JP2008231081A - Ketoprofen-containing external preparation - Google Patents
Ketoprofen-containing external preparation Download PDFInfo
- Publication number
- JP2008231081A JP2008231081A JP2007077504A JP2007077504A JP2008231081A JP 2008231081 A JP2008231081 A JP 2008231081A JP 2007077504 A JP2007077504 A JP 2007077504A JP 2007077504 A JP2007077504 A JP 2007077504A JP 2008231081 A JP2008231081 A JP 2008231081A
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- JP
- Japan
- Prior art keywords
- ketoprofen
- acid
- external preparation
- concentration
- weight
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
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Abstract
Description
本発明は、有効成分としてケトプロフェンを含有する関節リウマチの痛みに対する鎮痛効果を有する外用剤に関する。 The present invention relates to an external preparation having an analgesic effect on pain of rheumatoid arthritis containing ketoprofen as an active ingredient.
非ステロイド系消炎鎮痛剤は、変形性関節症、変形性脊椎症、腰痛などに広く用いられ(特許文献1)、その代表的なものとしてケトプロフェンが挙げられる。また、ケトプロフェンを消炎鎮痛剤の有効成分として用いた貼付剤が知られている(特許文献2および3)。
しかし、非ステロイド系消炎鎮痛剤を有効成分とする関節リウマチの痛みに対する鎮痛効果を有する外用剤の具体例は、これまで知られていない。これは、関節リウマチの治療薬、とくに外用剤においては、どの程度経皮を介して患部に移行すればよいかが明らかでなく、結果的に関節リウマチの痛みに効果を有する外用剤の開発が困難であったことが一因であった。
Nonsteroidal anti-inflammatory analgesics are widely used for osteoarthritis, osteoarthritis, low back pain, etc. (Patent Document 1), and representative examples thereof include ketoprofen. In addition, a patch using ketoprofen as an active ingredient of an anti-inflammatory analgesic is known (Patent Documents 2 and 3).
However, a specific example of an external preparation having an analgesic effect on rheumatoid arthritis pain comprising a nonsteroidal anti-inflammatory analgesic as an active ingredient has not been known so far. This is because it is not clear how much rheumatoid arthritis treatment, especially topical preparations, should be transferred to the affected area through the skin, and as a result, it is difficult to develop external preparations effective for rheumatoid arthritis pain. It was partly because it was.
本発明の課題は、新たに、ケトプロフェンを有効成分とする関節リウマチの痛みに対する鎮痛効果を有する外用剤を提供することにある。 The subject of this invention is providing the external preparation which has the analgesic effect with respect to the pain of rheumatoid arthritis which uses ketoprofen as an active ingredient newly.
本発明者らは、上記課題を解決すべく鋭意研究を重ねる中で、筋肉や腱などの組織中の消炎鎮痛剤の濃度を所定濃度以上に保ち、かつ、その所定濃度が長時間持続する薬物動態を実現できれば、関節リウマチの疼痛抑制に効果的であることを見出し、さらに研究を進めた結果、本発明を完成した。 In the course of earnest research to solve the above problems, the present inventors maintain a concentration of anti-inflammatory analgesic in tissues such as muscles and tendons at a predetermined concentration or more, and the predetermined concentration is a drug that lasts for a long time As a result of further research, it was found that if the kinetics can be realized, it is effective in suppressing pain in rheumatoid arthritis, and the present invention was completed.
すなわち、本発明は、投与後の筋肉内および/または腱内のケトプロフェン濃度が、30ng/g以上に達する、関節リウマチの痛みに対する鎮痛効果を有するケトプロフェン含有外用剤に関する。
さらに本発明は、筋肉内および/または腱内のケトプロフェン濃度が30ng/g以上に達してから、少なくとも投与14時間後まで前記濃度が30ng/g以上である、前記のケトプロフェン含有外用剤に関する。
また本発明は、投与1時間後の筋肉内および/または腱内のケトプロフェン濃度が、30ng/g以上である、前記のケトプロフェン含有外用剤に関する。
さらに本発明は、投与後、血漿中のケトプロフェン濃度が500ng/mLを超えない、前記のケトプロフェン含有外用剤に関する。
また本発明は、貼付剤である、前記のケトプロフェン含有外用剤に関する。
さらに本発明は、ケトプロフェン含有外用剤であって、上記のケトプロフェン含有外用剤と、生物学的同等性試験においてバイオアベイラビリティが同等である、前記ケトプロフェン含有外用剤に関する。
That is, the present invention relates to a ketoprofen-containing external preparation having an analgesic effect on rheumatoid arthritis pain, wherein the concentration of ketoprofen in muscle and / or tendon after administration reaches 30 ng / g or more.
Furthermore, the present invention relates to the above-mentioned ketoprofen-containing external preparation, wherein the concentration is 30 ng / g or more until at least 14 hours after administration after the intramuscular and / or tendon ketoprofen concentration reaches 30 ng / g or more.
The present invention also relates to the ketoprofen-containing external preparation described above, wherein the concentration of ketoprofen in muscle and / or
Furthermore, the present invention relates to the above-mentioned ketoprofen-containing external preparation, wherein the ketoprofen concentration in plasma does not exceed 500 ng / mL after administration.
Moreover, this invention relates to the said ketoprofen containing external preparation which is a patch.
Furthermore, the present invention relates to a ketoprofen-containing external preparation, which is a ketoprofen-containing external preparation and has the same bioavailability in the bioequivalence test as that of the above-mentioned ketoprofen-containing external preparation.
本発明の外用剤は、患部に投与(塗布、貼付、噴霧など)した後、有効量以上のケトプロフェンが筋肉組織や腱に到達することによって関節リウマチ疼痛に有効な効果を奏する。さらに本発明の外用剤は、全身血中濃度が経口剤に比べ低いためより安全であり、また外用剤、とくに貼付剤であることにより、より簡便で、よりコンプライアンスの高い関節リウマチ疼痛抑制治療薬を提供することができる。 The external preparation of the present invention has an effective effect on rheumatoid arthritis pain when administered to an affected area (application, sticking, spraying, etc.) and then an effective amount or more of ketoprofen reaches the muscle tissue or tendon. Furthermore, the external preparation of the present invention is safer because the systemic blood concentration is lower than that of the oral preparation, and it is a simpler and more compliant therapeutic agent for rheumatoid arthritis pain because it is an external preparation, particularly a patch. Can be provided.
以下、本発明の外用剤の好適な実施について詳細に説明する。
本発明の外用剤は、関節リウマチ疼痛の抑制効果の観点からみて、筋肉組織中において、ケトプロフェン濃度が、投与後、例えば投与1時間後に、30ng/g以上、とくに、40ng/g以上、とりわけ、50ng/g以上に達することが好ましい。さらにまた、投与後、少なくとも14時間、とくに20時間以上、当該所定濃度以上に維持されることがさらに好ましい。
Hereinafter, suitable implementation of the external preparation of the present invention will be described in detail.
From the viewpoint of the effect of suppressing rheumatoid arthritis, the external preparation of the present invention has a ketoprofen concentration of 30 ng / g or more, particularly 40 ng / g or more after administration, for example, 1 hour after administration, It is preferable to reach 50 ng / g or more. Furthermore, it is more preferable that the concentration is maintained at or above the predetermined concentration for at least 14 hours, particularly 20 hours or more after administration.
また腱組織中のケトプロフェン濃度としては、同じく投与後、例えば投与1時間後に、30ng/g以上、とくに、50ng/g以上、とりわけ、100ng/g以上に達することが好ましい。さらにまた、投与後、少なくとも14時間、とくに20時間以上、当該所定濃度以上に維持されることがさらに好ましい。
また本発明の外用剤は、副作用や身体への負担軽減などの観点から、ケトプロフェンを、血漿中において、投与後、500ng/mLを超えず、とくに、300ng/mLを超えず、とりわけ、200ng/mLを超えないことが好ましい。
Similarly, the ketoprofen concentration in the tendon tissue preferably reaches 30 ng / g or more, particularly 50 ng / g or more, particularly 100 ng / g or more after administration, for example, 1 hour after administration. Furthermore, it is more preferable that the concentration is maintained at or above the predetermined concentration for at least 14 hours, particularly 20 hours or more after administration.
Moreover, the external preparation of the present invention does not exceed 500 ng / mL after administration of ketoprofen in plasma from the viewpoint of side effects and reduction of burden on the body, in particular, does not exceed 300 ng / mL, and in particular, 200 ng / mL. It is preferred not to exceed mL.
そして、ケトプロフェンの前記組織中濃度、血漿中濃度により、外用剤として、関節リウマチの痛みに対する鎮痛効果を奏することができる。
本発明の外用剤は、経皮的に投与するものであれば、いかなる剤型でもよく、例えば、湿布剤またはプラスター剤といった貼付剤、液剤、ローション剤、クリーム剤、ゲル剤、軟膏剤、リニメント剤、スプレー剤などが挙げられる。とくに、十分な量の薬剤を長期間に亘って供給し続けるのに簡便であるため、貼付剤が好ましい。
And the analgesic effect with respect to the pain of rheumatoid arthritis can be show | played as an external preparation by the density | concentration in the said structure | tissue and plasma of the ketoprofen.
