Essential meiotic endonuclease 1 homolog 1 (EME1) is a key DNA repair protein that participates in the rec- ognition and repair of DNA double-strand breaks. Deficiency of the EME1 gene can lead to spontaneous genomic instability and thus contribute to tumorgenesis. We hypothesized that the exon variants of EME1 confer genetic susceptibility to breast cancer. In a case-control study of 748 breast cancer patients and 778 normal controls, we analyzed the association between two exon variants of EME! (i.e.,Ile350Thr: rs12450550T 〉 C and Glu69Asp: rs3760413T 〉 G) and breast cancer risk. We found that compared to the common lie/lie genotype, the Thr variant genotypes (Thr/lle + Thr/Thr) conferred a 1.47-fold increased risk of breast cancer (OR=1.47, 95% CI=I. 13-1.92). The variant Ile350Thr was also associated with early onset of breast cancer (r = -0.116, P = 0.002). The mean age of onset was 44.4 years for Thr/Thr genotype carders and 46.5 years for Thr/lle genotype carriers, which was significantly lower than that (49.4 years) for Ile/Ile genotype carriers (P = 0.006). Moreover, no significant as- sociation was observed between the Glu69Asp variant and breast cancer risk. Our findings suggest that the EME1 variant Ile350Thr contributes to an increased risk and early onset of breast cancer.
Jianwei ZhaoLin LiuAnqing ZhangQin ChenWenxiang FangLizhi ZengJiachun Lu