APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome

APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome

APOBEC3G (A3G) is a host enzyme that mutates the genomes of retroviruses like HIV. Since A3G is expressed pre-infection, it has classically been considered an agent of innate immunity. We and others previously showed that the impact of A3G-induced mutations on the HIV genome extends to adaptive immu...

Full description

Bibliographic Details
Main Authors: Faezeh Borzooee, Krista D. Joris, Michael D. Grant, Mani Larijani
Format: Article
Language:English
Published: Frontiers Media S.A. 2019-01-01
Series:Frontiers in Immunology
Subjects:
CTL epitope
APOBEC3G (A3G)
HIV
immune escape
viral evolution
Online Access:https://www.frontiersin.org/article/10.3389/fimmu.2018.03032/full
id doaj-a62c3e9fce5144838e1eb28e3d4d3bb0
record_format Article
spelling doaj-a62c3e9fce5144838e1eb28e3d4d3bb02020-11-24T22:23:01ZengFrontiers Media S.A.Frontiers in Immunology1664-32242019-01-01910.3389/fimmu.2018.03032414089APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV GenomeFaezeh BorzooeeKrista D. JorisMichael D. GrantMani LarijaniAPOBEC3G (A3G) is a host enzyme that mutates the genomes of retroviruses like HIV. Since A3G is expressed pre-infection, it has classically been considered an agent of innate immunity. We and others previously showed that the impact of A3G-induced mutations on the HIV genome extends to adaptive immunity also, by generating cytotoxic T cell (CTL) escape mutations. Accordingly, HIV genomic sequences encoding CTL epitopes often contain A3G-mutable “hotspot” sequence motifs, presumably to channel A3G action toward CTL escape. Here, we studied the depths and consequences of this apparent viral genome co-evolution with A3G. We identified all potential CTL epitopes in Gag, Pol, Env, and Nef restricted to several HLA class I alleles. We simulated A3G-induced mutations within CTL epitope-encoding sequences, and flanking regions. From the immune recognition perspective, we analyzed how A3G-driven mutations are predicted to impact CTL-epitope generation through modulating proteasomal processing and HLA class I binding. We found that A3G mutations were most often predicted to result in diminishing/abolishing HLA-binding affinity of peptide epitopes. From the viral genome evolution perspective, we evaluated enrichment of A3G hotspots at sequences encoding CTL epitopes and included control sequences in which the HIV genome was randomly shuffled. We found that sequences encoding immunogenic epitopes exhibited a selective enrichment of A3G hotspots, which were strongly biased to translate to non-synonymous amino acid substitutions. When superimposed on the known mutational gradient across the entire length of the HIV genome, we observed a gradient of A3G hotspot enrichment, and an HLA-specific pattern of the potential of A3G hotspots to lead to CTL escape mutations. These data illuminate the depths and extent of the co-evolution of the viral genome to subvert the host mutator A3G.https://www.frontiersin.org/article/10.3389/fimmu.2018.03032/fullCTL epitopeAPOBEC3G (A3G)HIVimmune escapeviral evolution
collection DOAJ
language English
format Article
sources DOAJ
author Faezeh Borzooee
Krista D. Joris
Michael D. Grant
Mani Larijani
spellingShingle Faezeh Borzooee
Krista D. Joris
Michael D. Grant
Mani Larijani
APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome
Frontiers in Immunology
CTL epitope
APOBEC3G (A3G)
HIV
immune escape
viral evolution
author_facet Faezeh Borzooee
Krista D. Joris
Michael D. Grant
Mani Larijani
author_sort Faezeh Borzooee
title APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome
title_short APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome
title_full APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome
title_fullStr APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome
title_full_unstemmed APOBEC3G Regulation of the Evolutionary Race Between Adaptive Immunity and Viral Immune Escape Is Deeply Imprinted in the HIV Genome
title_sort apobec3g regulation of the evolutionary race between adaptive immunity and viral immune escape is deeply imprinted in the hiv genome
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2019-01-01
description APOBEC3G (A3G) is a host enzyme that mutates the genomes of retroviruses like HIV. Since A3G is expressed pre-infection, it has classically been considered an agent of innate immunity. We and others previously showed that the impact of A3G-induced mutations on the HIV genome extends to adaptive immunity also, by generating cytotoxic T cell (CTL) escape mutations. Accordingly, HIV genomic sequences encoding CTL epitopes often contain A3G-mutable “hotspot” sequence motifs, presumably to channel A3G action toward CTL escape. Here, we studied the depths and consequences of this apparent viral genome co-evolution with A3G. We identified all potential CTL epitopes in Gag, Pol, Env, and Nef restricted to several HLA class I alleles. We simulated A3G-induced mutations within CTL epitope-encoding sequences, and flanking regions. From the immune recognition perspective, we analyzed how A3G-driven mutations are predicted to impact CTL-epitope generation through modulating proteasomal processing and HLA class I binding. We found that A3G mutations were most often predicted to result in diminishing/abolishing HLA-binding affinity of peptide epitopes. From the viral genome evolution perspective, we evaluated enrichment of A3G hotspots at sequences encoding CTL epitopes and included control sequences in which the HIV genome was randomly shuffled. We found that sequences encoding immunogenic epitopes exhibited a selective enrichment of A3G hotspots, which were strongly biased to translate to non-synonymous amino acid substitutions. When superimposed on the known mutational gradient across the entire length of the HIV genome, we observed a gradient of A3G hotspot enrichment, and an HLA-specific pattern of the potential of A3G hotspots to lead to CTL escape mutations. These data illuminate the depths and extent of the co-evolution of the viral genome to subvert the host mutator A3G.
topic CTL epitope
APOBEC3G (A3G)
HIV
immune escape
viral evolution
url https://www.frontiersin.org/article/10.3389/fimmu.2018.03032/full
work_keys_str_mv AT faezehborzooee apobec3gregulationoftheevolutionaryracebetweenadaptiveimmunityandviralimmuneescapeisdeeplyimprintedinthehivgenome
AT kristadjoris apobec3gregulationoftheevolutionaryracebetweenadaptiveimmunityandviralimmuneescapeisdeeplyimprintedinthehivgenome
AT michaeldgrant apobec3gregulationoftheevolutionaryracebetweenadaptiveimmunityandviralimmuneescapeisdeeplyimprintedinthehivgenome
AT manilarijani apobec3gregulationoftheevolutionaryracebetweenadaptiveimmunityandviralimmuneescapeisdeeplyimprintedinthehivgenome
_version_ 1725766320772874240

Similar Items