林奇综合征与胰腺癌中体细胞错配修复变异。
Lynch Syndrome and Somatic Mismatch Repair Variants in Pancreas Cancer.
机构信息
Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, New York.
Department of Biology, Davidson College, Davidson, North Carolina.
出版信息
JAMA Oncol. 2024 Nov 1;10(11):1511-1518. doi: 10.1001/jamaoncol.2024.3651.
IMPORTANCE
Microsatellite (MS) instability (MSI-H) occurs frequently in Lynch syndrome (LS)-associated tumors and is associated with response to immune checkpoint blockade (ICB) therapy. MSI-H is conferred by germline or somatic variants in mismatch repair genes. The contribution of somatic oncogenesis to MSI-H in pancreatic cancer (PC) is unknown.
OBJECTIVE
To evaluate an LS-related PC cohort to define clinicogenomic features, describe somatic MSI-H cases (germline negative), characterize response to ICB, and guide preferred MS testing methods.
DESIGN, SETTING, AND PARTICIPANTS: This single-institution, retrospective analysis was conducted from March 2012 to July 2023 at Memorial Sloan Kettering Cancer Center and included 55 patients with PC and either an LS germline pathogenic variant (gPV) or somatic mismatch repair (MMR) variant.
MAIN OUTCOMES AND MEASURES
Composite MMR and MS status determined using orthogonal methods. An artificial intelligence classifier was used to account for low-cellularity specimens. Demographic and clinical data were abstracted from medical record. Zygosity status and somatic comutation landscape analyzed.
RESULTS
Fifty-five patients (23 women [42%]) had PC and an MMR variant: 32 (58%) had LS (LS cohort) and 23 (42%) had a somatic MMR variant (no germline pathogenic variant, somatic MMR cohort). In the LS cohort, 10 (31%) had gMSH2, 9 (28%) gMSH6, 8 (25%) gPMS2, 4 (13%) gMLH1, 1 (3%) gEPCAM. The median age at diagnosis was 68 years (range, 45-88 years). For composite MS status, 17 (59%) were MSI-H, 12 (41%) MS stable, and 3 MS unknown. Five cases were reclassified as MSI-H by the artificial intelligence classifier. In the somatic MMR cohort, 11 (48%) had MSH6, 7 (30%) MLH1, 3 (13%) MSH2, and 2 (9%) PMS2. The median age at diagnosis was 72 years (range, 66-85 years). For composite MS status, 10 (43%) were MSI-H, 11 (48%) MS stable, and 2 (9%) MS indeterminate. Six cases were reclassified as MSI-H by the artificial intelligence classifier. For the LS and somatic MMR cohorts, 20 received ICB (n = 17 MSI-H). The median ICB duration was 27.7 months (95% CI, 11.5 to not reached); the disease control rate was 80%.
CONCLUSION
The results of this cross-sectional study suggest that MSI-H occurs due to LS or somatic oncogenesis in PC. Orthogonal MS testing is key in PC; the artificial intelligence classifier reclassified approximately 20% of cases, most of which were low cellularity. ICB for patients with LS or somatic MSI-H PC provided significant benefit.
重要性
微卫星(MS)不稳定(MSI-H)在林奇综合征(LS)相关肿瘤中经常发生,与免疫检查点阻断(ICB)治疗的反应相关。MSI-H 由错配修复基因的种系或体细胞变异赋予。体细胞发生在胰腺癌(PC)中导致 MSI-H 的作用尚不清楚。
目的
评估一个与 LS 相关的 PC 队列,以确定临床基因组特征,描述种系阴性的体细胞 MSI-H 病例,描述对 ICB 的反应,并指导首选的 MS 检测方法。
设计、地点和参与者:这是一项单中心、回顾性分析,于 2012 年 3 月至 2023 年 7 月在纪念斯隆凯特琳癌症中心进行,纳入了 55 名患有 PC 且存在 LS 种系致病性变异(gPV)或体细胞错配修复(MMR)变异的患者。
主要结果和措施
使用正交方法确定复合 MMR 和 MS 状态。人工智能分类器用于解释低细胞标本。从病历中提取人口统计学和临床数据。分析等位基因状态和体细胞共突变情况。
结果
55 名患者(23 名女性[42%])患有 PC 和 MMR 变异:32 名(58%)患有 LS(LS 队列)和 23 名(42%)患有体细胞 MMR 变异(无种系致病性变异,体细胞 MMR 队列)。在 LS 队列中,10 名(31%)有 gMSH2,9 名(28%)有 gMSH6,8 名(25%)有 gPMS2,4 名(13%)有 gMLH1,1 名(3%)有 gEPCAM。诊断时的中位年龄为 68 岁(范围,45-88 岁)。对于复合 MS 状态,17 名(59%)为 MSI-H,12 名(41%)为 MS 稳定,3 名(13%)为 MS 未知。5 例通过人工智能分类器重新分类为 MSI-H。在体细胞 MMR 队列中,11 名(48%)有 MSH6,7 名(30%)有 MLH1,3 名(13%)有 MSH2,2 名(9%)有 PMS2。诊断时的中位年龄为 72 岁(范围,66-85 岁)。对于复合 MS 状态,10 名(43%)为 MSI-H,11 名(48%)为 MS 稳定,2 名(9%)为 MS 不确定。通过人工智能分类器重新分类了 6 例为 MSI-H。对于 LS 和体细胞 MMR 队列,20 名患者接受了 ICB(n=17 名 MSI-H)。ICB 的中位持续时间为 27.7 个月(95%CI,11.5 至未达到);疾病控制率为 80%。
结论
这项横断面研究的结果表明,MSI-H 是由 LS 或 PC 中的体细胞发生引起的。正交 MS 检测在 PC 中至关重要;人工智能分类器重新分类了大约 20%的病例,其中大多数为低细胞标本。LS 或体细胞 MSI-H PC 患者接受 ICB 治疗有显著获益。
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