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新城疫病毒重组杆状病毒疫苗的构建及其免疫原性评估。

Construction of recombinant baculovirus vaccines for Newcastle disease virus and an assessment of their immunogenicity.

作者信息

Ge Jingping, Liu Ying, Jin Liying, Gao Dongni, Bai Chengle, Ping Wenxiang

机构信息

Key Laboratory of Microbiology, College of Life Science, Heilongjiang University, Harbin 150080, China.

Key Laboratory of Microbiology, College of Life Science, Heilongjiang University, Harbin 150080, China.

出版信息

J Biotechnol. 2016 Aug 10;231:201-211. doi: 10.1016/j.jbiotec.2016.03.037. Epub 2016 Mar 23.

DOI:10.1016/j.jbiotec.2016.03.037
PMID:27015979
Abstract

Newcastle disease (ND) is a lethal avian infectious disease caused by Newcastle disease virus (NDV) which poses a substantial threat to China's poultry industry. Conventional live vaccines against NDV are available, but they can revert to virulent strains and do not protect against mutant strains of the virus. Therefore, there is a critical unmet need for a novel vaccine that is safe, efficacious, and cost effective. Here, we designed novel recombinant baculovirus vaccines expressing the NDV F or HN genes. To optimize antigen expression, we tested the incorporation of multiple regulatory elements including: (1) truncated vesicular stomatitis virus G protein (VSV-GED), (2) woodchuck hepatitis virus post-transcriptional regulatory element (WPRE), (3) inverted terminal repeats (ITRs) of adeno-associated virus (AAV Serotype II), and (4) the cytomegalovirus (CMV) promoter. To test the in vivo efficacy of the viruses, we vaccinated chickens with each construct and characterized the cellular and humoral immune response to challenge with virulent NDV (F48E9). All of the vaccine constructs provided some level of protection (62.5-100% protection). The F-series of vaccines provided a greater degree of protection (87.5-100%) than the HN-series (62.5-87.5%). While all of the vaccines elicited a robust cellular and humoral response subtle differences in efficacy were observed. The combination of the WPRE and VSV-GED regulatory elements enhanced the immune response and increased antigen expression. The ITRs effectively increased the length of time IFN-γ, IL-2, and IL-4 were expressed in the plasma. The F-series elicited higher titers of neutralizing antibody and NDV-specific IgG. The baculovirus system is a promising platform for NDV vaccine development that combines the immunostimulatory benefits of a recombinant virus vector with the non-replicating benefits of a DNA vaccine.

摘要

新城疫(ND)是一种由新城疫病毒(NDV)引起的致死性禽类传染病,对中国的家禽业构成了重大威胁。针对NDV的传统活疫苗是可用的,但它们可能会回复为强毒株,并且不能抵御该病毒的突变株。因此,迫切需要一种安全、有效且经济高效的新型疫苗。在此,我们设计了表达NDV F或HN基因的新型重组杆状病毒疫苗。为了优化抗原表达,我们测试了多种调控元件的整合,包括:(1)截短的水疱性口炎病毒G蛋白(VSV-GED)、(2)土拨鼠肝炎病毒转录后调控元件(WPRE)、(3)腺相关病毒(AAV血清型II)的反向末端重复序列(ITRs)以及(4)巨细胞病毒(CMV)启动子。为了测试这些病毒在体内的功效,我们用每种构建体对鸡进行免疫接种,并对针对强毒NDV(F48E9)攻击的细胞免疫和体液免疫反应进行了表征。所有疫苗构建体都提供了一定程度的保护(62.5 - 100%的保护率)。F系列疫苗提供的保护程度(87.5 - 100%)高于HN系列(62.5 - 87.5%)。虽然所有疫苗都引发了强烈的细胞免疫和体液免疫反应,但在功效上观察到了细微差异。WPRE和VSV-GED调控元件的组合增强了免疫反应并增加了抗原表达。ITRs有效地延长了血浆中IFN-γ、IL-2和IL-4的表达时间。F系列引发了更高滴度的中和抗体和NDV特异性IgG。杆状病毒系统是NDV疫苗开发的一个有前景的平台,它将重组病毒载体的免疫刺激益处与DNA疫苗的非复制益处结合在一起。

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