JPH066534B2 - Transdermal patch - Google Patents
Transdermal patchInfo
- Publication number
- JPH066534B2 JPH066534B2 JP61240679A JP24067986A JPH066534B2 JP H066534 B2 JPH066534 B2 JP H066534B2 JP 61240679 A JP61240679 A JP 61240679A JP 24067986 A JP24067986 A JP 24067986A JP H066534 B2 JPH066534 B2 JP H066534B2
- Authority
- JP
- Japan
- Prior art keywords
- drug
- patch
- adhesive layer
- weight
- pressure
- 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
Links
Landscapes
- Medicinal Preparation (AREA)
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貼付剤に
関する。TECHNICAL FIELD The present invention relates to a transdermal patch having excellent transdermal absorbability 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、経皮吸収貼付
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。経皮吸収貼付剤は、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 patch is used to absorb a drug (physiologically active substance) through the skin. The transdermal patch has a flexible support and a pressure-sensitive 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貼付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 the 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 the drug is less than the saturated solubility, the amount of the drug absorbed by the human body is small, and thus a sufficient drug effect cannot be obtained. If the thickness of the pressure-sensitive adhesive layer is increased or the size of the patch is increased in order to increase the drug absorption amount, the cost becomes high and the user feels uncomfortable.
このような欠点を解決するために、例えば、特開昭60-1
85713号公報には、重合体(粘着基剤)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貼付剤が提案
されている。この貼付剤においては、飽和溶解度を越え
る薬物は、ほぼ均一の再結晶微粒子状態で分散されてい
る。このような貼付剤を皮膚表面に貼付すると、粘着剤
中の薬物は経皮吸収され、それに伴って非溶解状態(分
散状態)の薬物が、順次粘着剤中に補充される。このよ
うに、貼付剤の貼付後の粘着剤中の薬物濃度は、飽和溶
解度に保たれるか、もしくは薬物放出速度と薬物再溶解
速度とのバランスで決まる所定の(飽和溶解度以下の)
濃度に保たれる。従って、この貼付剤は、薬物の単位面
積あたりの含有量を高くする効果があるが、それは単に
粘着剤層の厚みを増したのと同等の効果であり、例え
ば、薬物の血中濃度や薬物の初期吸収性の改善はほとん
ど認められず、薬物の皮膚透過量の改善も顕著ではな
い。さらに、過剰の薬物が巨大な再結晶微粒子となつて
表面に偏在し、そのため粘着性が低下することもある。In order to solve such a defect, for example, JP-A-60-1
Japanese Patent No. 85713 proposes a transdermal patch in which a drug having a saturated solubility of a polymer (adhesive base) or more is contained in an adhesive layer. In this patch, the drug having a saturated solubility is dispersed in a substantially uniform recrystallized fine particle state. When such a patch is applied to the skin surface, the drug in the adhesive is percutaneously absorbed, and accordingly, the drug in a non-dissolved state (dispersed state) is sequentially replenished in the adhesive. In this way, the drug concentration in the adhesive after application of the patch is maintained at a saturated solubility or is determined by a balance between the drug release rate and the drug re-dissolution rate (below the saturated solubility).
Maintained at a concentration. Therefore, this patch has the effect of increasing the content of the drug per unit area, but it is the same effect as simply increasing the thickness of the adhesive layer, for example, the blood concentration of the drug or the drug. Almost no improvement in initial absorbability was observed, and the improvement in drug permeation through the skin was not significant. In addition, excessive drug may be distributed in the surface as huge recrystallized fine particles, which may reduce the stickiness.
