Centre for Epidemiology and Biostatistics, Melbourne School of Population and Global Health, The University of Melbourne, Melbourne, VIC, Australia.
Cancer Epidemiology and Intelligence Division, Cancer Council Victoria, Melbourne, VIC, Australia.
Int J Cancer. 2020 Mar 15;146(6):1541-1552. doi: 10.1002/ijc.32504. Epub 2019 Jun 26.
Adiposity increases estrogen receptor (ER)-positive postmenopausal breast cancer risk. While mechanisms underlying this relationship are uncertain, dysregulated sex-steroid hormone production and insulin signaling are likely pathways. Our aim was to quantify mediating effects of fasting insulin and free estradiol in the adiposity and ER-positive postmenopausal breast cancer association. We used data from a case-cohort study of sex hormones and insulin signaling nested within the Melbourne Collaborative Cohort Study. Eligible women, at baseline, were not diagnosed with cancer, were postmenopausal, did not use hormone therapy and had no history of diabetes or diabetes medication use. Women with ER-negative disease or breast cancer diagnosis within the first follow-up year were excluded. We analyzed the study as a cumulative sampling case-control study with 149 cases and 1,029 controls. Missing values for insulin and free estradiol were multiply imputed with chained equations. Interventional direct (IDE) and indirect (IIE) effects were estimated using regression-based multiple-mediator approach. For women with body mass index (BMI) >30 kg/m compared to women with BMI 18.5-25 kg/m , the risk ratio (RR) of breast cancer was 1.75 (95% confidence interval [CI] 1.05-2.91). The estimated IDE (RR) not through the mediators was 1.03 (95% CI 0.43-2.48). Percentage mediated effect through free estradiol was 72% (IIE-RR 1.56; 95% CI 1.11-2.19). There was no evidence for an indirect effect through insulin (IIE-RR 1.12; 95% CI 0.68-1.84; 28% mediated). Our results suggest that circulating free estradiol plays an important mediating role in the adiposity-breast cancer relationship but does not explain all of the association.
肥胖会增加雌激素受体(ER)阳性绝经后乳腺癌的风险。虽然这种关系的机制尚不确定,但性激素和胰岛素信号的失调可能是其中的途径。我们的目的是量化空腹胰岛素和游离雌二醇在肥胖和 ER 阳性绝经后乳腺癌发病机制中的中介作用。我们使用了嵌套在墨尔本合作队列研究中的激素和胰岛素信号的病例对照嵌套研究的数据。符合条件的女性在基线时未被诊断患有癌症、绝经后、未使用激素治疗且无糖尿病或糖尿病药物使用史。排除了患有 ER 阴性疾病或在首次随访年内被诊断患有乳腺癌的女性。我们将该研究分析为一项累积抽样病例对照研究,共有 149 例病例和 1029 例对照。使用连锁方程对胰岛素和游离雌二醇的缺失值进行了多次插补。使用基于回归的多重中介方法估计了干预性直接(IDE)和间接(IIE)效应。与 BMI 为 18.5-25kg/m 的女性相比,BMI 大于 30kg/m 的女性患乳腺癌的风险比(RR)为 1.75(95%置信区间 [CI] 1.05-2.91)。估计的不通过中介的 IDE(RR)为 1.03(95%CI 0.43-2.48)。通过游离雌二醇介导的效应占比为 72%(IIE-RR 为 1.56;95%CI 1.11-2.19)。没有证据表明通过胰岛素存在间接效应(IIE-RR 为 1.12;95%CI 0.68-1.84;28%的效应通过中介)。我们的结果表明,循环游离雌二醇在肥胖与乳腺癌之间的关系中起着重要的中介作用,但并不能解释所有的关联。
