MicroRNAâ29a enhances cisplatin sensitivity in nonâsmall cell lung cancer through the regulation of REV3L.
[No authors listed]
摘要
Cisplatinâbased chemotherapy may greatly enhance patient prognosis; however, chemotherapy resistance remains an obstacle to curing patients with nonâsmall cell lung cancer (NSCLC). The aim of the present study was to explore the microRNAs (miRs) that could regulate cisplatin sensitivity and provide a potential treatment method for cisplatin resistance in clinical. Results from the present study revealed that miRâ29a overexpression enhanced and miRâ29a inhibition reduced the sensitivity of two NSCLC cell lines, A549 and H1650, to cisplatin treatment. In addition, reduced miRâ29a expression levels were observed in cisplatinâresistant A549 cells (A549rCDDP), and increased expression of miRâ29a augmented cisplatinâinduced inhibition of proliferation and apoptosis in A549rCDDP cells. These data indicated that miRâ29a expression may be involved in the development of cisplatin resistance. miRâ29a was revealed to negatively regulate REV3âlike DNAâdirected polymerase ζ catalytic subunit (REV3L) expression in both A549 and H1650 cells; elevated expression of REV3L in A549rCDDP cells was also detected. REV3L encodes the catalytic subunit of DNA polymerase ζ and was hypothesized, based on results from the online tool TargetScan 7.1, to be a target gene of miRâ29a; this was confirmed with a dual luciferase assay. Cells treated with a very low concentration of cisplatin exhibited a significant reduction in proliferation and cell cycle arrest at the G2/M phase in REV3Lâknockdown as well as in miRâ29aâupregulated A549 cells. Notably, reduced miRâ29a expression and an increase in REV3L mRNA expression were observed in tumor tissues from patients with NSCLC. Additionally, a negative correlation between miRâ29a and REV3L mRNA expression levels in tumor tissues from patients with NSCLC was observed; low expression of miRâ29a and high expression of REV3L were closely associated with an advanced tumorânodeâmetastasis classification. The results of the present study suggested a pivotal role of miRâ29a in mediating NSCLC cell sensitivity towards cisplatin through the regulation of REV3L.
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基因功能
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原始数据
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文献解读
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