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首页> 外文期刊>International Journal of Pharmaceutics >Preparation of an extended-release matrix tablet using chitosan/Carbopol interpolymer complex.
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Preparation of an extended-release matrix tablet using chitosan/Carbopol interpolymer complex.

机译:使用壳聚糖/ Carbopol共聚体复合物制备缓释基质片剂。

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摘要

A chitosan and Carbopol interpolymer complex (IPC) was formed using a precipitation method in an acidic solution. The chitosan and Carbopol IPC was characterized by Fourier transform infrared spectroscopy (FT-IR), differential scanning calorimetry (DSC), and turbidity measurements. FT-IR demonstrated that the IPC formed a complex through an electrostatic interaction between the protonated amine (NH(3)(+)) group of chitosan and the carboxylate (COO(-)) group of Carbopol. DSC indicated the IPC to have different thermal characteristics from chitosan or Carbopol. The turbidity measurement revealed the complexation ratio of IPC between chitosan/Carbopol to be 1/4. A theophylline tablet was prepared using the IPC as a matrix material. The drug release profile from this tablet was similar to that from the HPMC tablet and showed a pH-independent release profile. The mechanisms for drug release from the IPC tablet were diffusional release at pH 6.8 and relaxational release at pH 1.2.
机译:使用沉淀法在酸性溶液中形成壳聚糖和Carbopol共聚复合物(IPC)。通过傅立叶变换红外光谱(FT-IR),差示扫描量热法(DSC)和浊度测量来表征壳聚糖和Carbopol IPC。 FT-IR证明IPC通过壳聚糖的质子化胺(NH(3)(+))基团和Carbopol的羧酸酯(COO(-))基团之间的静电相互作用形成复合物。 DSC指出IPC与壳聚糖或Carbopol具有不同的热特性。浊度测量显示壳聚糖/卡波姆之间的IPC的络合率为1/4。使用IPC作为基质材料制备茶碱片。该片剂的药物释放曲线与HPMC片剂的药物释放曲线相似,并显示出pH依赖性的释放曲线。从IPC片剂释放药物的机制是在pH 6.8时扩散释放和在pH 1.2时松弛释放。

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