Oncologie et Génétique Moléculaires, Service de Biochimie et Biologie Moléculaire HMNO, CHRU de Lille, France.
Hum Mutat. 2012 Jan;33(1):180-8. doi: 10.1002/humu.21617. Epub 2011 Oct 31.
Constitutional epimutations of DNA mismatch repair (MMR) genes have been recently reported as a possible cause of Lynch syndrome. However, little is known about their prevalence, the risk of transmission through the germline and the risk for carriers to develop cancers. In this study, we evaluated the contribution of constitutional epimutations of MMR genes in Lynch syndrome. A cohort of 134 unrelated Lynch syndrome-suspected patients without MMR germline mutation was screened for constitutional epimutations of MLH1 and MSH2 by quantitative bisulfite pyrosequencing. Patients were also screened for the presence of EPCAM deletions, a possible cause of MSH2 methylation. Tumors from patients with constitutional epimutations were extensively analyzed. We identified a constitutional MLH1 epimutation in two proband patients. For one of them, we report for the first time evidence of transmission to two children who also developed early colonic tumors, indicating that constitutional MLH1 epimutations are associated to a real risk of transgenerational inheritance of cancer susceptibility. Moreover, a somatic BRAF mutation was detected in one affected child, indicating that tumors from patients carrying constitutional MLH1 epimutation can mimic MSI-high sporadic tumors. These findings may have important implications for future diagnostic strategies and genetic counseling.
最近有报道称,DNA 错配修复(MMR)基因的结构突变可能是林奇综合征的一个原因。然而,对于它们的普遍性、通过种系传递的风险以及携带者发生癌症的风险知之甚少。在这项研究中,我们评估了 MMR 基因结构突变在林奇综合征中的作用。对 134 名无 MMR 种系突变的林奇综合征疑似患者进行了 MLH1 和 MSH2 结构突变的定量亚硫酸氢盐焦磷酸测序筛查。还对 EPCAM 缺失(MSH2 甲基化的一个可能原因)的存在进行了筛查。对有结构突变的患者的肿瘤进行了广泛分析。我们在两名先证者患者中发现了 MLH1 结构突变。其中一例是首次报道的向两名儿童的传递证据,这两名儿童也患有早期结肠肿瘤,表明 MLH1 结构突变与癌症易感性的跨代遗传的真实风险相关。此外,在一名受影响的儿童中检测到了体细胞 BRAF 突变,表明携带 MLH1 结构突变的患者的肿瘤可以模拟 MSI-高散发性肿瘤。这些发现可能对未来的诊断策略和遗传咨询具有重要意义。