The external preparation of the present invention may be in any dosage form as long as it is administered transdermally. For example, patches, liquids, lotions, creams, gels, ointments, liniments such as poultices or plasters. Agents, sprays and the like. In particular, a patch is preferred because it is convenient for supplying a sufficient amount of medicine for a long period of time.
以下に本発明の外用剤の各剤型に応じた基剤並びに処方例について説明する。
先ず、湿布剤またはプラスター剤といった貼付剤について説明する。本発明の貼付剤は、支持体、基剤(湿布基剤、プラスター基剤)、剥離シートからなり、基剤および/または支持体にはケトプロフェンが含まれる。
The bases and formulation examples according to each dosage form of the external preparation of the present invention will be described below.
First, a patch such as a poultice or a plaster will be described. The patch of the present invention comprises a support, a base (a poultice base, a plaster base), and a release sheet, and the base and / or the support contains ketoprofen.
湿布剤に用いられる湿布基剤としては、通常使用されているものの中より選択され、例えば、増粘剤(ポリアクリル酸ソーダ、ポリアクリル酸、ポリビニルアルコール、ポリビニルピロリドン、ポリエチレンオキサイド、ポリビニルメタアクリレート等の合成水溶性高分子、アラビアゴム、デンプン、ゼラチン等の天然物、メチルセルロース、ヒドロキシプロピルセルロース、アルギン酸、アルギン酸ナトリウム、アルギン酸アンモニウム、カルボキシメチルセルロースナトリウム等)、湿潤剤(尿素、グリセリン、ポリエチレングリコール、プロピレングリコール、ブチレングリコール、ソルビトール等)、充填剤(カオリン、タルク、ベンナイト、エポキシ樹脂類、有機酸(クエン酸、酒石酸、マレイン酸、無水マレイン酸、コハク酸等)、カルシウム、マグネシウム、アルミニウム等)、水、溶解補助剤(炭酸プロピレン、クロタミトン、ジイソプロピルアジペート等)、かぶれ防止剤(塩酸ジフェンヒドラミン、マレイン酸クロルフェニラミン、グリチルリチン酸、デキサメタゾン、ベタメタゾン、フルオシノロンアセトアニリド等)、その他の添加剤(サリチル酸、サリチル酸メチル、サリチル酸グリコール、l−メントール、カンフル、ノニル酸ワニリルアミド、トウガラシエキス、ハッカ油、エイゾン(登録商標)等)等が挙げられ、これらの中から選択される諸成分を混合してなる湿布基剤にケトプロフェンを配合することにより、本発明の湿布剤を得ることができる。 As the poultice base used in the poultice, it is selected from those usually used, for example, thickener (polyacrylic acid soda, polyacrylic acid, polyvinyl alcohol, polyvinylpyrrolidone, polyethylene oxide, polyvinyl methacrylate, etc. Synthetic water-soluble polymers, natural products such as gum arabic, starch, gelatin, methylcellulose, hydroxypropylcellulose, alginic acid, sodium alginate, ammonium alginate, sodium carboxymethylcellulose, etc., wetting agents (urea, glycerin, polyethylene glycol, propylene glycol) , Butylene glycol, sorbitol, etc.), fillers (kaolin, talc, bennite, epoxy resins, organic acids (citric acid, tartaric acid, maleic acid, maleic anhydride, succinic acid, etc.) , Calcium, magnesium, aluminum, etc.), water, solubilizers (propylene carbonate, crotamiton, diisopropyl adipate, etc.), anti-rash agents (diphenhydramine hydrochloride, chlorpheniramine maleate, glycyrrhizic acid, dexamethasone, betamethasone, fluocinolone acetanilide, etc. ), And other additives (salicylic acid, methyl salicylate, glycol salicylate, l-menthol, camphor, nonylic acid vanillylamide, red pepper extract, peppermint oil, Aison (registered trademark), etc.) and the like are selected. The poultice of the present invention can be obtained by blending ketoprofen into the poultice base formed by mixing various components.
次に、湿布剤の好適な一製造例(処方例)を示す。すなわち、先ず、ケトプロフェン0.1〜10重量部を溶解補助剤0.5〜8重量部に混合溶解し、均一な混合物Aを得る。一方、増粘剤5〜20重量部(好ましくは10〜15重量部)を湿潤剤5〜40重量部および水10〜80重量部に混合分散溶解し、さらに充填剤20重量部以下を加えて均一な練合物Bを得る。次いで、混合物Aを練合物Bに加えて混合し、均一な練合物を得る。得られた練合物を通常の方法で支持体上に展延塗布した後、その上に剥離シートを貼付することにより本発明の湿布剤が得られる。 Next, a suitable production example (formulation example) of the poultice is shown. That is, first, 0.1 to 10 parts by weight of ketoprofen is mixed and dissolved in 0.5 to 8 parts by weight of a solubilizing agent to obtain a uniform mixture A. On the other hand, 5 to 20 parts by weight (preferably 10 to 15 parts by weight) of a thickener is mixed and dispersed in 5 to 40 parts by weight of a wetting agent and 10 to 80 parts by weight of water, and further 20 parts by weight or less of a filler is added. A uniform kneaded product B is obtained. Next, the mixture A is added to the kneaded product B and mixed to obtain a uniform kneaded product. The obtained kneaded material is spread-coated on a support by a usual method, and then a release sheet is stuck thereon to obtain the poultice of the present invention.
なお、支持体としては、伸縮性または非伸縮性の支持体を用いることができる。かかる支持体としては、具体的には、織布、不織布、ポリウレタン、ポリエステル、ポリ酢酸ビニル、ポリ塩化ビニリデン、ポリエチレン、ポリエチレンテレフタレート、ポリブチレンテレフタレート、紙、アルミニウムシート、またはこれらの複合素材からなるもの等が挙げられる。とくにケトプロフェンの薬物吸着のないポリエチレンテレフタレートまたはポリブチレンテレフタレートからなるポリエステル布が好ましい。
また、剥離シートとしては、剥離処理を施した剥離紙、セロファン、ポリエチレン、ポリプロピレン、ポリ塩化ビニル、ポリエステル、ポリ塩化ビニリデン、シリコン加工紙からなるもの等が挙げられる。
In addition, as a support body, a stretchable or non-stretchable support body can be used. Specifically, the support is made of woven fabric, non-woven fabric, polyurethane, polyester, polyvinyl acetate, polyvinylidene chloride, polyethylene, polyethylene terephthalate, polybutylene terephthalate, paper, aluminum sheet, or a composite material thereof. Etc. In particular, a polyester cloth made of polyethylene terephthalate or polybutylene terephthalate free from ketoprofen drug adsorption is preferred.
Examples of the release sheet include release paper that has been subjected to release treatment, cellophane, polyethylene, polypropylene, polyvinyl chloride, polyester, polyvinylidene chloride, and silicon processed paper.
次に、プラスター剤について説明する。プラスター剤に用いられるプラスター基剤としては、通常使用されているものの中より選択され、例えば、高分子基剤(メタアクリル酸エステル類、アクリロニトリル、酢酸ビニル、プロピオン酸ビニル等のビニルモノマーとの共重合物であるアクリル系組成物、シリコン樹脂、ポリイソプレンゴム、天然ゴム、アクリルゴム、スチレン−ブタジエン−スチレンブロック共重合体、スチレン−イソプレン−スチレンブロック共重合体、スチレン−ブタジエン共重合体、ポリイソプレンおよびポリブタジエン等のゴム系高分子等)、油脂または高級脂肪酸(アーモンド油、オリーブ油、つばき油、パーシック油、ラッカセイ油、オレイン油、流動パラフィン、ポリブテン等)、粘着付与剤、脂肪酸金属塩(ウンデシレン酸亜鉛、ステアリン酸亜鉛、ステアリン酸カルシウム、ステアリン酸アルミニウム、ステアリン酸マグネシウム、ステアリン酸ナトリウム、パルミチン酸亜鉛、ミリスチン酸亜鉛、ミリスチン酸マグネシウム、ラウリン酸ナトリウム、ラウリン酸亜鉛等)、かぶれ防止剤、その他の添加物(サリチル酸、サリチル酸メチル、サリチル酸グリコール、l−メントール、カンフル、ノニル酸ワニリルアミド、トウガラシエキス、ハッカ油、エイゾン(登録商標)等)等が挙げられ、これらの中から選択される諸成分を混合してなるプラスター基剤にケトプロフェンを配合することにより、本発明のプラスター剤を得ることができる。 Next, the plaster agent will be described. The plaster base used for the plaster agent is selected from those usually used. For example, a polymer base (copolymer with a vinyl monomer such as methacrylic acid esters, acrylonitrile, vinyl acetate, vinyl propionate) is used. Acrylic composition which is a polymer, silicone resin, polyisoprene rubber, natural rubber, acrylic rubber, styrene-butadiene-styrene block copolymer, styrene-isoprene-styrene block copolymer, styrene-butadiene copolymer, poly Rubber polymers such as isoprene and polybutadiene), fats and oils or higher fatty acids (almond oil, olive oil, camellia oil, persic oil, peanut oil, olein oil, liquid paraffin, polybutene, etc.), tackifiers, fatty acid metal salts (undecylene) Zinc acid, stearic acid , Calcium stearate, aluminum stearate, magnesium stearate, sodium stearate, zinc palmitate, zinc myristate, magnesium myristate, sodium laurate, zinc laurate, etc., anti-rash agent, other additives (salicylic acid, salicylic acid) Methyl, salicylic acid glycol, l-menthol, camphor, nonylic acid vanillylamide, red pepper extract, peppermint oil, Azone (registered trademark), etc., and a plaster base formed by mixing various components selected from these The plaster agent of this invention can be obtained by mix | blending ketoprofen with.
