Free-energy landscapes of transmembrane homodimers by bias-exchange adaptively biased molecular dynamics

IF 3.3 3区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Shingo Ito , Yuji Sugita
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引用次数: 0

Abstract

Membrane proteins play essential roles in various biological functions within the cell. One of the most common functional regulations involves the dimerization of two single-pass transmembrane (TM) helices. Glycophorin A (GpA) and amyloid precursor protein (APP) form TM homodimers in the membrane, which have been investigated both experimentally and computationally. The homodimer structures are well characterized using only four collective variables (CVs) when each TM helix is stable. The CVs are the interhelical distance, the crossing angle, and the Crick angles for two TM helices. However, conformational sampling with multi-dimensional replica-exchange umbrella sampling (REUS) requires too many replicas to sample all the CVs for exploring the conformational landscapes. Here, we show that the bias-exchange adaptively biased molecular dynamics (BE-ABMD) with the four CVs effectively explores the free-energy landscapes of the TM helix dimers of GpA, wild-type APP and its mutants in the IMM1 implicit membrane. Compared to the original ABMD, the bias-exchange algorithm in BE-ABMD can provide a more rapidly converged conformational landscape. The BE-ABMD simulations could also reveal TM packing interfaces of the membrane proteins and the dependence of the free-energy landscapes on the membrane thickness. This approach is valuable for numerous other applications, including those involving explicit solvent and a lipid bilayer in all-atom force fields or Martini coarse-grained models, and enhances our understanding of protein-protein interactions in biological membranes.

Abstract Image

通过偏置交换自适应偏置分子动力学分析跨膜同源二聚体的自由能图谱
膜蛋白在细胞内的各种生物功能中发挥着至关重要的作用。最常见的功能调节之一涉及两个单程跨膜(TM)螺旋的二聚化。糖蛋白 A(GpA)和淀粉样前体蛋白(APP)在膜中形成 TM 同源二聚体,实验和计算都对其进行了研究。当每个 TM 螺旋稳定时,只需使用四个集合变量(CV)就能很好地描述同源二聚体结构。这些集体变量是两个 TM 螺旋的螺旋间距、交叉角和克里克角。然而,使用多维复制交换伞状采样(REUS)进行构象采样需要太多的复制来采样所有的 CVs 以探索构象景观。在这里,我们展示了具有四个 CV 的偏置交换自适应偏置分子动力学(BE-ABMD),它有效地探索了 IMM1 隐膜中 GpA、野生型 APP 及其突变体的 TM 螺旋二聚体的自由能谱。与原始的ABMD相比,BE-ABMD中的偏置交换算法能提供更快速收敛的构象景观。BE-ABMD模拟还能揭示膜蛋白的TM堆积界面以及自由能谱对膜厚度的依赖性。这种方法对许多其他应用都很有价值,包括在全原子力场或马蒂尼粗粒度模型中涉及显式溶剂和脂质双分子层的应用,并增强了我们对生物膜中蛋白质-蛋白质相互作用的理解。
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
Biophysical chemistry
Biophysical chemistry 生物-生化与分子生物学
CiteScore
6.10
自引率
10.50%
发文量
121
审稿时长
20 days
期刊介绍: Biophysical Chemistry publishes original work and reviews in the areas of chemistry and physics directly impacting biological phenomena. Quantitative analysis of the properties of biological macromolecules, biologically active molecules, macromolecular assemblies and cell components in terms of kinetics, thermodynamics, spatio-temporal organization, NMR and X-ray structural biology, as well as single-molecule detection represent a major focus of the journal. Theoretical and computational treatments of biomacromolecular systems, macromolecular interactions, regulatory control and systems biology are also of interest to the journal.
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