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病毒和纳米颗粒通过网格蛋白介导的内吞作用进行细胞摄取的动力学。

Kinetics of cellular uptake of viruses and nanoparticles via clathrin-mediated endocytosis.

作者信息

Banerjee Anand, Berezhkovskii Alexander, Nossal Ralph

机构信息

Program in Physical Biology, Eunice Kennedy Shriver National Institute of Child Health, and Human Development, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Phys Biol. 2016 Feb 12;13(1):016005. doi: 10.1088/1478-3975/13/1/016005.

Abstract

Several viruses exploit clathrin-mediated endocytosis to gain entry into host cells. This process is also used extensively in biomedical applications to deliver nanoparticles (NPs) to diseased cells. The internalization of these nano-objects is controlled by the assembly of a clathrin-containing protein coat on the cytoplasmic side of the plasma membrane, which drives the invagination of the membrane and the formation of a cargo-containing endocytic vesicle. Current theoretical models of receptor-mediated endocytosis of viruses and NPs do not explicitly take coat assembly into consideration. In this paper we study cellular uptake of viruses and NPs with a focus on coat assembly. We characterize the internalization process by the mean time between the binding of a particle to the membrane and its entry into the cell. Using a coarse-grained model which maps the stochastic dynamics of coat formation onto a one-dimensional random walk, we derive an analytical formula for this quantity. A study of the dependence of the mean internalization time on NP size shows that there is an upper bound above which this time becomes extremely large, and an optimal size at which it attains a minimum. Our estimates of these sizes compare well with experimental data. We also study the sensitivity of the obtained results on coat parameters to identify factors which significantly affect the internalization kinetics.

摘要

几种病毒利用网格蛋白介导的内吞作用进入宿主细胞。这个过程在生物医学应用中也被广泛用于将纳米颗粒(NPs)递送至病变细胞。这些纳米物体的内化由质膜细胞质侧含网格蛋白的蛋白衣被的组装所控制,该组装驱动膜内陷并形成含货物的内吞囊泡。目前关于病毒和纳米颗粒受体介导内吞作用的理论模型并未明确考虑衣被组装。在本文中,我们研究病毒和纳米颗粒的细胞摄取,重点关注衣被组装。我们通过颗粒与膜结合到其进入细胞的平均时间来表征内化过程。使用一个粗粒化模型,该模型将衣被形成的随机动力学映射到一维随机游走,我们推导出了这个量的解析公式。对平均内化时间对纳米颗粒大小的依赖性研究表明,存在一个上限,超过该上限这个时间会变得极大,并且存在一个最佳大小,在该大小下它达到最小值。我们对这些大小的估计与实验数据比较吻合。我们还研究了所得结果对衣被参数的敏感性,以确定显著影响内化动力学的因素。

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