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雌酮代谢物比值:2-羟基雌酮与 16α-羟基雌酮比值是否可预测乳腺癌?

Estrogen metabolite ratio: Is the 2-hydroxyestrone to 16α-hydroxyestrone ratio predictive for breast cancer?

机构信息

University Cancer Center Hamburg (UCCH)/Hubertus Wald Tumor Center, University Medical Center Hamburg-Eppendorf, Hamburg, Germany;

出版信息

Int J Womens Health. 2011 Feb 8;3:37-51. doi: 10.2147/IJWH.S7595.

Abstract

Experimental studies have shown that two main estrogen metabolites hydroxylated by CYP1A1 and CYP1B1 in the breast differentially affect breast cell proliferation and carcinogenesis. Although 16α-hydroxyestrone (16αOHE1) exerts estrogenic activity through covalent estrogen receptor (ER) binding, 2-hydroxyestrone (2OHE1) presumably has antiestrogenic capabilities. The ratio of 2OHE1 to 16αOHE1 represents the relative dominance of one pathway over the other and is believed to be modifiable by diet. It was hypothesized that women with or at high risk of breast cancer have a lower estrogen metabolite ratio (EMR) compared with women without breast cancer. We conducted a systematic review on the EMR as a predictor for breast cancer. A total of nine studies (six prospective and three retrospective) matched our inclusion criteria, comprising 682 premenopausal cases (1027 controls) and 1189 postmenopausal cases (1888 controls). For the highest compared with the lowest quantile of urinary EMR, nonsignificant associations suggested at best a weak protective effect in premenopausal but not in postmenopausal breast cancer (range of odds ratios: 0.50-0.75 for premenopausal and 0.71-1.31 for postmenopausal). Circulating serum/plasma EMR was not associated with breast cancer risk. Associations were inconclusive for receptor subtypes of breast cancer. Uncontrolled factors known to be involved in breast carcinogenesis, such as 4-hydroxyestrone (4OHE1) concentration, may have confounded results for EMR. Results of the prospective studies do not support the hypothesis that EMR can be used as a predictive marker for breast cancer risk. Future research should concentrate on profiles of estrogen metabolites, including 4OHE1, to gain a more complete picture of the relative importance of single metabolites for breast cancer.

摘要

实验研究表明,在乳腺中经 CYP1A1 和 CYP1B1 羟化的两种主要雌激素代谢物会对乳腺细胞增殖和癌变产生不同影响。虽然 16α-羟雌酮(16αOHE1)通过共价雌激素受体(ER)结合发挥雌激素活性,但 2-羟雌酮(2OHE1)可能具有抗雌激素作用。2OHE1 与 16αOHE1 的比值代表一种途径相对于另一种途径的相对优势,并且据信可以通过饮食进行调节。据推测,患有乳腺癌或有患乳腺癌风险的女性与没有乳腺癌的女性相比,其雌激素代谢物比值(EMR)较低。我们对 EMR 作为乳腺癌预测因子进行了系统评价。共有 9 项研究(6 项前瞻性研究和 3 项回顾性研究)符合我们的纳入标准,包括 682 例绝经前病例(1027 例对照)和 1189 例绝经后病例(1888 例对照)。对于尿液 EMR 最高与最低分位数相比,最佳情况下,绝经前乳腺癌的相关性提示具有较弱的保护作用(比值比范围:0.50-0.75 用于绝经前,0.71-1.31 用于绝经后)。循环血清/血浆 EMR 与乳腺癌风险无关。对于乳腺癌受体亚型,相关性尚无定论。已知与乳腺癌发生有关的未受控制的因素,如 4-羟雌酮(4OHE1)浓度,可能使 EMR 的结果产生混淆。前瞻性研究的结果不支持 EMR 可作为乳腺癌风险预测标志物的假设。未来的研究应集中于雌激素代谢物的谱,包括 4OHE1,以更全面地了解单个代谢物对乳腺癌的相对重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8171/3039007/c4e1e092d3bb/ijwh-3-037f1.jpg

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