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首页> 外文期刊>Molecular Immunology >Expression profiles of genes involved in TLRs and NLRs signaling pathways of water buffaloes infected with Fasciola gigantica
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Expression profiles of genes involved in TLRs and NLRs signaling pathways of water buffaloes infected with Fasciola gigantica

机译:参与参与TLRS和NLRS信号传导途径的基因表达谱,水牛感染Fasciola gigantica

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Infection of ruminants and humans with Fasciola gigantica is attracting increasing attention due to its economic impact and public health significance. However, little is known of innate immune responses during F. gigantica infection. Here, we investigated the expression profiles of genes involved in Toll-like receptors (TLRs) and NOD like receptors (NLRs) signaling pathways in buffaloes infected with 500 F. gigantica metacercariae. Serum, liver and peripheral blood mononuclear cell (PBMC) samples were collected from infected and control buffaloes at 3, 10, 28, and 70 days post infection (dpi). Then, the levels of 12 cytokines in serum samples were evaluated by ELISA. Also, the levels of expression of 42 genes, related to TLRs and NLRs signaling, in liver and PBMCs were determined using custom RT2 Profiler PCR Arrays. At 3 dpi, modest activation of TLR4 and TLR8 and the adaptor protein (TICAM1) was detected. At 10 dpi, NF-kappa B1 and Interferon Regulatory Factor signaling pathways were upregulated along with activation of TLR1, TLR2, TLR6, TLR10, TRAF6, IRF3, TBK1, CASP1, CD80, and IFNA1 in the liver, and inflammatory response with activated TLR4, TLR9, TICAM1, NLRP3, CD86, IL-1B, IL-6, and IL-8 in PBMCs. At 28 dpi, there was increase in the levels of cytokines along with induction of NLRP1 and NLRP3 inflammasomes-dependent immune responses in the liver and PBMCs. At 70 dpi, F. gigantica activated TLRs and NLRs, and their downstream interacting molecules. The activation of TLR7/9 signaling (perhaps due to increased B-cell maturation and activation) and upregulation of NLRP3 gene were also detected. These findings indicate that F. gigantica alters the expression of TLR5 and NLRs genes to evade host immune defenses. Elucidation of the roles of the downstream effectors interacting with these genes may aid in the development of new interventions to control disease caused by F. gigantica infection.
机译:由于经济影响和公共卫生意义,对反刍动物和人类的反刍动物和人类的感染吸引了越来越关注。然而,在F.Gigantica感染期间,已知本质免疫应答少。在此,我们研究了在感染500 f. gigantica metacariae感染的水牛中涉及的Toll样受体(TLR)和NOOD的基因的表达谱和NOOD(NLRS)信号传导途径。在感染后3,10,28和70天的感染和对照水牛收集血清,肝脏和外周血单核细胞(PBMC)样品。然后,通过ELISA评估血清样品中12个细胞因子的水平。此外,使用定制RT2分析器PCR阵列确定与TLR和NLR信号传导相关的42个基因的表达水平,肝脏和PBMC相关。在3 dpi下,检测到适度的TLR4和TLR8和适配器蛋白(Ticam1)的激活。在10dpi,在肝脏中的TLR1,TLR2,TLR6,TLR10,TRAF6,IRF3,TBK1,CASP1,CD80和IFNA1的激活,并激活NF-Kappa B1和干扰素调节因子信号传导途径,以及具有激活的TLR4的炎症反应,PBMC中的TLR9,Ticam1,NLRP3,CD86,IL-1B,IL-6和IL-8。在28 dpi下,细胞因子水平随诱导NLRP1和NLRP3炎症患者肝脏和PBMC中的依赖性免疫应答。在70dpi,F.Gigantica活化的TLR和NLR和下游相互作用分子。还发现了TLR7 / 9信号传导的激活(可能是由于B细胞成熟和激活增加)和NLRP3基因的上调。这些发现表明F.Gigantica改变了TLR5和NLRS基因的表达,以逃避宿主免疫防御。阐明与这些基因相互作用的下游效应器的作用可能有助于制定用于对F.Gigantica感染引起的控制疾病的新干预措施。

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