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需氧呼吸:以氧为中心的燃烧观点的概念验证。

Aerobic respiration: proof of concept for the oxygen-centric murburn perspective.

机构信息

Satyamjayatu: The Science and Ethics Foundation , Palakkad, Kerala, India.

Department of Biotechnology, Vignan's Foundation for Science, Technology & Research , Vadlamudi , Guntur, Andhra Pradesh, India.

出版信息

J Biomol Struct Dyn. 2019 Oct;37(17):4542-4556. doi: 10.1080/07391102.2018.1552896. Epub 2019 Jan 8.

Abstract

The inner mitochondrial membrane protein complexes (I-V) and prokaryotic respiratory machinery are examined for a deeper understanding of their structure-function correlations and dynamics. analysis of the structure of complexes I-IV, docking studies and erstwhile literature confirm that they carry sites which are in close proximity to DROS (diffusible reactive oxygen species) generating redox centers. These findings provide supportive evidence for the newly proposed oxygen-centric chemical-coupling mechanism (murburn concept), wherein DROS catalyzes the esterification of inorganic phosphate to ADP. Further, in a reductionist system, we demonstrate that a DROS (like superoxide) can effectively esterify inorganic phosphate to ADP. The impact of these findings and the interactive dynamics of classical inhibitors (rotenone and cyanide), uncouplers (dinitrophenol and uncoupling protein) and other toxins (atractyloside and oligomycin) are briefly discussed. • Earlier perception: Complexes (I-IV) pump protons and Complex V make ATP (aided by protons) • Herein: Respiratory molecular machinery is probed for new structure-function correlations • Analyses: Quantitative arguments discount proton-centric ATP synthesis in mitochondria and bacteria • data: ADP-binding sites and O/ diffusible reactive oxygen species (DROS)-accessible channels are unveiled in respiratory proteins • data: Using luminometry, ATP synthesis is demonstrated from ADP, Pi and superoxide • Inference: Findings agree with decentralized ADP-Pi activation via oxygen-centric murburn scheme Communicated by Ramaswamy H. Sarma.

摘要

为了更深入地了解它们的结构-功能关系和动态,我们研究了线粒体内膜蛋白复合物(I-V)和原核呼吸机制。对复合物 I-IV 的结构进行分析、对接研究和以往的文献证实,它们携带有与 DROS(可扩散活性氧)生成氧化还原中心密切相关的位点。这些发现为新提出的以氧为中心的化学偶联机制(murburn 概念)提供了支持性证据,其中 DROS 催化无机磷酸盐与 ADP 的酯化反应。此外,在一个还原系统中,我们证明 DROS(如超氧阴离子)可以有效地将无机磷酸盐酯化生成 ADP。这些发现的影响以及经典抑制剂(鱼藤酮和氰化物)、解偶联剂(二硝基苯酚和解偶联蛋白)和其他毒素(苍术苷和寡霉素)的相互作用动力学将简要讨论。• 早期认识:复合物(I-IV)泵质子,复合物 V 利用质子生成 ATP• 本文:探究呼吸分子机制以发现新的结构-功能关系• 分析:定量分析否定了线粒体和细菌中以质子为中心的 ATP 合成• 数据:揭示了呼吸蛋白中的 ADP 结合位点和 O/可扩散活性氧(DROS)可及通道• 数据:使用发光法,从 ADP、Pi 和超氧阴离子证明了 ATP 的合成• 推断:这些发现与通过以氧为中心的 murburn 方案分散激活 ADP-Pi 的观点一致。 通讯作者:Ramaswamy H. Sarma。

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