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乳腺密度与CYP1A2和COMT编码基因的多态性:多族裔队列研究

Breast density and polymorphisms in genes coding for CYP1A2 and COMT: the Multiethnic Cohort.

作者信息

Takata Yumie, Maskarinec Gertraud, Le Marchand Loïc

机构信息

Cancer Research Center of Hawaii, 1236 Lauhala Street, Honolulu, HI, USA.

出版信息

BMC Cancer. 2007 Feb 12;7:30. doi: 10.1186/1471-2407-7-30.

Abstract

BACKGROUND

Mammographic density is a strong predictor of breast cancer risk and is increased by hormone replacement therapy (HRT). Some associations with genetic polymorphisms in enzymes involved in estrogen metabolism have been described. This cross-sectional analysis examined the relation between mammographic density and the CYP1A2*1F and COMT Val58 Met polymorphisms among 332 breast cancer cases and 254 controls in the Hawaii component of the Multiethnic Cohort.

METHODS

Mammographic density, before diagnosis in cases, was quantified by using a validated computer-assisted method. Blood samples were genotyped by standard PCR/RFLP methods. Adjusted mean percent density was calculated by genotype using mixed models with the unstructured covariance option.

RESULTS

A positive association between the C allele in the CYP1A2*1F gene and percent density, but not the dense area, was suggested (p = 0.11). The relation was limited to controls (p = 0.045), postmenopausal women not using HRT (p = 0.08), and normal weight subjects (p = 0.046). We did not observe any relation between the COMT Val58 Met polymorphism and breast density.

CONCLUSION

The lack of an association between the CYP1A2 genotype and the size of the dense areas suggests an effect on the non-dense, i.e., fatty breast tissue. The discrepancies among studies may be due to differential susceptibility; changes in enzyme activity as a result of the CYP1A2*1F polymorphism may influence breast tissue differently depending on hormonal status. Larger studies with the ability to look at interactions would be useful to elucidate the influence of genetic variation in CYP1A2 and COMT on the risk of developing breast cancer.

摘要

背景

乳腺钼靶密度是乳腺癌风险的一个强有力的预测指标,且激素替代疗法(HRT)会使其增加。已经描述了一些与雌激素代谢相关酶的基因多态性之间的关联。这项横断面分析研究了多民族队列研究夏威夷部分的332例乳腺癌病例和254名对照中乳腺钼靶密度与CYP1A2*1F和儿茶酚-O-甲基转移酶(COMT)缬氨酸58蛋氨酸多态性之间的关系。

方法

病例在诊断前的乳腺钼靶密度通过一种经过验证的计算机辅助方法进行量化。血样通过标准聚合酶链反应/限制性片段长度多态性(PCR/RFLP)方法进行基因分型。使用具有非结构化协方差选项的混合模型按基因型计算调整后的平均密度百分比。

结果

提示CYP1A2*1F基因中的C等位基因与密度百分比之间存在正相关,但与致密区域无关(p = 0.11)。这种关系仅限于对照组(p = 0.045)、未使用HRT的绝经后女性(p = 0.08)和正常体重受试者(p = 0.046)。我们未观察到COMT缬氨酸58蛋氨酸多态性与乳腺密度之间存在任何关系。

结论

CYP1A2基因型与致密区域大小之间缺乏关联表明其对非致密的即脂肪性乳腺组织有影响。研究之间的差异可能是由于易感性不同;CYP1A2*1F多态性导致的酶活性变化可能根据激素状态对乳腺组织产生不同影响。能够研究相互作用的更大规模研究将有助于阐明CYP1A2和COMT基因变异对患乳腺癌风险的影响。

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