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多价配体-受体介导的小填充囊泡与细胞膜的相互作用。

Multivalent ligand-receptor-mediated interaction of small filled vesicles with a cellular membrane.

机构信息

Division of Biological Physics, Department of Physics, Chalmers University of Technology, S-41296 Göteborg, Sweden and Boreskov Institute of Catalysis, Russian Academy of Sciences, Novosibirsk 630090, Russia.

出版信息

Phys Rev E. 2017 Jul;96(1-1):012408. doi: 10.1103/PhysRevE.96.012408. Epub 2017 Jul 17.

Abstract

The ligand-receptor-mediated contacts of small sub-100-nm-sized lipid vesicles (or nanoparticles) with the cellular membrane are of interest in the contexts of cell-to-cell communication, endocytosis of membrane-coated virions, and drug (RNA) delivery. In all these cases, the interior of vesicles is filled by biologically relevant content. Despite the diversity of such systems, the corresponding ligand-receptor interaction possesses universal features. One of them is that the vesicle-membrane contacts can be accompanied by the redistribution of ligands and receptors between the contact and contact-free regions. In particular, the concentrations of ligands and receptors may become appreciably higher in the contact regions and their composition may there be different compared to that in the suspended state in the solution. A statistical model presented herein describes the corresponding distribution of various ligands and receptors and allows one to calculate the related change of the free energy with variation of the vesicle-engulfment extent. The results obtained are used to clarify the necessary conditions for the vesicle-assisted pathway of drug delivery.

摘要

小分子亚 100nm 脂质囊泡(或纳米颗粒)与细胞膜之间的配体-受体介导的接触,在细胞间通讯、膜包裹病毒的内吞作用以及药物(RNA)递送上引起了人们的兴趣。在所有这些情况下,囊泡的内部充满了具有生物学相关性的内容。尽管这些系统具有多样性,但相应的配体-受体相互作用具有普遍特征。其中之一是囊泡-膜接触可能伴随着配体和受体在接触区和非接触区之间的重新分布。特别是,在接触区中,配体和受体的浓度可能会显著升高,并且其组成可能与在溶液中悬浮状态下的组成不同。本文提出的统计模型描述了各种配体和受体的相应分布,并且可以用来计算随着囊泡包裹程度的变化,自由能的相关变化。所得到的结果用于阐明囊泡辅助药物递送途径的必要条件。

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