Journal article
Identification of novel variants in colorectal cancer families by high-throughput exome sequencing
MS DeRycke, SR Gunawardena, S Middha, YW Asmann, DJ Schaid, SK McDonnell, SM Riska, BW Eckloff, JM Cunningham, BL Fridley, DJ Serie, WR Bamlet, MS Cicek, MA Jenkins, DJ Duggan, D Buchanan, M Clendenning, RW Haile, MO Woods, SN Gallinger Show all
Cancer Epidemiology Biomarkers and Prevention | AMER ASSOC CANCER RESEARCH | Published : 2013
Abstract
Background: Colorectal cancer (CRC) in densely affected families without Lynch Syndrome may be due to mutations in undiscovered genetic loci. Familial linkage analyses have yielded disparate results; the use of exome sequencing in coding regions may identify novel segregating variants. Methods: We completed exome sequencing on 40 affected cases from 16 multicase pedigrees to identify novel loci. Variants shared among all sequenced cases within each family were identified and filtered to exclude common variants and single-nucleotide variants (SNV) predicted to be benign. Results: We identified 32 nonsense or splice-site SNVs, 375 missense SNVs, 1,394 synonymous or noncoding SNVs, and 50 indel..
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Grants
Awarded by National Cancer Institute
Funding Acknowledgements
This work was supported by the National Cancer Institute, NIH under RFA # CA-95-011 and through cooperative agreements with members of the Colon CFR and Principal Investigators. Collaborating centers include the Australian Colorectal CFR (UO1 CA097735), the Familial Colorectal Neoplasia Collaborative Group (UO1 CA074799), Mayo Clinic Cooperative Family Registry for Colon Cancer Studies (UO1 CA074800), Ontario Registry for Studies of Familial Colorectal Cancer (UO1 CA074783), and University of California, Irvine Informatics Center (UO1 CA078296).