Section of Oncology, Institute of Medicine, University of Bergen, Norway.
Eur J Cancer. 2012 Sep;48(13):1988-96. doi: 10.1016/j.ejca.2011.10.024. Epub 2011 Nov 24.
The MDM2 promoter polymorphism (SNP309T > G) extends a binding site for the transcription factor Sp1 and has been linked to elevated cancer risk and/or young age at cancer diagnosis, especially in females. Recently, we reported an adjacent polymorphism (SNP285G > C). SNP285C antagonises the effect of SNP309G by reducing Sp1 binding and lowers the risk of breast and ovarian cancer.
We assessed the potential gender specificity in the effect of this polymorphism. We performed in silico predictions of transcription factor binding sites in the MDM2 promoter and analysed MDM2 SNP285 and SNP309 status in two independent cohorts of endometrial (n = 438 and 472) and 666 prostatic cancer patients, and compared to 3.140 healthy controls.
We identified three oestrogen-receptor binding elements (EREs) within the MDM2 intronic promoter, one of which overlapping the Sp1 binding-site harbouring SNP285. The SNP285C/309G haplotype was associated with a reduced Odds Ratio (OR) for endometrial cancer (OR1: 0.55; Confidence Interval (CI) 0.32-0.97; OR2: 0.65; CI 0.40-1.08, especially for ER+ tumours; OR: 0.48; CI 0.28-0.87) but not for prostatic cancer among SNP309TG heterozygotes. SNP309G (SNP309TG or SNP309GG genotype) was associated with a moderately increased risk of endometrial cancer (OR: 1.17; CI 1.00-1.37) compared to SNP309TT homozygotes. Removing individuals harbouring the SNP309G-counteracting SNP285C polymorphism from the analysis strengthened this association (OR: 1.20; CI 1.02-1.41).
The finding of an ERE overlapping with the Sp1-binding site affected by SNP285, taken together with the significant impact of SNP285 on the risk of breast, ovarian and now endometrial cancer but not prostatic cancer, suggests a gender specific effect of SNP285C on cancer risk.
MDM2 启动子多态性(SNP309T>G)扩展了转录因子 Sp1 的结合位点,与癌症风险增加和/或癌症诊断时年龄较小有关,尤其是在女性中。最近,我们报道了一个相邻的多态性(SNP285G>C)。SNP285C 通过减少 Sp1 结合来拮抗 SNP309G 的作用,降低了乳腺癌和卵巢癌的风险。
我们评估了该多态性在性别特异性中的潜在作用。我们在 MDM2 启动子中进行了转录因子结合位点的计算机预测,并在两个独立的子宫内膜(n=438 和 472)和 666 例前列腺癌患者队列中分析了 MDM2 SNP285 和 SNP309 状态,并与 3140 名健康对照进行了比较。
我们在 MDM2 内含子启动子内发现了三个雌激素受体结合元件(EREs),其中一个与包含 SNP285 的 Sp1 结合位点重叠。SNP285C/309G 单倍型与子宫内膜癌的降低比值比(OR)相关(OR1:0.55;置信区间(CI)0.32-0.97;OR2:0.65;CI 0.40-1.08,特别是对于 ER+肿瘤;OR:0.48;CI 0.28-0.87),但 SNP309TG 杂合子中前列腺癌无相关性。与 SNP309TT 纯合子相比,SNP309G(SNP309TG 或 SNP309GG 基因型)与子宫内膜癌的中度风险增加相关(OR:1.17;CI 1.00-1.37)。从分析中去除携带 SNP309G 拮抗 SNP285C 多态性的个体,增强了这种相关性(OR:1.20;CI 1.02-1.41)。
重叠 Sp1 结合位点的 ERE 的发现受 SNP285 影响,再加上 SNP285 对乳腺癌、卵巢癌和现在的子宫内膜癌而不是前列腺癌风险的显著影响,表明 SNP285C 对癌症风险存在性别特异性影响。
