疑似林奇综合征患者癌症易感基因中多种突变的鉴定
Identification of a Variety of Mutations in Cancer Predisposition Genes in Patients With Suspected Lynch Syndrome.
作者信息
Yurgelun Matthew B, Allen Brian, Kaldate Rajesh R, Bowles Karla R, Judkins Thaddeus, Kaushik Praveen, Roa Benjamin B, Wenstrup Richard J, Hartman Anne-Renee, Syngal Sapna
机构信息
Division of Population Sciences, Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts; Harvard Medical School, Boston, Massachusetts; Department of Medicine, Brigham and Women's Hospital, Boston, Massachusetts.
Myriad Genetic Laboratories, Salt Lake City, Utah.
出版信息
Gastroenterology. 2015 Sep;149(3):604-13.e20. doi: 10.1053/j.gastro.2015.05.006. Epub 2015 May 14.
BACKGROUND & AIMS: Multigene panels are commercially available tools for hereditary cancer risk assessment that allow for next-generation sequencing of numerous genes in parallel. However, it is not clear if these panels offer advantages over traditional genetic testing. We investigated the number of cancer predisposition gene mutations identified by parallel sequencing in individuals with suspected Lynch syndrome.
METHODS
We performed germline analysis with a 25-gene, next-generation sequencing panel using DNA from 1260 individuals who underwent clinical genetic testing for Lynch syndrome from 2012 through 2013. All patients had a history of Lynch syndrome-associated cancer and/or polyps. We classified all identified germline alterations for pathogenicity and calculated the frequencies of pathogenic mutations and variants of uncertain clinical significance (VUS). We also analyzed data on patients' personal and family history of cancer, including fulfillment of clinical guidelines for genetic testing.
RESULTS
Of the 1260 patients, 1112 met National Comprehensive Cancer Network (NCCN) criteria for Lynch syndrome testing (88%; 95% confidence interval [CI], 86%-90%). Multigene panel testing identified 114 probands with Lynch syndrome mutations (9.0%; 95% CI, 7.6%-10.8%) and 71 with mutations in other cancer predisposition genes (5.6%; 95% CI, 4.4%-7.1%). Fifteen individuals had mutations in BRCA1 or BRCA2; 93% of these met the NCCN criteria for Lynch syndrome testing and 33% met NCCN criteria for BRCA1 and BRCA2 analysis (P = .0017). An additional 9 individuals carried mutations in other genes linked to high lifetime risks of cancer (5 had mutations in APC, 3 had bi-allelic mutations in MUTYH, and 1 had a mutation in STK11); all of these patients met NCCN criteria for Lynch syndrome testing. A total of 479 individuals had 1 or more VUS (38%; 95% CI, 35%-41%).
CONCLUSIONS
In individuals with suspected Lynch syndrome, multigene panel testing identified high-penetrance mutations in cancer predisposition genes, many of which were unexpected based on patients' histories. Parallel sequencing also detected a high number of potentially uninformative germline findings, including VUS.
背景与目的
多基因检测板是用于遗传性癌症风险评估的商业工具,可对多个基因进行并行的新一代测序。然而,尚不清楚这些检测板是否比传统基因检测具有优势。我们调查了疑似林奇综合征患者通过并行测序鉴定出的癌症易感基因突变数量。
方法
我们使用2012年至2013年接受林奇综合征临床基因检测的1260名个体的DNA,通过一个包含25个基因的新一代测序检测板进行种系分析。所有患者均有林奇综合征相关癌症和/或息肉病史。我们将所有鉴定出的种系改变按致病性进行分类,并计算致病性突变和临床意义不确定的变异(VUS)的频率。我们还分析了患者个人和家族癌症病史的数据,包括是否符合基因检测的临床指南。
结果
在1260名患者中,1112名符合美国国立综合癌症网络(NCCN)的林奇综合征检测标准(88%;95%置信区间[CI],86%-90%)。多基因检测板检测发现114名先证者有林奇综合征突变(9.0%;95%CI,7.6%-10.8%),71名有其他癌症易感基因突变(5.6%;95%CI,4.4%-7.1%)。15名个体有BRCA1或BRCA2突变;其中93%符合NCCN的林奇综合征检测标准,33%符合NCCN的BRCA1和BRCA2分析标准(P = 0.0017)。另有9名个体携带与高终生癌症风险相关的其他基因突变(5名有APC突变,3名有MUTYH双等位基因突变,1名有STK11突变);所有这些患者均符合NCCN的林奇综合征检测标准。共有479名个体有1个或更多VUS(38%;95%CI,35%-41%)。
结论
在疑似林奇综合征的个体中,多基因检测板检测发现了癌症易感基因中的高穿透性突变,其中许多基于患者病史是意外发现。并行测序还检测到大量可能无信息价值的种系发现,包括VUS。
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