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Eur J Appl Physiol. 2014 Feb;114(2):405-17. doi: 10.1007/s00421-013-2783-8. Epub 2013 Dec 11.
2
Oxygen-dependent expression of cytochrome c oxidase subunit 4-2 gene expression is mediated by transcription factors RBPJ, CXXC5 and CHCHD2.氧依赖型细胞色素 c 氧化酶亚基 4-2 基因表达的调控是由转录因子 RBPJ、CXXC5 和 CHCHD2 介导的。
Nucleic Acids Res. 2013 Feb 1;41(4):2255-66. doi: 10.1093/nar/gks1454. Epub 2013 Jan 8.
3
Cytochrome c oxidase subunit 4 isoform 2-knockout mice show reduced enzyme activity, airway hyporeactivity, and lung pathology.细胞色素 c 氧化酶亚基 4 同工型 2 敲除小鼠表现出酶活性降低、气道反应性降低和肺部病理学改变。
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Transcriptional regulation of temperature-induced remodeling of muscle bioenergetics in goldfish.金鱼中温度诱导的肌肉生物能量重塑的转录调控
Am J Physiol Regul Integr Comp Physiol. 2012 Jul 15;303(2):R150-8. doi: 10.1152/ajpregu.00603.2011. Epub 2012 May 23.
5
Multiple phosphorylations of cytochrome c oxidase and their functions.细胞色素c氧化酶的多重磷酸化及其功能。
Proteomics. 2012 Apr;12(7):950-9. doi: 10.1002/pmic.201100618.
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The power of life--cytochrome c oxidase takes center stage in metabolic control, cell signalling and survival.生命的力量——细胞色素 c 氧化酶在代谢控制、细胞信号转导和存活中占据中心舞台。
Mitochondrion. 2012 Jan;12(1):46-56. doi: 10.1016/j.mito.2011.05.003. Epub 2011 May 26.
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Origins of interspecies variation in mammalian muscle metabolic enzymes.哺乳动物肌肉代谢酶种间变异的起源。
Physiol Genomics. 2011 Jul 27;43(14):873-83. doi: 10.1152/physiolgenomics.00025.2011. Epub 2011 May 17.
8
Coordination of cytochrome c oxidase gene expression in the remodelling of skeletal muscle.细胞色素 c 氧化酶基因表达在骨骼肌重塑中的协调作用。
J Exp Biol. 2011 Jun 1;214(Pt 11):1880-7. doi: 10.1242/jeb.053322.
9
Moderate and high intensity sprint exercise induce differential responses in COX4I2 and PDK4 gene expression in Thoroughbred horse skeletal muscle.中等强度和高强度冲刺运动对纯种马骨骼肌中COX4I2和PDK4基因表达产生不同反应。
Equine Vet J Suppl. 2010 Nov(38):576-81. doi: 10.1111/j.2042-3306.2010.00206.x.
10
Transcription factor binding variation in the evolution of gene regulation.转录因子结合变异在基因调控进化中的作用。
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细胞色素c氧化酶亚基4的氧敏感性演变

Evolution of the oxygen sensitivity of cytochrome c oxidase subunit 4.

作者信息

Kocha K M, Reilly K, Porplycia D S M, McDonald J, Snider T, Moyes C D

机构信息

Department of Biology, Queen's University, Kingston, Ontario, Canada.

Department of Biology, Queen's University, Kingston, Ontario, Canada

出版信息

Am J Physiol Regul Integr Comp Physiol. 2015 Feb 15;308(4):R305-20. doi: 10.1152/ajpregu.00281.2014. Epub 2014 Dec 17.

DOI:10.1152/ajpregu.00281.2014
PMID:25519729
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4329467/
Abstract

Vertebrates possess two paralogs of cytochrome c oxidase (COX) subunit 4: a ubiquitous COX4-1 and a hypoxia-linked COX4-2. Mammalian COX4-2 is thought to have a role in relation to fine-tuning metabolism in low oxygen levels, conferred through both structural differences in the subunit protein structure and regulatory differences in the gene. We sought to elucidate the pervasiveness of this feature across vertebrates. The ratio of COX4-2/4-1 mRNA is generally low in mammals, but this ratio was higher in fish and reptiles, particularly turtles. The COX4-2 gene appeared unresponsive to low oxygen in nonmammalian models (zebrafish, goldfish, tilapia, anoles, and turtles) and fish cell lines. Reporter genes constructed from the amphibian and reptile homologues of the mammalian oxygen-responsive elements and hypoxia-responsive elements did not respond to low oxygen. Unlike the rodent ortholog, the promoter of goldfish COX4-2 did not respond to hypoxia or anoxia. The protein sequences of the COX4-2 peptide showed that the disulfide bridge seen in human and rodent orthologs would be precluded in other mammalian lineages and lower vertebrates, all of which lack the requisite pair of cysteines. The coordinating ligands of the ATP-binding site are largely conserved across mammals and reptiles, but in Xenopus and fish, sequence variations may disrupt the ability of the protein to bind ATP at this site. Collectively, these results suggest that many of the genetic and structural features of COX4-2 that impart responsiveness and benefits in hypoxia may be restricted to the Euarchontoglires lineage that includes primates, lagomorphs, and rodents.

摘要

脊椎动物拥有细胞色素c氧化酶(COX)亚基4的两个旁系同源物:普遍存在的COX4-1和与缺氧相关的COX4-2。哺乳动物的COX4-2被认为在低氧水平下对代谢的微调中发挥作用,这是通过亚基蛋白质结构的差异和基因调控的差异实现的。我们试图阐明这一特征在脊椎动物中的普遍性。COX4-2/4-1 mRNA的比例在哺乳动物中通常较低,但在鱼类和爬行动物中,尤其是海龟中,这一比例较高。在非哺乳动物模型(斑马鱼、金鱼、罗非鱼、安乐蜥和海龟)和鱼类细胞系中,COX4-2基因似乎对低氧无反应。由哺乳动物氧反应元件和缺氧反应元件的两栖动物和爬行动物同源物构建的报告基因对低氧无反应。与啮齿动物的直系同源物不同,金鱼COX4-2的启动子对缺氧或无氧无反应。COX4-2肽的蛋白质序列表明,在人类和啮齿动物直系同源物中看到的二硫键在其他哺乳动物谱系和低等脊椎动物中不存在,因为它们都缺乏必需的一对半胱氨酸。ATP结合位点的配位配体在哺乳动物和爬行动物中基本保守,但在非洲爪蟾和鱼类中,序列变异可能会破坏蛋白质在该位点结合ATP的能力。总的来说,这些结果表明,COX4-2的许多赋予缺氧反应性和益处的遗传和结构特征可能仅限于包括灵长类动物、兔形目动物和啮齿动物在内的真灵长大目谱系。