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首页> 外文期刊>European Polymer Journal >The role of polymer/drug interactions on the sustained release from poly(DL-lactic acid) tablets
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The role of polymer/drug interactions on the sustained release from poly(DL-lactic acid) tablets

机译:聚合物/药物相互作用对聚(DL-乳酸)片剂持续释放的作用

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摘要

The release profiles of model drugs (propranolol HCl, diclofenac sodium, salicylic acid and sulfasalazine) from low molecular weight poly(D,L-lactic acid) [D,L-PLA] tablets immersed in buffer solutions were investigated in an attempt to explore the mechanism of the related phenomena. It was confirmed that drug release is controlled by diffusion through the polymer matrix and by the erosion of the polymer. The pH of the surrounding medium influences the drug solubility as well as swelling and degradation rate of the polymer and therefore the overall drug release process. Physicochemical interaction between D,L-PLA and drug is an additional factor which influences the degree of matrix swelling and therefore its porosity and diffusion release process. Propranolol HCl shows extended delivery time at both examined pH values (5.4 and 7.4) and especially at pH 7.4 where release was accomplished in 190 days, most probably due to its decreased solubility at higher pH values. The acidic drugs gave shorter delivery times especially at pH 7.4. A slower drug release rate and more extended delivery time at pH 7.4 in comparison with that at pH 5.4 was recorded for tablets loaded with diclofenac sodium and salicylic acid. The opposite effect was observed with samples loaded with propranolol HCl. (c) 2006 Elsevier Ltd. All rights reserved.
机译:研究了模型药物(盐酸普萘洛尔,双氯芬酸钠,水杨酸和柳氮磺吡啶)从低分子量聚(D,L-乳酸)[D,L-PLA]片剂浸入缓冲溶液中的释放曲线,以探索相关现象的机理。证实了药物释放是通过在聚合物基质中的扩散和聚合物的侵蚀来控制的。周围介质的pH影响药物溶解度以及聚合物的溶胀和降解速率,从而影响整个药物释放过程。 D,L-PLA与药物之间的物理化学相互作用是影响基质溶胀程度的一个附加因素,因此会影响其孔隙度和扩散释放过程。盐酸普萘洛尔在所检查的pH值(5.4和7.4)下均显示出延长的递送时间,尤其是在pH 7.4下(在190天内完成释放),这很可能是由于其在较高pH值下的溶解度降低所致。酸性药物的递送时间更短,尤其是在pH 7.4时。与装有双氯芬酸钠和水杨酸的片剂相比,在pH 7.4时,在pH 7.4时,药物释放速度较慢,递送时间更长。在装有盐酸普萘洛尔的样品中观察到相反的效果。 (c)2006 Elsevier Ltd.保留所有权利。

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