Discover Oncology (Mar 2022)

miR-93-5p suppresses ovarian cancer malignancy and negatively regulate CCND2 by binding to its 3′UTR region

  • Guotong Chen,
  • Yiwei Yan,
  • Xiaojv Qiu,
  • Chengfeng Ye,
  • Xingmei Jiang,
  • Shuo Song,
  • Yibo Zhang,
  • Huanhuan Chang,
  • Leqi Wang,
  • Xuehuan He,
  • Lingrong Tang,
  • Qingyu Zhang,
  • Ying Zhang

DOI
https://doi.org/10.1007/s12672-022-00478-1
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 11

Abstract

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Abstract Ovarian cancer is the most fatal gynecological cancer worldwide, yet the fundamental mechanism of malignancy acquisition in ovarian cancer remains unknown. miRNA has been implicated to a variety of diseases, including cancer initiation and progression. Cyclin-D2 (CCND2) is ubiquitously implicated in cancer uncontrol cell proliferation. Bioinformatic research revealed that CCND2 is a candidate gene for miR-93-5p with a binding site in its 3′UTR region in the current study. Using our ovarian cancer sample, we verified that miR-93-5p is negatively correlated with CCND2 mRNA and protein levels. Luciferase report assay revealed miR-93-5p inhibits CCND2 production through binding to the 3′UTR region. The expression of miR-93-5p in ovarian cancer patient samples was then determined, and a survival analysis was performed. Our findings showed that miR-93-5p is downregulated in ovarian cancer and is a favorable predictive factor in ovarian cancer patient. CCK8 assay, wound healing assay and flow cytometry-based cell cycle and apoptotic cell analyses were employed here. We found that miR-93-5p suppresses ovarian cancer cell proliferation and migration while enhances cell death. Our research certified that miR-93-5p reduces ovarian cancer malignancy by targeting CCND2.