| Literature DB >> 25981045 |
Joshua R Kane1, David J Stanley2, Judd F Hultquist3, Jeffrey R Johnson1, Nicole Mietrach4, Jennifer M Binning2, Stefán R Jónsson4, Sarah Barelier2, Billy W Newton1, Tasha L Johnson1, Kathleen E Franks-Skiba5, Ming Li6, William L Brown6, Hörður I Gunnarsson4, Adalbjorg Adalbjornsdóttir4, James S Fraser7, Reuben S Harris6, Valgerður Andrésdóttir4, John D Gross8, Nevan J Krogan9.
Abstract
HIV-1 encodes the accessory protein Vif, which hijacks a host Cullin-RING ubiquitin ligase (CRL) complex as well as the non-canonical cofactor CBFβ, to antagonize APOBEC3 antiviral proteins. Non-canonical cofactor recruitment to CRL complexes by viral factors, to date, has only been attributed to HIV-1 Vif. To further study this phenomenon, we employed a comparative approach combining proteomic, biochemical, structural, and virological techniques to investigate Vif complexes across the lentivirus genus, including primate (HIV-1 and simian immunodeficiency virus macaque [SIVmac]) and non-primate (FIV, BIV, and MVV) viruses. We find that CBFβ is completely dispensable for the activity of non-primate lentiviral Vif proteins. Furthermore, we find that BIV Vif requires no cofactor and that MVV Vif requires a novel cofactor, cyclophilin A (CYPA), for stable CRL complex formation and anti-APOBEC3 activity. We propose modular conservation of Vif complexes allows for potential exaptation of functions through the acquisition of non-CRL-associated host cofactors while preserving anti-APOBEC3 activity.Entities:
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Year: 2015 PMID: 25981045 PMCID: PMC4613747 DOI: 10.1016/j.celrep.2015.04.038
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423