前記高分子基剤としては、とくに、極性の低いスチレン−イソプレン−スチレンブロック共重合体が好ましい。スチレン−イソプレン−スチレンブロック共重合体を用いた場合には、質量平均分子量が100,000〜300,000であることが好ましく、例えばクレイトンD−KX401CSまたはD−1107CU(シェル化学株式会社製)、カリフレックスTR−1107、TR−1111、TR−1112、TR−1117(シェル化学株式会社製)、SIS−5000またはSIS−5002(日本合成ゴム株式会社製)、クインタック3530、3421または3570C(日本ゼオン株式会社製)、ソルプレン428(フイリップペトロリアム株式会社製)が挙げられる。基剤にはこれらスチレン−イソプレン−スチレンブロック共重合体を1種または2種以上配合することができる。また、前記ゴム系高分子に加えて、合成ゴムあるいは天然ゴムとしてポリイソプレンゴム、ポリイソブチレンゴム、天然ゴム、スチレン−イソプレン共重合体、スチレン−イソプレン−ブタジエンブロック共重合体、スチレン−エチレン−プロピレン−スチレンブロック共重合体等を配合してもよい。 As the polymer base, a styrene-isoprene-styrene block copolymer having a low polarity is particularly preferable. When a styrene-isoprene-styrene block copolymer is used, the mass average molecular weight is preferably 100,000 to 300,000. For example, Kraton D-KX401CS or D-1107CU (manufactured by Shell Chemical Co., Ltd.), Califlex TR-1107, TR-1111, TR-1112, TR-1117 (manufactured by Shell Chemical Co., Ltd.), SIS-5000 or SIS-5002 (manufactured by Nippon Synthetic Rubber Co., Ltd.), Quintac 3530, 3421 or 3570C (Japan) Zeon Co., Ltd.) and Sorprene 428 (Philip Petroleum Co., Ltd.). One or more of these styrene-isoprene-styrene block copolymers can be blended in the base. In addition to the rubber-based polymer, polyisoprene rubber, polyisobutylene rubber, natural rubber, styrene-isoprene copolymer, styrene-isoprene-butadiene block copolymer, styrene-ethylene-propylene as synthetic rubber or natural rubber -You may mix | blend a styrene block copolymer etc.
本発明に係る好ましいプラスター基剤は、スチレン−イソプレン−スチレンブロック共重合体等のゴム系高分子、ポリイソブチレン等のその他のゴム系高分子、粘着付与剤および可塑剤を含有するものである。 A preferable plaster base according to the present invention contains a rubber polymer such as a styrene-isoprene-styrene block copolymer, another rubber polymer such as polyisobutylene, a tackifier, and a plasticizer.
前記粘着付与剤としては、軟化点が60℃〜150℃のものが好ましく、例えばロジンエステル、水添ロジンエステル、マレイン酸変性ロジンエステル、テルペン樹脂、石油樹脂を用いることができ、特に水添ロジンエステル、テルペン樹脂、石油樹脂が好ましく、水添ロジンエステルおよびテルペン樹脂の組み合わせが最も好ましい。具体的にはエステルガムA、AA−G、H、またはHP(荒川化学株式会社製)、ハリエスターL、S、またはP(播磨化成株式会社製)、パインクリスタルKE−100、またはKE−311(荒川化学株式会社製)、ハーコリンD(理化ハーキュレス株式会社製)、フォーラル85、または105(理化ハーキュレス株式会社製)、ステベライトエステル7、または10(理化ハーキュレス株式会社製)、ペンタリン4820、または4740(理化ハーキュレス株式会社製)、アルコンP−85、またはP−100(荒川化学株式会社製)、エスコレッツ5300(エクソン化学株式会社製)、クリアロンK、M、またはP、YSレジン PX1000、PX1150またはPX1250(ヤスハラケミカル株式会社製)等が挙げられ、これらの1種または2種以上を粘着性基剤に配合することができる。 As the tackifier, those having a softening point of 60 ° C. to 150 ° C. are preferable. For example, rosin ester, hydrogenated rosin ester, maleic acid-modified rosin ester, terpene resin, and petroleum resin can be used. Esters, terpene resins and petroleum resins are preferred, and a combination of hydrogenated rosin ester and terpene resin is most preferred. Specifically, ester gum A, AA-G, H, or HP (made by Arakawa Chemical Co., Ltd.), Harrier Star L, S, or P (made by Harima Kasei Co., Ltd.), Pine Crystal KE-100, or KE-311 (Arakawa Chemical Co., Ltd.), Hercolin D (Rika Hercules Co., Ltd.), Foral 85 or 105 (Rika Hercules Co., Ltd.), Stevelite Ester 7 or 10 (Rika Hercules Co., Ltd.), Pentaline 4820, or 4740 (Rika Hercules Co., Ltd.), Alcon P-85, or P-100 (Arakawa Chemical Co., Ltd.), Escorez 5300 (Exxon Chemical Co., Ltd.), Clearon K, M, or P, YS Resin PX1000, PX1150 or PX1250 (made by Yashara Chemical Co., Ltd.) It can be blended one or more of these in adhesive base material.
前記可塑剤としては、溶液粘度が10〜100センチストークス(40℃)のものが好ましく、例えばアーモンド油、オリーブ油、ツバキ油、パーシック油、ラッカセイ油、オレフィン酸、流動パラフィンが挙げられ、これらを1種または2種以上粘着性基剤に配合することができる。 The plasticizer preferably has a solution viscosity of 10 to 100 centistokes (40 ° C.), and examples thereof include almond oil, olive oil, camellia oil, persic oil, peanut oil, olefinic acid, and liquid paraffin. It can mix | blend with a seed | species or 2 or more types of adhesive bases.
前記プラスター基剤は、従来公知の充填剤、酸化防止剤、溶解剤等を含有することができる。充填剤としては、たとえば酸化亜鉛、酸化アルミニウム、二酸化チタン、炭酸カルシウム、合成ケイ酸アルミニウム、シリカ類、酸化マグネシウム、ステアリン酸金属塩類等が用いられる。酸化防止剤としては、たとえばアスコルビン酸、酢酸トコフェロール、天然ビタミンE、ジブチルヒドロキシトルエン、没食子酸プロピル等が用いられる。溶解剤としては、たとえばオレイン酸、ベンジルアルコール、ミリスチン酸イソプロピル、クロタミトン、オレイルアルコール、ユーカリ油、リモネン、イソプレゴール、アジピン酸ジイソプロピル、セバシン酸ジエチルまたはその他の製油類が用いられる。また、界面活性剤、油脂、高級脂肪酸、着香剤等を必要に応じて含有することができる。更に、L−メントール、カンフル、ハッカ油、トウガラシエキス、カプサイシン、ニコチン酸ベンジル、サリチル酸メチル、サリチル酸グリコール等の皮膚刺激剤(カウンターイリタント)を必要に応じて適宜配合することもできる。 The plaster base may contain conventionally known fillers, antioxidants, solubilizers and the like. As the filler, for example, zinc oxide, aluminum oxide, titanium dioxide, calcium carbonate, synthetic aluminum silicate, silicas, magnesium oxide, stearic acid metal salts and the like are used. As the antioxidant, for example, ascorbic acid, tocopherol acetate, natural vitamin E, dibutylhydroxytoluene, propyl gallate and the like are used. As the solubilizer, for example, oleic acid, benzyl alcohol, isopropyl myristate, crotamiton, oleyl alcohol, eucalyptus oil, limonene, isopulegol, diisopropyl adipate, diethyl sebacate or other oil refiners are used. Moreover, surfactant, fats and oils, a higher fatty acid, a flavoring agent, etc. can be contained as needed. Furthermore, skin irritants (counteriritant) such as L-menthol, camphor, peppermint oil, pepper extract, capsaicin, benzyl nicotinate, methyl salicylate, glycol salicylate, etc. can be appropriately blended as necessary.
