Dramatic Influence of Vβ Gene Polymorphism on an Antigen-Specific CD8+ T Cell Response In Vivo

Author:

Bour Hélène1,Michielin Olivier2,Bousso Philippe3,Cerottini Jean-Charles1,MacDonald H. Robson1

Affiliation:

1. *Ludwig Institute for Cancer Research, Lausanne Branch, University of Lausanne, Epalinges, Switzerland;

2. †Le Bel Institute, Louis Pasteur University, Strasbourg, France; and

3. ‡Laboratory of Molecular Biology of the Gene, Pasteur Institute, Institut National de la Santé et de la Recherche Médicale U277, Paris, France

Abstract

Abstract According to recent crystallographic studies, the TCR-αβ contacts MHC class I-bound antigenic peptides via the polymorphic V gene-encoded complementarity-determining region 1β (CDR1β) and the hypervariable (D)J-encoded CDR3β and CDR3α domains. To evaluate directly the relative importance of CDR1β polymorphism on the fine specificity of T cell responses in vivo, we have taken advantage of congenic Vβa and Vβb mouse strains that differ by a CDR1 polymorphism in the Vβ10 gene segment. The Vβ10-restricted CD8+ T cell response to a defined immunodominant epitope was dramatically reduced in Vβa compared with Vβb mice, as measured either by the expansion of Vβ10+ cells or by the binding of MHC-peptide tetramers. These data indicate that Vβ polymorphism has an important impact on TCR-ligand binding in vivo, presumably by modifying the affinity of CDR1β-peptide interactions.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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