JP2018030829A - Loxoprofen-containing pharmaceutical formulation - Google Patents

Abstract

PROBLEM TO BE SOLVED: To provide means for preventing discoloration of, during high-temperature storage, a liquid or semisolid composition containing loxoprofen or a salt thereof.SOLUTION: The present invention provides a pharmaceutical formulation in which a liquid or semisolid composition containing following components: (A) loxoprofen or a salt thereof and (B) capsicum or extract thereof is stored in a polyolefin resin container.SELECTED DRAWING: None

Description

  The present invention relates to a pharmaceutical preparation containing loxoprofen, which is also known as an active ingredient of Loxonin (registered trademark).

Loxoprofen is a kind of phenylpropionic acid-based non-steroidal anti-inflammatory analgesic (NSAID) (Non-Patent Document 1) and exhibits an excellent anti-inflammatory analgesic effect.
For this reason, it has been widely used as an active ingredient for external anti-inflammatory analgesics, and has been used to date for externally applied anti-arthritis, myalgia, post-traumatic swelling / pain, etc. Agents (such as poultices and tapes) and external coating agents (such as gels) have been developed and marketed (Non-patent Document 2).

  By the way, red pepper, pepper, such as nonanoic acid vanillylamide (nonylic acid vanillylamide) or an extract thereof is blended in an external anti-inflammatory analgesic agent, and an external preparation blended with loxoprofen is already known (for example, Patent Document 1). 2).

International Publication No. 2014/002599 Pamphlet Japanese Patent Laying-Open No. 2015-98469

The 16th revision Japanese Pharmacopoeia Manual Sasakawa Shoten Co., Ltd. C-5359-5364 Loxonin (registered trademark) gel 1% pharmaceutical interview form Daiichi Sankyo Co., Ltd. Revised October 2010 (3rd edition)

When using loxoprofen as an active ingredient of an external preparation, it is used by applying it to the affected area as a liquid or semi-solid composition such as a lotion preparation, gel preparation, cream preparation, etc. It is preferable from the viewpoint of administering a necessary amount flexibly according to the position, shape and range of the affected area. Moreover, if the technique which mix | blends loxoprofen stably with a liquid or semi-solid composition can be established, the application to not only an external preparation but an internal medicine (oral liquid etc.) will also become possible.
Therefore, in order to establish a technique for stably blending loxoprofen into a liquid or semi-solid composition, the present inventor prepares a liquid or semi-solid composition containing loxoprofen or a salt thereof and has storage stability. As a result of the evaluation, it was surprisingly found that discoloration can occur over time due to storage under high temperature conditions.

  Accordingly, an object of the present invention is to provide means for suppressing discoloration of a liquid or semi-solid composition containing loxoprofen or a salt thereof during high temperature storage.

  Therefore, the present inventor further studied to solve this problem. As a result, a liquid or semi-solid composition containing loxoprofen or a salt thereof was further added. It was found that discoloration during high-temperature storage can be suppressed by containing a product and storing it in a polyolefin resin container typified by polyethylene, and thus completed the present invention.

That is, the present invention includes the following components (A) and (B):
(A) Loxoprofen or a salt thereof;
(B) Capsicum or an extract thereof;
The present invention provides a pharmaceutical preparation in which a liquid or semi-solid composition containing is contained in a polyolefin resin container.
The present invention also includes the following components (A) and (B):
(A) Loxoprofen or a salt thereof;
(B) Capsicum or an extract thereof;
The present invention provides a method for suppressing discoloration of a composition, which comprises a step of containing a liquid or semi-solid composition containing a resin in a polyolefin resin container.

  ADVANTAGE OF THE INVENTION According to this invention, the discoloration at the time of high temperature preservation | save of the liquid or semisolid composition containing loxoprofen or its salt can be suppressed. Therefore, a medicament containing loxoprofen or a salt thereof having excellent storage stability can be provided.

First, the invention of the embodiment of “pharmaceutical preparation” will be described below.
<Component (A)>
In the present invention, “loxoprofen or a salt thereof” includes loxoprofen itself, a pharmaceutically acceptable salt of loxoprofen, and a solvate of loxoprofen or a pharmaceutically acceptable salt thereof with water, alcohol, or the like. It is. These are known compounds, and can be produced by known methods, or commercially available products can be used. In the present invention, loxoprofen or a salt thereof is preferably loxoprofen sodium hydrate (chemical name: Monosodium 2- [4-[(2-oxocyclopentyl) methyl] phenyl] propanoate dihydrate).

  In the present invention, the content of loxoprofen or a salt thereof in the liquid or semi-solid composition is not particularly limited, and may be determined as appropriate according to the desired anti-inflammatory analgesic effect. In the present invention, loxoprofen or a salt thereof is preferably contained in an amount of 0.01 to 10% by mass, more preferably 0.1 to 5% by mass, in terms of anhydrous loxoprofen sodium, based on the total mass of the composition. It is particularly preferable to contain 0.5 to 3 mass%.

<Component (B)>
In the present invention, “capsicum” is not particularly limited, and for example, capsicum (capsicum annuum Linne (Solanaceae) fruit) listed in the 16th revised Japanese pharmacopoeia can be suitably used. The shape of the pepper can be adjusted as needed, and can be cut or crushed into small pieces, small chunks, or pulverized into a powder. Can be used. In addition, in consideration of convenience in handling at the time of producing the composition / pharmaceutical preparation, a product obtained by subjecting the pepper to some kind of extraction treatment (referred to as “the pepper extract” in the present specification) may be used.
Note that the “capsicum extract” includes those subjected to processing such as heating, drying, and pulverization in addition to extraction processing. Specifically, after the capsicum is appropriately sized as required, an appropriate leaching solution (extraction solvent) is added and leached, or the leaching solution is concentrated (soft extract, tincture, etc.), A dried product (dried extract or the like) is also included in the “capsicum extract” of the present invention.
Furthermore, in the present invention, as the “capsicum extract”, a known capsaicinoid which is a main component of the capsicum may be used. As the capsaicinoid, capsaicin and nonanoic acid vanillylamide (also called nonyl acid vanillylamide) are preferable.

  In the present invention, the “capsicum or extract thereof” is preferably capsicum, capsicum powder, capsicum extract (soft extract, dry extract), capsaicin, nonanoic acid vanillylamide, and particularly preferably capsicum soft extract and nonanoic acid vanillylamide.

