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首页> 外文期刊>Nature Communications >Multi-omics profiling of younger Asian breast cancers reveals distinctive molecular signatures
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Multi-omics profiling of younger Asian breast cancers reveals distinctive molecular signatures

机译:亚洲年轻乳腺癌的多组学分析揭示了独特的分子特征

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摘要

Breast cancer (BC) in the Asia Pacific regions is enriched in younger patients and rapidly rising in incidence yet its molecular bases remain poorly characterized. Here we analyze the whole exomes and transcriptomes of 187 primary tumors from a Korean BC cohort (SMC) enriched in pre-menopausal patients and perform systematic comparison with a primarily Caucasian and post-menopausal BC cohort (TCGA). SMC harbors higher proportions of HER2+ and Luminal B subtypes, lower proportion of Luminal A with decreased ESR1 expression compared to TCGA. We also observe increased mutation prevalence affecting BRCA1, BRCA2, and TP53 in SMC with an enrichment of a mutation signature linked to homologous recombination repair deficiency in TNBC. Finally, virtual microdissection and multivariate analyses reveal that Korean BC status is independently associated with increased TIL and decreased TGF-β signaling expression signatures, suggesting that younger Asian BCs harbor more immune-active microenvironment than western BCs.
机译:亚太地区的乳腺癌(BC)在年轻患者中富集,发病率迅速上升,但其分子基础仍然不佳。在这里,我们分析了来自绝经前患者丰富的韩国BC队列(SMC)的187例原发肿瘤的整个外显子组和转录组,并与主要是白种人和绝经后BC队列(TCGA)进行了系统比较。与TCGA相比,SMC具有较高比例的HER2 +和Luminal B亚型,较低比例的Luminal A具有降低的ESR1表达。我们还观察到影响BRCA1,BRCA2和TP53的SMC中突变发生率增加,且突变签名的丰富与TNBC中的同源重组修复缺陷有关。最后,虚拟显微解剖和多变量分析表明,韩国BC的状态与TIL的增加和TGF-β信号表达表达特征的降低是独立相关的,这表明年轻的BC较西方BC具有更多的免疫活性微环境。

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