JPH078785B2 - Method for manufacturing transdermal preparations - Google Patents
Method for manufacturing transdermal preparationsInfo
- Publication number
- JPH078785B2 JPH078785B2 JP61119438A JP11943886A JPH078785B2 JP H078785 B2 JPH078785 B2 JP H078785B2 JP 61119438 A JP61119438 A JP 61119438A JP 11943886 A JP11943886 A JP 11943886A JP H078785 B2 JPH078785 B2 JP H078785B2
- Authority
- JP
- Japan
- Prior art keywords
- drug
- adhesive layer
- weight
- preparation
- solvent
- 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.)
- Expired - Lifetime
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Description
【発明の詳細な説明】 (産業上の利用分野) 本発明は,薬物の経皮吸収性に優れた経皮吸収性製剤の
製造方法に関する。TECHNICAL FIELD The present invention relates to a method for producing a percutaneous absorption preparation having excellent percutaneous absorption of a drug.
(従来の技術) 全身もしくは局部での薬効を得るために,経皮吸収性製
剤を用い,薬物(生理活性物質)を皮膚を介して吸収さ
せることが行われている。経皮吸収性製剤は,柔軟な支
持体と,薬物を含有する粘着剤層とを有する。粘着剤層
は,天然ゴム,合成ゴム,アクリル系樹脂などの重合体
から構成されている。(Prior Art) In order to obtain a drug effect systemically or locally, a transdermal drug is used to absorb a drug (physiologically active substance) through the skin. The transdermal preparation has a flexible support and an adhesive layer containing a drug. The pressure-sensitive adhesive layer is made of a polymer such as natural rubber, synthetic rubber or acrylic resin.
粘着剤層に含有される薬物量は,通常,重合体の飽和溶
解度以下とされている。しかし,飽和溶解度以下の薬物
量では,人体に吸収される薬物量が少ないため,充分な
薬効が得られない。薬物吸収量を増すために,粘着剤層
の層厚を厚くしたり製剤の寸法を大きくすれば,高価と
なるうえに使用者に違和感を与える。The amount of drug contained in the pressure-sensitive adhesive layer is usually set to be equal to or lower than the saturated solubility of the polymer. However, if the amount of drug is less than the saturated solubility, the amount of drug absorbed by the human body is small, and thus sufficient drug effect cannot be obtained. If the thickness of the pressure-sensitive adhesive layer is increased or the size of the preparation is increased in order to increase the amount of drug absorbed, the cost becomes high and the user feels uncomfortable.
このような欠点を解決するために,重合体の飽和溶解度
以上の薬物を粘着剤層に含有させた経皮吸収性製剤が提
案されている。飽和溶解度以上の薬物が重合体中に含有
されていれば,薬物の人体への経皮吸収に伴って非溶解
状態(分散状態)の薬物が順次重合体に溶解して補充さ
れるため,薬物吸収量が多くなる。薬物吸収の持続性も
得られる。特に,薬物を微粒子状とすれば,薬物が再溶
解しやすくなり,人体に吸収される薬物量が多くなるた
め好ましい。上記経皮吸収性製剤には,例えば,特開昭
60-185713号公報に開示されているように,飽和溶解度
以上の薬物が重合体中に再結晶微粒子状態で分散された
製剤がある。この製剤は,薬物および重合体を薬物良溶
媒に溶解させ,この溶液を支持体に塗布し乾燥して製造
される。しかし,この方法では,乾燥により薬物が再結
晶化して微粒子状とされるため,結晶化しきらない薬物
が粘着剤層に過飽和状態で溶解し,これが徐々に析出し
て巨大な再結晶粒子となる。乾燥工程での溶媒の揮散に
より,薬物の再結晶粒子が粘着剤層表面に偏在し(薬物
浮き現象),そのために粘着性が低下する。しかも,乾
燥条件により,薬物再結晶粒子の粒子径やその粘着剤層
中での分布状態が変わるため,微粒子状の薬物が粘着剤
層中に均一に分散した製剤を得ることが困難である。薬
物貧溶媒の薬物分散液と薬物良溶媒を用いた重合体溶液
とを混合する方法も開示されている。薬物分散液中に
は,薬物微粒子が分散されている。しかし,この方法で
は混合により薬物粒子同士が合着して巨大粒子となりや
すい。しかも,薬物粒子が粘着剤層中に均一に分散され
得ない。In order to solve such a drawback, a transdermal preparation in which a drug having a saturated solubility of a polymer or more is contained in an adhesive layer has been proposed. If a drug having a saturated solubility or higher is contained in the polymer, the drug in a non-dissolved state (dispersed state) is sequentially dissolved and replenished in the polymer due to percutaneous absorption of the drug into the human body. The absorption amount increases. Prolonged drug absorption is also obtained. In particular, it is preferable that the drug is in the form of fine particles because the drug is easily redissolved and the amount of the drug absorbed by the human body increases. The above-mentioned transdermal preparations include, for example, JP
As disclosed in JP-A-60-185713, there is a preparation in which a drug having a saturated solubility or higher is dispersed in a polymer in a recrystallized fine particle state. This preparation is manufactured by dissolving a drug and a polymer in a good drug solvent, applying this solution to a support, and drying. However, in this method, the drug is recrystallized by drying to be in the form of fine particles, so the drug that is not completely crystallized dissolves in the adhesive layer in a supersaturated state, and this gradually precipitates to form huge recrystallized particles. . Due to the evaporation of the solvent in the drying step, recrystallized particles of the drug are unevenly distributed on the surface of the pressure-sensitive adhesive layer (drug floating phenomenon), and thus the adhesiveness is reduced. Moreover, since the particle size of the drug recrystallized particles and the distribution state thereof in the pressure-sensitive adhesive layer change depending on the drying conditions, it is difficult to obtain a drug product in which finely divided drug is uniformly dispersed in the pressure-sensitive adhesive layer. A method of mixing a drug dispersion of a poor drug solvent and a polymer solution using a good drug solvent is also disclosed. Fine drug particles are dispersed in the drug dispersion liquid. However, with this method, drug particles tend to coalesce into giant particles due to mixing. Moreover, the drug particles cannot be uniformly dispersed in the adhesive layer.
