Hippo pathway monomerizes STAT3 to regulate prostate cancer growth |
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Authors: | Qingfeng Tang Jing Fang Weiqi Lai Yu Hu Chengwan Liu Xiaobo Hu Caiyong Song Tianmu Cheng Rui Liu Xiaoke Huang |
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Affiliation: | 1. Department of Urology, Xindu District People''s Hospital of Chengdu, Chengdu China ; 2. Department of Nephrology, The Sixth People''s Hospital of Chengdu, Chengdu China ; 3. State Key Laboratory of Oral Diseases, National Clinical Research Center for Oral Diseases, Research Unit of Oral Carcinogenesis and Management, Chinese Academy of Medical Sciences, West China Hospital of Stomatology, Sichuan University, Chengdu China |
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Abstract: | Prostate cancer ranks among the most commonly diagnosed malignancies for men and has become a non‐negligible threat for public health. Interplay between inflammatory factors and cancer cells renders inflammatory tissue environment as a predisposing condition for cancer development. The Hippo pathway is a conserved signaling pathway across multiple species during evolution that regulates tissue homeostasis and organ development. Nevertheless, whether Hippo pathway regulates cancer‐related inflammatory factors remains elusive. Here, we show that high cell density–mediated activation of the Hippo pathway blunts STAT3 activity in prostate cancer cells. Hippo pathway component MST2 kinase phosphorylates STAT3 at T622, which is located in the SH2 domain of STAT3. This phosphorylation blocks the SH2 domain in one STAT3 molecule to bind with the phosphorylated Y705 site in another STAT3 molecule, which further counteracts IL6‐induced STAT3 dimerization and activation. Expression of a nonphosphorylatable STAT3 T622A mutant enhances STAT3 activity and IL6 expression at high cell density and promotes tumor growth in a mice xenograft model. Our findings demonstrate that STAT3 is a novel phosphorylation substrate for MST2 and thereby highlight a regulatory cascade underlying the crosstalk between inflammation and the Hippo pathway in prostate cancer cells. |
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Keywords: | Hippo pathway MST2 prostate cancer SH2 domain STAT3 |
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