JP5535640B2 - Fentanyl-containing transdermal absorption preparation - Google Patents
Fentanyl-containing transdermal absorption preparation Download PDFInfo
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- JP5535640B2 JP5535640B2 JP2009538162A JP2009538162A JP5535640B2 JP 5535640 B2 JP5535640 B2 JP 5535640B2 JP 2009538162 A JP2009538162 A JP 2009538162A JP 2009538162 A JP2009538162 A JP 2009538162A JP 5535640 B2 JP5535640 B2 JP 5535640B2
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- fentanyl
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- patch
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/33—Heterocyclic compounds
- A61K31/395—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
- A61K31/435—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
- A61K31/44—Non condensed pyridines; Hydrogenated derivatives thereof
- A61K31/445—Non condensed piperidines, e.g. piperocaine
- A61K31/4468—Non condensed piperidines, e.g. piperocaine having a nitrogen directly attached in position 4, e.g. clebopride, fentanyl
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/70—Web, sheet or filament bases ; Films; Fibres of the matrix type containing drug
- A61K9/7023—Transdermal patches and similar drug-containing composite devices, e.g. cataplasms
- A61K9/703—Transdermal patches and similar drug-containing composite devices, e.g. cataplasms characterised by shape or structure; Details concerning release liner or backing; Refillable patches; User-activated patches
- A61K9/7038—Transdermal patches of the drug-in-adhesive type, i.e. comprising drug in the skin-adhesive layer
- A61K9/7046—Transdermal patches of the drug-in-adhesive type, i.e. comprising drug in the skin-adhesive layer the adhesive comprising macromolecular compounds
- A61K9/7053—Transdermal patches of the drug-in-adhesive type, i.e. comprising drug in the skin-adhesive layer the adhesive comprising macromolecular compounds obtained by reactions only involving carbon to carbon unsaturated bonds, e.g. polyvinyl, polyisobutylene, polystyrene
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/70—Web, sheet or filament bases ; Films; Fibres of the matrix type containing drug
- A61K9/7023—Transdermal patches and similar drug-containing composite devices, e.g. cataplasms
- A61K9/703—Transdermal patches and similar drug-containing composite devices, e.g. cataplasms characterised by shape or structure; Details concerning release liner or backing; Refillable patches; User-activated patches
- A61K9/7038—Transdermal patches of the drug-in-adhesive type, i.e. comprising drug in the skin-adhesive layer
- A61K9/7046—Transdermal patches of the drug-in-adhesive type, i.e. comprising drug in the skin-adhesive layer the adhesive comprising macromolecular compounds
- A61K9/7053—Transdermal patches of the drug-in-adhesive type, i.e. comprising drug in the skin-adhesive layer the adhesive comprising macromolecular compounds obtained by reactions only involving carbon to carbon unsaturated bonds, e.g. polyvinyl, polyisobutylene, polystyrene
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- A—HUMAN NECESSITIES
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- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P25/00—Drugs for disorders of the nervous system
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Description
本発明は、有効成分としてフェンタニルまたはその塩を含有する経皮吸収製剤に関する。 The present invention relates to a transdermally absorbable preparation containing fentanyl or a salt thereof as an active ingredient.
従来、癌性疼痛の鎮痛剤として、フェンタニルまたはその塩を有効成分とする注射剤が使用されていたが、近年、注射剤以外にもフェンタニル含有経皮吸収剤が開発され、薬物の経皮吸収性を向上させることや鎮痛効果の持続性を高めることなどについて検討がなされてきた(特許文献1〜3)。
Conventionally, injections containing fentanyl or a salt thereof as an active ingredient have been used as analgesics for cancer pain. Recently, in addition to injections, fentanyl-containing transdermal absorption agents have been developed, and percutaneous absorption of drugs is performed. Studies have been made on improving the performance and increasing the sustainability of the analgesic effect (
市販されているフェンタニル含有経皮吸収剤として、例えば、デュロテップパッチ(Durotep Patch)(登録商標)が挙げられるが、このような従来のフェンタニルを含有する経皮吸収製剤は、3日間貼付し続けることが必要とされているものの、その鎮痛効果の変動が極めて大きく、患者に負担を強いるものであり、患者コンプライアンスが低下する場合があった。 Examples of commercially available fentanyl-containing transdermal absorption agents include Durotep Patch (registered trademark), and such conventional transdermal preparations containing fentanyl should be applied for 3 days. However, the analgesic effect fluctuates greatly, which imposes a burden on the patient and sometimes reduces patient compliance.
本発明の課題は、新たに、患者の負担の軽減されたフェンタニル含有経皮吸収製剤を提供することにある。 An object of the present invention is to newly provide a fentanyl-containing transdermal absorption preparation with a reduced burden on the patient.
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、フェンタニル含有経皮吸収製剤のように癌などの長期療養を余儀なくされる患者の疼痛を治療対象とする製剤にあっては、鎮痛効果の変動が大きいと患者コンプライアンスを低下させるとの新たな知見を得、この問題を解決するため、さらに研究したところ、フェンタニル含有経皮吸収製剤のピーク/トラフ値をより適切に調整することによって、鎮痛効果の変動を小さく抑えることができ、患者の負担を軽減できることを見出し、さらに研究を進めた結果、本発明を完成した。 In the preparations for treating pain of patients who are forced to undergo long-term treatment such as cancer, such as fentanyl-containing transdermal absorption preparations, while the inventors have intensively studied to solve the above problems, In order to solve this problem, we have obtained new findings that patient compliance is reduced when the fluctuation in analgesic effect is large, and the peak / trough value of fentanyl-containing transdermal preparations is adjusted more appropriately. As a result of finding that the fluctuation of the analgesic effect can be suppressed and the burden on the patient can be reduced, the present invention has been completed.
すなわち本発明は、フェンタニルまたはその塩を含有する、1日1回投与用フェンタニル含有経皮吸収製剤に関する。
また本発明は、1日1回投与を繰り返し、定常状態に達した後の、少なくとも連続する3日間において1日毎に測定した血中フェンタニル濃度の平均値および標準偏差値から得られるCV値(標準偏差値/平均値×100(%))が40%以下である、前記の経皮吸収製剤に関する。
さらに本発明は、1日1回投与を繰り返し、定常状態に達した後の、少なくとも連続する3日間において1日毎に測定した血中フェンタニル濃度の最大値に対する最小値の比(最小値/最大値)が0.5以上である、前記の経皮吸収製剤に関する。
また本発明は、前記経皮吸収製剤が1日1回投与を連続した場合、定常状態における血中フェンタニル濃度の平均ピーク/トラフ値が1.8以下である、前記の経皮吸収製剤に関する。That is, the present invention relates to a once-daily fentanyl-containing transdermal absorption preparation containing fentanyl or a salt thereof.
In addition, the present invention repeats administration once a day, reaches a steady state, and then obtains a CV value (standard) obtained from an average value and a standard deviation value of blood fentanyl concentration measured every day for at least three consecutive days. It is related with the said transdermally absorbable preparation whose deviation value / average value x100 (%)) is 40% or less.
The present invention further relates to the ratio of the minimum value (minimum value / maximum value) to the maximum value of blood fentanyl concentration measured every day for at least three consecutive days after repeated administration once a day and reaching a steady state. ) Is 0.5 or more.
The present invention also relates to the above transdermally absorbable preparation, wherein when the transdermally absorbable preparation is continuously administered once a day, the average peak / trough value of blood fentanyl concentration in a steady state is 1.8 or less.
