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Strategies to Obtain Encapsulation and Controlled Release of Pentamidine in Mesoporous Silica Nanoparticles

机译:在中孔二氧化硅纳米颗粒中获得喷他idine的包封和控制释放的策略

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摘要

Pentamidine (PTM), an antiprotozoal agent used in clinics as pentamidine isethionate salt (PTM-S), recently showed high potential also for the treatment of cancer and myotonic dystrophy type I. However, a severe limit to the systemic administration of PTM is represented by its nephrotoxicity, leading to the need for a system able to achieve a controlled release of the drug. In this study, mesoporous silica nanoparticles (MSNs) were employed for the first time to encapsulate PTM. PTM-S was first used for loading experiments into bare (MSN-OH) and aminopropyl, cyanopropyl and carboxypropyl-functionalized MSNs (MSN-NH2, MSN-CN and MSN-COOH respectively) but it was not adequately loaded in any MSNs. The free base of PTM (PTM-B) was then obtained from PTM-S and successfully loaded into MSNs. Specifically, MSN-COOH exhibited the highest loading capacity. In vitro evaluation of PTM-B kinetic release from the different MSNs was carried out. An influence of the functional groups in slowing the release of the drug, when compared to bare MSNs was observed. Altogether, these results demonstrate that MSN-COOH could be a promising system to achieve a controlled release of PTM.
机译:戊tam(PTM)是临床上用作戊anti羟乙磺酸盐(PTM-S)的抗原生动物剂,最近也显示出了治疗癌症和I型肌强直性营养不良的巨大潜力。但是,PTM的全身给药受到严重限制由于其肾毒性,导致需要一种能够实现药物控释的系统。在这项研究中,首次使用中孔二氧化硅纳米粒子(MSN)封装PTM。 PTM-S首先用于将实验加载到裸露(MSN-OH)和氨基丙基,氰基丙基和羧丙基官能化的MSN(分别为MSN-NH2,MSN-CN和MSN-COOH)中,但没有将其适当地加载到任何MSN中。然后从PTM-S获得PTM的游离碱(PTM-B),并将其成功加载到MSN中。具体而言,MSN-COOH表现出最高的负载能力。从不同的MSNs进行PTM-B动力学释放的体外评估。与裸MSN相比,观察到官能团在减缓药物释放方面的影响。总而言之,这些结果表明MSN-COOH可能是实现PTM受控释放的有希望的系统。

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