首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Genomic and proteomic microglial profiling: pathways for neuroprotective inflammatory responses following nerve fragment clearance and activation.
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Genomic and proteomic microglial profiling: pathways for neuroprotective inflammatory responses following nerve fragment clearance and activation.

机译:基因组和蛋白质组学小胶质细胞分析:神经碎片清除和激活后神经保护性炎症反应的途径。

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摘要

Microglia, a primary immune effector cell of the central nervous system (CNS) affects homeostatic, neuroprotective, regenerative and degenerative outcomes in health and disease. Despite these broad neuroimmune activities linked to specific environmental cues, a precise cellular genetic profile for microglia in the context of disease and repair has not been elucidated. To this end we used nucleic acid microarrays, proteomics, immunochemical and histochemical tests to profile microglia in neuroprotective immune responses. Optic and sciatic nerve (ON and SN) fragments were used to stimulate microglia in order to reflect immune consequences of nervous system injury. Lipopolysaccharide and latex beads-induced microglial activation served as positive controls. Cytosolic and secreted proteins were profiled by surface enhanced laser desorption ionization-time of flight (SELDI-TOF) ProteinChip((R)), 1D and 2D difference gel electrophoresis. Proteins were identified by peptide sequencing with tandem mass spectrometry, ELISA and western blot tests. Temporal expression of pro-inflammatory cytokines, antioxidants, neurotrophins, and lysosomal enzyme expression provided, for the first time, a unique profile of secreted microglia proteins with neuroregulatory functions. Most importantly, this molecular and biochemical signature supports a broad range of microglial functions for debris clearance and promotion of neural repair after injury.
机译:小胶质细胞是中枢神经系统(CNS)的主要免疫效应细胞,可影响健康和疾病的体内稳态,神经保护,再生和退化。尽管这些广泛的神经免疫活性与特定的环境线索有关,但尚未阐明在疾病和修复情况下小胶质细胞的精确细胞遗传学特征。为此,我们使用了核酸微阵列,蛋白质组学,免疫化学和组织化学测试来对神经保护性免疫反应中的小胶质细胞进行分析。使用视神经和坐骨神经(ON和SN)片段刺激小胶质细胞,以反映神经系统损伤的免疫后果。脂多糖和乳胶珠诱导的小胶质细胞活化充当阳性对照。通过表面增强的激光解吸电离飞行时间(SELDI-TOF)ProteinChip(R),1D和2D差异凝胶电泳来分析胞浆和分泌的蛋白。通过串联质谱,ELISA和蛋白质印迹试验的肽测序鉴定蛋白质。促炎性细胞因子,抗氧化剂,神经营养蛋白和溶酶体酶的时间表达首次提供了分泌的具有神经调节功能的小胶质细胞蛋白的独特图谱。最重要的是,这种分子和生化特征支持广泛的小胶质细胞功能,以清除碎片并促进损伤后的神经修复。

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