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Stable Changes in Mesenchymal Stromal Cells from Multiple Myeloma Patients Revealed through Their Responses to Toll-Like Receptor Ligands and Epidermal Growth Factor

机译:多发性骨髓瘤患者间质基质细胞的稳定变化通过对收费受体配体和表皮生长因子的反应得以揭示

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In human multiple myeloma (MM), the tumor cells exhibit strict dependence on bone marrow (BM) stromal elements. It has been suggested that, in turn, MM cells modify multipotent stromal cells (MSCs), diverting them to support the myeloma. We investigated MM-derived MSCs by comparing their toll-like receptor (TLR) responses to those of MSCs derived from healthy controls. We now report that MM-derived MSCs manifested intact proliferation responses and IL-6 secretion and their adipose and osteogenic differentiation responses to TLR ligands were also similar to those of healthy controls, ranging from augmentation to inhibition. However, MM-derived MSCs were found to be defective in IL-8 secretion and ERK1/2 phosphorylation following TLR-2 activation. Moreover, MM-derived MSCs failed to respond to EGF by elevation of ERK1/2 phosphorylation. The persistence of these changes in extensively cultured MM-derived MSCs, suggests that these cells are stably, if not irreversibly modified.
机译:在人类多发性骨髓瘤(MM)中,肿瘤细胞表现出对骨髓(BM)基质成分的严格依赖性。已经提出,MM细胞依次修饰多能基质细胞(MSC),使其转移以支持骨髓瘤。我们通过比较其toll样受体(TLR)反应与源自健康对照的MSC的反应,研究了MM衍生的MSC。我们现在报道,MM来源的MSCs表现出完整的增殖反应和IL-6分泌,它们对TLR配体的脂肪和成骨分化反应也与健康对照相似,从增强到抑制。但是,发现在TLR-2激活后,MM来源的MSC在IL-8分泌和ERK1 / 2磷酸化方面存在缺陷。此外,MM来源的MSC不能通过提高ERK1 / 2磷酸化来响应EGF。这些变化在大量培养的MM来源的MSC中的持久性表明,这些细胞即使不是不可逆转地被修饰,也可以稳定存在。

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