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首页> 外文期刊>American Journal of Physiology >Neonatal stem cells exhibit specific characteristics in function, proliferation, and cellular signaling that distinguish them from their adult counterparts
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Neonatal stem cells exhibit specific characteristics in function, proliferation, and cellular signaling that distinguish them from their adult counterparts

机译:新生儿干细胞在功能,增殖和细胞信号传导方面表现出特定特征,这使其与成年干细胞有所区别

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Stem cells may be a novel treatment modality for organ ischemia, possibly through beneficial paracrine mechanisms. Stem cells from older hosts have been shown to exhibit decreased function during stress. We therefore hypothesized that 1) neonatal bone marrow mesenchymal stem cells (nBMSCs) would produce different levels of IL-6, VEGF, and IGF-1 compared with adults (aBMSCs) when stimulated with TNF or LPS; 2) differences in cytokines would be due to distinct cellular characteristics, such as proliferation or pluripotent potential; and 3) differences in cytokines would be associated with differences in p38 MAPK and ERK signaling within nBMSCs. BMSCs were isolated from adult and neonatal mice. Cells were exposed to TNF or LPS with or without p38 or ERK inhibition. Growth factors were measured via ELISA, proliferation via daily cell counts, cell surface markers via flow cytometry, and pluripotent potential via alkaline phosphatase activity. nBMSCs produced lower levels of IL-6 and VEGF, but higher levels of IGF-1 under basal conditions, as well as after stimulation with TNF, but not LPS. Neonatal and adult BMSCs had similar pluripotent potentials and cell surface markers, but nBMSCs proliferated faster. Furthermore, p38 and ERK appeared to play a more substantial role in nBMSC cytokine and growth factor production. Neonatal stem cells may aid in decreasing the local inflammatory response during ischemia, and could possibly be expanded more rapidly than adult cells prior to therapeutic use.
机译:干细胞可能是有益的旁分泌机制,可能是器官缺血的一种新型治疗方式。已经显示,来自较老宿主的干细胞在压力下表现出降低的功能。因此,我们假设1)当用TNF或LPS刺激时,与成人(aBMSC)相比,新生儿骨髓间充质干细胞(nBMSC)会产生不同水平的IL-6,VEGF和IGF-1; 2)细胞因子的差异将归因于明显的细胞特征,例如增殖或多能性; 3)细胞因子的差异与nBMSCs中p38 MAPK和ERK信号的差异有关。从成年和新生小鼠中分离出BMSC。使细胞暴露于具有或不具有p38或ERK抑制的TNF或LPS。通过ELISA测定生长因子,通过每日细胞计数测定增殖,通过流式细胞术测定细胞表面标志物,并通过碱性磷酸酶活性测定多潜能。 nBMSC在基础条件下以及在用TNF(而非LPS)刺激后产生较低水平的IL-6和VEGF,但较高水平的IGF-1。新生和成年BMSC具有相似的全能潜能和细胞表面标记,但nBMSC增殖更快。此外,p38和ERK在nBMSC细胞因子和生长因子的产生中似乎起着更重要的作用。新生儿干细胞可能有助于减少局部缺血过程中的局部炎症反应,并且可能比治疗前的成年细胞更快地扩增。

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