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The DNA methylation-regulated miR-193a-3p dictates the multi-chemoresistance of bladder cancer via repression of SRSF2/PLAU/HIC2 expression

机译:DNA甲基化调节的miR-193a-3p通过抑制SRSF2 / PLAU / HIC2表达来指示膀胱癌的多化学耐药性

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摘要

Chemoresistance hinders the curative cancer chemotherapy. To define the role of the DNA methylation-regulated microRNA (miR) genes in the chemoresistance of bladder cancer, we performed both DNA methylomic and miRomic analyses of a multi-chemosensitive (5637) versus a multi-chemoresistant (H-bc) cell line and found that miR-193a-3p is hypermethylated/silenced in 5637 and hypomethylated/expressed in H-bc cells. A forced reversal of its level turned around the chemoresistance in the cultured cells and the tumor xenografts in nude mice. Three of its targets: SRSF2, PLAU and HIC2, work in concert to relay the miR-193a-3p's impact on the bladder cancer chemoresistance by modulating the activities of the following five signaling pathways: DNA damage, Notch, NF-κB, Myc/Max, and Oxidative Stress. In addition to the mechanistic insights in how the newly identified miR-193a-3p/SRSF2,PLAU,HIC2/five signaling pathway axis regulates the chemoresistance of bladder cancer cells, our study provides a new set of diagnostic targets for the guided personalized chemotherapy of bladder cancer.
机译:化学抗性阻碍了治愈癌症的化学疗法。为了确定DNA甲基化调节的microRNA(miR)基因在膀胱癌化学耐药中的作用,我们对多化学敏感性(5637)与多化学抗性(H-bc)细胞系进行了DNA甲基组学和miRomic分析并且发现miR-193a-3p在5637中被高甲基化/沉默,并在H-bc细胞中低甲基化/表达。强制逆转其水平绕过培养细胞的化学抗性和裸鼠的肿瘤异种移植物。它的三个目标:SRSF2,PLAU和HIC2,通过调节以下五个信号传导途径的活性,共同传递miR-193a-3p对膀胱癌化学抗性的影响:DNA损伤,Notch,NF-κB,Myc /最大和氧化应力。除了新近鉴定出的miR-193a-3p / SRSF2,PLAU,HIC2 / 5信号通路轴如何调控膀胱癌细胞化学耐药性的机制外,我们的研究还提供了一套新的诊断靶点,用于指导个体化化疗膀胱癌。

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