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A molecular insight into the electro-transfer of small molecules through electropores driven by electric fields

机译:通过电场驱动的电探测器通过电磁探测的小分子电传递的分子洞察

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摘要

The transport of chemical compounds across the plasma membrane into the cell is relevant for several biological and medical applications. One of the most efficient techniques to enhance this uptake is reversible electroporation. Nevertheless, the detailed molecular mechanism of transport of chemical species (dyes, drugs, genetic materials, ...) following the application of electric pulses is not yet fully elucidated. In the past decade, molecular dynamics (MD) simulations have been conducted to model the effect of pulsed electric fields on membranes, describing several aspects of this phenomenon. Here, we first present a comprehensive review of the results obtained so far modeling the electroporation of lipid membranes, then we extend these findings to study the electrotransfer across lipid bilayers subject to microsecond pulsed electric fields of Tate, a small hydrophilic charged peptide, and of siRNA. We use in particular a MD simulation protocol that allows to characterize the transport of charged species through stable pores. Unexpectedly, our results show that for an electroporated bilayer subject to transmembrane voltages in the order of 500 mV, i.e. consistent with experimental conditions, both Tat(11) and siRNA can translocate through nanoelectropores within tens of ns. We discuss these results in comparison to experiments in order to rationalize the mechanism of drug uptake by cells. This article is part of a Special Issue entitled: Biosimulations edited by Ilpo Vattulainen and Tomasz Rog. (C) 2016 Elsevier B.V. All rights reserved.
机译:对于多种生物和医学应用,将化学化合物穿过血浆膜的传输是相关的。增强这种吸收的最有效的技术之一是可逆电穿孔。然而,尚未完全阐明化学物质(染料,药物,遗传物质,...)的详细分子机制(染料,药物,遗传物质,......)尚未完全阐明。在过去十年中,已经进行了分子动力学(MD)模拟以模拟脉冲电场对膜上的影响,描述了这种现象的若干方面。在这里,我们首先向迄今为止造型脂膜的电穿孔的综合审查综合评审,然后我们延长了这些发现,以研究脂质双层的电动转换器,该方法受到微秒的脉冲电场,一种小型亲水性带电肽,和siRNA。我们特别使用MD仿真协议,其允许通过稳定的孔来表征带电物种的传输。意外地,我们的结果表明,对于电穿孔双层,通过500mV的跨膜电压,即与实验条件一致,TAT(11)和siRNA都可以通过纳米电影泵在数十的纳米中倾斜。我们讨论这些结果与实验相比,以使细胞吸毒机制合理化。本文是题为特殊问题的一部分:ILPO Vattulainen和Tomasz Rog编辑的生物捕获。 (c)2016年Elsevier B.v.保留所有权利。

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