(発明が解決しようとする問題点) 本発明は上記従来の問題点を解決するものであり,その
目的とするところは,微粒子状の薬物が粘着剤層中に均
一に分散された経皮吸収性製剤の製造方法を提供するこ
とにある。本発明の他の目的は,粘着剤層中に飽和溶解
度以上の薬物が含有された経皮吸収性製剤の製造方法を
提供することにある。(Problems to be Solved by the Invention) The present invention is intended to solve the above-mentioned conventional problems, and it is an object of the present invention to provide a transdermal absorption in which a fine particle drug is uniformly dispersed in an adhesive layer. To provide a method for producing a sex preparation. Another object of the present invention is to provide a method for producing a transdermal preparation in which a drug having a saturated solubility or higher is contained in an adhesive layer.
(問題点を解決するための手段) 本発明の経皮吸収性製剤の製造方法は,飽和溶解度以上
の薬物を平均粒径が30μm以下の微粒子状で含有する粘
着剤層と支持体とを有する経皮吸収性製剤の製造方法で
あって,薬物貧溶媒の重合体溶液100重量部に対し薬物
良溶媒の薬物溶液を35重量部以下の割合で添加し,回転
速度30rpm以上で撹拌し均一混合することにより薬物微
粒子を析出させて薬物微粒子の分散液を得る工程および
該分散液を前記支持体上に塗布し乾燥して粘着剤層を形
成する工程,を包含し,そのことにより上記目的が達成
される。(Means for Solving Problems) The method for producing a percutaneously absorbable preparation of the present invention has a pressure-sensitive adhesive layer containing a drug having a saturated solubility or higher in the form of fine particles having an average particle size of 30 μm or less, and a support. A method for producing a percutaneously absorbable preparation, which comprises adding a drug solution of a good drug solvent at a ratio of 35 parts by weight or less to 100 parts by weight of a polymer solution of a poor drug solvent, and stirring the mixture at a rotation speed of 30 rpm or more to uniformly mix them. The steps of precipitating drug particles to obtain a dispersion of drug particles and applying the dispersion onto the support and drying to form a pressure-sensitive adhesive layer. To be achieved.
飽和溶解度以上の薬物を粘着剤層中に結晶状態で含有す
る経皮吸収性製剤の薬物放出挙動は,Journal of Pharma
ceutical Sciences(JPS),50,847,(1961);JPS,52,1
145,(1963);Journal of of the society of cosmetic
chemists,11,85,(1960);JPS,64,1643,(1975)など
に開示されている。JPS,54,1459(1965)には,粘着剤
層中の薬物粒子の粒経について述べられている。薬物の
皮膚への透過性を向上させるためには,熱力学的活性の
点から,飽和溶解度以上の薬物を微粒子状にして粘着剤
層中に含有させることが望ましい(月刊薬事,25,No.2,
(1983),小西良二)。本発明はこれらの知見にもとづ
いて完成された。The drug release behavior of percutaneously absorbable preparations containing a drug having a saturated solubility or higher in a crystalline state in the adhesive layer is described in the Journal of Pharmacology.
ceutical Sciences (JPS), 50 , 847, (1961); JPS, 52 , 1
145, (1963); Journal of of the society of cosmetic
chemists, 11 , 85, (1960); JPS, 64 , 1643, (1975). JPS, 54 , 1459 (1965) describes the particle size of drug particles in an adhesive layer. In order to improve the permeability of the drug to the skin, it is desirable from the viewpoint of thermodynamic activity that the drug having a saturated solubility or higher is made into fine particles and contained in the adhesive layer (Monthly Pharmaceutical Affairs, 25 , No. 2,
(1983), Ryoji Konishi). The present invention has been completed based on these findings.
薬物良溶媒には,例えば,テトラヒドロフラン,酢酸エ
チル,アセトン,メタノール,塩化メチレン,クロロホ
ルム,エーテルがある。薬物貧溶媒には,例えば,n−ヘ
キサン,シクロヘキサン,トルエンがある。しかし,薬
物良溶媒および薬物貧溶媒は使用される薬物によって異
なり,例えば,テトラヒドロフラン,酢酸エチルなどは
薬物貧溶媒となり得る。本発明に用いられる薬物良溶媒
および薬物貧溶媒の配合割合は薬物微結晶が析出しかつ
重合体の再沈が生じない範囲であり,薬物貧溶媒の重合
体溶液100重量部に対し薬物良溶媒の薬物溶液が35重量
部以下に限定される。また溶媒の種類および薬物濃度は
特に限定されないものの,上記範囲内で決定される。薬
物分散液中には微粒子状の薬物が均一に分散しており,
そのような分散液を得るには薬物溶液を重合体溶液に添
加し撹拌,均一混合する際の回転速度が30rpm以上に限
定される。薬物微粒子の平均粒径は30μm以下,好まし
くは15μm以下とされる。この微粒子状の薬物は粘着剤
層中に再溶解しやすいため,この薬物を粘着剤層に含有
する経皮吸収性製剤は,薬物放出性に優れている。その
結果,これを人体に貼付すれば,薬物吸収量が多くな
る。しかも,粘着剤層中には飽和溶解度以上の薬物が含
有されているため,薬物吸収の持続性も得られる。Examples of the good drug solvent include tetrahydrofuran, ethyl acetate, acetone, methanol, methylene chloride, chloroform and ether. Drug poor solvents include, for example, n-hexane, cyclohexane, and toluene. However, the drug good solvent and the drug poor solvent differ depending on the drug used, and for example, tetrahydrofuran, ethyl acetate, etc. can be the drug poor solvent. The mixing ratio of the drug good solvent and the drug poor solvent used in the present invention is such that the drug microcrystals do not precipitate and the polymer does not reprecipitate, and the drug good solvent is added to 100 parts by weight of the polymer solution of the drug poor solvent. The drug solution is limited to 35 parts by weight or less. The type of solvent and the drug concentration are not particularly limited, but are determined within the above range. The drug in the form of fine particles is uniformly dispersed in the drug dispersion,
In order to obtain such a dispersion, the rotation speed when the drug solution is added to the polymer solution and stirred and uniformly mixed is limited to 30 rpm or more. The average particle size of the drug fine particles is 30 μm or less, preferably 15 μm or less. Since the drug in the form of fine particles is easily redissolved in the pressure-sensitive adhesive layer, a transdermal preparation containing the drug in the pressure-sensitive adhesive layer is excellent in drug release. As a result, when it is attached to the human body, the amount of drug absorbed increases. Moreover, since the adhesive layer contains a drug having a saturated solubility or higher, the drug absorption can be maintained.