また本発明は、支持体、粘着剤および剥離シートを含む貼付剤である、前記の経皮吸収製剤に関する。
さらに本発明は、貼付剤が、マトリックス型である、前記の経皮吸収製剤に関する。
また本発明は、フェンタニルまたはその塩を0.10〜0.45mg/cm2で含有する、前記の経皮吸収型製剤に関する。
さらに本発明は、フェンタニルまたはその塩を0.10〜0.45mg/cm2で粘着剤中に含有し、かつ、粘着剤の質量が2〜10mg/cm2である、前記の経皮吸収製剤に関する。Moreover, this invention relates to the said transdermally absorbable preparation which is a patch containing a support body, an adhesive, and a peeling sheet.
Furthermore, the present invention relates to the above transdermally absorbable preparation, wherein the patch is a matrix type.
The present invention also relates to the above-mentioned transdermal preparation containing fentanyl or a salt thereof at 0.10 to 0.45 mg / cm 2 .
Furthermore, the present invention provides the transdermally absorbable preparation described above, wherein fentanyl or a salt thereof is contained in the adhesive at 0.10 to 0.45 mg / cm 2 and the mass of the adhesive is 2 to 10 mg / cm 2. About.
また本発明は、1枚あたりのフェンタニルまたはその塩の含有量が1〜2mgの貼付剤である、前記の経皮吸収製剤に関する。
さらに本発明は、粘着剤が、スチレン−イソプレン−スチレンブロック共重合体を含む、前記の経皮吸収製剤に関する。
また本発明は、粘着剤が、アクリル系高分子を含む、前記の経皮吸収製剤に関する。
さらに本発明は、支持体が、延伸ポリエチレンテレフタレートを含む、前記の経皮吸収製剤に関する。The present invention also relates to the above transdermally absorbable preparation, which is a patch having a fentanyl or salt content of 1 to 2 mg per sheet.
Furthermore, this invention relates to the said percutaneous absorption preparation in which an adhesive contains a styrene-isoprene-styrene block copolymer.
The present invention also relates to the above transdermally absorbable preparation, wherein the adhesive contains an acrylic polymer.
Furthermore, the present invention relates to the transdermally absorbable preparation, wherein the support contains stretched polyethylene terephthalate.
本発明の1日1回投与用フェンタニル含有経皮吸収製剤は、従来の3日間貼付する3日投与用経皮吸収製剤と異なり、血中フェンタニル濃度のピーク/トラフ値が小さく、鎮痛効果の変動が最小限に抑えられるため、患者の負担が軽減される。また、癌性疼痛などの疼痛を効果的に抑制できる、より患者コンプライアンスの高い経皮吸収製剤を提供することができる。
特に癌などの長期療養を余儀なくさせる疾患の疼痛を治療対象とする経皮吸収剤においては、従来、より長い期間の薬効の持続性を求めるあまり、患者コンプライアンスへの配慮が十分とはいえなかったが、本発明の1日1回投与用フェンタニル含有経皮吸収製剤は、薬効が長期に持続し、かつ鎮痛効果の変動が小さいため、患者コンプライアンスの高い薬剤を提供することができる。The once-daily fentanyl-containing percutaneous absorption preparation of the present invention has a small peak / trough value of blood fentanyl concentration and changes in analgesic effect, unlike the conventional 3-day percutaneous absorption preparation applied for 3 days. Can be kept to a minimum, reducing the burden on the patient. In addition, a percutaneous absorption preparation with higher patient compliance that can effectively suppress pain such as cancer pain can be provided.
In particular, in the case of transdermal absorbents for treating pain of diseases that necessitate long-term medical treatment such as cancer, it has been difficult to consider patient compliance due to the long-term demand for sustained drug efficacy. However, the once-daily fentanyl-containing percutaneous absorption preparation of the present invention can provide a drug with high patient compliance since the drug effect lasts for a long time and the fluctuation in analgesic effect is small.
以下、本発明のフェンタニル含有経皮吸収製剤の好適な実施について詳細に説明する。
本発明のフェンタニル含有経皮吸収製剤は、フェンタニルまたはその塩を含有し、1日1回投与用として用いる。
また本発明における薬理活性物質は、フェンタニル自体またはその塩であり、フェンタニル塩としては、薬学的に許容し得る塩であれば、特に限定されず、無機塩であっても有機塩であってもよく、代表的なフェンタニル塩であるクエン酸塩、塩酸塩、フマル酸塩等を挙げることができる。これらの中でも、クエン酸フェンタニルは特に好ましい。また、フェンタニルまたはその塩は、単独で用いることもできるが、2種以上を混合して用いてもよい。Hereinafter, preferred implementation of the fentanyl-containing transdermal preparation of the present invention will be described in detail.
The fentanyl-containing transdermal absorption preparation of the present invention contains fentanyl or a salt thereof and is used for once-daily administration.
The pharmacologically active substance in the present invention is fentanyl itself or a salt thereof, and the fentanyl salt is not particularly limited as long as it is a pharmaceutically acceptable salt, and may be an inorganic salt or an organic salt. Well, citrate, hydrochloride, fumarate, and the like, which are typical fentanyl salts, can be mentioned. Of these, fentanyl citrate is particularly preferred. Moreover, although fentanyl or its salt can also be used independently, you may mix and use 2 or more types.
さらに本発明のフェンタニル含有経皮吸収製剤は、1日1回投与を繰り返すことで、定常状態に達した後の、少なくとも連続する3日間において1日毎(24時間毎)に測定した血中フェンタニルの濃度の平均値(例えば図2における168、192、216時間の血中濃度の平均値)および標準偏差値により得られるCV値(標準偏差値/平均値×100(%))を40%以下とすることができる。さらに好ましくはCV値を30%以下、さらに好ましくはCV値を20%以下とすることによって、より高い患者コンプライアンスを得ることが可能となる。本発明は、少なくとも連続する3日間において1日毎に測定した血中フェンタニルの濃度の平均値および標準偏差値により得られるCV値を所定の範囲に留めることにより、連続して安定な鎮痛効果を得ることができるのである。なおここで、標準偏差値/平均値とは、変動係数であり、CV値として表し、いわゆる、複数または個人の患者における血中フェンタニルの濃度の測定により求まる血中濃度の平均値とその標準偏差値を用いて計算されるバラツキの指標である。 Furthermore, the fentanyl-containing percutaneous absorption preparation of the present invention repeats administration once a day, so that the concentration of fentanyl in blood measured every day (every 24 hours) in at least three consecutive days after reaching a steady state. The CV value (standard deviation value / average value × 100 (%)) obtained from the average value of the concentration (for example, the average value of blood concentration at 168, 192, and 216 hours in FIG. 2) and the standard deviation value is 40% or less. can do. More preferably, by setting the CV value to 30% or less, more preferably 20% or less, higher patient compliance can be obtained. The present invention obtains a continuous analgesic effect by keeping the CV value obtained by the mean value and standard deviation value of the blood fentanyl concentration measured every day for at least 3 consecutive days within a predetermined range. It can be done. Here, the standard deviation value / average value is a coefficient of variation, expressed as a CV value, and the so-called average value of blood concentration obtained by measuring the concentration of blood fentanyl in a plurality or individual patients and its standard deviation. It is a variation index calculated using the value.
