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Preparation and in vitro evaluation of a novel combined multiparticulate delayed-onset sustained-release formulation of diltiazem hydrochloride.

机译:盐酸地尔硫卓的新型复合多颗粒延迟发作缓释制剂的制备及体外评价。

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摘要

A combined delivery system, containing two kinds of diltiazem hydrochloride multi-layer coated pellets with different release characteristics, was developed to meet chronotherapeutic requirements. The dissolution studies in vitro indicated that the combined system could constantly release drug at a predetermined time in synchrony with the biologic rhythm of disease activity. These two kinds of pellets were mixed at the ratio 1:1. Pellet 2 could provide drug during the later phase of drug release from pellet 1, because the amount released was insufficient in the later phase (about 14-24 h after administration) for pellet 1. Addition of Tween 20 in the HPMC swelling layer was able to modify the hydration rate of HPMC layer which controlled the delayed time of the release system. It was found that the drug release kinetics followed Hixson-Crowell equation and this indicated that the main drug-transport mechanism inside the pellets was an erosion mechanism. The drug release rate was independent of the hydrodynamic conditions and pH of the external environment, and showed a decrease with increasing of osmotic pressure of the dissolution medium. These release characteristics indicated that the drug release from this system was driven by osmotic-pressure gradient.
机译:为了满足计时治疗的要求,开发了一种联合给药系统,其中包含两种具有不同释放特性的盐酸地尔硫卓多层包衣小丸。体外溶出度研究表明,该组合系统可在预定时间与疾病活动的生物节律同步释放药物。将这两种颗粒以1:1的比例混合。药丸2可以在从药丸1释放药物的后期提供药物,因为在药丸1的后期(给药后约14-24小时)释放的量不足。在HPMC溶胀层中加入Tween 20能够修改HPMC层的水合速率,以控制释放系统的延迟时间。发现药物释放动力学遵循Hixson-Crowell方程,这表明药丸内部的主要药物传输机制是腐蚀机制。药物释放速率与流体动力学条件和外部环境的pH无关,并且随着溶出介质渗透压的增加而降低。这些释放特征表明从该系统释放的药物是由渗透压梯度驱动的。

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