Attenuation of GammadeltaTCR Signaling Efficiently Diverts Thymocytes to the Alphabeta Lineage

Overview

Journal Immunity

Publisher Cell Press

Specialty Allergy & Immunology

Date 2005 May 17

PMID 15894277

Citations 116

Authors

Marielle C Haks

Juliette M Lefebvre

Jens Peter H Lauritsen

Michael Carleton

Michele Rhodes

Toru Miyazaki

Dietmar J Kappes

David L Wiest

Affiliations

Soon will be listed here.

Abstract

The role of the T cell antigen receptor complex (TCR) in alphabeta/gammadelta lineage commitment remains controversial, in particular whether different TCR isoforms intrinsically favor adoption of a certain lineage. Here, we demonstrate that impairing the signaling capacity of a gammadeltaTCR complex enables it to efficiently direct thymocytes to the alphabeta lineage. In the presence of a ligand, a transgenic gammadeltaTCR mediates almost exclusive adoption of the gammadelta lineage, while in the absence of ligand, the same gammadeltaTCR promotes alphabeta lineage development with efficiency comparable to the pre-TCR. Importantly, attenuating gammadeltaTCR signaling through Lck deficiency causes reduced ERK1/2 activation and Egr expression and diverts thymocytes to the alphabeta lineage even in the presence of ligand. Conversely, ectopic Egr overexpression favors gammadelta T cell development. Our data support a model whereby gammadelta versus alphabeta lineage commitment is controlled by TCR signal strength, which depends critically on the ERK MAPK-Egr pathway.

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