School of Chemistry and Biochemistry, Faculty of Science, The University of Western Australia Perth, WA, Australia ; School of Anatomy, Physiology and Human Biology, Faculty of Science, The University of Western Australia Perth, WA, Australia.
Front Oncol. 2013 Apr 11;3:79. doi: 10.3389/fonc.2013.00079. eCollection 2013.
Breast cancers with lactating features, some of which are associated with pregnancy and lactation, are often poorly differentiated, lack estrogen receptor, progesterone receptor, and HER2 expression and have high mortality. Very little is known about the molecular mechanisms that drive uncontrolled cell proliferation in these tumors and confer lactating features. We have recently reported expression of OCT4 and associated embryonic stem cell self-renewal genes in the normal lactating breast and breastmilk stem cells (hBSCs). This prompted us to examine OCT4 expression in breast cancers with lactating features and compare it with that observed during normal lactation, using rare specimens of human lactating breast. In accordance with previous literature, the normal resting breast (from non-pregnant, non-lactating women) showed minimal OCT4 nuclear expression (0.9%). However, this increased in the normal lactating breast (11.4%), with further increase in lactating adenomas, lactating carcinomas, and pregnancy-associated breast cancer (30.7-48.3%). OCT4 was expressed in the epithelium and at lower levels in the stroma, and was co-localized with NANOG. Comparison of normal non-tumorigenic hBSCs with OCT4-overexpressing tumorigenic breast cell lines (OTBCs) demonstrated upregulation of OCT4, SOX2, and NANOG in both systems, but OTBCs expressed OCT4 at significantly higher levels than SOX2 and NANOG. Similar to hBSCs, OTBCs displayed multi-lineage differentiation potential, including the ability to differentiate into functional lactocytes synthesizing milk proteins both in vitro and in vivo. Based on these findings, we propose a hypothesis of normal and malignant transformation in the breast, which centers on OCT4 and its associated gene network. Although minimal expression of these embryonic genes can be seen in the breast in its resting state throughout life, a controlled program of upregulation of this gene network may be a potential regulator of the normal remodeling of the breast toward a milk-secretory organ during pregnancy and lactation. Deregulation of this gene network either within or outside pregnancy and lactation may lead to aberrant breast cell proliferation and malignant transformation, suggesting a role of these genes in both normal lactation and breast oncogenesis.
具有泌乳特征的乳腺癌,其中一些与妊娠和哺乳有关,通常分化不良,缺乏雌激素受体、孕激素受体和 HER2 表达,死亡率高。对于驱动这些肿瘤中不受控制的细胞增殖并赋予泌乳特征的分子机制,我们知之甚少。我们最近报道了 OCT4 的表达及其相关的胚胎干细胞自我更新基因在正常泌乳乳房和乳腺干细胞 (hBSC) 中。这促使我们检查具有泌乳特征的乳腺癌中 OCT4 的表达,并使用人类泌乳乳房的罕见标本与正常泌乳时进行比较。与之前的文献一致,正常静止的乳房(来自非妊娠、非哺乳的女性)显示出最小的 OCT4 核表达(0.9%)。然而,在正常泌乳的乳房中,OCT4 的表达增加(11.4%),在泌乳腺瘤、泌乳癌和妊娠相关乳腺癌中进一步增加(30.7-48.3%)。OCT4 在乳腺上皮细胞中表达,在基质中表达水平较低,与 NANOG 共定位。将正常非致瘤性 hBSC 与过表达 OCT4 的致瘤性乳腺细胞系(OTBC)进行比较,结果表明两个系统中 OCT4、SOX2 和 NANOG 的表达均上调,但 OTBC 中 OCT4 的表达水平明显高于 SOX2 和 NANOG。与 hBSC 类似,OTBC 显示出多谱系分化潜能,包括在体外和体内分化为合成乳蛋白的功能性泌乳细胞的能力。基于这些发现,我们提出了一个关于乳房正常和恶性转化的假说,该假说以 OCT4 及其相关基因网络为中心。虽然在生命的整个静止状态,这些胚胎基因在乳房中可以看到最小程度的表达,但该基因网络的受控上调程序可能是妊娠和哺乳期间乳房向乳汁分泌器官正常重塑的潜在调节剂。该基因网络在妊娠和哺乳内外的失调可能导致异常的乳腺细胞增殖和恶性转化,这表明这些基因在正常泌乳和乳腺癌发生中都有作用。
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