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首页> 外文期刊>Carcinogenesis >MicroRNA-191, an estrogen-responsive microRNA, functions as an oncogenic regulator in human breast cancer
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MicroRNA-191, an estrogen-responsive microRNA, functions as an oncogenic regulator in human breast cancer

机译:MicroRNA-191是一种雌激素反应性microRNA,在人类乳腺癌中起致癌调节剂的作用

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Estrogen- and microRNA-mediated gene regulation play a crucial role in breast cancer biology. However, a functional link between the two major players remains unclear. This study reveals miR- 191 as an estrogen-inducible onco-miR in breast cancer, which promotes several hallmarks of cancer including enhanced cell proliferation, migration, chemoresistance and survival in tumor microenvironment. miR-191 is a direct estrogen receptor (ER) target and our results suggest existence of a positive regulatory feedback loop. We show miR-191 as critical mediator of estrogen- mediated cell proliferation. Investigations of mechanistic details of miR-191 functions identify several cancer-related genes like BDNF, CDK6 and SATB1 as miR-191 targets. miR-191 and SATB1 show inverse correlation of expression. miR-191-mediated enhanced cell proliferation and migration are partly dependent on targeted downregulation of SATB1. Further, functional validation of estrogen:miR-191:SATB1 link suggests a cascade initiated by estrogen that induces miR-191 in ER-dependent manner to target SATB1, a global chromatin remodeler, thereby contributing to estrogen-specific gene signature to regulate genes like ANXA1, PIWIL2, CASP4, ESR1/ESR2, PLAC1 and SOCS2 involved in breast cancer progression and migration. Overall, the identification of estrogen/ER/miR-191/SATB1 cascade seems to be a significant pathway in estrogen signaling in breast cancer with miR-191 as oncogenic player.
机译:雌激素和微RNA介导的基因调控在乳腺癌生物学中起着至关重要的作用。但是,两个主要参与者之间的功能联系仍然不清楚。这项研究揭示了miR-191在乳腺癌中是雌激素诱导的onco-miR,它促进了癌症的几个标志,包括增强的细胞增殖,迁移,化学抗性和在肿瘤微环境中的存活。 miR-191是直接雌激素受体(ER)的靶标,我们的结果表明存在正调节反馈回路。我们显示miR-191是雌激素介导的细胞增殖的关键介质。对miR-191功能的机械细节的研究确定了几种与癌症相关的基因,如BDNF,CDK6和SATB1,是miR-191的靶标。 miR-191和SATB1显示表达反相关。 miR-191介导的细胞增殖和迁移增强部分取决于SATB1的靶向下调。此外,对雌激素:miR-191:SATB1链接的功能验证表明,雌激素引发的级联反应以ER依赖性方式诱导miR-191靶向全球染色质重塑剂SATB1,从而促进了雌激素特异性基因签名,从而调控类似ANXA1,PIWIL2,CASP4,ESR1 / ESR2,PLAC1和SOCS2与乳腺癌的进展和迁移有关。总体而言,雌激素/ ER / miR-191 / SATB1级联的鉴定似乎是乳腺癌中雌激素信号传导的重要途径,而miR-191是致癌物。

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