| Literature DB >> 31975570 |
Yasutaka Yamada1,2, Nijiro Nohata3, Akifumi Uchida4, Mayuko Kato1,2, Takayuki Arai1,2, Shogo Moriya5, Keiko Mizuno4, Satoko Kojima6, Kazuto Yamazaki7, Yukio Naya6, Tomohiko Ichikawa2, Naohiko Seki1.
Abstract
Analysis of microRNA (miRNA) regulatory networks is useful for exploring novel biomarkers and therapeutic targets in cancer cells. The Cancer Genome Atlas dataset shows that low expression of both strands of pre-miR-101 (miR-101-5p and miR-101-3p) significantly predicted poor prognosis in clear cell renal cell carcinoma (ccRCC). The functional significance of miR-101-5p in cancer cells is poorly understood. Here, we focused on miR-101-5p to investigate the antitumor function and its regulatory networks in ccRCC cells. Ectopic expression of mature miRNAs or siRNAs was investigated in cancer cell lines to characterize cell function, ie, proliferation, apoptosis, migration, and invasion. Genome-wide gene expression and in silico database analyses were undertaken to predict miRNA regulatory networks. Expression of miR-101-5p caused cell cycle arrest and apoptosis in ccRCC cells. Downstream neighbor of son (DONSON) was directly regulated by miR-101-5p, and its aberrant expression was significantly associated with shorter survival in propensity score-matched analysis (P = .0001). Knockdown of DONSON attenuated ccRCC cell aggressiveness. Several replisome genes controlled by DONSON and their expression were closely associated with ccRCC pathogenesis. The antitumor miR-101-5p/DONSON axis and its modulated replisome genes might be a novel diagnostic and therapeutic target for ccRCC.Entities:
Keywords: zzm321990DONSONzzm321990; zzm321990miR-101-5pzzm321990; microRNA; renal cell carcinoma; replisome
Year: 2020 PMID: 31975570 DOI: 10.1111/cas.14327
Source DB: PubMed Journal: Cancer Sci ISSN: 1347-9032 Impact factor: 6.716