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Development and Evaluation of Ca+ 2Ion Cross-Linked Carboxymethyl Xanthan Gum Tablet Prepared by Wet Granulation Technique

机译:湿法制粒制备Ca + 2离子交联羧甲基黄原胶的研究与开发

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摘要

The objective of this work was to study the release behavior of prednisolone from calcium-cross-linked carboxymethyl xanthan gum (CMXG) tablets in dissolution medium having different pH values prevailing in the gastrointestinal lumen. Xanthan gum (XG) was derivatized to CMXG which was then cross-linked in situ with Ca+2 ion during wet massing step of tablet preparation. Fourier transform infrared (FTIR) spectroscopy and differential scanning calorimetry studies did not show any drug-polymer interaction although the drug underwent solid-state transformation during compression as evident from X-ray diffraction analysis. In vitro release study demonstrated that increase in the amount of Ca+2 ion decreased the drug release, and beyond a certain amount, the drug release increased. While increase in both drug load and tablet crushing strength decreased the drug release, increase in exposure time in acid solution of pH 1.2 increased the overall release of the drug. The mechanism of drug release was non-Fickian/anomalous. The results indicated that variation in the amount of Ca+2 ion can modulate the drug release from CMXG matrix tablets as needed.
机译:这项工作的目的是研究强的松龙从钙交联的羧甲基黄原胶(CMXG)片剂在胃肠腔中存在不同pH值的溶出介质中的释放行为。将黄原胶(XG)衍生为CMXG,然后在片剂制备的湿法制备步骤中将其与Ca +2 离子原位交联。傅里叶变换红外(FTIR)光谱和差示扫描量热法研究未显示任何药物与聚合物的相互作用,尽管该药物在压缩过程中经历了固态转化(从X射线衍射分析可以明显看出)。体外释放研究表明,Ca +2 离子的增加会降低药物的释放,超过一定量后,药物的释放会增加。虽然增加载药量和压片强度会降低药物释放,但在pH 1.2的酸性溶液中暴露时间的增加会增加药物的总体释放。药物释放的机制是非菲克/异常的。结果表明,Ca +2 离子含量的变化可根据需要调节CMXG基质片剂中的药物释放。

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