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miR-193a-3p regulates the multi-drug resistance of bladder cancer by targeting the LOXL4 gene and the Oxidative Stress pathway

机译:miR-193a-3p通过靶向LOXL4基因和氧化应激途径来调节膀胱癌的多药耐药性

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Background Chemoresistance is a major obstacle to the curative cancer chemotherapy and presents one of the most formidable challenges in both research and management of cancer. Results From the detailed studies of a multi-chemosensitive (5637) versus a chemoresistant (H-bc) bladder cancer cell lines, we showed that miR-193a-3p [GenBank: NR_029710.1] promotes the multi-chemoresistance of bladder cancer cells. We further demonstrated that lysyl oxidase-like 4 (LOXL4) gene [GenBank: NM_032211.6] is a direct target of miR-193a-3p and executes the former’s impact on bladder cancer chemoresistance. The Oxidative Stress pathway activity is drastically affected by a forced reversal of miR-193a-3p or LOXL4 levels in cell and may act at the downstream of LOXL4 gene to relay the miR-193a-3p’s impact on the multi-chemoresistance in both cultured cells and the tumor xenografts in nude mice. Conclusions In addition to a new mechanistic insight, our results provide a set of the essential genes in this newly identified miR-193a-3p/LOXL4/Oxidative Stress axis as the diagnostic targets for a guided anti-bladder cancer chemotherapy.
机译:背景化学抗性是治愈性癌症化学疗法的主要障碍,并且在癌症的研究和管理中提出了最严峻的挑战之一。结果通过对多化学敏感性(5637)与化学抗性(H-bc)膀胱癌细胞系进行的详细研究,我们显示miR-193a-3p [GenBank:NR_029710.1]促进了膀胱癌细胞的多化学耐药性。我们进一步证明,赖氨酰氧化酶样4(LOXL4)基因[GenBank:NM_032211.6]是miR-193a-3p的直接靶标,并执行前者对膀胱癌化学耐药性的影响。氧化应激途径的活性受细胞中miR-193a-3p或LOXL4水平的强制逆转的剧烈影响,并且可能在LOXL4基因的下游起作用,以传递miR-193a-3p对两种培养细胞中多化学耐药性的影响和裸鼠体内的肿瘤异种移植。结论除了获得新的机制洞察力外,我们的结果还提供了这一新鉴定的miR-193a-3p / LOXL4 /氧化应激轴中的一组必需基因,作为指导性抗膀胱癌化学疗法的诊断目标。

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