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Viral miRNA adaptor differentially recruits miRNAs to target mRNAs through alternative base-pairing.


ABSTRACT: HSUR2 is a viral non-coding RNA (ncRNA) that functions as a microRNA (miRNA) adaptor. HSUR2 inhibits apoptosis in infected cells by recruiting host miRNAs miR-142-3p and miR-16 to mRNAs encoding apoptotic factors. HSUR2's target recognition mechanism is not understood. It is also unknown why HSUR2 utilizes miR-16 to downregulate only a subset of transcripts. We developed a general method for individual-nucleotide resolution RNA-RNA interaction identification by crosslinking and capture (iRICC) to identify sequences mediating interactions between HSUR2 and target mRNAs in vivo. Mutational analyses confirmed identified HSUR2-mRNA interactions and validated iRICC as a method that confidently determines sequences mediating RNA-RNA interactions in vivo. We show that HSUR2 does not display a 'seed' region to base-pair with most target mRNAs, but instead uses different regions to interact with different transcripts. We further demonstrate that this versatile mode of interaction via variable base-pairing provides HSUR2 with a mechanism for differential miRNA recruitment.

SUBMITTER: Gorbea C 

PROVIDER: S-EPMC6763288 | biostudies-literature | 2019 Sep

REPOSITORIES: biostudies-literature

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Viral miRNA adaptor differentially recruits miRNAs to target mRNAs through alternative base-pairing.

Gorbea Carlos C   Mosbruger Tim T   Nix David A DA   Cazalla Demián D  

eLife 20190920


HSUR2 is a viral non-coding RNA (ncRNA) that functions as a microRNA (miRNA) adaptor. HSUR2 inhibits apoptosis in infected cells by recruiting host miRNAs miR-142-3p and miR-16 to mRNAs encoding apoptotic factors. HSUR2's target recognition mechanism is not understood. It is also unknown why HSUR2 utilizes miR-16 to downregulate only a subset of transcripts. We developed a general method for <i>i</i>ndividual-nucleotide resolution <i>R</i>NA-RNA <i>i</i>nteraction identification by <i>c</i>rossl  ...[more]

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