In the present study, an attempt was made to develop the pulsatile drug delivery of fluvastatin sodium to the colon. Formaldehyde-treated capsule bodies were used for the preparation of pulsincaps. It was sealed with a unhardened cap of the capsule. The microspheres were prepared by emulsion solvent evaporation technique. Optimized microsphere formulations were selected based on dissolution studies. Hydrogel plug (HP) (Karaya gum and lactose in 1:1 ratio) having 4.5 kg/cm hardness and 100 mg weight was placed in the capsule opening and found that it was satisfactory to retard the drug release in small intestinal fluid and to eject out the plugin colonic fluid and releasing the microspheres into colonic fluid after a lag time criterion of 5 hrs. The sealed capsules were completely coated by dip coating method with 5% cellulose acetate phthalate to prevent variable gastric emptying. Dissolution studies of pulsatile capsule device in media with different pH (1.2, 7.4 and 6.8) showed that drug release in the colon could be modulated by optimizing the concentration of polymers in the microspheres. Drug-polymer interaction studies indicated no interaction in between the drug and the polymer. Among all the formulations, fluvastatin sodium microspheres prepared with Eudragit RS 100 in 1:3 ratio shown prolonged release for a period of 12 hrs. The obtained results showed the capability of the system in delaying drug release for a programmable period of time and to deliver the drug in the early morning hours when cholesterol synthesis are more prevalent. 2
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机译:在本研究中,已尝试开发氟伐他汀钠向结肠的搏动性药物递送。甲醛处理的胶囊体用于制备脉冲胶囊。用未硬化的胶囊盖密封。通过乳液溶剂蒸发技术制备微球。基于溶出度研究选择了优化的微球配方。将具有4.5 kg / cm硬度和100 mg重量的水凝胶塞(HP)(Karaya胶和乳糖以1:1的比例)放入胶囊开口中,发现延迟药物在小肠液中的释放并排出是令人满意的在5小时的滞后时间标准后,取出插件结肠液并将微球释放到结肠液中。密封的胶囊通过浸涂法完全用5%醋酸邻苯二甲酸纤维素覆盖,以防止胃排空不均。脉冲胶囊装置在具有不同pH值(1.2、7.4和6.8)的介质中的溶解研究表明,可以通过优化微球中聚合物的浓度来调节结肠中的药物释放。药物与聚合物的相互作用研究表明,药物与聚合物之间没有相互作用。在所有制剂中,用Eudragit RS 100以1:3比例制备的氟伐他汀钠微球在12小时内显示出延长释放。获得的结果表明,该系统具有将药物释放延迟一段可编程的时间并在胆固醇合成更为普遍的清晨时间递送药物的能力。 2
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