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Genotypic and functional impact of HIV-1 adaptation to its host population during the North American epidemic

  1. Author:
    Cotton, L. A.
    Kuang, X. T.
    Le, A. Q.
    Carlson, J. M.
    Chan, B.
    Chopera, D. R.
    Brumme, C. J.
    Markle, T. J.
    Martin, E.
    Shahid, A.
    Anmole, G.
    Mwimanzi, P.
    Nassab, P.
    Penney, K. A.
    Rahman, M. A.
    Milloy, M. J.
    Schechter, M. T.
    Markowitz, M.
    Carrington, M.
    Walker, B. D.
    Wagner, T.
    Buchbinder, S.
    Fuchs, J.
    Koblin, B.
    Mayer, K. H.
    Harrigan, P. R.
    Brockman, M. A.
    Poon, A. F.
    Brumme, Z. L.

  2. Author Address

    Faculty of Health Sciences, Simon Fraser University, Burnaby, British Columbia, Canada. Department of Molecular Biology and Biochemistry, Faculty of Science, Simon Fraser University, Burnaby, British Columbia, Canada. Microsoft Research, Los Angeles, California, United States of America. Faculty of Health Sciences, Simon Fraser University, Burnaby, British Columbia, Canada; KwaZulu-Natal Research Institute for Tuberculosis and HIV, Nelson R. Mandela School of Medicine, University of KwaZulu-Natal, Durban, KwaZulu-Natal, South Africa. British Columbia Centre for Excellence in HIV/AIDS, Vancouver, British Columbia, Canada. Department of Molecular Biology and Biochemistry, Faculty of Science, Simon Fraser University, Burnaby, British Columbia, Canada; British Columbia Centre for Excellence in HIV/AIDS, Vancouver, British Columbia, Canada. British Columbia Centre for Excellence in HIV/AIDS, Vancouver, British Columbia, Canada; Faculty of Medicine, University of British Columbia, Vancouver, British Columbia, Canada. Faculty of Medicine, University of British Columbia, Vancouver, British Columbia, Canada. Aaron Diamond AIDS Research Center, The Rockefeller University, New York, New York, United States of America. Cancer and Inflammation Program, Laboratory of Experimental Immunology, Leidos Biomedical Research Inc., Frederick National Laboratory for Cancer Research, Frederick, Maryland, United States of America; Ragon Institute of MGH, MIT and Harvard University, Cambridge, Massachusetts, United States of America. Ragon Institute of MGH, MIT and Harvard University, Cambridge, Massachusetts, United States of America. San Francisco Department of Public Health, San Francisco, California, United States of America. New York Blood Center, New York, New York, United States of America. Fenway Community Health, Boston, Massachusetts, United States of America; Harvard Medical School, Boston, Massachusetts, United States of America. Faculty of Health Sciences, Simon Fraser University, Burnaby, British Columbia, Canada; Department of Molecular Biology and Biochemistry, Faculty of Science, Simon Fraser University, Burnaby, British Columbia, Canada; British Columbia Centre for Excellence in HIV/AIDS, Vancouver, British Columbia, Canada. Faculty of Health Sciences, Simon Fraser University, Burnaby, British Columbia, Canada; British Columbia Centre for Excellence in HIV/AIDS, Vancouver, British Columbia, Canada; Faculty of Medicine, University of British Columbia, Vancouver, British Columbia, Canada. Faculty of Health Sciences, Simon Fraser University, Burnaby, British Columbia, Canada; British Columbia Centre for Excellence in HIV/AIDS, Vancouver, British Columbia, Canada.
    1. Year: 2014
    2. Date: Apr
    3. Epub Date: 4/26/2014
  2. Journal: Plos Genetics
    1. 10
    2. 4
    3. Pages: e1004295
  4. Type of Article: Article
  5. ISSN: 1553-7404 (Electronic) 1553-7390 (Linking)
  1. Abstract:

    HLA-restricted immune escape mutations that persist following HIV transmission could gradually spread through the viral population, thereby compromising host antiviral immunity as the epidemic progresses. To assess the extent and phenotypic impact of this phenomenon in an immunogenetically diverse population, we genotypically and functionally compared linked HLA and HIV (Gag/Nef) sequences from 358 historic (1979-1989) and 382 modern (2000-2011) specimens from four key cities in the North American epidemic (New York, Boston, San Francisco, Vancouver). Inferred HIV phylogenies were star-like, with approximately two-fold greater mean pairwise distances in modern versus historic sequences. The reconstructed epidemic ancestral (founder) HIV sequence was essentially identical to the North American subtype B consensus. Consistent with gradual diversification of a "consensus-like" founder virus, the median "background" frequencies of individual HLA-associated polymorphisms in HIV (in individuals lacking the restricting HLA[s]) were approximately 2-fold higher in modern versus historic HIV sequences, though these remained notably low overall (e.g. in Gag, medians were 3.7% in the 2000s versus 2.0% in the 1980s). HIV polymorphisms exhibiting the greatest relative spread were those restricted by protective HLAs. Despite these increases, when HIV sequences were analyzed as a whole, their total average burden of polymorphisms that were "pre-adapted" to the average host HLA profile was only approximately 2% greater in modern versus historic eras. Furthermore, HLA-associated polymorphisms identified in historic HIV sequences were consistent with those detectable today, with none identified that could explain the few HIV codons where the inferred epidemic ancestor differed from the modern consensus. Results are therefore consistent with slow HIV adaptation to HLA, but at a rate unlikely to yield imminent negative implications for cellular immunity, at least in North America. Intriguingly, temporal changes in protein activity of patient-derived Nef (though not Gag) sequences were observed, suggesting functional implications of population-level HIV evolution on certain viral proteins.

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  2. DOI: 10.1371/journal.pgen.1004295
  3. PMID: 24762668
  4. PMCID: PMC3998893

Library Notes

  1. Fiscal Year: FY2013-2014
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