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首页> 外文期刊>Probiotics and Antimicrobial Proteins >Oral Vaccination with Hepatitis E Virus Capsid Protein and Immunobiotic Bacterium-Like Particles Induce Intestinal and Systemic Immunity in Mice
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Oral Vaccination with Hepatitis E Virus Capsid Protein and Immunobiotic Bacterium-Like Particles Induce Intestinal and Systemic Immunity in Mice

机译:用乙型肝炎病毒衣壳囊蛋白和免疫杀菌菌状颗粒的口腔疫苗接种诱导小鼠肠道和全身免疫力

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摘要

The hepatitis E virus (HEV) genotype 3 (GT3) is an emergent pathogen in industrialized countries. It is transmitted zoonotically and may lead to chronic hepatitis in immunocompromised individuals. We evaluated if the major antigen of HEV, the capsid protein, can be used in combination with immunobiotic bacterium-like particles (IBLP) for oral vaccination in a mouse model. We have cloned and expressed the RGS-His(5)-tagged HEV GT3 capsid protein (ORF2) in E. coli and purified it by NiNTA. IBLP were obtained from two immunobiotic Lactobacillus rhamnosus strains acid- and heat-treated. ORF2 and the IBLP were orally administered to Balb/c mice. After three oral immunizations (14-day intervals), blood, intestinal fluid, Peyer ' s patches, and spleen samples were drawn. IgA- and IgG-specific antibodies were determined by ELISA. Mononuclear cell populations from Peyer's patches and spleen were analyzed by flow cytometry, and the cytokine profiles were determined by ELISA to study cellular immunity. Orally administered recombinant ORF2 and IBLP from two L. rhamnosus strains (CRL1505 and IBL027) induced both antigen-specific humoral and cellular immune responses in mice. IBLP027 was more effective in inducing specific secretory IgA in the gut. IFN-gamma, TNF-alpha, and IL-4 were produced by Peyer's plaques lymphocytes stimulated with ORF2 ex vivo suggesting a mixed Th1/Th2-type adaptive immune response in immunized mice. Oral vaccines are not invasive, do not need to be administered by specialized personal, and elicit both systemic and local immune responses at the port of entry. Here, we present an experimental oral vaccine for HEV GT3, which could be further developed for human and/or veterinary use.
机译:乙型肝炎病毒(HEV)基因型3(GT3)是工业化国家的出新的病原体。它被繁殖,可能导致免疫普及的个体中的慢性肝炎。我们评估了HEV,衣壳蛋白的主要抗原,可与免疫杀菌颗粒(IBLP)组合使用,用于在小鼠模型中口服疫苗接种。我们已经克隆并表达了RGS-His(5) - 他(5)的HEV GT3 Capsid蛋白(ORF2)在大肠杆菌中并通过Ninta纯化。 IBLP是从两种免疫乳杆菌菌株酸和热处理的两种免疫酸乳杆菌获得的。 ORF2和IBLP对BALB / C小鼠进行口服。在三次口服免疫(14天间隔)后,拉出血液,肠道,Peyer的贴剂和脾样品。通过ELISA测定IgA-和IgG特异性抗体。通过流式细胞术分析来自Peyer的贴剂和脾脏的单核细胞群,通过ELISA测定细胞因子型材以研究细胞免疫。来自两种L. rhamosus菌株(CRL1505和IBL027)的口服给药的重组ORF2和IBLP诱导小鼠抗原特异性体液和细胞免疫应答。 IBLP027更有效地在肠道中诱导特定的分泌IGA。 IFN-Gamma,TNF-α和IL-4由Peyer的斑块淋巴细胞产生,所述肌肉淋巴细胞刺激,所述ORF2离体刺激,表明免疫小鼠中的混合Th1 / Th2型自适应免疫应答。口腔疫苗没有侵入性,不需要通过专业的个人进行管理,并在入境港口引出全身和局部免疫应答。在这里,我们提出了一种用于HEV GT3的实验性口腔疫苗,其可以进一步开发用于人和/或兽医使用。

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  • 作者单位

    UNT Inst Super Invest Biol INSIBIO CONICET Av Kirchner 2100 RA-4000 San Miguel De Tucuman Tucuman Argentina;

    UNT Inst Super Invest Biol INSIBIO CONICET Av Kirchner 2100 RA-4000 San Miguel De Tucuman Tucuman Argentina;

    Univ Nacl Tucuman Fac Med Lab Ciencias Basicas OR Genet San Miguel De Tucuman Argentina;

    UNT Inst Super Invest Biol INSIBIO CONICET Av Kirchner 2100 RA-4000 San Miguel De Tucuman Tucuman Argentina;

    Consejo Nacl Invest Cient &

    Tecn CERELA Lab Inmunobioteenol Chacabuco 145 RA-4000 San Miguel De Tucuman Tucuman Argentina;

    Consejo Nacl Invest Cient &

    Tecn CERELA Lab Inmunobioteenol Chacabuco 145 RA-4000 San Miguel De Tucuman Tucuman Argentina;

    Bavarian Hlth &

    Food Safety Author LGL Oberschleissheim Germany;

    Consejo Nacl Invest Cient &

    Tecn CERELA Lab Inmunobioteenol Chacabuco 145 RA-4000 San Miguel De Tucuman Tucuman Argentina;

    UNT Inst Super Invest Biol INSIBIO CONICET Av Kirchner 2100 RA-4000 San Miguel De Tucuman Tucuman Argentina;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 微生物学;
  • 关键词

    Oral immunization; Lactobacillus rhamnosus; Hepatitis E virus; Bacterium-like particles; Recombinant ORF2;

    机译:口服免疫;乳酸杆菌;乙型肝炎病毒;脱脂颗粒;重组orf2;

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