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建模两亲性聚合物纳米颗粒与生物膜的相互作用,指导药物输送系统的合理设计。

Modeling the interaction of amphiphilic polymer nanoparticles with biomembranes to Guide rational design of drug delivery systems.

机构信息

NanoBioLab, Dipartimento di Biotecnologie e Bioscienze, Università di Milano-Bicocca, Piazza della Scienza 2, 20126, Milano, Italy.

NanoBioLab, Dipartimento di Biotecnologie e Bioscienze, Università di Milano-Bicocca, Piazza della Scienza 2, 20126, Milano, Italy; Nanomedicine Laboratory, ICS Maugeri S.p.A. SB, via S. Maugeri 10, 27100, Pavia, Italy.

出版信息

Colloids Surf B Biointerfaces. 2020 Dec;196:111366. doi: 10.1016/j.colsurfb.2020.111366. Epub 2020 Sep 19.

DOI:10.1016/j.colsurfb.2020.111366
PMID:32992287
Abstract

Nanoparticle assisted drug delivery to the cytoplasm is limited by sequestration of nanoparticles in endosomes. Endosomal escape through polymer-induced membrane destabilization is one of a few well characterized mechanisms to overcome it. Aiming to utilize this method in vivo, it is necessary to understand how modulating the structural and chemical features of the polymer and the presence of proteins in biological fluids can affect this activity. Here, as a model for the endosomal membrane, we use the membrane of red blood cells to evaluate the membrane destabilization ability of a model amphiphilic polymer in the presence of blood plasma using a hemolysis assay. This allows determination of red blood cells membrane permeabilization through the quantification of hemoglobin leakage. Our results showed a strong inhibitory effect of plasma, and that hemolytic activity can be improved by chemical modification of the polymeric micelle, reducing its interaction with plasma proteins. Finally, a second mechanism of pH-induced direct diffusion is proposed and tested using an oil/water partitioning model. These results offer a body of knowledge to improve delivery of drugs across biological membranes using carefully designed polymeric nanocarriers.

摘要

纳米颗粒辅助药物递送至细胞质受到纳米颗粒在内体中隔离的限制。通过聚合物诱导的膜去稳定化实现内体逃逸是少数几种经过充分表征的克服该限制的机制之一。为了在体内利用这种方法,有必要了解调节聚合物的结构和化学特征以及生物流体中蛋白质的存在如何影响这种活性。在这里,我们使用红细胞膜作为内体膜的模型,使用溶血测定法在血浆存在的情况下评估模型两亲聚合物的膜去稳定化能力。这允许通过定量血红蛋白泄漏来确定红细胞膜的通透性。我们的结果表明血浆具有很强的抑制作用,并且通过化学修饰聚合物胶束可以提高溶血活性,从而减少其与血浆蛋白的相互作用。最后,使用油水分配模型提出并测试了第二种 pH 诱导的直接扩散机制。这些结果为使用精心设计的聚合物纳米载体改善跨生物膜药物递送提供了知识体系。

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