T cell development is dependent on the integration of multiple signaling pathways, although few links between signaling cascades and downstream nuclear factors that play a role in thymocyte differentiation have been identified. We show here that expression of the HMG box protein TOX is sufficient to induce changes in coreceptor gene expression associated with β-selection, including CD8 gene demethylation. TOX expression is also sufficient to initiate positive selection to the CD8 lineage in the absence of MHC–TCR interactions. TOX-mediated positive selection is associated with up-regulation of Runx3, implicating CD4 silencing in the process. Interestingly, a strong T cell receptor–mediated signal can modify this cell fate. We further demonstrate that up-regulation of TOX in double positive thymocytes is calcineurin dependent, linking this critical signaling pathway to nuclear changes during positive selection.
TOX Provides a Link Between Calcineurin Activation and CD8 Lineage Commitment
P. Aliahmad and E. O'Flaherty contributed equally to this work.
Abbreviations used in this paper: CD8ISP, CD4−CD8+ immature single positive thymocyte; Cn, calcineurin; DN, CD4−8− double negative thymocyte; DP, CD4+8+ double positive thymocyte; HMG, high mobility group; MAPK, mitogen-activated protein kinase; SP, CD4+8− or CD4−8+ single positive thymocyte; Tg, transgenic; TOX, thymocyte selection-associated HMG box protein.
Parinaz Aliahmad, Emmett O'Flaherty, Peggy Han, Olivia D. Goularte, Beverley Wilkinson, Masanobu Satake, Jeffery D. Molkentin, Jonathan Kaye; TOX Provides a Link Between Calcineurin Activation and CD8 Lineage Commitment . J Exp Med 19 April 2004; 199 (8): 1089–1099. doi: https://doi.org/10.1084/jem.20040051
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