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三羧酸循环重编程促进了啮齿动物和人类骨骼肌对氧限制的代谢适应。

TCA cycle rewiring fosters metabolic adaptation to oxygen restriction in skeletal muscle from rodents and humans.

机构信息

Department of Biomedical Sciences for Health, University of Milan, Segrate, (MI), Italy.

UO Proteomica Clinica, IRCCS Policlinico San Donato, San Donato Milanese, (MI), Italy.

出版信息

Sci Rep. 2017 Aug 29;7(1):9723. doi: 10.1038/s41598-017-10097-4.

Abstract

In mammals, hypoxic stress management is under the control of the Hypoxia Inducible Factors, whose activity depends on the stabilization of their labile α subunit. In particular, the skeletal muscle appears to be able to react to changes in substrates and O delivery by tuning its metabolism. The present study provides a comprehensive overview of skeletal muscle metabolic adaptation to hypoxia in mice and in human subjects exposed for 7/9 and 19 days to high altitude levels. The investigation was carried out combining proteomics, qRT-PCR mRNA transcripts analysis, and enzyme activities assessment in rodents, and protein detection by antigen antibody reactions in humans and rodents. Results indicate that the skeletal muscle react to a decreased O delivery by rewiring the TCA cycle. The first TCA rewiring occurs in mice in 2-day hypoxia and is mediated by cytosolic malate whereas in 10-day hypoxia the rewiring is mediated by Idh1 and Fasn, supported by glutamine and HIF-2α increments. The combination of these specific anaplerotic steps can support energy demand despite HIFs degradation. These results were confirmed in human subjects, demonstrating that the TCA double rewiring represents an essential factor for the maintenance of muscle homeostasis during adaptation to hypoxia.

摘要

在哺乳动物中,缺氧应激管理受缺氧诱导因子(Hypoxia Inducible Factors,HIFs)的控制,其活性取决于其不稳定的α亚基的稳定。特别是骨骼肌似乎能够通过调节其代谢来对底物和 O 输送的变化做出反应。本研究在小鼠和暴露于高海拔环境 7/9 和 19 天的人类受试者中,全面概述了骨骼肌对缺氧的代谢适应。该研究结合蛋白质组学、qRT-PCR mRNA 转录物分析和酶活性评估在啮齿动物中进行,并在人类和啮齿动物中通过抗原抗体反应进行蛋白质检测。结果表明,骨骼肌通过重新布线三羧酸(TCA)循环来应对 O 输送减少。在 2 天的缺氧中,小鼠中的第一次 TCA 重新布线发生在细胞质苹果酸中,而在 10 天的缺氧中,重新布线由 Idh1 和 Fasn 介导,由谷氨酰胺和 HIF-2α 的增加支持。这些特定的氨酰化步骤的组合可以支持能量需求,尽管 HIFs 降解。这些结果在人类受试者中得到了证实,表明 TCA 双重新布线是维持缺氧适应期间肌肉内稳态的重要因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b199/5575144/4f67cefa3193/41598_2017_10097_Fig4_HTML.jpg

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