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探索 A 型细胞色素 c 氧化酶中的氧气扩散:分子动力学模拟揭示了两条通向双核位点的替代通道。

Exploring O2 diffusion in A-type cytochrome c oxidases: molecular dynamics simulations uncover two alternative channels towards the binuclear site.

作者信息

Oliveira A Sofia F, Damas João M, Baptista António M, Soares Cláudio M

机构信息

ITQB - Instituto de Tecnologia Química e Biológica António Xavier, Universidade Nova de Lisboa, Oeiras, Portugal.

出版信息

PLoS Comput Biol. 2014 Dec 4;10(12):e1004010. doi: 10.1371/journal.pcbi.1004010. eCollection 2014 Dec.

Abstract

Cytochrome c oxidases (Ccoxs) are the terminal enzymes of the respiratory chain in mitochondria and most bacteria. These enzymes couple dioxygen (O2) reduction to the generation of a transmembrane electrochemical proton gradient. Despite decades of research and the availability of a large amount of structural and biochemical data available for the A-type Ccox family, little is known about the channel(s) used by O2 to travel from the solvent/membrane to the heme a3-CuB binuclear center (BNC). Moreover, the identification of all possible O2 channels as well as the atomic details of O2 diffusion is essential for the understanding of the working mechanisms of the A-type Ccox. In this work, we determined the O2 distribution within Ccox from Rhodobacter sphaeroides, in the fully reduced state, in order to identify and characterize all the putative O2 channels leading towards the BNC. For that, we use an integrated strategy combining atomistic molecular dynamics (MD) simulations (with and without explicit O2 molecules) and implicit ligand sampling (ILS) calculations. Based on the 3D free energy map for O2 inside Ccox, three channels were identified, all starting in the membrane hydrophobic region and connecting the surface of the protein to the BNC. One of these channels corresponds to the pathway inferred from the X-ray data available, whereas the other two are alternative routes for O2 to reach the BNC. Both alternative O2 channels start in the membrane spanning region and terminate close to Y288I. These channels are a combination of multiple transiently interconnected hydrophobic cavities, whose opening and closure is regulated by the thermal fluctuations of the lining residues. Furthermore, our results show that, in this Ccox, the most likely (energetically preferred) routes for O2 to reach the BNC are the alternative channels, rather than the X-ray inferred pathway.

摘要

细胞色素c氧化酶(Ccoxs)是线粒体和大多数细菌中呼吸链的末端酶。这些酶将双氧(O₂)还原与跨膜电化学质子梯度的产生相偶联。尽管对A型Ccox家族进行了数十年的研究,且已有大量的结构和生化数据,但对于O₂从溶剂/膜传输至血红素a₃-CuB双核中心(BNC)所使用的通道仍知之甚少。此外,识别所有可能的O₂通道以及O₂扩散的原子细节对于理解A型Ccox的工作机制至关重要。在这项工作中,我们测定了处于完全还原状态的球形红细菌Ccox内的O₂分布,以识别和表征通向BNC的所有假定O₂通道。为此,我们采用了一种综合策略,将原子分子动力学(MD)模拟(有无明确的O₂分子)和隐式配体采样(ILS)计算相结合。基于Ccox内O₂的三维自由能图,识别出了三个通道,它们均始于膜疏水区域,并将蛋白质表面连接至BNC。其中一个通道对应于根据现有X射线数据推断出的途径,而另外两个是O₂到达BNC的替代途径。这两个替代O₂通道均始于跨膜区域,并在靠近Y288I处终止。这些通道是多个瞬时相互连接的疏水腔的组合,其打开和关闭由内衬残基的热涨落调节。此外,我们的结果表明,在这种Ccox中,O₂到达BNC的最可能(能量上更有利)途径是替代通道,而非X射线推断的途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f972/4256069/f7134ab83794/pcbi.1004010.g001.jpg

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