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RNA 结合蛋白 La 的新型 RNA 伴侣结构域受 AKT 磷酸化调控。

Novel RNA chaperone domain of RNA-binding protein La is regulated by AKT phosphorylation.

作者信息

Kuehnert Julia, Sommer Gunhild, Zierk Avery W, Fedarovich Alena, Brock Alexander, Fedarovich Dzmitry, Heise Tilman

机构信息

Department of Biochemistry and Molecular Biology, Medical University of South Carolina, Charleston, SC 29425, USA.

Department of Biochemistry and Molecular Biology, Medical University of South Carolina, Charleston, SC 29425, USA

出版信息

Nucleic Acids Res. 2015 Jan;43(1):581-94. doi: 10.1093/nar/gku1309. Epub 2014 Dec 17.

Abstract

The cellular function of the cancer-associated RNA-binding protein La has been linked to translation of viral and cellular mRNAs. Recently, we have shown that the human La protein stimulates IRES-mediated translation of the cooperative oncogene CCND1 in cervical cancer cells. However, there is little known about the underlying molecular mechanism by which La stimulates CCND1 IRES-mediated translation, and we propose that its RNA chaperone activity is required. Herein, we show that La binds close to the CCND1 start codon and demonstrate that La's RNA chaperone activity can change the folding of its binding site. We map the RNA chaperone domain (RCD) within the C-terminal region of La in close proximity to a novel AKT phosphorylation site (T389). Phosphorylation at T389 by AKT-1 strongly impairs its RNA chaperone activity. Furthermore, we demonstrate that the RCD as well as T389 is required to stimulate CCND1 IRES-mediated translation in cells. In summary, we provide a model whereby a novel interplay between RNA-binding, RNA chaperoning and AKT phosphorylation of La protein regulates CCND1 IRES-mediated translation.

摘要

癌症相关RNA结合蛋白La的细胞功能与病毒和细胞信使核糖核酸(mRNA)的翻译有关。最近,我们发现人类La蛋白能刺激子宫颈癌细胞中协同致癌基因CCND1的内部核糖体进入位点(IRES)介导的翻译。然而,关于La刺激CCND1的IRES介导翻译的潜在分子机制,我们知之甚少,我们推测这需要其RNA伴侣活性。在此,我们表明La与CCND1起始密码子附近结合,并证明La的RNA伴侣活性可改变其结合位点的折叠。我们在La的C端区域内靠近一个新的蛋白激酶B(AKT)磷酸化位点(T389)处定位了RNA伴侣结构域(RCD)。AKT-1对T389的磷酸化强烈损害其RNA伴侣活性。此外,我们证明RCD以及T389是在细胞中刺激CCND1的IRES介导翻译所必需的。总之,我们提供了一个模型,即La蛋白的RNA结合、RNA伴侣活性和AKT磷酸化之间的新型相互作用调节CCND1的IRES介导翻译。

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