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Frequent MYC coamplification and DNA hypomethylation of multiple genes on 8q in 8p11-p12-amplified breast carcinomas

机译:在8p11-p12扩增的乳腺癌中频繁进行MYC共扩增和8q上多个基因的DNA低甲基化

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摘要

Genetic and epigenetic (DNA methylation, histone modifications, microRNA expression) crosstalk promotes inactivation of tumor suppressor genes or activation of oncogenes by gene loss/hypermethylation or duplications/hypomethylation, respectively. The 8p11-p12 chromosomal region is a hotspot for genomic aberrations (chromosomal rearrangements, amplifications and deletions) in several cancer forms, including breast carcinoma where amplification has been associated with increased proliferation rates and reduced patient survival. Here, an integrative genomics screen (DNA copy number, transcriptional and DNA methylation profiling) performed in 229 primary invasive breast carcinomas identified substantial coamplification of the 8p11-p12 genomic region and the MYC oncogene (8q24.21), as well as aberrant methylation and transcriptional patterns for several genes spanning the 8q12.1-q24.22 genomic region (ENPP2, FABP5, IMPAD1, NDRG1, PLEKHF2, RRM2B, SQLE, TAF2, TATDN1, TRPS1, VPS13B). Taken together, our findings suggest that MYC activity and aberrant DNA methylation may also have a pivotal role in the aggressive tumor phenotype frequently observed in breast carcinomas harboring 8p11-p12 regional amplification.
机译:遗传和表观遗传(DNA甲基化,组蛋白修饰,microRNA表达)串扰分别通过基因丢失/超甲基化或重复/低甲基化促进肿瘤抑制基因的失活或癌基因的激活。 8p11-p12染色体区域是几种癌症形式(包括乳腺癌)中的基因组畸变(染色体重排,扩增和缺失)的热点,其中扩增与增殖率增加和患者存活率降低相关。在这里,在229例原发性浸润性乳腺癌中进行的综合基因组学筛选(DNA拷贝数,转录和DNA甲基化图谱)确定了8p11-p12基因组区域和MYC癌基因(8q24.21)的大量共扩增,以及异常的甲基化和跨越8q12.1-q24.22基因组区域的几个基因(ENPP2,FABP5,IMPAD1,NDRG1,PLEKHF2,RRM2B,SQLE,TAF2,TATDN1,TRPS1,VPS13B)的转录模式。两者合计,我们的发现表明,MYC活性和异常的DNA甲基化也可能在具有8p11-p12区域扩增的乳腺癌中经常观察到的侵袭性肿瘤表型中起关键作用。

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