によるIC₅₀のずれによるものだと考えられる)。

* 1: 12.17 (w / w%) of nemoloson is included in propolyspace.
* 2: Since the contribution rate is 100% or more in the calculation, it is described as 100% (it is considered to be due to the IC ₅₀ deviation due to test error).

  From the results in Table 1, it can be seen that Cuban propolis has an excellent testosterone-5α-reductase inhibitory action. Moreover, it can be seen from the results in Table 2 that the testosterone-5α-reductase inhibitory action of Cuban propolis is derived from nemoloson.

  The Brazilian propolis and the Chinese propolis, which are known to have testosterone-5α-reductase inhibitory action, do not contain nemoloson as shown below. Therefore, it is a new finding that Cuban propolis containing nemoloson has testosterone-5α-reductase inhibitory action.

Test example 2
Quantitative analysis was performed on nemoloson in the propolis extracts of Example 1 and Comparative Examples 1 and 2. Sample solutions were prepared by dissolving each propolis extract of Examples and Comparative Examples in absolute ethanol at a concentration of 0.001% by mass. These sample solutions were analyzed by HPLC, and the concentration of nemoloson (μg / mL) was measured. And the total solid content concentration in this ethanol extract was measured, and it converted into content (w / w%) per solid content of each component contained in the ethanol extract.

  HPLC analysis conditions were as follows: Column: Cosmosil 5C18-AR-II (5 μm, 4.6 mm ID × 250 mm, manufactured by Nacalai Tesque) Guard column: Cosmosil 5C18-AR-II (5 μm, 4.6 mm ID × 10 mm, Nacalai Tesque) Manufactured), column oven: 40 ° C., solvent: solution A; water containing 0.1 vol% TFA, solution B; methanol, gradient condition: 0 minutes → 5 minutes; A / B = 40/60 (v / v), 5 minutes → 50 minutes; A / B = 40/60 (v / v) → 0: 100 (v / v), 50 minutes → 60 minutes; A / B = 0/100 (v / v), 60 minutes → 70 minutes A / B = 40/60 (v / v), flow rate: 1 ml / min, injection volume: 10 μL, detection wavelength: 280 nm, retention time of nemoloson: 42 minutes. The results are shown in Table 3.

  From the results in Table 3, it can be seen that Cuban propolis contains nemoloson, while Brazilian and Chinese propolis do not contain nemoloson.

Formulation Example Hereinafter, a formulation example of the present invention will be shown.

Formulation Example 1
200 ml of 80% ethanol extract of Cupolis propolis was sprayed and dried into 1 kg of lactose, powdered and filled into hard capsules to obtain capsules containing ethanol extract of propolis.

Formulation example 2
250 g of starch syrup, 300 g of sugar and 50 ml of water were dissolved by heating, and 50 ml of an ethanol extract of 10 vol% propolis concentrated with nemoloson was added. In particular, it was molded into a suitable size to obtain a propolis ethanol extract-containing candy.

Formulation Example 3
30% ethanol extract of Cuban propolis 0.5 ml
Ascorbic acid 300 mg
Honey 10 g
Lemon juice 10 ml
A proper amount of water The above ingredients were mixed to obtain a total amount of 50 ml of propolis containing an ethanol extract-containing drink.

Formulation Example 4
A supplement was prepared according to the following formulation using a 70 vol% ethanol extract of propolis enriched with nemoloson. The powder of the following prescription was uniformly mixed, and a 160 mg tablet supplement was prepared by a conventional method using a tableting machine.
Spray dried product of ethanol extract of 70 vol% propolis enriched with nemoloson 10 mg
Dry beer yeast powder 50 mg
Reduced maltose 75 mg
Sucrose fatty acid ester 20 mg
Cellulose 5 mg

Formulation Example 5
Tablets were prepared according to the following formulation using a freeze-dried 100% ethanol extract of propolis enriched with nemoloson.
Spray dried 10% ethanol extract of propolis enriched with nemoloson 10 mg
Microcrystalline cellulose 80 mg
Corn starch 78 mg
Magnesium stearate 2 mg

Formulation Example 6
As a coating agent, 32.15 g of corn starch was added (coated) to 75 g of 60 vol% ethanol extract concentrated with nemoloson to obtain 107.15 g of coated granules of ethanol extract. The coating ratio of this granule is 0.3.

Formulation Example 7
Mix 50 mg of 50% ethanol by volume with nemoloson, 150 mg soybean oil, 20 mg beeswax, 30 mg glycerin fatty acid ester, and 50 μg crucian rengelioz 70% ethanol extract according to standard methods, and fill into gelatin soft capsules And a granular health food.

