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Mimicking the Tumor Microenvironment to Regulate Macrophage Phenotype and Assessing Chemotherapeutic Efficacy in Embedded Cancer Cell/Macrophage Spheroid Models

机译:模拟肿瘤微环境来调节巨噬细胞表型和评估嵌入式癌细胞/巨噬细胞球体模型中的化学治疗功效。

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摘要

Tumor associated macrophages (TAMs) are critical stromal components intimately involved with the progression, invasion, and metastasis of cancer cells. To address the need for an in vitro system that mimics the clinical observations of TAM localizations and subsequent functional performance, a cancer cell/macrophage spheroid model is described. The central component of the model is a triple negative breast cancer spheroid embedded in a three-dimensional collagen gel. Macrophages are incorporated in two different ways. The first is a heterospheroid, a spheroid containing both tumor cells and macrophages. The heterospheroid mimics the population of TAMs infiltrated into the tumor mass, thus being exposed to hypoxia and metabolic gradients. In the second model, macrophages are diffusely seeded in the collagen surrounding the spheroid, thus modeling TAMs in the cancer stroma. The inclusion of macrophages as a heterospheroid changes the metabolic profile, indicative of synergistic growth. In contrast, macrophages diffusely seeded in the collagen bear the same profile regardless of the presence of a tumor cell spheroid. The macrophages in the heterospheroid secrete EGF, a cytokine critical to tumor/macrophage co-migration, and an EGF inhibitor decreases the metabolic activity of the heterospheroid, which is not observed in the other systems. The increased secretion of IL-10 indicates that the heterospheroid macrophages follow an M2/TAM differentiation pathway. Lastly, the heterospheroid exhibits resistance to paclitaxel. In summary, the collagen embedded heterospheroid model promotes TAM-like characteristics, and will be of utility in cancer biology and drug discovery.
机译:肿瘤相关的巨噬细胞(TAM)是与癌细胞的进展,侵袭和转移密切相关的关键基质成分。为了满足对模拟TAM定位和后续功能性能的临床观察的体外系统的需求,描述了癌细胞/巨噬细胞球体模型。该模型的主要组成部分是嵌入三维胶原蛋白凝胶中的三阴性乳腺癌球体。巨噬细胞以两种不同方式结合。第一个是异球体,既包含肿瘤细胞又包含巨噬细胞的球体。异球体模拟渗透到肿瘤块中的TAM群体,从而暴露于低氧和代谢梯度中。在第二种模型中,巨噬细胞散布在球体周围的胶原蛋白中,从而在癌症基质中模拟TAM。巨噬细胞作为异球体的包含改变了代谢谱,表明协同生长。相反,分散存在于胶原蛋白中的巨噬细胞具有相同的轮廓,而与肿瘤细胞球体的存在无关。异球体中的巨噬细胞分泌EGF,这是一种对肿瘤/巨噬细胞共迁移至关重要的细胞因子,而EGF抑制剂会降低异球体的代谢活性,这在其他系统中没有观察到。 IL-10分泌的增加表明异球形巨噬细胞遵循M2 / TAM分化途径。最后,异球形体显示出对紫杉醇的抗性。总之,胶原蛋白嵌入的异球形模型促进了TAM样特征,并将在癌症生物学和药物发现中有用。

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