特公昭60-59207号公報には、接触した薬物が移行しうる
重合物性フィルムを支持体として用いた複合製剤(貼付
剤)の製法が開示されている。この貼付剤は、上記フィ
ルム(もしくはシート)表面に、経皮吸収性薬物(少な
くとも0℃で固体である)を粘着基剤に該薬物の飽和溶
解度以上の割合で添加した粘着剤の層を形成してなる。
このような貼付剤では、粘着剤層の飽和溶解度を越える
量の薬物は、支持体中に移行する。貼付剤を皮膚表面に
貼付すると、粘着剤中の薬物の経皮吸収に伴い支持体中
の薬物が順次粘着剤中に移行して補充されるため、薬物
吸収量が増す。このような貼付剤では、薬物が結晶化し
て粘着剤の粘着性が低下したり、結晶化薬物の再溶解速
度が遅いことに起因する薬物放出速度の低下が起こらな
い。しかし、支持体の薬物飽和溶解度を越える過剰の薬
物を粘着基剤中に含有させることはできないため、支持
体の薬物溶解能や厚みにより薬物含有量が制限される。
この貼付剤の支持体からは、放出された薬物を補う量の
薬物が分配に従って供給されるが、粘着剤層の薬物濃度
は飽和溶解度以下に保たれる。それゆえ、この貼付剤も
上記薬物微粒子を粘着剤層中に含有する貼付剤と同様、
薬物の血中濃度、薬物の初期吸収性の改善はほとんど認
められず、薬物の皮膚透過量の改善も顕著ではない。Japanese Examined Patent Publication No. 60-59207 discloses a method for producing a composite preparation (patch) using as a support a polymer film capable of migrating a contacted drug. This patch forms a layer of adhesive on the surface of the above film (or sheet) by adding a transdermal drug (solid at least at 0 ° C.) to an adhesive base at a ratio of saturated solubility of the drug or more. I will do it.
In such a patch, an amount of drug exceeding the saturated solubility of the pressure-sensitive adhesive layer migrates into the support. When the patch is applied to the surface of the skin, the drug in the support is sequentially transferred into the adhesive for transdermal absorption of the drug in the adhesive, and the drug absorption is increased. In such a patch, the drug does not crystallize and the adhesiveness of the adhesive decreases, and the drug release rate does not decrease due to the slow re-dissolution rate of the crystallized drug. However, an excessive amount of drug exceeding the drug saturation solubility of the support cannot be contained in the adhesive base, and thus the drug content is limited by the drug solubility and thickness of the support.
From the support of this patch, an amount of the drug that supplements the released drug is supplied in accordance with the distribution, but the drug concentration in the adhesive layer is kept below the saturated solubility. Therefore, this patch is also similar to the patch containing the drug fine particles in the adhesive layer,
Almost no improvement in blood concentration of the drug or initial absorbability of the drug was observed, and improvement in the skin permeation amount of the drug was not remarkable.
(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、単位面積あたりの薬物含量が高
く、かつその薬物量に比例して薬物の皮膚透過性の高い
経皮吸収貼付剤を提供することにある。本発明の他の目
的は、上記特徴に加えさらに薬物の初期放出性が高く、
かつ高レベルの血中濃度を維持しうる、経皮吸収貼付剤
を提供することにある。(Problems to be Solved by the Invention) The present invention is to solve the above-mentioned conventional problems, and an object of the present invention is to provide a drug having a high drug content per unit area and in proportion to the drug amount. To provide a percutaneous absorption patch having high skin permeability. Another object of the present invention is, in addition to the above characteristics, a high initial release property of a drug,
Another object of the present invention is to provide a transdermal patch that can maintain a high level of blood concentration.
(問題点を解決するための手段および作用) 本発明の経皮吸収貼付剤は、薬物不透過性支持体表面
に、少なくとも30℃で固体の薬物を含有する粘着剤層
が形成された経皮吸収貼付剤であつて、該粘着剤が該薬
物を飽和溶解度以上の割合で含有し、該貼付剤があらか
じめ加熱され、該薬物が該粘着剤層中に過飽和溶解状態
で存在し、そのことにより上記目的が達成される。(Means and Actions for Solving Problems) The transdermal patch of the present invention is a transdermal skin in which an adhesive layer containing a solid drug at least 30 ° C. is formed on the surface of a drug impermeable support. Absorption patch, wherein the adhesive contains the drug in a ratio of saturated solubility or more, the patch is preheated, the drug is present in the adhesive layer in a supersaturated dissolution state, thereby The above object is achieved.
本発明の経皮吸収貼付剤の粘着剤層に用いられる粘着基
剤としては、通常の貼付剤の粘着剤層に用いられる重合
体が用いられる。それには例えば、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
ンブロツク共重合体、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。As the pressure-sensitive adhesive base used in the pressure-sensitive adhesive layer of the transdermal absorption patch of the present invention, a polymer used in a normal pressure-sensitive adhesive layer of a patch is used. For example, 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,
There is a terpene resin. Known tackifiers, softening agents, fillers, antioxidants, etc. may be added to these polymers in order to impart pressure-sensitive adhesiveness.