本発明の経皮吸収性製剤に含有される薬物は,経皮的に
吸収されて薬効を発揮する薬物であり,例えば,ハイド
ロコーチゾン,プレドニゾロン,ベクロメタゾンプロピ
オナート,フルメタゾン,ベータメタゾン,トリアムシ
ノロン,トリアムシノロンアセトニド,フルオシノロ
ン,フルオシノロンアセトニド,フルオシノロンアセト
ニドアセテート,プロピオン酸クロベタゾールなどのコ
ルチコステロイド類;アセトアミノフェン,メフェナム
酸,フルフェナム酸,インドメタシン,ジクロフェナッ
ク,ジクロフェナックナトリウム,アルクロフェナッ
ク,オキシフェンブタゾン,フェニルブタゾン,イブプ
ロフェン,フルルブプロフェン,サリチル酸,サリチル
酸メチル,l−メントール,カンファー,スリンダック,
トルメチンナトリウム,ナプロキセン,フェンブフェン
などの鎮痛消炎剤;フェノバルビタール,アモルバルビ
タール,シクロバルビタール,トルアゾラム,ニトラゼ
パム,ロラゼパム,ハロペリドールなどの催眠鎮静剤;
フルフェナジン,チオリダジン,ジアゼパム,フルジア
ゼパム,フルニトラゼパム,クロルプロマジンなどの精
神安定剤;クロニジン,塩酸クロニジン,ピンドロー
ル,プロプラノロール,塩酸プロプラノロール,ブフラ
ノール,インデノロール,ニバジピン,ロフェジキシ
ン,ニブラジロール,ブクモロール,ニフェジピンなど
の抗高血圧剤;ハイドロサイアザイド,ベンドロフルメ
サイアザイド,シクロペンチアザイドなどの降圧利尿
剤;ペニシリン,テトラサイクリン,オキシテトラサイ
クリン,硫酸フラジオマイシン,エリスロマイシン,ク
ロラムフェニコールなどの抗生物質;リドカイン,ベン
ゾカイン,アミノ安息香酸エチルなどの麻酔剤;塩化ベ
ンザルコニウム,ニトロフラゾン,ナイスタチン,アセ
トスルファミン,クロトリマゾールなどの抗菌性物質;
ペンタマイシン,アムホテリシンB,ピロールニトリン,
クロトリマゾールなどの抗真菌物質;ビタミンA,エルゴ
カルシフェロール,コレカルシフェロール,オクトチア
ミン,リボフラビン酪酸エステルなどのビタミン剤;ニ
トラゼパム,メプロパメート,クロナゼパムなどの抗て
んかん剤;イソソルビドジナイトレート,エリスリトー
ステトラナイトレイト,ペンタエリトーステトラナイト
レイト,プロパチルナイトレートなどの冠血管拡張剤;
塩酸ジフェンヒドラミン,クロルフェニラミン,ジフェ
ニルイミダゾールなどの抗ヒスタミン剤;デキストロメ
トルファン,テルブタリン,エフェドリン,塩酸エフェ
ドリンサルブタモール,イソプロテノールなどの鎮咳
剤;ボロゲステロン,エストラジオールなどの性ホルモ
ン;ドキセピンなどの抗鬱剤;5−フルオロウラシル,ジ
ヒドロエルゴタミン,フェンタニール,デスモプレシ
ン,ジゴキシン,メトクロプラシド,ドンペリド,スコ
ポラミン,臭化水素酸スコポラミン,プロスタグランデ
ィンなどの他の薬剤がある。The drug contained in the percutaneously absorbable preparation of the present invention is a drug that is transdermally absorbed and exerts a medicinal effect, and examples thereof include hydrocortisone, prednisolone, beclomethasone propionate, flumethasone, betamethasone, triamcinolone, triamcinolone acetolone. Corticosteroids such as nido, fluocinolone, fluocinolone acetonide, fluocinolone acetonide acetate, clobetasol propionate; acetaminophen, mefenamic acid, flufenamic acid, indomethacin, diclofenac, diclofenac sodium, alclofenac, oxyphene Butazone, phenylbutazone, ibuprofen, flurbuprofen, salicylic acid, methyl salicylate, l-menthol, camphor, sulindac,
Analgesic and anti-inflammatory agents such as tolmetin sodium, naproxen and fenbufen; hypnotic sedatives such as phenobarbital, amorbarbital, cyclobarbital, toluazolam, nitrazepam, lorazepam, haloperidol;
Fluentazine, thioridazine, diazepam, fludiazepam, flunitrazepam, chlorpromazine, and other tranquilizers; clonidine, clonidine hydrochloride, pindolol, propranolol, propranolol hydrochloride, bufanol, indenolol, nivadipine, rofedixine, nibradirol, bucumolol, antihypertensive, etc .; Antihypertensive diuretics such as hydrothiazide, bendroflumesiazide, cyclopenthiazide; antibiotics such as penicillin, tetracycline, oxytetracycline, fradiomycin sulfate, erythromycin, chloramphenicol; lidocaine, benzocaine, ethyl aminobenzoate, etc. Anesthetic: benzalkonium chloride, nitrofurazone, nystatin, acetosulfamine, croto Antibacterial substances such as Mazoru;
Pentamycin, amphotericin B, pyrrolenitrin,
Antifungal substances such as clotrimazole; vitamins such as vitamin A, ergocalciferol, cholecalciferol, octothiamine, riboflavin butyrate; antiepileptics such as nitrazepam, mepropamate, clonazepam; isosorbide dinitrate, erythritol. Coronary vasodilators such as tetranitrate, pentaerytose tetranitrate, propatil nitrate;
Antihistamines such as diphenhydramine hydrochloride, chlorpheniramine, diphenylimidazole; antitussives such as dextromethorphan, terbutaline, ephedrine, ephedrine salbutamol hydrochloride, isoprotenol; sex hormones such as borogesterone and estradiol; antidepressants such as doxepin; 5-fluorouramin, dihydroeramine, dihydroeramine , Fentanyl, desmopressin, digoxin, metoclopramide, domperide, scopolamine, scopolamine hydrobromide, and prostaglandin.
