Contributions of the T Cell Receptor-associated CD3{gamma}-ITAM to Thymocyte Selection

doi:10.1084/jem.20020268

Published online 24 June 2002 doi:10.1084/jem.20020268

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© Rockefeller University Press, 0022-1007/2002/7/1/ $5.00
The Journal of Experimental Medicine, Volume 196, Number 1, July 1, 2002 1-13

Contributions of the T Cell Receptor–associated CD3 ${gamma}$ –ITAM to Thymocyte Selection

Mariëlle C. Haks¹, Elsa Pépin¹, Jeroen H.N. van den Brakel¹, Sigrid A.A. Smeele¹, Stanley M. Belkowski³, Helmut W.H.G. Kessels¹, Paul Krimpenfort² and Ada M. Kruisbeek¹

¹ Division of Immunology, Netherlands Cancer Institute, 1066 CX Amsterdam, Netherlands
² Division of Molecular Genetics, Netherlands Cancer Institute, 1066 CX Amsterdam, Netherlands
³ Division of Basic Sciences, Immunobiology Working Group, Fox Chase Cancer Center, Philadelphia, PA 19111

Address correspondence to Ada M. Kruisbeek, Division of Immunology, The Netherlands Cancer Institute, Plesmanlaan 121, 1066 CX Amsterdam, Netherlands. Phone: 31-20-5122056; Fax: 31-20-5122057; E-mail: ma.v.halem{at}nki.nl

The immunoreceptor tyrosine-based activation motifs (ITAMs)in the CD3 chains associated with the T cell receptor (TCR)are crucial for TCR signaling. To probe the role of the CD3 ${gamma}$ –ITAMin T cell development, we created knock-in mice in which theCD3 ${gamma}$ chain of the TCR complex is replaced by a mutant signaling-deficientCD3 ${gamma}$ chain, lacking the CD3 ${gamma}$ –ITAM. This mutation resultsin considerable impairment in positive selection in the polyclonalTCR repertoire. When CD3 ${gamma}$ – ${Delta}$ ITAM mice are crossed to miceexpressing transgenic F5 TCRs, their thymocytes are completelyunable to perform positive selection in vivo in response tointrathymic ligands. Also, the in vitro positive selection responseof double-positive (DP) thymocytes with F5–CD3 ${gamma}$ – ${Delta}$ ITAMmutant receptors to their agonist ligand and many of its variantsis severely impaired or abrogated. Yet, the binding and dissociationconstants of agonist ligands for the F5 receptor are not affectedby the CD3 ${gamma}$ – ${Delta}$ ITAM mutation. Furthermore, DP thymocytes withmutant receptors can respond to agonist ligand with normal antigensensitivity and to normal levels, as shown by their abilityto induce CD69 up-regulation, TCR down-regulation, negativeselection, and ZAP70 and c-Jun NH₂-terminal kinase activation.In sharp contrast, induction of extracellular signal-regulatedkinase (ERK) activation and linker for activation of T cells(LAT) phosphorylation are severely impaired in these cells.Together, these findings underscore that intrinsic propertiesof the TCR–CD3 complex regulate selection at the DP checkpoint.More importantly, this analysis provides the first direct geneticevidence for a role of the CD3 ${gamma}$ –ITAM in TCR-driven thymocyteselection.

Key Words: thymocyte selection • CD3 ${gamma}$ –ITAM • ITAM multiplicity • T cell activation • TCR signaling

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