貼付剤の支持体は、経皮吸収貼付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、薬剤不透過性の材が用いられる。それ
には、例えば、ポリエチレン、ポリプロピレン、ポリア
クリル酸エステル、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ゴム、からなるフ
ィルムまたはシート;これらの積層体;上記素材を用い
た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
らのうち、皮膚面に対して追従性を有する支持体が好適
に用いられる。支持体の厚みは、500μm以下、好ま
しくは5〜150μmとされる。The support of the patch is provided in order to impart self-supporting property to the transdermal patch and prevent volatilization and migration of the drug in the pressure-sensitive adhesive layer, and a drug-impermeable material is used. For example, a film or sheet made of polyethylene, polypropylene, polyacrylic ester, polyurethane, polyester, polyvinyl alcohol, polyvinyl chloride, polyvinylidene chloride, polyamide, ethylenic copolymer rubber; a laminate of these; There are porous films or sheets using raw materials; fibrous films or sheets such as non-woven fabrics, woven fabrics, and papers; metal foils; films or sheets of metal foils whose surfaces are metal-deposited. Of these, a support having conformability to the skin surface is preferably 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、カンフアー、スリンダツ
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
トスルフアミン、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、メトクロプラミド、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物がある。The drug contained in the percutaneously absorbable preparation of the present invention is a drug which is transdermally absorbed and exerts a medicinal effect, for example, 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, tolmetin sodium , Naproxen, fenbufen and other analgesic / anti-inflammatory agents; phenobarbital, amobarbital, cyclobarbital, toluazolam, nitrazepam, lorazepam, haloperidol, and other sedatives; fluphenazine, thioridazine, diazepam, fludiazepam, flunitrazepam, chlorpromazine, etc. Antihypertensive agents such as clonidine, clonidine hydrochloride, pindolol, propranolol, propranolol hydrochloride, bufuranol, indenolol, nivadipine, lofedixin, nibradirol, bucumolol, nifedipine; antihypertensive diuretics such as hydrothiazide, bendroflumethiazide, cyclopentiazide; Penicillin, tetracycline, oxytetracycline, fradiomycin sulfate, erythromycin Emissions, chloramphenicol antibiotics such as chloramphenicol; lidocaine, benzocaine, an anesthetic, such as aminoethyl benzoate, benzalkonium chloride, nitrofurazone, nystatin, antibacterial substances such as acetoacetic sulphates amines, clotrimazole;
Antifungal substances such as pentamycin, amphotericin B, pyrrolenitrin, clotrimazole; vitamin A,
Vitamin preparations such as ergocalciferol, cholecalciferol, octothiamine and riboflavin butyrate; antiepileptic agents such as nitrazepam, mepropamate and clonazepam; isosorbide dinitrate, erythritol tetranitrate, pentaerythrose tetranitrate, pro Coronary vasodilators such as patylnitrate; diphenhydramine hydrochloride, chlorpheniramine,
Antihistamines such as diphenylimidazole, antitussives such as dextromethorphan, terbutaline, ephedrine, ephedrine hydrochloride, salbutamol, and isoprotenol; sex hormones such as borogesterone and estradiol; antidepressants such as doxepin; 5-fluorouracil, dihydroergotamine, fentanyl, desmopressin, desmopressin, , Metoclopramide, domperide, scopolamine, scopolamine hydrobromide, and other drugs such as prostaglandin.
本発明の経皮吸収貼付剤の粘着剤層には、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
れる。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。To the adhesive layer of the transdermal absorption patch of the present invention, an absorption promoter is added, if necessary, 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; oils and fats such as olive oil, squalene and lanolin; urine derivatives such as urea and allantoin; isopropyl myristate and isopropyl palmitate;
Higher fatty acid esters such as diethyl sebacate, higher fatty acid triglycerides; fatty acid (mono) diethanolamides; salicylic acid; salicylates. The absorption promoter is used alone or in combination of two or more, and is contained in the pressure-sensitive adhesive layer in an amount of 30% by weight or less.
