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αCP 聚(C)结合蛋白作为可变多聚腺苷酸化的全局调节剂。

αCP Poly(C) binding proteins act as global regulators of alternative polyadenylation.

机构信息

Department of Genetics, University of Pennsylvania, Philadelphia, Pennsylvania, USA.

出版信息

Mol Cell Biol. 2013 Jul;33(13):2560-73. doi: 10.1128/MCB.01380-12. Epub 2013 Apr 29.

Abstract

We have previously demonstrated that the KH-domain protein αCP binds to a 3' untranslated region (3'UTR) C-rich motif of the nascent human alpha-globin (hα-globin) transcript and enhances the efficiency of 3' processing. Here we assess the genome-wide impact of αCP RNA-protein (RNP) complexes on 3' processing with a specific focus on its role in alternative polyadenylation (APA) site utilization. The major isoforms of αCP were acutely depleted from a human hematopoietic cell line, and the impact on mRNA representation and poly(A) site utilization was determined by direct RNA sequencing (DRS). Bioinformatic analysis revealed 357 significant alterations in poly(A) site utilization that could be specifically linked to the αCP depletion. These APA events correlated strongly with the presence of C-rich sequences in close proximity to the impacted poly(A) addition sites. The most significant linkage was the presence of a C-rich motif within a window 30 to 40 bases 5' to poly(A) signals (AAUAAA) that were repressed upon αCP depletion. This linkage is consistent with a general role for αCPs as enhancers of 3' processing. These findings predict a role for αCPs in posttranscriptional control pathways that can alter the coding potential and/or levels of expression of subsets of mRNAs in the mammalian transcriptome.

摘要

我们之前已经证明,KH 结构域蛋白 αCP 与新生人类α-珠蛋白(hα-globin)转录本的 3'非翻译区(3'UTR)富含 C 的基序结合,并提高了 3'加工的效率。在这里,我们评估了 αCP RNA-蛋白(RNP)复合物对 3'加工的全基因组影响,特别关注其在可变多聚腺苷酸化(APA)位点利用中的作用。主要的 αCP 同工型被急性耗尽人造血细胞系中,通过直接 RNA 测序(DRS)确定其对 mRNA 表达和多聚(A)位点利用的影响。生物信息学分析显示,多聚(A)位点利用有 357 个显著改变,这些改变可以与 αCP 耗竭特异性相关。这些 APA 事件与受影响的多聚(A)添加位点附近紧密接近的富含 C 的序列密切相关。最显著的联系是在距多聚(A)信号(AAUAAA)5'端 30 到 40 个碱基的范围内存在富含 C 的基序,而当 αCP 耗尽时,该基序被抑制。这一联系与 αCP 作为 3'加工增强子的一般作用一致。这些发现预测了 αCP 在转录后控制途径中的作用,这些途径可以改变哺乳动物转录组中部分 mRNA 的编码潜力和/或表达水平。

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