CN1640500A - 丙烯酸基粘合剂组合物及其药物组合物和透皮治疗系统 - Google Patents
丙烯酸基粘合剂组合物及其药物组合物和透皮治疗系统 Download PDFInfo
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- CN1640500A CN1640500A CN 200410000394 CN200410000394A CN1640500A CN 1640500 A CN1640500 A CN 1640500A CN 200410000394 CN200410000394 CN 200410000394 CN 200410000394 A CN200410000394 A CN 200410000394A CN 1640500 A CN1640500 A CN 1640500A
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Images
Landscapes
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
- Medicinal Preparation (AREA)
- Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
Abstract
Description
NO | 丙烯酸丁酯(%) | 丙烯酸异辛酯(%) | 醋酸乙烯酯(%) | 甲基丙烯酸正丁酯(%) | 丙烯酰胺(%) | 二异丙基丙烯酰胺(%) | α-甲基丙烯酸(%) | 玻璃化温度Tg(℃) |
比较例1PSA-8-K | 36.9 | 40.9 | 21.0 | 1.2 | -47.1 | |||
实施例1PSA-9-K | 36.4 | 40.9 | 21.0 | 0.5 | 1.2 | -47.0 | ||
实施例2PSA-10-K | 33.1 | 40.9 | 21.0 | 3.8 | 1.2 | -44.0 | ||
实施例3PSA-11-K | 29.3 | 40.9 | 21.0 | 7.6 | 1.2 | -41.2 | ||
实施例4PSA-12-K | 19.3 | 40.9 | 34.8 | 3.8 | 1.2 | -33.1 | ||
实施例5PSA-13-K | 33.1 | 40.9 | 21.0 | 3.8 | 1.2 | -44.1 | ||
实施例6PSA-14-K | 26.4 | 40.9 | 21.0 | 10.5 | 1.2 | -40.1 | ||
实施例7PSA-15-K | 36.4 | 40.9 | 21.0 | 3.8 | 1.2 | -43.2 | ||
实施例8PSA-16-K | 31.4 | 40.9 | 21.0 | 0.5 | 6.2 | -45.3 |
比较例1PSA-8-K | 实施例1PSA-9-K | 实施例2PSA-10-K | 实施例3PSA-11-K | 实施例4PSA-12-K | 实施例5PSA-13-K | 实施例6PSA-14-K | 实施例7PSA-15-K | 实施例8PSA-16-K | |
初粘力(#球) | 20 | 20 | 20 | 18 | 17 | 20 | 19 | 18 | 18 |
持粘力(min) | 543 | 735 | 1281 | 1987 | 1774 | 1213 | 2099 | 1346 | 1178 |
热流 | 3 | 2 | 2 | 1 | 1 | 2 | 1 | 2 | 2 |
冷流 | 3 | 3 | 2 | 2 | 2 | 2 | 2 | 2 | 2 |
NO | 组分含量 | Tg(℃) | 持粘力(min)及实验时破坏状态 | 热流 | 冷流 | |
组分(A) | 组分(B)E100 | |||||
比较例2 | (PSA-8-K) 80% | 20% | -32.7 | 1143内聚破坏 | 3 | 3 |
实施例9 | (PSA-9-K) 80% | 20% | -32.6 | 1668胶层与被粘物之间的界面破坏 | 1 | 2 |
实施例10 | (PSA-10-K) 80% | 20% | -29.8 | 2516胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例11 | (PSA-11-K) 80% | 20% | -27.3 | 2745胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例12 | (PSA-12-K) 80% | 20% | -20.0 | 2696胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例13 | (PSA-13-K) 80% | 20% | -29.9 | 2488胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例14 | (PSA-14-K) 80% | 20% | -28.9 | 2802胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例15 | (PSA-15-K) 80% | 20% | -29.1 | 2534胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例16 | (PSA-16-K) 80% | 20% | -31.0 | 2341胶层与被粘物之间的界面破坏 | 1 | 1 |
NO | 组分含量 | Tg(℃) | 持粘力(min)及实验时破坏状态 | 热流 | 冷流 | |
PSA-10-K | E100 | |||||
比较例3 | 100% | 0% | -44 | 1281胶层与被粘物之间的界面破坏 | 2 | 2 |