次に、プラスター剤の好適な一製造例(処方例)を示す。すなわち、先ず、ホットメルト法で製造する場合は、先ず、ニーダー、ミキサー等の混合機を用い120〜160℃で前記高分子基剤5〜40重量部、前記油脂または高級脂肪酸20〜70重量部、前記粘着付与剤10〜40重量部および前記脂肪酸金属塩0.1〜10重量部を加熱混合し、次いでケトプロフェン0.1〜10重量部を添加混合する。得られた混合物を、直接支持体上に展延するか、あるいは離型処理の施された紙、フィルム等の上に、一旦展延した後に所望の支持体を覆った状態として圧着転写させてもよい。他方、溶剤法で製造する場合は、防爆対応のミキサー等の混合機を用いて前記成分をトルエン、ヘキサン、塩化メチレン等の溶媒中で溶解し、得られた溶液を離型処理の施された紙、フィルム等の上に展延し、乾燥機で溶媒を留去させた後、所望の支持体を覆った状態として圧着転写させる。支持体上の展延塗布上に剥離シートを貼付することにより本発明のプラスター剤が得られる。 Next, a suitable production example (formulation example) of a plaster agent is shown. That is, first, in the case of producing by a hot melt method, first, 5 to 40 parts by weight of the polymer base, 20 to 70 parts by weight of the fat or higher fatty acid at 120 to 160 ° C. using a mixer such as a kneader or a mixer. Then, 10 to 40 parts by weight of the tackifier and 0.1 to 10 parts by weight of the fatty acid metal salt are heated and mixed, and then 0.1 to 10 parts by weight of ketoprofen is added and mixed. The obtained mixture is directly spread on a support, or on a paper, film, etc. that has been subjected to a release treatment, and after being spread, the desired support is covered and transferred by pressure. Also good. On the other hand, in the case of manufacturing by the solvent method, the above components were dissolved in a solvent such as toluene, hexane, methylene chloride using a mixer such as an explosion-proof mixer, and the resulting solution was subjected to a release treatment. After spreading on paper, film, etc., the solvent is distilled off with a drier, and then a pressure transfer is performed with the desired support covered. The plaster agent of the present invention is obtained by applying a release sheet on the spread coating on the support.
かかる支持体としては、具体的には、織布、不織布、ポリウレタン、ポリエステル、ポリ酢酸ビニル、ポリ塩化ビニリデン、ポリエチレン、ポリエチレンテレフタレート、ポリブチレンテレフタレート、紙、アルミニウムシート、またはこれらの複合素材からなるもの等が挙げられる。とくにケトプロフェンの薬物吸着のないポリエチレンテレフタレートまたはポリブチレンテレフタレートからなるポリエステル布が好ましい。
また、剥離シートとしては、剥離処理を施した剥離紙、セロファン、ポリエチレン、ポリプロピレン、ポリ塩化ビニル、ポリエステル、ポリ塩化ビニリデン、シリコン加工紙からなるもの等が挙げられる。
Specifically, the support is made of woven fabric, non-woven fabric, polyurethane, polyester, polyvinyl acetate, polyvinylidene chloride, polyethylene, polyethylene terephthalate, polybutylene terephthalate, paper, aluminum sheet, or a composite material thereof. Etc. In particular, a polyester cloth made of polyethylene terephthalate or polybutylene terephthalate free from ketoprofen drug adsorption is preferred.
Examples of the release sheet include release paper that has been subjected to release treatment, cellophane, polyethylene, polypropylene, polyvinyl chloride, polyester, polyvinylidene chloride, and silicon processed paper.
次に、軟膏剤について説明する。軟膏剤に用いられる軟膏基剤は、通常使用されているものの中より選択され、例えば、高級脂肪酸またはそれらのエステル類(アジピン酸、ミリスチン酸、パルミチン酸、ステアリン酸、オレイン酸、アジピン酸エステル、ミリスチン酸エステル、パルミチン酸エステル、セバシン酸ジエチル、ラウリン酸ヘキシル、イソオクタン酸セチル等)、ロウ類(鯨ロウ、ミツロウ、セシレン等)、界面活性剤(ポリオキシエチレンアルキルエーテルリン酸エステル等)、高級アルコール(セタノール、ステアリルアルコール、セトステアリルアルコール等)、シリコン油(ジメチルポリシロキサン、メチルフェニルポリシロキサン、グリコールメチルポリシロキサン、シリコングリコールポリマー等)、炭化水素類(親水ワセリン、白色ワセリン、精製ラノリン、流動パラフィン等)、水、吸収促進剤(炭酸プロピレン、ジイソプロピルアジペート、クロタミトン、エイゾン(登録商標)等)、保湿剤(グリセリン、プロピレングリコール、ブチレングリコール、ソルビトール等)、かぶれ防止剤、その他の添加物(サリチル酸、サリチル酸メチル、サリチル酸グリコール、l−メントール、カンフル、ハッカ油等)等が挙げられ、これらの中から選択される諸成分を混合してなる軟膏基剤にケトプロフェンを配合することにより、本発明の軟膏剤を得ることができる。 Next, the ointment will be described. The ointment base used in the ointment is selected from those usually used, for example, higher fatty acids or their esters (adipic acid, myristic acid, palmitic acid, stearic acid, oleic acid, adipic acid ester, Myristic acid ester, palmitic acid ester, diethyl sebacate, hexyl laurate, cetyl isooctanoate, etc., waxes (eg, whale wax, beeswax, cecilene, etc.), surfactants (polyoxyethylene alkyl ether phosphate, etc.), high grade Alcohol (cetanol, stearyl alcohol, cetostearyl alcohol, etc.), silicone oil (dimethylpolysiloxane, methylphenylpolysiloxane, glycol methylpolysiloxane, silicone glycol polymer, etc.), hydrocarbons (hydrophilic petrolatum, white petrolatum, Lanolin, liquid paraffin, etc.), water, absorption promoters (propylene carbonate, diisopropyl adipate, crotamiton, Azone (registered trademark), etc.), moisturizers (glycerin, propylene glycol, butylene glycol, sorbitol, etc.), anti-rash agents, etc. Additives such as salicylic acid, methyl salicylate, glycol salicylate, l-menthol, camphor, mint oil, etc., etc., and blending ketoprofen with an ointment base made by mixing various components selected from these Thus, the ointment of the present invention can be obtained.
次に、軟膏剤の好適な一製造例(処方例)を示す。すなわち、先ず、高級脂肪酸エステル5〜15重量部、界面活性剤1〜10重量部にケトプロフェン0.1〜10重量部を室温または加熱下に混合し、ロウ類4〜10重量部、炭化水素50〜90重量部を加えて加熱し、50〜100℃に保つ。全成分が透明溶解液となった後、ホモミキサーで均一に混和する。その後、得られた混和物を攪拌しながら室温まで下げることにより本発明の軟膏剤が得られる。 Next, a suitable production example (formulation example) of an ointment will be shown. That is, first, 5 to 15 parts by weight of a higher fatty acid ester, 1 to 10 parts by weight of a surfactant and 0.1 to 10 parts by weight of ketoprofen are mixed at room temperature or under heating, and 4 to 10 parts by weight of waxes and 50 hydrocarbons. Add ~ 90 parts by weight, heat and maintain at 50-100 ° C. After all the components become a transparent solution, mix uniformly with a homomixer. Then, the ointment of the present invention is obtained by lowering the resulting mixture to room temperature while stirring.
次に、ゲル剤について説明する。ゲル剤に用いられるゲル基剤は、通常使用されているものの中より選択され、例えば、低級アルコール(エタノール、イソプロパノール等)、水、ゲル化剤(カルボキシビニル重合体、ヒドロキシエチルセルロース、ヒドロキシプロピルセルロース、メチルセルロース、エチルセルロース、カルボキシメチルセルロース、アルギン酸プロピレングリコールエステル等)、中和剤(トリエタノールアミン、ジイソプロパノールアミン、水酸化ナトリウム等)、界面活性剤(セスキオレイン酸ソルビタン、トリオレイン酸ソルビタン、モノオレイン酸ソルビタン、モノステアリン酸ソルビタン、モノラウリン酸ソルビタン、モノステアリン酸ポリエチレングリコール、ポリオキシエチレンノニルフェニルエーテル、ポリオキシエチレンセチルエーテル、ポリオキシエチレンラウリルエーテル等)、吸収促進剤(炭酸プロピレン、ジエチルセパケート、ジイソプロピルアジペート、クロタミトン、エイゾン(登録商標)、プロピレングリコール等)、溶解剤(エタノール、イソプロパノール等の低級アルコール、セチルアルコール、ステアリルアルコール、バチルアルコール、ベヘニルアルコール、オレイルアルコール、ヘキサデシルアルコール、オクチルドデカノール等の高級アルコール、ミリスチン酸イソプロピル、ミリスチン酸オクチルドデシル、ミリスチン酸セチル、ミリスチン酸ミリスチル、セバシン酸ジエチル、セバシン酸ジイソプロピル、アジピン酸ジイソプロピル、オレイン酸オレイル、ラウリン酸ヘキシル、イソオクタン酸セチル、中鎖脂肪酸トリグリセライド、プロピレングリコール脂肪酸エステル等の脂肪酸エステル、N−メチル−2−ピロリドン、トリアセチン、ベンジルアルコール、ラノリンアルコール、l−メンチルグリセリルエーテル等)、グリコール類(グリセリン、プロピレングリコール、ポリエチレングリコール、ポリプロピレングリコール、ソルビトール、1,3−ブチレングリコール、ジプロピレングリコール等)、かぶれ防止剤、その他の添加物(サリチル酸、サリチル酸メチル、サリチル酸グリコール、l−メントール、カンフル、ハッカ油等)等が挙げられ、これらの中から選択される諸成分を混合してなるゲル基剤にケトプロフェンを配合することにより、本発明のゲル剤を得ることができる。 Next, the gel agent will be described. The gel base used for the gel is selected from those usually used. For example, lower alcohol (ethanol, isopropanol, etc.), water, gelling agent (carboxyvinyl polymer, hydroxyethyl cellulose, hydroxypropyl cellulose, Methyl cellulose, ethyl cellulose, carboxymethyl cellulose, propylene glycol alginate, etc.), neutralizer (triethanolamine, diisopropanolamine, sodium hydroxide, etc.), surfactant (sorbitan sesquioleate, sorbitan trioleate, sorbitan monooleate) Sorbitan monostearate, sorbitan monolaurate, polyethylene glycol monostearate, polyoxyethylene nonylphenyl ether, polyoxyethylene cetyl acetate , Polyoxyethylene lauryl ether, etc.), absorption accelerators (propylene carbonate, diethyl sepacate, diisopropyl adipate, crotamiton, Aison (registered trademark), propylene glycol, etc.), solubilizers (lower alcohols such as ethanol and isopropanol, cetyl alcohol) , Stearyl alcohol, batyl alcohol, behenyl alcohol, oleyl alcohol, hexadecyl alcohol, octyldodecanol and other higher alcohols, isopropyl myristate, octyldodecyl myristate, cetyl myristate, myristyl myristate, diethyl sebacate, diisopropyl sebacate, adipine Diisopropyl acid, oleyl oleate, hexyl laurate, cetyl isooctanoate, medium chain fatty acid triglyceride, pro Fatty acid esters such as lenglycol fatty acid esters, N-methyl-2-pyrrolidone, triacetin, benzyl alcohol, lanolin alcohol, l-menthyl glyceryl ether, etc.), glycols (glycerin, propylene glycol, polyethylene glycol, polypropylene glycol, sorbitol, 1 , 3-butylene glycol, dipropylene glycol, etc.), anti-rash agent, and other additives (salicylic acid, methyl salicylate, glycol salicylate, l-menthol, camphor, mint oil, etc.) and the like are selected. The gel agent of the present invention can be obtained by blending ketoprofen with a gel base obtained by mixing various components.
