Energetics of the H-Bond Network in Exiguobacterium sibiricum Rhodopsin

IF 2.9 3区生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY

Biochemistry Biochemistry Pub Date : 2024-05-14 DOI:10.1021/acs.biochem.4c00182

Tomoyasu Noji, Yoshihiro Chiba, Keisuke Saito and Hiroshi Ishikita*,

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Abstract

Exiguobacterium sibiricum rhodopsin (ESR) functions as a light-driven proton pump utilizing Lys96 for proton uptake and maintaining its activity over a wide pH range. Using a combination of methodologies including the linear Poisson–Boltzmann equation and a quantum mechanical/molecular mechanical approach with a polarizable continuum model, we explore the microscopic mechanisms underlying its pumping activity. Lys96, the primary proton uptake site, remains deprotonated owing to the loss of solvation in the ESR protein environment. Asp85, serving as a proton acceptor group for Lys96, does not form a low-barrier H-bond with His57. Instead, deprotonated Asp85 forms a salt-bridge with protonated His57, and the proton is predominantly located at the His57 moiety. Glu214, the only acidic residue at the end of the H-bond network exhibits a pK_a value of ∼6, slightly elevated due to solvation loss. It seems likely that the H-bond network [Asp85···His57···H₂O···Glu214] serves as a proton-conducting pathway toward the protein bulk surface.

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西西伯利亚外分支杆菌罗丹明中 H 键网络的能量学。

西伯利亚外分支杆菌（Exiguobacterium sibiricum）的罗丹明（ESR）是一种光驱动质子泵，利用 Lys96 吸收质子，并在很宽的 pH 值范围内保持其活性。我们综合运用线性泊松-波尔兹曼方程和量子力学/分子力学方法以及可极化连续体模型，探索了其泵活性的微观机制。Lys96 是主要的质子吸收位点，由于在 ESR 蛋白环境中失去了溶解作用而保持去质子状态。作为 Lys96 质子接受基团的 Asp85 不会与 His57 形成低阻 H 键。相反，去质子化的 Asp85 与质子化的 His57 形成盐桥，质子主要位于 His57 分子。H 键网络末端唯一的酸性残基 Glu214 的 pKa 值为 6，由于溶解损失而略有升高。看来H键网络[Asp85--His57--H2O--Glu214]很可能是质子向蛋白质体表面传导的途径。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Biochemistry Biochemistry 生物-生化与分子生物学

CiteScore

5.50

自引率

3.40%

发文量

336

审稿时长

1-2 weeks

期刊介绍： Biochemistry provides an international forum for publishing exceptional, rigorous, high-impact research across all of biological chemistry. This broad scope includes studies on the chemical, physical, mechanistic, and/or structural basis of biological or cell function, and encompasses the fields of chemical biology, synthetic biology, disease biology, cell biology, nucleic acid biology, neuroscience, structural biology, and biophysics. In addition to traditional Research Articles, Biochemistry also publishes Communications, Viewpoints, and Perspectives, as well as From the Bench articles that report new methods of particular interest to the biological chemistry community.