本発明の経皮吸収貼付剤は、上記粘着基剤、支持体、薬
物および必要に応じて吸収促進剤などを用いて通常の貼
付剤に準じて調製される。例えば、粘着基剤となるポリ
マーの有機溶剤溶液に薬物および必要に応じて吸収促進
剤などを加えて、これを支持体表面の塗布し乾燥させ
る。剥離紙上に粘着剤層を形成し、これを支持体と密着
させてもよい。このような貼付剤調製時には、薬物は、
使用する粘着基剤(必要に応じて粘着性付与剤や吸収促
進剤を含む)の該薬物の飽和溶解度の1.2倍以上、好ま
しくは1.5〜3.0倍の割合で粘着剤中に配合する。粘着剤
中に混合された薬物は過飽和溶解状態で存在する。The percutaneous absorption patch of the present invention is prepared according to an ordinary patch using the above-mentioned adhesive base, support, drug and, if necessary, absorption promoter. For example, a drug and, if necessary, an absorption promoter are added to an organic solvent solution of a polymer serving as an adhesive base, and the support surface is coated and dried. A pressure-sensitive adhesive layer may be formed on the release paper and brought into close contact with the support. When preparing such a patch, the drug
It is blended in the pressure-sensitive adhesive at a ratio of 1.2 times or more, preferably 1.5 to 3.0 times, the saturated solubility of the drug of the pressure-sensitive adhesive base (including a tackifier and an absorption promoter if necessary). The drug mixed in the adhesive exists in a supersaturated dissolution state.
このような貼付剤を長期間保存すると、過飽和溶解状態
の薬物が微細な結晶となって粘着剤層中に徐々に析出す
るようになる。そのため、本発明においては、この貼付
剤は使用前に加熱される。加熱により、析出した薬物も
再び過飽和溶解状態となって粘着剤層中に存在するよう
になる。加熱の温度は、含有される薬物が粘着剤中に再
溶解できる温度であればよい。ここで、加熱とは、直接
熱を加えること以外に、電磁波を照射して分子運動を活
発化し熱を発生させる電子レンジなどによる処理をも包
含していう。When such a patch is stored for a long time, the drug in a supersaturated dissolution state becomes fine crystals and gradually precipitates in the pressure-sensitive adhesive layer. Therefore, in the present invention, this patch is heated before use. By heating, the precipitated drug again becomes in a supersaturated dissolution state and remains in the pressure-sensitive adhesive layer. The heating temperature may be any temperature at which the contained drug can be redissolved in the adhesive. Here, the term "heating" includes not only the direct application of heat but also the treatment by a microwave oven or the like that radiates an electromagnetic wave to activate molecular motion and generate heat.
このように薬物を過飽和溶解状態で含有する貼付剤は、
従来の薬物再結晶微粒子が粘着剤層に存在する貼付剤や
薬物が移行しうる支持体を備えた貼付剤に比べ、貼付剤
を皮膚表面に貼付したときの薬物濃度グラジェントが大
きい。従ってフイツクの拡散方程式による薬物経皮透過
量が大きくなる。本発明の経皮吸収貼付剤は、それゆえ
高い血中濃度レベルを長時間にわたって維持でき、バイ
オアベイラビリティが高い。薬物の初期放出性も良好で
ある。このような貼付剤を用いると、より小面積であっ
ても従来と同一レベルの薬効が得られる。Thus, the patch containing the drug in a supersaturated dissolution state,
The drug concentration gradient when the patch is applied to the skin surface is larger than that of the conventional patch in which the drug recrystallized fine particles are present in the pressure-sensitive adhesive layer and the patch including the support to which the drug can be transferred. Therefore, the percutaneous drug permeation amount according to the Fick's diffusion equation increases. Therefore, the transdermal patch of the present invention can maintain a high blood concentration level for a long time and has high bioavailability. The initial release of the drug is also good. When such a patch is used, the same level of medicinal effect as conventional can be obtained even with a smaller area.
