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首页> 外文期刊>Nucleic acids research >Twist2, a novel ADD1/SREBP1c interacting protein, represses the transcriptional activity of ADD1/SREBP1c
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Twist2, a novel ADD1/SREBP1c interacting protein, represses the transcriptional activity of ADD1/SREBP1c

机译:Twist2是一种新型ADD1 / SREBP1c相互作用蛋白,可抑制ADD1 / SREBP1c的转录活性

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Adipocyte determination and differentiation dependent factor 1 (ADD1)/sterol regulatory element binding protein isoform (SREBP1c) is a key transcription factor in fatty acid metabolism and insulin‐ dependent gene expression. Although its transcriptional and post‐translational regulation has been extensively studied, its regulation by interacting proteins is not well understood. To identify cellular proteins that associate with ADD1/SREBP1c, we employed the yeast two‐hybrid system with an adipocyte cDNA library. Using the N‐terminal domain of ADD1/SREBP1c as bait, we identified Twist2 (also known as Dermo‐1), a basic helix–loop–helix (bHLH) protein, as a novel ADD1/SREBP1c interacting protein. Over‐expression of Twist2 strongly repressed the transcriptional activity of ADD1/SREBP1c, primarily by reducing its binding to target sequences. Inhibition of histone deacetylase (HDAC) activity with HDAC inhibitors relieved this repression. Our data suggest that physical interaction between Twist2 and ADD1/SREBP1c attenuates transcriptional activation by ADD1/SREBP1c by inhibiting its binding to DNA, and that this inhibition is at least partly dependent on chromatin modification by HDACs.
机译:脂肪细胞的确定和分化依赖性因子1(ADD1)/固醇调节元件结合蛋白同工型(SREBP1c)是脂肪酸代谢和胰岛素依赖性基因表达的关键转录因子。尽管已经对其转录和翻译后调控进行了广泛研究,但对与蛋白质相互作用的调控却知之甚少。为了鉴定与ADD1 / SREBP1c相关的细胞蛋白,我们采用了带有脂肪细胞cDNA文库的酵母双杂交系统。使用ADD1 / SREBP1c的N末端结构域作为诱饵,我们将基本的螺旋-环-螺旋(bHLH)蛋白Twist2(也称为Dermo-1)识别为一种新型的ADD1 / SREBP1c相互作用蛋白。 Twist2的过表达强烈抑制了ADD1 / SREBP1c的转录活性,主要是通过减少其与靶序列的结合来实现的。用HDAC抑制剂抑制组蛋白脱乙酰基酶(HDAC)活性可缓解这种抑制作用。我们的数据表明Twist2和ADD1 / SREBP1c之间的物理相互作用通过抑制ADD1 / SREBP1c与DNA的结合而减弱了ADD1 / SREBP1c的转录激活,并且这种抑制作用至少部分取决于HDAC对染色质的修饰。

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