  The method for producing the extract of chili pepper is not particularly limited. For example, the description of the “Extract”, “Dipping / decoction”, “Tincture”, “Flux Extract” in the 16th revised Japanese Pharmacopoeia It can be produced with reference to known methods for producing plant extracts. Specifically, for example, the pepper can be cut, heated, dried, pulverized, etc. as necessary, and then extracted by adding an appropriate extraction solvent. The obtained extract may be further concentrated, dried, etc. as necessary.

Examples of the extraction solvent include lower monohydric alcohols such as methanol, ethanol, isopropanol, and n-butanol; lower polyhydric alcohols such as ethylene glycol, propylene glycol, 1,3-butylene glycol, and glycerin; ethers such as diethyl ether. Ketones such as acetone and ethyl methyl ketone; esters such as ethyl acetate; nitriles such as acetonitrile; alkanes such as pentane, hexane, cyclopentane and cyclohexane; halogenoalkanes such as dichloromethane and chloroform; benzene, toluene and the like Aromatic hydrocarbons; dimethylformamide; dimethyl sulfoxide; water (including hot water). These may be used alone or in combination of two or more. In the present invention, water, ethanol, or a water / ethanol mixture is preferred.
The extraction operation is not particularly limited, and a known method used for an extraction operation from a plant can be appropriately adopted. Specifically, for example, immersion in an extraction solvent (cold immersion, digestion, percolation, etc.) Extraction using a supercritical fluid or subcritical fluid may be mentioned. In addition, in order to raise extraction efficiency, you may homogenize in stirring or an extraction solvent.
The extraction temperature is not particularly limited and varies depending on the extraction solvent to be used, the extraction operation, and the like, but is preferably set to a temperature from about 5 ° C. to the boiling point of the extraction solvent.
The extraction time is not particularly limited and varies depending on the extraction solvent to be used, the extraction operation, and the like, but is preferably about 1 hour to 14 days.

  In the present invention, a commercially available product can be used as the pepper or an extract thereof. Specific examples of the commercially available product include pepper extract-B, pepper extract-D, pepper extract-N, pepper extract-S, ( Bureau) Pepper tincture, (Place) Pepper powder (Nippon Powder Chemical Co., Ltd.), Nonylic acid vanillylamide (Nagaoka Jitsugyo Co., Ltd.) and the like.

  In the present invention, the content of the pepper or the extract thereof in the liquid or semi-solid composition is not particularly limited, but from the viewpoint of the discoloration inhibiting action, the pepper or the extract thereof is the total mass of the composition in terms of the active ingredient. The content is preferably 0.01 to 15% by mass, more preferably 0.05 to 10% by mass, and particularly preferably 0.1 to 8% by mass. In particular, when capsaicin such as capsaicin or nonanoic acid vanillylamide is used as a capsicum or an extract thereof, the capsaicinoid is contained in an amount of 0.0001 to 2% by mass with respect to the total mass of the composition from the viewpoint of discoloration inhibiting action. Preferably, the content is 0.0005 to 1% by mass, more preferably 0.001 to 0.5% by mass, and particularly preferably 0.005 to 0.1% by mass.

  In the present invention, the content ratio of loxoprofen or a salt thereof and capsicum or an extract thereof in a liquid or semi-solid composition is not particularly limited and may be appropriately determined and determined from the viewpoint of a discoloration suppressing action. From the viewpoint of the inhibitory action, it is preferable to contain 0.01 to 15 parts by mass of chili pepper or an extract thereof in terms of bulk drug substance with respect to 1 part by mass of loxoprofen or a salt thereof in terms of loxoprofen anhydride. The content is more preferably 10 parts by mass, and particularly preferably 0.1 to 8 parts by mass. Further, particularly when capsaicinoids such as capsaicin and nonanoic acid vanillylamide are used as capsicum or an extract thereof, from the viewpoint of discoloration inhibiting action, capsaicinoid is added to 1 part by mass of loxoprofen sodium salt in terms of loxoprofen sodium anhydride. It is preferable to contain 0.0001 to 2 parts by mass, more preferably 0.0005 to 1 part by mass, still more preferably 0.001 to 0.2 parts by mass, and 0.005 to 0.1 parts by mass. It is particularly preferred to contain parts.

<Liquid or semi-solid composition>
In the present invention, the “liquid or semi-solid composition” means a liquid or semi-solid composition at normal temperature (any temperature within the range of 15 to 25 ° C.).
In the present invention, the properties of the composition are not particularly limited, and may be any of a solution, a colloidal solution (sol (suspension or emulsion)), a gel, and the like. In addition, the type and properties of the solvent or base are not particularly limited, and may be hydrophilic or hydrophobic such as oily. Further, a plurality of different types of solvents and bases may be appropriately mixed and emulsified, etc. May be used. Specific examples of such a solvent / base include components exemplified as additives described later.

  In the present invention, from the viewpoint of safety during use of the pharmaceutical preparation, the liquid or semi-solid composition preferably contains water. Here, the content of water in the composition is not particularly limited, but it is preferably 1% by mass or more based on the total mass of the composition from the viewpoint of safety and discoloration-inhibiting action during use of the pharmaceutical preparation. It is more preferably 5% by mass or more, further preferably 10 to 90% by mass, still more preferably 20 to 70% by mass, and particularly preferably 30 to 50% by mass.

  Moreover, in this invention, it is preferable that a liquid or semi-solid composition contains a lower alcohol from a viewpoint of the usability | use_condition of a pharmaceutical formulation. Here, the “lower alcohol” means a linear or branched monovalent alcohol having 1 to 6 carbon atoms, and specific examples include ethanol, isopropanol, n-propanol, and the like. Isopropanol and mixtures thereof are preferred. Here, the content of the lower alcohol in the composition is not particularly limited, but is preferably 5% by mass or more based on the total mass of the composition from the viewpoint of the usability of the pharmaceutical preparation and the discoloration-inhibiting action. More preferably, it is 90 mass%, It is further more preferable that it is 15-70 mass%, It is especially preferable that it is 20-50 mass%.

  In the present invention, it is preferable that the liquid or semi-solid composition contains both water and a lower alcohol from the viewpoints of safety and usability when using the pharmaceutical preparation. Even when the composition is a composition containing at least one of water and a lower alcohol (particularly a composition containing both water and a lower alcohol), discoloration is suppressed.

  In the present invention, the liquid or semi-solid composition includes a pharmaceutical ingredient other than those described above, for example, analgesic ingredients, anti-inflammatory ingredients, antihistamine ingredients, bactericidal ingredients, astringent / protective ingredients, blood circulation promoting ingredients, warming ingredients, Sensitive ingredients, local anesthetic ingredients, antitussives, noscapine, bronchodilators, expectorants, hypnotic sedatives, vitamins, gastric mucosal protective agents, antacids, anticholinergics, herbal medicines, Kampo prescriptions, etc. 1 type (s) or 2 or more types may be included.

