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3' Uridylation Confers miRNAs with Non-canonical Target Repertoires.


ABSTRACT: Many microRNAs (miRNAs) exist alongside abundant miRNA isoforms (isomiRs), most of which arise from post-maturation sequence modifications such as 3' uridylation. However, the ways in which these sequence modifications affect miRNA function remain poorly understood. Here, using human miR-27a in cell lines as a model, we discovered that a nonfunctional target site unable to base-pair extensively with the miRNA seed sequence can regain function when an upstream adenosine is able to base-pair with a post-transcriptionally added uridine in the miR-27a tail. This tail-U-mediated repression (TUMR) is abolished in cells lacking the uridylation enzymes TUT4 and TUT7, indicating that uridylation alters miRNA function by modulating target recognition. We identified a set of non-canonical targets in human cells that are specifically regulated by uridylated miR-27a. We provide evidence that TUMR expands the targets of other endogenous miRNAs. Our study reveals a function of uridylated isomiRs in regulating non-canonical miRNA targets.

SUBMITTER: Yang A 

PROVIDER: S-EPMC6688926 | biostudies-literature | 2019 Aug

REPOSITORIES: biostudies-literature

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3' Uridylation Confers miRNAs with Non-canonical Target Repertoires.

Yang Acong A   Bofill-De Ros Xavier X   Shao Tie-Juan TJ   Jiang Minjie M   Li Katherine K   Villanueva Patricia P   Dai Lisheng L   Gu Shuo S  

Molecular cell 20190606 3


Many microRNAs (miRNAs) exist alongside abundant miRNA isoforms (isomiRs), most of which arise from post-maturation sequence modifications such as 3' uridylation. However, the ways in which these sequence modifications affect miRNA function remain poorly understood. Here, using human miR-27a in cell lines as a model, we discovered that a nonfunctional target site unable to base-pair extensively with the miRNA seed sequence can regain function when an upstream adenosine is able to base-pair with  ...[more]

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