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首页> 外文期刊>The Journal of biological chemistry >Fat-specific Protein 27 Inhibits Lipolysis by Facilitating the Inhibitory Effect of Transcription Factor Egr1 on Transcription of Adipose Triglyceride Lipase
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Fat-specific Protein 27 Inhibits Lipolysis by Facilitating the Inhibitory Effect of Transcription Factor Egr1 on Transcription of Adipose Triglyceride Lipase

机译:脂肪特异性蛋白27通过促进转录因子EGR1对脂肪甘油三酯脂肪酶转录的抑制作用来抑制脂解

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摘要

Lipolysis in fat tissue represents a major source of circulating fatty acids. Previously, we have found that lipolysis in adipocytes is controlled by early growth response transcription factor Egr1 that directly inhibits transcription of adipose triglyceride lipase, ATGL (Chakrabarti, P., Kim, J. Y., Singh, M., Shin, Y. K., Kim, J., Kumbrink, J., Wu, Y., Lee, M. J., Kirsch, K. H., Fried, S. K., and Kandror, K. V. (2013) Mol. Cell. Biol. 33, 3659–3666). Here we demonstrate that knockdown of the lipid droplet protein FSP27 (a.k.a. CIDEC) in human adipocytes increases expression of ATGL at the level of transcription, whereas overexpression of FSP27 has the opposite effect. FSP27 suppresses the activity of the ATGL promoter in vitro, and the proximal Egr1 binding site is responsible for this effect. FSP27 co-immunoprecipitates with Egr1 and increases its association with and inhibition of the ATGL promoter. Knockdown of Egr1 attenuates the inhibitory effect of FSP27. These results provide a new model of transcriptional regulation of ATGL.
机译:脂肪组织中的脂肪分解代表循环脂肪酸的主要来源。以前,我们发现脂肪细胞中的脂解是由早期生长反应转录因子EGR1控制,即直接抑制脂肪甘油三酯脂肪酶,ATG1(Chakrabarti,P.,Kim,Jy,Singh,M.,Shin,YK,Kim,J 。,Kumbrink,J.,Wu,Y.,Lee,MJ,Kirsch,Kh,炒,SK和Kandror,KV(2013)Mol。细胞。Biol.33,3659-3666)。在这里,我们证明人类脂肪细胞中脂液滴蛋白FSP27(A.K.A.CIDEC)的敲低增加了ATGL在转录水平上的表达,而FSP27的过度表达具有相反的效果。 FSP27在体外抑制ATGL启动子的活性,近端EGR1结合位点对此效果负责。 FSP27用EGR1共免疫沉淀并增加其与ATGL启动子的关系和抑制。 EGR1的敲低衰减FSP27的抑制作用。这些结果提供了ATGL的新转录调节模型。

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