As an analgesic component, for example, aspirin, aspirin aluminum, acetaminophen, isopropylantipyrine, ibuprofen, ethenzamide, sazapyrine, salicylamide, salicylic acid, ethylene glycol salicylate, glycol salicylate, sodium salicylate, methyl salicylate, thiaramide hydrochloride, lactylphenetidine Etc.
Anti-inflammatory components include, for example, sodium guaiazulene sulfonate, glycyrrhizic acid and derivatives thereof, and salts thereof (for example, dipotassium glycyrrhizinate, monoammonium glycyrrhizinate), glycyrrhetinic acid, ceaprose, semi-alkaline proteinase, serrapeptase, proctase, Examples include pronase and bromelain.

  Antihistamine components include, for example, azelastine hydrochloride, alimemazine tartrate, istipendil hydrochloride, iproheptin hydrochloride, ebastine, epinastine hydrochloride, emedastine fumarate, oxatomide, carbinoxamine diphenyldisulfonate, carbinoxamine Maleate, clemastine fumarate, d-chlorpheniramine maleate, dl-chlorpheniramine maleate, ketotifen fumarate, dipheterol hydrochloride, difeterol phosphate, diphenylpyraline hydrochloride, diphenylpyraline Theocurate, diphenhydramine hydrochloride, diphenhydramine salicylate, diphenhydramine tannate, cetirizine hydrochloride, triprolyzine hydrochloride, tripelenamine hydrochloride, tondilamine hydrochloride, fe Sofenajin, fenethazine hydrochloride, promethazine hydrochloride, promethazine methylene two salicylates, bepotastine besilate, homochlorcyclizine hydrochloride, mequitazine, methdilazine hydrochloride, main blanking hydro Linna Paji sill acid salts.

  Examples of the sterilizing component include benzalkonium chloride. Examples of the astringent / protective component include zinc oxide. Examples of the blood circulation promoting component include tocopherol acetate, benzyl nicotinate, heparin-like substances, sodium polyethylene sulfonate, and the like. Examples of the local anesthetic component include lidocaine, clove oil, belladonna extract and the like.

  Antitussives include, for example, aloclamide hydrochloride, eprazinone hydrochloride, carbetapentane enoate, cloperastine hydrochloride, cloperastine phendizoate, dibutate sodium, dimemorphan phosphate, tipepidine citrate, And tipepidine hibenzate.

Examples of noscapine include noscapine hydrochloride and noscapine.
Examples of the bronchodilator include trimethquinol hydrochloride, phenylephrine hydrochloride, methoxyphenamine hydrochloride and the like.

  Examples of expectorants include ammonia, fennel, ammonium chloride and the like.

Examples of the hypnotic sedative include allyl isopropyl acetyl urea and bromovalerylurea.
Examples of vitamins include vitamin B ₁ , vitamin B ₂ , vitamin B ₅ , vitamin B ₆ , vitamin B ₁₂ , vitamin C, hesperidin and derivatives thereof, and salts thereof (for example, thiamine, thiamine chloride hydrochloride, Thiamine nitrate, dicetiamine hydrochloride, sethiamine hydrochloride, fursultiamine, fursultiamine hydrochloride, octothiamine, chicotiamine, thiamine disulfide, bisibutiamine, bisbenchamine, prosultiamine, benfotiamine, riboflavin, riboflavinline Acid ester, riboflavin butyrate, riboflavin sodium phosphate, panthenol, pantethine, sodium pantothenate, pyridoxine hydrochloride, pyridoxal phosphate, cyanocobalamin, mecobalamin, ascorbic acid, Sodium ascorbate, calcium ascorbate, hesperidin, etc.).

Examples of the gastric mucosa protective agent include gefarnate, cetraxate hydrochloride, sofalcone, teprenone, methylmethionine sulfonium chloride and the like.
Examples of antacids include aminoacetic acid, magnesium aluminate silicate, magnesium silicate, synthetic aluminum silicate, synthetic hydrotalcite, magnesium oxide, dihydroxyaluminum aminoacetate, magnesium alumina hydroxide, aluminum hydroxide gel, and dry. Aluminum hydroxide gel, aluminum hydroxide / magnesium carbonate mixed dry gel, aluminum hydroxide / sodium bicarbonate coprecipitation product, aluminum hydroxide / calcium carbonate / magnesium carbonate coprecipitation product, magnesium hydroxide, magnesium hydroxide・ Coprecipitation product of aluminum potassium sulfate, magnesium carbonate, sodium hydrogen carbonate, precipitated calcium carbonate, magnesium metasilicate aluminate, anhydrous calcium hydrogen phosphate, calcium hydrogen phosphate, bandit bone, Ke'Akira, Borei, and the like.

  Examples of the anticholinergic agents include oxyphencyclimine hydrochloride, dicyclomine hydrochloride, methixene hydrochloride, tipepidium bromide, methylbenactidium bromide, pirenzepine hydrochloride, isopropamide iodide, diphenylpiperidinomethyldioxolane iodide, and the like. Can be mentioned.

  Herbal medicines include, for example, Akamegashiwa (red buds), Asenyaku (Asenyaku), Arnica, Yinakukaku (Ryokan), Fennel (Yellow), Turmeric (Yongin), Engosaku (Yangxiao), Ogon (Yellow), Ousei ( Yellow spirit), Owaku (yellow jade), Spruce (cherry bark), Oulen (Yelen), Onji (distance), Gajutsu (weather), Valerian (deer herb), Chamomile, Caronin (Karojin), Kyokyo (kikyo) , Kyonin (Kyojin), Kukoshi (Reiko), Kukoyo (Kashihaha), Keigai (Kashiwagi), Keihi (Katsuhashi), Ketsumeishi (Kemeko), Gentiana, Gennoshouko (current evidence), Kouka (Safflower), Koubushi (Katsukiko) ), Gooh (beef yellow), trash (gomiko), saishin (spicy), sanshishi (yamashiko), sansho (yamashiro), sion (purple potato), dicoppi (skin), sicon (purple) Peonies (gakuyaku), musks (scented incense), shajin (shasan), shazenshi (car front child), shazensou (car front grass), beast gall (including yutan (bear gall)), ginger (ginger), giryu (earth dragon) ), Shinyi (Pepper), Horse Chestnut, Sexan (Ishibuchi), Senega, Senkyu (Ryukyu), Zenko (Mae-Hu), Senburi (Senshu), Sojutsu (蒼朮), Sohakuhi (Mulberry white skin), Soyo (Su) Leaf), Taisan (Daegu), Chixetsu carrot (Bamboo ginseng), chimpi (Chen), Toki (Tochigi), Tokon (Nangen), Nantenjitsu (Minami Tenjin), Carrot (Ginseng), Baimo (shellfish mother), Bakumondou (Bakumon winter), Hange (half-summer), Bankou (Banka), Hampi (anti-nasal), Byakushi (white bean), Byakuju (white birch), Bukryu (茯苓), Button pi (peony skin), Yobai (Plum) Leather), Rokujo (deer) ) And the like of crude drugs and extracts thereof (extract, tincture, dry extract, etc.) and the like.

