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首页> 外文期刊>Journal of Microencapsulation: Microcapsules Liposomes Nanoparticles Microcells Microspheres >Microencapsulation of hydrophilic drug substances using biodegradable polyesters.Part II:Implants allowing controlled drug release-a feasibility study using bisphosphonates
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Microencapsulation of hydrophilic drug substances using biodegradable polyesters.Part II:Implants allowing controlled drug release-a feasibility study using bisphosphonates

机译:使用可生物降解的聚酯对亲水性药物物质进行微囊封装。第二部分:允许药物受控释放的扩增剂-使用双膦酸酯的可行性研究

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摘要

The prolonged delivery of hydrophilic drug salts from hydrophobic polymer carriers at high drug loading is an ambitious goal.Pamidronate disodium salt (APD) containing implants prepared from spray-dried microparticles were investigated using a laboratory ram extruder.An APD-containing polymer matrix consisting of an APD-chitosan implant embedded in the biodegradable polymer D,L-poly(lactide-co-glycolide acid-glucose) (PLG-GLU) was compared with a matrix system with the micronized drug distributed in the PLG-GLU.The APD-chitosan matrix system showed a triphasic release behaviour at loading levels of 6.86 and 15.54% (w/w) over 36 days under in-vitro conditions.At higher loading (31.92%),a drug burst was observed within 6 days clue to the formation of pores and channels in the polymeric matrix.In contrast,implants containing the micronized drug showed a more continuous release profile over 48 days up to a loading of 31.78% (w/w).At a drug loading of 46.17% (w/w),a drug burst was observed.Using micronized drug salts and reducing the surface area available for diffusion,parenteral delivery systems for highly water-soluble drug candidates were shown to be technically feasible at high drug loadings.
机译:在高载药量下,从疏水性聚合物载体中延长亲水性药物盐的递送是一个宏伟的目标。使用实验室柱塞式挤出机研究了由喷雾干燥的微粒制备的含有帕米膦酸二钠盐(APD)的植入物。将嵌入可生物降解的聚合物D,L-聚(丙交酯-乙交酯-葡萄糖酸-葡萄糖)(PLG-GLU)中的APD-壳聚糖植入物与微粉化药物分布在PLG-GLU中的基质系统进行了比较。壳聚糖基质系统在体外条件下在36天内的负载水平为6.86和15.54%(w / w)时表现出三态释放行为。在较高负载(31.92%)下,在6天之内观察到药物爆发是线索相比之下,含有微粉化药物的植入物在48天内显示出更连续的释放特性,负载量为31.78%(w / w)。载药量为46.17%(w / w) ),观察到药物爆炸。使用微粉化的药物盐并减少可扩散的表面积,高水溶性药物候选物的肠胃外给药系统在高药物载量下在技术上是可行的。

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