Mutations in BRCA1 and BRCA2 are associated with increased breast cancer risk. While numerous non-synonymous SNPs in BRCA1/2 have been investigated for breast cancer risk, the impact of synonymous SNPs has not been studied so far. Recently, it has been reported that synonymous SNPs leading to an aberration from the preferred codon-usage can have functional effects and consequently be associated with disease. This motivated us to search for SNPs with the tendency to differential codon-usage in BRCA1/BRCA2. Based on defined criteria, two codon-usage-changing variants, Ser455Ser (1365A > G) and Ser2414Ser (7242A > G), were detected in BRCA2, whereas no such variant could be identified in BRCA1. We investigated the impact of these variants on breast cancer risk in a large case-control study. However, both SNPs, BRCA2 Ser2414Ser (7242A > G) and Ser455Ser (1365A > G), showed no association with breast cancer risk. This indicates that these codon-usage-changing SNPs have no major impact on familial breast cancer risk.
%0 Journal Article
%1 Yang.2009
%A Yang, Rongxi
%A Chen, Bowang
%A Hemminki, Kari
%A Wappenschmidt, Barbara
%A Engel, Christoph
%A Sutter, Christian
%A Ditsch, Nina
%A Weber, Bernhard H F,
%A Niederacher, Dieter
%A Arnold, Norbert
%A Meindl, Alfons
%A Bartram, Claus R.
%A Schmutzler, Rita K.
%A Burwinkel, Barbara
%D 2009
%J Breast cancer research and treatment
%K Adolescent Adult Aged Aged,_80_and_over Breast_Neoplasms/genetics Case-Control_Studies Codon Female Genes,_BRCA1 Genes,_BRCA2 Genetic_Predisposition_to_Disease Genotype Humans Middle_Aged Polymorphism,_Single_Nucleotide Young_Adult
%N 2
%P 407–413
%T Polymorphisms in BRCA2 resulting in aberrant codon-usage and their analysis on familial breast cancer risk
%V 118
%X Mutations in BRCA1 and BRCA2 are associated with increased breast cancer risk. While numerous non-synonymous SNPs in BRCA1/2 have been investigated for breast cancer risk, the impact of synonymous SNPs has not been studied so far. Recently, it has been reported that synonymous SNPs leading to an aberration from the preferred codon-usage can have functional effects and consequently be associated with disease. This motivated us to search for SNPs with the tendency to differential codon-usage in BRCA1/BRCA2. Based on defined criteria, two codon-usage-changing variants, Ser455Ser (1365A > G) and Ser2414Ser (7242A > G), were detected in BRCA2, whereas no such variant could be identified in BRCA1. We investigated the impact of these variants on breast cancer risk in a large case-control study. However, both SNPs, BRCA2 Ser2414Ser (7242A > G) and Ser455Ser (1365A > G), showed no association with breast cancer risk. This indicates that these codon-usage-changing SNPs have no major impact on familial breast cancer risk.
@article{Yang.2009,
abstract = {Mutations in BRCA1 and BRCA2 are associated with increased breast cancer risk. While numerous non-synonymous SNPs in BRCA1/2 have been investigated for breast cancer risk, the impact of synonymous SNPs has not been studied so far. Recently, it has been reported that synonymous SNPs leading to an aberration from the preferred codon-usage can have functional effects and consequently be associated with disease. This motivated us to search for SNPs with the tendency to differential codon-usage in BRCA1/BRCA2. Based on defined criteria, two codon-usage-changing variants, Ser455Ser (1365A > G) and Ser2414Ser (7242A > G), were detected in BRCA2, whereas no such variant could be identified in BRCA1. We investigated the impact of these variants on breast cancer risk in a large case-control study. However, both SNPs, BRCA2 Ser2414Ser (7242A > G) and Ser455Ser (1365A > G), showed no association with breast cancer risk. This indicates that these codon-usage-changing SNPs have no major impact on familial breast cancer risk.},
added-at = {2014-10-15T15:04:34.000+0200},
author = {Yang, Rongxi and Chen, Bowang and Hemminki, Kari and Wappenschmidt, Barbara and Engel, Christoph and Sutter, Christian and Ditsch, Nina and {Weber, Bernhard H F} and Niederacher, Dieter and Arnold, Norbert and Meindl, Alfons and Bartram, Claus R. and Schmutzler, Rita K. and Burwinkel, Barbara},
biburl = {https://www.bibsonomy.org/bibtex/2bb0dd0515452ecdff6325b49edcc89df/drtester},
interhash = {9341f48e1d0081981c95d571dd613cd9},
intrahash = {bb0dd0515452ecdff6325b49edcc89df},
journal = {Breast cancer research and treatment},
keywords = {Adolescent Adult Aged Aged,_80_and_over Breast_Neoplasms/genetics Case-Control_Studies Codon Female Genes,_BRCA1 Genes,_BRCA2 Genetic_Predisposition_to_Disease Genotype Humans Middle_Aged Polymorphism,_Single_Nucleotide Young_Adult},
number = 2,
pages = {407–413},
timestamp = {2014-10-15T15:04:34.000+0200},
title = {Polymorphisms in BRCA2 resulting in aberrant codon-usage and their analysis on familial breast cancer risk},
volume = 118,
year = 2009
}