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通过3'非翻译区缩短调控AGR2表达。

Regulation of AGR2 expression via 3'UTR shortening.

作者信息

Matoulkova Eva, Sommerova Lucia, Pastorek Michal, Vojtesek Borivoj, Hrstka Roman

机构信息

Regional Centre for Applied Molecular Oncology, Masaryk Memorial Cancer Institute, Zluty kopec 7, 656 53 Brno, Czechia.

Regional Centre for Applied Molecular Oncology, Masaryk Memorial Cancer Institute, Zluty kopec 7, 656 53 Brno, Czechia.

出版信息

Exp Cell Res. 2017 Jul 1;356(1):40-47. doi: 10.1016/j.yexcr.2017.04.011. Epub 2017 Apr 11.

Abstract

One recently discussed general mechanism affecting gene expression is 3'-untranslated region (3'UTR) length. Events such as shortening, translocation or loss of 3'UTRs are observed within oncogenes and are proposed to associate with increased expression. Thus, increased efforts are being made to understand constitutive and differential transcript 3'end formation. Investigation of AGR2 mRNA revealed a direct impact of its 3'UTR length on AGR2 expression. In silico analyses identified several regulatory sequences within the distal part of AGR2 mRNA that may regulate 3'UTR length and associated protein levels. Short 3'UTRs were observed in a panel of AGR2-positive cancer cell lines and in human breast cancer specimens, in which more extensive 3'UTR shortening correlated with increased AGR2 protein levels. AGR2 is an important member of PI3K/AKT signalling pathway, which along with the proposed involvement of mTOR in the regulation of alternative polyadenylation, prompted us to study the role of mTOR in relation to AGR2 mRNA 3'UTR shortening. A direct impact of mTOR signalling on AGR2 3'UTR shortening associated with increased protein synthesis was found, which led to the identification of a novel molecular mechanism involved in upregulation of AGR2 levels in mTOR-activated cells via modulating the 3'UTR length of AGR2 mRNA.

摘要

一种最近被讨论的影响基因表达的普遍机制是3'非翻译区(3'UTR)的长度。在癌基因中观察到3'UTR缩短、易位或缺失等事件,并推测这些事件与基因表达增加有关。因此,人们正在加大力度了解组成型和差异转录本3'端的形成。对AGR2 mRNA的研究揭示了其3'UTR长度对AGR2表达的直接影响。计算机分析在AGR2 mRNA远端部分鉴定出几个调控序列,这些序列可能调节3'UTR长度及相关蛋白水平。在一组AGR2阳性癌细胞系和人乳腺癌标本中观察到短的3'UTR,其中更广泛的3'UTR缩短与AGR2蛋白水平升高相关。AGR2是PI3K/AKT信号通路的重要成员,鉴于mTOR可能参与替代多聚腺苷酸化的调控,促使我们研究mTOR与AGR2 mRNA 3'UTR缩短的关系。研究发现mTOR信号传导对与蛋白质合成增加相关的AGR2 3'UTR缩短有直接影响,这导致鉴定出一种新的分子机制,该机制通过调节AGR2 mRNA的3'UTR长度参与mTOR激活细胞中AGR2水平的上调。

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