实施例17 | 90% | 10% | -37.1 | 1783胶层与被粘物之间的界面破坏 | 1 | 2 |
实施例18 | 80% | 20% | -29.8 | 2516胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例99 | 70% | 30% | -22.1 | 2847胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例20 | 60% | 40% | -13.6 | 3251胶层与被粘物之间的界面破坏 | 1 | 1 |
实施例21 | 50% | 50% | -5.0 | 3557胶层与被粘物之间的界面破坏 | 1 | 1 |
NO | 组分含量 | Tg(℃) | 热流 | 冷流 | ||
PSA-10-K | 促进剂 | E100 | ||||
比较例4 | 100% | 0% | 0% | -44.0 | 2 | 2 |
比较例5 | 90% | 10% | 0% | -44.6 | 2 | 3 |
比较例6 | 80% | 20% | 0% | -45.2 | 3 | 3 |
比较例7 | 70% | 30% | 0% | -45.7 | 3 | 4 |
比较例8 | 60% | 40% | 0% | -46.4 | 3 | 4 |
比较例9 | 50% | 50% | 0% | -47.1 | 4 | 5 |
比较例10 | 40% | 60% | 0% | -47.6 | 4 | 5 |
实施例18 | 80% | 0% | 20% | -29.8 | 1 | 1 |
实施例22 | 70% | 10% | 20% | -30.5 | 1 | 1 |
实施例23 | 60% | 20% | 20% | -31.2 | 1 | 2 |
实施例24 | 50% | 30% | 20% | -31.9 | 1 | 2 |
实施例25 | 40% | 40% | 20% | -32.6 | 1 | 2 |
实施例26 | 30% | 50% | 20% | -33.3 | 2 | 3 |
实施例27 | 20% | 60% | 20% | -34.1 | 2 | 3 |
NO | 组分含量 | Tg(℃) | 持粘力(min)及破坏状态 | 有无结晶析出 | 冷流 | |||
PSA-10-K | ISDN | 促进剂 | RS100 | |||||
比较例11 | 80% | 0% | 20% | 0% | -45.2 | 256药膜与被粘物之间的界面破坏 | 3 | |
比较例12 | 65% | 15% | 20% | 0% | -33.6 | 4内聚破坏 | 无 | 3 |
实施例28 | 57% | 3% | 20% | 20% | -28.7 | 467药膜与被粘物之间的界面破坏 | 无 | 2 |
实施例29 | 54% | 6% | 20% | 20% | -26.1 | 356药膜与被粘物之间的界面破坏 | 无 | 1 |
实施例30 | 51% | 9% | 20% | 20% | -23.5 | 243药膜与被粘物之间的界面破坏 | 无 | 1 |
实施例31 | 48% | 12% | 20% | 20% | -20.8 | 121药膜与被粘物之间的界面破坏 | 无 | 1 |
实施例32 | 45% | 15% | 20% | 20% | -18.1 | 47药膜与被粘物之间的界面破坏 | 无 | 1 |
NO | 组分含量 | Tg(℃) | 持粘力(min)及破坏状态 | 有无结晶析出 | 冷流 | |||
PSA-10-K | NIF | 促进剂 | E100 | |||||
比较例13 | 80% | 0% | 20% | 0% | -45.8 | 287内聚破坏 | 3 | |
比较例14 | 70% | 10% | 20% | 0% | -33.9 | 28内聚破坏 | 无 | 3 |
实施例33 | 60% | 10% | 20% | 10% | -29.7 | 64内聚破坏 | 无 | 2 |
实施例34 | 55% | 10% | 20% | 15% | -25.7 | 93药膜与被粘物之间的界面破坏 | 无 | 1 |
实施例35 | 50% | 10% | 20% | 20% | -21.9 | 124药膜与被粘物之间的界面破坏 | 无 | 1 |
实施例36 | 45% | 10% | 20% | 25% | -17.9 | 157药膜与被粘物之间的界面破坏 | 无 | 1 |
NO | 组分含量 | Tg(℃) | 持粘力(min)及破坏状态 | 有无结晶析出 | 冷流 | ||||||
粘合剂组合物 | 药物 | AZONE | IPM | DEM | PG | OA | |||||
比较例14 | PSA-10-K(70%) | NIF(10%) | 15% | 5% | -33.9 | 28内聚破坏 | 无 | 3 | |||
比较例15 | PSA-10-K(70%) | NIF(10%) | 4% | 4% | 8% | 4% | -34.4 | 11内聚破坏 | 无 | 3 | |
实施例35 | PSA-10-K(50%)E100(20%) | NIF(10%) | 4% | 4% | 8% | 4% | -21.9 | 124药膜与被粘物之间的界面破坏 | 无 | 1 | |
比较例16 | PSA-10-K(70%) | ASA(15%) | 2% | 10% | 3% | -29.4 | 17内聚破坏 | 有 | 3 | ||
实施例37 | PSA-10-K(44%)RS100(20%) | ASA(15%) | 2% | 3% | 10% | 2% | 3% | -14.5 | 58药膜与被粘物之间的界面破坏 | 无 | 1 |
