CircUBE2D2 regulates HMGB1 through miR-885-5p to promote ovarian cancer malignancy

Authors

  • RuiXue Yan Cangzhou Central Hospital https://orcid.org/0009-0000-6115-1492
  • SaiTian Zeng Cangzhou Central Hospital
  • FangYuan Gao Cangzhou Central Hospital
  • LingLing Li Cangzhou Central Hospital
  • XiYun Xiao Cangzhou Central Hospital

DOI:

https://doi.org/10.1016/

Keywords:

Ovarian Cancer, CircUBE2D2, miR-885-5p, ceRNA, HMGB1

Abstract

Background: The newly discovered CircUBE2D2 has been shown to abnormally upregulate and promote cancer progression in a variety of cancers. The present study explored circUBE2D2 (hsa_circ_0005728) in Ovarian Cancer (OC) progression. Methods: CircUBE2D2, miR-885-5p, and HMGB1 were examined by RT-qPCR or WB. SKOV-3 cell functions (including cell viability, apoptosis, migration, and invasion) were validated using the CCK-8, flow cytometry, scratch assay, and transwell assay, respectively. The direct relationship between miR-885-5p and circUBE2D2 or HMGB1 was confirmed by a dual-luciferase reporter and RNA pull-down analysis. circUBE2D2′s role in vivo tumor xenograft experiment was further probed. Results: OC tissue and cell lines had higher circUBE2D2 and HMGB1 and lower miR-885-5p. Mechanically, CircUBE2D2 shared a binding relation with miR-885-5p, while miR-885-5p can directly target HMGB1. Eliminating circUBE2D2 or miR-885-5p induction inhibited OC cell activities. However, these functions were relieved by down-regulating miR-885-5p or HMGB1 induction. Furthermore, circUBE2D2 knockout reduced tumor growth. Conclusion: CircUBE2D2 regulates the expression of HMGB1 by acting as a sponge of ceRNA as miR-885-5p, thereby promoting the control of OC cell proliferation and migration and inhibiting cell apoptosis. Targeting CircUBE2D2 could serve as a new potential treatment strategy for OC.

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Published

2024-02-15

Issue

Section

Original Articles

How to Cite

Yan, R., Zeng, S., Gao, F., Li, L., & Xiao, X. (2024). CircUBE2D2 regulates HMGB1 through miR-885-5p to promote ovarian cancer malignancy. Clinics, 79, 100391. https://doi.org/10.1016/