Non-AUG HIV-1 uORF translation elicits specific T cell immune response and regulates viral transcript expression

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Labaronne, Emmanuel | Décimo, Didier | Bertrand, Lisa | Guiguettaz, Laura | Sohier, Thibault | Cluet, David | Vivet‐boudou, Valérie | Chaves Valadão, Ana Luiza | Dahoui, Clara | François, Pauline | Hatin, Isabelle | Lambotte, Olivier | Samri, Assia | Autran, Brigitte | Etienne, Lucie | Goujon, Caroline | Paillart, Jean-Christophe | Namy, Olivier | Ramirez, Bertha Cecilia | Ohlmann, Théophile | Moris, Arnaud | Ricci, Emiliano

Edité par CCSD ; Nature Publishing Group -

International audience. Human immunodeficiency virus type-1 (HIV-1) is a complex retrovirus that relies on alternative splicing, translational, and post-translational mechanisms to produce over 15 functional proteins from its single ~10 kb transcriptional unit. Using ribosome profiling, nascent protein labeling, RNA sequencing, and whole-proteomics of infected CD4 + T lymphocytes, we characterized the transcriptional, translational, and post-translational landscape during infection. While viral infection exerts a significant impact on host transcript abundance, global translation rates are only modestly affected. Proteomics data reveal extensive transcriptional and post-translational regulation, with many genes showing opposing trends between transcript/ribosome profiling and protein abundance. These findings highlight a complex regulatory network orchestrating gene expression at multiple levels. Viral ribosome profiling further uncovered extensive non-AUG translation of small peptides from upstream open reading frames (uORFs) within the 5’ long terminal repeat, which elicit specific T cell responses in people living with HIV. Conservation of uORF translation among retroviruses, along with TAR sequences, shapes DDX3 dependency for efficient translation of the main viral open reading frames.

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