Evidence for a TCR Affinity Threshold Delimiting Maximal CD8 T Cell Function

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2010 Mar 31

PMID 20351194

Citations 133

Authors

Daphne A Schmid

Melita B Irving

Vilmos Posevitz

Michael Hebeisen

Anita Posevitz-Fejfar

J-C Floyd Sarria

Raquel Gomez-Eerland

Margot Thome

Ton N M Schumacher

Pedro Romero

Daniel E Speiser

Vincent Zoete

Olivier Michielin

Nathalie Rufer

Affiliations

Soon will be listed here.

Abstract

Protective adaptive immune responses rely on TCR-mediated recognition of Ag-derived peptides presented by self-MHC molecules. However, self-Ag (tumor)-specific TCRs are often of too low affinity to achieve best functionality. To precisely assess the relationship between TCR-peptide-MHC binding parameters and T cell function, we tested a panel of sequence-optimized HLA-A(*)0201/NY-ESO-1(157-165)-specific TCR variants with affinities lying within physiological boundaries to preserve antigenic specificity and avoid cross-reactivity, as well as two outliers (i.e., a very high- and a low-affinity TCR). Primary human CD8 T cells transduced with these TCRs demonstrated robust correlations between binding measurements of TCR affinity and avidity and the biological response of the T cells, such as TCR cell-surface clustering, intracellular signaling, proliferation, and target cell lysis. Strikingly, above a defined TCR-peptide-MHC affinity threshold (K(D) < approximately 5 muM), T cell function could not be further enhanced, revealing a plateau of maximal T cell function, compatible with the notion that multiple TCRs with slightly different affinities participate equally (codominantly) in immune responses. We propose that rational design of improved self-specific TCRs may not need to be optimized beyond a given affinity threshold to achieve both optimal T cell function and avoidance of the unpredictable risk of cross-reactivity.

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