电渗透后带电小分子的输运——漂移和扩散。

Q1 Biochemistry, Genetics and Molecular Biology
BMC Biophysics Pub Date : 2018-03-21 eCollection Date: 2018-01-01 DOI:10.1186/s13628-018-0044-2
Esin B Sözer, C Florencia Pocetti, P Thomas Vernier
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引用次数: 31

摘要

背景:电场诱导细胞渗透的应用范围从癌症治疗到废水处理。然而,对膜电渗透的潜在机制的统一理解尚未实现。协议是经验性的,模型是描述性的而不是预测性的,这阻碍了基于电穿孔技术的优化和扩展。现有模型的一个共同特征是假设渗透膜是被动的,并且通过它的运输完全是扩散的。为了证明超越这一假设的必要性,我们在这里对三种常用的电穿孔研究小分子——yopro -1、丙酸和钙黄蛋白——在细胞暴露于最小干扰的6ns电脉冲后的渗透后转运进行了定量分析。结果:YO-PRO-1从外部介质流入细胞的量超过丙膜,这与许多已发表的研究结果一致。两者都比钙素的流入要大得多。相比之下,经电渗透后,钙黄素从预负载细胞向介质的归一化摩尔流出大致相当于YO-PRO-1和丙烯的内流。这些相对输运速率与分子的大小或横截面无关,而与分子的电荷极性有关。结论:对三个带电小分子通过电渗透细胞膜的分子运输动力学的比较揭示了电穿孔机制的一个组成部分,而这个部分通常只在电脉冲传递期间被考虑。丙酸、YO-PRO-1(阳离子)和钙黄蛋白(阴离子)内流速率之间的巨大差异,以及钙黄蛋白内流和流出速率之间的巨大差异,表明脉冲后跨膜电位在离子和带电小分子跨渗透细胞膜迁移中的重要作用,这在电穿孔模型中很大程度上被忽视了。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Transport of charged small molecules after electropermeabilization - drift and diffusion.

Transport of charged small molecules after electropermeabilization - drift and diffusion.

Transport of charged small molecules after electropermeabilization - drift and diffusion.

Transport of charged small molecules after electropermeabilization - drift and diffusion.

Background: Applications of electric-field-induced permeabilization of cells range from cancer therapy to wastewater treatment. A unified understanding of the underlying mechanisms of membrane electropermeabilization, however, has not been achieved. Protocols are empirical, and models are descriptive rather than predictive, which hampers the optimization and expansion of electroporation-based technologies. A common feature of existing models is the assumption that the permeabilized membrane is passive, and that transport through it is entirely diffusive. To demonstrate the necessity to go beyond that assumption, we present here a quantitative analysis of the post-permeabilization transport of three small molecules commonly used in electroporation research - YO-PRO-1, propidium, and calcein - after exposure of cells to minimally perturbing, 6 ns electric pulses.

Results: Influx of YO-PRO-1 from the external medium into the cell exceeds that of propidium, consistent with many published studies. Both are much greater than the influx of calcein. In contrast, the normalized molar efflux of calcein from pre-loaded cells into the medium after electropermeabilization is roughly equivalent to the influx of YO-PRO-1 and propidium. These relative transport rates are correlated not with molecular size or cross-section, but rather with molecular charge polarity.

Conclusions: This comparison of the kinetics of molecular transport of three small, charged molecules across electropermeabilized cell membranes reveals a component of the mechanism of electroporation that is customarily taken into account only for the time during electric pulse delivery. The large differences between the influx rates of propidium and YO-PRO-1 (cations) and calcein (anion), and between the influx and efflux of calcein, suggest a significant role for the post-pulse transmembrane potential in the migration of ions and charged small molecules across permeabilized cell membranes, which has been largely neglected in models of electroporation.

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BMC Biophysics
BMC Biophysics BIOPHYSICS-
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