粘着剤層を形成する重合体には,例えば,ポリビニルア
ルキルエーテル,ポリ(メタ)アクリレート,アクリル
酸2エチルヘキシル−メタクリル酸2エチルヘキシル共
重合体,アクリル酸2エチルヘキシル−ビニルピロリド
ン共重合体,ポリウレタン,スチレン−イソプレン−ス
チレンブロック共重合体,ポリイソブチレンゴム,ポリ
イソプレンゴム,ブチルゴム,天然ゴム,シリコーン樹
脂,テルペン樹脂がある。これら重合体には,感圧接着
性を付与するために,公知の粘着性付与剤,軟化剤,充
填剤,老化防止剤などが添加されてもよい。Examples of the polymer forming the adhesive layer include polyvinyl alkyl ether, poly (meth) acrylate, 2-ethylhexyl acrylate-2-ethylhexyl methacrylate copolymer, 2-ethylhexyl acrylate-vinylpyrrolidone copolymer, polyurethane, styrene. -Isoprene-styrene block copolymer, polyisobutylene rubber, polyisoprene rubber, butyl rubber, natural rubber, silicone resin, and terpene resin. Known tackifiers, softeners, fillers, antioxidants, etc. may be added to these polymers in order to impart pressure-sensitive adhesiveness.
支持体は,経皮吸収性製剤に自己支持性を付与するとと
もに粘着剤層中の薬物の揮散や移行を防止するために設
けられ,例えば,ポリエチレン,ポリプロピレン,ポリ
アクリル,ポリウレタン,ポリエステル,ポリビニルア
ルコール,ポリ塩化ビニル,ポリ塩化ビニリデン,ポリ
アミド,エチレン性共重合体からなるフィルムまたはシ
ート;これらの積層フィルム;ゴムおよび/または合成
樹脂製の多孔性フィルムまたはシート;不織布,織布,
紙などの繊維性フィルムまたはシート;金属箔;表面に
金属蒸着を施した金属箔のフィルムまたはシートがあ
る。これら素材のうち,皮膚面に対して追従性を有する
素材が用いられる。支持体の厚みは,500μm以下,好ま
しくは5〜150μmとされる。The support is provided to impart self-supporting properties to the transdermal preparation and to prevent volatilization and migration of the drug in the adhesive layer, such as polyethylene, polypropylene, polyacryl, polyurethane, polyester, polyvinyl alcohol. , Polyvinyl chloride, polyvinylidene chloride, polyamide, film or sheet made of ethylenic copolymer; laminated film thereof; porous film or sheet made of rubber and / or synthetic resin; non-woven fabric, woven fabric,
There are fibrous films or sheets of paper and the like; metal foils; films or sheets of metal foil having metal vapor deposition on the surface. Among these materials, a material having a conformability to the skin surface is used. The thickness of the support is 500 μm or less, preferably 5 to 150 μm.
本発明の経皮吸収性製剤には,さらに,薬物の経皮吸収
を促進するために,必要に応じて吸収促進剤が添加され
てもよい。吸収促進剤には,例えば,ジエチレングリコ
ール,プロピレングリコール,ポリエチレングリコール
などのグリコール類;オリーブ油,スクアレンラノリン
などの油脂類;尿素,アラントインなどの尿素誘導体;
ミリスチン酸イソプロピル,パルミチン酸イソプロピ
ル,セバシン酸ジエチルなどの高級脂肪酸エステル,高
級脂肪酸トリグリセリド;脂肪酸(モノ)ジエタノール
アミド;サリチル酸;サリチル酸エステルなどがある。
吸収促進剤は,一種または二種以上混合して用いられ,
粘着剤層中に30重量%以下の範囲で含有される。If necessary, an absorption enhancer may be added to the percutaneous absorption preparation of the present invention in order to promote percutaneous absorption of the drug. Examples of the absorption enhancer include glycols such as diethylene glycol, propylene glycol and polyethylene glycol; fats and oils such as olive oil and squalene lanolin; urea derivatives such as urea and allantoin;
Higher fatty acid esters such as isopropyl myristate, isopropyl palmitate and diethyl sebacate, higher fatty acid triglycerides; fatty acid (mono) diethanolamides; salicylic acid; salicylates.
