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Experimental Type 2 Diabetes Differently Impacts on the Select Functions of Bone Marrow-Derived Multipotent Stromal Cells

机译:实验2型糖尿病对骨髓衍生的多能基质细胞的选择功能不同

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摘要

Bone marrow-derived multipotent stromal cells (BMMSCs) represent an attractive therapeutic modality for cell therapy in type 2 diabetes mellitus (T2DM)-associated complications. T2DM changes the bone marrow environment; however, its effects on BMMSC properties remain unclear. The present study aimed at investigating select functions and differentiation of BMMSCs harvested from the T2DM microenvironment as potential candidates for regenerative medicine. BMMSCs were obtained from Zucker diabetic fatty (ZDF; an obese-T2DM model) rats and their lean littermates (ZL; controls), and cultured under normoglycemic conditions. The BMMSCs derived from ZDF animals were fewer in number, with limited clonogenicity (by 2-fold), adhesion (by 2.9-fold), proliferation (by 50%), migration capability (by 25%), and increased apoptosis rate (by 2.5-fold) compared to their ZL counterparts. Compared to the cultured ZL-BMMSCs, the ZDF-BMMSCs exhibited (i) enhanced adipogenic differentiation (increased number of lipid droplets by 2-fold; upregulation of the Pparg, AdipoQ, and Fabp genes), possibly due to having been primed to undergo such differentiation in vivo prior to cell isolation, and (ii) different angiogenesis-related gene expression in vitro and decreased proangiogenic potential after transplantation in nude mice. These results provided evidence that the T2DM environment impairs BMMSC expansion and select functions pertinent to their efficacy when used in autologous cell therapies.
机译:骨髓衍生的多能基质细胞(BMMSCs)代表2型糖尿病(T2DM)的细胞疗法的有吸引力的治疗方式。 T2DM改变骨髓环境;然而,它对BMMSC性质的影响仍然不清楚。目前研究旨在研究从T2DM微环境收获的BMMSCs的选择和分化作为再生医学的潜在候选者。从Zucker糖尿病脂肪(ZDF;肥胖-T2DM模型)大鼠及其瘦凋落物(ZL;对照组)获得BMMSCs,并在正常血糖条件下培养。源自ZDF动物的BMMSC数量较少,克隆因克隆性有限(2倍),粘附(递增2.9倍),增殖(50%),迁移能力(递增25%),并增加凋亡率(通过2.5倍)与其ZL对应物相比。与培养的ZL-BMMSCs相比,ZDF-BMMSCs表现出来(i)增强脂肪发生分化(增加脂液滴数增加2倍; PPARG,AdipoQ和Fabp基因的上调),可能是由于被灌注来进行在细胞分离之前体内的这种分化,和(ii)在体外不同血管生成相关的基因表达,并在裸鼠移植后降低致癌潜力。这些结果提供了证据表明,T2DM环境损害BMMSC扩展,并在用于自体细胞疗法中使用时选择与它们的功效相关的功能。

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