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首页> 外文期刊>Applied Microbiology and Biotechnology >High-level mucosal and systemic immune responses induced by oral administration with Lactobacillus-expressed porcine epidemic diarrhea virus (PEDV) S1 region combined with Lactobacillus-expressed N protein
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High-level mucosal and systemic immune responses induced by oral administration with Lactobacillus-expressed porcine epidemic diarrhea virus (PEDV) S1 region combined with Lactobacillus-expressed N protein

机译:口服表达乳杆菌的猪流行性腹泻病毒(PEDV)S1区和表达乳杆菌的N蛋白联合诱导的高水平粘膜和全身免疫反应

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摘要

To develop effective mucosal vaccine formulation against porcine epidemic diarrhea virus (PEDV) infection, the DNA fragments encoding spike protein immunodominant region S1 and nucleocapsid N of PEDV were inserted into pPG1 (surface-displayed) or pPG2 (secretory) plasmids followed by electrotransformation into Lactobacillus casei (Lc) to yield four recombinant strains: PG1-S1, PG2-S1, PG1-N, and PG2-N. After intragastric administration, it was observed that live Lc-expressing S1 protein combined with Lc-expressing N protein could elicit much more potent mucosal and systemic immune responses than the former alone (P 0.05). Furthermore, the surface-displayed mixture (PG1-S1+ PG1-N) revealed stronger immunogenicity than the secretory mixture (PG2-S1+ PG2-N) as well as PEDV-neutralizing potency in vitro (P < 0.001). On 49th day after the last immunization, splenocytes were prepared from mice immunized with surface-displayed mixture, secretory mixture and negative control to be stimulated by purified N and S protein, respectively. The results of ELISA analysis showed that N protein was capable of inducing a higher level of IL-4 (P < 0.001) and IFN-γ (P < 0.001) than S1 protein in the immunized mice. Taken together, Lc-expressed N protein as molecular adjuvant or immunoenhancer was able to effectively facilitate the induction of mucosal and systemic immune responses by Lc-expressing S1 region.
机译:为了开发针对猪流行性腹泻病毒(PEDV)感染的有效粘膜疫苗制剂,将编码PEDV的刺突蛋白免疫优势区S1和核衣壳N的DNA片段插入pPG1(表面展示)或pPG2(分泌型)质粒,然后电转化为乳杆菌casei(Lc)产生四个重组菌株:PG1-S1,PG2-S1,PG1-N和PG2-N。胃内给药后,观察到活的表达Lc的S1蛋白与表达Lc的N蛋白结合可以比单独的前者引起更强的粘膜和全身免疫反应(P 0.05)。此外,表面展示的混合物(PG1-S1 + PG1-N)显示出比分泌性混合物(PG2-S1 + PG2-N)更强的免疫原性,并且在体外具有PEDV中和能力(P <0.001)。在最后一次免疫后第49天,从分别用纯化的N和S蛋白刺激的表面展示混合物,分泌混合物和阴性对照免疫的小鼠中制备脾细胞。 ELISA分析的结果表明,在免疫小鼠中,N蛋白能够诱导更高水平的IL-4(P <0.001)和IFN-γ(P <0.001)。总之,表达Lc的N蛋白作为分子佐剂或免疫增强剂能够有效地促进表达Lc的S1区诱导粘膜和全身免疫反应。

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