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首页> 外文期刊>Acta biomaterialia >Colloidal stability of nano-sized particles in the peritoneal fluid: Towards optimizing drug delivery systems for intraperitoneal therapy
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Colloidal stability of nano-sized particles in the peritoneal fluid: Towards optimizing drug delivery systems for intraperitoneal therapy

机译:腹膜液中纳米尺寸颗粒的胶体稳定性:优化用于腹膜内治疗的药物输送系统

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摘要

Intraperitoneal (IP) administration of nano-sized delivery vehicles containing small interfering RNA (siRNA) has recently gained attention as an alternative route for the efficient treatment of peritoneal carcinomatosis. The colloidal stability of nanomatter following IP administration has, however, not been thoroughly investigated yet. Here, enabled by advanced microscopy methods such as single particle tracking and fluorescence correlation spectroscopy, we follow the aggregation and cargo release of nano-scaled systems directly in peritoneal fluids from healthy mice and ascites fluid from a patient diagnosed with peritoneal carcinomatosis. The colloidal stability in the peritoneal fluids was systematically studied as a function of the charge (positive or negative) and poly(ethylene glycol) (PEG) degree of liposomes and polystyrene nanoparticles, and compared to human serum. Our data demonstrate strong aggregation of cationic and anionic nanoparticles in the peritoneal fluids, while only slight aggregation was observed for the PEGylated ones. PEGylated liposomes, however, lead to a fast and premature release of siRNA cargo in the peritoneal fluids. Based on our observations, we reflect on how to tailor improved delivery systems for IP therapy.
机译:含有小干扰RNA(siRNA)的纳米级运载工具的腹膜内(IP)管理最近作为一种有效治疗腹膜癌的替代途径而受到关注。 IP给药后,纳米物质的胶体稳定性尚未得到彻底研究。在这里,通过先进的显微镜方法(例如单颗粒跟踪和荧光相关光谱法),我们可以直接在健康小鼠的腹膜液和诊断为腹膜癌的患者的腹水中跟踪纳米级系统的聚集和释放。根据脂质体和聚苯乙烯纳米颗粒的电荷(正或负)和聚(乙二醇)(PEG)度,系统地研究了腹膜液中的胶体稳定性,并与人血清进行了比较。我们的数据表明,腹膜液中阳离子和阴离子纳米颗粒的强聚集性,而聚乙二醇化的仅观察到轻微聚集。但是,聚乙二醇化脂质体会导致siRNA货物在腹膜液中快速过早释放。根据我们的观察,我们思考如何为IP治疗量身定制改进的输送系统。

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