| Literature DB >> 24530303 |
Yangmeng Wang1, Hongxiu Ning2, Fangli Ren1, Yuanjiang Zhang1, Yu Rong1, Yinyin Wang1, Fuqin Su1, Chenguang Cai1, Zhe Jin1, Zhiyong Li1, Xinqi Gong1, Yonggong Zhai3, Dianjun Wang4, Baoqing Jia4, Ying Qiu1, Yasuhiko Tomita5, Joseph J Y Sung6, Jun Yu6, David M Irwin7, Xiao Yang8, Xinyuan Fu9, Y Eugene Chin10, Zhijie Chang11.
Abstract
Impaired phosphatase activity contributes to the persistent activation of STAT3 in tumors. Given that STAT family members with various or even opposite functions are often phosphorylated or dephosphorylated by the same enzymes, the mechanism for STAT3-specific dephosphorylation in cells remains largely unknown. Here, we report that GdX (UBL4A) promotes STAT3 dephosphorylation via mediating the interaction between TC45 (the nuclear isoform of TC-PTP) and STAT3 specifically. GdX stabilizes the TC45-STAT3 complex to bestow upon STAT3 an efficient dephosphorylation by TC45. Inasmuch, GdX suppresses tumorigenesis and tumor development by reducing the level of phospho-STAT3 (p-STAT3), whereas deletion of GdX results in a high level of p-STAT3 and accelerated colorectal tumorigenesis induced by AOM/DSS. Thus, GdX converts TC45, a nonspecific phosphatase, into a STAT3-specific phosphatase by bridging an association between TC45 and STAT3.Entities:
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Year: 2014 PMID: 24530303 DOI: 10.1016/j.molcel.2014.01.020
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970