A. Puccini , F. Grillo , M. Fassan , S. Lonardi , M. Genuardi , R. Cannizzaro , G.M. Cavestro , F. Marmorino , V. Conca , L. Salvatore , F. Bergamo , F. Tosi , F. Morano , V. Daprà , C. Molica , D. Barana , A. Guglielmi , C. Signorelli , M. D’Amico , F. Zoratto , S. Sciallero
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We aim to evaluate the feasibility of the mainstreaming diagnostic algorithm for LS.</p></div><div><h3>Patients and methods</h3><p>ItaLynch is an ongoing, prospective, observational, multicenter, multidisciplinary, Italian study in patients with dMMR CRC. Being descriptive in nature, it does not attempt to test any specific, <em>a priori</em>, hypothesis. Patients with dMMR CRC are selected by universal screening by immunohistochemistry (IHC). In <em>MLH1</em>-deficient patients, reflex testing for <em>BRAF</em><sup><em>V600E</em></sup> and, when appropriate, for <em>MLH1</em> promoter hypermethylation is carried out. For all dMMR CRC, a ‘Lynch Alert’ is added to the pathology report: positive when a patient is at high risk for LS, due to reflex testing results or to loss of non-MLH1 proteins. Conversely, a ‘Lynch Alert’ is negative when the patient is likely to be a nonhereditary case (i.e. MLH1 loss and <em>BRAF</em><sup><em>V600E</em></sup> or <em>MLH1</em> promoter hypermethylation). In patients with a positive ‘Lynch Alert’, after providing a brief explanation about the risks and benefits of genetic testing, the oncologist asks patients for their consent to mainstream genetic testing. Thus a blood sample is drawn for constitutional variants of the MMR genes. Carriers of a germline variant are then referred to post-test genetic counseling. 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引用次数: 0
摘要
背景国际指南建议通过对所有结直肠癌(CRC)进行体细胞DNA错配修复缺陷(dMMR)检测,普遍筛查林奇综合征(LS)。然而,林奇综合征在很大程度上仍然诊断不足。通过肿瘤学家驱动的基因检测将 LS 诊断纳入主流可提高检出率,从而将精准预防的益处扩大到 LS 患者及其家属。我们旨在评估 LS 主流化诊断算法的可行性。患者和方法ItaLynch 是一项正在进行的前瞻性、观察性、多中心、多学科的意大利研究,研究对象为 dMMR CRC 患者。该研究属于描述性研究,并不试图检验任何特定的先验假设。dMMR CRC 患者通过免疫组化(IHC)进行普遍筛查。对于 MLH1 缺乏的患者,要进行 BRAFV600E 的条件反射检测,适当时还要进行 MLH1 启动子超甲基化的条件反射检测。对于所有 dMMR CRC,病理报告中都会添加 "林奇警报"(Lynch Alert):当患者因反射检测结果或非 MLH1 蛋白缺失而面临 LS 高风险时,该警报为阳性。相反,如果患者可能是非遗传性病例(即 MLH1 缺失和 BRAFV600E 或 MLH1 启动子超甲基化),则 "林奇警报 "为阴性。对于 "林奇警报 "呈阳性的患者,肿瘤学家在简要解释基因检测的风险和益处后,会征求患者对主流基因检测的同意。这样,就会抽取血液样本,检测 MMR 基因的基因变异。然后,种系变异携带者会被转介到检测后遗传咨询。对于符合临床可疑标准的患者,还建议转诊至临床遗传服务机构。
ItaLynch: an ongoing Italian study to evaluate the feasibility of mainstreaming the diagnosis of Lynch syndrome in colorectal cancer patients
Background
International guidelines recommend universal screening for Lynch syndrome (LS) through somatic DNA mismatch repair deficiency (dMMR) testing in all colorectal cancers (CRCs). However, LS remains largely underdiagnosed. Mainstreaming LS diagnosis through oncologist-driven genetic testing could increase detection rates, thus extending the benefits of precision prevention to patients with LS and their families. We aim to evaluate the feasibility of the mainstreaming diagnostic algorithm for LS.
Patients and methods
ItaLynch is an ongoing, prospective, observational, multicenter, multidisciplinary, Italian study in patients with dMMR CRC. Being descriptive in nature, it does not attempt to test any specific, a priori, hypothesis. Patients with dMMR CRC are selected by universal screening by immunohistochemistry (IHC). In MLH1-deficient patients, reflex testing for BRAFV600E and, when appropriate, for MLH1 promoter hypermethylation is carried out. For all dMMR CRC, a ‘Lynch Alert’ is added to the pathology report: positive when a patient is at high risk for LS, due to reflex testing results or to loss of non-MLH1 proteins. Conversely, a ‘Lynch Alert’ is negative when the patient is likely to be a nonhereditary case (i.e. MLH1 loss and BRAFV600E or MLH1 promoter hypermethylation). In patients with a positive ‘Lynch Alert’, after providing a brief explanation about the risks and benefits of genetic testing, the oncologist asks patients for their consent to mainstream genetic testing. Thus a blood sample is drawn for constitutional variants of the MMR genes. Carriers of a germline variant are then referred to post-test genetic counseling. Referral to clinical genetic services is also advised for patients with clinical suspect criteria.