首页> 美国卫生研究院文献>European Journal of Histochemistry : EJH >Histomorphometric characteristics of immune cells in small intestine of pigs perorally immunized with vaccine candidate F18ac+ nonenterotoxigenic E. coli strain
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Histomorphometric characteristics of immune cells in small intestine of pigs perorally immunized with vaccine candidate F18ac+ nonenterotoxigenic E. coli strain

机译:候选疫苗F18ac +非肠毒素的大肠杆菌经口免疫的猪小肠免疫细胞的组织形态学特征

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摘要

Colidiarrhea and colienterotoxemia caused by F4+ and/or F18+ enterotoxigenic E. coli (ETEC) strains are the most prevalent infections of suckling and weaned pigs. Here we tested the immunogenicity and protective effectiveness of attenuated F18ac+ non-ETEC vaccine candidate strain against challenge infection with F4ac+ ETEC strain by quantitative phenotypic analysis of small intestinal leukocyte subsets in weaned pigs.We also evaluated levamisole as an immune response modifier (IRM) and its adjuvanticity when given in the combination with the experimental vaccine. The pigs were parenterally immunized with either levamisole (at days -2, -1 and 0) or with levamisole and perorally given F18ac+ non-ETEC strain (at day 0), and challenged with F4ac+ ETEC strain 7 days later.At day 13 the pigs were euthanatized and sampled for immunohistological/histomorphometrical analyses. Lymphoid CD3+, CD45RA+, CD45RC+, CD21+, IgA+ and myeloid SWC3+ cell subsets were identified in jejunal and ileal epithelium, lamina propria and Peyer’s patches using the avidin-biotin complex method, and their numbers were determined by computer-assisted histomorphometry. Quantitative immunophenotypic analyses showed that levamisole treated pigs had highly increased numbers of jejunal CD3+, CD45RC+ and SWC3+ cells (p<0.05) as compared to those recorded in nontreated control pigs.In the ileum of these pigs we have recorded that only CD21+ cells were significantly increased (p<0.01). The pigs that were treated with levamisole adjuvanted experimental vaccine had significantly increased numbers of all tested cell subsets in both segments of the small intestine. It was concluded that levamisole adjuvanted F18ac+ non-ETEC vaccine was a requirement for the elicitation of protective gut immunity in this model; nonspecific immunization with levamisole was less effective, but confirmed its potential as an IRM.
机译:F4 + 和/或F18 + 产肠毒素的大肠杆菌(ETEC)菌株引起的腹泻和大肠杆菌肠毒素是乳猪和断奶猪中最常见的感染。在这里,我们通过对小肠白细胞亚群的定量表型分析,测试了减毒的F18ac + 非ETEC疫苗候选株对F4ac + ETEC株挑战感染的免疫原性和保护效果。断奶仔猪。我们还评估了左旋咪唑作为免疫应答调节剂(IRM)及其与实验疫苗联合使用时的佐剂性。用左旋咪唑(在第-2,-1和0天)或左旋咪唑对猪进行肠胃外免疫,并口服给予F18ac + 非ETEC菌株(在第0天),然后用F4ac + ETEC株7天后。在第13天,对猪实施安乐死并取样进行免疫组织学/组织形态分析。淋巴CD3 + ,CD45RA + ,CD45RC + ,CD21 + ,IgA + 使用抗生物素蛋白-生物素复合物法在空肠和回肠上皮,固有层和Peyer斑片中鉴定了髓样SWC3 + 细胞亚群,并通过计算机辅助组织形态测定法确定了它们的数目。定量免疫表型分析显示,用左旋咪唑治疗的猪空肠CD3 + ,CD45RC + 和SWC3 + 细胞数量显着增加(p <0.05),与未治疗的对照猪相比,我们观察到在这些猪的回肠中,只有CD21 + 细胞显着增加(p <0.01)。用左旋咪唑佐剂实验疫苗治疗的猪在小肠的两个部分中所有受试细胞亚群的数量均显着增加。结论是左旋咪唑佐剂的F18ac + 非ETEC疫苗是引发保护性肠道免疫的必需条件。左旋咪唑的非特异性免疫效果较差,但证实了其作为IRM的潜力。

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