NO | 组分含量 | Tg(℃) | 持粘力(min)及破坏状态 | 有无结晶析出 | 冷流 | ||||
粘合剂组合物 | 药物 | AZONE | IPM | DEM | |||||
比较例16 | PSA-10-K(65%) | NIF(7.5%)+Pr(7.5%) | 5% | 5% | 10% | -33.9 | 9内聚破坏 | 有 | 3 |
实施例38 | PSA-10-K(30%)+E100(25%) | NIF(7.5%)+Pr(7.5%) | 5% | 5% | 20% | -21.1 | 65药膜与被粘物之间的界面破坏 | 无 | 1 |
比较例17 | PSA-10-K(65%) | NIF(9%)+Pr(6%) | 5% | 5% | 10% | -33.3 | 13内聚破坏 | 有 | 2 |
实施例39 | PSA-10-K(30%)+E100(25%) | NIF(9%)+Pr(6%) | 5% | 5% | 20% | -20.4 | 78药膜与被粘物之间的界面破坏 | 无 | 1 |
比较例18 | PSA-10-K(65%) | NIF(6%)+Pr(9%) | 5% | 5% | 10% | -34.5 | 6内聚破坏 | 有 | 3 |
实施例40 | PSA-10-K(30%)+E100(25%) | NIF(6%)+Pr(9%) | 5% | 5% | 20% | -17.5 | 61药膜与被粘物之间的界面破坏 | 无 | 2 |
体系 | 组分含量 | 活性药物稳态透皮速率(ug·cm-2·h-1) | 体系 | 组分含量 | 活性药物稳态透皮速率(ug·cm-2·h-1) |
比较例19ISDN | ISDN(15%) | 30.04 | 实施例41 | ISDN(15%) | 48.68 |
促进剂(15%) | 促进剂(20%) | ||||
PSA-10-K(70%) | PSA-10-K(45%) | ||||
RS100(20%) | |||||
比较例20Pr | Pr(15%) | 12.52 | 实施例42 | Pr(15%) | 20.55 |
促进剂(15%) | 促进剂(20%) | ||||
PSA-10-K(70%) | PSA-10-K(45%) | ||||
E100(20%) | |||||
比较例21NIF | NIF(10%) | 3.89 | 实施例43 | NIF(10%) | 7.81 |
促进剂(20%) | 促进剂(30%) | ||||
PSA-10-K(70%) | PSA-10-K(40%) | ||||
E100(20%) | |||||
比较例22LDC | LDC(20%) | 80.74 | 实施例44LDC | LDC(20%) | 125.56 |
促进剂(15%) | 促进剂(20%) | ||||
PSA-10-K(65%) | PSA-10-K(30%) | ||||
E100(30%) |
体系 | 组分含量 | 活性药物稳态透皮速率(ug·cm-2·h-1) | 体系 | 组分含量 | 活性药物稳态透皮速率(ug·cm-2·h-1) | 活性药物稳态透皮速率增加倍数 |
比较例25NIF | NIF(5%) | 2.71 | 实施例47 | NIF(5%) | 4.28 | 1.58 |
促进剂(20%) | 促进剂(25%) | |||||
PSA-10-K(75%) | PSA-10-K(55%) | |||||
E100(15%) | ||||||
比较例26NIF | NIF(10%) | 3.89 | 实施例48 | NIF(10%) | 7.81 | 2.01 |
促进剂(20%) | 促进剂(30%) | |||||
PSA-10-K(70%) | PSA-10-K(40%) | |||||
E100(20%) | ||||||
比较例27NIF | NIF(15%) | 4.52 | 实施例49 | NIF(15%) | 11.24 | 2.49 |
促进剂(20%) | 促进剂(40%) | |||||
PSA-10-K(65%) | PSA-10-K(15%) | |||||
E100(30%) |
体系 | 组分含量 | 活性药物稳态透皮速率(ug·cm-2·h-1) | 体系 | 组分含量 | 活性药物稳态透皮速率(ug·cm-2·h-1) |
比较例28NIF+Pr | NIF(7.5%)+Pr(7.5%) | NIF-2.64.PR-7.62 | 实施例50 | NIF(7.5%)+Pr(7.5%) | NIF-4.75PR-11.36 |
促进剂(20%) | 促进剂(30%) | ||||
PSA-10-K(65%) | PSA-10-K(30%) | ||||
E100(25%) | |||||
比较例29NIF+Pr | NIF(9)+Pr(6%) | NIF-3.34Pr-5.58 | 实施例51 | NIF(9%)+Pr(6%) | NIF-5.96Pr-8.93 |
促进剂(20%) | 促进剂(30%) | ||||
PSA-10-K(65%) | PSA-10-K(30%) | ||||
E100(25%) | |||||
比较例30NIF+Pr | NIF(6%)+Pr(9%) | NIF-2.14PR-8.17 | 实施例52 | NIF(6%)+Pr(9%) | NIF-3.86PR-12.96 |
促进剂(20%) | 促进剂(30%) | ||||
PSA-10-K(65%) | PSA-10-K(30%) | ||||
E100(25%) | |||||
比较例31ISDN+Pr | ISDN(7.5%)+Pr(7.5%) | ISDN-12.27PR-4.83 | 实施例53 | ISDN(7.5%)+Pr(7.5%) | ISDN-23.52PR-11.68 |
促进剂(15%) | 促进剂(20%) | ||||
