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首页> 外文期刊>Modern Pathology >Subsets of microsatellite-unstable colorectal cancers exhibit discordance between the CpG island methylator phenotype and MLH1 methylation status
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Subsets of microsatellite-unstable colorectal cancers exhibit discordance between the CpG island methylator phenotype and MLH1 methylation status

机译:微卫星不稳定结直肠癌的亚集显示CpG岛甲基化子表型和MLH1甲基化状态之间的不一致

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Although the presence of MLH1 methylation in microsatellite-unstable colorectal cancer generally indicates involvement of the CpG island methylator phenotype (CIMP) in the development of the tumor, these two conditions do not always correlate. A minority of microsatellite-unstable colorectal cancers exhibit discordance between CIMP and MLH1 methylation statuses. However, the clinicopathological features of such microsatellite-unstable colorectal cancers with discrepant MLH1 methylation and CIMP statuses remain poorly studied. Microsatellite-unstable colorectal cancers (n=220) were analyzed for CIMP and MLH1 methylation statuses using the MethyLight assay. Based on the combinatorial CIMP and MLH1 methylation statuses, the microsatellite-unstable colorectal cancers were grouped into four subtypes (CIMP-high (CIMP-H) MLH1 methylation-positive (MLH1m+), CIMP-H MLH1 methylation-negative, CIMP-low/0 (CIMP-L/0) MLH1m+, and CIMP-L/0 MLH1 methylation-negative), which were compared in terms of their associations with clinicopathological and molecular features. The CIMP-L/0 MLH1 methylation-negative and CIMP-H MLH1m+ subtypes were predominant, comprising 63.6 and 24.1% of total microsatellite-unstable colorectal cancers, respectively. The discordant subtypes, CIMP-H MLH1 methylation-negative and CIMP-L/0 MLH1m+, were found in 5 and 7% of microsatellite-unstable colorectal cancers, respectively. The CIMP-H MLH1 methylation-negative subtype exhibited elevated incidence rates in male patients and was associated with larger tumor size, more frequent loss of MSH2 expression, increased frequency of KRAS mutation, and advanced cancer stage. The CIMP-L/0 MLH1m+ subtype was associated with onset at an earlier age, a predominance of MLH1 loss, and earlier cancer stage. None of the CIMP-L/0 MLH1m+ subtype patients succumbed to death during the follow-up. Our findings suggest that the discordant subtypes of colorectal cancers exhibit distinct clinicopathological and molecular features, although the proportion of discordant subtypes is low. The microsatellite-unstable colorectal cancers of the same CIMP status tended to exhibit different clinicopathological features depending on MLH1 methylation status.
机译:尽管微卫星不稳定结直肠癌中MLH1甲基化的存在通常表明CpG岛甲基化子表型(CIMP)参与了肿瘤的发展,但这两个条件并不总是相关的。少数微卫星不稳定的结直肠癌表现出CIMP和MLH1甲基化状态之间的不一致。但是,这种微卫星不稳定的结肠直肠癌的MLH1甲基化和CIMP状态存在差异,其临床病理特征仍未得到很好的研究。使用MethyLight分析法分析了微卫星不稳定结直肠癌(n = 220)的CIMP和MLH1甲基化状态。根据组合的CIMP和MLH1甲基化状态,将微卫星不稳定结直肠癌分为四个亚型(CIMP高(CIMP-H)MLH1甲基化阳性(MLH1m +),CIMP-H MLH1甲基化阴性,CIMP-low / 0(CIMP-L / 0)MLH1m +和CIMP-L / 0 MLH1甲基化阴性),将它们与临床病理和分子特征的关联进行了比较。 CIMP-L / 0 MLH1甲基化阴性和CIMP-H MLH1m +亚型占主导,分别占总微卫星不稳定大肠癌的63.6和24.1%。在5%和7%的微卫星不稳定结直肠癌中分别发现了不一致的亚型CIMP-H MLH1甲基化阴性和CIMP-L / 0 MLH1m +。 CIMP-H MLH1甲基化阴性亚型在男性患者中显示出较高的发病率,并与更大的肿瘤大小,更频繁的MSH2表达丧失,KRAS突变频率增加和晚期癌症相关。 CIMP-L / 0 MLH1m +亚型与更早发病,主要MLH1丢失和癌症早期有关。在随访期间,没有CIMP-L / 0 MLH1m +亚型患者死亡。我们的发现表明,尽管不一致亚型的比例很低,但结直肠癌的不一致亚型表现出独特的临床病理和分子特征。具有相同CIMP状态的微卫星不稳定结直肠癌倾向于表现出不同的临床病理特征,具体取决于MLH1甲基化状态。

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