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理论证据表明细菌视紫红质存在多种电荷转移途径。

Theoretical Evidence for Multiple Charge Transfer Pathways in Bacteriorhodopsin.

机构信息

C. Eugene Bennett Department of Chemistry, West Virginia University , Morgantown, West Virginia 26506, United States.

出版信息

J Chem Theory Comput. 2016 Apr 12;12(4):1639-46. doi: 10.1021/acs.jctc.6b00033. Epub 2016 Mar 14.

Abstract

The development of molecular-scale junctions utilizing biomolecules is a challenging field that requires intimate knowledge of the relationship between molecular structure and conductance characteristics. One of the key parameters to understanding conductance efficiency is the charge mobility, which strongly influences the response time of electronic devices. The charge mobility of bacteriorhodopsin (bR), a membrane protein that has been studied experimentally in detail, was theoretically investigated using extended Marcus-Hush theory. Charge mobilities of 1.3 × 10(-2) and 9.7 × 10(-4) cm(2)/(V s) for hole and electron transfer, respectively, were determined. The computed electron mobility is comparable to experimentally measured values (9 × 10(-4) cm(2)/(V s)). Interestingly, the pathways for hole and electron hopping were very distinct from each other, utilizing different transmembrane helices to traverse the protein. In particular, only the electron transfer pathway involved the retinal chromophore, indicating that the efficiency of charge transfer is directly affected by the tertiary arrangement of proteins. Our results provide a template for obtaining the molecular and electronic-level details that can reveal fundamental insights into experimental studies on protein electron transport and inform efficient design of biomolecular-based junctions on the nanoscale.

摘要

利用生物分子开发分子尺度结是一个具有挑战性的领域,需要深入了解分子结构与电导特性之间的关系。理解电导效率的关键参数之一是电荷迁移率,它强烈影响电子设备的响应时间。细菌视紫红质(bR)是一种已在实验中详细研究过的膜蛋白,我们使用扩展的马库斯-休斯理论对其电荷迁移率进行了理论研究。分别确定了空穴和电子转移的电荷迁移率为 1.3×10(-2)和 9.7×10(-4)cm(2)/(V s)。计算出的电子迁移率与实验测量值(9×10(-4)cm(2)/(V s))相当。有趣的是,空穴和电子跳跃的途径彼此非常不同,利用不同的跨膜螺旋穿越蛋白质。特别是,只有电子转移途径涉及视黄醛发色团,这表明电荷转移的效率直接受到蛋白质三级结构的影响。我们的结果为获得分子和电子层面的细节提供了模板,这些细节可以揭示蛋白质电子输运实验研究的基本见解,并为纳米尺度上基于生物分子的结的有效设计提供信息。

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