Biochemistry and Pharmacology - Research Publications

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Start date: 2002 × End date: 2002 × Type: Journal Article × Author: COLE, TIMOTHY × Author: Lew, Andrew ×

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    Glucocorticoid receptor deficient thymic and peripheral T cells develop normally in adult mice
    Purton, JF ; Zhan, YF ; Liddicoat, DR ; Hardy, CL ; Lew, AM ; Cole, TJ ; Godfrey, DI (WILEY-V C H VERLAG GMBH, 2002-12)
    The involvement of glucocorticoid receptor (GR) signaling in T cell development is highly controversial, with several studies for and against. We have previously demonstrated that GR(-/-) mice, which usually die at birth because of impaired lung development, exhibit normal T cell development, at least in embryonic mice and in fetal thymus organ cultures. To directly investigate the role of GR signaling in adult T cell development, we analyzed the few GR(-/-) mice that occasionally survive birth, and irradiated mice reconstituted with GR(-/-) fetal liver precursors. All thymic and peripheral T cells, as well as other leukocyte lineages, developed and were maintained at normal levels. Anti-CD3-induced cell death of thymocytes in vitro, T cell repertoire heterogeneity and T cell proliferation in response to anti-CD3 stimulation were normal in the absence of GR signaling. Finally, we show that metyrapone, an inhibitor of glucocorticoid synthesis (commonly used to demonstrate a role for glucocorticoids in T cell development), impaired thymocyte development regardless of GR genotype indicating that this reagent inhibits thymocyte development in a glucocorticoid-independent fashion. These data demonstrate that GR signaling is not required for either normal T cell development or peripheral maintenance in embryonic or adult mice.