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首页> 外文期刊>Veterinary Pathology >Salmonella enterica causes more severe inflammatory disease in C57/BL6 Nramp1G169 mice than Sv129s6 mice.
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Salmonella enterica causes more severe inflammatory disease in C57/BL6 Nramp1G169 mice than Sv129s6 mice.

机译:肠炎沙门氏菌在C57 / BL6 Nramp1 G169 小鼠中比Sv129s6小鼠引起更严重的炎症性疾病。

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摘要

Salmonella enterica serovar Typhimurium (S. Typhimurium) causes systemic inflammatory disease in mice by colonizing cells of the mononuclear leukocyte lineage. Mouse strains resistant to S. Typhimurium, including Sv129S6, have an intact Nramp1 (Slc11a1) allele and survive acute infection, whereas C57/BL6 mice, homozygous for a mutant Nramp1 allele, Nramp1G169D, develop lethal infections. Restoration of Nramp1 (C57/BL6 Nramp1G169) reestablishes resistance to S. Typhimurium; mice survive at least 3 to 4 weeks postinfection. Since many transgenic mouse strains are on a C57/BL6 genetic background, C57/BL6 Nramp1G169 mice provide a model to examine host genetic determinants of resistance to infection. To further evaluate host immune response to S. Typhimurium, we performed comparative analyses of Sv129S6 and C57/BL6 Nramp1G169 mice 3 weeks following oral S. Typhimurium infection. C57/BL6 Nramp1G169 mice developed more severe inflammatory disease with splenic bacterial counts 1000-fold higher than Sv129S6 mice and relatively greater splenomegaly and blood neutrophil and monocyte counts. Infected C57/BL6 Nramp1G169 mice developed higher proinflammatory serum cytokine and chemokine responses (interferon- gamma , tumor necrosis factor- alpha , interleukin [IL]-1 beta , and IL-2 and monocyte chemotactic protein-1 and chemokine [C-X-C motif] ligand 1, respectively) and marked decreases in anti-inflammatory serum cytokine concentrations (IL-10, IL-4) compared with Sv129S6 mice postinfection. Splenic dendritic cells and macrophages in infected compared with control mice increased to a greater extent in C57/BL6 Nramp1G169 mice than in Sv129S6 mice. Overall, data show that despite the Nramp1 gene present in both strains, C57/BL6 Nramp1G169 mice develop more severe, Th1-skewed, acute inflammatory responses to S. Typhimurium infection compared with Sv129S6 mice. Both strains are suitable model systems for studying inflammation in the context of adaptive immunity.
机译:鼠伤寒沙门氏菌鼠伤寒沙门氏菌(S. Typhimurium)通过使单核白细胞谱系的细胞定殖而在小鼠中引起全身性炎性疾病。对鼠伤寒沙门氏菌具有抗性的小鼠品系,包括Sv129S6,具有完整的Nramp1(Slc11a1)等位基因,并且可以在急性感染中幸存下来,而突变型Nramp1等位基因Nramp1 的纯合子C57 / BL6小鼠则可以致命。 。恢复Nramp1(C57 / BL6 Nramp1 G169 )可恢复对鼠伤寒沙门氏菌的抗性。小鼠在感染后至少存活3至4周。由于许多转基因小鼠品系都具有C57 / BL6遗传背景,因此C57 / BL6 Nramp1 G169 小鼠提供了一个模型来检查宿主抗感染的遗传决定因素。为了进一步评估宿主对鼠伤寒沙门氏菌的免疫反应,我们对鼠伤寒沙门氏菌感染后3周对Sv129S6和C57 / BL6 Nramp1 G169 小鼠进行了比较分析。 C57 / BL6 Nramp1 G169 小鼠发展为更严重的炎症性疾病,脾脏细菌数比Sv129S6小鼠高1000倍,脾肿大,血液中性粒细胞和单核细胞数相对较高。感染的C57 / BL6 Nramp1 G169 小鼠出现较高的促炎血清细胞因子和趋化因子反应(干扰素-γ,肿瘤坏死因子-α,白介素[IL] -1 beta和IL-2和单核细胞趋化蛋白-与感染后的Sv129S6小鼠相比,抗炎血清细胞因子浓度(IL-10,IL-4)显着降低(分别为1和趋化因子[CXC基序]配体1)和明显降低。与Sv129S6小鼠相比,C57 / BL6 Nramp1 G169 小鼠与对照组小鼠相比,脾脏树突状细胞和巨噬细胞的增加幅度更大。总体而言,数据显示,尽管这两个毒株中都存在Nramp1基因,但与Sv129S6小鼠相比,C57 / BL6 Nramp1 G169 小鼠对鼠伤寒沙门氏菌感染产生了更严重的,Th1偏向的急性炎性反应。两种菌株都是用于在适应性免疫的背景下研究炎症的合适模型系统。

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