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热熔挤出法制备的缓释片的性质

Properties of sustained-release tablets prepared by hot-melt extrusion.

作者信息

Zhang F, McGinity J W

机构信息

College of Pharmacy, University of Texas at Austin 78712, USA.

出版信息

Pharm Dev Technol. 1999 May;4(2):241-50. doi: 10.1081/pdt-100101358.

Abstract

The objectives of the present study were to investigate the properties of polyethylene oxide (PEO) as a drug carrier and to study the release mechanism of chlorpheniramine maleate (CPM) from matrix tablets prepared by hot-melt extrusion. During the hot-melt extrusion process, a dry powder blend of drug, polymer, and other adjuvants was fed into the extruder and melted inside the barrel of the machine. The molten mass was extruded through a rod-shaped die and then cut manually into 400-mg tablets. CPM and PEO were shown to be stable under the processing conditions. The molecular weight of the PEO, the drug loading percentage, and the inclusion of polyethylene glycol as a processing aid, were all found to influence the processing conditions and the drug release properties of the extruded tablets. Faster release of CPM from the matrix tablets was observed in acidic medium than in purified water and phosphate buffer (pH 7.4). Drug release from the matrix tablet was controlled by erosion of the PEO matrix and the diffusion of the drug through the swollen gel layer at the surface of the tablets. CPM was dispersed at the molecular level in the PEO matrix at low drug loading level and recrystallization of CPM was observed at high drug loading levels. Hot-melt extrusion was demonstrated to be a viable novel method to prepare sustained-release tablets. PEO was shown to be a suitable polymeric carrier for this process.

摘要

本研究的目的是研究聚环氧乙烷(PEO)作为药物载体的性质,并研究马来酸氯苯那敏(CPM)从热熔挤出制备的基质片剂中的释放机制。在热熔挤出过程中,将药物、聚合物和其他辅料的干粉混合物加入到挤出机中,并在机器的料筒内熔化。将熔融物料通过棒形模头挤出,然后手动切成400毫克的片剂。结果表明,CPM和PEO在加工条件下是稳定的。发现PEO的分子量、载药百分比以及聚乙二醇作为加工助剂的加入,均会影响挤出片剂的加工条件和药物释放性能。与在纯化水和磷酸盐缓冲液(pH 7.4)中相比,在酸性介质中观察到CPM从基质片剂中的释放更快。基质片剂中的药物释放是通过PEO基质的侵蚀以及药物通过片剂表面溶胀凝胶层的扩散来控制的。在低载药量水平下,CPM在分子水平上分散在PEO基质中,而在高载药量水平下观察到CPM的重结晶。热熔挤出被证明是一种制备缓释片剂的可行新方法。PEO被证明是该过程合适的聚合物载体。

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