次に、ゲル剤の好適な一製造法(処方例)を示す。すなわち、先ず、水55重量部以下にゲル化剤0.5〜5重量部を加えて膨潤させて膨潤物Aを得る。一方、ケトプロフェン0.1〜10重量部を溶解剤0.1〜10重量部に溶解もしくは懸濁し、さらにこれをグリコール類40重量部以下と低級アルコール60重量部以下との混合物に溶解して溶解物Bを得る。次いで、溶解物Bを膨潤物Aに加えた後に、中和剤を添加してpH値が4〜7になるように調整することにより、本発明のゲル剤が得られる。 Next, one suitable manufacturing method (formulation example) of a gel is shown. That is, first, 0.5 to 5 parts by weight of a gelling agent is added to 55 parts by weight or less of water and swollen to obtain a swollen material A. On the other hand, 0.1 to 10 parts by weight of ketoprofen is dissolved or suspended in 0.1 to 10 parts by weight of a solubilizer, and further dissolved in a mixture of 40 parts by weight or less of glycols and 60 parts by weight or less of lower alcohol. Object B is obtained. Next, after adding the dissolved material B to the swollen material A, the neutralizing agent is added to adjust the pH value to be 4 to 7, whereby the gel agent of the present invention is obtained.
次に、クリーム剤について説明する。クリーム剤に用いられるクリーム基剤は、通常使用されているものの中より選択され、例えば、高級脂肪酸エステル類(アジピン酸エステル、ミリスチン酸エステル、パルミチン酸エステル、セバシン酸ジエチル、ラウリン酸ヘキシル、イソオクタン酸セチル等)、低級アルコール(エタノール、イソプロパノール等)、炭水化物(流動パラフィン、スクワラン等)、多価アルコール(プロピレングリコール、1,3−ブチレングリコール等)、高級アルコール(2−ヘキシルデカノール、セタノール、2−オクチルドデカノール等)、乳化剤(ポリオキシエチレンアルキルエーテル類、脂肪酸エステル類、ポリエチレングリコール脂肪酸エステル等)、防腐剤(パラオキシ安息香酸エステル等)、吸収促進剤(炭酸プロピレン、ジエチルセパケート、ジイソプロピルアジペート、クロタミトン、エイゾン(登録商標)、プロピレングリコール等)、かぶれ防止剤、その他の添加物(サリチル酸、サリチル酸メチル、サリチル酸グリコール、l−メントール、カンフル、ハッカ油等)等が挙げられ、これらの中から選択される諸成分を混合してなるクリーム基剤にケトプロフェンを配合することにより、本発明のクリーム剤を得ることができる。 Next, the cream will be described. The cream base used in the cream is selected from those usually used, for example, higher fatty acid esters (adipic acid ester, myristic acid ester, palmitic acid ester, diethyl sebacate, hexyl laurate, isooctanoic acid Cetyl, etc.), lower alcohols (ethanol, isopropanol, etc.), carbohydrates (liquid paraffin, squalane, etc.), polyhydric alcohols (propylene glycol, 1,3-butylene glycol, etc.), higher alcohols (2-hexyldecanol, cetanol, 2-octyl) Dodecanol, etc.), emulsifiers (polyoxyethylene alkyl ethers, fatty acid esters, polyethylene glycol fatty acid esters, etc.), preservatives (paraoxybenzoic acid esters, etc.), absorption promoters (propylene carbonate, diethyl ether) Kate, diisopropyl adipate, crotamiton, Azone (registered trademark), propylene glycol, etc.), anti-rash agent, other additives (salicylic acid, methyl salicylate, glycol salicylate, l-menthol, camphor, mint oil, etc.), etc. The cream of the present invention can be obtained by blending ketoprofen with a cream base obtained by mixing various components selected from these.
また、クリーム剤とゲル剤の中間の性質を有するゲル状クリーム剤とするためには、上記のクリーム剤にゲル化剤(カルボキシビニル重合体、ヒドロキシエチルセルロース、ヒドロキシプロピルセルロース、メチルセルロース、エチルセルロース、カルボキシメチルセルロース、アルギン酸プロピレングリコールエステル等)、および中和剤(トリエタノールアミン、ジイソプロパノールアミン、水酸化ナトリウム等)を加え、pHを4〜8(好ましくは5〜6.5)に調整することにより、本発明のゲル状クリーム剤を得ることができる。 In addition, in order to obtain a gel cream having intermediate properties between a cream and a gel, a gelling agent (carboxyvinyl polymer, hydroxyethylcellulose, hydroxypropylcellulose, methylcellulose, ethylcellulose, carboxymethylcellulose is added to the above cream. , Propylene glycol alginate, etc.), and neutralizing agents (triethanolamine, diisopropanolamine, sodium hydroxide, etc.) are added, and the pH is adjusted to 4-8 (preferably 5-6.5). The gel cream of the invention can be obtained.
次に、ゲル状クリーム剤の好適な一製造例(処方例)を示す。すなわち、先ず、ケトプロフェン0.1〜10重量部を高級脂肪酸エステル25重量部以下と低級アルコール40重量部以下の混合物に溶解し、さらに防腐剤0.5重量部以下、乳化剤5重量部以下を加えて混合物Aを得る。一方、水に濃度が0.5〜5重量部となるようにゲル化剤を加えて膨潤させて膨潤物Bを得る。次いで、膨潤物Bを混合物Aに加えてホモミキサーで均一に乳化させた後、得られた乳化物に中和剤を添加してpH値が4〜8になるように調整することにより、本発明のゲル状クリーム剤が得られる。 Next, a preferred production example (formulation example) of a gel cream will be shown. That is, first, 0.1 to 10 parts by weight of ketoprofen is dissolved in a mixture of 25 parts by weight or less of a higher fatty acid ester and 40 parts by weight or less of a lower alcohol, and 0.5 parts by weight or less of an antiseptic and 5 parts by weight or less of an emulsifier are added. To obtain mixture A. On the other hand, a swelling agent B is obtained by adding a gelling agent to water so as to have a concentration of 0.5 to 5 parts by weight to swell. Next, after adding the swollen material B to the mixture A and uniformly emulsifying with a homomixer, a neutralizing agent is added to the obtained emulsion to adjust the pH value to 4 to 8, thereby The gel cream of the invention is obtained.
