机构通用微卫星不稳定性(MSI)反射测试对年轻和老年癌症大肠癌患者分子谱差异的影响

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2023-03-01 DOI:10.1016/j.clcc.2022.09.004
Ellery Altshuler , Aaron J. Franke , William Paul Skelton IV , Michael Feely , Yu Wang , Ji-Hyun Lee , Thomas Read , Krista Terracina , Xiang-Yang Lou , Yunfeng Dai , Thomas J. George
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引用次数: 2

摘要

DNA错配修复缺陷(dMMR)或微卫星不稳定性高(MSI-H)的癌症(CRC)在约15%的早期疾病和5%的转移性疾病中发现。在CRC中实施通用反射dMMR/MSI-H检测后,我们回顾了一个大型、单一的机构数据库,以比较年轻(≤50)和老年(>;50)患者的情况。患者和方法2009年至2017年间,佛罗里达大学所有诊断为CRC的患者都通过免疫组织化学(MLH1、PMS2、MSH2、MSH6)、PCR和下一代测序对dMMR进行了反射性体细胞肿瘤检测。采用2样本比较检验和逻辑回归模型进行统计分析。结果纳入最终分析的患者共375例。患者分为较年轻(年龄≤50岁;n=80)或较年长(>;50岁;n=295)。与老年患者的肿瘤相比,年轻患者的肿瘤不太可能是dMMR/MSI-H(12.5%对21.4%,P=0.013),也不太可能有BRAF突变(1.5%对16.1%,P=0.002)。BRAF突变状态与MMR状态高度相关;BRAF突变肿瘤发生dMMR/MSI-H或BRAF突变的可能性是BRAF-WT肿瘤的29.7倍(P=0.001,95%CI 11.3-78.3)。在我们的数据集中,通用MMR/MSI测试确定了相对较大的老年散发性CRC患者群体,他们有资格接受免疫治疗。
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Impact of Institutional Universal Microsatellite-Instability (MSI) Reflex Testing on Molecular Profiling Differences Between Younger and Older Patients with Colorectal Cancer

Introduction

DNA mismatch repair deficient (dMMR) or microsatellite instability-high (MSI-H) colorectal cancer (CRC) is found in about 15% of early-stage diseases and 5% of metastatic diseases. We reviewed a large, single-institutional database after implementation of universal reflex dMMR/MSI-H testing in CRC to compare profiles of younger (≤50) and older (>50) patients.

Patients and Methods

Between 2009 and 2017, all patients diagnosed with CRC at the University of Florida underwent reflex somatic tumor testing for dMMR by immunohistochemistry (MLH1, PMS2, MSH2, MSH6), MSI by PCR, and Next-Generation Sequencing. Statistical analysis was conducted with 2-sample comparison tests and logistic regression models.

Results

There were 375 patients included in the final analysis. Patients were grouped as younger (ages ≤50 years-old; n = 80) or older (>50 years-old; n = 295). Compared to tumors from older patients, tumors from younger patients were less likely to be dMMR/MSI-H (12.5% vs. 21.4%, P = .013) and less likely to have a BRAF mutation (1.5% vs. 16.1%, P = .002). BRAF mutation status was highly associated with MMR status; BRAF-mutated tumors were 29.7 times more likely than BRAF-WT tumors to be dMMR/MSI-H (P = < .001, 95% CI 11.3-78.3).

Conclusions

Tumors of younger patients were less likely than tumors of older patients to have a dMMR/MSI-H or BRAF mutation. Universal MMR/MSI testing in our dataset identified a relatively large population of older patients with sporadic CRC who were eligible for immunotherapy.

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