  Examples of Kampo prescriptions include Keishito (Katsura-yu), Kousosan (Kousosan), Psycho-keito (Shibako), Bakumondou (Bakumontoyu), Hange Examples include Kokubokuto (half-summer Koboku-yu).

  In the present invention, the liquid or semi-solid composition may be blended with additives used in the pharmaceutical field, cosmetic field, etc. depending on the dosage form, administration method, etc. of the pharmaceutical preparation. Examples of such additives include gelling agents, polyhydric alcohols, fats and oils, emulsifiers, solubilizers, pH adjusters, antioxidants, softeners, thickeners, moisturizers, preservatives, stabilizers, Examples include transdermal absorption enhancers, taste-masking agents / sweeteners, and terpenes.

Examples of the gelling agent include acrylic acid polymers such as carboxyvinyl polymer; water-soluble or water-swellable cellulose polymers such as hydroxyethylcellulose, hydroxypropylcellulose, hydroxypropylmethylcellulose, methylcellulose, and ethylcellulose; polyvinyl alcohol; Polyvinyl pyrrolidone etc. are mentioned.
Examples of the polyhydric alcohol include glycerin, ethylene glycol, propylene glycol, 1,3-butylene glycol, macrogol, and polypropylene glycol.
Examples of the fats and oils include hydrocarbons such as squalane, paraffin, liquid paraffin, light liquid paraffin, petrolatum; fatty acid esters such as isopropyl myristate and octyldodecyl myristate; behenyl alcohol, lauryl alcohol, myristyl alcohol, Higher alcohols such as cetyl alcohol, stearyl alcohol, isostearyl alcohol, oleyl alcohol; higher fatty acids such as behenic acid, lauric acid, myristic acid, stearic acid, isostearic acid, oleic acid; carnauba wax, whale wax, shellac, jojoba oil, Waxes such as beeswax, white beeswax, montan wax, lanolin, purified lanolin, and reduced lanolin; silicone oil and the like.

Examples of the emulsifier include polyhydric alcohols such as propylene glycol monofatty acid ester, ethylene glycol monofatty acid ester, glycerin monofatty acid ester, polyglycerin fatty acid ester, sorbitan fatty acid ester, sucrose fatty acid ester, methylglucoside fatty acid ester, and alkylpolyglucoside. Fatty acid ester or polyhydric alcohol alkyl ether; polyoxyethylene ether such as polyoxyethylene alkyl ether, polyoxyethylene alkylphenyl ether, polyoxyethylene phytosterol, polyoxyethylene phytostanol, polyoxyethylene polyoxypropylene alkyl ether; polyoxy Ethylene monofatty acid ester, polyethylene glycol difatty acid ester, polyoxyethylene Lysine fatty acid ester, polyoxyethylene sorbitan fatty acid ester, polyoxyethylene sorbitol fatty acid ester, polyoxyethylene methyl glucoside fatty acid ester, polyoxyethylene hydrogenated castor oil, polyoxyethylene castor oil, polyoxyethylene vegetable oil, polyoxyethylene alkyl ether fatty acid Examples thereof include nonionic surfactants such as esters and ether esters such as polyoxyethylene polyoxypropylene glycol, or ionic surfactants such as sodium lauryl sulfate and sodium cetyl sulfate.
Examples of the solubilizer include glycerin, liquid paraffin, crotamiton, macrogol and the like in addition to the nonionic surfactant or ionic surfactant exemplified as the emulsifier.

Examples of the pH adjuster include citric acid, sodium citrate, anhydrous citric acid, malic acid, maleic acid, succinic acid, fumaric acid, tartaric acid, sodium tartrate, lactic acid, calcium lactate, sodium lactate, acetic acid, sodium acetate, ice Organic acids such as acetic acid or salts thereof; inorganic acids or salts thereof such as hydrochloric acid, sulfuric acid, phosphoric acid, sodium hydrogen phosphate, potassium dihydrogen phosphate, sodium dihydrogen phosphate, sodium carbonate, sodium hydrogen carbonate; sodium hydroxide And alkali hydroxides such as potassium hydroxide, calcium hydroxide and magnesium hydroxide; amines such as triethanolamine, diethanolamine and diisopropanolamine.
Examples of the antioxidant include sodium sulfite, ascorbic acid, sodium hydrogen sulfite, sodium sulfite, sodium edetate, erythorbic acid, cysteine hydrochloride, citric acid, tocopherol, tocopherol acetate, soybean lecithin, propyl gallate and the like.
Examples of the softener include allantoin, almond oil, olive oil, glycerin, liquid paraffin, squalane, squalene, purified lanolin, medium chain fatty acid triglyceride, rapeseed oil, castor oil, propylene glycol, polybutene and the like.
Examples of the thickener include polyvinylpyrrolidone, carboxymethylcellulose, colloidal aluminum silicate, xanthan gum, locust bean gum, tragacanth gum, guar gum, gelatin, gum arabic, alginic acid, albumin and the like.
Examples of the humectant include sodium hyaluronate, glycerin, 1,3-butylene glycol, propylene glycol, urea, sucrose, erythritol, sorbitol and the like.
Examples of preservatives include methyl paraoxybenzoate, ethyl paraoxybenzoate, propyl paraoxybenzoate, isopropyl paraoxybenzoate, butyl paraoxybenzoate, isobutyl paraoxybenzoate, benzyl paraoxybenzoate, sodium benzoate, benzoic acid, benzoic acid Examples thereof include benzyl acid, benzalkonium chloride, cetylpyridinium chloride, benzethonium chloride, aminoethylsulfonic acid and the like.
Examples of the stabilizer include adipic acid, ascorbic acid, sodium sulfite, sodium hydrogen sulfite, sodium chloride, hydrogenated oil, cysteine and the like.
Examples of the transdermal absorption enhancer include fatty acid esters such as diisopropyl adipate.
Examples of the corrigent and sweetener include acesulfame potassium, stevia, thaumatin, sucralose, panose, trehalose, erythritol, lactitol, reduced palatinose, coupling sugar, fructooligosaccharide, galactooligosaccharide, dairy oligosaccharide, isomaltoligosaccharide, palatinose. Examples include oligosaccharide, raffinose, aspartame, fructose, xylitol, brown sugar, saccharin or a salt thereof, sorbitol, lactose, sucrose, honey, glucose, maltitol, maltose, mannitol, water candy and the like.

