EPM2AIP1免疫组化不能作为结直肠癌MLH1启动子超甲基化检测的替代标记物

IF 2.7 2区 医学 Q2 PATHOLOGY
Bindu Challa , Wendy L. Frankel , Deborah Knight , Rachel Pearlman , Heather Hampel , Wei Chen
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引用次数: 0

摘要

MLH1启动子超甲基化(MPH)分析是林奇综合征(最常见的遗传性结直肠癌(CRC)易感性)通用肿瘤检测算法中的一个重要步骤。MPH 通常预示着散发性 CRC。EPM2AIP1 基因与 MLH1 基因共享相同的启动子,因此 MPH 也会抑制 EPM2AIP1 的转录,导致免疫组化(IHC)中蛋白表达的缺失。以前曾有报道称,EPM2AIP1 IHC 可用作子宫内膜癌中 MPH 的替代物。我们的目标是评估 EPM2AIP1 IHC 作为 MPH 在 CRC 中的替代物的可行性。我们选择了 101 例微卫星不稳定的 CRC 病例,其中 19 例来自整个肿瘤切片,82 例来自组织芯片。74例有MPH,27例无MPH。所有74例患有MPH的病例均在IHC上显示MLH1缺失,但只有47例(64%)显示EPM2AIP1表达缺失。在 27 例无 MPH 的病例中,有 9 例(33%)意外地出现了 EPM2AIP1 表达缺失。值得注意的是,10 例为无 MPH 的 MLH1 基因突变林奇综合征病例中,有 2 例出现了意想不到的 EPM2AIP1 染色缺失。在 6 例 MLH1 基因双体细胞突变(无 MPH)的病例中,只有 4 例如期显示出完整的 EPM2AIP1 表达。综上所述,EPM2AIP1 缺失对 MPH 的敏感性为 64%,特异性为 67%,准确率为 64%。我们的结论是,除非不同克隆或平台的染色质量有所提高,否则 EPM2AIP1 IHC 很可能无法作为 CRC MPH 的替代检测方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
EPM2AIP1 immunohistochemistry is inadequate as a surrogate marker for MLH1 promoter hypermethylation testing in colorectal cancer

MLH1 promoter hypermethylation (MPH) analysis is an essential step in the universal tumor testing algorithm for Lynch syndrome, the most common inherited predisposition to colorectal cancer (CRC). MPH usually indicates sporadic CRC. EPM2AIP1 gene shares the same promoter as MLH1, therefore MPH should also silence EPM2AIP1 transcription leading to loss of protein expression on immunohistochemistry (IHC). It has been previously reported that EPM2AIP1 IHC can be used as a surrogate for MPH in endometrial cancer. Our goal was to evaluate the feasibility of EPM2AIP1 IHC as a surrogate for MPH in CRC. 101 microsatellite instable CRC cases were selected, including 19 cases from whole tumor sections and 82 cases from tissue microarrays. 74 cases were with MPH and 27 without MPH. All 74 cases with MPH showed absent MLH1 by IHC, but only 47 (64%) exhibited loss of expression of EPM2AIP1. Of the 27 cases without MPH, 9 (33%) cases had unexpected loss of EPM2AIP1 expression. Of note, 10 cases were MLH1-mutated Lynch syndrome without MPH, and 2 of these cases showed unexpected loss of EPM2AIP1 staining. Of the 6 cases with double somatic mutations of MLH1 gene (without MPH), only 4 cases demonstrated intact expression of EPM2AIP1 as expected. Taken together, EPM2AIP1 loss was 64% sensitive and 67% specific for MPH, with an accuracy of 64%. We conclude that, unless stain quality improves with different clones or platforms, EPM2AIP1 IHC will likely not be useful as a surrogate test for MPH in CRC.

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来源期刊
Human pathology
Human pathology 医学-病理学
CiteScore
5.30
自引率
6.10%
发文量
206
审稿时长
21 days
期刊介绍: Human Pathology is designed to bring information of clinicopathologic significance to human disease to the laboratory and clinical physician. It presents information drawn from morphologic and clinical laboratory studies with direct relevance to the understanding of human diseases. Papers published concern morphologic and clinicopathologic observations, reviews of diseases, analyses of problems in pathology, significant collections of case material and advances in concepts or techniques of value in the analysis and diagnosis of disease. Theoretical and experimental pathology and molecular biology pertinent to human disease are included. This critical journal is well illustrated with exceptional reproductions of photomicrographs and microscopic anatomy.
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