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粘性介质中片剂的崩解和药物溶出:对乙酰氨基酚红外片

Tablet disintegration and drug dissolution in viscous media: paracetamol IR tablets.

作者信息

Parojcić Jelena, Vasiljević Dragana, Ibrić Svetlana, Djurić Zorica

机构信息

Department of Pharmaceutical Technology, Faculty of Pharmacy, University of Belgrade, Vojvode Stepe 450, 11221 Belgrade, Serbia.

出版信息

Int J Pharm. 2008 May 1;355(1-2):93-9. doi: 10.1016/j.ijpharm.2007.11.058. Epub 2007 Dec 5.

Abstract

An investigation into the influence of viscous media on tablet disintegration and drug dissolution was performed with the aim to simulate the potential formulation-specific food effect for a selected highly soluble model drug. Literature data on the in vivo drug absorption in fasted and fed state have been evaluated for in vitro-in vivo correlation (IVIVC) purposes. In vitro studies were conducted in simple buffer media with or without addition of HPMC K4M as a viscosity enhancing agent. Good IVIVC correlation (r>0.95) was obtained for paracetamol dissolution in viscous media at 50rpm and fed state absorption profiles, while in vitro dissolution in simple media at lower stirring speed was predictable of drug products in vivo behaviour in the fasted state. The data obtained support the existing idea that relatively simple dissolution media and/or set of experimental conditions may be used to differentiate formulation-specific food-drug interactions. Such tests would be a useful tool in the development of formulations that would not be susceptible to the influence of co-administered meal and, furthermore, facilitate regulatory decision on the necessity to conduct food effect studies in vivo.

摘要

开展了一项关于粘性介质对片剂崩解和药物溶出影响的研究,旨在模拟一种选定的高溶解性模型药物潜在的特定剂型食物效应。为了体外-体内相关性(IVIVC)研究目的,评估了空腹和进食状态下该药物体内吸收的文献数据。体外研究在添加或不添加羟丙基甲基纤维素K4M(作为增粘剂)的简单缓冲介质中进行。对乙酰氨基酚在粘性介质中以50转/分钟的速度溶出以及进食状态下的吸收曲线呈现出良好的IVIVC相关性(r>0.95),而在较低搅拌速度下于简单介质中的体外溶出情况可预测药物制剂在空腹状态下的体内行为。所获得的数据支持了现有观点,即相对简单的溶出介质和/或一组实验条件可用于区分特定剂型的食物-药物相互作用。此类试验将成为开发不易受同时摄入食物影响的制剂的有用工具,此外,有助于监管部门决定是否有必要开展体内食物效应研究。

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