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首页> 外文期刊>Stem cells and development >Regulation of Mouse Microglia Activation and Effector Functions by Bone Marrow-Derived Mesenchymal Stem Cells
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Regulation of Mouse Microglia Activation and Effector Functions by Bone Marrow-Derived Mesenchymal Stem Cells

机译:小鼠骨髓间充质干细胞对小鼠小胶质细胞活化和效应子功能的调节

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摘要

Mesenchymal stems or stromal cells (MSCs) are rare multipotent cells with potent regenerative and immunomodulatory properties. Microglial cells (MGs) are specialized tissue macrophages of the central nervous system (CNS) that continuously survey their environment with highly motile extensions. Recently, several studies have shown that MSCs are capable of reprogramming microglia into an "M2-like" phenotype characterized by increased phagocytic activity and upregulated expression of anti-inflammatory mediators in vitro. However, the precise polarization states of microglia in the presence of MSCs under physiological or under inflammatory conditions remain largely unknown. In this study, we found that MSCs induce a mixed microglia phenotype defined as Arg1-high, CD86-high, CD206-high, IL-10-high, PGE2-high, MCP-1/CCL2-high, IL-1 beta-moderate, NALP-3-low, and TNF-alpha-low cells. These MSC-elicited MGs have high phagocytic activity and antigen-presenting ability. Lipopolysaccharide is able to shape this microglia phenotype quantitatively, but not qualitatively in the presence of MSCs. This unique polarization state resembles a novel regulatory microglia phenotype, which might contribute to the resolution of inflammation and to tissue repair in the CNS.
机译:间充质干或基质细胞(MSCs)是罕见的多能细胞,具有有效的再生和免疫调节特性。小神经胶质细胞(MGs)是中枢神经系统(CNS)的专门组织巨噬细胞,通过高能动性延伸连续观察其环境。最近,一些研究表明,MSC能够在体外将小胶质细胞重编程为“ M2样”表型,其特征在于吞噬活性增强和抗炎介质的表达上调。但是,在生理或炎症条件下存在MSC的小胶质细胞的精确极化状态仍然未知。在这项研究中,我们发现MSC诱导了混合小胶质细胞表型,定义为Arg1高,CD86高,CD206高,IL-10-高,PGE2高,MCP-1 / CCL2高,IL-1β-中度,NALP-3低和TNF-α低细胞。这些由MSC引起的MG具有高吞噬活性和抗原呈递能力。脂多糖能够定量地塑造这种小胶质细胞表型,但在MSC存在下不能定性地塑造它。这种独特的极化状态类似于新的调节性小胶质细胞表型,可能有助于炎症的消退和中枢神经系统的组织修复。

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