Pan-cancer genomic analysis reveals FOXA1 amplification is associated with adverse outcomes in non-small cell lung, prostate, and breast cancers.

Alexander G Goglia,Mohammed Alshalalfa,Anwar Khan,Danielle R Isakov,Helen Y Hougen,Nishwant Swami,Jasmine Kannikal,Sean M Mcbride,Daniel R Gomez,Sanoj Punnen,Paul L Nguyen,Puneeth Iyengar,Emmanuel S Antonarakis,Brandon A Mahal,Edward Christopher Dee
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Abstract

INTRODUCTION Alterations in forkhead box A1 (FOXA1), a pioneer transcription factor, are associated with poor prognosis in breast cancer (BC) and prostate cancer (PC). We characterized FOXA1 genomic alterations and their clinical impacts in a large pan-cancer cohort from the AACR GENIE database. METHODS FOXA1 alterations were characterized across >87,000 samples from >30 cancer types for primary and metastatic tumors alongside patient characteristics and clinical outcomes. FOXA1 alterations were queried in the MSK-MET cohort (a GENIE subset), allowing definition of hazard ratios (HRs) and survival estimates based on Cox proportional hazard models. RESULTS FOXA1 was altered in 1,869 samples (2.1%), with distinct patterns across different cancers: PC enriched with indel-inframe alterations, BC with missense mutations, and lung cancers with copy number (CN) amplifications.Of 74,715 samples with FOXA1 CN profiles, amplification was detected in 834 (1.1%). Amplification was most common in non-small cell lung cancer (NSCLC, 3% in primary; 6% in metastatic) and small cell lung cancer (4.1% primary; 3.5% metastatic), followed by BC (2% primary; 1.6% metastatic) and PC (2.2% primary; 1.6% metastatic).CN amplifications were associated with decreased overall survival in NSCLC (HR: 1.45, 95%CI: 1.06-1.99, p = .02), BC (HR: 3.04, 95%CI: 1.89-4.89, p = 4e-6), and PC (HR: 1.94, 95%CI: 1.03-3.68, p = .04). Amplifications were associated with wide-spread metastases in NSCLC, BC, and PC. CONCLUSIONS FOXA1 demonstrates distinct alteration profiles across cancer sites. Our findings suggest an association between FOXA1 amplification and both enhanced metastatic potential and decreased survival, highlighting prognostic and therapeutic potential in breast cancer, prostate cancer, and NSCLC.
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泛癌症基因组分析显示,FOXA1扩增与非小细胞肺癌、前列腺癌和乳腺癌的不良预后有关。
简介叉头盒 A1(FOXA1)是一种先驱转录因子,它的改变与乳腺癌(BC)和前列腺癌(PC)的不良预后有关。我们从 AACR GENIE 数据库的大型泛癌症队列中鉴定了 FOXA1 基因组的改变及其临床影响。对 MSK-MET 队列(GENIE 子集)中的 FOXA1 改变进行了查询,从而根据 Cox 比例危险模型定义了危险比(HRs)和生存估计值:在74,715个具有FOXA1 CN图谱的样本中,有834个样本(1.1%)检测到扩增。扩增最常见于非小细胞肺癌(NSCLC,原发占 3%;转移占 6%)和小细胞肺癌(原发占 4.1%;转移占 3.5%),其次是 BC(原发占 2%;转移占 1.6%)和 PC(原发占 2.2%;转移占 1.6%)。在NSCLC(HR:1.45,95%CI:1.06-1.99,p = .02)、BC(HR:3.04,95%CI:1.89-4.89,p = 4e-6)和PC(HR:1.94,95%CI:1.03-3.68,p = .04)中,CN扩增与总生存率下降相关。)扩增与 NSCLC、BC 和 PC 的广泛转移有关。我们的研究结果表明,FOXA1扩增与转移潜能增强和生存率降低有关,突出了乳腺癌、前列腺癌和NSCLC的预后和治疗潜力。
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