首页> 外文期刊>European journal of pharmaceutical sciences >In situ forming microparticle system for controlled delivery of leuprolide acetate: Influence of the formulation and processing parameters.
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In situ forming microparticle system for controlled delivery of leuprolide acetate: Influence of the formulation and processing parameters.

机译:原位形成微粒系统以控制醋酸亮丙瑞林的递送:配方和加工参数的影响。

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摘要

The objective of present study was to control the delivery of leuprolide acetate using in situ forming microparticle (ISM) systems. A solution of leuprolide acetate and poly(lactide-co-glycolide) (PLGA RG 503H) or poly(lactide) (PLA R 202H) in N-methyl-2-pyrrolideone (NMP) was emulsified into an external oil phase using a two-syringe/connector system. After injection into an aqueous environment, NMP diffusion led to polymer precipitation and microparticle formation in situ. ISM-systems were characterized with respect to particle morphology and the influence of formulation and processing parameters on the in vitro release. ISM from RG 503H showed a high initial release (approximately 40%), which could be attributed to the high porosity of microparticles. The initial release could be reduced by increasing the polymer concentration, increasing the amount and viscosity of the oil phase, and decreasing the drug loading. ISM-systems from R 202H had a much lower initial release (approximately 9%) compared to that from RG 503H, which was followed by a slow and continuous drug release. In comparison to conventional microparticles prepared by a solvent evaporation method, ISM from R 202H showed a lower initial release and a more linear continuous release.
机译:本研究的目的是使用原位形成微粒(ISM)系统控制醋酸亮丙瑞林的递送。将乙酸亮丙瑞林和聚丙交酯-乙交酯共聚物(PLGA RG 503H)或聚丙交酯(PLA R 202H)在N-甲基-2-吡咯烷酮(NMP)中的溶液乳化为外部油相,使用两种方法-注射器/连接器系统。注入水性环境后,NMP扩散导致聚合物沉淀和原位形成微粒。表征了ISM系统的颗粒形态以及制剂和加工参数对体外释放的影响。 RG 503H的ISM显示出较高的初始释放(约40%),这可能归因于微粒的高孔隙率。初始释放可通过增加聚合物浓度,增加油相的量和粘度以及减少载药量来减少。与RG 503H相比,R 202H的ISM系统的初始释放量低得多(约9%),随后缓慢而连续地释放药物。与通过溶剂蒸发法制备的常规微粒相比,R 202H的ISM表现出较低的初始释放和更线性的连续释放。

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