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原子尺度和粗粒度模拟中的膜孔形成

Membrane pore formation in atomistic and coarse-grained simulations.

作者信息

Kirsch Sonja A, Böckmann Rainer A

机构信息

Computational Biology, Department of Biology, Friedrich-Alexander Universität Erlangen-Nürnberg, Erlangen, Germany.

Computational Biology, Department of Biology, Friedrich-Alexander Universität Erlangen-Nürnberg, Erlangen, Germany.

出版信息

Biochim Biophys Acta. 2016 Oct;1858(10):2266-2277. doi: 10.1016/j.bbamem.2015.12.031. Epub 2015 Dec 31.

Abstract

Biological cells and their organelles are protected by ultra thin membranes. These membranes accomplish a broad variety of important tasks like separating the cell content from the outer environment, they are the site for cell-cell interactions and many enzymatic reactions, and control the in- and efflux of metabolites. For certain physiological functions e.g. in the fusion of membranes and also in a number of biotechnological applications like gene transfection the membrane integrity needs to be compromised to allow for instance for the exchange of polar molecules across the membrane barrier. Mechanisms enabling the transport of molecules across the membrane involve membrane proteins that form specific pores or act as transporters, but also so-called lipid pores induced by external fields, stress, or peptides. Recent progress in the simulation field enabled to closely mimic pore formation as supposed to occur in vivo or in vitro. Here, we review different simulation-based approaches in the study of membrane pores with a focus on lipid pore properties such as their size and energetics, poration mechanisms based on the application of external fields, charge imbalances, or surface tension, and on pores that are induced by small molecules, peptides, and lipids. This article is part of a Special Issue entitled: Biosimulations edited by Ilpo Vattulainen and Tomasz Róg.

摘要

生物细胞及其细胞器由超薄膜保护。这些膜完成各种各样重要的任务,如将细胞内容物与外部环境分隔开,它们是细胞间相互作用和许多酶促反应的场所,并控制代谢物的流入和流出。对于某些生理功能,例如在膜融合过程中,以及在许多生物技术应用(如基因转染)中,需要破坏膜的完整性,以便例如使极性分子能够穿过膜屏障进行交换。使分子跨膜运输的机制涉及形成特定孔道或充当转运体的膜蛋白,也包括由外部电场、应力或肽诱导形成的所谓脂质孔道。模拟领域的最新进展使得能够紧密模拟体内或体外可能发生的孔道形成过程。在此,我们综述了基于模拟的不同方法在膜孔道研究中的应用,重点关注脂质孔道的性质,如大小和能量学,基于外部电场、电荷失衡或表面张力应用的成孔机制,以及由小分子、肽和脂质诱导形成的孔道。本文是由伊尔波·瓦图莱宁(Ilpo Vattulainen)和托马什·罗格(Tomasz Róg)编辑的名为《生物模拟》特刊的一部分。

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