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首页> 外文期刊>Pharmaceutical development and technology >Design and evaluation of enteric-coated tablets for rifampicin and isoniazid combinations.
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Design and evaluation of enteric-coated tablets for rifampicin and isoniazid combinations.

机译:利福平和异烟肼组合的肠溶片的设计和评估。

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摘要

In order to improve the bioavailability of rifampicin (RIF) from rifampicin and isoniazid (INH) combination formulations, the physicochemical characteristics of RIF, stability of RIF in different pH buffers in the presence of INH, as well as the effect of particle size of RIF materials on the dissolution rate were investigated. On the basis of the above examinations, enteric-coated tablets for RIF and INH combinations were designed and prepared. RIF showed low solubility and high apparent distribution coefficient in the intestinal pH (pH 4.0-7.4). With the decrease in pH, the degradation of RIF increase and the presence of INH deepen the degradation. Enteric-coated tablets were prepared after grinding the RIF materials by dry granulation technique. The pharmacokinetics of RIF and INH of self-made enteric-coated tablets in dogs were studied by comparing with the reference tablets. The AUC(0-48) of RIF in both reference and test tablets were 304.77 ± 42.27 and 353.79 ± 31.63 μg·h·mL(-1), respectively. The AUC(0-48) of INH in both reference and test tablets were 17.14 ± 8.59 and 19.62 ± 10.57 μg·h·mL(-1), respectively. Enteric-coated tablets may minimize the decomposition of RIF in gastrointestinal tract and improve the bioavailability.
机译:为了提高利福平和异烟肼(INH)组合制剂中的利福平(RIF)的生物利用度,RIF的理化特性,RIF在INH存在下在不同pH缓冲液中的稳定性以及RIF粒径的影响研究了物料对溶出度的影响。在上述检查的基础上,设计和制备了用于RIF和INH组合的肠溶片。 RIF在肠道pH(pH 4.0-7.4)中显示出低溶解度和高表观分布系数。随着pH的降低,RIF的降解增加,而INH的存在加深了降解。通过干法制粒将RIF材料研磨后,制备肠溶片。通过与参考片剂比较,研究了自制肠溶片的RIF和INH在犬体内的药代动力学。参比片剂和受试片剂的RIF的AUC(0-48)分别为304.77±42.27和353.79±31.63μg·h·mL(-1)。参比片剂和受试片剂中INH的AUC(0-48)分别为17.14±8.59和19.62±10.57μg·h·mL(-1)。肠溶片可以最大程度地减少RIF在胃肠道中的分解,并提高生物利用度。

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