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细胞色素氧化酶亚基 4 同工型交换导致氧亲和力的调节。

Cytochrome Oxidase Subunit 4 Isoform Exchange Results in Modulation of Oxygen Affinity.

机构信息

Department of Bioenergetics, Institute of Physiology, Czech Academy of Sciences, 14220 Prague 4, Czech Republic.

Department of Cell Biology, Faculty of Science, Charles University, 12000 Prague 2, Czech Republic.

出版信息

Cells. 2020 Feb 14;9(2):443. doi: 10.3390/cells9020443.

Abstract

Cytochrome oxidase (COX) is regulated through tissue-, development- or environment-controlled expression of subunit isoforms. The COX4 subunit is thought to optimize respiratory chain function according to oxygen-controlled expression of its isoforms COX4i1 and COX4i2. However, biochemical mechanisms of regulation by the two variants are only partly understood. We created an HEK293-based knock-out cellular model devoid of both isoforms (COX4i1/2 KO). Subsequent knock-in of COX4i1 or COX4i2 generated cells with exclusive expression of respective isoform. Both isoforms complemented the respiratory defect of COX4i1/2 KO. The content, composition, and incorporation of COX into supercomplexes were comparable in COX4i1- and COX4i2-expressing cells. Also, COX activity, cytochrome affinity, and respiratory rates were undistinguishable in cells expressing either isoform. Analysis of energy metabolism and the redox state in intact cells uncovered modestly increased preference for mitochondrial ATP production, consistent with the increased NADH pool oxidation and lower ROS in COX4i2-expressing cells in normoxia. Most remarkable changes were uncovered in COX oxygen kinetics. The p (partial pressure of oxygen at half-maximal respiration) was increased twofold in COX4i2 versus COX4i1 cells, indicating decreased oxygen affinity of the COX4i2-containing enzyme. Our finding supports the key role of the COX4i2-containing enzyme in hypoxia-sensing pathways of energy metabolism.

摘要

细胞色素氧化酶(COX)通过组织、发育或环境控制亚基同工型的表达进行调节。COX4 亚基被认为根据其同工型 COX4i1 和 COX4i2 的氧控表达来优化呼吸链功能。然而,两种变体的调节生化机制仅部分了解。我们创建了一个基于 HEK293 的敲除细胞模型,该模型缺乏两种同工型(COX4i1/2 KO)。随后敲入 COX4i1 或 COX4i2 生成仅表达各自同工型的细胞。两种同工型均能弥补 COX4i1/2 KO 的呼吸缺陷。COX4i1 和 COX4i2 表达细胞中的 COX 含量、组成和掺入超复合物相当。此外,表达任一同工型的细胞中的 COX 活性、细胞色素亲和力和呼吸速率均无差异。在完整细胞中分析能量代谢和氧化还原状态发现,对线粒体 ATP 生成的偏好略有增加,这与 COX4i2 表达细胞在常氧条件下 NADH 池氧化增加和 ROS 降低一致。最显著的变化是在 COX 氧动力学中发现的。COX4i2 细胞中的 p(呼吸一半时的氧分压)比 COX4i1 细胞增加了两倍,表明 COX4i2 所含酶的氧亲和力降低。我们的发现支持 COX4i2 所含酶在能量代谢缺氧感应途径中的关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ef90/7072730/9bf1d757af33/cells-09-00443-g001.jpg

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