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Parity, hormones and breast cancer subtypes - results from a large nested case-control study in a national screening program

机译:奇偶校验,激素和乳腺癌亚型-国家筛查计划中一项大型嵌套病例对照研究的结果

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BackgroundBreast cancer comprises several molecular subtypes with different prognoses and possibly different etiology. Reproductive and hormonal factors are associated with breast cancer overall, and with luminal subtypes, but the associations with other subtypes are unclear. We used data from a national screening program to conduct a large nested case-control study. MethodsWe conducted a nested case-control study on participants in the Norwegian Breast Cancer Screening Program in 2006???2014. There was information on estrogen receptor (ER), progesterone receptor (PR) and human epidermal growth factor receptor 2 (HER2) for 4748 cases of breast cancer. Breast cancer subtypes were defined as luminal A-like (ER+ PR+ HER2-), luminal B-like (ER+ PR- HER2- or ER+ PR+/PR-HER2+), HER2-positive (ER- PR- HER2+) and triple-negative (ER- PR- HER2-). Conditional logistic regression was used to estimate odds ratios (ORs) of breast cancer associated with age at first birth, number of pregnancies, oral contraceptive use, intrauterine devices and menopausal hormone therapy. Analyses were adjusted for age, body mass index, education, age at menarche, number of pregnancies and menopausal status. ResultsNumber of pregnancies was inversely associated with relative risk of luminal-like breast cancers ( p -trend ≤0.02), and although not statistically significant, with HER2-positive (OR?=?0.60, 95% CI 0.31–1.19) and triple-negative cancer (OR?=?0.70, 95% CI 0.41–1.21). Women who had ≥4 pregnancies were at >40% lower risk of luminal-like and HER2-positive cancers than women who had never been pregnant. However, there was a larger discrepancy between tumor subtypes with menopausal hormone use. Women who used estrogen and progesterone therapy (EPT) had almost threefold increased risk of luminal A-like cancer (OR?=?2.92, 95% CI 2.36–3.62) compared to never-users, but were not at elevated risk of HER2-positive (OR?=?0.88, 95% CI 0.33–2.30) or triple-negative (OR?=?0.92, 95% CI 0.43???1.98) subtypes. ConclusionsReproductive factors were to some extent associated with all subtypes; the strongest trends were with luminal-like subtypes. Hormone therapy use was strongly associated with risk of luminal-like breast cancer, and less so with risk of HER2-positive or triple-negative cancer. There are clearly some, but possibly limited, etiologic differences between subtypes, with the greatest contrast between luminal A-like and triple-negative subtypes. Trial registrationNot applicable.
机译:背景乳腺癌包括几种预后不同,病因可能不同的分子亚型。生殖和激素因素总体上与乳腺癌以及管腔亚型相关,但尚不清楚与其他亚型的相关性。我们使用了来自国家筛查计划的数据来进行大型的嵌套病例对照研究。方法我们在2006年至2014年间对挪威乳腺癌筛查计划的参与者进行了巢式病例对照研究。有关4748例乳腺癌的雌激素受体(ER),孕激素受体(PR)和人表皮生长因子受体2(HER2)的信息。乳腺癌亚型定义为腔A样(ER + PR + HER2-),腔B样(ER + PR- HER2-或ER + PR + / PR-HER2 +),HER2阳性(ER- PR- HER2 +)和三阴性(ER-PR-HER2-)。使用条件对数回归来估计与初生年龄,怀孕次数,口服避孕药,宫内节育器和更年期激素疗法相关的乳腺癌的优势比(OR)。对年龄,体重指数,教育程度,初潮年龄,怀孕次数和绝经状态进行了调整。结果怀孕人数与管腔样乳腺癌的相对风险呈负相关(p趋势≤0.02),尽管无统计学意义,但HER2阳性(OR?=?0.60,95%CI 0.31-1.19)和三联阴性(OR = 0.70,95%CI 0.41-1.21)。妊娠≥4的女性比从未怀孕的女性发生腔样和HER2阳性癌症的风险低40%以上。但是,使用更年期激素的肿瘤亚型之间存在较大差异。与从未使用过激素的女性相比,使用雌激素和孕酮疗法(EPT)的女性与管腔A样癌症的风险增加了将近三倍(OR?=?2.92,95%CI 2.36–3.62),但未增加HER2-阳性(ORα=?0.88,95%CI 0.33–2.30)或三阴性(ORα=?0.92,95%CI 0.43 ??? 1.98)亚型。结论生殖因子在一定程度上与所有亚型有关。最强烈的趋势是腔样亚型。使用激素治疗与管腔样乳腺癌的风险密切相关,而与HER2阳性或三阴性肿瘤的风险相关性较小。显然,亚型之间存在一些但可能有限的病因学差异,管腔A型和三阴性亚型之间的差异最大。试用注册不适用。

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