Evolutionary Paradigms from Ancient and Ongoing Conflicts between the Lentiviral Vif Protein and Mammalian APOBEC3 Enzymes

Lentiviruses are a unique class of retroviruses that infect a subset of mammalian species, including humans. Human immunodeficiency virus type 1 and 2 (HIV-1 and HIV-2), simian immunodeficiency virus (SIV), feline immunodeficiency virus (FIV), bovine immunodeficiency virus (BIV), maedi-visna virus (MVV), and caprine arthritis encephalitis virus (CAEV) infections result in immunodeficiency syndromes, neurological diseases, and other conditions. Disease is chronic, lifelong, and often fatal. Pathology is due in part to a capacity to immortalize by integrating into a host’s genomic DNA and a remarkable genetic plasticity that enables escape from potent adaptive immune responses without compromising vital viral functions. Lentiviruses encode three universal retroviral proteins (Gag, Pol, and Env), one lentivirus-specific protein called Vif (virus infectivity factor), and a handful of other less conserved accessory factors. Vif is required to protect lentiviruses from restriction by several members of the APOBEC3 family of DNA cytosine deaminases by forming a cellular polyubiquitin ligase complex to degrade these enzymes (Fig 1A). Viruses lacking Vif are inactivated because cytoplasmic APOBEC3 enzymes remain abundant, package into assembling virus particles, and prevent the production of a viable DNA copy of the viruses’ RNA genome by catalyzing the deamination of viral cDNA cytosines to uracils. Viral DNA genomes that make it through this gauntlet are rendered nonfunctional by the resulting guanine to adenine hypermutations (cDNA uracils template the insertion of genomic strand adenines that become immortalized as G-to-A mutations). In this Pearl, we review recent progress in understanding the Vif-APOBEC3 interaction and discuss a model that provides a molecular explanation for past zoonotic transmission events as well as present-day, likely ongoing optimizations that enable lentiviruses to thrive.