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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Mitochondrial ABC transporters function: The role of ABCB10 (ABC-me) as a novel player in cellular handling of reactive oxygen species
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Mitochondrial ABC transporters function: The role of ABCB10 (ABC-me) as a novel player in cellular handling of reactive oxygen species

机译:线粒体ABC转运蛋白的功能:ABCB10(ABC-me)在细胞处理活性氧中的作用

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摘要

Mitochondria are one of the major sources of reactive oxygen species (ROS) in the cell. When exceeding the capacity of antioxidant mechanisms, ROS production may lead to different pathologies, such as ischemia-reperfusion injury, neurodegeneration, anemia and ageing. As a consequence of the endosymbiotic origin of mitochondria, eukaryotic cells have developed different transport mechanisms that coordinate mitochondrial function with other cellular compartments. Four mitochondrial ATP-binding cassette (ABC) transporters have been described to date in mammals: ABCB6, ABCB8, ABCB7 and ABCB10. ABCB10 is located in the inner mitochondrial membrane forming homodimers, with the ATP binding domain facing the mitochondrial matrix. ABCB10 expression is highly induced during erythroid differentiation and its overexpression increases hemoglobin synthesis in erythroid cells. However, ABCB10 is also expressed in nonerythroid tissues, suggesting a role not directly related to hemoglobin synthesis. Recent evidence points toward ABCB10 as an important player in the protection from oxidative stress in mammals. In this regard, ABCB10 is required for normal erythropoiesis and cardiac recovery after ischemia-reperfusion, processes intimately related to mitochondrial ROS generation. Here, we review the current knowledge on mitochondrial ABC transporters and ABCB10 and discuss the potential mechanisms by which ABCB10 and its transport activity may regulate oxidative stress. We discuss ABCB10 as a potential therapeutic target for diseases in which increased mitochondrial ROS production and oxidative stress play a major role.
机译:线粒体是细胞中活性氧(ROS)的主要来源之一。当超过抗氧化剂机制的能力时,ROS的产生可能导致不同的病理,例如缺血再灌注损伤,神经变性,贫血和衰老。作为线粒体内共生起源的结果,真核细胞已发展出不同的转运机制,可协调线粒体功能与其他细胞区室。迄今为止,已经在哺乳动物中描述了四种线粒体ATP结合盒(ABC)转运蛋白:ABCB6,ABCB8,ABCB7和ABCB10。 ABCB10位于线粒体内膜上,形成同型二聚体,ATP结合域面向线粒体基质。 ABCB10表达在红系分化过程中被高度诱导,其过表达增加了红系细胞中血红蛋白的合成。但是,ABCB10也可在非红系组织中表达,提示其作用与血红蛋白合成没有直接关系。最近的证据表明,ABCB10是保护哺乳动物免受氧化应激的重要因素。在这方面,缺血再灌注后正常的红细胞生成和心脏恢复需要ABCB10,这与线粒体ROS的产生密切相关。在这里,我们审查有关线粒体ABC转运蛋白和ABCB10的当前知识,并讨论ABCB10及其转运活性可能调节氧化应激的潜在机制。我们讨论ABCB10作为疾病的潜在治疗靶点,其中线粒体ROS产生增加和氧化应激起主要作用。

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