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Dysregulation of miRNAs-COUP-TFII-FOXM1-CENPF axis contributes to the metastasis of prostate cancer

机译:miRNAs-COUP-TFII-FOXM1-CENPF轴的失调有助于前列腺癌的转移

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摘要

Although early detection and treatment of prostate cancer (PCa) improves outcomes, many patients still die of metastatic PCa. Here, we report that metastatic PCa exhibits reduced levels of the microRNAsmiR-101 and miR-27a. These micro-RNAs (miRNAs) negatively regulate cell invasion and inhibit the expression of FOXM1 and CENPF, two master regulators of metastasis in PCa. Interestingly, the repression of FOXM1 and CENPF by these miRNAs occurs through COUP-TFII, a member of the orphan nuclear receptors family. Loss of miR-101 positively correlates with the increase of COUP-TFII-FOXM1-CENPF activity in clinical PCa data sets, implicating clinical relevance of such regulation. Further studies show that COUP-TFII is a critical factor controlling metastatic gene networks to promote PCa metastasis. Most importantly, this miRNA-COUP-TFII-FOXM1-CENPF regulatory axis is also involved in the development of enzalutaminde resistance. Taken together, our findings highlight the contribution of specific miRNAs through the regulation of the COUP-TFII-FOXM1-CENPF cascade in PCa metastasis and drug resistance.
机译:尽管早期检测和治疗前列腺癌(PCa)可以改善结局,但许多患者仍死于转移性PCa。在这里,我们报告转移性PCa表现出降低的microRNAsmiR-101和miR-27a水平。这些微RNA(miRNA)负调控细胞侵袭并抑制FOXM1和CENPF(PCa中两个主要的转移转移调节剂)的表达。有趣的是,这些miRNA抑制FOXM1和CENPF的过程是通过孤儿核受体家族成员COUP-TFII进行的。在临床PCa数据集中,miR-101的丢失与COUP-TFII-FOXM1-CENPF活性的增加呈正相关,这暗示了这种调节的临床意义。进一步的研究表明,COUP-TFII是控制转移性基因网络促进PCa转移的关键因素。最重要的是,这个miRNA-COUP-TFII-FOXM1-CENPF调控轴也参与了恩杂胺抗性的发展。综上所述,我们的发现突出了特定的miRNA通过调节COUP-TFII-FOXM1-CENPF级联在PCa转移和耐药中的作用。

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