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CHIKV infection reprograms codon optimality to favor viral RNA translation by altering the tRNA epitranscriptome.


ABSTRACT: Ample evidence indicates that codon usage bias regulates gene expression. How viruses, such as the emerging mosquito-borne Chikungunya virus (CHIKV), express their genomes at high levels despite an enrichment in rare codons remains a puzzling question. Using ribosome footprinting, we analyze translational changes that occur upon CHIKV infection. We show that CHIKV infection induces codon-specific reprogramming of the host translation machinery to favor the translation of viral RNA genomes over host mRNAs with an otherwise optimal codon usage. This reprogramming was mostly apparent at the endoplasmic reticulum, where CHIKV RNAs show high ribosome occupancy. Mechanistically, it involves CHIKV-induced overexpression of KIAA1456, an enzyme that modifies the wobble U34 position in the anticodon of tRNAs, which is required for proper decoding of codons that are highly enriched in CHIKV RNAs. Our findings demonstrate an unprecedented interplay of viruses with the host tRNA epitranscriptome to adapt the host translation machinery to viral production.

SUBMITTER: Jungfleisch J 

PROVIDER: S-EPMC9366759 | biostudies-literature | 2022 Aug

REPOSITORIES: biostudies-literature

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CHIKV infection reprograms codon optimality to favor viral RNA translation by altering the tRNA epitranscriptome.

Jungfleisch Jennifer J   Böttcher René R   Talló-Parra Marc M   Pérez-Vilaró Gemma G   Merits Andres A   Novoa Eva Maria EM   Díez Juana J  

Nature communications 20220811 1


Ample evidence indicates that codon usage bias regulates gene expression. How viruses, such as the emerging mosquito-borne Chikungunya virus (CHIKV), express their genomes at high levels despite an enrichment in rare codons remains a puzzling question. Using ribosome footprinting, we analyze translational changes that occur upon CHIKV infection. We show that CHIKV infection induces codon-specific reprogramming of the host translation machinery to favor the translation of viral RNA genomes over h  ...[more]

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