| Literature DB >> 34645979 |
Chen-Hui Cao1, Han Ling1, Kai Han1,2, Xiao-Peng Lu3, Mu-Yan Cai1,4, Jing-Hua Cao1, Jie Zhou1, Zhi-Cheng Xiang1, Jie-Wei Chen1,4, Si Li1, Jin-Long Lin1, Jin-Ling Duan1, Jie Luo1, Yu-Jing Fang1,2, Zhi-Zhong Pan1,2, Li Liang5, Feng Wang1, Dan Xie6,7, Feng-Wei Wang8.
Abstract
Colorectal carcinoma (CRC) is the second most deadly cancer worldwide. Therapies that take advantage of DNA repair defects have been explored in various tumors but not yet systematically in CRC. Here, we found that Diphosphoinositol Pentakisphosphate Kinase 2 (PPIP5K2), an inositol pyrophosphate kinase, was highly expressed in CRC and associated with a poor prognosis of CRC patients. In vitro and in vivo functional studies demonstrated that PPIP5K2 could promote the proliferation and migration ability of CRC cells independent of its inositol pyrophosphate kinase activity. Mechanically, S1006 dephosphorylation of PPIP5K2 could accelerate its dissociation with 14-3-3 in the cytoplasm, resulting in more nuclear distribution. Moreover, DNA damage treatments such as doxorubicin (DOX) or irradiation (IR) could induce nuclear translocation of PPIP5K2, which subsequently promoted homologous recombination (HR) repair by binding and recruiting RPA70 to the DNA damage site as a novel scaffold protein. Importantly, we verified that S1006 dephosphorylation of PPIP5K2 could significantly enhance the DNA repair ability of CRC cells through a series of DNA repair phenotype assays. In conclusion, PPIP5K2 is critical for enhancing the survival of CRC cells via facilitating DNA HR repair. Our findings revealed an unrecognized biological function and mechanism model of PPIP5K2 dependent on S1006 phosphorylation and provided a potential therapeutic target for CRC patients.Entities:
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Year: 2021 PMID: 34645979 DOI: 10.1038/s41388-021-02052-5
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867