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微卫星高度不稳定/错配修复缺陷肿瘤诊断:筛查和诊断采用何种标准?结肠及其他部位的诊断方法:肿瘤之间的差异。

MSI/MMR-deficient tumor diagnosis: Which standard for screening and for diagnosis? Diagnostic modalities for the colon and other sites: Differences between tumors.

作者信息

Svrcek Magali, Lascols Olivier, Cohen Romain, Collura Ada, Jonchère Vincent, Fléjou Jean-François, Buhard Olivier, Duval Alex

机构信息

AP-HP, Sorbonne université, hôpital Saint-Antoine, department of Pathology, 75012 Paris, France; Centre de recherche Saint-Antoine, Inserm UMR_S 938, équipe "instabilité des microsatellites et cancers", 75012 Paris, France.

AP-HP, Sorbonne université, hôpital Saint-Antoine, department of biochemistry, 75012 Paris, France.

出版信息

Bull Cancer. 2019 Feb;106(2):119-128. doi: 10.1016/j.bulcan.2018.12.008. Epub 2019 Feb 1.

DOI:10.1016/j.bulcan.2018.12.008
PMID:30713006
Abstract

Microsatellite instability (MSI), which is caused by deficiency of the DNA mismatch repair (MMR) system, is the molecular abnormality observed in tumors associated with Lynch syndrome. Lynch syndrome represents one of the most frequent conditions of cancer predisposition in human, thus requiring specific care and genetic counseling. Moreover, research has recently focused increasingly on MMR deficiency due to its positive predictive value for the efficacy of immune checkpoints inhibitors (ICKi) in metastatic tumors, regardless of their primary origin. MSI has also been demonstrated to constitute an independent prognostic factor in several tumor types, being also associated with alternative response to chemotherapy. These observations have led many professional medical organizations to recommend universal screening of all newly diagnosed colorectal cancers for dMMR/MSI status and increasing evidence support the evaluation of MSI in all human tumors regardless of the cancer tissue of origin. Currently, two standard reference methods, namely immunohistochemistry and polymerase chain reaction, are recommended for the detection of dMMR/MSI status. These methods are equally valid as the initial screening test for dMMR/MSI in colorectal cancer. To date, there is no recommendation for the detection of dMMR/MSI in other primary tumors. In this review, we will present a comprehensive overview of the methods used for evaluation of tumor dMMR/MSI status in colorectal cancer, as well as in other tumor sites. We will see that the evaluation of this status remains challenging in some clinical settings, with the need to improve the above methods in these specific contexts.

摘要

微卫星不稳定性(MSI)由DNA错配修复(MMR)系统缺陷引起,是在与林奇综合征相关的肿瘤中观察到的分子异常。林奇综合征是人类最常见的癌症易患疾病之一,因此需要特殊护理和遗传咨询。此外,最近的研究越来越关注MMR缺陷,因为其对转移性肿瘤中免疫检查点抑制剂(ICKi)疗效具有阳性预测价值,无论其原发部位如何。MSI也已被证明是几种肿瘤类型中的独立预后因素,还与化疗的替代反应相关。这些观察结果促使许多专业医学组织建议对所有新诊断的结直肠癌进行错配修复缺陷/微卫星高度不稳定(dMMR/MSI)状态的普遍筛查,并且越来越多的证据支持对所有人类肿瘤进行MSI评估,无论癌症的原发组织如何。目前,推荐两种标准参考方法,即免疫组织化学和聚合酶链反应,用于检测dMMR/MSI状态。这些方法作为结直肠癌dMMR/MSI的初始筛查试验同样有效。迄今为止,尚无关于检测其他原发性肿瘤中dMMR/MSI的建议。在本综述中,我们将全面概述用于评估结直肠癌以及其他肿瘤部位肿瘤dMMR/MSI状态的方法。我们将看到,在某些临床环境中,这种状态的评估仍然具有挑战性,需要在这些特定背景下改进上述方法。

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