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Synovial expression of Th17-related and cancer-associated genes is regulated by the arthritis severity locus Cia10

机译:Th17相关基因和癌症相关基因的滑膜表达受关节炎严重程度基因座Cia10调控

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We have previously identified Cia10 as an arthritis severity and articular damage quantitative trait locus. In this study, we used Illumina RatRef-12 microarrays to analyze the expression of 21 922 genes in synovial tissues from arthritis-susceptible DA and arthritis-protected DA.ACI(Cia10) congenics with pristane-induced arthritis. 310 genes had significantly different expression. The genes upregulated in DA, and reciprocally downregulated in DA.ACI(Cia10) included IL-11, Ccl12 and Cxcl10, as well as genes implicated in Th17 responses such as IL-17A, IL-6, Ccr6, Cxcr3 and Stat4. Suppressors of immune responses Tgfb and Vdr, and inhibitors of oxidative stress were upregulated in congenics. There was an over-representation of genes implicated in cancer and cancer-related phenotypes such as tumor growth and invasion among the differentially expressed genes. Cancer-favoring genes like Ctsd, Ikbke, and Kras were expressed in increased levels in DA, whereas inhibitors of cancer phenotypes such as Timp2, Reck and Tgfbr3 were increased in DA.ACI(Cia10). These results suggest that Cia10 may control arthritis severity, synovial hyperplasia and joint damage via the regulation of the expression of cancer-related genes, inflammatory mediators and Th17-related markers. These new findings have the potential to generate new targets for therapies aimed at reducing arthritis severity and joint damage in rheumatoid arthritis.
机译:我们之前已将Cia10确定为关节炎严重程度和关节损伤定量特征性位点。在这项研究中,我们使用Illumina RatRef-12芯片分析了关节炎易感DA和关节炎保护的DA.ACI(Cia10)同基因同rist烷诱导的关节炎的滑膜组织中21 922个基因的表达。 310个基因的表达明显不同。在DA中上调的基因,在DA.ACI(Cia10)中相反地下调的基因包括IL-11,Ccl12和Cxcl10,以及与Th17反应有关的基因,例如IL-17A,IL-6,Ccr6,Cxcr3和Stat4。免疫应答Tgfb和Vdr的抑制剂以及氧化应激的抑制剂在同类动物中上调。在差异表达的基因之间存在与癌症和与癌症相关的表型(如肿瘤生长和侵袭)有关的基因的过度表达。有利于癌症的基因(如Ctsd,Ikbke和Kras)在DA中表达水平升高,而癌症表型的抑制剂(如Timp2,Reck和Tgfbr3)在DA.ACI中表达升高(Cia10)。这些结果表明,Cia10可能通过调节癌症相关基因,炎症介质和Th17相关标志物的表达来控制关节炎的严重程度,滑膜增生和关节损伤。这些新发现有可能为减少类风湿性关节炎的关节炎严重程度和关节损伤的疗法产生新的靶标。

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