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Molecular profiling of human mammary gland links breast cancer risk to a p27(+) cell population with progenitor characteristics.

机译:人类乳腺的分子剖面将乳腺癌风险与P27(+)细胞群进行祖细胞特征。

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摘要

Early full-term pregnancy is one of the most effective natural protections against breast cancer. To investigate this effect, we have characterized the global gene expression and epigenetic profiles of multiple cell types from normal breast tissue of nulliparous and parous women and carriers of BRCA1 or BRCA2 mutations. We found significant differences in CD44(+) progenitor cells, where the levels of many stem cell-related genes and pathways, including the cell-cycle regulator p27, are lower in parous women without BRCA1/BRCA2 mutations. We also noted a significant reduction in the frequency of CD44(+)p27(+) cells in parous women and showed, using explant cultures, that parity-related signaling pathways play a role in regulating the number of p27(+) cells and their proliferation. Our results suggest that pathways controlling p27(+) mammary epithelial cells and the numbers of these cells relate to breast cancer risk and can be explored for cancer risk assessment and prevention.
机译:早期怀孕是对乳腺癌最有效的自然保护之一。 为了研究这种效果,我们已经表征了来自BRCA1或BRCA2突变的尿道和寄生妇女和载体的正常乳腺组织的多种细胞类型的全球基因表达和表观遗传谱。 我们发现CD44(+)祖细胞的显着差异,其中许多干细胞相关基因和途径,包括细胞周期调节剂P27的途径在没有BRCA1 / BRCA2突变的寄生女性中较低。 我们还注意到寄生妇女的CD44(+)P27(+)细胞的频率显着降低,并使用外植体培养表明,奇偶植信相关的信号传导途径在调节P27(+)细胞的数量及其中起作用 增殖。 我们的研究结果表明,控制P27(+)乳腺上皮细胞的途径和这些细胞的数量涉及乳腺癌风险,可以探索癌症风险评估和预防。

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