Litcius/Paper detail

Backbone Modifications of HLA-A2-Restricted Antigens Induce Diverse Binding and T Cell Activation Outcomes

Ruslan Gibadullin, Caleb J. Randall, John Sidney, Alessandro Sette, Samuel H. Gellman

2021Journal of the American Chemical Society17 citationsDOIOpen Access PDF

Abstract

T cells express T cell receptors (TCRs) that recognize short peptide antigens in the context of major histocompatibility class I (MHC I) molecules. This recognition process produces an array of cytokine-mediated signals that help to govern immunological responses. Design of biostable MHC I peptide vaccines containing unnatural subunits is desirable, and synthetic antigens in which a native α-amino acid residue is replaced by a homologous β-amino acid residue (native side chain but extended backbone) might be useful in this regard. We have evaluated the impact of α-to-β backbone modification at a single site on T cell-mediated recognition of six clinically important viral and tumor-associated antigens bound to an MHC I. Effects of this modification on MHC I affinity and T cell activation were measured. Many of these modifications diminish or prevent T cell response. However, a number of α/β-peptide antigens were found to mimic the activity of natural antigens or to enhance maximal T cell response, as measured by interferon-γ release. Results from this broad exploratory study advance our understanding of immunological responses to antigens bearing unnatural modifications and suggest that α/β-peptides could be a source of potent and proteolytically stable variants of native antigens.

Topics & Concepts

ChemistryAntigenMajor histocompatibility complexCytotoxic T cellCD8T-cell receptorMHC restrictionT cellHuman leukocyte antigenAntigen presentationPeptideMHC class IAntigen-presenting cellCell biologyBiochemistryImmune systemImmunologyBiologyIn vitroImmunotherapy and Immune Responsesvaccines and immunoinformatics approachesT-cell and B-cell Immunology