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首页> 外文期刊>Breast Cancer Research >Breast cancer biologic and etiologic heterogeneity by young age and menopausal status in the Carolina Breast Cancer Study: a case-control study
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Breast cancer biologic and etiologic heterogeneity by young age and menopausal status in the Carolina Breast Cancer Study: a case-control study

机译:Carolina乳腺癌研究中的年轻年龄和绝经状态乳腺癌生物和病因异质性:一个案例对照研究

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Young-onset breast cancer (40?years) is associated with worse prognosis and higher mortality. Breast cancer risk factors may contribute to distinct tumor biology and distinct age at onset, but understanding of these relationships has been hampered by limited representation of young women in epidemiologic studies and may be confounded by menopausal status. We examined tumor characteristics and epidemiologic risk factors associated with premenopausal women’s and young women’s breast cancer in phases I–III of the Carolina Breast Cancer Study (5309 cases, 2022 control subjects). Unconditional logistic regression was used to assess heterogeneity by age (40 vs. ≥40?years) and menopausal status. In both premenopausal and postmenopausal strata, younger women had more aggressive disease, including higher stage, hormone receptor-negative, disease as well as increased frequency of basal-like subtypes, lymph node positivity, and larger tumors. Higher waist-to-hip ratio was associated with reduced breast cancer risk among young women but with elevated risk among older women. Parity was associated with increased risk among young women and reduced risk among older women, while breastfeeding was more strongly protective for young women. Longer time since last birth was protective for older women but not for young women. In comparison, when we stratified by age, menopausal status was not associated with distinct risk factor or tumor characteristic profiles, except for progesterone receptor status, which was more commonly positive among premenopausal women. Age is a key predictor of breast cancer biologic and etiologic heterogeneity and may be a stronger determinant of heterogeneity than menopausal status. Young women’s breast cancer appears to be etiologically and biologically distinct from that among older women.
机译:幼眼乳腺癌(<40岁)与更严重的预后和更高的死亡率有关。乳腺癌风险因素可能导致肿瘤生物学和明显的年龄,但是对这些关系的理解,流行病学研究的少妇的有限表示受到限制,可能被更年期的地位混淆。在Carolina乳腺癌研究中的I-III阶段,检查了与前辈妇女和年轻女性乳腺癌相关的肿瘤特征和流行病学风险因素(5309例,2022例对照科目)。无条件逻辑回归用于评估异质性(<40vs≥40.年)和更长期的状态。在前辈和绝经后的地层中,年轻女性具有更具侵略性的疾病,包括较高阶段,激素受体 - 阴性,疾病以及增加次数亚型的频率,淋巴结阳性和较大的肿瘤。腰部到髋关节比率较高与年轻女性的乳腺癌风险降低有关,但老年妇女的风险很高。平价与年轻女性的风险增加以及老年妇女的风险降低有关,而母乳喂养对年轻女性更加强烈保护。自上次出生以来的时间较长,对老年女性来说是保护性,而不是年轻女性。相比之下,除了年龄的年龄分层时,未经孕酮受体状态除了孕激素受体状态外,未经可能的风险因素或肿瘤特征谱无比危险因素或肿瘤特征谱无关,其在前一妇女中更常见。年龄是乳腺癌生物学和病因异质性的关键预测因子,并且可能是超均相的较强的决定因子,而不是预期状态。年轻女性的乳腺癌似乎在病因学上和生物学上不同于老年女性。

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