Absorption enhancers may be used alone or in combination of two or more,
It is contained in the adhesive layer in an amount of 30% by weight or less.
(実施例) 以下に本発明を実施例について述べる。(Examples) The present invention will be described below with reference to Examples.
実施例および比較例において,イソソルビドジナイトレ
ートの薬物血中濃度はガスクロマトグラフィー,そして
インドメタシンの薬物血中濃度は液体クロマトグラフィ
ーにて測定した。In the examples and comparative examples, the drug blood concentration of isosorbide dinitrate was measured by gas chromatography, and the drug blood concentration of indomethacin was measured by liquid chromatography.
実施例1 アクリル酸2エチルヘキシル−メタクリル酸2エチルヘ
キシル共重合体(アクリル酸2エチルヘキシル75重量部
に対しメタクリル酸2エチルヘキシルを25重量部含有す
る)の21重量%シクロヘキサン溶液100重量部に,イソ
ソルビドジナイトレート(ISDN)の30重量%塩化メチレ
ン溶液12.35重量部を添加し,回転速度50rpmでディゾル
バーにて均一混合した。得られたISDN微結晶の分散液
を,ポリエチレンテレフタレート(PET)フィルム(片
面がシリコーン剥離剤で処理された。厚さ45μm)上に
塗布し,70℃で30分間乾燥して粘着剤層を形成した。こ
の粘着剤層にPETフィルム(厚さ10μm)を積層して,
経皮吸収性製剤を得た。粘着剤層中には,偏光顕微鏡に
よる観察により,平均粒径約6μmの針状薬物微結晶が
均一に分散していた。粘着剤層の厚さは50μmであり,
粘着剤層中の薬物濃度は15重量%であった。Example 1 100 parts by weight of a 21% by weight cyclohexane solution of a 2-ethylhexyl acrylate / 2-ethylhexyl methacrylate copolymer (containing 25 parts by weight of 2 ethylhexyl methacrylate for 75 parts by weight of 2 ethylhexyl acrylate) in 100 parts by weight of isosorbidogenite 12.35 parts by weight of a 30% by weight methylene chloride solution of rate (ISDN) was added and uniformly mixed with a dissolver at a rotation speed of 50 rpm. The resulting ISDN microcrystal dispersion is applied on a polyethylene terephthalate (PET) film (one side treated with a silicone release agent, thickness: 45 μm) and dried at 70 ° C for 30 minutes to form an adhesive layer. did. PET film (10 μm thick) is laminated on this adhesive layer,
A transdermal preparation was obtained. Observation with a polarization microscope revealed that needle-shaped drug microcrystals having an average particle size of about 6 μm were uniformly dispersed in the adhesive layer. The thickness of the adhesive layer is 50 μm,
The drug concentration in the adhesive layer was 15% by weight.
このようにして得られた経皮吸収性製剤10cm2を,脱毛
処理した日本白色種家兎の背部に貼付し,薬物血中濃度
の経時変化を測定した。これらの結果を表1に示す。The percutaneously absorbable preparation (10 cm 2) thus obtained was applied to the back of a dehaired Japanese white rabbit and the time-dependent change in drug blood concentration was measured. The results are shown in Table 1.
実施例2 アクリル酸2エチルヘキシル−メタクリル酸2エチルヘ
キシル共重合体の21重量%シクロヘキサン溶液に代え
て,天然ゴム55重量部およびテルペン樹脂45重量部の混
合物の10重量%シクロヘキサン溶液を用い,イソソルビ
ドジナイトレート(ISDN)の30重量%塩化メチレン溶液
3.704重量部を添加したこと以外は,実施例1と同様に
して経皮吸収性製剤を得た。Example 2 Instead of a 21 wt% cyclohexane solution of a 2-ethylhexyl acrylate / 2-ethylhexyl methacrylate copolymer, a 10 wt% cyclohexane solution of a mixture of 55 parts by weight of natural rubber and 45 parts by weight of a terpene resin was used, and isosorbidogenite was used. 30 wt% methylene chloride solution of rate (ISDN)
A transdermal preparation was obtained in the same manner as in Example 1 except that 3.704 parts by weight was added.
この経皮吸収性製剤の粘着剤層中には,偏光顕微鏡によ
る観察により,平均粒径3μmの針状薬物微結晶が均一
に分散していた。粘着剤層の厚さは50μmであり,粘着
剤層中の薬物濃度は10重量%であった。Observation with a polarizing microscope revealed that needle-shaped drug microcrystals having an average particle diameter of 3 μm were uniformly dispersed in the adhesive layer of this transdermal preparation. The thickness of the adhesive layer was 50 μm, and the drug concentration in the adhesive layer was 10% by weight.
このようにして得られた経皮吸収性製剤10cm2を,脱毛
処理した日本白色種家兎の背部に貼付し,薬物血中濃度
の経時変化を測定した。これらの結果を表1に示す。The percutaneously absorbable preparation (10 cm 2) thus obtained was applied to the back of a dehaired Japanese white rabbit and the time-dependent change in drug blood concentration was measured. The results are shown in Table 1.
実施例3 アクリル酸2エチルヘキシル−メタクリル酸2エチルヘ
キシル共重合体の21重量%シクロヘキサン溶液に代え
て,アクリル酸2エチルヘキシル−ビニルピロリドン共
重合体(アクリル酸2エチルヘキシル85重量部に対し,
ビニルピロリドンを15重量部含有する)の15重量%シク
ロヘキサン溶液を用い,イソソルビドジナイトレートの
30重量%塩化メチレン溶液に代えて,インドメタシンの
15重量%テトラヒドロフラン溶液30重量部を添加したこ
と以外は,実施例1と同様にして経皮吸収性製剤を得
た。Example 3 Instead of a 21 wt% cyclohexane solution of a 2-ethylhexyl acrylate / 2-ethylhexyl methacrylate copolymer, a 2-ethylhexyl acrylate-vinylpyrrolidone copolymer (85 parts by weight of 2-ethylhexyl acrylate,
Vinylpyrrolidone (containing 15 parts by weight) in a 15% by weight cyclohexane solution.
