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首页> 外文期刊>The journal of clinical investigation >Transcription factor ICBP90 regulates the MIF promoter and immune susceptibility locus
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Transcription factor ICBP90 regulates the MIF promoter and immune susceptibility locus

机译:转录因子ICBP90调节MIF启动子和免疫敏感性基因座

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The immunoregulatory cytokine macrophage migration inhibitory factor (MIF) is encoded in a functionally polymorphic locus that is linked to the susceptibility of autoimmune and infectious diseases. The MIF promoter contains a 4-nucleotide microsatellite polymorphism (–794 CATT) that repeats 5 to 8 times in the locus, with greater numbers of repeats associated with higher mRNA levels. Because there is no information about the transcriptional regulation of these common alleles, we used oligonucleotide affinity chromatography and liquid chromatography–mass spectrometry to identify nuclear proteins that interact with the –794 CATT_(5–8) site. An analysis of monocyte nuclear lysates revealed that the transcription factor ICBP90 (also known as UHRF1) is the major protein interacting with the MIF microsatellite. We found that ICBP90 is essential for MIF transcription from monocytes/macrophages, B and T lymphocytes, and synovial fibroblasts, and TLR-induced MIF transcription is regulated in an ICBP90- and –794 CATT_(5–8) length–dependent manner. Whole-genome transcription analysis of ICBP90 shRNA–treated rheumatoid synoviocytes uncovered a subset of proinflammatory and immune response genes that overlapped with those regulated by MIF shRNA. In addition, the expression levels of ICBP90 and MIF were correlated in joint synovia from patients with rheumatoid arthritis. These findings identify ICBP90 as a key regulator of MIF transcription and provide functional insight into the regulation of the polymorphic MIF locus.
机译:免疫调节细胞因子巨噬细胞迁移抑制因子(MIF)在功能多态性位点编码,该位点与自身免疫和传染病的易感性有关。 MIF启动子包含4个核苷酸的微卫星多态性(–794 CATT),在基因座中重复5至8次,重复次数越多,mRNA水平越高。由于没有关于这些常见等位基因转录调控的信息,我们使用寡核苷酸亲和色谱和液相色谱-质谱法鉴定与–794 CATT_(5-8)位点相互作用的核蛋白。对单核细胞核裂解物的分析显示,转录因子ICBP90(也称为UHRF1)是与MIF微卫星相互作用的主要蛋白质。我们发现ICBP90对于从单核细胞/巨噬细胞,B和T淋巴细胞以及滑膜成纤维细胞进行MIF转录至关重要,并且TLR诱导的MIF转录以ICBP90和–794 CATT_(5-8)长度依赖的方式调控。对经ICBP90 shRNA处理的类风湿滑膜细胞进行全基因组转录分析,发现了与MIF shRNA调控的基因重叠的促炎和免疫应答基因子集。另外,类风湿关节炎患者的关节滑膜中ICBP90和MIF的表达水平相关。这些发现确定ICBP90是MIF转录的关键调节因子,并为多态性MIF基因座的调控提供了功能性见解。

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