HumanMethylation450K阵列鉴定的生物标志物在高风险非肌肉浸润性膀胱癌的初始诊断中预测肿瘤复发/进展

Biomarkers in cancer Pub Date : 2018-01-08 eCollection Date: 2018-01-01 DOI:10.1177/1179299X17751920

Mark O Kitchen, Richard T Bryan, Richard D Emes, Christopher J Luscombe, K K Cheng, Maurice P Zeegers, Nicholas D James, Lyndon M Gommersall, Anthony A Fryer

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引用次数: 10

摘要

背景:高风险非肌肉浸润性膀胱癌(HR-NMIBC)是一种临床不可预测的疾病。尽管有临床风险评估工具，但许多患者单独使用膀胱内治疗治疗不足，而其他患者可能通过早期根治性手术过度治疗。分子生物标志物，特别是DNA甲基化，已被报道为预测许多实体器官和血液恶性肿瘤的肿瘤/患者预后;然而，关于HR-NMIBC的报道很少，也没有使用全基因组阵列评估。因此，我们试图确定HR-NMIBC临床结果的新型DNA甲基化标记物，这些标记物可能在初始诊断时预测肿瘤行为并帮助指导患者管理。患者和方法:通过Illumina HumanMethylation450头芯片阵列和随后的亚硫酸焦磷酸测序对21例原发性原发性HR-NMIBC肿瘤进行分析。总的来说，7例在切除后1年没有复发，14例在膀胱内卡介苗后复发和/或进展。另一个独立队列的32例HR-NMIBC肿瘤(17例无复发，15例复发和/或进展，尽管卡介苗)也通过亚硫酸盐焦磷酸测序进行评估。结果:阵列分析确定了206个CpG基因座，将非复发性HR-NMIBC肿瘤与临床更具侵袭性的复发/进展肿瘤区分开来。CpG cg11850659的高甲基化和CpG cg01149192的低甲基化联合预测HR-NMIBC诊断1年内的复发和/或进展，敏感性83%，特异性79%，阳性预测值83%，阴性预测值79%。结论:这是第一个独特的HR-NMIBC肿瘤队列的全基因组DNA甲基化分析，包括已知的1年临床结果。我们的分析确定了潜在的新型表观遗传标记，可以帮助指导这种临床不可预测疾病的个体患者管理。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

HumanMethylation450K Array-Identified Biomarkers Predict Tumour Recurrence/Progression at Initial Diagnosis of High-risk Non-muscle Invasive Bladder Cancer.

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HumanMethylation450K Array-Identified Biomarkers Predict Tumour Recurrence/Progression at Initial Diagnosis of High-risk Non-muscle Invasive Bladder Cancer.

Background: High-risk non-muscle invasive bladder cancer (HR-NMIBC) is a clinically unpredictable disease. Despite clinical risk estimation tools, many patients are undertreated with intra-vesical therapies alone, whereas others may be over-treated with early radical surgery. Molecular biomarkers, particularly DNA methylation, have been reported as predictive of tumour/patient outcomes in numerous solid organ and haematologic malignancies; however, there are few reports in HR-NMIBC and none using genome-wide array assessment. We therefore sought to identify novel DNA methylation markers of HR-NMIBC clinical outcomes that might predict tumour behaviour at initial diagnosis and help guide patient management.

Patients and methods: A total of 21 primary initial diagnosis HR-NMIBC tumours were analysed by Illumina HumanMethylation450 BeadChip arrays and subsequently bisulphite Pyrosequencing. In all, 7 had not recurred at 1 year after resection and 14 had recurred and/or progressed despite intra-vesical BCG. A further independent cohort of 32 HR-NMIBC tumours (17 no recurrence and 15 recurrence and/or progression despite BCG) were also assessed by bisulphite Pyrosequencing.

Results: Array analyses identified 206 CpG loci that segregated non-recurrent HR-NMIBC tumours from clinically more aggressive recurrence/progression tumours. Hypermethylation of CpG cg11850659 and hypomethylation of CpG cg01149192 in combination predicted HR-NMIBC recurrence and/or progression within 1 year of diagnosis with 83% sensitivity, 79% specificity, and 83% positive and 79% negative predictive values.

Conclusions: This is the first genome-wide DNA methylation analysis of a unique HR-NMIBC tumour cohort encompassing known 1-year clinical outcomes. Our analyses identified potential novel epigenetic markers that could help guide individual patient management in this clinically unpredictable disease.

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Biomarkers in cancer

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