中介激酶 CDK8/CDK19 驱动 YAP1 依赖性 BMP4 诱导的癌症 EMT。
Mediator kinase CDK8/CDK19 drives YAP1-dependent BMP4-induced EMT in cancer.
机构信息
Department of Chemistry and Biochemistry, University of South Carolina, Columbia, SC, USA.
Department of Drug Discovery and Biomedical Sciences, University of South Carolina, Columbia, SC, USA.
出版信息
Oncogene. 2018 Aug;37(35):4792-4808. doi: 10.1038/s41388-018-0316-y. Epub 2018 May 21.
CDK8 is a transcription-regulating kinase that controls TGF-β/BMP-responsive SMAD transcriptional activation and turnover through YAP1 recruitment. However, how the CDK8/YAP1 pathway influences SMAD1 response in cancer remains unclear. Here we report that SMAD1-driven epithelial-to-mesenchymal transition (EMT) is critically dependent on matrix rigidity and YAP1 in a wide spectrum of cancer models. We find that both genetic and pharmacological inhibition of CDK8 and its homologous twin kinase CDK19 leads to abrogation of BMP-induced EMT. Notably, selectively blocking CDK8/19 specifically abrogates tumor cell invasion, changes in EMT-associated transcription factors, E-cadherin expression and YAP nuclear localization both in vitro and in vivo in a murine syngeneic EMT model. Furthermore, RNA-seq meta-analysis reveals a direct correlation between CDK8 and EMT-associated transcription factors in patients. Our findings demonstrate that CDK8, an emerging therapeutic target, coordinates growth factor and mechanical cues during EMT and invasion.
CDK8 是一种转录调节激酶,通过招募 YAP1 来控制 TGF-β/BMP 反应性 SMAD 转录激活和周转。然而,CDK8/YAP1 通路如何影响癌症中的 SMAD1 反应尚不清楚。在这里,我们报告在广泛的癌症模型中,SMAD1 驱动的上皮-间充质转化 (EMT) 严重依赖于基质刚度和 YAP1。我们发现,遗传和药理学抑制 CDK8 及其同源双激酶 CDK19 都会导致 BMP 诱导的 EMT 丧失。值得注意的是,选择性阻断 CDK8/19 特异性地阻断了肿瘤细胞的侵袭,改变了 EMT 相关转录因子、E-钙粘蛋白表达和 YAP 核定位,无论是在体外还是在体内的鼠同源 EMT 模型中。此外,RNA-seq 荟萃分析显示 CDK8 与患者 EMT 相关转录因子之间存在直接相关性。我们的研究结果表明,CDK8 作为一个新兴的治疗靶点,在 EMT 和侵袭过程中协调生长因子和机械线索。
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