Targeted sequencing of 36 known or putative colorectal cancer susceptibility genes

被引:32
作者
DeRycke, Melissa S. [1 ]
Gunawardena, Shanaka [1 ]
Balcom, Jessica R. [1 ]
Pickart, Angela M. [1 ]
Waltman, Lindsey A. [1 ]
French, Amy J. [1 ]
McDonnell, Shannon [2 ]
Riska, Shaun M. [2 ]
Fogarty, Zachary C. [2 ]
Larson, Melissa C. [2 ]
Middha, Sumit [2 ]
Eckloff, Bruce W. [3 ]
Asmann, Yan W. [4 ]
Ferber, Matthew J. [1 ]
Haile, Robert W. [5 ]
Gallinger, Steven [6 ]
Clendenning, Mark [7 ]
Rosty, Christophe [7 ,8 ,9 ]
Win, Aung K. [10 ,11 ]
Buchanan, Daniel D. [7 ,10 ,11 ]
Hopper, John L. [10 ]
Newcomb, Polly A. [12 ]
Le Marchand, Loic [13 ]
Goode, Ellen L. [1 ]
Lindor, Noralane M. [14 ]
Thibodeau, Stephen N. [1 ]
机构
[1] Mayo Clin, Dept Lab Med & Pathol, Rochester, MN USA
[2] Mayo Clin, Dept Biomed Stat & Informat, Rochester, MN USA
[3] Mayo Clin, Med Genome Facil, Rochester, MN USA
[4] Mayo Clin, Dept Hlth Sci Res, Jacksonville, FL 32224 USA
[5] Stanford Univ, Dept Med, Div Oncol, Stanford, CA 94305 USA
[6] Mt Sinai Hosp, Dept Surg, Toronto, ON, Canada
[7] Univ Melbourne, Dept Pathol, Genet Epidemiol Lab, Colorectal Oncogen Grp, Parkville, Vic, Australia
[8] Envoi Specialist Pathol, Herston, Qld, Australia
[9] Univ Queensland, Sch Med, Herston, Qld, Australia
[10] Univ Melbourne, Melbourne Sch Populat & Global Hlth, Ctr Epidemiol & Biostat, Parkville, Vic, Australia
[11] Royal Melbourne Hosp, Genet Med & Familial Canc Ctr, Parkville, Vic, Australia
[12] Fred Hutchinson Canc Res Ctr, Publ Hlth Sci Div, 1124 Columbia St, Seattle, WA 98104 USA
[13] Univ Hawaii, Canc Ctr, Epidemiol Program, Honolulu, HI 96822 USA
[14] Mayo Clin, Dept Hlth Sci Res, Scottsdale, AR USA
来源
MOLECULAR GENETICS & GENOMIC MEDICINE | 2017年 / 5卷 / 05期
关键词
Colorectal cancer; Familial Colorectal Cancer Type X; germline variants; young onset; MISMATCH REPAIR; COLON-CANCER; LYNCH SYNDROME; MUTATIONS; PROTEIN; EXPRESSION; GUIDELINES; VARIANTS; GENETICS; RISK;
D O I
10.1002/mgg3.317
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
BackgroundMutations in several genes predispose to colorectal cancer. Genetic testing for hereditary colorectal cancer syndromes was previously limited to single gene tests; thus, only a very limited number of genes were tested, and rarely those infrequently mutated in colorectal cancer. Next-generation sequencing technologies have made it possible to sequencing panels of genes known and suspected to influence colorectal cancer susceptibility. MethodsTargeted sequencing of 36 known or putative CRC susceptibility genes was conducted for 1231 CRC cases from five subsets: (1) Familial Colorectal Cancer Type X (n=153); (2) CRC unselected by tumor immunohistochemical or microsatellite stability testing (n=548); (3) young onset (age <50years) (n=333); (4) proficient mismatch repair (MMR) in cases diagnosed at 50years (n=68); and (5) deficient MMR CRCs with no germline mutations in MLH1, MSH2, MSH6, or PMS2 (n=129). Ninety-three unaffected controls were also sequenced. ResultsOverall, 29 nonsense, 43 frame-shift, 13 splice site, six initiator codon variants, one stop codon, 12 exonic deletions, 658 missense, and 17 indels were identified. Missense variants were reviewed by genetic counselors to determine pathogenicity; 13 were pathogenic, 61 were not pathogenic, and 584 were variants of uncertain significance. Overall, we identified 92 cases with pathogenic mutations in APC, MLH1, MSH2, MSH6, or multiple pathogenic MUTYH mutations (7.5%). Four cases with intact MMR protein expression by immunohistochemistry carried pathogenic MMR mutations. ConclusionsResults across case subsets may help prioritize genes for inclusion in clinical gene panel tests and underscore the issue of variants of uncertain significance both in well-characterized genes and those for which limited experience has accumulated.
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页码:553 / 569
页数:17
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