在为精准医疗对接受肿瘤基因组分析的晚期结直肠癌患者进行肿瘤基因组分析时,检测致病性种系变异。
Detection of Pathogenic Germline Variants Among Patients With Advanced Colorectal Cancer Undergoing Tumor Genomic Profiling for Precision Medicine.
机构信息
Department of Surgical Oncology, University of Texas MD Anderson Cancer Center, Houston, Texas.
Department of Clinical Cancer Prevention, University of Texas MD Anderson Cancer Center, Houston, Texas.
出版信息
Dis Colon Rectum. 2019 Apr;62(4):429-437. doi: 10.1097/DCR.0000000000001322.
BACKGROUND
Genomic profiling of colorectal cancer aims to identify actionable somatic mutations but can also discover incidental germline findings.
OBJECTIVE
The purpose of this study was to report the detection of pathogenic germline variants that confer heritable cancer predisposition.
DESIGN
This was a retrospective study.
SETTINGS
The study was conducted at a tertiary-referral institution.
PATIENTS
Between 2012 and 2015, 1000 patients with advanced cancer underwent targeted exome sequencing of a 202-gene panel. The subgroup of 151 patients with advanced colorectal cancer who underwent matched tumor-normal (blood) sequencing formed our study cohort.
INTERVENTIONS
Germline variants in 46 genes associated with hereditary cancer predisposition were classified according to a defined algorithm based on in silico predictions of pathogenicity. Patients with presumed pathogenic variants were examined for type of mutation, as well as clinical, pedigree, and clinical genetic testing data.
MAIN OUTCOME MEASURES
We measured detection of pathogenic germline variants.
RESULTS
A total of 1910 distinct germline variants were observed in 151 patients. After filtering, 15 pathogenic germline variants (9.9%) were found in 15 patients, arising from 9 genes of varying penetrance for colorectal cancer (APC (n = 2; 13%), ATM (n = 1; 6%), BRCA1 (n = 2; 13%), CDH1 (n = 2; 13%), CHEK2 (n = 4; 27%), MSH2 (n = 1; 7%), MSH6 (n = 1; 7%), NF2 (n = 1; 7%), and TP53 (n = 1; 7%)). Patients with pathogenic variants were diagnosed at a younger age than those without (median, 45 vs 52 y; p = 0.03). Of the 15 patients, 7 patients (46.7%) with variants in low/moderate- penetrant genes for colorectal cancer would likely have not been tested based on clinical and pedigree criteria, where 2 harbored clinically actionable variants (CDH1 and NF2, 28.5% of 7).
LIMITATIONS
This study was limited by its small sample size and advanced-stage patients.
CONCLUSIONS
Tumor-normal sequencing can incidentally discover clinically unsuspected germline variants that confer cancer predisposition in 9.9% of patients with advanced colorectal cancer. Precision medicine should integrate clinical cancer genetics to inform and interpret the actionability of germline variants and to provide follow-up care to mutation carriers. See Video Abstract at http://links.lww.com/DCR/A906.
背景
结直肠癌的基因组分析旨在确定有治疗作用的体细胞突变,也能发现偶然的种系发现。
目的
本研究的目的是报告检测到有遗传易感性的致病性种系变异。
设计
这是一项回顾性研究。
地点
在一家三级转诊机构进行。
患者
2012 年至 2015 年间,1000 名晚期癌症患者接受了靶向外显子组测序 202 个基因组。在接受匹配的肿瘤-正常(血液)测序的 151 名晚期结直肠癌患者亚组中,我们的研究队列。
干预措施
根据基于种系突变致病性预测的明确定义的算法,对与遗传性癌症易感性相关的 46 个基因中的种系变异进行分类。对疑似致病性变异的患者进行突变类型以及临床、家族史和临床遗传检测数据的检查。
主要观察指标
我们测量了致病性种系变异的检测情况。
结果
在 151 名患者中观察到 1910 种不同的种系变异。经过过滤,在 15 名患者中发现了 15 种致病性种系变异(9.9%),这些变异来自于 APC(2 名患者;13%)、ATM(1 名患者;6%)、BRCA1(2 名患者;13%)、CDH1(2 名患者;13%)、CHEK2(4 名患者;27%)、MSH2(1 名患者;7%)、MSH6(1 名患者;7%)、NF2(1 名患者;7%)和 TP53(1 名患者;7%)等不同外显率的 9 个基因。携带致病性变异的患者比不携带致病性变异的患者诊断年龄更小(中位数 45 岁比 52 岁;p=0.03)。在 15 名患者中,7 名(46.7%)低/中度结直肠癌外显率基因变异的患者可能不会根据临床和家族史标准进行检测,其中 2 名患者携带临床上有意义的变异(CDH1 和 NF2,占 7 名患者的 28.5%)。
局限性
本研究的局限性在于样本量小和晚期患者。
结论
肿瘤-正常序列分析可能偶然发现临床上未被怀疑的种系变异,这些变异使 9.9%的晚期结直肠癌患者易患癌症。精准医学应整合临床癌症遗传学,以告知和解释种系变异的可操作性,并为突变携带者提供后续护理。在 http://links.lww.com/DCR/A906 观看视频摘要。
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