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Publication : Impaired thymic selection and abnormal antigen-specific T cell responses in Foxn1(Δ/Δ) mutant mice.

First Author  Xiao S Year  2010
Journal  PLoS One Volume  5
Issue  11 Pages  e15396
PubMed ID  21079757 Mgi Jnum  J:166826
Mgi Id  MGI:4849862 Doi  10.1371/journal.pone.0015396
Citation  Xiao S, et al. (2010) Impaired thymic selection and abnormal antigen-specific T cell responses in Foxn1(Delta/Delta) mutant mice. PLoS One 5(11):e15396
abstractText  BACKGROUND: Foxn1(Delta/Delta) mutant mice have a specific defect in thymic development, characterized by a block in TEC differentiation at an intermediate progenitor stage, and blocks in thymocyte development at both the DN1 and DP cell stages, resulting in the production of abnormally functioning T cells that develop from an atypical progenitor population. In the current study, we tested the effects of these defects on thymic selection. METHODOLOGY/PRINCIPAL FINDINGS: We used Foxn1(Delta/Delta); DO11 Tg and Foxn1(Delta/Delta); OT1 Tg mice as positive selection and Foxn1(Delta/Delta); MHCII I-E mice as negative selection models. We also used an in vivo system of antigen-specific reactivity to test the function of peripheral T cells. Our data show that the capacity for positive and negative selection of both CD4 and CD8 SP thymocytes was reduced in Foxn1(Delta/Delta) mutants compared to Foxn1(+/Delta) control mice. These defects were associated with reduction of both MHC Class I and Class II expression, although the resulting peripheral T cells have a broad TCR Vbeta repertoire. In this deficient thymic environment, immature CD4 and CD8 SP thymocytes emigrate from the thymus into the periphery. These T cells had an incompletely activated profile under stimulation of the TCR signal in vitro, and were either hypersensitive or hyporesponsive to antigen-specific stimulation in vivo. These cell-autonomous defects were compounded by the hypocellular peripheral environment caused by low thymic output. CONCLUSIONS/SIGNIFICANCE: These data show that a primary defect in the thymic microenvironment can cause both direct defects in selection which can in turn cause indirect effects on the periphery, exacerbating functional defects in T cells.
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