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Effect of Polymer Permeability and Solvent Removal Rate on In Situ Forming Implants: Drug Burst Release and Microstructure

机译:聚合物渗透性和溶剂去除率对原位形成植入物的影响:药物爆发释放和微观结构

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摘要

To explore the mechanism of drug release and depot formation of in situ forming implants (ISFIs), osthole-loaded ISFIs were prepared by dissolving polylactide, poly(lactide- -glycolide), polycaprolactone, or poly(trimethylene carbonate) in different organic solvents, including -methyl-2-pyrrolidone (NMP), dimethyl sulfoxide (DMSO), and triacetin (TA). Drug release, polymer degradation, solvent removal rate and depot microstructure were examined. The burst release effect could be reduced by using solvents exhibit slow forming phase inversion and less permeable polymers. Both the drug burst release and polymer depot microstructure were closely related to the removal rate of organic solvent. Polymers with higher permeability often displayed faster drug and solvent diffusion rates. Due to high polymer-solvent affinity, some of the organic solvent remained in the depot even after the implant was completely formed. The residual of organic solvent could be predicted by solubility parameters. The ISFI showed a lower initial release in vivo than that in vitro. In summary, the effects of different polymers and solvents on drug release and depot formation in ISFI systems were extensively investigated and discussed in this article. The two main factors, polymer permeability and solvent removal rate, were involved in different stages of drug release and depot formation in ISFI systems.
机译:为了探索原位形成植入物(ISFI)的药物释放和储库形成的机理,通过将聚丙交酯,聚丙交酯-乙交酯,聚己内酯或聚碳酸三亚甲基酯溶解,制备了载有osthole的ISFI,包括-甲基-2-吡咯烷酮(NMP),二甲基亚砜(DMSO)和三醋精(TA)。检查了药物释放,聚合物降解,溶剂去除率和储库微观结构。通过使用表现出缓慢的形成相转化和较低渗透性的聚合物的溶剂,可以降低爆裂释放效果。药物的爆发释放和聚合物贮库的微观结构都与有机溶剂的去除率密切相关。具有较高渗透性的聚合物通常显示出较快的药物和溶剂扩散速率。由于高的聚合物-溶剂亲和力,即使在完全形成植入物之后,一些有机溶剂仍保留在储库中。有机溶剂的残留量可以通过溶解度参数来预测。 ISFI显示体内的初始释放低于体外。总而言之,本文对ISFI系统中不同聚合物和溶剂对药物释放和储库形成的影响进行了广泛的研究和讨论。聚合物渗透率和溶剂去除速率这两个主要因素涉及ISFI系统中药物释放和储库形成的不同阶段。

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