また本発明のフェンタニル含有経皮吸収製剤は、フェンタニルまたはその塩を含有し、1日1回投与用の経皮吸収製剤であって、1日1回投与を連続することによって、定常状態における血中フェンタニル濃度の平均ピーク/トラフ値が1.8以下とすることができ、定常状態における血中フェンタニル濃度の平均ピーク/トラフ値を所定の範囲に留めることにより、患者の鎮痛効果の変動を最小限に抑え、癌性疼痛などの患者の疼痛を軽減することができる。さらに好ましくは1.6以下、特に好ましくは、1.3以下とすることで、上記効果をより効果的に得ることが可能になる。 The fentanyl-containing transdermal absorption preparation of the present invention contains fentanyl or a salt thereof, and is a transdermal absorption preparation for once-daily administration. By continuously administering once a day, blood in a steady state is obtained. The average peak / trough value of the intermediate fentanyl concentration can be 1.8 or less, and the fluctuation of the analgesic effect of the patient is minimized by keeping the average peak / trough value of the blood fentanyl concentration in the steady state within a predetermined range. The pain of patients such as cancer pain can be reduced. More preferably, it is 1.6 or less, and particularly preferably 1.3 or less, the above-mentioned effect can be obtained more effectively.
なお、本発明におけるピーク/トラフ値とは、連続投与期間中の定常状態になった後に、経皮吸収製剤の適用期間(1日投与用の場合は1日間)におけるピーク(最大血中濃度)とトラフ(最小血中濃度)との比を意味する。前記定常状態とは、通常、投与開始から血中濃度の見かけ上の半減期の3倍以上の時間が経過した後の状態、または、血中濃度のピーク値もしくはトラフ値がほぼ一定に保たれる状態、すなわちその変動が20%以内にある状態をいう。 The peak / trough value in the present invention refers to the peak (maximum blood concentration) in the application period of the transdermally absorbable preparation (one day for daily administration) after the steady state during the continuous administration period. And the trough (minimum blood concentration). The steady state is usually a state after the time at least 3 times the apparent half-life of the blood concentration has elapsed from the start of administration, or the peak value or trough value of the blood concentration is kept almost constant. State in which the fluctuation is within 20%.
また本発明のフェンタニル含有経皮吸収製剤は、1日1回投与を繰り返すことにより、定常状態に達した後の、少なくとも連続する3日間において1日毎に測定した血中フェンタニル濃度の最大値に対する最小値の比(最小値/最大値)が0.5以上であることが好ましい。前記最小値/最大値をかかる範囲にすることにより、患者の鎮痛効果の変動を最小限に抑え、癌性疼痛などの患者の疼痛を軽減することができる。 In addition, the fentanyl-containing transdermal absorption preparation of the present invention is the minimum of the maximum value of the blood fentanyl concentration measured every day for at least 3 consecutive days after reaching a steady state by repeating administration once a day. The value ratio (minimum value / maximum value) is preferably 0.5 or more. By setting the minimum value / maximum value in such a range, it is possible to minimize fluctuations in the analgesic effect of the patient and reduce patient pain such as cancer pain.
なお、本発明における血中フェンタニル濃度の最大値に対する最小値の比とは、1日1回投与を繰り返し、定常状態に達した後の少なくとも連続する3日間において、少なくとも各日毎に平均血中フェンタニル濃度を測定し、血中フェンタニル濃度が測定した3日間のうち最大である日の値(最大値)と、最小である日の値(最小値)との比を意味する。 The ratio of the minimum value to the maximum value of the blood fentanyl concentration in the present invention is the average blood fentanyl at least every day for at least 3 consecutive days after repeated administration once a day and reaching a steady state. The concentration is measured, and the ratio of the maximum day value (maximum value) to the minimum day value (minimum value) among the three days in which the blood fentanyl concentration is measured is meant.
さらに本発明においては、経皮吸収製剤に含有されるフェンタニルまたはその塩の単位面積当たりの含有量が0.10〜0.45mg/cm2であることが好ましい。
本発明の経皮吸収製剤は、本発明の特徴である血中濃度の特性を示せば特に限定されないが、支持体、粘着剤および剥離シートを含む貼付剤とすることが好ましい。かかる貼付剤としては、特に限定されないが、リザーバー型、マトリックス型であってもよく、特に、有機溶媒中に薬物を含有させるリザーバー型よりも、粘着剤中に薬物を含有させるマトリックス型の方が、有機溶媒に起因する皮膚刺激、かぶれ等が生じにくいとの利点から、マトリックス型が好ましい。なお、マトリックス型とは、水などの液体を含んだ粘着剤層を有する場合も含まれる。Furthermore, in the present invention, the content per unit area of fentanyl or a salt thereof contained in the transdermally absorbable preparation is preferably 0.10 to 0.45 mg / cm 2 .
The percutaneously absorbable preparation of the present invention is not particularly limited as long as it shows the blood concentration characteristic of the present invention, but it is preferably a patch comprising a support, an adhesive and a release sheet. Such a patch is not particularly limited, but may be a reservoir type or a matrix type, and in particular, a matrix type containing a drug in an adhesive is more preferable than a reservoir type containing a drug in an organic solvent. From the advantage that skin irritation, rash and the like caused by an organic solvent hardly occur, the matrix type is preferable. Note that the matrix type includes a case where an adhesive layer containing a liquid such as water is included.
本発明の経皮吸収剤がマトリックス型の貼付剤である場合、該貼付剤における支持体を構成する材料は、薬物の支持体への移行を防止する観点から、ポリエステル系フィルムが好ましく、特にポリエチレンテレフタレートまたはポリエチレンテレフタレートとエチレン酢酸ビニル共重合体を含有するフェルムが好ましい。また、ポリエチレンテレフタレートとエチレン酢酸ビニル共重合体を含有するフィルムの場合はそれらを積層し使用することもできる。 When the transdermal absorbent of the present invention is a matrix-type patch, the material constituting the support in the patch is preferably a polyester film from the viewpoint of preventing migration of the drug to the support, particularly polyethylene. Ferme containing terephthalate or polyethylene terephthalate and ethylene vinyl acetate copolymer is preferred. In the case of a film containing polyethylene terephthalate and an ethylene vinyl acetate copolymer, they can be laminated and used.
ポリウレタンなどの伸縮性フィルム等を用いると、薬物の支持体への移行が認められる傾向があり、ポリエチレンテレフタレート等のポリエステル系フィルムを用いると、このようなフェンタニルの支持体への移行は減少する傾向にある。
さらに、フェルムには延伸型および非延伸型があるが、ポリエチレンテレフタレート製フィルムを用いた場合は延伸ポリエチレンテレフタレートを含むフィルムを用いた場合にフェンタニルまたはその塩の支持体への吸着も抑制されるため、結果として粘着剤に含有されるフェンタニルまたはその塩を効率的に経皮吸収製剤に用いることができ、本発明における血中濃度の特性が得られやすく特に好ましい。When stretchable films such as polyurethane are used, there is a tendency that migration of the drug to the support tends to be observed, and when polyester films such as polyethylene terephthalate are used, such transition of fentanyl to the support tends to decrease. It is in.
Furthermore, although there are stretched and non-stretched types of ferm, when a film made of polyethylene terephthalate is used, adsorption of fentanyl or its salt to the support is suppressed when a film containing stretched polyethylene terephthalate is used. As a result, fentanyl or a salt thereof contained in the pressure-sensitive adhesive can be efficiently used for a transdermally absorbable preparation, and the characteristics of blood concentration in the present invention are easily obtained, which is particularly preferable.