次に、リニメント剤について説明する。リニメント剤に用いられるリニメント基剤は、通常使用されているものの中より選択され、例えば、アルコール類(エタノール、プロパノール、イソプロパノール等の1価のアルコール、ポリエチレングリコール、プロピレングリコール、ブチレングリコール等の多価アルコール等)10〜70重量部、脂肪酸エステル(アジピン酸、セバシン酸、ミリスチン酸の各種エステル等)60重量部以下、界面活性剤(ポリオキシエチレンアルキルエーテル、ポリオキシエチレン硬化ヒマシ油等)10重量部以下を混合してなるものが挙げられ、このようなリニメント基剤にケトプロフェン0.1〜10重量部を配合することにより、本発明のリニメント剤を得ることができる。なお、リニメント剤においては、必要に応じてpH調整のための中和剤あるいはメチルセルロース等の粘性付与剤、かぶれ防止剤、その他の添加物(サリチル酸、サリチル酸メチル、サリチル酸グリコール、l−メントール、カンフル、ハッカ油、トウガラシエキス、ノニル酸ワニリルアミド、クロタミトン、エイゾン(登録商標)、炭酸プロピレン、ジイソプロピルアジペート等)等を配合してもよい。 Next, the liniment is described. The liniment base used in the liniment is selected from those commonly used. For example, alcohols (monohydric alcohols such as ethanol, propanol and isopropanol, polyvalent glycols such as polyethylene glycol, propylene glycol and butylene glycol) Alcohol, etc.) 10-70 parts by weight, fatty acid ester (adipic acid, sebacic acid, various esters of myristic acid, etc.) 60 parts by weight or less, surfactant (polyoxyethylene alkyl ether, polyoxyethylene hydrogenated castor oil, etc.) 10 weight The liniment of the present invention can be obtained by blending 0.1 to 10 parts by weight of ketoprofen with such a liniment base. In the liniment, if necessary, a neutralizing agent for adjusting pH or a viscosity imparting agent such as methylcellulose, a rash prevention agent, and other additives (salicylic acid, methyl salicylate, glycol salicylate, l-menthol, camphor, Peppermint oil, pepper extract, nonyl acid vanillylamide, crotamiton, Azone (registered trademark), propylene carbonate, diisopropyl adipate, etc.) may be blended.
以上、本発明の外用剤の各剤型に応じた基剤並びに処方例の好適な実施形態について説明したが、剤型並びに処方例はこれらのものに限定されず、各成分の配合順序も特に限定されるものではない。例えば、従来公知のエアゾール剤の処方において、薬効成分をケトプロフェン0.1〜10重量部に置換することにより、本発明のエアゾール剤を得ることができる。 As mentioned above, although the suitable embodiment of the base according to each dosage form of the external preparation of the present invention and a prescription example was described, the dosage form and the prescription example are not limited to these, and the blending order of each component is particularly It is not limited. For example, the aerosol agent of the present invention can be obtained by substituting 0.1 to 10 parts by weight of a medicinal component in a conventionally known aerosol formulation.
また、本発明の外用剤においては、上記処方に加えてさらに抗酸化剤、UVA遮断剤、UVB遮断剤などが配合されてもよい。前記抗酸化剤としては、tert−ブチルヒドロキシアニソール、ジ−tert−ブチルヒドロキシトルエン、チモール、没食子酸プロピル等のフェノール誘導体、トコフェロールおよびそのエステル誘導体、アスコルビン酸およびそのエステル誘導体等が好ましい。このような抗酸化剤は、1種を単独で用いてもよく、2種以上を組み合わせて用いてもよい。その配合量は特に制限されないが、製剤全量を基準として0〜10重量%であることが好ましく、0〜5重量%であることがより好ましい。 Moreover, in the external preparation of this invention, in addition to the said prescription, antioxidant, UVA blocker, UVB blocker, etc. may be further mix | blended. As the antioxidant, tert-butylhydroxyanisole, di-tert-butylhydroxytoluene, thymol, phenol derivatives such as propyl gallate, tocopherol and its ester derivatives, ascorbic acid and its ester derivatives are preferable. Such antioxidant may be used individually by 1 type, and may be used in combination of 2 or more type. The blending amount is not particularly limited, but is preferably 0 to 10% by weight, and more preferably 0 to 5% by weight based on the total amount of the preparation.
前記UVA遮断剤は、無機系UVA遮断剤、または、ジベンゾイルメタン誘導体、ベンゾフェノン誘導体、ケイ皮酸誘導体、カンファー誘導体、ベンゾトリアゾール誘導体、アミノ酸系化合物、ベンゾイルピナコロン誘導体等の有機系UVA遮断剤であってもよい。無機系UVA遮断剤としては、酸化亜鉛、ジベンゾイルメタン誘導体としては、4−tert−ブチル−4’−メトキシジベンゾイルメタン、ベンゾフェノン誘導体としては、2−(4−ジエチルアミノ−2−ヒドロキシベンゾイル)安息香酸n−ヘキシルエステル、ケイ皮酸誘導体およびそのエステルとしては、4−ヒドロキシ−3−メトキシケイ皮酸、4−ヒドロキシ−3−メトキシケイ皮酸イソステアリル等の4−ヒドロキシ−3−メトキシケイ皮酸の分枝鎖状アルキルエステル、カンファー誘導体としては、テレフタリリデン−3,3’−ジカンファー−10,10’−ジスルホン酸、ベンゾトリアゾール誘導体としては、2−(2H−ベンゾトリアゾール−2−イル)−4−メチル−6−[2−メチル−3−[1,3,3,3−テトラメチル−1−[(トリメチルシリル)オキシ]ジシロキサニール]プロピル]フェノール、アミノ酸系化合物としては、ジメトキシベンジリデンジオキソイミダゾリジンプロピオン酸2−ヘキシルエステル、ベンゾイルピナコロン誘導体としては、1−(3,4−ジメトキシフェニル)−4,4−ジメチル−1,3−ペンタンジオンが、それぞれ好ましい。前記UVA遮断剤の配合量は特に制限されないが、製剤全量を基準として例えば、0.01〜20重量%であり、0.5〜20質量%であることが好ましく、より好ましくは1〜15質量%、さらに好ましくは2〜10質量%である。 The UVA blocking agent is an inorganic UVA blocking agent or an organic UVA blocking agent such as a dibenzoylmethane derivative, a benzophenone derivative, a cinnamic acid derivative, a camphor derivative, a benzotriazole derivative, an amino acid compound, or a benzoyl pinacolone derivative. May be. Inorganic UVA blocking agents include zinc oxide, dibenzoylmethane derivatives as 4-tert-butyl-4′-methoxydibenzoylmethane, and benzophenone derivatives as 2- (4-diethylamino-2-hydroxybenzoyl) benzoic acid. Examples of the acid n-hexyl ester, cinnamic acid derivative and esters thereof include 4-hydroxy-3-methoxycinnamic acid such as 4-hydroxy-3-methoxycinnamic acid and 4-hydroxy-3-methoxycinnamic acid isostearyl. Branched alkyl esters of acids, camphor derivatives as terephthalylidene-3,3′-diccamphor-10,10′-disulfonic acid, and benzotriazole derivatives as 2- (2H-benzotriazol-2-yl) -4-methyl-6- [2-methyl-3- [1,3,3,3-teto Methyl-1-[(trimethylsilyl) oxy] disiloxanyl] propyl] phenol, dimethoxybenzylidenedioxoimidazolidinepropionic acid 2-hexyl ester as an amino acid compound, and 1- (3,4-dimethoxyphenyl) as a benzoylpinacolone derivative ) -4,4-dimethyl-1,3-pentanedione is preferred respectively. The blending amount of the UVA blocking agent is not particularly limited, but is, for example, 0.01 to 20% by weight, preferably 0.5 to 20% by weight, more preferably 1 to 15% by weight based on the total amount of the preparation. %, More preferably 2 to 10% by mass.
前記UVB遮断剤は、UVB遮断剤は、ベンゾフェノン誘導体、ケイ皮酸誘導体、カンファー誘導体、アミノ酸系化合物、ベンゾイルピナコロン誘導体等であって、ベンゾフェノン誘導体としては、2−(4−ジエチルアミノ−2−ヒドロキシベンゾイル)安息香酸n−ヘキシルエステル、ケイ皮酸誘導体およびそのエステルとしては、4−ヒドロキシ−3−メトキシケイ皮酸、4−ヒドロキシ−3−メトキシケイ皮酸イソステアリル等の4−ヒドロキシ−3−メトキシケイ皮酸の分枝鎖状アルキルエステル、カンファー誘導体としては、テレフタリリデン−3,3’−ジカンファー−10,10’−ジスルホン酸、アミノ酸系化合物としては、ジメトキシベンジリデンジオキソイミダゾリジンプロピオン酸2−ヘキシルエステル、ベンゾイルピナコロン誘導体としては、1−(3,4−ジメトキシフェニル)−4,4−ジメチル−1,3−ペンタンジオンがそれぞれ好ましい。前記UVB遮断剤の配合量は特に制限されないが、製剤全量を基準として例えば、0.01〜20重量%であり、0.5〜20質量%であることが好ましく、より好ましくは1〜15質量%、さらに好ましくは2〜10質量%である。 The UVB blocker is a benzophenone derivative, cinnamic acid derivative, camphor derivative, amino acid compound, benzoyl pinacolone derivative, etc., and the benzophenone derivative is 2- (4-diethylamino-2-hydroxybenzoyl) ) Benzoic acid n-hexyl ester, cinnamic acid derivatives and esters thereof include 4-hydroxy-3-methoxy such as 4-hydroxy-3-methoxycinnamic acid and 4-hydroxy-3-methoxycinnamic acid isostearyl. Cinnamic acid branched chain alkyl esters, camphor derivatives include terephthalylidene-3,3′-diccamphor-10,10′-disulfonic acid, and amino acid compounds include dimethoxybenzylidene dioxoimidazolidinepropionic acid 2- Hexyl ester, benzoy The pinacolone derivative, 1- (3,4-dimethoxyphenyl) -4,4-dimethyl-1,3-pentanedione is preferable, respectively. The blending amount of the UVB blocking agent is not particularly limited, but is, for example, 0.01 to 20% by weight, preferably 0.5 to 20% by weight, more preferably 1 to 15% by weight based on the total amount of the preparation. %, More preferably 2 to 10% by mass.