Instead of 30 wt% methylene chloride solution, indomethacin
A transdermal preparation was obtained in the same manner as in Example 1 except that 30 parts by weight of a 15% by weight tetrahydrofuran solution was added.
この経皮吸収性製剤の粘着剤層中には,偏光顕微鏡によ
る観察により,平均粒径7μmの針状薬物微結晶が均一
に分散していた。粘着剤層の厚さは50μmであり,粘着
剤層中の薬物濃度は23重量%であった。Observation with a polarization microscope revealed that needle-shaped drug microcrystals having an average particle size of 7 μm were uniformly dispersed in the adhesive layer of the transdermal preparation. The thickness of the adhesive layer was 50 μm, and the drug concentration in the adhesive layer was 23% by weight.
このようにして得られた経皮吸収性製剤30cm2を,脱毛
処理した日本白色種家兎の背部に貼付し,薬物血中濃度
の経時変化を測定した。これらの結果を表2に示す。The percutaneously absorbable preparation (30 cm 2) thus obtained was applied to the back of a dehaired Japanese White Rabbit and the time-dependent change in drug blood concentration was measured. The results are shown in Table 2.
実施例4 アクリル酸2エチルヘキシル−メタクリル酸2エチルヘ
キシル共重合体の21重量%シクロヘキサン溶液に代え
て,スチレン−イソプレン−スチレンブロック共重合体
50重量部およびテルペン樹脂50重量部の混合物の30重量
%シクロヘキサン溶液を用い,イソソルビドジナイトレ
ートの30重量%塩化メチレン溶液に代えて,インドメタ
シンの15重量%テトラヒドロフラン溶液20重量部を添加
したこと以外は,実施例1と同様にして経皮吸収性製剤
を得た。Example 4 A styrene-isoprene-styrene block copolymer was used instead of a 21 wt% cyclohexane solution of a 2-ethylhexyl acrylate-diethylhexyl methacrylate copolymer.
Using a 30% by weight cyclohexane solution of a mixture of 50 parts by weight and 50 parts by weight of a terpene resin, except that 20 parts by weight of a 15% by weight solution of indomethacin in tetrahydrofuran was added instead of a 30% by weight methylene chloride solution of isosorbide dinitrate. In the same manner as in Example 1, a transdermal preparation was obtained.
この経皮吸収性製剤の粘着剤層中には,偏光顕微鏡によ
る観察により,平均粒径2μmの針状薬物微結晶が均一
に分散していた。粘着剤層の厚さは50μmであり,粘着
剤層中の薬物濃度は9.09重量%であった。Observation with a polarizing microscope revealed that needle-shaped drug microcrystals having an average particle diameter of 2 μm were uniformly dispersed in the pressure-sensitive adhesive layer of this transdermal preparation. The thickness of the adhesive layer was 50 μm, and the drug concentration in the adhesive layer was 9.09% by weight.
このようにして得られた経皮吸収性製剤30cm2を,脱毛
処理した日本白色種家兎の背部に貼付し,薬物血中濃度
の経時変化を測定した。これらの結果を表2に示す。The percutaneously absorbable preparation (30 cm 2) thus obtained was applied to the back of a dehaired Japanese White Rabbit and the time-dependent change in drug blood concentration was measured. The results are shown in Table 2.
実施例5 アクリル酸2エチルヘキシル−メタクリル酸2エチルヘ
キシル共重合体(アクリル酸2エチルヘキシル75重量部
に対し,メタクリル酸2エチルヘキシルを25重量部含有
する)の10重量%シクロヘキサン溶液を用い,イソソル
ビドジナイトレート(ISDN)の30重量%塩化メチレン溶
液に代えて,プレドニゾロンの7重量%アセトン/メタ
ノール混合溶媒溶液(1/1体積比)14.29重量部を添加し
たこと以外は,実施例1と同様にして経皮吸収性製剤を
得た。Example 5 Isosorbide dinitrate was prepared by using a 10 wt% cyclohexane solution of a 2-ethylhexyl acrylate / 2-ethylhexyl methacrylate copolymer (containing 25 parts by weight of 2-ethylhexyl methacrylate for 75 parts by weight of 2-ethylhexyl acrylate). The same procedure as in Example 1 was carried out except that 14.29 parts by weight of a 7% by weight acetone / methanol mixed solvent solution (1/1 volume ratio) of prednisolone was added in place of the 30% by weight methylene chloride solution of (ISDN). A skin absorbable preparation was obtained.
この経皮吸収性製剤の粘着剤層中には,偏光顕微鏡によ
る観察により,平均粒径12μmの針状薬物微結晶が均一
に分散していた。粘着剤層の厚さは50μmであり,粘着
剤層中の薬物濃度は10重量%であった。Observation with a polarizing microscope revealed that needle-shaped drug microcrystals having an average particle diameter of 12 μm were uniformly dispersed in the adhesive layer of this transdermal preparation. The thickness of the adhesive layer was 50 μm, and the drug concentration in the adhesive layer was 10% by weight.