またポリエステル系フィルムを単独で使用する場合のその厚みについては、特に限定はないが、2〜50μmであることが好ましく、さらに好ましくは5〜40μm、特に20〜30μmであることが、製造時の取り扱い性や、貼付時の使用感などの観点から好ましい。
ポリエステル系フィルムは複層で用いてもよい。積層する素材については、特にその限定はないが、ポリエステル系繊維製の不織布、織布、ウレタン、エチレン酢酸ビニル共重合体膜などの柔らかい素材が好ましく、さらに不織布、織布、エチレン酢酸ビニル共重合体膜が好ましく、特にエチレン酢酸ビニル共重合体膜が好ましい。複層で用いる場合の厚みについては、特に限定はないが、積層した状態での厚みは同じ理由でポリエステル系フィルムを単層で用いる場合と同様な厚みで使用することができる。The thickness of the polyester film used alone is not particularly limited, but is preferably 2 to 50 μm, more preferably 5 to 40 μm, and particularly 20 to 30 μm. It is preferable from the viewpoints of handleability and the feeling of use at the time of sticking.
The polyester film may be used in multiple layers. The material to be laminated is not particularly limited, but a soft material such as a non-woven fabric made of polyester fiber, a woven fabric, urethane, an ethylene vinyl acetate copolymer film is preferable, and a non-woven fabric, woven fabric, ethylene vinyl acetate copolymer A combined membrane is preferred, and an ethylene vinyl acetate copolymer membrane is particularly preferred. Although there is no limitation in particular about the thickness in the case of using by a multilayer, it can use by the same thickness as the case where a polyester-type film is used by a single layer for the same reason as the thickness in the laminated state.
さらに、上記支持体に顔料(着色顔料)を練りこむことによって着色してもよい。例えば、酸化チタンを加えることによって白色の支持体とすることができる。このように白色とすることで、支持体表面に文字等を印刷しやすくなり、取扱いに注意を要する薬物を使用する際にも、取扱いの注意事項等をわかりやすく印刷することができる他、半透明であれば皮膚に貼付した際にはより目立たなくなるため患者の精神的負担もより軽減される場合がある。 Further, the support may be colored by kneading a pigment (color pigment). For example, a white support can be obtained by adding titanium oxide. This white color makes it easy to print letters on the surface of the support, and even when using drugs that require attention in handling, the handling precautions can be printed in an easy-to-understand manner. If it is transparent, it becomes less noticeable when applied to the skin, which may reduce the mental burden of the patient.
本発明において、支持体の透湿度は、15〜30g/m2・24hrであることが好ましい。この範囲の透湿度とすることで、貼付中、剥がれることなく、1日間貼付でき、本発明の効果が得られやすい傾向がある。
また支持体の曲げ剛性は、0.01〜0.20g・cm2/cmであることが好ましい。支持体の曲げ剛性が小さいと、貼付剤が絡み付いたり、シワになったりして取扱い性が困難になる傾向があり、他方、大きすぎると貼付剤が硬く、取り扱いが困難となるなどの問題を生じたりヒトの体の貼付部位の凹凸に合わせて貼付するのが困難になり、また、皮膚の少しの動きに対しても剥がれやすくなるため、貼付面積の変化により十分な薬物の効果が得られないおそれもあるからである。
また、フェンタニルまたはその塩は粘着剤全体の質量に基づいて、0.05〜20質量%の量で配合することが、透過量、製剤自体の物性の観点から好ましい。In the present invention, the moisture permeability of the support is preferably 15 to 30 g / m 2 · 24 hr. By setting the moisture permeability within this range, it can be applied for one day without peeling during application, and the effects of the present invention tend to be easily obtained.
Moreover, it is preferable that the bending rigidity of a support body is 0.01-0.20 g * cm < 2 > / cm. If the flexural rigidity of the support is small, the patch tends to become entangled or wrinkled, making it difficult to handle.On the other hand, if it is too large, the patch is hard and difficult to handle. It is difficult to apply it according to the unevenness of the application part of the human body, and it is easy to peel off even with a slight movement of the skin, so a sufficient drug effect can be obtained by changing the application area This is because there is a possibility of not.
Moreover, it is preferable to mix | blend a fentanyl or its salt with the quantity of 0.05-20 mass% based on the mass of the whole adhesive from the viewpoint of the permeation | transmission amount and the physical property of formulation itself.
本発明の経皮吸収製剤を貼付剤とした場合は、支持体の少なくとも一方の面に皮膚に接着するために粘着剤を有する。
この場合、粘着剤層の厚みは、20〜200μmであることが好ましい。この厚みが小さすぎると支持体上に粘着剤層をうまく延ばして塗ることができず、製造工程中不都合が生じ、また、透過速度もよくなくなる傾向があり、他方、厚みが大きすぎると製造工程上の不都合を生じ、また必要以上に薬物を用いることになり、無駄が生じる傾向があるからである。
また、フェンタニルまたはその塩を0.10〜0.45mg/cm2で粘着剤中に含有し、かつ、粘着剤層の質量が2〜10mg/cm2であることが好ましい。When the transdermally absorbable preparation of the present invention is used as a patch, it has an adhesive to adhere to the skin on at least one surface of the support.
In this case, the thickness of the pressure-sensitive adhesive layer is preferably 20 to 200 μm. If the thickness is too small, the pressure-sensitive adhesive layer cannot be extended and coated on the support, which causes inconveniences during the manufacturing process, and the permeation rate tends to be poor. On the other hand, if the thickness is too large, the manufacturing process This is because the above inconvenience occurs and the drug is used more than necessary, which tends to cause waste.
Moreover, it is preferable that fentanyl or its salt is contained in an adhesive at 0.10-0.45 mg / cm < 2 >, and the mass of an adhesive layer is 2-10 mg / cm < 2 >.
本発明の粘着剤に配合される脂溶性ポリマーは、特に限定されないが、好ましい例として、ポリイソブチレン(PIB)、スチレン−イソプレン−スチレンブロック共重合体(SIS)、イソプレンゴム、スチレン−ブタジエン−スチレンブロック共重合体(SBS)、アクリル系高分子(2−エチルヘキシルアクリレート、酢酸ビニル、メタクリレート、メトキシエチルアクリレート、アクリル酸の少なくとも2種の共重合体)等を挙げることができ、これらを単独または2種以上を混合して用いることができる。これらの中でも、PIB、SIS、アクリル系ポリマーを用いることが好ましい。
脂溶性ポリマーは、製剤自体の物性及び人体皮膚に対する良好な粘着力を考慮して、本発明の貼付剤の粘着剤全体の質量に基づいて、0.1〜98質量%、好ましくは0.1〜70質量%、さらに好ましくは0.1〜50質量%配合する。The fat-soluble polymer blended in the pressure-sensitive adhesive of the present invention is not particularly limited, but preferred examples include polyisobutylene (PIB), styrene-isoprene-styrene block copolymer (SIS), isoprene rubber, styrene-butadiene-styrene. Examples thereof include a block copolymer (SBS), an acrylic polymer (2-ethylhexyl acrylate, vinyl acetate, methacrylate, methoxyethyl acrylate, acrylic acid at least two types of copolymers) and the like. A mixture of seeds or more can be used. Among these, it is preferable to use PIB, SIS, and an acrylic polymer.
The fat-soluble polymer is 0.1 to 98% by mass, preferably 0.1 based on the total mass of the adhesive of the patch of the present invention, taking into consideration the physical properties of the preparation itself and good adhesion to human skin. -70 mass%, More preferably, 0.1-50 mass% is mix | blended.