  Terpenes include, for example, isoborneol, iron, osimene, carbeol, carbotane seton, carbomenton, carvone, caren, caron, camphene, camphor, geraniol, sabinene, safranal, cyclocitral, citral, citronellal, citronellic acid, citronellol, cineol , Cymen, Silvestrene, Thymol, Isotjojol, Tujon, Terpineol, Terpinene, Terpinolene, Tricyclene, Nellore, Pinene, Pinoccampheol, Pinol, Piperithenone, Ferrandral, Ferrandren, Fentchen, Fentyl alcohol, Perillyl alcohol, Perylaldehyde, borneol, myrcene, menthol, menthone, yonor, yonon, linalool, limonene, etc. That.

  Examples of essential oils containing terpenes include anise oil, ylang ylang oil, iris oil, fennel oil, orange oil, cananga oil, chamomile oil, kayap oil, caraway oil, kubeb oil, grapefruit oil, cinnamon oil, coriander oil, Saffron oil, salamander oil, perilla oil, citriodora oil, citronella oil, ginger oil, gingergrass oil, gingergrass oil, spearmint oil, mint oil, geranium oil, daikyo oil, clove oil, turpentine oil, spruce Oil, neroli oil, basil oil, peppermint oil, palmarosa oil, pimento oil, petitgren oil, bay oil, peniroyal oil, henoposi oil, bergamot oil, bored rose oil, pepper oil, marjolan oil, mandarin oil, melissa oil, eucalyptus oil, Lime oil, lavender oil, linaloe , Lemon oil, lemon grass oil, rose oil, rosemary oil, and Roman chamomile oil, and the like.

  In the present invention, the method for producing a liquid or semi-solid composition is not particularly limited, and the type and amount of components to be blended, the composition properties, the shape of the container, the dosage form of the pharmaceutical preparation, the administration route, the use, etc. Accordingly, it can be produced by a known method described in, for example, the 16th revised Japanese Pharmacopoeia General Rules for Preparations.

<Polyolefin resin container>
In the present invention, the “container” means a package that directly contains a liquid or semi-solid composition. The shape of the container is not particularly limited as long as it can accommodate a liquid or semi-solid composition, and should be appropriately examined according to the properties of the composition, the dosage form of the pharmaceutical preparation, the administration route, the use, etc. Just decide.
Examples of the shape of such a container include an aerosol agent container, a pump spray agent container, and a bottle container (more specifically, for example, a bottle container having a sponge-like application member (head), a roll-on container, and a jar bottle container. Etc.), tube containers, eye drop containers and the like. These containers are all known and may be manufactured by a known method, or commercially available products may be used.

In the present invention, as a container, the following (1) or (2):
(1) A container that includes a container body and an application member, such as a bottle container including a sponge-like application member, and is used by impregnating the application member with the composition contained in the container body;
(2) A container comprising a flexible container body and a discharge port, such as a tube container;
The container of the embodiment (1) is particularly preferable.

[(1) A container that includes a container body and an application member, and is used by impregnating the application member with a composition contained in the container body]
In the case of such a container, the composition can be applied by impregnating and holding the composition contained in the container main body in the application member and bringing the application member into contact with the portion to be applied. In this case, the container body and the application member may be prepared as independent members, and then the application member may be attached to the container body, or may be integrally molded.
The application member only needs to have a configuration capable of impregnating and holding a liquid or semi-solid composition, and examples thereof include a porous member such as a sponge or a brush-like member.

Examples of such a container include a container that is provided with an application member at the mouth of a container body, and that is used by impregnating the application member with a composition contained in the container body.
As a more specific example, for example, a container provided with a container main body having a mouth portion and a porous (sponge-like, etc.) application member attached to the mouth portion can be cited. In this case, the composition accommodated in the container body is impregnated and held in a porous application member whose pore diameter, porosity, etc. are appropriately adjusted, and then the application member is brought into contact with the portion to be applied, thereby forming the composition. A thing can be apply | coated to a to-be-coated part.
As another specific example, for example, a container including a container body having a mouth portion and a brush-like application member attached to the mouth portion can be given. In this case, the composition contained in the container body is impregnated and held in a brush whose hair length and spacing are appropriately adjusted, and then the coating member is brought into contact with the portion to be coated. It can apply | coat to to-be-coated part.

Since the container of such an embodiment is used by impregnating and holding the composition in the application member, for example, when the pharmaceutical preparation is an external application agent, the problem of dripping does not easily occur in the applied part, and the application member is directly applied. Advantages such as that the finger is not soiled by using it in contact with the part to be coated, or that the area where the composition is applied can be adjusted flexibly by adjusting the shape and size of the coating member. Have. However, since the composition is impregnated and retained in the application member, when the composition is discolored, the entire application member is discolored. Therefore, for example, when the application member is exposed to the outside, such as when using a pharmaceutical preparation, discoloration is particularly noticeable in appearance. However, according to the present invention, since the discoloration of the composition is suppressed, it has an excellent effect that the above-mentioned merit can be fully enjoyed by solving such a problem in appearance. In the case of such a container, it is particularly preferable that the container body and the coating member are both made of a polyolefin resin.
In addition, such a container can be particularly suitably employed when the composition to be contained is, for example, a liquid composition or a low-viscosity semisolid composition.

  Such a container is known and disclosed in, for example, Japanese Patent No. 5570089. In the present invention, a commercially available product may be used as the container of such an embodiment. As such a commercially available product, for example, MAPS (Inoac Co., Ltd.), which is a continuous porous body made of low density polyethylene as an application member, is used. And a container using (corporation).

[(2) Container provided with flexible container body and discharge port]
In the case of such a container, the composition is applied to the portion to be applied by applying pressure to the inside of the container by pressing a flexible container body and discharging the composition contained in the container from the discharge port. Can be applied. In such a container, the discharge port may not be provided in the container in advance, and the container may be provided with a discharge port by perforating the container before the start of use. And a container having a container body and a discharge port.

The container of such an aspect has a simple structure and low manufacturing cost, and the composition in the container is not contaminated because it is used by discharging the composition from the discharge port by pressing the container body. Have
In addition, the container of such an embodiment can be particularly suitably employed when the composition to be contained is, for example, a highly viscous semi-solid composition.

