| Literature DB >> 31431461 |
Yi Zhang1, Zhuqing Li1, Qiang Hao1, Wei Tan1, Jing Sun1, Jing Li1, Chi-Wei Chen1, Zongzhu Li1, Yunxiao Meng1, Yuan Zhou1, Zhiyong Han2, Huadong Pei1, Melvin L DePamphilis3, Wenge Zhu4.
Abstract
DNA rereplication leads to genomic instability and has been implicated in the pathology of a variety of human cancers. Eukaryotic DNA replication is tightly controlled to ensure it occurs only once during each cell cycle. Geminin is a critical component of this control, it prevents DNA rereplication from occurring during S, G2, and early M phases by preventing MCM helicases from forming prereplication complexes. Geminin is targeted for degradation by the anaphase-promoting complex (APC/C) from anaphase through G1-phase, however, accumulating evidence indicates that Geminin is downregulated in late S-phase due to an unknown mechanism. Here, we used a high-throughput screen to identify miRNAs that can induce excess DNA replication and found that miR-571 could reduce the protein level of Geminin in late S-phase independent of the APC/C. Furthermore, miR-571 regulated efficient DNA replication and S-phase cell-cycle progression. Strikingly, c-Myc suppressed miR-571 expression by binding directly to the miR-571 promoter. At the beginning of S-phase, Cdk2 phosphorylated c-Myc at Serine 62, promoting its association with the miR-571 promoter region. Collectively, we identify miR-571 as the first miRNA that prevents aberrant DNA replication and the Cdk2-c-Myc-miR-571 axis as a new pathway for regulating DNA replication, cell cycle, and genomic stability in cancer cells. SIGNIFICANCE: These findings identify a novel regulatory mechanism that is critical for maintaining genome integrity by regulating DNA replication and cell-cycle progression. ©2019 American Association for Cancer Research.Entities:
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Year: 2019 PMID: 31431461 PMCID: PMC7451049 DOI: 10.1158/0008-5472.CAN-19-0020
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701