比較例1 シクロヘキサン(薬物貧溶媒)に代えて酢酸エチル(薬
物良溶媒)を用いたこと以外は,実施例1と同様にして
経皮吸収性製剤を得た。粘着剤層中には,薬物が過飽和
に溶解しており,偏光顕微鏡による観察でも,結晶の析
出は認められなかった。この製剤を室温下で2日間放置
したところ,製剤の全面にわたって平均粒径約80μmの
ひげ状巨大結晶が析出した。Comparative Example 1 A transdermal preparation was obtained in the same manner as in Example 1 except that ethyl acetate (good solvent for drug) was used instead of cyclohexane (poor solvent for drug). The drug was supersaturated in the pressure-sensitive adhesive layer, and no crystal precipitation was observed by observation with a polarizing microscope. When this preparation was left to stand at room temperature for 2 days, giant whiskers with an average particle size of about 80 μm were deposited on the entire surface of the preparation.
結晶が析出した経皮吸収性製剤10cm2を,脱毛処理した
日本白色種家兎の背部に貼付し,薬物血中濃度の経時変
化を測定した。これらの結果を表1に示す。A 10 cm 2 percutaneous absorption preparation in which crystals were deposited was attached to the back of a dehaired Japanese white rabbit, and the time-dependent change in drug blood concentration was measured. The results are shown in Table 1.
比較例2 シクロヘキサン(薬物貧溶媒)に代えてテトラヒドロフ
ラン(薬物良溶媒)を用いたこと以外は,実施例2と同
様にして経皮吸収性製剤を得た。粘着剤層中には,薬物
が過飽和に溶解しており,偏光顕微鏡による観察でも,
結晶の析出は認められなかった。この製剤を室温下で2
日間放置したところ,製剤の側面の一部において,放射
状に広がる平均粒経60μmの針状巨大結晶が析出した。
室温下で1ヵ月放置後,析出結晶は製剤の全面に認めら
れた。Comparative Example 2 A transdermal preparation was obtained in the same manner as in Example 2 except that tetrahydrofuran (good drug solvent) was used instead of cyclohexane (drug poor solvent). The drug is supersaturated in the adhesive layer, and even when observed with a polarizing microscope,
No precipitation of crystals was observed. This formulation at room temperature 2
When left for a day, acicular giant crystals with an average particle size of 60 μm that spread radially were deposited on a part of the side surface of the preparation.
After standing for 1 month at room temperature, precipitated crystals were observed on the entire surface of the preparation.
結晶が析出した経皮吸収性製剤10cm2を,脱毛処理した
日本白色種家兎の背部に貼付し,薬物血中濃度の経時変
化を測定した。これらの結果を表1に示す。A 10 cm 2 percutaneous absorption preparation in which crystals were deposited was attached to the back of a dehaired Japanese white rabbit, and the time-dependent change in drug blood concentration was measured. The results are shown in Table 1.
比較例3 シクロヘキサン(薬物貧溶媒)に代えて酢酸エチル(薬
物良溶媒)を用いたこと以外は,実施例3と同様にして
経皮吸収性製剤を得た。粘着剤層中には,薬物が過飽和
に溶解しており,偏光顕微鏡による観察でも,結晶の析
出は認められなかった。この製剤を室温下で2日間放置
したところ,製剤の一部に平均粒径70μmのひげ状巨大
結晶が析出した。室温下で3カ月放置後,析出結晶は製
剤の全面に認められた。Comparative Example 3 A transdermal preparation was obtained in the same manner as in Example 3 except that ethyl acetate (good drug solvent) was used in place of cyclohexane (drug poor solvent). The drug was supersaturated in the pressure-sensitive adhesive layer, and no crystal precipitation was observed by observation with a polarizing microscope. When this formulation was left to stand at room temperature for 2 days, giant whiskers having an average particle size of 70 μm were precipitated in a part of the formulation. After standing for 3 months at room temperature, precipitated crystals were observed on the entire surface of the preparation.
結晶が析出した経皮吸収性製剤10cm2を,脱毛処理した
日本白色種家兎の背部に貼付し,薬物血中濃度の経時変
化を測定した。これらの結果を表2に示す。A 10 cm 2 percutaneous absorption preparation in which crystals were deposited was attached to the back of a dehaired Japanese white rabbit, and the time-dependent change in drug blood concentration was measured. The results are shown in Table 2.
比較例4 シクロヘキサン(薬物貧溶媒)に代えてテトラヒドロフ
ラン(薬物良溶媒)を用いたこと以外は,実施例4と同
様にして経皮吸収性製剤を得た。粘着剤層中には,薬物
が過飽和に溶解しており,偏光顕微鏡による観察でも,
結晶の析出は認められなかった。この製剤を室温下で2
日間放置したところ,製剤の全面にわたって平均粒径40
μmの針状巨大結晶が析出した。この結晶は核を中心に
円形に広がっていた。Comparative Example 4 A transdermal preparation was obtained in the same manner as in Example 4 except that tetrahydrofuran (good solvent for drug) was used instead of cyclohexane (poor solvent for drug). The drug is supersaturated in the adhesive layer, and even when observed with a polarizing microscope,
No precipitation of crystals was observed. This formulation at room temperature 2
When left for a day, the average particle size was 40
Large needle-like crystals of μm were deposited. This crystal was spread in a circle around the nucleus.
結晶が析出した経皮吸収性製剤10cm2を,脱毛処理した
日本白色種家兎の背部に貼付し,薬物血中濃度の経時変
化を測定した。これらの結果を表2に示す。A 10 cm 2 percutaneous absorption preparation in which crystals were deposited was attached to the back of a dehaired Japanese white rabbit, and the time-dependent change in drug blood concentration was measured. The results are shown in Table 2.