(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−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87重量部に対しビニル
ピロリドンを13重量部の割合で含有する)の20重量%酢
酸エチル溶液100重量部に、イソソルビドジナイトレー
ト(ISDN)5重量部を添加し、ディゾルバーにて均一に
混合した。得られた溶液を、厚さ45μmのポリエチレン
テレフタレート(PET)製離型フィルム上に塗布し、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)支持体に積層して、経皮吸収貼付剤を
得た。粘着剤層の厚さは40μmであり、粘着剤層中の薬
物濃度は20重量%であった。上記粘着基材のISDN飽和溶
解度は11.1重量%である。Example 1 100 parts by weight of a 20% by weight ethyl acetate solution of 2 ethylhexyl acrylate-vinylpyrrolidone copolymer (containing 87 parts by weight of 2 ethylhexyl acrylate and 13 parts by weight of vinylpyrrolidone) was added to isosorbidogenite. A rate (ISDN) of 5 parts by weight was added and uniformly mixed by a dissolver. The obtained solution was applied on a polyethylene terephthalate (PET) release film having a thickness of 45 μm and dried to form a pressure-sensitive adhesive layer. This adhesive layer was laminated on a PET film (thickness 10 μm) support to obtain a transdermal patch. The pressure-sensitive adhesive layer had a thickness of 40 μm, and the drug concentration in the pressure-sensitive adhesive layer was 20% by weight. The ISDN saturated solubility of the adhesive substrate is 11.1% by weight.
このようにして得られた貼付剤を室温で3ヶ月間放置し
たところ、粘着剤層中にISDNの微細な結晶が析出した。
この貼付剤をギヤーオーブン中、70℃で10分間加熱し
た。ISDNの結晶は完全に溶解し、粘着剤中に過飽和溶解
状態で存在するようになった。このようにして得られた
経皮吸収貼付剤10cm3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。実施例2および比較例1〜
3の結果もあわせて表1に示す。When the thus obtained patch was left at room temperature for 3 months, fine ISDN crystals were precipitated in the pressure-sensitive adhesive layer.
The patch was heated in a gear oven at 70 ° C for 10 minutes. The ISDN crystals were completely dissolved and existed in the adhesive in a supersaturated dissolved state. 10 cm 3 of the transdermal absorption patch obtained in this manner 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. Example 2 and Comparative Examples 1-
The results of 3 are also shown in Table 1.
比較例1 ISDN結晶の析出した貼付剤を加熱せずにそのまま家兎背
部に貼付して血中濃度を測定したこと以外は実施例1と
同様である。Comparative Example 1 The same as Example 1 except that the patch on which ISDN crystals were deposited was directly applied to the back of the rabbit without heating and the blood concentration was measured.
比較例2 ISDN添加量を2.5重量部とすること以外は、実施例1と
同様の方法で経皮吸収貼付剤の調製を行なった。但し、
粘着剤層の厚さは80μmである。粘着剤層中のISDN濃度
は11.1重量%であり、3ヶ月経過後もISDNは粘着剤層中
に均一に溶解していた。Comparative Example 2 A transdermal patch was prepared in the same manner as in Example 1, except that the amount of ISDN added was 2.5 parts by weight. However,
The thickness of the adhesive layer is 80 μm. The ISDN concentration in the adhesive layer was 11.1% by weight, and ISDN was uniformly dissolved in the adhesive layer even after 3 months.
実施例2 粘着基剤溶液としてスチレン−イソプレン−スチレンブ
ロック共重合体25重量部、ポリイソプレンゴム25重量部
およびテルペン樹脂50重量部の混合物の20重量%テトラ
ヒドロフラン溶液を用い、ISDN 1.04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貼付剤を得
た。但し、粘着剤層の厚さは100μmである。粘着剤層
中のISDN濃度は4.94重量%であり、ISDNは均一に溶解し
ていた。上記粘着基剤のISDNの飽和溶解度は2.8重量%
である。Example 2 A 20 wt% tetrahydrofuran solution of a mixture of 25 parts by weight of styrene-isoprene-styrene block copolymer, 25 parts by weight of polyisoprene rubber and 50 parts by weight of terpene resin was used as an adhesive base solution, and 1.04 parts by weight of ISDN was added. A transdermal patch was obtained in the same manner as in Example 1 except for the above. However, the thickness of the adhesive layer is 100 μm. The ISDN concentration in the adhesive layer was 4.94% by weight, and ISDN was uniformly dissolved. The saturated solubility of ISDN of the above adhesive base is 2.8% by weight.
Is.
