MPS blockade with liposomes controls pharmacokinetics of nanoparticles in a size-dependent manner.

Biomedical materials (Bristol, England) Pub Date : 2024-10-09 DOI:10.1088/1748-605X/ad7e6f

Iaroslav B Belyaev, Aziz B Mirkasymov, Vladislav I Rodionov, Julia S Babkova, Petr I Nikitin, Sergey M Deyev, Ivan V Zelepukin

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Abstract

Pharmacokinetics of nanomedicines can be improved by a temporal blockade of mononuclear phagocyte system (MPS) through the interaction with other biocompatible nanoparticles. Liposomes are excellent candidates as blocking agents, but the efficiency of the MPS blockade can greatly depend on the liposome properties. Here, we investigated the dependence of the efficiency of the induced MPS blockadein vitroandin vivoon the size of blocking liposomes in the 100-500 nm range. Saturation of RAW 264.7 macrophage uptake was observed for phosphatidylcholine/cholesterol liposomes larger than 200 nmin vitro. In mice, liposomes of all sizes exhibited a blocking effect on liver macrophages, prolonging the circulation of subsequently administrated magnetic nanoparticles in the bloodstream, reducing their liver uptake, and increasing accumulation in the spleen and lungs. Importantly, these effects became more pronounced with the increase of liposome size. Optimization of the size of the blocking liposomes holds the potential to enhance drug delivery and improve cancer therapy.

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用脂质体阻断 MPS 可控制纳米粒子的药代动力学，其方式取决于纳米粒子的大小。

纳米药物的药代动力学可以通过与其他生物相容性纳米颗粒的相互作用，对单核吞噬细胞系统（MPS）进行暂时性阻断而得到改善。脂质体是阻断剂的最佳候选者，但 MPS 的阻断效率在很大程度上取决于脂质体的特性。在此，我们研究了体外和体内诱导的 MPS 阻断效率与 100-500 nm 范围内阻断脂质体大小的关系。在体外，大于 200 nm 的磷脂酰胆碱/胆固醇脂质体对 RAW 264.7 巨噬细胞的摄取达到饱和。在小鼠体内，各种尺寸的脂质体都对肝脏巨噬细胞有阻滞作用，延长了随后给药的磁性纳米粒子在血液中的循环时间，减少了肝脏对它们的摄取，增加了在脾脏和肺部的积聚。重要的是，随着脂质体体积的增大，这些效果会变得更加明显。优化阻断脂质体的大小有望增强药物输送和改善癌症治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Biomedical materials (Bristol, England)

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