AI Article Synopsis

  • T cell cross-reactivity allows the immune system to recognize a wide range of pathogens by utilizing a diverse repertoire of T cell receptors (TCRs), particularly relevant in cases like HIV infection.
  • Recent research focused on a specific HIV-related TCR (AGA1 TCR) using advanced technology to analyze a vast array of peptides, unveiling its preference for a particular peptide motif.
  • The study suggests that microbial peptides presented by MHC class I proteins could potentially affect the behavior of virus-specific T cell populations, highlighting the complex interactions between different microbes and the immune response.

Article Abstract

T cell cross-reactivity ensures that diverse pathogen-derived epitopes encountered during a lifetime are recognized by the available TCR repertoire. A feature of cross-reactivity where previous exposure to one microbe can alter immunity to subsequent, non-related pathogens has been mainly explored for viruses. Yet cross-reactivity to additional microbes is important to consider, especially in HIV infection where gut-intestinal barrier dysfunction could facilitate T cell exposure to commensal/pathogenic microbes. Here we evaluated the cross-reactivity of a 'public', HIV-specific, CD8 T cell-derived TCR (AGA1 TCR) using MHC class I yeast display technology. Via screening of MHC-restricted libraries comprising ~2×10 sequence-diverse peptides, AGA1 TCR specificity was mapped to a central peptide di-motif. Using the top TCR-enriched library peptides to probe the non-redundant protein database, bacterial peptides that elicited functional responses by AGA1-expressing T cells were identified. The possibility that in context-specific settings, MHC class I proteins presenting microbial peptides influence virus-specific T cell populations in vivo is discussed.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7384859PMC
http://dx.doi.org/10.7554/eLife.58128DOI Listing

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