このようにして得られた貼付剤を室温で3ヶ月間放置し
たところ、粘着剤層中にISDNの微細な結晶が析出した。
この貼付剤をアルミ包材でシールし、沸騰水中で10分間
加熱した。ISDNの結晶は完全に溶解し、粘着剤中に過飽
和溶解状態で存在するようになった。この貼付剤を用
い、実施例1と同様の方法でISDNの血中濃度の測定を行
なった。When the thus obtained patch was left at room temperature for 3 months, fine ISDN crystals were precipitated in the pressure-sensitive adhesive layer.
The patch was sealed with an aluminum packaging material and heated in boiling water for 10 minutes. The ISDN crystals were completely dissolved and existed in the adhesive in a supersaturated dissolved state. Using this patch, the blood concentration of ISDN was measured in the same manner as in Example 1.
比較例3 ISDN結晶の析出した貼付剤を加熱せずにそのまま家兎背
部に貼付して血中濃度を測定したこと以外は実施例2と
同様である。Comparative Example 3 The same as Example 2 except that the patch on which ISDN crystals were deposited was directly applied to the back of the rabbit without heating and the blood concentration was measured.
実施例3 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97重量部に対し、ビニ
ルピロリドンを3重量部の割合で含有する)の20重量%
酢酸エチル溶液に、薬物としてインドメタシン2重量部
を添加し、実施例1に準じて経皮吸収貼付剤を得た。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。上記粘着基剤のインドメタシン飽
和溶解度は4.8重量%である。Example 3 20% by weight of 2 ethylhexyl acrylate-vinylpyrrolidone copolymer (containing 3 parts by weight of vinylpyrrolidone for 97 parts by weight of 2 ethylhexyl acrylate)
2 parts by weight of indomethacin as a drug was added to the ethyl acetate solution to obtain a transdermal patch in the same manner as in Example 1. The thickness of the adhesive layer is 50 μm, and the drug concentration in the adhesive layer is
It was 9.09% by weight. The saturated solubility of indomethacin of the above adhesive base is 4.8% by weight.
このようにして得られた貼付剤を室温で3ヶ月間放置し
たところ、粘着剤層中にインドメタシンの微細な結晶が
析出した。この貼付剤を電子レンジ(940W)で5分間
加熱した。インドメタシンの結晶は完全に溶解し、粘着
剤中に過飽和溶解状態で存在するようになった。この貼
付剤を用い、実施例1と同様の方法でインドメタシンの
血中濃度の測定を行なった。その結果を表2に示す。実
施例4および比較例4〜6の結果もあわせて表2に示
す。When the patch thus obtained was allowed to stand at room temperature for 3 months, fine crystals of indomethacin were precipitated in the pressure-sensitive adhesive layer. The patch was heated in a microwave oven (940W) for 5 minutes. The crystals of indomethacin were completely dissolved and became present in the adhesive in a supersaturated dissolved state. Using this patch, the blood concentration of indomethacin was measured in the same manner as in Example 1. The results are shown in Table 2. The results of Example 4 and Comparative Examples 4 to 6 are also shown in Table 2.
比較例4 インドメタシン結晶の析出した貼付剤を加熱せずにその
まま家兎背部に貼付して血中濃度を測定したこと以外は
実施例3と同様である。Comparative Example 4 The same as Example 3 except that the patch on which the indomethacin crystals were deposited was directly applied to the back of the rabbit without heating and the blood concentration was measured.
比較例5 インドメタシン添加量を1重量部にすること以外は、実
施例3と同様の方法で経皮吸収貼付剤を調製し、血中濃
度の測定を行なった。但し、粘着剤層の厚さは95μmで
あり、粘着剤層中の薬物濃度は、4.76重量%であり、3
ヶ月経過後も薬物は粘着剤層中に均一に溶解していた。Comparative Example 5 A transdermal patch was prepared in the same manner as in Example 3 except that the amount of indomethacin added was 1 part by weight, and the blood concentration was measured. However, the thickness of the adhesive layer was 95 μm, and the drug concentration in the adhesive layer was 4.76% by weight.
The drug was uniformly dissolved in the adhesive layer even after a lapse of months.
