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通过平行激活对氧化磷酸化的调节

Regulation of oxidative phosphorylation through parallel activation.

作者信息

Korzeniewski Bernard

机构信息

Faculty of Biochemistry, Biophysics and Biotechnology, Jagiellonian University, ul. Gronostajowa 7, 30-387 Kraków, Poland.

出版信息

Biophys Chem. 2007 Sep;129(2-3):93-110. doi: 10.1016/j.bpc.2007.05.013. Epub 2007 May 31.

Abstract

When the mechanical work intensity in muscle increases, the elevated ATP consumption rate must be matched by the rate of ATP production by oxidative phosphorylation in order to avoid a quick exhaustion of ATP. The traditional mechanism of the regulation of oxidative phosphorylation, namely the negative feedback involving [ADP] and [Pi] as regulatory signals, is not sufficient to account for various kinetic properties of the system in intact skeletal muscle and heart in vivo. Theoretical studies conducted using a dynamic computer model of oxidative phosphorylation developed previously strongly suggest the so-called each-step-activation (or parallel activation) mechanism, due to which all oxidative phosphorylation complexes are directly activated by some cytosolic factor/mechanism related to muscle contraction in parallel with the activation of ATP usage and substrate dehydrogenation by calcium ions. The present polemic article reviews and discusses the growing evidence supporting this mechanism and compares it with alternative mechanisms proposed in the literature. It is concluded that only the each-step-activation mechanism is able to explain the rich set of various experimental results used as a reference for estimating the validity and applicability of particular mechanisms.

摘要

当肌肉中的机械工作强度增加时,升高的ATP消耗速率必须与氧化磷酸化产生ATP的速率相匹配,以避免ATP迅速耗尽。传统的氧化磷酸化调节机制,即以[ADP]和[Pi]作为调节信号的负反馈,不足以解释完整骨骼肌和心脏在体内系统的各种动力学特性。使用先前开发的氧化磷酸化动态计算机模型进行的理论研究有力地表明了所谓的逐步激活(或平行激活)机制,由于该机制,所有氧化磷酸化复合物都被一些与肌肉收缩相关的胞质因子/机制直接激活,这与钙离子对ATP利用和底物脱氢的激活是平行的。这篇有争议的文章回顾并讨论了支持该机制的越来越多的证据,并将其与文献中提出的替代机制进行了比较。得出的结论是,只有逐步激活机制能够解释丰富多样的各种实验结果,这些结果被用作评估特定机制的有效性和适用性的参考。

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