Circular RNA hsa_circ_0000282 contributes to osteosarcoma cell proliferation by regulating miR-192/XIAP axis
作者: Houkun Li , Limin He , Yuan Tuo , Yansheng Huang , Bing Qian
DOI: 10.1186/S12885-020-07515-8
关键词: XIAP 、 Cell growth 、 Flow cytometry 、 Cancer research 、 Gene expression 、 Gene knockdown 、 Chemistry 、 Circular RNA 、 Apoptosis 、 Inhibitor of apoptosis 、 Genetics 、 Oncology
摘要: Background Circular RNAs (circRNAs) have emerged as a novel category of non-coding RNA, which exhibit a pivotal effect on regulating gene expression and biological functions, yet how circRNAs function in osteosarcoma (OSA) still demands further investigation. This study aimed at probing into the function of hsa_circ_0000282 in OSA. Methods The expressions of circ_0000282 and miR-192 in OSA tissues and cell lines were examined by quantitative real-time polymerase chain reaction (qRT-PCR), and the correlation between the expression level of circ_0000282 and clinicopathological features of OSA patients was analyzed. The expressions of X-linked inhibitor of apoptosis protein (XIAP), B-cell lymphoma-2 (Bcl-2) and Bcl-2 associated X protein (Bax) in OSA cells were assayed by Western blot. The proliferation and apoptosis of OSA cells were examined by CCK-8, BrdU and flow cytometry, respectively. Bioinformatics analysis, dual-luciferase reporter gene assay and RIP experiments were employed to predict and validate the targeting relationships between circ_0000282 and miR-192, and between miR-192 and XIAP, respectively. Results Circ_0000282 was highly expressed in OSA tissues and cell lines, which represented positive correlation with Enneking stage of OSA patients and negative correlation with tumor differentiation degree. In vitro experiments confirmed that overexpression of circ_0000282 markedly facilitated OSA cell proliferation and repressed cancer cell apoptosis in comparison to control group. Besides, knockdown of circ_0000282 repressed OSA cell proliferation and promoted apoptosis. Additionally, the binding relationships between circ_0000282 and miR-192, and between miR-192 and XIAP were validated. Circ_0000282 indirectly up-regulated XIAP expression by adsorbing miR-192, thereby playing a role in promoting cancer in OSA. Conclusion Circ_0000282 was a novel oncogenic circRNA in OSA. Circ_0000282/miR-192/XIAP axis regulated OSA cell proliferation apoptosis with competitive endogenous RNA mechanism.
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Jian-Gang Shi, Lian-Shun Jia, Ke-Fu Cheng, Zhao Wu, Hai-Bo Wang, Tao Xu, Yuan Wang, Wen Yuan, Jing-Chuan Sun, Low miR-34a and miR-192 are associated with unfavorable prognosis in patients suffering from osteosarcoma. American Journal of Translational Research. ,vol. 7, pp. 111- 119 ,(2015)
S Galbán, C S Duckett, XIAP as a ubiquitin ligase in cellular signaling Cell Death & Differentiation. ,vol. 17, pp. 54- 60 ,(2010) , 10.1038/CDD.2009.81
A D Schimmer, S Dalili, R A Batey, S J Riedl, Targeting XIAP for the treatment of malignancy Cell Death & Differentiation. ,vol. 13, pp. 179- 188 ,(2006) , 10.1038/SJ.CDD.4401826
YANG QU, PENG XIA, SHANYONG ZHANG, SU PAN, JIANWU ZHAO, Silencing XIAP suppresses osteosarcoma cell growth, and enhances the sensitivity of osteosarcoma cells to doxorubicin and cisplatin. Oncology Reports. ,vol. 33, pp. 1177- 1184 ,(2015) , 10.3892/OR.2014.3698
Michael S. Isakoff, Stefan S. Bielack, Paul Meltzer, Richard Gorlick, Osteosarcoma: Current Treatment and a Collaborative Pathway to Success Journal of Clinical Oncology. ,vol. 33, pp. 3029- 3035 ,(2015) , 10.1200/JCO.2014.59.4895
Fang Lin, Ghita Ghislat, Shouqing Luo, Maurizio Renna, Farah Siddiqi, David C. Rubinsztein, XIAP and cIAP1 amplifications induce Beclin 1-dependent autophagy through NFκB activation Human Molecular Genetics. ,vol. 24, pp. 2899- 2913 ,(2015) , 10.1093/HMG/DDV052
Steven P. Barrett, Julia Salzman, Circular RNAs: analysis, expression and potential functions Development. ,vol. 143, pp. 1838- 1847 ,(2016) , 10.1242/DEV.128074
Leo Kager, Gevorg Tamamyan, Stefan Bielack, Novel insights and therapeutic interventions for pediatric osteosarcoma Future Oncology. ,vol. 13, pp. 357- 368 ,(2017) , 10.2217/FON-2016-0261
Hongya Guan, Xinjie Li, Yuebai Li, Yisheng Wang, Yadong Wang, Shanfeng Zhang, Yan Xu, Yan Zhang, Upregulation of miR-192 inhibits cell growth and invasion and induces cell apoptosis by targeting TCF7 in human osteosarcoma Tumor Biology. ,vol. 37, pp. 15211- 15220 ,(2016) , 10.1007/S13277-016-5417-Z
Hannah K. Brown, Marta Tellez-Gabriel, Dominique Heymann, Cancer stem cells in osteosarcoma Cancer Letters. ,vol. 386, pp. 189- 195 ,(2017) , 10.1016/J.CANLET.2016.11.019