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新型生长相关RNA解旋酶DDX39的细胞内特性分析

Intracellular characterization of DDX39, a novel growth-associated RNA helicase.

作者信息

Sugiura Takeyuki, Sakurai Kayo, Nagano Yuki

机构信息

Discovery Research Laboratory, Tokyo R&D Center, Daiichi Pharmaceutical Co. Ltd., 16-13, Kitakasai 1-Chome, Edogawa-ku, Tokyo 134-8630, Japan.

出版信息

Exp Cell Res. 2007 Feb 15;313(4):782-90. doi: 10.1016/j.yexcr.2006.11.014. Epub 2006 Dec 5.

Abstract

DDX39 belongs to the DEAD box RNA helicase family and is overexpressed in human lung squamous cell carcinoma. In this study, in order to seek the biological relevance of DDX39, we conducted its intracellular characterization. When expressed in 293 cells, DDX39 undergoes heavy ubiquitylation and the stability of DDX39 is regulated via a ubiqutin-proteasome pathway. DDX39 tethers ALY, an essential mRNA export factor, in vivo, confirming the role of DDX39 in the RNA splicing/export process. Co-immunoprecipitation and mass spectrometry analyses detected CIP29, a recently discovered growth and cell cycle-related factor, as a main DDX39-interacting protein. CIP29 binds RNA on its own and enhances RNA unwinding activity of DDX39. Thus, CIP29 physically and functionally associates with DDX39, suggesting their cooperation in the RNA metabolism. Extension of the search for the protein-protein interactions encompassing DDX39 identified FUS/TLS, a nucleic acid binding protein participating in both transcription and splicing, as a CIP29-interacting protein. The connections comprising ALY, DDX39, CIP29 and FUS/TLS may be an integral part of transcription, splicing and RNA export. We simultaneously examined the properties of DDX39-S, a C-terminally truncated variant of DDX39 stemmed from alternative splicing, to understand its biological significance.

摘要

DDX39属于DEAD盒RNA解旋酶家族,在人肺鳞状细胞癌中过表达。在本研究中,为了探寻DDX39的生物学相关性,我们对其进行了细胞内特性分析。当在293细胞中表达时,DDX39会发生大量泛素化,并且DDX39的稳定性通过泛素-蛋白酶体途径进行调节。DDX39在体内与一种重要的mRNA输出因子ALY结合,证实了DDX39在RNA剪接/输出过程中的作用。免疫共沉淀和质谱分析检测到CIP29(一种最近发现的与生长和细胞周期相关的因子)是与DDX39相互作用的主要蛋白。CIP29自身能结合RNA,并增强DDX39的RNA解旋活性。因此,CIP29在物理和功能上与DDX39相关联,表明它们在RNA代谢中存在合作。对包含DDX39的蛋白质-蛋白质相互作用的进一步研究确定FUS/TLS(一种参与转录和剪接的核酸结合蛋白)是与CIP29相互作用的蛋白。由ALY、DDX39、CIP29和FUS/TLS组成的联系可能是转录、剪接和RNA输出的一个整体部分。我们同时研究了DDX39-S(一种由可变剪接产生的DDX39的C末端截短变体)的特性,以了解其生物学意义。

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