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CpG 岛甲基化表型在神经母细胞瘤预后诊断中的临床应用。

Clinical application of the CpG island methylator phenotype to prognostic diagnosis in neuroblastomas.

机构信息

Division of Epigenomics, National Cancer Center Research Institute, Tokyo, Japan.

出版信息

J Hum Genet. 2013 Jul;58(7):428-33. doi: 10.1038/jhg.2013.64. Epub 2013 Jun 6.

DOI:10.1038/jhg.2013.64
PMID:23739128
Abstract

Clinical applications of aberrant DNA methylation to cancer diagnostics and therapeutics are accelerating. Especially, the CpG island methylator phenotype (CIMP), simultaneous methylation of multiple genes, provides information that cannot be obtained by other diagnostic methods and therapeutic opportunities. CIMP is known to be associated with poor or good prognosis depending upon cancer types. We identified that CIMP in neuroblastomas (NBLs) is strongly associated with poor prognosis in Japanese NBL cases (hazard ratio (HR)=22). Almost all NBLs with MYCN amplification displayed CIMP, and even among NBLs without MYCN amplification, NBLs with CIMP had worse prognosis (HR=12). The prognostic power was faithfully reproduced in German NBL cases by the same methods, and also in Italian and Swedish NBL cases with different analytical methods. Mechanistically, methylation silencing of different sets of tumor-suppressor genes is involved in poor prognosis of NBLs with CIMP, and the presence of CIMP is most sensitively detected by methylation of the PCDHB family. For therapeutic purposes, a combination of 5-aza-2'-deoxycytidine, a DNA-demethylating drug, with 13-cis-retinoic acid, a differentiating drug, has been shown to be effective for NBLs in vitro, and further development of a better combination(s) is awaited. Now, epigenetic diagnosis and therapeutics are becoming or have become an important choice for cancer patients.

摘要

异常 DNA 甲基化在癌症诊断和治疗中的临床应用正在加速。特别是,CpG 岛甲基化表型(CIMP),即多个基因的同时甲基化,提供了其他诊断方法无法获得的信息和治疗机会。CIMP 与癌症类型有关,预后不良或良好。我们发现神经母细胞瘤(NBL)中的 CIMP 与日本 NBL 病例的不良预后密切相关(风险比(HR)=22)。几乎所有 MYCN 扩增的 NBL 都显示 CIMP,即使在没有 MYCN 扩增的 NBL 中,具有 CIMP 的 NBL 预后也更差(HR=12)。通过相同的方法在德国 NBL 病例中忠实地再现了预后能力,并且在使用不同分析方法的意大利和瑞典 NBL 病例中也是如此。从机制上讲,CIMP 与 NBL 预后不良相关的是不同肿瘤抑制基因的甲基化沉默,而 CIMP 的存在最敏感地通过 PCDHB 家族的甲基化来检测。为了治疗目的,DNA 去甲基化药物 5-氮杂-2'-脱氧胞苷与分化药物 13-顺式维甲酸的联合应用已被证明对体外 NBL 有效,并且正在等待更好的联合药物的进一步开发。现在,表观遗传学诊断和治疗正在成为或已经成为癌症患者的重要选择。

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