本発明の粘着剤には、酢酸ナトリウムを配合することによって、フェンタニルまたはその塩の皮膚透過性が非常に高くなる。酢酸ナトリウムは、粘着剤全体の質量に基づいて、0.01〜15質量%、さらに0.01〜10質量%、特に0.01〜5質量%配合することが好ましい。酢酸ナトリウムの配合量が少ないと、皮膚透過性を著しく向上させるという効果が十分得られず、多すぎると、皮膚への刺激性が強くなる傾向があるからである。
フェンタニル塩がクエン酸フェンタニルの場合には、クエン酸フェンタニルと酢酸ナトリウムの配合質量比は物性及び皮膚透過性の面で効果が得られる配合比であればよいが、典型的には2:1の場合に最大の効果が得られる。酢酸ナトリウムの配合比が小さいと急激に薬物皮膚透過性が低下する傾向があり、逆に酢酸ナトリウムの配合比が大きいと不均一な製剤となり付着性が悪くなる傾向がある。By adding sodium acetate to the pressure-sensitive adhesive of the present invention, the skin permeability of fentanyl or a salt thereof becomes very high. Sodium acetate is preferably blended in an amount of 0.01 to 15% by mass, further 0.01 to 10% by mass, particularly 0.01 to 5% by mass, based on the mass of the entire pressure-sensitive adhesive. This is because if the amount of sodium acetate is small, the effect of remarkably improving skin permeability cannot be obtained sufficiently, and if it is too large, the irritation to the skin tends to increase.
When the fentanyl salt is fentanyl citrate, the blending mass ratio of fentanyl citrate and sodium acetate may be a blending ratio that is effective in terms of physical properties and skin permeability, but is typically 2: 1. The maximum effect is obtained. If the blending ratio of sodium acetate is small, the drug skin permeability tends to decrease rapidly, and conversely if the blending ratio of sodium acetate is large, it becomes a non-uniform preparation and adhesion tends to be poor.
なお、脂溶性ポリマ−の粘着性は低いので、製剤に粘着性を付与するために、製剤の粘着剤に、粘着付与剤を配合することができる。粘着付与剤としては、ポリテルペン樹脂系、石油樹脂系、ロジン系、ロジンエステル系、油溶性フェノ−ル樹脂系の粘着付与剤等を好ましい例として挙げることができる。粘着付与剤は、本発明の製剤の粘着剤全体の質量に基づいて、0.1〜70質量%、さらに5〜50質量%、特に10〜35質量%の量で配合されることが好ましい。 In addition, since the tackiness of the fat-soluble polymer is low, a tackifier can be added to the pressure-sensitive adhesive of the preparation in order to impart the pressure-sensitive adhesive to the preparation. Preferable examples of the tackifier include polyterpene resin-based, petroleum resin-based, rosin-based, rosin ester-based, and oil-soluble phenol resin-based tackifiers. The tackifier is preferably blended in an amount of 0.1 to 70% by mass, further 5 to 50% by mass, and particularly 10 to 35% by mass based on the mass of the entire adhesive of the preparation of the present invention.
また、本発明の貼付剤の加工性の向上や粘着性の調整のために、粘着剤に油脂を可塑剤として配合することもできる。油脂としては、例えば、流動パラフィン、スクワラン、オリ−ブ油、ツバキ油、バーショック油、ラッカセイ油等が好ましく、特に流動パラフィンは好ましい。油脂は、本発明の製剤の粘着剤全体の質量に基づいて、1.0〜70質量%、さらに10〜60質量%、特に20〜50質量%の量で配合されることが好ましい。 Moreover, fats and oils can also be mix | blended with an adhesive as a plasticizer for the improvement of the workability of the patch of this invention, and adjustment of adhesiveness. As fats and oils, for example, liquid paraffin, squalane, olive oil, camellia oil, bar shock oil, peanut oil and the like are preferable, and liquid paraffin is particularly preferable. It is preferable that fats and oils are mix | blended in the quantity of 1.0-70 mass%, further 10-60 mass%, especially 20-50 mass% based on the mass of the whole adhesive of the formulation of this invention.
また、本発明の製剤の粘着剤には、必要に応じて吸収促進剤を配合することもできる。吸収促進剤としては、皮膚での吸収促進作用が認められている化合物であればいずれのものでもよく、例えば炭素鎖数6〜20の脂肪酸、脂肪族アルコ−ル、脂肪酸エステルまたはエーテル、芳香族系有機酸、芳香族系アルコ−ル、芳香族系有機酸エステルまたはエ−テルを挙げることができる。さらに、乳酸エステル類、酢酸エステル類、モノテルペン系化合物、セスキテルペン系化合物、アゾン(Azone)またはその誘導体、グリセリン脂肪酸エステル類、ソルビタン脂肪酸エステル類、ポリソルベート系、ポリエチレングリコ−ル脂肪酸エステル類、ポリオキシエチレン硬化ヒマシ油系、ショ糖脂肪酸エステル類等を挙げることができる。具体的には、カプリル酸、カプリン酸、カプロン酸、ラウリン酸、ミリスチン酸、パルミチン酸、ステアリン酸、オレイン酸、リノール酸、リノレン酸、ラウリルアルコール、ミリスチルアルコール、オレイルアルコール、セチルアルコール、ラウリン酸メチル、ミリスチン酸イソプロピル、ミリスチン酸ミリスチル、ミリスチン酸オクチルドデシル、パルミチン酸セチル、サリチル酸、サリチル酸メチル、サリチル酸エチレングリコール、ケイ皮酸、ケイ皮酸メチル、クレゾール、乳酸セチル、酢酸エチル、酢酸プロピル、ゲラニオール、チモール、オイゲノール、テルピネオール、l−メントール、ボルネオロール、d−リモネン、イソオイゲノール、イソボルネオール、ネロール、dl−カンフル、グリセリンモノラウレート、グリセリンモノオレエート、ソルビタンモノラウレート、ショ糖モノラウレート、ポリソルベート20、ポリエチレングリコールモノラウレート、ポリエチレングリコールモノステアレート、HCO−60(硬化ヒマシ油)、1−[2−(デシルチオ)エチル]アザシクロペンタン−2−オン(以下、「ピロチオデカン」と略記する。)が好ましく、特に、ラウリルアルコール、ミリスチルアルコール、サリチル酸エチレングリコール、ピロチオデカンが好ましい。 Moreover, an absorption promoter can also be mix | blended with the adhesive of the formulation of this invention as needed. The absorption enhancer may be any compound as long as it has a skin absorption promoting effect. For example, a fatty acid having 6 to 20 carbon chains, aliphatic alcohol, fatty acid ester or ether, aromatic And organic organic acids, aromatic alcohols, aromatic organic acid esters and ethers. Furthermore, lactic acid esters, acetate esters, monoterpene compounds, sesquiterpene compounds, Azone or its derivatives, glycerin fatty acid esters, sorbitan fatty acid esters, polysorbate, polyethylene glycol fatty acid esters, poly Examples thereof include oxyethylene hydrogenated castor oil type and sucrose fatty acid esters. Specifically, caprylic acid, capric acid, caproic acid, lauric acid, myristic acid, palmitic acid, stearic acid, oleic acid, linoleic acid, linolenic acid, lauryl alcohol, myristyl alcohol, oleyl alcohol, cetyl alcohol, methyl laurate , Isopropyl myristate, myristyl myristate, octyldodecyl myristate, cetyl palmitate, salicylic acid, methyl salicylate, ethylene glycol salicylate, cinnamic acid, methyl cinnamate, cresol, cetyl lactate, ethyl acetate, propyl acetate, geraniol, thymol Eugenol, terpineol, l-menthol, borneol, d-limonene, isoeugenol, isoborneol, nerol, dl-camphor, glycerin monolaurate, glyce Monooleate, sorbitan monolaurate, sucrose monolaurate, polysorbate 20, polyethylene glycol monolaurate, polyethylene glycol monostearate, HCO-60 (hardened castor oil), 1- [2- (decylthio) ethyl] azacyclopentane 2-one (hereinafter abbreviated as “pyrothiodecane”) is preferable, and lauryl alcohol, myristyl alcohol, ethylene glycol salicylate, and pyrothiodecane are particularly preferable.
