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Mapping the landscape of host-pathogen coevolution: HLA class I binding and its relationship with evolutionary conservation in human and viral proteins

Journal of Virology, ISSN: 0022-538X, Vol: 85, Issue: 3, Page: 1310-1321
2011
  • 56
    Citations
  • 0
    Usage
  • 139
    Captures
  • 0
    Mentions
  • 55
    Social Media
Metric Options:   Counts1 Year3 Year

Metrics Details

  • Citations
    56
  • Captures
    139
  • Social Media
    55
    • Shares, Likes & Comments
      55
      • Facebook
        55

Article Description

The high diversity of HLA binding preferences has been driven by the sequence diversity of short segments of relevant pathogenic proteins presented by HLA molecules to the immune system. To identify possible commonalities in HLA binding preferences, we quantify these using a novel measure termed "targeting efficiency," which captures the correlation between HLA-peptide binding affinities and the conservation of the targeted proteomic regions. Analysis of targeting efficiencies for 95 HLA class I alleles over thousands of human proteins and 52 human viruses indicates that HLA molecules preferentially target conserved regions in these proteomes, although the arboviral Flaviviridae are a notable exception where nonconserved regions are preferentially targeted by most alleles. HLA-A alleles and several HLA-B alleles that have maintained close sequence identity with chimpanzee homologues target conserved human proteins and DNA viruses such as Herpesviridae and Adenoviridae most efficiently, while all HLA-B alleles studied efficiently target RNA viruses. These patterns of host and pathogen specialization are both consistent with coevolutionary selection and functionally relevant in specific cases; for example, preferential HLA targeting of conserved proteomic regions is associated with improved outcomes in HIV infection and with protection against dengue hemorrhagic fever. Efficiency analysis provides a novel perspective on the coevolutionary relationship between HLA class I molecular diversity, self-derived peptides that shape T-cell immunity through ontogeny, and the broad range of viruses that subsequently engage with the adaptive immune response. Copyright © 2011, American Society for Microbiology. All Rights Reserved.

Bibliographic Details

Hertz, Tomer; Nolan, David; James, Ian; John, Mina; Gaudieri, Silvana; Phillips, Elizabeth; Huang, Jim C; Riadi, Gonzalo; Mallal, Simon; Jojic, Nebojsa

American Society for Microbiology

Immunology and Microbiology; Agricultural and Biological Sciences

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