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首页> 外文期刊>The Biochemical Journal >Regulation of mitochondrial biogenesis in brown adipose tissue: nuclear respiratory factor-2/GA-binding protein is responsible for the transcriptional regulation of the gene for the mitochondrial ATP synthase beta subunit
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Regulation of mitochondrial biogenesis in brown adipose tissue: nuclear respiratory factor-2/GA-binding protein is responsible for the transcriptional regulation of the gene for the mitochondrial ATP synthase beta subunit

机译:棕色脂肪组织中线粒体生物发生的调控:核呼吸因子2 / GA结合蛋白负责线粒体ATP合酶β亚基基因的转录调控

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The regulation of transcription of the gene for the beta subunit of the FoF1 ATP synthase (ATPsyn beta) in brown adipose tissue has been studied as a model to determine the molecular mechanisms for mitochondrial biogenesis associated with brown adipocyte differentiation. The expression of the ATPsyn beta mRNA is induced during the brown adipocyte differentiation that occurs during murine prenatal development or when brown adipocytes differentiate in culture, This induction occurs in parallel with enhanced gene expression for other nuclear and mitochondrially-encoded components of the respiratory chain/oxidative phosphorylation system (OXPHOS). Transient transfection assays indicated that the expression of the ATPsyn beta gene promoter is higher in differentiated HIB-1B brown adipocytes than in non-differentiated HIB-1B cells. A major transcriptional regulatory site was identified between nt -306 and -266 in the ATPsyn beta promoter. This element has a higher enhancer capacity in differentiated brown adipocyte HIB-1B cells than in non-differentiated cells. Electrophoretic shift analysis indicated that Spland nuclear respiratory factor-2/GA-binding protein (NRF2/GABP) were the main nuclear proteins present in brown adipose tissue that bind this site. Double-point mutant analysis indicated a major role for the NRF2/GABP site in the enhancer capacity of this element in brown fat cells. It is proposed that NRF2/GABP plays a pivotal role in the co-ordinated enhancement of OXPHOS gene expression associated with mitochondrial biogenesis In brown adipocyte differentiation. [References: 46]
机译:已经研究了褐色脂肪组织中FoF1 ATP合酶β亚基的基因转录调控(ATPsyn beta),作为确定与褐色脂肪细胞分化相关的线粒体生物发生的分子机制的模型。 ATPsynβmRNA的表达是在鼠产前发育过程中棕色脂肪细胞分化过程中或培养中棕色脂肪细胞分化过程中诱导的。这种诱导与呼吸链其他核和线粒体编码成分的基因表达增强同时发生。氧化磷酸化系统(OXPHOS)。瞬时转染分析表明,分化的HIB-1B棕色脂肪细胞中ATPsynβ基因启动子的表达高于未分化的HIB-1B细胞。在ATPsyn beta启动子的nt -306和-266之间鉴定出一个主要的转录调控位点。该元素在分化的棕色脂肪细胞HIB-1B细胞中比未分​​化的细胞具有更高的增强能力。电泳迁移分析表明,Spland核呼吸因子2 / GA结合蛋白(NRF2 / GABP)是棕色脂肪组织中结合该位点的主要核蛋白。双点突变分析表明,NRF2 / GABP位点在棕色脂肪细胞中该元素的增强子能力中起主要作用。有人提出,NRF2 / GABP在棕色脂肪细胞分化中与线粒体生物发生有关的OXPHOS基因表达的协同增强中起着关键作用。 [参考:46]

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