1. Impact of Exogenous Galectin-9 on Human T Cells
- Author
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Françoise Praz, Olivier Moralès, Sylvie Souquere, Clément Barjon, Toshiro Niki, Mitsuomi Hirashima, Olivier Dellis, Claire Lhuillier, Philippe Busson, Ming Wei, and Aurore Gelin
- Subjects
Interleukin 21 ,ZAP70 ,CD28 ,Cytotoxic T cell ,Cell Biology ,IL-2 receptor ,Biology ,Natural killer T cell ,Antigen-presenting cell ,Molecular Biology ,Biochemistry ,Jurkat cells ,Cell biology - Abstract
Galectin-9 (gal-9) is a multifunctional β-galactoside-binding lectin, frequently released in the extracellular medium, where it acts as a pleiotropic immune modulator. Despite its overall immunosuppressive effects, a recent study has reported bimodal action of gal-9 on human resting blood T cells with apoptosis occurring in the majority of them, followed by a wave of activation and expansion of Th1 cells in the surviving population. Our knowledge of the signaling events triggered by exogenous gal-9 in T cells remains limited. One of these events is cytosolic calcium (Ca2+) release reported in some murine and human T cells. The aim of this study was to investigate the contribution of Ca2+ mobilization to apoptotic and nonapoptotic effects of exogenous gal-9 in human T cells. We found that the T cell receptor (TCR)-CD3 complex and the Lck kinase were required for Ca2+ mobilization but not for apoptosis induction in Jurkat cells. These data were confirmed in human CD4+ T cells from peripheral blood as follows: a specific Lck chemical inhibitor abrogated Ca2+ mobilization but not apoptosis induction. Moreover, Lck activity was also required for the production of Th1-type cytokines, i.e. interleukin-2 and interferon-γ, which resulted from gal-9 stimulation in peripheral CD4+ T cells. These findings indicate that gal-9 acts on T cells by two distinct pathways as follows: one mimicking antigen-specific activation of the TCR with a mandatory contribution of proximal elements of the TCR complex, especially Lck, and another resulting in apoptosis that is independent of this complex.
- Published
- 2015