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Macrophages in multiple myeloma: Emerging concepts and therapeutic implications

机译:多发性骨髓瘤中的巨噬细胞:新兴概念和治疗意义。

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Multiple myeloma, a clonal plasma cell malignancy, has long provided a prototypic model to study regulatory interactions between malignant cells and their microenvironment. Myeloma-associated macrophages have historically received limited scrutiny, but recent work points to central and non-redundant roles in myeloma niche homeostasis. The evidence supports a paradigm of complex, dynamic and often mutable interactions between macrophages and other cellular constituents of the niche. We and others have shown that macrophages support myeloma cell growth, viability and drug resistance through both contact-mediated and non-contact-mediated mechanisms. These tumor-beneficial roles have evolved in opposition to, or in parallel with, intrinsic pro-inflammatory and tumoricidal properties. Thus, simple blockade of protective "don't eat me" signals on the surface of myeloma cells leads to macrophage-mediated myeloma cell killing. Macrophages also enhance the tumor-supportive role of mesenchymal stem/stromal cells (MSCs) in the niche: importantly, this interaction is bidirectional, producing a distinct state of macrophage polarization that we termed "MSC-educated macrophages." The intriguing pattern of cross-talk between macrophages, MSCs and tumor cells highlights the myeloma niche as a dynamic multi-cellular structure. Targeted reprogramming of these interactions harbors significant untapped therapeutic potential, particularly in the setting of minimal residual disease, the main obstacle toward a cure.
机译:多发性骨髓瘤是一种克隆性浆细胞恶性肿瘤,长期以来一直为研究恶性细胞与其微环境之间的调控相互作用提供了一种原型模型。历史上,与骨髓瘤相关的巨噬细胞受到严格的审查,但最近的工作指出了骨髓瘤生态位稳态中的中心作用和非冗余作用。证据支持巨噬细胞和利基的其他细胞成分之间复杂,动态且经常可变的相互作用的范例。我们和其他人已经表明,巨噬细胞通过接触介导的和非接触介导的机制支持骨髓瘤细胞的生长,存活力和耐药性。这些有益于肿瘤的作用已经与固有的促炎和杀肿瘤特性相反或并行发展。因此,对骨髓瘤细胞表面的保护性“不要吃我”信号的简单封锁会导致巨噬细胞介导的骨髓瘤细胞杀伤。巨噬细胞还在小生境中增强了间充质干/基质细胞(MSCs)的肿瘤支持作用:重要的是,这种相互作用是双向的,产生了一种独特的巨噬细胞极化状态,我们称之为“ MSC培养的巨噬细胞”。巨噬细胞,MSC和肿瘤细胞之间有趣的串扰模式突显出骨髓瘤的生态位是动态的多细胞结构。这些相互作用的针对性重编程具有巨大的尚未开发的治疗潜力,尤其是在最小残留疾病(治愈的主要障碍)的情况下。

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