実施例4 粘着基剤溶液として天然ゴム55重量部およびテルペン樹
脂45重量部の混合物の15重量%テトラヒドロフラン溶液
を用い、薬物としてインドメタシン0.7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貼付剤を
得、血中濃度の測定を行なった。但し、粘着剤層の厚み
は100μmである。粘着剤層中にインドメタシンは均一
に溶解しており、その濃度は4.46重量%であった。本実
施例の粘着基剤のインドメタシン飽和溶解度は2.3重量
%である。Example 4 As Example 1 except that a 15 wt% tetrahydrofuran solution of a mixture of 55 parts by weight of natural rubber and 45 parts by weight of terpene resin was used as the adhesive base solution, and 0.7 part by weight of indomethacin was added as the drug. A transdermal patch was obtained and the blood concentration was measured. However, the thickness of the pressure-sensitive adhesive layer is 100 μm. Indomethacin was uniformly dissolved in the adhesive layer, and its concentration was 4.46% by weight. The saturated solubility of indomethacin of the adhesive base of this example is 2.3% by weight.
このようにして得られた貼付剤を室温で3ヶ月間放置し
たところ、粘着剤層中にインドメタシンの微細な結晶が
析出した。この貼付剤を電子レンジ(940W)で5分間
加熱した。インドメタシンの結晶は完全に溶解し、粘着
剤中に過飽和溶解状態で存在するようになった。この貼
付剤を用い、実施例1と同様の方法でインドメタシンの
血中濃度の測定を行なった。When the patch thus obtained was allowed to stand at room temperature for 3 months, fine crystals of indomethacin were precipitated in the pressure-sensitive adhesive layer. The patch was heated in a microwave oven (940W) for 5 minutes. The crystals of indomethacin were completely dissolved and became present in the adhesive in a supersaturated dissolved state. Using this patch, the blood concentration of indomethacin was measured in the same manner as in Example 1.
比較例6 インドメタシン結晶の析出した貼付剤を加熱せずにその
まま家兎背部に貼付して血中濃度を測定したこと以外は
実施例4と同様である。Comparative Example 6 The same as Example 4 except that the patch in which indomethacin crystals were deposited was directly applied to the back of the rabbit without heating and the blood concentration was measured.
表1および表2から、薬物が粘着剤層中に過飽和溶解状
態で存在する本発明の貼付剤を用いると薬物の血中濃度
が長時間にわたり高レベルに維持されることが明らかで
ある。薬物の初期血中濃度も高レベルであることがわか
る。 From Table 1 and Table 2, it is clear that the blood concentration of the drug is maintained at a high level for a long time by using the patch of the present invention in which the drug is present in the adhesive layer in a supersaturated dissolution state. It can be seen that the initial blood concentration of the drug is also high.
(発明の効果) 本発明によれば、このように、薬物が粘着剤層に過飽和
溶解状態で存在する経皮吸収貼付剤が得られる。この経
皮吸収貼付剤は、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、この経皮吸収貼付剤を皮
膚に貼付すれば、高レベルの薬物血中濃度が得られる。
薬物の初期血中濃度も高く、血中濃度の持続性にも優れ
る。(Effect of the Invention) According to the present invention, a transdermal patch in which the drug is present in the adhesive layer in a supersaturated dissolution state is thus obtained. This transdermal patch has excellent drug release properties. A sustained drug release is also obtained. As a result, when this transdermal patch is applied to the skin, a high level of blood drug concentration can be obtained.
The initial blood concentration of the drug is also high and the blood concentration is excellent in sustainability.
Claims (2)
℃で固体の薬物を含有する粘着剤層が形成された経皮吸
収貼付剤であって、 該粘着剤が該薬物を飽和溶解度以上の割合で含有し、 該貼付剤があらかじめ加熱され、該薬物が該粘着剤層中
に過飽和溶解状態で存在する、 経皮吸収貼付剤。1. A drug-impermeable support surface having at least 30
A percutaneously absorbable patch having a pressure-sensitive adhesive layer containing a drug which is solid at 0 ° C., wherein the adhesive contains the drug at a ratio of saturated solubility or more, and the patch is preheated to Is present in the pressure-sensitive adhesive layer in a supersaturated dissolution state.
2倍以上の割合で含有する特許請求の範囲第1項に記載
の経皮吸収貼付剤。2. The adhesive has a saturation solubility of 1.