  The container of such an aspect is publicly known, for example, is disclosed in Japanese Patent No. 5302550, Japanese Patent No. 5525135, and the like. Moreover, in this invention, you may use a commercial item as a container of such an aspect.

In the present invention, the “polyolefin resin” is not particularly limited, and may be a polymer of a single type of monomer (homopolymer) or a copolymer of a plurality of types of monomers (copolymer). In the case of a copolymer, the polymerization mode is not particularly limited, and may be random polymerization or block polymerization. Furthermore, the stereoregularity (tacticity) is not particularly limited.
Specific examples of such polyolefin resins include polyethylene (more specifically, for example, low density polyethylene (including linear low density polyethylene), high density polyethylene, medium density polyethylene, etc.), polypropylene, and cyclic. Polyolefin, poly (4-methylpentene), polytetrafluoroethylene, ethylene / propylene copolymer, ethylene / α-olefin copolymer, ethylene / acrylic acid copolymer, ethylene / methacrylic acid copolymer, ethylene / acetic acid Examples thereof include vinyl copolymers and ethylene / ethyl acrylate copolymers. In the present invention, these can be used alone or in combination.
In the present invention, as the polyolefin-based resin, polyethylene, polypropylene, and cyclic polyolefin are preferable, and polyethylene and polypropylene are particularly preferable from the viewpoint of discoloration suppressing action.
In the present invention, “made of polyolefin resin” means that at least a part of the material contains a polyolefin resin, and, for example, two or more resins of a polyolefin resin and another resin (Polyolefin alloy) is also included in the “made of polyolefin resin”.

In the present invention, the “polyolefin-based resin container” means at least a part of a portion in contact with the liquid or semi-solid composition contained in the container (preferably the composition during normal storage) 10% or more of the part in contact with the composition, more preferably 30% or more of the part in contact with the composition during normal storage, particularly preferably the whole part in contact with the composition during normal storage) It means “container” which is “resin”. Therefore, for example, a polyolefin-based resin layer is provided on at least a part of the layer (innermost layer of the container) in contact with the liquid or semi-solid composition, and another material such as resin or aluminum foil is laminated on the outside. The container formed is also a “polyolefin resin container”.
As such a container formed by laminating a plurality of types of materials, specifically, for example, a layer composed of a polyolefin-based resin is used as an innermost layer, and an aluminum foil is formed directly on the outside or via another layer. And a laminate film container or the like formed by laminating other layers on the outer side of the layer as necessary.

  In the present invention, the means for accommodating the liquid or semi-solid composition in the container is not particularly limited, and it may be filled by a conventional method according to the shape of the container and the properties of the composition. Thus, the pharmaceutical preparation of the present invention can be produced.

<Pharmaceutical formulation>
In the present invention, the administration method and application method of the “pharmaceutical preparation” are not particularly limited, and examples thereof include oral and parenteral such as transdermal and vaginal. In the present invention, parenteral is preferable because of the characteristics of the liquid or semi-solid composition (the point that it can be flexibly applied in a necessary amount depending on the position, shape and range of the affected area). Skin administration is particularly preferred.

In the present invention, the dosage form of the pharmaceutical preparation is not particularly limited as long as the composition contained in the container is liquid or semi-solid, and depending on the purpose of use, for example, the 16th revision It can be appropriately selected from the dosage forms described in the Japanese Pharmacopoeia General Rules for Preparations. Specifically, such dosage forms include, for example, preparations for application to the skin (external solutions, sprays, ointments, creams, gels, etc.), orally administered preparations (oral liquids, syrups, oral jelly preparations). Etc.) and the dosage forms described in the Japanese Pharmacopoeia General Rules for Preparations.
In the present invention, the pharmaceutical preparation is preferably a dosage form selected from the group consisting of an external solution, a spray, an ointment, a cream, and a gel, a liniment, a lotion, an external aerosol, a pump spray, A dosage form selected from the group consisting of ointments, creams and gels is more preferred, and a dosage form selected from the group consisting of lotions, ointments, creams and gels is particularly preferred.

  Since the pharmaceutical preparation of the present invention contains loxoprofen, which is a kind of NSAID, or a salt thereof, it can be used as a medical drug or an OTC drug. Specifically, for example, an external anti-inflammatory analgesic; an antipyretic analgesic, a general cold It is useful as an internal medicine such as a medicine (cold medicine).

Next, the invention of the “method” aspect will be described below.
The present invention includes the following components (A) and (B):
(A) Loxoprofen or a salt thereof;
(B) Capsicum or an extract thereof;
The present invention also relates to a method for suppressing discoloration of a composition, which comprises a step of containing a liquid or semi-solid composition containing a resin in a polyolefin resin container.
In the invention of such an embodiment, the order of the step of blending the component (A), the step of blending the component (B), and the step of storing the composition in a polyolefin resin container is not particularly limited, and the component (A) And the state by which the liquid or semisolid composition containing (B) was accommodated in the polyolefin resin container should just be produced directly or indirectly.
In the aspect of the invention, the meanings of various words, the blending amount of each component, and the like are all the same as those described for the “pharmaceutical preparation”.

Although this specification discloses the invention illustrated below, for example in relation to the above embodiment, it is not limited to these at all.
[1] The following components (A) and (B):
(A) Loxoprofen or a salt thereof;
(B) Capsicum or an extract thereof;
A pharmaceutical preparation in which a liquid or semi-solid composition containing is contained in a polyolefin resin container.
[2] The pharmaceutical preparation according to [1], wherein component (A) is loxoprofen sodium hydrate.
[3] Component (B) is at least one selected from the group consisting of pepper, pepper powder, pepper soft extract, dried pepper extract, capsaicin and nonanoic acid vanillylamide (nonylic acid vanillylamide), [1] or [2 ] Pharmaceutical formulation of description.
[4] The pharmaceutical preparation according to [1] or [2], wherein the component (B) is at least one selected from the group consisting of soft pepper extract and nonanoic acid vanillylamide (nonylic acid vanillylamide).

