H1亚型流感病毒通用疫苗的构建及其对小鼠免疫保护效力研究

畜牧兽医学报

H1亚型流感病毒通用疫苗的构建及其对小鼠免疫保护效力研究

杨馥如，于海，王斌，黄梦，马继红，温峰，周艳君，童光志^*

(中国农业科学院上海兽医研究所，上海 200241)

收稿日期:2012-07-25 出版日期:2013-02-23 发布日期:2013-02-23
通讯作者: 童光志，男，湖北蕲春人，研究员，博士，E-mail: gztong@shvri.ac.cn
作者简介:杨馥如（1986-），女，四川广安人，研究实习员，硕士生，主要从事兽医传染病及其病原和分子免疫学研究，E-mail：yangfuru819@163.com
基金资助:
国家科技支撑计划重点项目 (2010BAD04B03)；国家国际科技合作项目 (2010DFB33920)；中央级公益性科研院所基本科研业务费项目（2010JB01）；上海市科委基础研究重点项目（10JC1417300）

Construction of a Universal Vaccine against H1 Subtype Influenza Viruses and Its Protective Efficacy in Mice

YANG Fu-ru, YU Hai, WANG Bin, HUANG Meng, MA Ji-hong, WEN Feng, ZHOU Yan-jun, TONG Guang-zhi^*

(Shanghai Veterinary Research Institute, Chinese Academy of Agricultural Sciences, Shanghai 200241, China)

Received:2012-07-25 Online:2013-02-23 Published:2013-02-23

摘要/Abstract

摘要：

本研究旨在为研制一种安全、有效并具有广泛保护作用的流感病毒通用疫苗进行初步的探索。从GenBank上获得所有H1亚型经典猪源流感病毒和甲型流感病毒的HA基因序列，通过系统进化分析获得其共有序列，并对共有序列进行密码子优化（Optimized consensus, optiCS），同时将H1亚型的A/Swine/Guangdong/1/01(H1N1)和重组甲型流感病毒rPan09(H1N1，其HA和NA来自A/Swine/California/04/09，其余6个片段来自PR8的重组病毒)的HA基因分别进行密码子优化（opti-G11,opti-r09），并将这3种片段与真核表达载体pCAGGS连接获得重组质粒pCA-opti-CS、pCA-opti-G11和pCA-opti-r09。将重组质粒瞬时转染293T细胞，检测HA基因在哺乳动物细胞中的表达情况。免疫6~8周雌性BALB/c小鼠，免疫3次，每次间隔3周，同时设立空载体pCAGGS对照。三免2周后从每个质粒免疫组中选取一半小鼠每只以50 μL 10^3.87EID₅₀的剂量接种A/Swine/Guangdong/1/01(H1N1)病毒，另一半小鼠每只以50 μL 10^7.45EID₅₀的剂量接种rPan09病毒。采集血清，对HA抗体水平、HI滴度、细胞因子产生情况、肺组织病毒含量进行检测，并对肺组织病理学变化进行观察。结果显示：重组质粒中HA基因均能够在哺乳动物细胞中有效的表达。pCA-opti-CS免疫后能够诱导小鼠产生较高的HA抗体水平，较高的HI滴度，并且能够诱导机体产生较高水平的IL-4和IFN-γ。肺组织病毒含量测定以及组织病理学观察结果显示：HA共有序列密码子优化的DNA疫苗pCA-opti-CS免疫后能够有效限制病毒A/Swine/Guangdong/1/01(H1N1) 和rPan09HA在肺脏中的复制，减轻肺脏病理变化。结果提示：HA共有序列密码子优化的DNA疫苗pCA-opti-CS能够诱导小鼠产生较高水平的体液免疫和细胞免疫应答，并具有较好的交叉保护效力，能够保护小鼠抵抗异源流感病毒的攻击。本研究为流感通用疫苗的研究提供了有益的参考。

Abstract:

The aim of this study was to investigate a safe and effective universal vaccine. A consensus HA gene sequence was found by phylogenetic analysis all of the HA gene sequences of H1 subtype classical swine influenza virus and influenza A virus from GenBank and optimized according to the swine bias codon usages（optimized consensus, opti-CS）, we also selected another two HA genes and optimized (one is from A/Swine/Guangdong/1/01 strain and the other one is from rPan09 strain),then the three opti-HAs were inserted into pCAGGS vector, and constructed three recombinant plasmids named pCA-opti-CS, pCA-opti-G11 and pCA-opti-r09, respectively. The HA protein transiently expressed in 293T cell was detected in indirect immunofluorescence. Groups of six to eight week-old BALB/c were intramuscular inoculated singly with pCA-opti-CS, pCA-opti-G11, pCA-opti-r09 and PCAGGS vector, respectively. A total of immunity was three times interval of three weeks with the same dosage. Mice of each Group were divided into two parts after two weeks of the third immunity, then challenged with 10^3.87EID₅₀ of A/Swine/Guangdong/1/01(H1N1) and 10^7.45EID₅₀ of rPan09, respectively. Sera were collected, antibodies to HA and HI antibodies, level of IL-4 and IFN-γ were detected. The lungs were used for virus titer detection and histopathological observation. The result showed that HA can be expressed in 293T cell, plasmid pCA-opti-CS can induce high level of HA antibodies, high HI titer and can induce high level of IL-4 and IFN-γ. The result of determination of virus content in lungs and histopathological observation were showed that pCA-opti-CS DNA vaccine could effectively limited viral replication and attenuated histopathological damage in mice lungs. Based on our research, we conclude that recombinant plasmid pCA-opti-CS can induced high level of humoral and cellular immune response and own a good heterologous protecting capacity. Our study had made beneficial exploration in universal vaccine against influenza virus.

中图分类号:

S852.659.5

杨馥如，于海，王斌，黄梦，马继红，温峰，周艳君，童光志. H1亚型流感病毒通用疫苗的构建及其对小鼠免疫保护效力研究[J]. 畜牧兽医学报, doi: .

YANG Fu-ru, YU Hai, WANG Bin, HUANG Meng, MA Ji-hong, WEN Feng, ZHOU Yan-jun, TONG Guang-zhi. Construction of a Universal Vaccine against H1 Subtype Influenza Viruses and Its Protective Efficacy in Mice[J]. ACTA VETERINARIA ET ZOOTECHNICA SINICA, doi: .

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