Natural mutations in IFITM3 modulate post‐translational regulation and toggle antiviral specificity |
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| Authors: | Alex A Compton Nicolas Roy Françoise Porrot Anne Billet Nicoletta Casartelli Jacob S Yount Chen Liang Olivier Schwartz |
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| Institution: | 1. Virus & Immunity Unit, Institut Pasteur, Paris, France;2. Department of Microbial Infection & Immunity, The Ohio State University, Columbus, OH, USA;3. Lady Davis Institute, McGill University, Montreal, QC, Canada;4. CNRS‐URA 3015, Paris, France;5. Vaccine Research Institute, Creteil, France |
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| Abstract: | The interferon‐induced transmembrane (IFITM) proteins protect host cells from diverse virus infections. IFITM proteins also incorporate into HIV‐1 virions and inhibit virus fusion and cell‐to‐cell spread, with IFITM3 showing the greatest potency. Here, we report that amino‐terminal mutants of IFITM3 preventing ubiquitination and endocytosis are more abundantly incorporated into virions and exhibit enhanced inhibition of HIV‐1 fusion. An analysis of primate genomes revealed that IFITM3 is the most ancient antiviral family member of the IFITM locus and has undergone a repeated duplication in independent host lineages. Some IFITM3 genes in nonhuman primates, including those that arose following gene duplication, carry amino‐terminal mutations that modify protein localization and function. This suggests that “runaway” IFITM3 variants could be selected for altered antiviral activity. Furthermore, we show that adaptations in IFITM3 result in a trade‐off in antiviral specificity, as variants exhibiting enhanced activity against HIV‐1 poorly restrict influenza A virus. Overall, we provide the first experimental evidence that diversification of IFITM3 genes may boost the antiviral coverage of host cells and provide selective functional advantages. |
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| Keywords: | evolution HIV IFITM innate immunity virus |
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