3' Uridylation controls mature microRNA turnover during CD4 T-cell activation

3' 尿苷酸化控制 CD4 T 细胞活化过程中成熟 microRNA 的周转

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作者：Cristina Gutiérrez-Vázquez, Anton J Enright, Ana Rodríguez-Galán, Arantxa Pérez-García, Paul Collier, Matthew R Jones, Vladimir Benes, Joseph P Mizgerd, María Mittelbrunn, Almudena R Ramiro, Francisco Sánchez-Madrid

期刊：	RNA	影响因子：	4.200
时间：	2017	起止号：	2017 Jun;23(6):882-891.
doi：	10.1261/rna.060095.116	研究方向：	细胞生物学
细胞类型：	T细胞

Abstract

Activation of T lymphocytes requires a tight regulation of microRNA (miRNA) expression. Terminal uridyltransferases (TUTases) catalyze 3' nontemplated nucleotide addition (3'NTA) to miRNAs, which may influence miRNA stability and function. Here, we investigated 3'NTA to mature miRNA in CD4 T lymphocytes by deep sequencing. Upon T-cell activation, miRNA sequences bearing terminal uridines are specifically decreased, concomitantly with down-regulation of TUT4 and TUT7 enzymes. Analyzing TUT4-deficient T lymphocytes, we proved that this terminal uridyltransferase is essential for the maintenance of miRNA uridylation in the steady state of T lymphocytes. Analysis of synthetic uridylated miRNAs shows that 3' addition of uridine promotes degradation of these uridylated miRNAs after T-cell activation. Our data underline post-transcriptional uridylation as a mechanism to fine-tune miRNA levels during T-cell activation.

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