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BRCA1 is a novel regulator of metabolic function in skeletal muscle

机译:BRCA1是骨骼肌代谢功能的新型调节剂

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摘要

Breast cancer type 1 (BRCA1) susceptibility protein is expressed across multiple tissues including skeletal muscle. The overall objective of this investigation was to define a functional role for BRCA1 in skeletal muscle using a translational approach. For the first time in both mice and humans, we identified the presence of multiple isoforms of BRCA1 in skeletal muscle. In response to an acute bout of exercise, we found increases in the interaction between the native forms of BRCA1 and the phosphorylated form of acetyl-CoA carboxylase. Decreasing BRCA1 content using a shRNA approach in cultured primary human myotubes resulted in decreased oxygen consumption by the mitochondria and increased reactive oxygen species production. The decreased BRCA1 content also resulted in increased storage of intracellular lipid and reduced insulin signaling. These results indicate that BRCA1 plays a critical role in the regulation of metabolic function in skeletal muscle. Collectively, these data reveal BRCA1 as a novel target to consider in our understanding of metabolic function and risk for development of metabolic-based diseases.
机译:乳腺癌1型(BRCA1)易感蛋白在包括骨骼肌在内的多个组织中表达。这项研究的总体目标是使用翻译方法确定BRCA1在骨骼肌中的功能作用。在小鼠和人类中,我们都首次在骨骼肌中发现了BRCA1的多种同工型。为了应对剧烈运动,我们发现天然形式的BRCA1和磷酸化形式的乙酰辅酶A羧化酶之间的相互作用增加。使用shRNA方法在培养的原代人肌管中降低BRCA1含量会导致线粒体耗氧量减少,并增加活性氧的产生。降低的BRCA1含量还导致细胞内脂质的储存增加和胰岛素信号传导减少。这些结果表明BRCA1在骨骼肌代谢功能的调节中起关键作用。总体而言,这些数据表明BRCA1是我们了解代谢功能和基于代谢疾病的风险的新靶标。

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