结直肠癌患者的癌症易感基因突变
Cancer Susceptibility Gene Mutations in Individuals With Colorectal Cancer.
作者信息
Yurgelun Matthew B, Kulke Matthew H, Fuchs Charles S, Allen Brian A, Uno Hajime, Hornick Jason L, Ukaegbu Chinedu I, Brais Lauren K, McNamara Philip G, Mayer Robert J, Schrag Deborah, Meyerhardt Jeffrey A, Ng Kimmie, Kidd John, Singh Nanda, Hartman Anne-Renee, Wenstrup Richard J, Syngal Sapna
机构信息
Matthew B. Yurgelun, Matthew H. Kulke, Charles S. Fuchs, Hajime Uno, Chinedu I. Ukaegbu, Lauren K. Brais, Philip G. McNamara, Robert J. Mayer, Deborah Schrag, Jeffrey A. Meyerhardt, Kimmie Ng, and Sapna Syngal, Dana-Farber Cancer Institute; Matthew B. Yurgelun, Matthew H. Kulke, Charles S. Fuchs, Hajime Uno, Jason L. Hornick, Robert J. Mayer, Deborah Schrag, Jeffrey A. Meyerhardt, Kimmie Ng, and Sapna Syngal, Harvard Medical School; Matthew B. Yurgelun, Matthew H. Kulke, Charles S. Fuchs, Jason L. Hornick, Robert J. Mayer, Deborah Schrag, Jeffrey A. Meyerhardt, Kimmie Ng, and Sapna Syngal, Brigham and Women's Hospital, Boston, MA; and Brian A. Allen, John Kidd, Nanda Singh, Anne-Renee Hartman, and Richard J. Wenstrup, Myriad Genetics, Salt Lake City, UT.
出版信息
J Clin Oncol. 2017 Apr 1;35(10):1086-1095. doi: 10.1200/JCO.2016.71.0012. Epub 2017 Jan 30.
Purpose Hereditary factors play an important role in colorectal cancer (CRC) risk, yet the prevalence of germline cancer susceptibility gene mutations in patients with CRC unselected for high-risk features (eg, early age at diagnosis, personal/family history of cancer or polyps, tumor microsatellite instability [MSI], mismatch repair [MMR] deficiency) is unknown. Patients and Methods We recruited 1,058 participants who received CRC care in a clinic-based setting without preselection for age at diagnosis, personal/family history, or MSI/MMR results. All participants underwent germline testing for mutations in 25 genes associated with inherited cancer risk. Each gene was categorized as high penetrance or moderate penetrance on the basis of published estimates of the lifetime cancer risks conferred by pathogenic germline mutations in that gene. Results One hundred five (9.9%; 95% CI, 8.2% to 11.9%) of 1,058 participants carried one or more pathogenic mutations, including 33 (3.1%) with Lynch syndrome (LS). Twenty-eight (96.6%) of 29 available LS CRCs demonstrated abnormal MSI/MMR results. Seventy-four (7.0%) of 1,058 participants carried non-LS gene mutations, including 23 (2.2%) with mutations in high-penetrance genes (five APC, three biallelic MUTYH, 11 BRCA1/2, two PALB2, one CDKN2A, and one TP53), 15 of whom lacked clinical histories suggestive of their underlying mutation. Thirty-eight (3.6%) participants had moderate-penetrance CRC risk gene mutations (19 monoallelic MUTYH, 17 APC*I1307K, two CHEK2). Neither proband age at CRC diagnosis, family history of CRC, nor personal history of other cancers significantly predicted the presence of pathogenic mutations in non-LS genes. Conclusion Germline cancer susceptibility gene mutations are carried by 9.9% of patients with CRC. MSI/MMR testing reliably identifies LS probands, although 7.0% of patients with CRC carry non-LS mutations, including 1.0% with BRCA1/2 mutations.
目的 遗传因素在结直肠癌(CRC)风险中起重要作用,但在未因高风险特征(如诊断时年龄小、个人/家族癌症或息肉病史、肿瘤微卫星不稳定性[MSI]、错配修复[MMR]缺陷)而被选择的CRC患者中,种系癌症易感基因突变的患病率尚不清楚。患者与方法 我们招募了1058名在临床环境中接受CRC治疗的参与者,未根据诊断年龄、个人/家族病史或MSI/MMR结果进行预先选择。所有参与者均接受了25个与遗传性癌症风险相关基因的种系突变检测。根据已发表的该基因致病性种系突变所赋予的终生癌症风险估计值,将每个基因分为高外显率或中等外显率。结果 1058名参与者中有105名(9.9%;95%CI,8.2%至11.9%)携带一个或多个致病性突变,其中33名(3.1%)患有林奇综合征(LS)。29例可用的LS CRC中有28例(96.6%)显示MSI/MMR结果异常。1058名参与者中有74名(7.0%)携带非LS基因突变,其中23名(2.2%)携带高外显率基因突变(5例APC、3例双等位基因MUTYH、11例BRCA1/2、2例PALB2、1例CDKN2A和1例TP53),其中15名缺乏提示其潜在突变的临床病史。38名(3.6%)参与者有中等外显率的CRC风险基因突变(19例单等位基因MUTYH、17例APC*I1307K、2例CHEK2)。CRC诊断时的先证者年龄、CRC家族史或其他癌症个人史均不能显著预测非LS基因中致病性突变的存在。结论 9.9%的CRC患者携带种系癌症易感基因突变。MSI/MMR检测可可靠地识别LS先证者,尽管7.0%的CRC患者携带非LS突变,其中1.0%携带BRCA1/2突变。
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