このような吸収促進剤は、本発明の製剤の粘着剤全質量に基づいて、0.01〜20質量%が好ましく、さらに0.1〜10質量%が、特に0.5〜5質量%の量で配合されることが好ましい。吸収促進剤の配合量が多すぎると、発赤、浮腫等の皮膚への刺激性が認められ、少なすぎると吸収促進剤の配合の効果が得られない傾向があるからである。 Such an absorption promoter is preferably 0.01 to 20% by weight, more preferably 0.1 to 10% by weight, particularly 0.5 to 5% by weight, based on the total weight of the adhesive of the preparation of the present invention. It is preferable to mix | blend in quantity. This is because if the amount of the absorption enhancer is too large, irritation to the skin such as redness and edema is observed, and if it is too small, the effect of the absorption enhancer tends not to be obtained.
さらに、本発明の貼付剤において、皮膚から発生した汗等の水性成分を吸収させるために、必要に応じて親水性ポリマ−を配合することもできる。親水性ポリマ−としては、例えば、軽質無水ケイ酸、セルロ−ス誘導体(カルボキシメチルセルロース(CMC)、カルボキシメチルセルロースナトリウム(CMCNa)、メチルセルロース(MC)、ヒドロキシプロピルメチルセルロース(HPMC)、ヒドロキシプロピルセルロース(HPC)、ヒドロキシエチルセルロース(HEC)、デンプン誘導体(プルラン)、ポリビニルアルコール(PVA)、ポリビニルピロリドン(PVP)、酢酸ビニル(VA)、カルボキシビニルポリマー(CVP)、エチル酢酸ビニル(EVA)、オイドラギット(商品名)、ゼラチン、ポリアクリル酸、ポリアクリル酸ソーダ、ポリイソブチレン無水マレイン酸共重合体、アルギン酸、アルギン酸ナトリウム、カラギーナン、アラビアゴム、トラガント、カラヤゴム、ポリビニルメタクリレートが好ましく、特に軽質無水ケイ酸、セルロース誘導体(CMCNa、HPMC、HPC、MC)、オイドラギットが好ましい。
親水性ポリマーは、本発明の貼付剤の粘着剤全体の質量に基づいて、0.1〜20質量%、特に0.5〜10質量%配合することが好ましい。Furthermore, in the patch of the present invention, a hydrophilic polymer can be blended as necessary to absorb aqueous components such as sweat generated from the skin. Examples of the hydrophilic polymer include light anhydrous silicic acid, cellulose derivatives (carboxymethylcellulose (CMC), sodium carboxymethylcellulose (CMCNa), methylcellulose (MC), hydroxypropylmethylcellulose (HPMC), and hydroxypropylcellulose (HPC). , Hydroxyethyl cellulose (HEC), starch derivative (pullulan), polyvinyl alcohol (PVA), polyvinyl pyrrolidone (PVP), vinyl acetate (VA), carboxyvinyl polymer (CVP), ethyl vinyl acetate (EVA), Eudragit (trade name) , Gelatin, polyacrylic acid, sodium polyacrylate, polyisobutylene maleic anhydride copolymer, alginic acid, sodium alginate, carrageenan, gum arabic, traga DOO, karaya, polyvinyl methacrylate are preferable, and light silicic anhydride, cellulose derivatives (CMCNa, HPMC, HPC, MC), Eudragit are preferred.
The hydrophilic polymer is preferably blended in an amount of 0.1 to 20% by mass, particularly 0.5 to 10% by mass, based on the mass of the entire adhesive of the patch of the present invention.
また、本発明の貼付剤の粘着剤には、架橋剤、防腐剤、抗酸化剤等のその他の成分を配合することができる。
架橋剤としては、アミノ樹脂、フェノ−ル樹脂、エポキシ樹脂、アルキド樹脂、不飽和ポリエステル等の熱硬化性樹脂、イソシアネ−ト化合物、ブロックイソシアネート化合物、有機系架橋剤、金属または金属化合物等の無機系架橋剤が好ましい。防腐剤としては、パラオキシ安息香酸エチル、パラオキシ安息香酸プロピル、パラオキシ安息香酸ブチル等が好ましい。抗酸化剤としては、トコフェロ−ルおよびそのエステル誘導体、アスコルビン酸、ステアリン酸エステル、ノルジヒトログアレチン酸、ジブチルヒドロキシトルエン(BHT)、ブチルヒドロキシアニソ−ル(BHA)等が好ましい。なお、本発明の貼付剤の粘着剤は、非水系の基材からなることが特に好ましい。The adhesive of the patch of the present invention can contain other components such as a crosslinking agent, preservative, and antioxidant.
Examples of the crosslinking agent include amino resins, phenol resins, epoxy resins, alkyd resins, unsaturated polyester, and other thermosetting resins, isocyanate compounds, blocked isocyanate compounds, organic crosslinking agents, metals, and metal compounds such as inorganic compounds. System crosslinking agents are preferred. As the preservative, ethyl paraoxybenzoate, propyl paraoxybenzoate, butyl paraoxybenzoate and the like are preferable. As the antioxidant, tocopherol and its ester derivatives, ascorbic acid, stearic acid ester, nordihuman logaretic acid, dibutylhydroxytoluene (BHT), butylhydroxyanisole (BHA) and the like are preferable. The adhesive of the patch of the present invention is particularly preferably composed of a non-aqueous base material.
上記粘着剤は、いずれの方法によっても製造することができる。例えば、溶剤法により製造する場合には、配合されるポリマ−の有機溶剤溶液に、他の成分を添加、撹拌後、支持体に伸展し、乾燥させて本製剤を得ることができる。また、配合されるポリマ−がホットメルト法により塗工可能である場合には、高温でポリマ−成分を溶解させた後、他の成分を添加し、撹拌し、支持体に伸展して本発明の貼付剤を得ることができる。 The pressure-sensitive adhesive can be produced by any method. For example, in the case of producing by the solvent method, other components are added to the organic solvent solution of the polymer to be blended, and after stirring, it is extended to a support and dried to obtain this preparation. Further, when the polymer to be blended can be applied by the hot melt method, after the polymer component is dissolved at a high temperature, the other components are added, stirred, and extended to the support. Can be obtained.
また、本発明の貼付剤の面積は、十分な薬物の効果が得られる面積ならば特に制限はないが、5〜60cm2であることが、薬効効果、取り扱い性、皮膚刺激などの観点から好ましい。
そして、本発明の上記により構成される貼付剤においては、粘着剤中にフェンタニルまたはその塩を含有し、その単位面積当たりの含有量が0.10〜0.45mg/cm2、かつ、粘着剤の単位面積あたり質量が2〜10mg/cm2とすることが好ましい。かかる範囲にすることにより、本発明のフェンタニルの血中濃度の特性が生じやすくなる傾向がある。Further, the area of the patch of the present invention is not particularly limited as long as it is an area where a sufficient drug effect can be obtained, but it is preferably 5 to 60 cm 2 from the viewpoint of medicinal effect, handleability, skin irritation and the like. .