本発明のケトプロフェン含有外用剤には、前記の筋肉および腱などの組織中のケトプロフェン濃度を所定濃度以上に保つ外用剤と、生物学的同等性試験においてバイオアベイラビリティが同等であるケトプロフェン含有外用剤が含まれる。ここで生物学的同等性試験とは、生物学的に同等、すなわちバイオアベイラビリティ(未変化体または活性代謝物が、体循環血中に入る速度と量または作用部位に到達する速度と量)が同等であるか否かを判定する試験のことをいい、具体的にバイオアベイラビリティが同等であるか否かは、例えば、平成18年(2006年)11月24日付の薬食審査発第1124005において、日本国の厚生労働省が定める「後発医薬品の生物学的同等性試験ガイドライン」や「局所皮膚適用製剤の後発医薬品のための生物学的同等性試験ガイドライン」などに記載の生物学的同等性試験によって判定することができる。 The ketoprofen-containing external preparation of the present invention includes the above-described external preparation that maintains the ketoprofen concentration in tissues such as muscles and tendons at a predetermined concentration or more, and a ketoprofen-containing external preparation that has the same bioavailability in a bioequivalence test. included. A bioequivalence test here is bioequivalent, ie, bioavailability (the rate and amount of unchanged or active metabolites entering the systemic blood or the rate and amount of reaching the site of action). This refers to a test for determining whether or not they are equivalent. Specifically, whether or not the bioavailability is equivalent is described in, for example, No. 1124005 of the Dietary Diet Review dated November 24, 2006 (2006). , The bioequivalence test described in the “Guidelines for Bioequivalence Tests for Generic Drugs” and “Guidelines for Bioequivalence Tests for Generic Drugs for Topical Skin Application” established by the Ministry of Health, Labor and Welfare in Japan Can be determined.
例えば、「後発医薬品の生物学的同等性試験ガイドライン」では、原則としてクロスオーバー法を行い、血液を採取体液とする場合には、単回投与試験では、AUCt(最終サンプリング時間tまでのAUC(血中濃度−時間曲線下面積))およびCmax(最高血中濃度)を生物学的同等性判定パラメータとする。デコンボルーションでF(被験製剤の基準製剤(水溶液又は静脈内投与)に対する相対吸収率)が算出できる場合は、AUCの代わりにFを用いることができる。また参考パラメータとして、AUC∞(無限大時間までのAUC)、tmax(最高血中濃度到達時間又は最高尿中排泄速度到達時間)、MRT(平均滞留時間)、kel(消失速度定数)などを用いる。尿を採取体液とする場合には、Aet(最終サンプリング時間tまでの累積尿中排泄量)、Aeτ(定常状態に達した後の一投与間隔(τ)内の累積尿中排泄量)、Ae∞(無限大時間までの累積尿中排泄量)、Umax(最大尿中排泄速度)およびUτ(定常状態における投与後τ時間での尿中排泄速度)をAUCt、AUCτ(定常状態に達した後の一投与間隔(τ)内のAUC)、ΑUC∞、CmaxおよびCτ(定常状態における投与後τ時間での血中濃度)に代わるパラメータとして用いる。 For example, in the “Guidelines for Bioequivalence Testing of Generic Drugs”, when the crossover method is performed in principle and blood is used as a collected body fluid, AUC t (AUC up to the final sampling time t) is used in a single-dose test. (Area under blood concentration-time curve)) and Cmax (maximum blood concentration) are used as bioequivalence determination parameters. When F (relative absorption rate of the test preparation relative to the reference preparation (aqueous solution or intravenous administration)) can be calculated by deconvolution, F can be used instead of AUC. For reference parameter, AUC ∞ (infinity AUC up to the time), tmax (in maximum blood concentration arrival time or maximum urinary excretion rate arrival time), MRT (mean residence time), the like kel (elimination rate constant) . When urine is used as a collected body fluid, Ae t (cumulative urinary excretion up to the final sampling time t), Ae τ (cumulative urinary excretion within one administration interval (τ) after reaching a steady state) , Ae ∞ (cumulative urinary excretion up to infinite time), Umax (maximum urinary excretion rate) and U τ (urinary excretion rate at τ time after administration in steady state) are expressed as AUC t and AUC τ (steady state) Used as parameters to replace AUC),) ∞ ∞ , Cmax and C τ (blood concentration at τ time after administration in steady state) after reaching the state.
また、「局所皮膚適用製剤の後発医薬品のための生物学的同等性試験ガイドライン」では、1.皮膚薬物動態学的試験(同等性評価パラメータ:定常状態における薬物回収量、平均角層内薬物濃度または角層内薬物濃度)、2.薬理学的試験(同等性評価パラメータ:AUEC(製剤除去後の蒼白化の強度−時間曲線下面積))、3.残存量試験(同等性評価パラメータ:薬物が製剤から皮膚へ分布した量)、4.薬物動態学的試験(同等性評価パラメータ:AUCまたは定常状態における血中濃度)、5.臨床試験(臨床効果を指標とする)、6.in vitro 効力試験(in vitroにおける効力を指標とする)、7.動物試験(製剤を適用することにより動物の皮膚表面に生じる薬理学的反応を指標とする)など、局所皮膚適用製剤の生物学的同等性の評価にあたって、薬物および製剤の特性に応じて最適の試験法を選択できる。 The “Bioequivalence Test Guidelines for Generic Drugs for Topical Skin Application Formulations” 1. Skin pharmacokinetic test (equivalence evaluation parameter: drug recovery amount in the steady state, average drug concentration in stratum corneum or drug concentration in stratum corneum) 2. Pharmacological test (equivalence evaluation parameter: AUEC (whitening intensity after preparation removal—area under the time curve)) 3. Residual amount test (equivalence evaluation parameter: amount of drug distributed from the preparation to the skin) 4. Pharmacokinetic test (equivalence evaluation parameter: blood concentration in AUC or steady state), 5. Clinical trial (with clinical effect as index), 6. In vitro efficacy test (in vitro efficacy is used as an index), When assessing the bioequivalence of topical skin preparations, such as animal studies (indicating pharmacological reactions that occur on the skin surface of animals as a result of application of the preparations) You can select the test method.
以上のような各試験方法を適宜選択し、得られた試験製剤と標準製剤の前記生物学的同等性判定パラメータを統計処理し、所定の範囲内にあるときに試験製剤と標準製剤とが生物学的に同等であると判定できるが、例えば、前記「後発医薬品の生物学的同等性試験ガイドライン」では、生物学的同等の許容域は、AUCおよびCmaxが対数正規分布する場合には、試験製剤と標準製剤のパラメータの母平均の比で表すとき0.80〜1.25とされ、試験製剤と標準製剤の生物学的同等性判定パラメータの対数値の平均値の差の90%信頼区間が、log(0.80)〜log(1.25)の範囲にあるとき、試験製剤と標準製剤は生物学的に同等と判定される。また前記「局所皮膚適用製剤の後発医薬品のための生物学的同等性試験ガイドライン」では、生物学的同等性の許容域は、同等性評価パラメータが対数正規分布するとみなせる場合には、試験製剤と標準製剤のパラメータの母平均の比で表すとき、作用が強い医薬品では0.80〜1.25、作用が強い医薬品以外の医薬品では0.70〜1.43であり、同等性評価パラメータが正規分布するとみなせる場合には、試験製剤と標準製剤のパラメータの母平均の差を標準製剤の母平均に対する比として表すとき、作用が強い医薬品では−0.20〜+0.20、作用が強い医薬品以外の医薬品では−0.30〜+0.30である。効力試験または臨床試験で評価を行う場合には、医薬品の特性に応じて適切な許容域を設定することができる。
なお、これらのガイドラインに記載の生物学的同等性試験は、当業者にはよく知られている。
以下、実施例を挙げて本発明をより詳細に説明するが、本発明はこれら実施例に限定されるものではない。なお、実施例中、部とあるのはすべて重量部を意味する。
Each test method as described above is appropriately selected, and the bioequivalence determination parameters of the obtained test preparation and standard preparation are statistically processed. When the test preparation and the standard preparation are within a predetermined range, For example, in the above-mentioned “Guidelines for Bioequivalence Testing of Generic Drugs”, the bioequivalent tolerance range is a test when AUC and Cmax are lognormally distributed. 90% confidence interval for the difference between the mean values of the logarithmic values of the bioequivalence determination parameters of the test formulation and the standard formulation, which is 0.80 to 1.25 when expressed as the population average ratio of the formulation and standard formulation parameters Is in the range of log (0.80) to log (1.25), the test formulation and the standard formulation are determined to be bioequivalent. In the “Bioequivalence Test Guidelines for Generic Drugs for Topical Skin Formulations” described above, when the equivalence evaluation parameter can be regarded as a lognormal distribution, When expressed as the population average ratio of the parameters of the standard formulation, 0.80 to 1.25 for drugs with strong action, 0.70 to 1.43 for drugs with strong action, and the equivalence evaluation parameter is normal. When the distribution is considered to be distributed, when the difference between the population mean of the parameters of the test product and the standard product is expressed as the ratio to the population mean of the standard product, it is -0.20 to +0.20 for drugs with strong action, other than those with strong action -0.30 to +0.30 for pharmaceuticals of When an evaluation is conducted in an efficacy test or a clinical trial, an appropriate tolerance can be set according to the characteristics of the drug.
