微卫星不稳定性与林奇综合征泛癌的存在相关。
Microsatellite Instability Is Associated With the Presence of Lynch Syndrome Pan-Cancer.
机构信息
1 Memorial Sloan Kettering Cancer Center, New York, NY.
2 Weill Cornell Medical College, New York, NY.
出版信息
J Clin Oncol. 2019 Feb 1;37(4):286-295. doi: 10.1200/JCO.18.00283. Epub 2018 Oct 30.
PURPOSE
Microsatellite instability (MSI) and/or mismatch repair deficiency (MMR-D) testing has traditionally been performed in patients with colorectal (CRC) and endometrial cancer (EC) to screen for Lynch syndrome (LS)-associated cancer predisposition. The recent success of immunotherapy in high-frequency MSI (MSI-H) and/or MMR-D tumors now supports testing for MSI in all advanced solid tumors. The extent to which LS accounts for MSI-H across heterogeneous tumor types is unknown. Here, we establish the prevalence of LS across solid tumors according to MSI status.
METHODS
MSI status was determined using targeted next-generation sequencing, with tumors classified as MSI-H, MSI-indeterminate, or microsatellite-stable. Matched germline DNA was analyzed for mutations in LS-associated mismatch repair genes ( MLH1, MSH2, MSH6, PMS2, EPCAM). In patients with LS with MSI-H/I tumors, immunohistochemical staining for MMR-D was assessed.
RESULTS
Among 15,045 unique patients (more than 50 cancer types), LS was identified in 16.3% (53 of 326), 1.9% (13 of 699), and 0.3% (37 of 14,020) of patients with MSI-H, MSI-indeterminate, and microsatellite-stable tumors, respectively ( P < .001). Among patients with LS with MSI-H/I tumors, 50% (33 of 66) had tumors other than CRC/EC, including urothelial, prostate, pancreas, adrenocortical, small bowel, sarcoma, mesothelioma, melanoma, gastric, and germ cell tumors. In these patients with non-CRC/EC tumors, 45% (15 of 33) did not meet LS genetic testing criteria on the basis of personal/family history. Immunohistochemical staining of LS-positive MSI-H/I tumors demonstrated MMR-D in 98.2% (56 of 57) of available cases.
CONCLUSION
MSI-H/MMR-D is predictive of LS across a much broader tumor spectrum than currently appreciated. Given implications for cancer surveillance and prevention measures in affected families, these data support germline genetic assessment for LS for patients with an MSI-H/MMR-D tumor, regardless of cancer type or family cancer history.
目的
微卫星不稳定性 (MSI) 和/或错配修复缺陷 (MMR-D) 检测传统上用于结直肠癌 (CRC) 和子宫内膜癌 (EC) 患者,以筛查林奇综合征 (LS) 相关的癌症易感性。免疫疗法在高频 MSI (MSI-H) 和/或 MMR-D 肿瘤中的近期成功现在支持对所有晚期实体瘤进行 MSI 检测。LS 在不同肿瘤类型的 MSI-H 中的占比程度尚不清楚。在此,我们根据 MSI 状态确定实体瘤中 LS 的患病率。
方法
使用靶向下一代测序确定 MSI 状态,将肿瘤分为 MSI-H、MSI 不确定或微卫星稳定。对 LS 相关错配修复基因 (MLH1、MSH2、MSH6、PMS2、EPCAM) 的种系 DNA 进行突变分析。在 MSI-H/I 肿瘤的 LS 患者中,评估 MMR-D 的免疫组织化学染色。
结果
在 15045 名患者中(超过 50 种癌症类型),MSI-H、MSI 不确定和微卫星稳定肿瘤患者的 LS 发生率分别为 16.3%(53/326)、1.9%(13/699)和 0.3%(37/14020)( P <.001)。在 MSI-H/I 肿瘤的 LS 患者中,50%(33/66)的患者患有 CRC/EC 以外的肿瘤,包括尿路上皮癌、前列腺癌、胰腺癌、肾上腺皮质癌、小肠癌、肉瘤、间皮瘤、黑色素瘤、胃癌和生殖细胞肿瘤。在这些非 CRC/EC 肿瘤患者中,45%(15/33)根据个人/家族史不符合 LS 基因检测标准。LS 阳性 MSI-H/I 肿瘤的免疫组织化学染色显示 98.2%(56/57)的 MMR-D 阳性。
结论
MSI-H/MMR-D 可预测比目前认识到的更广泛的肿瘤谱中的 LS。鉴于对受影响家族的癌症监测和预防措施的影响,这些数据支持对 MSI-H/MMR-D 肿瘤患者进行 LS 的种系基因评估,无论癌症类型或家族癌症史如何。
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