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Structural basis for self-discrimination by neoantigen-specific TCRs

John P. Finnigan, Jenna H. Newman, Y. Patskovsky, Larysa Patskovska, Andrew S. Ishizuka, Geoffrey M. Lynn, Robert A. Seder, Michelle Krogsgaard, Nina Bhardwaj

2024Nature Communications15 citationsDOIOpen Access PDF

Abstract

Abstract T cell receptors (TCR) are pivotal in mediating tumour cell cytolysis via recognition of mutation-derived tumour neoantigens (neoAgs) presented by major histocompatibility class-I (MHC-I). Understanding the factors governing the emergence of neoAg from somatic mutations is a major focus of current research. However, the structural and cellular determinants controlling TCR recognition of neoAgs remain poorly understood. This study describes the multi-level analysis of a model neoAg from the B16F10 murine melanoma, H2-D b /Hsf2 p.K72N 68-76 , as well as its cognate TCR 47BE7. Through cellular, molecular and structural studies we demonstrate that the p.K72N mutation enhances H2-D b binding, thereby improving cell surface presentation and stabilizing the TCR 47BE7 epitope. Furthermore, TCR 47BE7 exhibited high functional avidity and selectivity, attributable to a broad, stringent, binding interface enabling recognition of native B16F10 despite low antigen density. Our findings provide insight into the generation of anchor-residue modified neoAg, and emphasize the value of molecular and structural investigations of neoAg in diverse MHC-I contexts for advancing the understanding of neoAg immunogenicity.

Topics & Concepts

T-cell receptorAvidityMajor histocompatibility complexEpitopeBiologyT cellCytolysisImmunogenicityComputational biologyAntigen presentationCell biologyAntigenGeneticsCytotoxic T cellImmune systemIn vitroCAR-T cell therapy researchImmunotherapy and Immune ResponsesImmune Cell Function and Interaction
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