HIV-1 Vpu is a potent transcriptional suppressor of NF-κB-elicited antiviral immune responses.
Simon LangerChristian HammerKristina HopfenspergerLukas KleinDominik HotterPaul D De JesusKristina M HerbertLars PacheNikaïa SmithJohannes A van der MerweSumit K ChandaJacques FellayFrank KirchhoffDaniel SauterPublished in: eLife (2019)
Many viral pathogens target innate sensing cascades and/or cellular transcription factors to suppress antiviral immune responses. Here, we show that the accessory viral protein U (Vpu) of HIV-1 exerts broad immunosuppressive effects by inhibiting activation of the transcription factor NF-κB. Global transcriptional profiling of infected CD4 +T cells revealed that vpu-deficient HIV-1 strains induce substantially stronger immune responses than the respective wild type viruses. Gene set enrichment analyses and cytokine arrays showed that Vpu suppresses the expression of NF-κB targets including interferons and restriction factors. Mutational analyses demonstrated that this immunosuppressive activity of Vpu is independent of its ability to counteract the restriction factor and innate sensor tetherin. However, Vpu-mediated inhibition of immune activation required an arginine residue in the cytoplasmic domain that is critical for blocking NF-κB signaling downstream of tetherin. In summary, our findings demonstrate that HIV-1 Vpu potently suppresses NF-κB-elicited antiviral immune responses at the transcriptional level.
Keyphrases
- immune response
- signaling pathway
- transcription factor
- antiretroviral therapy
- hiv positive
- hiv infected
- hiv testing
- lps induced
- human immunodeficiency virus
- pi k akt
- hepatitis c virus
- hiv aids
- nuclear factor
- men who have sex with men
- toll like receptor
- oxidative stress
- dendritic cells
- wild type
- gene expression
- sars cov
- dna binding
- genome wide identification
- inflammatory response
- copy number
- escherichia coli
- gram negative
- heat shock
- genome wide
- amino acid
- small molecule