Identification of Novel Candidate Genes for Early-Onset Colorectal Cancer Susceptibility

被引:53
作者
de Voer, Richarda M. [1 ]
Hahn, Marc-Manuel [1 ]
Weren, Robbert D. A. [1 ]
Mensenkamp, Arjen R. [1 ]
Gilissen, Christian [1 ]
van Zelst-Stams, Wendy A. [1 ]
Spruijt, Liesbeth [1 ]
Kets, C. Marleen [1 ]
Zhang, Junxiao [1 ]
Venselaar, Hanka [2 ]
Vreede, Lilian [1 ]
Schubert, Nil [1 ]
Tychon, Marloes [1 ]
Derks, Ronny [1 ]
Schackert, Hans K. [3 ]
van Kessel, Ad Geurts [1 ]
Hoogerbrugge, Nicoline [1 ]
Ligtenberg, Marjolijn J. L. [1 ,4 ]
Kuiper, Roland P. [1 ]
机构
[1] Radboud Univ Nijmegen, Med Ctr, Dept Human Genet, NL-6525 ED Nijmegen, Netherlands
[2] Radboud Univ Nijmegen, Med Ctr, Ctr Mol & Biomol Informat, Radboud Inst Mol Life Sci, NL-6525 ED Nijmegen, Netherlands
[3] Tech Univ Dresden, Abt Chirurg Forsch, D-01062 Dresden, Germany
[4] Radboud Univ Nijmegen, Med Ctr, Dept Pathol, NL-6525 ED Nijmegen, Netherlands
关键词
OF-FUNCTION VARIANTS; GERMLINE MUTATIONS; RISK; PREDISPOSITION; HETEROZYGOSITY; RECEPTOR; MOTILITY; CATENIN; COMPLEX; BREAST;
D O I
10.1371/journal.pgen.1005880
中图分类号
Q3 [遗传学];
学科分类号
071007 [遗传学];
摘要
Approximately 25-30% of colorectal cancer (CRC) cases are expected to result from a genetic predisposition, but in only 5-10% of these cases highly penetrant germline mutations are found. The remaining CRC heritability is still unexplained, and may be caused by a hitherto-undefined set of rare variants with a moderately penetrant risk. Here we aimed to identify novel risk factors for early-onset CRC using whole-exome sequencing, which was performed on a cohort of CRC individuals (n = 55) with a disease onset before 45 years of age. We searched for genes that were recurrently affected by rare variants (minor allele frequency <= 0.001) with potentially damaging effects and, subsequently, re-sequenced the candidate genes in a replication cohort of 174 early-onset or familial CRC individuals. Two functionally relevant genes with low frequency variants with potentially damaging effects, PTPN12 and LRP6, were found in at least three individuals. The protein tyrosine phosphatase PTP-PEST, encoded by PTPN12, is a regulator of cell motility and LRP6 is a component of the WNT-FZD-LRP5-LRP6 complex that triggers WNT signaling. All variants in LRP6 were identified in individuals with an extremely early-onset of the disease (<= 30 years of age), and two of the three variants showed increased WNT signaling activity in vitro. In conclusion, we present PTPN12 and LRP6 as novel candidates contributing to the heterogeneous susceptibility to CRC.
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页数:19
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