首页> 外文期刊>Veterinary Immunology and Immunopathology >Single dose adenovirus vectored vaccine induces a potent and long-lasting immune response against rabbit hemorrhagic disease virus after parenteral or mucosal administration
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Single dose adenovirus vectored vaccine induces a potent and long-lasting immune response against rabbit hemorrhagic disease virus after parenteral or mucosal administration

机译:肠胃外或粘膜给药后,单剂量腺病毒载体疫苗可诱导针对兔出血性疾病病毒的强效和持久免疫应答

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Rabbit hemorrhagic disease virus (RHDV) is the etiological agent of a lethal and contagious disease of rabbits that remains as a serious problem worldwide. As this virus does not replicate in cell culture systems, the capsid protein gene has been expressed in heterologous hosts or inserted in replication-competent viruses in order to obtain non-conventional RHDV vaccines. However, due to technological or safety issues, current RHDV vaccines are still prepared from organs of infected rabbits. In this work, two human type 5 derived replication-defective adenoviruses encoding the rabbit hemorrhagic disease virus VP60 capsid protein were constructed. The recombinant protein was expressed as a multimer in mouse and rabbit cell lines at levels that ranged from approximately 120 to 160 mg/L of culture. Mice intravenously or subcutaneously inoculated with a single 10(8) gene transfer units (GTU) dose of the AdVP60 vector (designed for VP60 intracellular expression) seroconverted at days 7 and 14 post-immunization, respectively. This vector generated a stronger response than that obtained with a second vector (AdVP60sec) designed for VP60 secretion. Rabbits were then immunized by parenteral or mucosal routes with a single 10(9) GTU dose of the AdVP60 and the antibody response was evaluated using a competition ELISA specific for RH DV or RHDVa. Protective hemagglutination inhibition (HI) titers were also promptly detected and IgG antibodies corresponding with inhibition percentages over 85% persisted up to one year in all rabbits, independently of the immunization route employed. These levels were similar to those elicited with inactivated RHDV or with VP60 obtained from yeast or insect cells. IgA specific antibodies were only found in saliva of rabbits immunized by intranasal instillation. The feasibility of VP60 production and vaccination of rabbits with replication-defective adenoviral vectors was demonstrated
机译:兔出血性疾病病毒(RHDV)是兔致命和传染性疾病的病原体,至今仍是世界范围内的严重问题。由于该病毒不能在细胞培养系统中复制,因此衣壳蛋白基因已在异源宿主中表达或插入了具有复制能力的病毒中,以获得非常规的RHDV疫苗。但是,由于技术或安全问题,当前的RHDV疫苗仍是从受感染兔子的器官中制备的。在这项工作中,构建了两种人类5型衍生的复制缺陷型腺病毒,它们编码兔出血性疾病病毒VP60衣壳蛋白。重组蛋白在小鼠和兔细胞系中表达为多聚体,水平范围约为120到160 mg / L。分别在免疫后第7天和第14天分别将单次10(8)基因转移单位(GTU)剂量的AdVP60载体(设计用于VP60细胞内表达)静脉内或皮下接种小鼠。该载体产生的应答比使用专为VP60分泌设计的第二个载体(AdVP60sec)获得的应答强。然后,通过肠胃外或粘膜途径用10(9)GTU单剂量的AdVP60免疫兔子,并使用对RH DV或RHDVa特异的竞争ELISA评估抗体反应。还迅速检测到了保护性血凝抑制(HI)滴度,并且在所有兔中,与抑制率超过85%相对应的IgG抗体都能持续长达一年,而与所采用的免疫途径无关。这些水平类似于用灭活的RHDV或从酵母或昆虫细胞获得的VP60引起的水平。 IgA特异性抗体仅在通过鼻内滴注免疫的兔子的唾液中发现。证明了用复制缺陷型腺病毒载体对兔进行VP60生产和疫苗接种的可行性

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