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首页> 外文期刊>Cell death & disease. >Epothilone B impairs functional recovery after spinal cord injury by increasing secretion of macrophage colony-stimulating factor
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Epothilone B impairs functional recovery after spinal cord injury by increasing secretion of macrophage colony-stimulating factor

机译:埃博霉素B通过增加巨噬细胞集落刺激因子的分泌而损害脊髓损伤后的功能恢复

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摘要

The microtubule-stabilizing drug epothilone B (epoB) has shown potential value in the treatment of spinal cord injury (SCI) through diverse mechanisms. However, it remains elusive why a limited overall effect was observed. We aim to investigate the limiting factors underlying functional recovery promoted by epoB. The same SCI model treated by epoB was established as discussed previously. We used a cerebrospinal fluid (CSF) sample to assess the changes in cytokines in milieu of the SCI lesion site after epoB treatment. We then analyzed the source of cytokines, the state of microglia/macrophages/monocytes (M/Ms), and the recruitment of neutrophil in the lesion site by using the results of antibody array. Following these findings, we further evaluated the motor functional recovery caused by the reshaped microenvironment. Systemic administration of epoB significantly increased levels of several cytokines in the CSF of the rat SCI model; macrophage colony-stimulating factor (M-CSF) secreted by intact central nervous system (CNS) cells was one of the cytokines with increased levels. Along with epoB and other cytokines, M-CSF reshapes the SCI milieu by activating the microglias, killing bone marrow-derived macrophages, polarizing the M/M to M1 phenotype, and activating downstream cytokines to exacerbate the SCI injury, but it also increases the expression of neurotrophic factors. Anti-inflammatory therapy using a neutralizing antibody mix shows encouraging results. Using in vivo experiments, our findings indicate that epoB inhibits the SCI functional recovery in many ways by reshaping the milieu, which counteracts the therapeutic efficacy that led to the limited overall effectiveness.
机译:微管稳定药物埃坡霉素B(epoB)已通过多种机制在治疗脊髓损伤(SCI)中显示出潜在价值。但是,为什么观察到有限的整体效果仍然难以捉摸。我们旨在调查由epoB促进功能恢复的限制因素。如前所述,建立了由epoB处理的相同SCI模型。我们使用脑脊液(CSF)样本评估epoB治疗后SCI病变部位环境中细胞因子的变化。然后,我们通过使用抗体阵列的结果分析了细胞因子的来源,小胶质细胞/巨噬细胞/单核细胞(M / Ms)的状态以及病变部位中性粒细胞的募集。根据这些发现,我们进一步评估了由重塑的微环境引起的运动功能恢复。全身施用epoB会显着增加大鼠SCI模型的CSF中几种细胞因子的水平;完整的中枢神经系统(CNS)细胞分泌的巨噬细胞集落刺激因子(M-CSF)是水平升高的细胞因子之一。 M-CSF与epoB和其他细胞因子一起,通过激活小胶质细胞,杀死骨髓衍生的巨噬细胞,将M / M极化为M1表型以及激活下游细胞因子来加剧SCI损伤,从而重塑SCI损伤,但同时也增加了SCI损伤。神经营养因子的表达。使用中和抗体混合物的抗炎治疗显示出令人鼓舞的结果。使用体内实验,我们的发现表明epoB通过重塑环境以多种方式抑制SCI功能恢复,这抵消了导致有限整体效果的治疗功效。

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