And in the patch comprised by the above of this invention, fentanyl or its salt is contained in an adhesive, The content per unit area is 0.10-0.45 mg / cm < 2 >, and an adhesive The mass per unit area is preferably 2 to 10 mg / cm 2 . By setting it in such a range, there is a tendency that characteristics of blood concentration of fentanyl of the present invention are likely to occur.
本発明の経皮吸収製剤はまた、1枚あたりのフェンタニルまたはその塩の含有量が1〜10mgの貼付剤とすることができ、1〜2mgの低用量であってもよい。
また、癌性疼痛の痛みの程度において、各々使い分けられるように、例えば、1枚あたりのフェンタニルまたはその塩の含有量が、1〜10mg含まれる1種または2種以上の貼付剤を組合せて、1日1回の投与において用量を調節することができるように規格されている貼付剤とすることができる。このようにすることで各種の癌による疼痛の緩和を目的とでき、例えば痛みが酷いときなどに用量を調節できる。The transdermally absorbable preparation of the present invention can also be a patch with a content of fentanyl or a salt thereof of 1 to 10 mg, and may be a low dose of 1 to 2 mg.
In addition, for example, in combination with one or more patches containing 1 to 10 mg of fentanyl or a salt thereof, so that each can be properly used in the degree of pain of cancer pain, The patch can be standardized so that the dose can be adjusted by administration once a day. By doing in this way, it can aim at the relief of the pain by various cancers, for example, when the pain is severe, the dose can be adjusted.
剥離シートとしては、剥離処理を施した剥離紙(離型紙)、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。
なお、本発明の経皮吸収製剤は、本発明のフェンタニルの血中濃度の特性を示すことができれば特に貼付剤に限られるわけではなく、ゲル剤、クリーム剤等の塗布剤でもよいし、さらに貼付剤においても支持体、粘着剤のみからなる必要もなく、場合によっては薬物透過性を調整する膜や透過性を促進するためのマイクロニードル等の種々の構造を備えてもよい。Examples of the release sheet include release paper (release paper) that has been subjected to release treatment, cellophane, polyethylene, polypropylene, polyvinyl chloride, polyester, polyvinylidene chloride, and silicon processed paper.
The transdermally absorbable preparation of the present invention is not particularly limited to a patch as long as it can exhibit the blood concentration characteristics of the fentanyl of the present invention, and may be a coating agent such as a gel or cream, The patch does not need to be composed only of a support and an adhesive, and may be provided with various structures such as a membrane for adjusting drug permeability and a microneedle for promoting permeability depending on circumstances.
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。 EXAMPLES Hereinafter, although an Example is given and this invention is demonstrated in detail, this invention is not limited to these Examples.
実施例1
(処方)
成分名 含有量(%)
SIS 16.0
PIB 7.0
脂環族飽和炭化水素樹脂 40.0
流動パラフィン 31.0
酢酸ナトリウム 2.0
クエン酸フェンタニル 4.0
全量 100.0Example 1
(Prescription)
Ingredient name Content (%)
SIS 16.0
PIB 7.0
Alicyclic saturated hydrocarbon resin 40.0
Liquid paraffin 31.0
Sodium acetate 2.0
Fentanyl citrate 4.0
Total amount 100.0
(製法)
クエン酸フェンタニル、酢酸ナトリウムおよび流動パラフィンを乳鉢に取りよく混合した後、トルエンに溶解した残りの成分と混合した。得られた混合物を離型紙(剥離シート)上に塗工後、溶剤を乾燥除去し、延伸PET支持体(厚み:20μm)と貼り合わせて経皮吸収製剤(マトリックス型)を得た。なお、クエン酸フェンタニルを含有する粘着剤は50g/m2とした(単位面積あたりのクエン酸フェンタニル:0.2/cm2)。(Manufacturing method)
Fentanyl citrate, sodium acetate and liquid paraffin were mixed in a mortar and mixed with the remaining ingredients dissolved in toluene. After coating the obtained mixture on a release paper (release sheet), the solvent was removed by drying, and the mixture was bonded to a stretched PET support (thickness: 20 μm) to obtain a transdermal absorption preparation (matrix type). The pressure-sensitive adhesive containing fentanyl citrate was 50 g / m 2 (fentanyl citrate per unit area: 0.2 / cm 2 ).
実施例2
(処方)
成分名 含有量(%)
アクリル粘着剤(Duro−Tak387−2287) 80.0
ミリスチン酸イソプロピル 10.0
フェンタニル 10.0
全量 100.0Example 2
(Prescription)
Ingredient name Content (%)
Acrylic adhesive (Duro-Tak387-2287) 80.0
Isopropyl myristate 10.0
Fentanyl 10.0
Total amount 100.0
(製法)
フェンタニルおよびミリスチン酸イソプロピルを乳鉢に取りよく混合した後、アクリル粘着剤溶液と混合した。得られた混合物を離型紙(剥離シート)上に塗工後、溶剤を乾燥除去し、延伸PET支持体(厚み:20μm)と貼り合わせて経皮吸収製剤(マトリックス型)を得た。なお、フェンタニルを含有する粘着剤は30g/m2とした(単位面積あたりのフェンタニル:0.3mg/cm2)。(Manufacturing method)
Fentanyl and isopropyl myristate were placed in a mortar and mixed well, and then mixed with an acrylic adhesive solution. After coating the obtained mixture on a release paper (release sheet), the solvent was removed by drying, and the mixture was bonded to a stretched PET support (thickness: 20 μm) to obtain a transdermal absorption preparation (matrix type). The pressure-sensitive adhesive containing fentanyl was 30 g / m 2 (fentanyl per unit area: 0.3 mg / cm 2 ).
実施例3
(処方)
成分名 含有量(%)
アクリル粘着剤(Duro−Tak387−2516) 90.0
フェンタニル 10.0
全量 100.0Example 3
(Prescription)
Ingredient name Content (%)
Acrylic adhesive (Duro-Tak387-2516) 90.0
Fentanyl 10.0
Total amount 100.0
(製法)
フェンタニルとアクリル粘着剤溶液と混合し、得られた混合物を離型紙(剥離シート)上に塗工後、溶剤を乾燥除去し、延伸PET支持体(厚み:20μm)と貼り合わせて経皮吸収製剤(マトリックス型)を得た。なお、フェンタニルを含有する粘着剤は20g/m2とした(単位面積あたりのフェンタニル:0.2mg/cm2)。(Manufacturing method)
Fentanyl and an acrylic adhesive solution are mixed, and the resulting mixture is coated on a release paper (release sheet), then the solvent is removed by drying, and bonded to a stretched PET support (thickness: 20 μm) to be transdermally absorbed. (Matrix type) was obtained. The pressure-sensitive adhesive containing fentanyl was 20 g / m 2 (fentanyl per unit area: 0.2 mg / cm 2 ).
実施例4
実施例1の支持体を、延伸PET支持体から延伸PETとEVA膜とのラミネート支持体(3M社製:ScotchPak9732)へ変更した以外は同じ製法で経皮吸収製剤(マトリックス型)を得た。Example 4
A transdermally absorbable preparation (matrix type) was obtained by the same production method except that the support of Example 1 was changed from a stretched PET support to a laminate support of stretched PET and EVA membrane (manufactured by 3M: ScotchPak9732).
実施例5
実施例2の支持体を、延伸PET支持体から延伸PETとEVA膜とのラミネート支持体(3M社製:ScotchPak9732)へ変更した以外は同じ製法で経皮吸収製剤(マトリックス型)を得た。Example 5
A percutaneously absorbable preparation (matrix type) was obtained by the same production method except that the support of Example 2 was changed from a stretched PET support to a laminate support of stretched PET and EVA membrane (manufactured by 3M: ScotchPak9732).
