4.8 Article

Structurally silent peptide anchor modifications allosterically modulate T cell recognition in a receptor-dependent manner

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA (2021)

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Journal

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
Volume 118, Issue 4, Pages -

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.2018125118

Keywords

T cell receptor; MHC; binding; allostery; molecular dynamics

Categories

Multidisciplinary Sciences

Funding

  1. National Institute of General Medical Sciences, National Institutes of Health [R35GM118166]
  2. Walther Cancer Foundation Interdisciplinary Interface Training Project fellowship
  3. National Institutes of Health [S10RR25528, S10RR028976]
  4. National Cancer Institute [ACB-12002]
  5. National Institute of General Medical Sciences [AGM-12006]
  6. U.S. Department of Energy, Office of Science, Office of Basic Energy Sciences [W-31-109-Eng-38]

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This study shows that modifications at primary anchors, even without structural impact, can significantly affect T cell recognition depending on the TCR. The impact of peptide anchor modification can be sensed by a TCR at regions distant from the modification site, indicating a through-protein mechanism. These findings have implications for the use of anchor-modified peptides and predicting the immunogenicity of tumor neoantigens.
Presentation of peptides by class I MHC proteins underlies T cell immune responses to pathogens and cancer. The association between peptide binding affinity and immunogenicity has led to the engineering of modified peptides with improved MHC binding, with the hope that these peptides would be useful for eliciting cross-reactive immune responses directed toward their weak binding, unmodified counterparts. Increasing evidence, however, indicates that T cell receptors (TCRs) can perceive such anchor-modified peptides differently than wild-type (WT) peptides, although the scope of discrimination is unclear. We show here that even modifications at primary anchors that have no discernible structural impact can lead to substantially stronger or weaker T cell recognition depending on the TCR. Surprisingly, the effect of peptide anchor modification can be sensed by a TCR at regions distant from the site of modification, indicating a through-protein mechanism in which the anchor residue serves as an allosteric modulator for TCR binding. Our findings emphasize caution in the use and interpretation of results from anchormodified peptides and have implications for how anchor modifications are accounted for in other circumstances, such as predicting the immunogenicity of tumor neoantigens. Our data also highlight an important need to better understand the highly tunable dynamic nature of class I MHC proteins and the impact this has on various forms of immune recognition.

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