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国家自然科学基金(81241052)

作品数:2 被引量:9H指数:1
相关作者:王春梅陈京潘衍有白波更多>>
相关机构:济宁医学院更多>>
发文基金:国家自然科学基金更多>>
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小鼠OX2βR突变体表达载体的构建
2013年
目的通过分子生物学方法构建小鼠Orexin 2β受体(mOX2βR)C末端突变表达载体。方法设计特异性引物,采用聚合酶链反应(PCR)技术,通过胶回收、酶切、连接、转化和测序等生物技术,构建mOX2βR突变体的表达载体。结果成功构建mOX2βR突变表达载体,将其分别命名为mu1、mu2和mu3。结论成功构建了mOX2βR C端不同的突变体,为进一步研究mOX2βR C末端氨基酸在信号通路中的作用奠定了基础。
潘衍有王春梅陈京白波
关键词:突变体G蛋白耦联受体
Programmed Death Ligand-1 on Microglia Regulates Th1 Differentiation via Nitric Oxide in Experimental Autoimmune Encephalomyelitis被引量:9
2016年
Microglia are considered to be potential anti- gen-presenting cells and have the ability to present antigen under pathological conditions. Nevertheless, whether and how microglia are involved in immune regulation are lar- gely unknown. Here, we investigated the suppressive activity of microglia during experimental autoimmune encephalomyelitis (EAE) induced by myelin oligodendro- cyte glycoprotein, with the goal of understanding their role in regulating the T cell reaction. Using flow cytometric analysis, we found that microglia were characterized by increased cell number and up-regulated programmed death ligand-1 (PD-L1) at the peak phase of EAE. Meanwhile, both the CD4+ T cells and microglia that infiltrated the central nervous system expressed higher levels of PD1, the receptor for PD-L1, accompanied by a decline of Thl cells. In an ex vivo co-culture system, microglia from EAE mice inhibited the proliferation of antigen-specific CD4+ T cells and the differentiation of Thl cells, and this was significantly inhibited by PD-L 1 blockade. Further, microglia suppressed Thl cells via nitric oxide (NO), the production of which was dependent on PD-L1. Thus, these data suggest a scenario in which microglia are involved in the regulation of EAE by suppressing Thl-cell differenti- ation via the PD-L1-NO pathway.
Jingxia HuHao HeZhengang YangGuangming ZhuLi KangXiuli JingHai LuWengang SongBo BaiHua Tang
关键词:MICROGLIA
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