Circ_0000140 Alters miR-527/SLC7A11-Mediated Ferroptosis to Influence Oral Squamous Cell Carcinoma Cell Resistance to DDP

Yu Ma, Jinbo Gao, Hongning Guo
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Abstract

Background: While there is prior evidence for the ability of circular RNAs (circRNAs) to shape the cisplatin (DDP) resistance of cancers in human patients, there has been relatively little research to date focused on the interplay between circRNAs and DDP resistance in the context of OSCC progression to date. In the present analysis, the functional role that circ_0000140 plays as a mediator of chemoresistance to DDP was thus explored in greater detail.
Methods: Both qPCR and Western immunoblotting were employed as appropriate to detect circ_0000140, miR-527, and SLC7A11 levels, while interactions among these factors were detected through RNA immunoprecipitation, RNA pull-down, and dual luciferase report assays. MTT assays were used to assess cellular viability as a means of gauging DDP sensitivity.
Results: Both tissue samples from DDP-resistant OSCC patient tumors and OSCC cell lines resistant to DDP exhibited pronounced circ_0000140 upregulation. Knocking down this circRNA significantly increased the DDP sensitivity of both tested DDP-resistant OSCC cell lines and promoted ferroptosis, whereas knocking down miR-527 was sufficient to reverse these effects, which were recapitulated by miR-527 overexpression. Conversely, the effects of overexpressing miR-527 were reversed by the restoration of SLC7A11 expression. Consistently, this circRNA was able to increase DDP IC50 values and to suppress ferroptosis in both tested cell lines through this miR-527/SLC7A11 signaling axis.
Conclusion: These results revealed that circ_0000140/miR-527/SLC7A11-mediated ferroptosis may provide novel insights into the development of this cancer type and the emergence of chemoresistance in the future.

Circ_0000140 可改变 miR-527/SLC7A11 介导的铁突变,从而影响口腔鳞状细胞癌细胞对 DDP 的耐受性
背景:尽管已有证据表明环状RNA(circRNA)能够影响人类癌症患者的顺铂(DDP)耐药性,但迄今为止,关于环状RNA与OSCC进展背景下DDP耐药性之间相互作用的研究相对较少。在本分析中,我们更详细地探讨了circ_0000140作为DDP化疗耐药性介质的功能作用:方法:采用 qPCR 和 Western 免疫印迹法检测 circ_0000140、miR-527 和 SLC7A11 的水平,同时通过 RNA 免疫沉淀、RNA 拉取和双荧光素酶报告检测这些因子之间的相互作用。MTT测定用于评估细胞活力,作为衡量DDP敏感性的一种手段:结果:对DDP耐药的OSCC患者肿瘤组织样本和对DDP耐药的OSCC细胞系均表现出明显的circ_0000140上调。敲除该circRNA可显著提高两种耐DDP OSCC细胞系的DDP敏感性并促进铁变态反应,而敲除miR-527足以逆转这些效应,miR-527的过表达可再现这些效应。相反,恢复 SLC7A11 的表达可逆转过表达 miR-527 的影响。一致的是,该circRNA能够通过miR-527/SLC7A11信号轴增加DDP IC50值并抑制两种测试细胞系的铁突变:这些结果表明,circ_0000140/miR-527/SLC7A11介导的铁突变可能为该癌症类型的发展和未来化疗耐药性的出现提供了新的见解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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