PSA-10-K(70%) | PSA-10-K(45%) | ||||
RS100(20%) |
体系 | 含药量 | 药物稳态透皮速率(ug·cm-2·h-1) | 热流 | 体系 | 含药量 | 药物稳态透皮速率(ug·cm-2·h-1) | 热流 |
比较例32Catapress-TTS | 2.5mg(3.5cm2) | 3.11 | 3 | 实施例54 | 2.5mg(2.5cm2) | 4.30 | 1 |
体系 | 结构 | 组分含量 | 体系 | 结构 | 组分含量 |
比较例33 | 药物储库层 | PSA-10-K(50%) | 实施例55 | 粘胶层 | PSA-10-K(80%) |
RS100(15%) | |||||
促进剂(5%) | |||||
药物储库层 | PSA-10-K(60%) | ||||
促进剂(20%) | 促进剂(10%) | ||||
NIP(10%) | NIP(10%) | ||||
RS100(20%) | RS100(20%) |
体系 | 商品名 | 规格 | 体系 | 结构 | 组分含量 |
比较例34 | HokunalinTape | 2mg/10cm2 | 实施例56 | 低含量药物储库层 | PSA-10-K(68.5%) |
促进剂(10%) | |||||
TBR(1.5%) | |||||
E100(20%) | |||||
中含量药物储库层 | PSA-10-K(72%) | ||||
促进剂(5%) | |||||
TBR(3.0%) | |||||
E100(20%) | |||||
高含量药物储库层 | PSA-10-K(70.5%) | ||||
促进剂(4.5%) | |||||
TBR(5.0%) | |||||
E100(20%) |
体系 | 含药量(mg/cm2) | 活性药物稳态透皮速率(ug·cm-2·h-1) | 体系 | 含活性药物(mg/cm2) | 活性药物稳态透皮速率(ug·cm-2·h-1) |
比较例35ISDN1 | 1.0(40cm2) | 26.75 | 实施例41ISDN3 | 2.0(20cm2) | 48.68 |
比较例36NIP2 | 2.10(24cm2) | 1.35 | 实施例55NIP4 | 2.00(10cm2) | 3.61 |
比较例32clonidine5 | 2.5mg/3.5cm2 | 3.11 | 实施例54clonidine6 | 2.5mg/2.5cm2 | 4.30 |
体系 | 贴片规格 | 刺激性 | 致敏性 | ||
刺激强度均分 | 结论 | 致敏率(%) | 结论 | ||
ISDN比较例3 | 40mg(40cm2) | 1.9 | 轻度刺激性 | 7 | 轻微 |
ISDN实施例4 | 40mg(20cm2) | 0.5 | 轻度刺激性 | 0 | 无 |
NIF比较例5 | 30mg(30cm2) | 1.4 | 轻度刺激性 | 5 | 轻微 |
NIF实施例6 | 30mg(15cm2) | 0.5 | 轻度刺激性 | 0 | 无 |
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CNB2004100003947A CN100411692C (zh) | 2004-01-13 | 2004-01-13 | 丙烯酸基粘合剂组合物及其药物组合物和透皮治疗系统 |
HK06100171.5A HK1080397B (zh) | 2004-01-13 | 2006-01-04 | 丙烯酸基粘合劑組合物及其藥物組合物和透皮治療系統 |
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EG20380A (en) * | 1991-10-16 | 1999-02-28 | Richardson Vicks Inc | Enhanced skin penetration system for improved topical delivery of drugs |
CA2141192C (en) * | 1992-07-28 | 1999-02-02 | Roberta C. Bloom | Pharmaceutical composition for topical use containing a crosslinked cationic polymer and an alkoxylated ether |
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2004
- 2004-01-13 CN CNB2004100003947A patent/CN100411692C/zh not_active Expired - Lifetime
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2006
- 2006-01-04 HK HK06100171.5A patent/HK1080397B/zh not_active IP Right Cessation
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Also Published As
Publication number | Publication date |
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HK1080397A1 (en) | 2006-04-28 |
CN100411692C (zh) | 2008-08-20 |
HK1080397B (zh) | 2009-05-29 |
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