A novel lncRNA Discn fine-tunes replication protein A (RPA) availability to promote genomic stability

被引:0
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作者
Lin Wang
Jingzheng Li
Hu Zhou
Weidao Zhang
Jing Gao
Ping Zheng
机构
[1] Kunming Institute of Zoology,State Key Laboratory of Genetic Resources and Evolution
[2] Chinese Academy of Sciences,Yunnan Key Laboratory of Animal Reproduction
[3] Kunming Institute of Zoology,Department of Analytical Chemistry and CAS Key Laboratory of Receptor Research
[4] Chinese Academy of Sciences,KIZ/CUHK Joint Laboratory of Bioresources and Molecular Research in Common Diseases
[5] University of Chinese Academy of Sciences,Center for Excellence in Animal Evolution and Genetics
[6] Shanghai Institute of Materia Medica,undefined
[7] Chinese Academy of Sciences,undefined
[8] Kunming Institute of Zoology,undefined
[9] Chinese Academy of Sciences,undefined
[10] Chinese Academy of Sciences,undefined
来源
Nature Communications | / 12卷
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摘要
RPA is a master regulator of DNA metabolism and RPA availability acts as a rate-limiting factor. While numerous studies focused on the post-translational regulations of RPA for its functions, little is known regarding how RPA availability is controlled. Here we identify a novel lncRNA Discn as the guardian of RPA availability in stem cells. Discn is induced upon genotoxic stress and binds to neucleolin (NCL) in the nucleolus. This prevents NCL from translocation into nucleoplasm and avoids undesirable NCL-mediated RPA sequestration. Thus, Discn-NCL-RPA pathway preserves a sufficient RPA pool for DNA replication stress response and repair. Discn loss causes massive genome instability in mouse embryonic stem cells and neural stem/progenigor cells. Mice depleted of Discn display newborn death and brain dysfunctions due to DNA damage accumulation and associated inflammatory reactions. Our findings uncover a key regulator of DNA metabolism and provide new clue to understand the chemoresistance in cancer treatment.
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