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首页> 外文期刊>Acta Virologica: International Journal >Expression of duck hepatitis A virus type 1 VP3 protein mediated by avian adeno-associated virus and its immunogenicity in ducklings
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Expression of duck hepatitis A virus type 1 VP3 protein mediated by avian adeno-associated virus and its immunogenicity in ducklings

机译:鸭甲型肝炎病毒表达1型VP3蛋白介导的禽腺相关病毒及其在鸭鱼中的免疫原性

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摘要

The avian adeno-associated virus (AAAV) is a replication-defective nonpathogenic virus that has been proved to be useful as a viral vector in gene delivery. In this study, the feasibility of AAAV for transgenic expression of duck hepatitis A virus (DHAV) VP3 structural protein and its ability to induce protective immunity in ducklings was assessed. The recombinant AAAV (rAAAV-VP3) expressing the VP3 protein was prepared by co-infection of Sf9 cells with recombinant baculovirus (rBac-VP3) containing VP3 gene flanked by inverted terminal repeats (ITRs) of AAAV and the other two recombinant baculovirus expressing AAAV functional and structural genes, respectively. The generation of rAAAV-VP3 was demonstrated by electron microscopy, immunofluorescence assay, and western blot analysis. One day old ducklings were inoculated with rAAAV-VP3 or commercial attenuated vaccine and then challenged with DHAV-1 strain SH two weeks post vaccination. Anti-DHAV-1 antibodies were detected in all vaccinated groups by ELISA, and the titers between the rAAAV-VP3 group and the attenuated vaccine group were not statistically significant. Real time RT-PCR analysis showed that the virus copy numbers in the livers of the PBS control group were significantly higher than that of the rAAAV-VP3 and attenuated vaccine groups. In conclusion, we demonstrated that the VP3 expression mediated by rAAAV in ducklings could induce protective immunity against DHAV challenge, and this could be a candidate vaccine for the control of duck viral hepatitis.
机译:禽腺相关病毒(AAAV)是一种复制缺陷的非遗传病毒,已被证明是可用作基因递送中的病毒载体。在这项研究中,评估AAAAV用于鸭甲型肝炎的转基因表达的可行性(DHAV)VP3结构蛋白及其在鸭鱼中诱导保护性免疫的能力。表达VP3蛋白的重组AAAV(RAAAV-VP3)通过与含有VP3基因的重组杆状病毒(RBAC-VP3)的SF9细胞共感染含有VP3基因的RB3基因的逆转末端重复(ITRS)和表达AAAV的其他两种重组杆状病毒功能性和结构基因分别。通过电子显微镜,免疫荧光测定和蛋白质印迹分析证明了RaAAV-VP3的产生。用RAAAV-VP3或商业减毒疫苗接种一天的鸭子,然后用DHAV-1菌株SH接种后两周攻击。通过ELISA在所有接种疫苗中检测到抗DHAV-1抗体,并且RAAAV-VP3组和减毒疫苗基团之间的滴度在统计学上没有统计学意义。实时RT-PCR分析表明,PBS对照组肝脏中的病毒拷贝数显着高于RAAAV-VP3和减毒疫苗基团的病毒拷贝数。总之,我们证明,鸭草中rav介导的VP3表达可能会对Dhav挑战产生保护性免疫力,这可能是用于控制鸭病毒性肝炎的候选疫苗。

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  • 作者单位

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

    Jiangsu Agrianim Husb Vocat Coll Jiangsu Key Lab High Tech Res &

    Dev Vet Biopharma 8 East Phoenix;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医学微生物学(病原细菌学、病原微生物学);
  • 关键词

    avian adeno-associated virus; duck hepatitis A virus; VP3 gene; immunogenicity;

    机译:禽腺相关病毒;鸭甲型肝炎病毒;VP3基因;免疫原性;

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