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首页> 外文期刊>Clinical and experimental pharmacology & physiology >Pharmacological evaluation of membrane-moderated transdermal system of glipizide.
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Pharmacological evaluation of membrane-moderated transdermal system of glipizide.

机译:格列吡嗪的膜调节透皮系统的药理评价。

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1. Membrane-moderated transdermal systems of glipizide were prepared using drug-containing carbopol gel (drug reservoir) and ethyl cellulose, as well as Eudragit RS-100, Eudragit RL-100 (Rohm Pharma, Darmstadt, Germany) and ethylene vinyl acetate (EVA; 2, 9 and 19% vinyl acetate content) rate-controlling membranes, and were subsequently evaluated in vitro (drug content and drug permeation studies) and in vivo (acute and long-term hypoglycaemic activity, effect on glucose tolerance, biochemical and histopathological studies, skin irritation test and pharmacokinetic studies in mice). 2. The drug content of the systems was found to be more than 99%. Variations in drug permeation patterns were observed among the formulations containing different rate-controlling membranes. 3. The system with the EVA (19% vinyl acetate) rate-controlling membrane was selected for in vivo experiments. This transdermal system produced better improvement with respect to hypoglycaemic activity, glucose tolerance and tested biochemical, histopathological and pharmacokinetic parameters all compared with oral administration and exhibited negligible skin irritation. 4. The transdermal system successfully prevented severe hypoglycaemia in the initial hours and it was also effective for chronic application.
机译:1.使用含药物的carbopol凝胶(药物储库)和乙基纤维素,Eudragit RS-100,Eudragit RL-100(德国达姆施塔特罗姆制药)和乙烯醋酸乙烯酯( EVA,2%,9%和19%的醋酸乙烯酯含量控制膜,随后在体外(药物含量和药物渗透研究)和体内(急性和长期降血糖活性,对葡萄糖耐量,生化和代谢的影响)进行评估小鼠的组织病理学研究,皮肤刺激试验和药代动力学研究)。 2.发现系统中的药物含量超过99%。在包含不同速率控制膜的制剂中观察到药物渗透模式的变化。 3.选择具有EVA(19%醋酸乙烯酯)速率控制膜的系统进行体内实验。与口服给药相比,该透皮系统在降血糖活性,葡萄糖耐受性和经测试的生化,组织病理学和药代动力学参数方面均产生了更好的改善,并且对皮肤的刺激作用可忽略不计。 4.透皮系统在开始的几个小时内成功地预防了严重的低血糖症,并且对于慢性应用也有效。

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