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Age and the means of bypassing stasis influence the intrinsic subtype of immortalized human mammary epithelial cells

机译:年龄和绕淤的方法影响永生化人类乳腺上皮细胞的内在亚型

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摘要

Based on molecular features, breast cancers are grouped into intrinsic subtypes that have different prognoses and therapeutic response profiles. With increasing age, breast cancer incidence increases, with hormone receptor-positive and other luminal-like subtype tumors comprising a majority of cases. It is not known at what stage of tumor progression subtype specification occurs, nor how the process of aging affects the intrinsic subtype. We examined subtype markers in immortalized human mammary epithelial cell lines established following exposure of primary cultured cell strains to a two-step immortalization protocol that targets the two main barriers to immortality: stasis (stress-associated senescence) and replicative senescence. Cell lines derived from epithelial cells obtained from non-tumorous pre- and post-menopausal breast surgery tissues were compared. Additionally, comparisons were made between lines generated using two different genetic interventions to bypass stasis: transduction of either an shRNA that down-regulated p16INK4A, or overexpressed constitutive active cyclin D1/CDK2. In all cases, the replicative senescence barrier was bypassed by transduction of c-Myc. Cells from all resulting immortal lines exhibited normal karyotypes. Immunofluorescence, flow cytometry, and gene expression analyses of lineage-specific markers were used to categorize the intrinsic subtypes of the immortalized lines. Bypassing stasis with p16 shRNA in young strains generated cell lines that were invariably basal-like, but the lines examined from older strains exhibited some luminal features such as keratin 19 and estrogen receptor expression. Overexpression of cyclin D1/CDK2 resulted in keratin 19 positive, luminal-like cell lines from both young and old strains, and the lines examined from older strains exhibited estrogen receptor expression. Thus age and the method of bypassing stasis independently influence the subtype of immortalized human mammary epithelial cells.
机译:基于分子特征,乳腺癌被分为具有不同预后和治疗反应特征的内在亚型。随着年龄的增长,乳腺癌的发病率增加,激素受体阳性和其他腔样亚型肿瘤占大多数病例。尚不清楚在肿瘤进展亚型的哪个阶段发生,也不知道衰老过程如何影响内在亚型。我们检查了永生化的人类乳腺上皮细胞系中的亚型标记,该细胞系在将原代培养的细胞株暴露于针对永生的两个主要障碍的两步永生化方案后进行:停滞(应力相关衰老)和复制性衰老。比较了从绝经前和绝经后乳房手术组织获得的上皮细胞衍生的细胞系。此外,比较了使用两种不同的遗传干预技术绕过停滞产生的品系:转导下调p16 INK4A 的shRNA或过度表达的组成型活性细胞周期蛋白D1 / CDK2。在所有情况下,复制性衰老屏障都被c-Myc的转导所绕过。来自所有产生的永生系的细胞均表现出正常的核型。沿袭特异性标记的免疫荧光,流式细胞仪和基因表达分析被用于对永生化系的内在亚型进行分类。在年轻菌株中用p16 shRNA绕过淤滞产生的细胞系始终是基底样的,但从较老菌株检测的细胞系表现出一些管腔特征,例如角蛋白19和雌激素受体表达。细胞周期蛋白D1 / CDK2的过表达导致年轻和老菌株产生角蛋白19阳性,管腔样细胞系,而从老菌株中检出的细胞系显示雌激素受体表达。因此,年龄和绕过淤滞的方法独立地影响着永生化的人类乳腺上皮细胞的亚型。

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