TY - JOUR
T1 - A recurrent truncating germline mutation in the BRIP1/FANCJ gene and susceptibility to prostate cancer
AU - Kote-Jarai, Z.
AU - Jugurnauth, S.
AU - Mulholland, S.
AU - Leongamornlert, D. A.
AU - Guy, M.
AU - Edwards, S.
AU - Tymrakiewitcz, M.
AU - O'Brien, L.
AU - Hall, A.
AU - Wilkinson, R.
AU - Al Olama, A. A.
AU - Morrison, J.
AU - Muir, K.
AU - Neal, D.
AU - Donovan, J.
AU - Hamdy, F.
AU - Easton, D. F.
AU - Eeles, R.
PY - 2009/1/27
Y1 - 2009/1/27
N2 - Although prostate cancer (PrCa) is one of the most common cancers in men in Western countries, little is known about the inherited factors that influence PrCa risk. On the basis of the fact that BRIP1/FANCJ interacts with BRCA1 and functions as a regulator of DNA double-strand break repair pathways, and that germline mutations within the BRIP1/FANCJ gene predispose to breast cancer, we chose this gene as a candidate for mutation screening in familial and young-onset PrCa cases. We identified a truncating mutation, R798X, in the BRIP1/FANCJ gene in 4 out of 2714 UK PrCa cases enriched for familial (2 out of 641; 0.3%) and young-onset cases (2 out of 2073; 0.1%). On screening 2045 controls from the UK population, we found one R798X sequence alteration (0.05%; odds ratio 2.4 (95% CI 0.25-23.4)). In addition, using our data from a genome-wide association study, we analysed 25 SNPs in the genomic region of the BRIP1/FANCJ gene. Two SNPs showed evidence of association with familial and young-onset PrCa (rs6504074; Ptrend=0.04 and rs8076727; P trend=0.01). These results suggest that truncating mutations in BRIP1/FANCJ might confer an increased risk of PrCa and common SNPs might also contribute to the alteration of risk, but larger case-control series will be required to confirm or refute this association.
AB - Although prostate cancer (PrCa) is one of the most common cancers in men in Western countries, little is known about the inherited factors that influence PrCa risk. On the basis of the fact that BRIP1/FANCJ interacts with BRCA1 and functions as a regulator of DNA double-strand break repair pathways, and that germline mutations within the BRIP1/FANCJ gene predispose to breast cancer, we chose this gene as a candidate for mutation screening in familial and young-onset PrCa cases. We identified a truncating mutation, R798X, in the BRIP1/FANCJ gene in 4 out of 2714 UK PrCa cases enriched for familial (2 out of 641; 0.3%) and young-onset cases (2 out of 2073; 0.1%). On screening 2045 controls from the UK population, we found one R798X sequence alteration (0.05%; odds ratio 2.4 (95% CI 0.25-23.4)). In addition, using our data from a genome-wide association study, we analysed 25 SNPs in the genomic region of the BRIP1/FANCJ gene. Two SNPs showed evidence of association with familial and young-onset PrCa (rs6504074; Ptrend=0.04 and rs8076727; P trend=0.01). These results suggest that truncating mutations in BRIP1/FANCJ might confer an increased risk of PrCa and common SNPs might also contribute to the alteration of risk, but larger case-control series will be required to confirm or refute this association.
KW - Deleterious mutation
KW - FANCJ/BRIP1
KW - Prostate cancer predisposition
KW - SNPs
UR - http://www.scopus.com/inward/record.url?scp=58749096682&partnerID=8YFLogxK
U2 - 10.1038/sj.bjc.6604847
DO - 10.1038/sj.bjc.6604847
M3 - Artículo
C2 - 19127258
AN - SCOPUS:58749096682
SN - 0007-0920
VL - 100
SP - 426
EP - 430
JO - British Journal of Cancer
JF - British Journal of Cancer
IS - 2
ER -