[5] The pharmaceutical preparation according to any one of [1] to [4], wherein the composition further contains water.
[6] The pharmaceutical preparation according to any one of [1] to [5], wherein the composition further contains a lower alcohol.
[7] The pharmaceutical preparation according to [6], wherein the lower alcohol is one or more selected from the group consisting of ethanol and isopropanol.
[8] The pharmaceutical preparation according to any one of [1] to [7], wherein the polyolefin resin is one or more selected from the group consisting of polyethylene and polypropylene.
[9] The pharmaceutical preparation according to any one of [1] to [8], wherein the container is an aerosol container, a pump spray container, a bottle container, a tube container, or an eye drop container.
[10] The container has the following (1) or (2):
(1) A container that includes a container body and an application member, and is used by impregnating the application member with a composition contained in the container body;
(2) A container comprising a flexible container body and a discharge port;
The pharmaceutical preparation according to any one of [1] to [8].
[11] The pharmaceutical preparation according to any one of [1] to [8], wherein the container is a bottle container provided with a sponge-like application member or a tube container.
[12] The agent according to any one of [1] to [11], which is a dosage form selected from the group consisting of an externally applied solution, spray, ointment, cream, gel, oral solution, syrup and oral jelly. Pharmaceutical formulation.
[13] The pharmaceutical preparation according to any one of [1] to [11], which is a dosage form selected from the group consisting of an external solution, a spray, an ointment, a cream, and a gel.
[14] The pharmaceutical preparation according to any one of [1] to [11], which is a dosage form selected from the group consisting of a liniment, a lotion, an aerosol, a pump spray, an ointment, a cream, and a gel.
[15] The pharmaceutical preparation according to any one of [1] to [11], which is a dosage form selected from the group consisting of lotions, ointments, creams and gels.

[16] The following components (A) and (B):
(A) Loxoprofen or a salt thereof;
(B) Capsicum or an extract thereof;
The method of suppressing discoloration of a composition including the process of accommodating the liquid or semisolid composition containing this in a polyolefin resin container.
[17] The method according to [16], wherein the component (A) is loxoprofen sodium hydrate.
[18] The component (B) is at least one selected from the group consisting of pepper, pepper powder, pepper soft extract, dried pepper extract, capsaicin, and nonanoic acid vanillylamide (nonyl acid vanillylamide), [16] or [17 The method described.
[19] The method according to [16] or [17], wherein the component (B) is at least one selected from the group consisting of a red pepper soft extract and nonanoic acid vanillylamide (nonylic acid vanillylamide).

[20] The method according to any one of [16] to [19], wherein the composition further contains water.
[21] The method according to any one of [16] to [20], wherein the composition further comprises a lower alcohol.
[22] The method according to [21], wherein the lower alcohol is one or more selected from the group consisting of ethanol and isopropanol.
[23] The method according to any one of [16] to [22], wherein the polyolefin resin is at least one selected from the group consisting of polyethylene and polypropylene.
[24] The method according to any one of [16] to [23], wherein the container is an aerosol container, a pump spray container, a bottle container, a tube container, or an eye drop container.
[25] The container has the following (1) or (2):
(1) A container that includes a container body and an application member, and is used by impregnating the application member with a composition contained in the container body;
(2) A container comprising a flexible container body and a discharge port;
The method according to any one of [16] to [23].
[26] The method according to any one of [16] to [23], wherein the container is a bottle container having a sponge-like application member or a tube container.

  EXAMPLES The present invention will be described in detail below with reference to examples, but the present invention is not limited to these examples.

[Test Example 1] Preservation test 1
A liquid composition containing the components and amounts shown in Table 1 was prepared and accommodated in a polyethylene or glass container to obtain pharmaceutical preparations of Example 1 and Comparative Examples 1 and 2, respectively.
The obtained various pharmaceutical preparations were stored in a dark place at 80 ° C. for 1 week, and the presence or absence of discoloration (yellowing) after storage for 3 days and after storage for 1 week was visually evaluated. The results were evaluated as ◯ when no discoloration occurred and x when discoloration occurred.
The results are shown in Table 1.

By comparing Comparative Example 1 (Polyethylene container accommodation) and Comparative Example 2 (Glass container accommodation), the discoloration after storage for 3 days is suppressed by accommodating the composition in a polyethylene container, and a slight discoloration inhibiting action is achieved. However, its action was not sufficient, and it was confirmed that discoloration occurred after storage for 1 week.
On the other hand, compared with Example 1 (capsicum soft extract blend, polyethylene container accommodation) and Comparative Example 1 (polyethylene container accommodation), the composition is further blended with a soft pepper extract and then accommodated in a polyethylene container. As a result, it was confirmed that discoloration after storage for 1 week was suppressed, and a sufficient discoloration suppressing effect was exhibited.

  From the above test results, a liquid or semi-solid composition containing loxoprofen or a salt thereof was further added with a red pepper or an extract thereof, and this was contained in a polyolefin resin container, thereby increasing the temperature. It became clear that discoloration during storage could be suppressed.

[Test Example 2] Preservation test 2
A liquid composition containing the components and amounts shown in Table 2 was prepared, and contained in a polyethylene or glass container to obtain pharmaceutical preparations of Example 2, Comparative Examples 3 and 4, respectively, as in Test Example 1. The method was evaluated for the presence or absence of discoloration after storage in a dark place at 80 ° C. for 3 days and 1 week.
The results are shown in Table 2.

  From the above test results, it was confirmed that discoloration during high-temperature storage was similarly suppressed even when nonanoic acid vanillylamide was contained instead of the red pepper soft extract.

[Test Example 3] Preservation test 3
A liquid composition containing the components and amounts shown in Table 3 was prepared, and contained in a polyethylene container to obtain a pharmaceutical preparation of Example 3, and in the dark at 80 ° C. for 1 week by the same method as in Test Example 1. The presence or absence of discoloration after storage was evaluated.
The results are shown in Table 3.

  From the above test results, even when ethanol was used in place of isopropanol as the lower alcohol, it was confirmed that discoloration was similarly suppressed during high-temperature storage.

  From the results of the above Test Examples 1 to 3, the liquid or semi-solid composition containing loxoprofen or a salt thereof was further incorporated with a red pepper soft extract, a red pepper represented by nonanoic acid vanillylamide or an extract thereof, and It was revealed that discoloration during high-temperature storage can be suppressed by housing in a polyolefin resin container.

[Test Example 4] Preservation test 4
A liquid composition containing the components and amounts shown in Table 4 was prepared, and contained in a polyethylene or glass container to obtain a pharmaceutical preparation of Example 4, Comparative Example 5, 6 or Reference Example 1, respectively. By the same method as in Example 1, the presence or absence of discoloration after storage for 2 weeks in a dark place at 80 ° C. was evaluated.
The results are shown in Table 4.