The bioequivalence tests described in these guidelines are well known to those skilled in the art.
EXAMPLES Hereinafter, although an Example is given and this invention is demonstrated in detail, this invention is not limited to these Examples. In the examples, “parts” means all parts by weight.
実施例1
スチレン−イソプレン−スチレンブロック共重合体 25.0部
流動パラフィン(軟化剤) 55.0部
ロジンエステル誘導体 18.0部
ケトプロフェン 2.0部
上記処方で貼付剤を作成した。すなわち、混合機としてニーダーを用い、120〜160℃でスチレン−イソプレン−スチレンブロック共重合体と軟化剤およびロジンエステル誘導体を加熱混合し、次いでケトプロフェンを添加混合し、直接ポリエステル布(PET)に展延し、所望の大きさに切断した。
Example 1
Styrene-isoprene-styrene block copolymer 25.0 parts Liquid paraffin (softener) 55.0 parts Rosin ester derivative 18.0 parts Ketoprofen 2.0 parts A patch was prepared according to the above formulation. That is, using a kneader as a mixer, heat-mix the styrene-isoprene-styrene block copolymer, softener and rosin ester derivative at 120-160 ° C., then add and mix ketoprofen, and directly spread on a polyester cloth (PET). And then cut to the desired size.
(組織内および血漿中ケトプロフェン濃度測定試験)
膝前十字靭帯再建術を実施する患者(37例)を以下の6群に分けてケトプロフェンを投与した。所定時間後、移植の材料となる半腱様筋腱を摘出し、不必要な組織(筋肉および腱)中および血漿中のケトプロフェン濃度を測定した。
(1)群:貼付剤1時間貼付群(7例)
(2)群:貼付剤6時間貼付群(6例)
(3)群:貼付剤14時間貼付群(6例)
(4)群:貼付剤20時間貼付群(2例)
(5)群:経口剤投与群(6例)
(6)群:対照群(10例)
(Tissue and plasma ketoprofen concentration measurement test)
Patients undergoing anterior cruciate ligament reconstruction (37 cases) were divided into the following 6 groups and administered with ketoprofen. After a predetermined time, the half-tendon-like muscle tendon as a material for transplantation was removed, and the concentration of ketoprofen in unnecessary tissues (muscles and tendons) and in plasma was measured.
(1) Group: One hour patch group (7 cases)
(2) Group: 6-hour patch group (6 cases)
(3) Group: Patch 14-hour patch group (6 cases)
(4) Group: 20-hour patch group (2 cases)
(5) Group: Oral administration group (6 cases)
(6) Group: Control group (10 cases)
なお、(1)〜(4)群は、本発明の貼付剤(実施例1)(7cm×10cm)を半腱様筋腱から半腱様筋の上に一致するように2枚貼付した。(5)群は、手術開始14時間前にケトプロフェン徐放カプセル(オルヂスSR150(アボット・ジャパン(株))を1カプセル経口投与した。(6)群は薬剤の投与を行なわなかった。 In the groups (1) to (4), two patches (Example 1) (7 cm × 10 cm) of the present invention were affixed on the semi-tendon-like muscles so as to coincide with each other. The group (5) orally administered ketoprofen sustained release capsule (Ordis SR150 (Abbott Japan Co., Ltd.)) 14 hours before the start of surgery, and the group (6) was not administered any drug.
(ケトプロフェンの定量方法)
−20℃で保存していた血漿および各組織内のケトプロフェン濃度をHPLCで、LC−MS−MS法(Liquid chromatography coupled with mass spectrometry)によって測定した。
(結果)
(1)群〜(4)群における各組織および血漿中ケトプロフェン濃度(平均値)を表1に示す。
The plasma stored at −20 ° C. and ketoprofen concentration in each tissue were measured by HPLC by LC-MS-MS (Liquid chromatography coupled with mass spectrometry).
(result)
Table 1 shows the concentration (average value) of ketoprofen in each tissue and plasma in groups (1) to (4).
本発明の貼付剤14時間貼付群((3)群)の組織中のケトプロフェン濃度は、経口剤投与群((5)群)と比較して同程度の濃度であった、そのときの(3)群における血漿中ケトプロフェン濃度は196ng/mLであり、(5)群(3365ng/mL)の約1/17であった(図1)。
本発明の貼付剤14時間貼付群((3)群)の血漿中ケトプロフェン濃度に対する組織中ケトプロフェン濃度の比は、経口剤投与群((5)群)に対して15〜20倍程度であった(表2)。
The ratio of the tissue ketoprofen concentration to the plasma ketoprofen concentration in the 14-hour patch group (group (3)) of the present invention was about 15 to 20 times that of the oral preparation group (group (5)). (Table 2).
(1)〜(4)群における経時的な組織中および血漿中ケトプロフェン濃度の推移は、血漿中よりも組織中の方が速やかに増加した。組織中の濃度は貼付1時間後で速やかに経口剤投与群((5)群)と同程度の濃度となり、貼付20時間後まで維持された(図2)。
本発明の貼付剤は、速効性があり、経口剤と同程度の効果が長時間維持できる。また、本発明の貼付剤は、全身血中濃度が低く、経口剤よりも安全性が高い。本発明の貼付剤では、ケトプロフェンが貼付位置から直下の組織に直接移行していることが示唆された。
In the groups (1) to (4), changes in the tissue and plasma ketoprofen concentrations over time increased more rapidly in the tissue than in the plasma. The concentration in the tissue quickly became the same level as that in the oral administration group (group (5)) 1 hour after the application, and was maintained until 20 hours after the application (FIG. 2).
The patch of the present invention is fast-acting and can maintain the same effect as an oral preparation for a long time. The patch of the present invention has a low systemic blood concentration and is safer than an oral preparation. In the patch of the present invention, it was suggested that ketoprofen was directly transferred from the application position to the tissue immediately below.
(関節リウマチ患者に対する関節疼痛抑制効果)
本発明の貼付剤(実施例1)(7cm×10cm)を、手首に持続的な疼痛が残る関節リウマチ患者300人を対象とし、被験部位1箇所に1日1回(1回につき1枚貼付)で2週間連日貼付したときの関節疼痛改善効果について、患者による疼痛VAS値変化率を主要評価項目として、プラセボ対照ランダム化二重盲検法により優越を検証した。
(結果)
本発明の貼付剤に有意な効果が見られた。
(Inhibition of joint pain in patients with rheumatoid arthritis)
The patch of the present invention (Example 1) (7 cm × 10 cm) is applied to 300 patients with rheumatoid arthritis with persistent pain on the wrist, once a day (one per time) to one test site. ), The superiority of the joint pain improvement effect was verified by a placebo-controlled randomized double-blind method with the rate of change in pain VAS by the patient as the primary endpoint.
(result)
A significant effect was observed in the patch of the present invention.
以上の結果から、投与後の一定期間、組織中で所定濃度以上のケトプロフェン濃度を実現する本発明の外用剤が、またこのようなケトプロフェン濃度を実現する外用剤が関節リウマチ疼痛抑制効果があることが見出された。 From the above results, the external preparation of the present invention that achieves a ketoprofen concentration of a predetermined concentration or more in the tissue for a certain period after administration, and the external preparation that realizes such a ketoprofen concentration has an effect of suppressing rheumatoid arthritis pain Was found.
Claims (6)
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP2007077504A JP2008231081A (en) | 2007-02-23 | 2007-03-23 | Ketoprofen-containing external preparation |
Applications Claiming Priority (2)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP2007043914 | 2007-02-23 | ||
| JP2007077504A JP2008231081A (en) | 2007-02-23 | 2007-03-23 | Ketoprofen-containing external preparation |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| JP2008231081A true JP2008231081A (en) | 2008-10-02 |
Family
ID=39904314
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP2007077504A Pending JP2008231081A (en) | 2007-02-23 | 2007-03-23 | Ketoprofen-containing external preparation |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JP2008231081A (en) |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN106692114A (en) * | 2016-12-27 | 2017-05-24 | 毛嘉明 | Novel ketoprofen patch and preparation method thereof |
| CN114869936A (en) * | 2022-04-19 | 2022-08-09 | 通化万通药业股份有限公司 | External traditional Chinese medicine composition with effects of dispelling wind and cold, promoting blood circulation and relieving pain and preparation method and application thereof |
-
2007
- 2007-03-23 JP JP2007077504A patent/JP2008231081A/en active Pending
Cited By (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN106692114A (en) * | 2016-12-27 | 2017-05-24 | 毛嘉明 | Novel ketoprofen patch and preparation method thereof |
| CN114869936A (en) * | 2022-04-19 | 2022-08-09 | 通化万通药业股份有限公司 | External traditional Chinese medicine composition with effects of dispelling wind and cold, promoting blood circulation and relieving pain and preparation method and application thereof |
| CN114869936B (en) * | 2022-04-19 | 2023-09-22 | 通化万通药业股份有限公司 | External traditional Chinese medicine composition with effects of dispelling wind, dispelling cold, promoting blood circulation and relieving pain, and preparation method and application thereof |
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