比較例5 シクロヘキサン(薬物貧溶媒)に代えて酢酸エチル(薬
物良溶媒)を用いたこと以外は,実施例5と同様にして
経皮吸収性製剤の製造を試みたものの,粘着剤層の表面
には平均粒径約200μmの巨大結晶が析出しており(薬
物浮き現象),粘着性が低いため支持体に積層され得な
かった。 Comparative Example 5 A transdermal absorbable preparation was produced in the same manner as in Example 5 except that ethyl acetate (good drug solvent) was used in place of cyclohexane (drug poor solvent), but the surface of the pressure-sensitive adhesive layer was tried. A huge crystal with an average particle size of about 200 μm was deposited on the film (drug floating phenomenon) and could not be laminated on the support due to its low adhesiveness.
実施例および比較例から明らかなように,本発明の経皮
吸収性製剤の製造方法によれば,粘着剤層中に薬物微粒
子が均一に分散されうる。そのために,この経皮吸収性
製剤を皮膚に貼付すれば,高レベルの薬物血中濃度が得
られ,しかも薬物血中濃度の持続性が良好となる。薬物
および重合体を薬物良溶媒に溶解させ,この溶液を支持
体に塗布し乾燥する従来の経皮吸収性製剤の製造方法に
よれば,粘着剤層中に薬物の巨大粒子が析出する。その
ために,この経皮吸収性製剤を皮膚に貼付すれば,薬物
血中濃度が低く,しかもその持続性にも欠ける。As is clear from Examples and Comparative Examples, according to the method for producing a percutaneously absorbable preparation of the present invention, fine drug particles can be uniformly dispersed in the adhesive layer. Therefore, when this percutaneously absorbable preparation is applied to the skin, a high level of drug blood concentration can be obtained and the drug blood concentration can be maintained well. According to the conventional method for producing a percutaneously absorbable preparation in which a drug and a polymer are dissolved in a good drug solvent, and the solution is applied to a support and dried, giant particles of the drug are deposited in the adhesive layer. Therefore, if this percutaneous absorption preparation is applied to the skin, the blood concentration of the drug will be low, and its sustainability will be lacking.
(発明の効果) 本発明によれば,このように,微粒子状の薬物が粘着剤
層中に均一に分散された経皮吸収性製剤が得られる。こ
の経皮吸収性製剤は,薬物放出性に優れている。薬物放
出の持続性も得られる。その結果,この経皮吸収性製剤
を皮膚に貼付すれば,高レベルの薬物血中濃度が得られ
る。薬物血中濃度の持続性にも優れる。(Effects of the Invention) According to the present invention, a percutaneous absorption preparation in which a drug in the form of fine particles is uniformly dispersed in an adhesive layer is thus obtained. This percutaneously absorbable preparation is excellent in drug release. A sustained drug release is also obtained. As a result, when this percutaneously absorbable preparation is applied to the skin, a high level of drug concentration in blood can be obtained. It also excels in the sustainability of drug concentration in blood.
Claims (1)
以下の微粒子状で含有する粘着剤層と支持体とを有する
経皮吸収性製剤の製造方法であって, 薬物貧溶媒の重合体溶液100重量部に対し薬物良溶媒の
薬物溶液を35重量部以下の割合で添加し,回転速度30rp
m以下で撹拌し均一混合することにより薬物微粒子を析
出させて薬物微粒子の分散液を得る工程および該分散液
を前記支持体上に塗布し乾燥して粘着剤層を形成する工
程, を包含する経皮吸収性製剤の製造方法。1. A drug having a saturated solubility or higher and an average particle size of 30 μm.
A method for producing a percutaneously absorbable preparation having the following adhesive layer containing fine particles and a support, wherein 35 parts by weight of a drug solution of a good drug solvent is added to 100 parts by weight of a polymer solution of a poor drug solvent. Add at the following ratio, rotation speed 30rp
a step of precipitating drug fine particles to obtain a dispersion liquid of the drug fine particles by stirring at m or less and uniformly mixing, and a step of applying the dispersion liquid on the support and drying to form an adhesive layer. Method for manufacturing transdermal preparations.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP61119438A JPH078785B2 (en) | 1986-05-23 | 1986-05-23 | Method for manufacturing transdermal preparations |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP61119438A JPH078785B2 (en) | 1986-05-23 | 1986-05-23 | Method for manufacturing transdermal preparations |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPS62273913A JPS62273913A (en) | 1987-11-28 |
| JPH078785B2 true JPH078785B2 (en) | 1995-02-01 |
Family
ID=14761419
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP61119438A Expired - Lifetime JPH078785B2 (en) | 1986-05-23 | 1986-05-23 | Method for manufacturing transdermal preparations |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPH078785B2 (en) |
Families Citing this family (6)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| EP0319988A1 (en) * | 1987-12-09 | 1989-06-14 | Showa Denko Kabushiki Kaisha | External dermatological composition |
| JP2681365B2 (en) * | 1988-04-11 | 1997-11-26 | 日東電工株式会社 | Percutaneous absorption preparation and its manufacturing method |
| JP2681375B2 (en) * | 1988-08-26 | 1997-11-26 | 日東電工株式会社 | Therapeutic adhesive formulation |
| JP4641394B2 (en) * | 2004-08-06 | 2011-03-02 | リンテック株式会社 | Method for producing transdermal preparation |
| US20090130188A9 (en) * | 2005-09-29 | 2009-05-21 | National Starch And Chemical Investment Holding Company | Acrylic pressure sensitive adhesives |
| JP5243254B2 (en) * | 2006-10-11 | 2013-07-24 | 久光製薬株式会社 | Crystal-containing patch |
Family Cites Families (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPS60185713A (en) * | 1984-03-05 | 1985-09-21 | Nitto Electric Ind Co Ltd | Percutaneous preparation and its production |
-
1986
- 1986-05-23 JP JP61119438A patent/JPH078785B2/en not_active Expired - Lifetime
Also Published As
| Publication number | Publication date |
|---|---|
| JPS62273913A (en) | 1987-11-28 |
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