Gaozhong Sun, Kewei Ni, Jian Shen, Dongdong Liu, Haitao Wang
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引用次数: 0
摘要
肺腺癌(LUAD)严重影响人类健康,顺铂(DDP)耐药是LUAD治疗的主要障碍,其机制尚不清楚。利用生物信息学方法预测了AURKB在LUAD组织中的表达和相关通路,以及上游调控的microRNA。RIP 和双荧光素酶实验验证了这两个基因之间的结合和相互作用。CCK-8 用于检测细胞增殖能力和 IC50 值。流式细胞仪用于评估细胞周期。彗星试验和 Western 印迹分别检测 DNA 损伤和 γ-H2AX 蛋白表达。在 LUAD 中,AURKB 上调,但 microRNA-486-5p 下调。RIP和双荧光素酶实验证实了两者之间的靶向关系。细胞实验表明,敲除 AURKB 会抑制细胞增殖,降低 IC50 值,诱导细胞周期停滞,并造成 DNA 损伤。microRNA-486-5p通过靶向AURKB调控DNA损伤以抑制LUAD的DDP耐药,这意味着microRNA-486-5p/AURKB轴可能是LUAD患者DDP耐药的治疗靶点。
microRNA-486-5p Regulates DNA Damage Inhibition and Cisplatin Resistance in Lung Adenocarcinoma by Targeting AURKB.
Lung adenocarcinoma (LUAD) severely affects human health, and cisplatin (DDP) resistance is the main obstacle in LUAD treatment, the mechanism of which is unknown. Bioinformatics methods were utilized to predict expression and related pathways of AURKB in LUAD tissues, as well as the upstream regulated microRNAs. qRT-PCR assayed expression of AURKB and microRNA-486-5p. RIP and dual-luciferase experiments verified the binding and interaction between the two genes. CCK-8 was used to detect cell proliferation ability and IC50 values. Flow cytometry was utilized to assess the cell cycle. Comet assay and western blot tested DNA damage and γ-H2AX protein expression, respectively. In LUAD, AURKB was upregulated, but microRNA-486-5p was downregulated. The targeted relationship between the two was confirmed by RIP and dual-luciferase experiments. Cell experiments showed that AURKB knock-down inhibited cell proliferation, reduced IC50 values, induced cell cycle arrest, and caused DNA damage. The rescue experiment presented that high expression of microRNA-486-5p could weaken the impact of AURKB overexpression on LUAD cell behavior and DDP resistance. microRNA-486-5p regulated DNA damage to inhibit DDP resistance in LUAD by targeting AURKB, implying that microRNA-486-5p/AURKB axis may be a possible therapeutic target for DDP resistance in LUAD patients.
期刊介绍:
Critical ReviewsTM in Eukaryotic Gene Expression presents timely concepts and experimental approaches that are contributing to rapid advances in our mechanistic understanding of gene regulation, organization, and structure within the contexts of biological control and the diagnosis/treatment of disease. The journal provides in-depth critical reviews, on well-defined topics of immediate interest, written by recognized specialists in the field. Extensive literature citations provide a comprehensive information resource.
Reviews are developed from an historical perspective and suggest directions that can be anticipated. Strengths as well as limitations of methodologies and experimental strategies are considered.