Department of Anatomy, Yong Loo Lin School of Medicine, National University of Singapore, Singapore.
J Neurochem. 2014 Aug;130(3):388-401. doi: 10.1111/jnc.12731. Epub 2014 May 9.
Chronic activation of microglia, the macrophages of the CNS, has been shown to enhance neuronal damage because of excessive release of proinflammatory cytokines and neurotoxic molecules in a number of neurodegenerative diseases. Recent reports showed altered microRNA (miRNA) expression in immune-mediated pathologies, thus suggesting that miRNAs modulate expression of genes involving immune responses. This study demonstrates that miRNA-200b is expressed in microglia and modulates inflammatory response of microglia by regulating mitogen-activated protein kinase pathway. miRNA-200b expression was found to be down-regulated in activated microglia in vivo (traumatic brain injury rat model) and in vitro. A luciferase assay and loss- and gain-of-function studies revealed c-Jun, the transcription factor of cJun-N terminal kinase (JNK) mitogen-activated protein kinase pathway to be the target of miR-200b. Knockdown of miR-200b in microglia increased JNK activity along with an increase in pro-inflammatory cytokines, inducible nitric oxide synthase expression and nitric oxide (NO) production. Conversely, over-expression of miRNA-200b in microglia resulted in a decrease in JNK activity, inducible nitric oxide synthase expression, NO production and migratory potential of activated microglia. Furthermore, miR-200b inhibition resulted in increased neuronal apoptosis after treatment of neuronal cells with conditioned medium obtained from microglial culture. Taken together, these results indicate that miRNA-200b modulates microglial inflammatory process including cytokine secretion, NO production, migration and neuronal survival.
小胶质细胞的慢性激活已被证明会增强神经元损伤,因为在许多神经退行性疾病中,过多释放促炎细胞因子和神经毒性分子。最近的报告显示,免疫介导的病理变化中改变了 microRNA(miRNA)的表达,因此表明 miRNA 调节涉及免疫反应的基因的表达。本研究表明 miRNA-200b 在小胶质细胞中表达,并通过调节丝裂原活化蛋白激酶途径来调节小胶质细胞的炎症反应。miRNA-200b 的表达在体内(创伤性脑损伤大鼠模型)和体外被发现下调。荧光素酶测定和缺失及获得功能研究表明,c-Jun,JNK 丝裂原活化蛋白激酶途径的转录因子,是 miR-200b 的靶标。miR-200b 在小胶质细胞中的敲低增加了 JNK 活性,同时增加了促炎细胞因子、诱导型一氧化氮合酶表达和一氧化氮(NO)的产生。相反,miR-200b 在小胶质细胞中的过表达导致 JNK 活性、诱导型一氧化氮合酶表达、NO 产生和激活小胶质细胞的迁移潜力降低。此外,miR-200b 抑制导致神经元细胞在用小胶质细胞培养物获得的条件培养基处理后神经元凋亡增加。总之,这些结果表明 miRNA-200b 调节小胶质细胞炎症过程,包括细胞因子分泌、NO 产生、迁移和神经元存活。
