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重新审视缺氧状态下活性氧的产生

Revisiting reactive oxygen species production in hypoxia.

作者信息

Alva Ricardo, Wiebe Jacob E, Stuart Jeffrey A

机构信息

Department of Biological Sciences, Brock University, St. Catharines, ON, L2S 3A1, Canada.

出版信息

Pflugers Arch. 2024 Sep;476(9):1423-1444. doi: 10.1007/s00424-024-02986-1. Epub 2024 Jul 3.

DOI:10.1007/s00424-024-02986-1
PMID:38955833
Abstract

Cellular responses to hypoxia are crucial in various physiological and pathophysiological contexts and have thus been extensively studied. This has led to a comprehensive understanding of the transcriptional response to hypoxia, which is regulated by hypoxia-inducible factors (HIFs). However, the detailed molecular mechanisms of HIF regulation in hypoxia remain incompletely understood. In particular, there is controversy surrounding the production of mitochondrial reactive oxygen species (ROS) in hypoxia and how this affects the stabilization and activity of HIFs. This review examines this controversy and attempts to shed light on its origin. We discuss the role of physioxia versus normoxia as baseline conditions that can affect the subsequent cellular response to hypoxia and highlight the paucity of data on pericellular oxygen levels in most experiments, leading to variable levels of hypoxia that might progress to anoxia over time. We analyze the different outcomes reported in isolated mitochondria, versus intact cells or whole organisms, and evaluate the reliability of various ROS-detecting tools. Finally, we examine the cell-type and context specificity of oxygen's various effects. We conclude that while recent evidence suggests that the effect of hypoxia on ROS production is highly dependent on the cell type and the duration of exposure, efforts should be made to conduct experiments under carefully controlled, physiological microenvironmental conditions in order to rule out potential artifacts and improve reproducibility in research.

摘要

细胞对缺氧的反应在各种生理和病理生理环境中都至关重要,因此已得到广泛研究。这使得人们对缺氧诱导因子(HIFs)调控的缺氧转录反应有了全面的了解。然而,缺氧条件下HIF调控的详细分子机制仍未完全明确。特别是,关于缺氧条件下线粒体活性氧(ROS)的产生及其如何影响HIF的稳定性和活性存在争议。本综述探讨了这一争议,并试图阐明其根源。我们讨论了作为基线条件的生理性氧分压与常氧对后续细胞缺氧反应的影响,并强调大多数实验中关于细胞周围氧水平的数据匮乏,这导致缺氧程度各异,且可能随时间发展为无氧状态。我们分析了在分离的线粒体、完整细胞或整个生物体中报道的不同结果,并评估了各种ROS检测工具的可靠性。最后,我们研究了氧的各种效应的细胞类型和环境特异性。我们得出结论,虽然最近的证据表明缺氧对ROS产生的影响高度依赖于细胞类型和暴露持续时间,但仍应努力在精心控制的生理微环境条件下进行实验,以排除潜在的人为因素并提高研究的可重复性。

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SIRT3 Regulates the ROS-FPR1/HIF-1α Axis under Hypoxic Conditions to Influence Lung Cancer Progression.SIRT3 通过调控低氧条件下 ROS-FPR1/HIF-1α 轴影响肺癌进展。
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