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线粒体三羧酸循环、氧化磷酸化、代谢物转运及电生理学的计算机建模

Computer modeling of mitochondrial tricarboxylic acid cycle, oxidative phosphorylation, metabolite transport, and electrophysiology.

作者信息

Wu Fan, Yang Feng, Vinnakota Kalyan C, Beard Daniel A

机构信息

Biotechnology and Bioengineering Center and Department of Physiology, Medical College of Wisconsin, Milwaukee, Wisconsin 53226, USA.

出版信息

J Biol Chem. 2007 Aug 24;282(34):24525-37. doi: 10.1074/jbc.M701024200. Epub 2007 Jun 25.

Abstract

A computational model of mitochondrial metabolism and electrophysiology is introduced and applied to analysis of data from isolated cardiac mitochondria and data on phosphate metabolites in striated muscle in vivo. This model is constructed based on detailed kinetics and thermodynamically balanced reaction mechanisms and a strict accounting of rapidly equilibrating biochemical species. Since building such a model requires introducing a large number of adjustable kinetic parameters, a correspondingly large amount of independent data from isolated mitochondria respiring on different substrates and subject to a variety of protocols is used to parameterize the model and ensure that it is challenged by a wide range of data corresponding to diverse conditions. The developed model is further validated by both in vitro data on isolated cardiac mitochondria and in vivo experimental measurements on human skeletal muscle. The validated model is used to predict the roles of NAD and ADP in regulating the tricarboxylic acid cycle dehydrogenase fluxes, demonstrating that NAD is the more important regulator. Further model predictions reveal that a decrease of cytosolic pH value results in decreases in mitochondrial membrane potential and a corresponding drop in the ability of the mitochondria to synthesize ATP at the hydrolysis potential required for cellular function.

摘要

介绍了一种线粒体代谢和电生理的计算模型,并将其应用于分析来自分离的心脏线粒体的数据以及体内横纹肌中磷酸盐代谢物的数据。该模型基于详细的动力学和热力学平衡反应机制构建,并严格考虑了快速平衡的生化物种。由于构建这样一个模型需要引入大量可调节的动力学参数,因此使用了来自在不同底物上呼吸并接受各种实验方案的分离线粒体的相应大量独立数据来对模型进行参数化,并确保它受到对应于不同条件的广泛数据的检验。所开发的模型通过关于分离的心脏线粒体的体外数据和关于人类骨骼肌的体内实验测量进一步验证。经过验证的模型用于预测NAD和ADP在调节三羧酸循环脱氢酶通量中的作用,表明NAD是更重要的调节因子。进一步的模型预测表明,细胞质pH值的降低会导致线粒体膜电位降低,以及线粒体在细胞功能所需的水解电位下合成ATP的能力相应下降。

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