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首页> 美国卫生研究院文献>Journal of Virology >Role of NF-κB in Cell Survival and Transcription of Latent Membrane Protein 1-Expressing or Epstein-Barr Virus Latency III-Infected Cells
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Role of NF-κB in Cell Survival and Transcription of Latent Membrane Protein 1-Expressing or Epstein-Barr Virus Latency III-Infected Cells

机译:NF-κB在潜伏膜蛋白1表达或爱泼斯坦-巴尔病毒潜伏期III感染细胞的存活和转录中的作用

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Epstein-Barr virus (EBV) latency III infection converts B lymphocytes into lymphoblastoid cell lines (LCLs) by expressing EBV nuclear and membrane proteins, EBNAs, and latent membrane proteins (LMPs), which regulate transcription through Notch and tumor necrosis factor receptor pathways. The role of NF-κB in LMP1 and overall EBV latency III transcriptional effects was investigated by treating LCLs with BAY11-7082 (BAY11). BAY11 rapidly and irreversibly inhibited NF-κB, decreased mitochondrial membrane potential, induced apoptosis, and altered LCL gene expression. BAY11 effects were similar to those of an NF-κB inhibitor, ΔN-IκBα, in effecting decreased JNK1 expression and in microarray analyses. More than 80% of array elements that decreased with ΔN-IκBα expression decreased with BAY11 treatment. Newly identified NF-κB-induced, LMP1-induced, and EBV-induced genes included pleckstrin, Jun-B, c-FLIP, CIP4, and IκBɛ. Of 776 significantly changed array elements, 134 were fourfold upregulated in EBV latency III, and 74 were fourfold upregulated with LMP1 expression alone, whereas only 28 were more than fourfold downregulated by EBV latency III. EBV latency III-regulated gene products mediate cell migration (EBI2, CCR7, RGS1, RANTES, MIP1α, MIP1β, CXCR5, and RGS13), antigen presentation (major histocompatibility complex proteins and JAW1), mitogen-activated protein kinase pathway (DUSP5 and p62Dok), and interferon (IFN) signaling (IFN-γRα, IRF-4, and STAT1). Comparison of EBV latency III LCL gene expression to immunoglobulin M (IgM)-stimulated B cells, germinal-center B cells, and germinal-center-derived lymphomas clustered LCLs with IgM-stimulated B cells separately from germinal-center cells or germinal-center lymphoma cells. Expression of IRF-2, AIM1, ASK1, SNF2L2, and components of IFN signaling pathways further distinguished EBV latency III-infected B cells from IgM-stimulated or germinal-center B cells.
机译:爱泼斯坦-巴尔病毒(EBV)潜伏期III感染通过表达EBV核蛋白和膜蛋白,EBNA和潜伏膜蛋白(LMP)将B淋巴细胞转化为成淋巴细胞样细胞系(LCL),后者通过Notch和肿瘤坏死因子受体途径调节转录。通过用BAY11-7082(BAY11)处理LCL,研究了NF-κB在LMP1和总体EBV潜伏期III转录作用中的作用。 BAY11快速且不可逆地抑制NF-κB,降低线粒体膜电位,诱导细胞凋亡,并改变LCL基因表达。在降低JNK1表达和微阵列分析中,BAY11的作用类似于NF-κB抑制剂ΔN-IκBα。 BAY11处理后,随着ΔN-IκBα表达而减少的阵列元素中,有80%以上会减少。新近鉴定的NF-κB诱导,LMP1诱导和EBV诱导的基因包括pleckstrin,Jun-B,c-FLIP,CIP4和IκBɛ。在776个显着变化的阵列元件中,有134个在EBV潜伏期III中被上调了四倍,而74个在单独的LMP1表达中被上调了四倍,而只有28个在EBV潜伏期III中被下调了四倍以上。 EBV潜伏期III调节的基因产物介导细胞迁移(EBI2,CCR7,RGS1,RANTES,MIP1α,MIP1β,CXCR5和RGS13),抗原呈递(主要组织相容性复合蛋白和JAW1),促分裂原激活的蛋白激酶途径(DUSP5和p62Dok) )和干扰素(IFN)信号传导(IFN-γRα,IRF-4和STAT1)。 EBV潜伏期III LCL基因表达与免疫球蛋白M(IgM)刺激的B​​细胞,生发中心B细胞和生发中心衍生的淋巴瘤的比较,将LCL与IgM刺激的B细胞与生发中心细胞或生发中心分开淋巴瘤细胞。 IRF-2,AIM1,ASK1,SNF2L2和IFN信号通路的表达进一步区分了EBV潜伏期感染的B细胞与IgM刺激或生发中心B细胞。

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