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• W1992543348 abstract "Summary E2A has been shown to be an important transcription factor downstream of the T‐cell receptor (TCR) signal during T‐cell development. The TCR signal is known to elicit different cellular responses at different stages of T‐cell development. Whether E2A is still required for normal TCR signalling in mature T cells is unknown. Here we examined T‐cell function after disruption of the E2A gene exclusively in the T‐cell lineage. The conditional E2A‐deficient mice show enhanced humoral immunity to a T‐dependent antigen. We further show that E2A is involved in regulating TCR‐induced T‐cell proliferation events. However, E2A seems to play opposite roles in naïve and effector T cells. In the absence of E2A, TCR‐induced proliferation is increased in naïve T cells and decreased in effector T cells. At older ages, these mice frequently develop antinuclear antibodies and proteinuria. Our studies suggest that E2A regulates T‐cell function and the loss of E2A may promote age‐dependent autoimmune diseases." @default.
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• W1992543348 date "2004-01-21" @default.
• W1992543348 modified "2023-10-16" @default.
• W1992543348 title "Altered T-dependent antigen responses and development of autoimmune symptoms in mice lacking E2A in T lymphocytes" @default.
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• W1992543348 doi "https://doi.org/10.1111/j.0019-2805.2003.01802.x" @default.
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