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Microglia Stimulation by Protein Extract of Injured Rat Spinal Cord. A Novel In vitro Model for Studying Activated Microglia

机译:受伤大鼠脊髓蛋白质提取物的小凝血酶刺激。一种研究活性微胶囊的新型体外模型

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摘要

Research on microglia has established the differentiation between the so-called M1 and M2 phenotypes. However, new frameworks have been proposed attempting to discern between meaningful microglia profiles. We have set up an in vitro microglial activation model by adding an injured spinal cord (SCI) lysate to microglial cultures, obtained from postnatal rats, in order to mimic the environment of the spinal cord after injury. We found that under the presence of the SCI lysate microglial cells changed their phenotype, developing less ramified but longer processes, and proliferated. The SCI lysate also led to upregulation of pro-inflammatory cytokines, such as IL-1β, IL-6, and TNF-α, downregulation of the anti-inflammatory cytokines IL-10 and IL-4, and a biphasic profile of iNOS. In addition, a latex beads phagocytosis assay revealed the SCI lysate stimulated the phagocytic capacity of microglia. Flow cytometry analysis indicated that microglial cells showed a pro-inflammatory profile in the presence of SCI lysate. Finally, characterization of the microglial activation in the spinal cord on day 7 after contusion injury, we showed that these cells have a pro-inflammatory phenotype. Overall, these results indicate that the use of SCI lysates could be a useful tool to skew microglia towards a closer phenotype to that observed after the spinal cord contusion injury than the use of LPS or IFNγ.
机译:微胶质细胞研究建立了所谓的M1和M2表型之间的分化。但是,已经提出了新的框架试图在有意义的微胶质细胞概况之间辨别。我们通过将受损的脊髓(SCI)裂解物添加到从产后大鼠获得的小胶质型培养物中,以模仿肺部后脊髓的环境来建立体外的微胶质激活模型。我们发现在SCI裂解物的存在下,微胶质细胞改变了它们的表型,显影性较少但更长的过程,并增殖。 SCI裂解物还导致促炎细胞因子的上调,例如IL-1β,IL-6和TNF-α,下调抗炎细胞因子IL-10和IL-4,以及INOS的双相曲线。此外,乳胶珠吞噬症测定显示SCI裂解物刺激了微胶质细胞的吞噬能力。流式细胞术分析表明,在SCI裂解物存在下,微胶质细胞显示出促炎症。最后,在挫伤后第7天在第7天脊髓中微胶质激活的表征,我们表明这些细胞具有促炎表型。总的来说,这些结果表明,使用SCI裂解物可以是抗脊髓挫伤后观察到的较近表型的有用工具,而不是使用LPS或IFNγ。

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