実施例6
実施例3の支持体を、延伸PET支持体から延伸PETとEVA膜とのラミネート支持体(3M社製:ScotchPak9732)へ変更した以外は同じ製法で経皮吸収製剤(マトリックス型)を得た。Example 6
A transdermal absorption preparation (matrix type) was obtained by the same production method except that the support of Example 3 was changed from a stretched PET support to a laminate support of stretched PET and EVA membrane (manufactured by 3M: ScotchPak9732).
試験例1
実施例1に記載のクエン酸フェンタニルを4%含有する貼付剤10cm2について、成人5人を対象に1日(24時間)貼付、また、別の成人5人を対象に3日(72時間)貼付を夫々行い、経時的に採血を行なった。次いで、得られた血液中の血中フェンタニル濃度を、ガスクロマトグラフィー・マススペクトロメトリー法にて測定した。測定結果を基に、1日貼付を14回連続して行い、3日貼付を5回連続して行った場合の一例のグラフを図1に示す。Test example 1
About 10 cm 2 of a patch containing 4% of fentanyl citrate described in Example 1, it was applied to 5 adults for 1 day (24 hours), and another 5 adults for 3 days (72 hours) Pasting was performed, and blood was collected over time. Next, the blood fentanyl concentration in the obtained blood was measured by gas chromatography / mass spectrometry. Based on the measurement results, a graph of an example when the 1-day sticking is performed 14 times continuously and the 3-day sticking is performed 5 times continuously is shown in FIG.
表1は、上記結果から得られる各貼付時間でのピーク/トラフ値を示す。
試験例2
実施例1に記載のクエン酸フェンタニルを4%含有する貼付剤10cm2について、成人7人を対象に1日貼付を連続9回実施し、また、別の成人7人を対象に3日貼付を連続3回実施し、それぞれ経時的に採血を行なった。次いで、得られた血液中の血中フェンタニル濃度をガスクロマトグラフィー・マススペクトロメトリー法にて測定した。
上記の各々群における貼付後6日目(144時間)以降のフェンタニル平均血中濃度(C)の推移を図2に示す。Test example 2
About 10 cm 2 of the patch containing 4% of fentanyl citrate described in Example 1, it was applied 9 times a day for 7 adults, and 3 days for another 7 adults. The test was performed three times in succession, and blood was collected over time. Subsequently, the blood fentanyl concentration in the obtained blood was measured by a gas chromatography / mass spectrometry method.
FIG. 2 shows the transition of fentanyl mean blood concentration (C) after 6 days (144 hours) after application in each of the above groups.
また、血中フェンタニル濃度が定常状態に達した日以降の任意の連続する3日間における、血中フェンタニル濃度の平均値および標準偏差値を求め、それから得られる各群のCV値(標準偏差値/平均値×100(%))を表2に示す。
また、血中フェンタニル濃度が定常状態に達した日以降の任意の連続する3日間における、各群の血中フェンタニル濃度の最大値/最小値の比を表3に示す。
試験例3
実施例1〜6で用いた支持体を、約70mmφに打ち抜き、試験片とし、JIS Z0208条件Bに準じて透湿度試験を行なった(各々n=3)。
試験の結果、実施例1〜6で用いた支持体の透湿度は、19〜26g/m2・24hrであった。Test example 3
The support used in Examples 1 to 6 was punched out to about 70 mmφ to obtain a test piece, and a moisture permeability test was performed in accordance with JIS Z0208 Condition B (each n = 3).
As a result of the test, the moisture permeability of the support used in Examples 1 to 6 was 19 to 26 g / m 2 · 24 hr.
試験例4
実施例1〜6で用いた支持体を3cm幅に切り取って試料とし、純曲げ試験機(KES-FB-M2測定機械装置、カトーテック株式会社製)にセットし、曲率を0.5〜1.5cm−1にて測定した。
測定の結果、実施例1〜6で用いた支持体の曲げ剛性は、0.0363〜0.0716g・cm2/cmであった。Test example 4
The support used in Examples 1 to 6 was cut to a width of 3 cm to obtain a sample, which was set in a pure bending tester (KES-FB-M2 measuring machine, manufactured by Kato Tech Co., Ltd.), and the curvature was 0.5 to 1 Measured at 0.5 cm −1 .
As a result of the measurement, the bending rigidity of the support used in Examples 1 to 6 was 0.0363 to 0.0716 g · cm 2 / cm.
試験例5
実施例1記載の製剤を3日貼付した場合と、1日貼付した場合の疼痛抑制効果を比較するため、以下の試験を行なった。
同一患者に、実施例1記載の製剤を、3回連続して3日貼付(9日間)し、さらに続けて同製剤を、3回連続して1日貼付(3日間)し(計12日間)、3回目の3日貼付(第7〜9日目)以降の各日のVAS値(痛みの指標)を測定した。Test Example 5
In order to compare the pain-suppressing effect when the preparation described in Example 1 was applied for 3 days and when applied for 1 day, the following test was performed.
To the same patient, the preparation described in Example 1 was applied 3 times in succession for 3 days (9 days), and then the preparation was applied 3 times in succession for 1 day (3 days) (total 12 days). ) The VAS value (pain index) of each day after the third 3rd day application (7th to 9th days) was measured.
3日貼付を2回繰り返し、3回目を開始してから24時間後を基準とし(VAS値を1とする)その後24時間ごとにVAS値の変化率を求め、図3にその推移を示す。
その結果、3日貼付の場合は、3回目の貼付後48時間を経過した後に、VAS値が上昇し、痛みが増強したが、1日貼付に(第10日目以降)に切り替えた後には、VAS値が再び低下し、一旦増強した痛みを抑制した。Three days pasting was repeated twice, and the change rate of the VAS value was obtained every 24 hours after 24 hours from the start of the third time (VAS value is 1), and the transition is shown in FIG.
As a result, in the case of 3-day application, after 48 hours had elapsed after the third application, the VAS value increased and the pain increased, but after switching to 1-day application (after the 10th day) , VAS value decreased again, and once enhanced pain was suppressed.
Claims (12)
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| JP2009538162A JP5535640B2 (en) | 2007-10-17 | 2008-10-17 | Fentanyl-containing transdermal absorption preparation |
| PCT/JP2008/068836 WO2009051217A1 (en) | 2007-10-17 | 2008-10-17 | Fentanyl-containing percutaneous absorption preparation |
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| JP5631854B2 (en) * | 2010-12-13 | 2014-11-26 | 久光製薬株式会社 | Pharmaceutical composition and patch |
| CN107106552A (en) * | 2014-12-19 | 2017-08-29 | 3M创新有限公司 | Transdermal drug delivery device comprising fentanyl |
| US20200297654A1 (en) | 2017-10-17 | 2020-09-24 | Lubrizol Advanced Materials, Inc. | Composition and device for delivery of active agents to skin surfaces |
| JP7179501B2 (en) * | 2018-06-06 | 2022-11-29 | 久光製薬株式会社 | Patches containing fentanyl |
| JP7260726B1 (en) | 2018-06-06 | 2023-04-18 | 久光製薬株式会社 | Patches containing fentanyl |
| JP7253127B2 (en) * | 2018-06-06 | 2023-04-05 | 久光製薬株式会社 | Patches containing fentanyl |
| JP7253126B2 (en) * | 2018-06-06 | 2023-04-05 | 久光製薬株式会社 | Patches containing fentanyl |
| JP7216867B2 (en) * | 2018-06-06 | 2023-02-01 | 久光製薬株式会社 | Patches containing fentanyl |
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