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甾体激素生成急性调节蛋白(StAR)的活性需要位于线粒体的激酶级联反应的激素激活。

Hormonal activation of a kinase cascade localized at the mitochondria is required for StAR protein activity.

作者信息

Poderoso Cecilia, Maloberti Paula, Duarte Alejandra, Neuman Isabel, Paz Cristina, Cornejo Maciel Fabiana, Podesta Ernesto J

机构信息

Instituto de Investigaciones Moleculares de Enfermedades Hormonales, Neurodegenerativas y Oncológicas (IIMHNO), Department of Biochemistry, School of Medicine, University of Buenos Aires, Paraguay 2155, 5th, C1121ABG Buenos Aires, Argentina.

出版信息

Mol Cell Endocrinol. 2009 Mar 5;300(1-2):37-42. doi: 10.1016/j.mce.2008.10.009. Epub 2008 Oct 19.

Abstract

It is known that ERK1/2 and MEK1/2 participate in the regulation of Star gene transcription. However, their role in StAR protein post-transcriptional regulation is not described yet. In this study we analyzed the relationship between the MAPK cascade and StAR protein phosphorylation and function. We have demonstrated that (a) steroidogenesis in MA-10 Leydig cells depends on the specific of ERK1/2 activation at the mitochondria; (b) ERK1/2 phosphorylation is driven by mitochondrial PKA and constitutive MEK1/2 in this organelle; (c) active ERK1/2 interacts with StAR protein, leads to StAR protein phosphorylation at Ser(232) only in the presence of cholesterol; (d) directed mutagenesis of Ser(232) (S232A) inhibited in vitro StAR protein phosphorylation by ERK1; (e) transient transfection of MA-10 cells with StAR S232A cDNA markedly reduced the yield of progesterone production. We show that StAR protein is a substrate of ERK1/2, and that mitochondrial ERK1/2 is part of a multimeric complex that regulates cholesterol transport.

摘要

已知ERK1/2和MEK1/2参与星状基因转录的调控。然而,它们在类固醇生成急性调节蛋白(StAR)蛋白转录后调控中的作用尚未见报道。在本研究中,我们分析了丝裂原活化蛋白激酶(MAPK)级联反应与StAR蛋白磷酸化及功能之间的关系。我们已经证明:(a)MA-10睾丸间质细胞中的类固醇生成取决于线粒体中ERK1/2激活的特异性;(b)ERK1/2磷酸化由该细胞器中的线粒体蛋白激酶A(PKA)和组成型MEK1/2驱动;(c)活性ERK1/2与StAR蛋白相互作用,仅在胆固醇存在的情况下导致StAR蛋白在Ser(232)位点磷酸化;(d)Ser(232)(S232A)的定向诱变抑制了ERK1对体外StAR蛋白的磷酸化;(e)用StAR S232A cDNA瞬时转染MA-10细胞显著降低了孕酮的产量。我们表明,StAR蛋白是ERK1/2的底物,并且线粒体ERK1/2是调节胆固醇转运的多聚体复合物的一部分。

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