The percutaneous absorption patch according to claim 1, which is contained at a ratio of 2 times or more.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP61240679A JPH066534B2 (en) | 1986-10-09 | 1986-10-09 | Transdermal patch |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP61240679A JPH066534B2 (en) | 1986-10-09 | 1986-10-09 | Transdermal patch |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPS6393714A JPS6393714A (en) | 1988-04-25 |
| JPH066534B2 true JPH066534B2 (en) | 1994-01-26 |
Family
ID=17063094
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP61240679A Expired - Lifetime JPH066534B2 (en) | 1986-10-09 | 1986-10-09 | Transdermal patch |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPH066534B2 (en) |
Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| EP3542862A1 (en) | 2018-03-22 | 2019-09-25 | Nitto Denko Corporation | Production method of pregabalin-containing composition and pregabalin-containing composition |
Families Citing this family (17)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPH03123727A (en) * | 1989-10-04 | 1991-05-27 | Nitto Denko Corp | Percutaneous absorption preparation |
| WO1992014442A1 (en) * | 1991-02-18 | 1992-09-03 | Commonwealth Scientific And Industrial Research Organisation | Composition for use in transdermal administration |
| US5906830A (en) * | 1995-09-08 | 1999-05-25 | Cygnus, Inc. | Supersaturated transdermal drug delivery systems, and methods for manufacturing the same |
| US6007837A (en) * | 1996-07-03 | 1999-12-28 | Alza Corporation | Drug delivery devices and process of manufacture |
| ATE226816T1 (en) * | 1996-07-03 | 2002-11-15 | Alza Corp | DEVICES FOR DRUG DELIVERY AND PRODUCTION METHOD |
| US6174545B1 (en) | 1997-07-01 | 2001-01-16 | Alza Corporation | Drug delivery devices and process of manufacture |
| WO2002043766A1 (en) * | 2000-11-29 | 2002-06-06 | Takeda Chemical Industries, Ltd. | Medicinal compositions and process for producing the same |
| DE10261696A1 (en) * | 2002-12-30 | 2004-07-15 | Schwarz Pharma Ag | Device for the transdermal administration of rotigotine base |
| JP4641394B2 (en) * | 2004-08-06 | 2011-03-02 | リンテック株式会社 | Method for producing transdermal preparation |
| US20080226698A1 (en) * | 2007-03-16 | 2008-09-18 | Mylan Technologies, Inc. | Amorphous drug transdermal systems, manufacturing methods, and stabilization |
| US8441800B2 (en) | 2009-03-26 | 2013-05-14 | Panasonic Corporation | Vehicle-mounted electronic device |
| DE102009052972A1 (en) | 2009-11-12 | 2011-09-15 | Lts Lohmann Therapie-Systeme Ag | Process for preventing the crystallization of drugs in a polymer film |
| US9155710B2 (en) | 2011-05-31 | 2015-10-13 | Hisamitsu Pharmaceutical Co., Inc. | Ropinirole-containing patch and package thereof |
| EP2716287B1 (en) | 2011-05-31 | 2017-11-15 | Hisamitsu Pharmaceutical Co., Inc. | Ropinirole-containing adhesive skin patch and packaged product thereof |
| JP5270035B1 (en) | 2012-12-06 | 2013-08-21 | 久光製薬株式会社 | Patch and method for producing the same |
| JP5307931B1 (en) | 2012-12-27 | 2013-10-02 | 久光製薬株式会社 | Patch and method for producing the same |
| JP5415645B1 (en) | 2013-06-28 | 2014-02-12 | 久光製薬株式会社 | Manufacturing method of patch, patch and package |
Citations (2)
| 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 |
| JPS61148117A (en) * | 1984-12-21 | 1986-07-05 | Sekisui Chem Co Ltd | Application agent and production thereof |
-
1986
- 1986-10-09 JP JP61240679A patent/JPH066534B2/en not_active Expired - Lifetime
Patent Citations (2)
| 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 |
| JPS61148117A (en) * | 1984-12-21 | 1986-07-05 | Sekisui Chem Co Ltd | Application agent and production thereof |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| EP3542862A1 (en) | 2018-03-22 | 2019-09-25 | Nitto Denko Corporation | Production method of pregabalin-containing composition and pregabalin-containing composition |
| US10952973B2 (en) | 2018-03-22 | 2021-03-23 | Nitto Denko Corporation | Production method of pregabalin-containing composition and pregabalin-containing composition |
Also Published As
| Publication number | Publication date |
|---|---|
| JPS6393714A (en) | 1988-04-25 |
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