From the comparison between Comparative Example 5 and Reference Example 1 (without loxoprofen), the discoloration confirmed after storage at 80 ° C. for 2 weeks may be due to the incorporation of loxoprofen into the liquid composition. confirmed.
And compared with Example 4 and Comparative Example 5 (glass container accommodation) and Comparative Example 6 (nonanoic acid vanillylamide non-blending), nonanoic acid vanillylamide was further blended with the liquid composition, and the product made of polyethylene was used. It was confirmed that such discoloration can be suppressed by accommodating in a container.

[Test Example 5] Preservation test 5
A liquid composition containing the components and amounts shown in Table 5 was prepared and contained in a polypropylene container to obtain the pharmaceutical preparations of Examples 5 and 6, and in the dark at 80 ° C. in the same manner as in Test Example 1. The presence or absence of discoloration after storage for 2 weeks was evaluated.
The results are shown in Table 5.

  From the above test results, even when a polypropylene container was used as the polyolefin resin container instead of the polyethylene container, it was confirmed that discoloration was suppressed during high temperature storage.

[Test Example 6] Preservation test 6
A liquid composition identical to that contained in the pharmaceutical preparations of Examples 1 and 3 was prepared, and this was used as a continuous porous body made of low-density polyethylene (MAPS: ) INOAC Corporation) was impregnated and stored in a dark place at 80 ° C. for 1 week, but no obvious discoloration was observed in any of the compositions.

Production Example 1 (Lotion)
By a conventional method, a liquid composition (Prescription Examples 1 to 8) containing 100 g of the components and amount (g) shown in Table 6 below is produced, and a sponge-like polyurethane is formed at the mouth of a polypropylene container body. It accommodated in the bottle container equipped with the manufacture application member, and it was set as the pharmaceutical formulation (lotion agent) of manufacture example 1-1 to 1-8, respectively.

Production Example 2 (Lotion)
By a conventional method, a liquid composition (Prescription Examples 1 to 8) containing 100 g of the components and amount (g) described in Table 6 above was produced, and a sponge-like low-powder was formed in the mouth of the polyethylene container body. It accommodated in the bottle container equipped with the application member (MAPS: INOAC Corporation) made from a density polyethylene, and it was set as the pharmaceutical formulation (lotion agent) of manufacture example 2-1 to 2-8, respectively.

Production Example 3 (Lotion)
By a conventional method, a liquid composition (Prescription Examples 9 to 16) containing 100 g of the components and amounts (g) shown in Table 7 below was produced, and a sponge-like polyurethane was formed at the mouth of a polypropylene container body. It accommodated in the bottle container equipped with the manufacture application | coating member, and it was set as the pharmaceutical formulation (lotion agent) of manufacture example 3-1 to 3-8, respectively.

Production Example 4 (Lotion)
By a conventional method, a liquid composition (Prescription Examples 9 to 16) containing 100 g of the components and amounts (g) described in Table 7 above was produced, and a sponge-like low-powder was formed in the mouth of the polyethylene container body. It accommodated in the bottle container equipped with the application member (MAPS: INOAC Corporation) made from a density polyethylene, and it was set as the pharmaceutical formulation (lotion agent) of manufacture example 4-1 to 4-8, respectively.

Production Example 5 (Gel)
By a conventional method, a semi-solid composition (Prescription Examples 17 to 24) containing 100 g of the components and amount (g) described in Table 8 below is produced, and a film made of low-density polyethylene is used as the innermost layer. It is housed in a tube container (laminated tube) made of a laminated film in which an aluminum foil is laminated on the outer side (intermediate layer) and a film made of low density polyethylene is laminated on the outer side, and the pharmaceutical preparations of Production Examples 5-1 to 5-8 ( Gel agent).

Production Example 6 (ointment)
By a conventional method, a semi-solid composition (Prescription Examples 25 to 32) containing 100 g of the components and amount (g) described in Table 9 below was produced, and a film made of high-density polyethylene was used as the innermost layer. The film is made of a polyethylene terephthalate film on the outer side (intermediate layer) and further laminated in a tube container (laminated tube) made of a high-density polyethylene film on the outer side. It was set as the pharmaceutical formulation (ointment).

Production Example 7 (Cream)
By a conventional method, a semi-solid composition (Prescription Examples 33 to 40) containing 100 g of the components and amount (g) shown in Table 10 below is produced, and a film made of low-density polyethylene is used as the innermost layer. It is housed in a tube container (laminated tube) made of a laminate film in which a nylon film is laminated on the outside (intermediate layer) and a low density polyethylene film is laminated on the outside, and the pharmaceuticals of Production Examples 7-1 to 7-8, respectively. It was set as the formulation (cream agent).

Production Example 8 (oral solution)
According to a conventional method, liquid compositions (formulation examples 41 to 48) containing the components and amounts (mg) described in Table 11 below in 30 mL are prepared and accommodated in polypropylene bottle containers. It was set as the pharmaceutical formulation (oral solution) of -1-8-8.

  ADVANTAGE OF THE INVENTION According to this invention, the discoloration at the time of high temperature preservation | save of the liquid or semisolid composition containing loxoprofen or its salt can be suppressed. Therefore, a drug containing loxoprofen or a salt thereof having excellent storage stability can be provided and can be suitably used in the pharmaceutical industry and the like.

Claims (8)

The following components (A) and (B):
(A) Loxoprofen or a salt thereof;
(B) Capsicum or an extract thereof;
A pharmaceutical preparation in which a liquid or semi-solid composition containing is contained in a polyolefin resin container.   The pharmaceutical preparation according to claim 1, wherein the component (B) is at least one selected from the group consisting of pepper, pepper powder, pepper soft extract, dried pepper extract, capsaicin and nonanoic acid vanillylamide.   The pharmaceutical preparation according to claim 1 or 2, wherein the component (B) is at least one selected from the group consisting of a red pepper soft extract and nonanoic acid vanillylamide.   The pharmaceutical preparation according to any one of claims 1 to 3, wherein the polyolefin resin is at least one selected from the group consisting of polyethylene and polypropylene.   The pharmaceutical preparation according to any one of claims 1 to 4, wherein the container is an aerosol container, a pump spray container, a bottle container, a tube container or an eye drop container. The container is the following (1) or (2):
(1) A container that includes a container body and an application member, and is used by impregnating the application member with a composition contained in the container body;
(2) A container comprising a flexible container body and a discharge port;
The pharmaceutical formulation of any one of Claims 1-4 which is.   The pharmaceutical preparation according to any one of claims 1 to 4, wherein the container is a bottle container or a tube container provided with a sponge-like application member.   The pharmaceutical preparation according to any one of claims 1 to 7, which is a dosage form selected from the group consisting of an external preparation, a spray, an ointment, a cream, a gel, an oral solution, a syrup, and an oral jelly.