Thymocytes depend on the interaction with thymic epithelial cells for the generation of a diverse, nonautoreactive T cell repertoire. In turn, thymic epithelial cells acquire their three-dimensional cellular organization via instructive signals from developing thymocytes. The nature of these signals has been elusive so far. We show that thymocytes and medullary epithelial cells (MECs) communicate via the lymphotoxin β receptor (LTβR) signaling axis. Normal differentiation of thymic MECs requires LTβR ligand on thymocytes and LTβR together with nuclear factor–κB-inducing kinase (Nik) in thymic epithelial cells. Impaired lympho–epithelial cross talk in the absence of the LTβR causes aberrant differentiation and reduced numbers of thymic MECs, leads to the retention of mature T lymphocytes, and is associated with autoimmune phenomena, suggesting an unexpected role for LTβR signaling in central tolerance induction.
Thymic Medullary Epithelial Cell Differentiation, Thymocyte Emigration, and the Control of Autoimmunity Require Lympho–Epithelial Cross Talk via LTβR
Abbreviations used in this paper: BrdU, 5-bromo-2′deoxyuridine; LTβR, lymphotoxin β receptor; MEC, medullary epithelial cell; Nik, nuclear factor–κB-inducing kinase; RTE, recent thymic emigrant; UEA-1, ulex europaeus agglutinin 1.
The online version of this article includes supplemental material.
The present address of S. Scheu is the Howard Hughes Medical Institute, University of California, San Francisco, San Francisco, CA 94143.
Thomas Boehm, Stefanie Scheu, Klaus Pfeffer, Conrad C. Bleul; Thymic Medullary Epithelial Cell Differentiation, Thymocyte Emigration, and the Control of Autoimmunity Require Lympho–Epithelial Cross Talk via LTβR . J Exp Med 1 September 2003; 198 (5): 757–769. doi: https://doi.org/10.1084/jem.20030794
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