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Association of imputed prostate cancer transcriptome with disease risk reveals novel mechanisms

机译:随着疾病风险的算前列腺癌转录组的关联揭示了新的机制

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Here we train cis-regulatory models of prostate tissue gene expression and impute expression transcriptome-wide for 233,955 European ancestry men (14,616 prostate cancer (PrCa) cases, 219,339 controls) from two large cohorts. Among 12,014 genes evaluated in the UK Biobank, we identify 38 associated with PrCa, many replicating in the Kaiser Permanente RPGEH. We report the association of elevated TMPRSS2 expression with increased PrCa risk (independent of a previously-reported risk variant) and with increased tumoral expression of the TMPRSS2:ERG fusion-oncogene in The Cancer Genome Atlas, suggesting a novel germline-somatic interaction mechanism. Three novel genes, HOXA4, KLK1, and TIMM23, additionally replicate in the RPGEH cohort. Furthermore, 4 genes, MSMB, NCOA4, PCAT1, and PPP1R14A, are associated with PrCa in a trans-ethnic meta-analysis (N?=?9117). Many genes exhibit evidence for allele-specific transcriptional activation by PrCa master-regulators (including androgen receptor) in Position Weight Matrix, Chip-Seq, and Hi-C experimental data, suggesting common regulatory mechanisms for the associated genes.
机译:在这里,我们培养Quostate组织基因表达的顺式调节模型,并赋予两种欧洲血统男性的233,955名欧洲血统男性(14,616名前列腺癌(PRCA)案例,219,339次控制)。在英国Biobank评估的12,014个基因中,我们鉴定了与PRCA相关的38个,许多在Kaiser Permanente RPGEH中复制。我们报告了升高的TMPRSS2表达的关联,增加了PRCA风险(独立于先前报告的风险变体),并且随着TMPRSS2的肿瘤表达增加:ERG融合在癌症基因组Atlas中的肿瘤表达,表明一种新的种系 - 体细胞相互作用机制。三个新型基因,Hoxa4,Klk1和TimM23另外在RPGEH队列中复制。此外,4个基因,MSMB,NCOA4,PCAT1和PPP1R14A与在反式族元分析中的PRCA相关(N?= 9117)。许多基因表现出由PRCA母体调节剂(包括雄激素受体)在适当重量基质,芯片-SEQ和HI-C实验数据中的等位基因特异性转录激活的证据,这表明相关基因的共同调节机制。

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