信使核糖核酸
核糖核酸
五素未翻译区
细胞生物学
RNA结合蛋白
基因
遗传学
RNA剪接
翻译(生物学)
平动调节
抄写(语言学)
劈理(地质)
基因表达调控
小RNA
真核翻译
转录后修饰
转录后调控
基因表达
作者
Georges Martín,Andreas Gruber,Walter Keller,Mihaela Zavolan
出处
期刊:Cell Reports
[Elsevier]
日期:2012-06-01
卷期号:1 (6): 753-763
被引量:318
标识
DOI:10.1016/j.celrep.2012.05.003
摘要
Through alternative polyadenylation, human mRNAs acquire longer or shorter 3' untranslated regions, the latter typically associated with higher transcript stability and increased protein production. To understand the dynamics of polyadenylation site usage, we performed transcriptome-wide mapping of both binding sites of 3' end processing factors CPSF-160, CPSF-100, CPSF-73, CPSF-30, Fip1, CstF-64, CstF-64τ, CF I(m)25, CF I(m)59, and CF I(m)68 and 3' end processing sites in HEK293 cells. We found that although binding sites of these factors generally cluster around the poly(A) sites most frequently used in cleavage, CstF-64/CstF-64τ and CFI(m) proteins have much higher positional specificity compared to CPSF components. Knockdown of CF I(m)68 induced a systematic use of proximal polyadenylation sites, indicating that changes in relative abundance of a single 3' end processing factor can modulate the length of 3' untranslated regions across the transcriptome and suggesting a mechanism behind the previously observed increase in tumor cell invasiveness upon CF I(m)68 knockdown.
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