Nuclear factor of activated T cells transcription factor NFATp controls superantigen-induced lethal shock

AV Tsytsykova, AE Goldfeld - The Journal of Experimental Medicine, 2000 - rupress.org
AV Tsytsykova, AE Goldfeld
The Journal of Experimental Medicine, 2000rupress.org
Tumor necrosis factor α (TNF-α) is the key mediator of superantigen-induced T cell lethal
shock. Here, we show that nuclear factor of activated T cells transcription factor, NFATp,
controls susceptibility to superantigen-induced lethal shock in mice through its activation of
TNF-α gene transcription. In NFATp-deficient mice, T cell stimulation leads to delayed
induction and attenuation of TNF-α mRNA levels, decreased TNF-α serum levels, and
resistance to superantigen-induced lethal shock. By contrast, after lipopolysaccharide (LPS) …
Tumor necrosis factor α (TNF-α) is the key mediator of superantigen-induced T cell lethal shock. Here, we show that nuclear factor of activated T cells transcription factor, NFATp, controls susceptibility to superantigen-induced lethal shock in mice through its activation of TNF-α gene transcription. In NFATp-deficient mice, T cell stimulation leads to delayed induction and attenuation of TNF-α mRNA levels, decreased TNF-α serum levels, and resistance to superantigen-induced lethal shock. By contrast, after lipopolysaccharide (LPS) challenge, serum levels of TNF-α and susceptibility to shock are unaffected. These results demonstrate that NFATp is an essential activator of immediate early TNF-α gene expression in T cells and they present in vivo evidence of the inducer- and cell type–specific regulation of TNF-α gene expression. Furthermore, they suggest NFATp as a potential selective target in the treatment of superantigen-induced lethal shock.
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