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The importance of the microenvironment in breast cancer progression: recapitulation of mammary tumorigenesis using a unique human mammary epithelial cell model and a three-dimensional culture assay

机译:微环境在乳腺癌进展中的重要性:使用独特的人类乳腺上皮细胞模型和三维培养测定法概述乳腺肿瘤发生

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摘要

The extracellular matrix (ECM) is a dominant regulator of tissue development and homeostasis. “Designer microenvironments” in culture and in vivo model systems have shown that the ECM regulates growth, differentiation, and apoptosis in murine and human mammary epithelial cells (MEC) through a hierarchy of transcriptional events involving the intricate interplay between soluble and physical signaling pathways. Furthermore, these studies have shown that these pathways direct and in turn are influenced by the tissue structure. Tissue structure is directed by the cooperative interactions of the cell–cell and cell–ECM pathways and can be modified by stromal factors. Not surprisingly then, loss of tissue structure and alterations in ECM components are associated with the appearance and dissemination of breast tumors, and malignancy is associated with perturbations in cell adhesion, changes in adhesion molecules, and a stromal reaction. Several lines of evidence now support the contention that the pathogenesis of breast cancer is determined (at least in part) by the dynamic interplay between the ductal epithelial cells, the microenvironment, and the tissue structure (acini). Thus, to understand the mechanisms involved in carcinogenesis, the role of the microenvironment (ECM as well as the stromal cells) with respect to tissue structure should be considered and studied. Towards this goal, we have established a unique human MEC model of tumorigenesis, which in concert with a three-dimensional assay, recapitulates many of the genetic and morphological changes observed in breast cancer in vivo. We are currently using this system to understand the role of the microenvironment and tissue structure in breast cancer progression.
机译:细胞外基质(ECM)是组织发育和体内平衡的主要调节剂。培养物和体内模型系统中的“设计者微环境”表明,ECM通过涉及可溶性和物理信号通路之间复杂相互作用的转录事件层次,调节鼠类和人类乳腺上皮细胞(MEC)的生长,分化和凋亡。此外,这些研究表明,这些途径直接并依次受到组织结构的影响。组织结构由细胞-细胞和细胞-ECM途径的协同相互作用所指导,并可以通过基质因子进行修饰。因此,毫不奇怪,组织结构的丧失和ECM组件的改变与乳腺肿瘤的出现和扩散有关,而恶性与细胞粘附的紊乱,粘附分子的变化和基质反应有关。现在有几条证据支持这样的论点,即乳腺癌的发病机理(至少部分地)由导管上皮细胞,微环境和组织结构(腺泡)之间的动态相互作用决定。因此,要了解与致癌作用有关的机制,应考虑和研究微环境(ECM以及基质细胞)相对于组织结构的作用。为了实现这一目标,我们建立了独特的人类MEC肿瘤发生模型,该模型与三维分析相结合,概括了体内乳腺癌中观察到的许多遗传和形态变化。我们目前正在使用该系统来了解微环境和组织结构在乳腺癌进展中的作用。

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