Cell Host & Microbe
Volume 19, Issue 5, 11 May 2016, Pages 675-685
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Article
Posttranscriptional m6A Editing of HIV-1 mRNAs Enhances Viral Gene Expression

https://doi.org/10.1016/j.chom.2016.04.002Get rights and content
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Highlights

  • The HIV-1 RNA genome is edited by addition of specific m6A residues

  • These m6A residues largely map to viral 3′ UTRs and enhance mRNA expression

  • m6A recruits cellular YTHDF proteins to mRNA transcripts

  • Inhibiting YTHDF binding to m6A inhibits HIV-1 replication

Summary

Covalent addition of a methyl group to adenosine N6 (m6A) is an evolutionarily conserved and common RNA modification that is thought to modulate several aspects of RNA metabolism. While the presence of multiple m6A editing sites on diverse viral RNAs was reported starting almost 40 years ago, how m6A editing affects virus replication has remained unclear. Here, we used photo-crosslinking-assisted m6A sequencing techniques to precisely map several m6A editing sites on the HIV-1 genome and report that they cluster in the HIV-1 3′ untranslated region (3′ UTR). Viral 3′ UTR m6A sites or analogous cellular m6A sites strongly enhanced mRNA expression in cis by recruiting the cellular YTHDF m6A “reader” proteins. Reducing YTHDF expression inhibited, while YTHDF overexpression enhanced, HIV-1 protein and RNA expression, and virus replication in CD4+ T cells. These data identify m6A editing and the resultant recruitment of YTHDF proteins as major positive regulators of HIV-1 mRNA expression.

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