Formulation Example 8
Cuban propolis 70% ethanol extract 0.2 g, pyridoxine hydrochloride 0.1 g, L solcin 0.01 g, D-pantothenyl alcohol 0.1 g, dipotassium glycyrrhizinate 0.1 g, l-menthol 0.05 g, 1,3-butylene glycol 4.0 g Ginseng extract 0.5 g, ethanol 25.0 g, perfume as appropriate, and purified water (with a total amount of 100 g) were treated according to a conventional method to produce a hair tonic.

Formulation Example 9
Cuban propolis 90 vol% ethanol extract 0.2 g, polyoxyethylene alkyl ether sodium sulfate 30.0 g, polyoxyethylene alkyl ether ammonium sulfate 20.0 g, coconut oil fatty acid amidopropyl betaine 6.0 g, coconut oil fatty acid diethanolamide 4.0 g, distearic acid Ethylene glycol 2.0 g, preservative (methyl paraoxybenzoate) 0.15 g, Crucia Rosea 70 vol% ethanol extract, fragrance 0.01 g, 1,3-butylene glycol 3.0 g, and purified water (total amount 100 g) The shampoo was manufactured by processing according to a conventional method.

Formulation Example 10
Cuban Propolis 60% ethanol extract 0.2 g, stearyltrimethylammonium chloride 1.5 g, polyoxyethylene cetyl ether 1.0 g, cetyl alcohol 2.0 g, octyldodecanol 1.0 g, cationized cellulose 0.5 g, propylene glycol 5.0 g, crusia・ Grandiflora 70 vol% ethanol extract, fragrance 3.0 g, and purified water (total amount 100 g) were treated according to a conventional method to produce a rinse.

Formulation Example 11
Cuban propolis 50% ethanol extract 0.2 g, dipotassium glycyrrhizinate 0.2 g, 1,3-butylene glycol 4.0 g, oleyl alcohol 4.0 g, polyoxyethylene sorbitan monolaurate (20E.O) 1.5 g, polyoxyethylene Lauryl ether (20E.O) 0.5 g, Kursia hilariana 70 vol% ethanol extract 0.2 g, ethanol 15 g, preservative appropriate, perfume appropriate, and purified water (total amount 100 g) were treated according to a conventional method, and sebum A lotion having a secretory inhibitory effect was prepared.

Formulation Example 12
Cuban propolis water extract 0.2 g, stearyl glycyrrhetinate 0.1 g, beeswax 10.0 g, cetanol 5.0 g, hydrophilic lanolin 8.0 g, squalane 35.5 g, glyceryl monostearate 2.0 g, Crucia insignis 70 vol% ethanol extraction 0.2 g of polyoxyethylene sorbitan monolaurate (20E.O), 0.5 g of polyethylene glycol, 0.5 g of preservatives, fragrance, and purified water (100 g in total) were treated according to the standard method to suppress sebum secretion A cream with action was produced.

Claims (7)

  Garcinol, isogarcinol, xanthothymol, isoxanthothymol, gucciferon E, garcinielipton I, hiperibone B, propolon A, propolon C, proporon D, curcyanone, nemoloson, nemoloson II, 7-epinemoloson, methylnemoloson II or A testosterone-5α-reductase inhibitor comprising as an active ingredient a benzophenone which is hydroxynemoloson or a salt thereof.   The testosterone-5α-reductase inhibitor according to claim 1, wherein the benzophenones are nemoloson, nemoloson II, 7-epinemoloson, methylnemoloson II or hydroxynemoloson.   The testosterone-5α-reductase inhibitor according to claim 2, comprising a propolis containing nemoloson, nemoloson II, 7-epinemoloson, methylnemoloson II or hydroxynemoloson or an extract thereof as an active ingredient.   The testosterone-5α-reductase inhibitor according to claim 3, wherein the propolis is a Cuban propolis.   Clusia rosea, Clusia grandiflora, Clusia hilariana, Clusia insignis, Clusia renggerioides or Clusia nemorosa The testosterone-5α-reductase inhibitor according to claim 2, comprising a plant or an extract thereof as an active ingredient.   A hair restorer containing the testosterone-5α-reductase inhibitor according to any one of claims 1 to 5 as an active ingredient.   A prostate hypertrophy inhibitor comprising the testosterone-5α-reductase inhibitor according to any one of claims 1 to 5 as an active ingredient.