Mediator kinase module proteins, genetic alterations and expression of super-enhancer regulated genes in colorectal cancer

IF 3.6 3区 医学 Q2 PHARMACOLOGY & PHARMACY Pharmacological Reports Pub Date : 2024-04-11 DOI:10.1007/s43440-024-00589-2
Ioannis A. Voutsadakis
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Abstract

Background

Genetic alterations are well characterized as contributors to the pathogenesis of cancers. Epigenetic abnormalities can lead to perturbations of the expression of genes in cancer cells without structural defects. Deregulation of proteins of the transcription machinery may result in perturbations of target genes. Mediator, a multiprotein component of the transcription machinery facilitates the function of RNA polymerase II, which transcribes most human genes. A part of the mediator with kinase activity, called the Mediator kinase module shows genetic alterations in a sub-set of colorectal cancers.

Methods

Data from publicly available genomic series of colorectal cancer patients were examined to determine alterations of Mediator kinase module component genes, including MED12, MED12L, MED13, MED13L, CDK8, CDK19, and CCNC. The prevalence of alterations in genomically defined colorectal cancer sub-sets was also interrogated. The effect of Mediator kinase module member gene expression on colorectal cancer relapse-free survival was investigated.

Results

Mutations in genes of the Mediator kinase module were present in a small percentage of colorectal cancers, ranging between 2 to 10% for MED12 and MED13 and alternative units MED12L and MED13L and below 2% for kinases CDK8 and CDK19 and cyclin C. Amplifications of the CDK8 gene were observed in 3% to 5% of colorectal cancers. The highest prevalence of mutations was observed in MSI cancers and the equivalent CMS1 group, with other genomic groups showing much lower frequency. An association of higher expression of MED12 with inferior relapse-free survival was observed. In contrast, higher expression of cyclin C was associated with improved survival. Colorectal cancer cell lines with CDK8 amplifications displayed sensitivity to several small molecule inhibitors of the KRAS/PI3K pathway but not to BET inhibitors.

Conclusion

The Mediator kinase module is deregulated in a sub-set of colorectal cancers with differences observed in genomically defined groups. These variations may result in differences in sensitivity to targeted therapies and may have to be taken into consideration as such therapies are developed.

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大肠癌中的介导激酶模块蛋白、基因改变和超级增强子调控基因的表达
背景基因改变是导致癌症发病的重要因素。表观遗传学异常可导致癌细胞中基因的表达发生紊乱,而不存在结构缺陷。转录机制蛋白的失调可能会导致靶基因的紊乱。中间体是转录机制中的一种多蛋白成分,可促进 RNA 聚合酶 II 的功能,而 RNA 聚合酶 II 可转录大多数人类基因。方法研究了公开的结直肠癌患者基因组系列数据,以确定MED12、MED12L、MED13、MED13L、CDK8、CDK19和CCNC等Mediator激酶模块组成基因的改变。研究人员还调查了基因组学定义的结直肠癌亚组中基因改变的发生率。结果在小部分结直肠癌中存在Mediator激酶模块基因的突变,MED12和MED13以及替代单位MED12L和MED13L的突变率在2%到10%之间,激酶CDK8、CDK19和细胞周期蛋白C的突变率低于2%。在 MSI 癌症和相当于 CMS1 的组别中观察到的突变发生率最高,其他基因组组别的发生率要低得多。研究发现,MED12表达较高与无复发生存率较低有关。相反,细胞周期蛋白 C 的高表达与生存率的提高有关。CDK8扩增的结直肠癌细胞系对KRAS/PI3K通路的几种小分子抑制剂敏感,但对BET抑制剂不敏感。这些差异可能导致对靶向疗法的敏感性不同,因此在开发此类疗法时必须加以考虑。
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来源期刊
Pharmacological Reports
Pharmacological Reports 医学-药学
CiteScore
8.40
自引率
0.00%
发文量
91
审稿时长
6 months
期刊介绍: Pharmacological Reports publishes articles concerning all aspects of pharmacology, dealing with the action of drugs at a cellular and molecular level, and papers on the relationship between molecular structure and biological activity as well as reports on compounds with well-defined chemical structures. Pharmacological Reports is an open forum to disseminate recent developments in: pharmacology, behavioural brain research, evidence-based complementary biochemical pharmacology, medicinal chemistry and biochemistry, drug discovery, neuro-psychopharmacology and biological psychiatry, neuroscience and neuropharmacology, cellular and molecular neuroscience, molecular biology, cell biology, toxicology. Studies of plant extracts are not suitable for Pharmacological Reports.
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