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The Costimulatory Molecule CD226 Signals Through VAV1 to Amplify TCR Signals and Promote IL-17 Production by CD4 T Cells

Overview
Journal Sci Signal
Specialties Cell Biology
Physiology
Science
Date 2018 Jul 12
PMID 29991650
Citations 22
Authors
Guillaume Gaud
Romain Roncagalli
Karima Chaoui
Isabelle Bernard
Julien Familiades
Celine Colacios
Sahar Kassem
Bernard Monsarrat
Odile Burlet-Schiltz
Anne Gonzalez de Peredo
Bernard Malissen
Abdelhadi Saoudi
Affiliations
Soon will be listed here.
Abstract

The activation of T cells requires the guanine nucleotide exchange factor VAV1. Using mice in which a tag for affinity purification was attached to endogenous VAV1 molecules, we analyzed by quantitative mass spectrometry the signaling complex that assembles around activated VAV1. Fifty VAV1-binding partners were identified, most of which had not been previously reported to participate in VAV1 signaling. Among these was CD226, a costimulatory molecule of immune cells. Engagement of CD226 induced the tyrosine phosphorylation of VAV1 and synergized with T cell receptor (TCR) signals to specifically enhance the production of interleukin-17 (IL-17) by primary human CD4 T cells. Moreover, co-engagement of the TCR and a risk variant of CD226 that is associated with autoimmunity (rs763361) further enhanced VAV1 activation and IL-17 production. Thus, our study reveals that a VAV1-based, synergistic cross-talk exists between the TCR and CD226 during both physiological and pathological T cell responses and provides a rational basis for targeting CD226 for the management of autoimmune diseases.

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