首页> 外文期刊>Acta pharmaceutica: a quarterly journal of Croatian Pharmaceutical Society and Slovenian Pharmaceutical Society, dealing with all branches of pharmacy and allied sciences >Formulation and evaluation of delayed-onset extended-release tablets of metoprolol tartrate using hydrophilic-swellable polymers
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Formulation and evaluation of delayed-onset extended-release tablets of metoprolol tartrate using hydrophilic-swellable polymers

机译:酒石酸美托洛尔缓释缓释片的制备及使用亲水可溶胀聚合物的评估

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摘要

In view of the circadian rhythm of cardiovascular diseases, a delayed-onset extended-release (DOER) formulation of metoprolol tartrate (MT) was prepared. This was achieved through dissolution-guided optimization of the proportion of Methocel K4M and Methocel K15M. Core erosion ratio was greater than 50 %, thereby showing steady release of the drug after the lag time until complete dissolution. Optimized formulation produced a lag phase of 6 h followed by complete release of 98.7 ± 2.1 % in 24 h. Water uptake study revealed that Methocel K15M has lower water uptake (30 ± 1 %) than Methocel K4M (40 ± 2 %) after 24 h. Axial swelling of polymers was higher than swelling in the radial direction. Drug-polymer interaction study precludes any interaction between drug and polymer. Such a drug delivery system may provide a viable alternative for effective management of hypertension and other related disorders. This work also proposes an approach to attain DOER for a hydrophilic drug by using a hydrophilic swellable polymer in press coat.
机译:鉴于心血管疾病的昼夜节律,制备了酒石酸美托洛尔(MT)的延迟发作缓释(DOER)制剂。这是通过溶解指导优化Methocel K4M和Methocel K15M的比例来实现的。核心侵蚀率大于50%,因此在滞后时间直至完全溶解后显示出稳定的药物释放。优化的配方产生了6小时的滞后阶段,然后在24小时内完全释放98.7±2.1%。吸水率研究表明,在24小时后,Methocel K15M的吸水率(30±1%)比Methocel K4M(40±2%)低。聚合物的轴向溶胀高于径向的溶胀。药物与聚合物的相互作用研究排除了药物与聚合物之间的任何相互作用。这样的药物输送系统可以为有效治疗高血压和其他相关疾病提供可行的替代方案。这项工作还提出了一种通过在压涂中使用亲水性可溶胀聚合物来获得亲水性药物DOER的方法。

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