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Inhibition of TPL2 by interferon-α suppresses bladder cancer through activation of PDE4D.

Zhe QiangZong-Yuan ZhouTing PengPu-Zi JiangNan ShiEmmanuel Mfotie NjoyaBahtigul AzimovaWan-Li LiuWei-Hua ChenGuo-Lin ZhangFei Wang
Published in: Journal of experimental & clinical cancer research : CR (2018)
Our data reveal that IFN-α can exert its antitumor effect through a non-canonical JAK-STAT pathway in the bladder cancer cells with low activity of IFN pathway, and the TPL2 inhibition is another function of IFN-α in the context of bladder cancer therapy. The antitumor effects of IFN-α and MEK inhibition also depend on the PDE4D-mediated cAMP level in bladder cancer cells. Suppression of the TPL2 phosphorylation and intracellular cAMP level may be possible therapeutic strategies for enhancing the effectiveness of IFN-α and MEK inhibitors in bladder cancer treatment.
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