经鼻内接种截短型NS1修饰的流感病毒活疫苗在猪身上的效力
Efficacy of intranasal administration of a truncated NS1 modified live influenza virus vaccine in swine.
作者信息
Vincent Amy L, Ma Wenjun, Lager Kelly M, Janke Bruce H, Webby Richard J, García-Sastre Adolfo, Richt Jürgen A
机构信息
Virus and Prion Diseases of Livestock Research Unit, National Animal Disease Center, USDA, Agricultural Research Service, Ames, IA 50010, United States.
出版信息
Vaccine. 2007 Nov 19;25(47):7999-8009. doi: 10.1016/j.vaccine.2007.09.019. Epub 2007 Sep 29.
In the U.S., despite available swine influenza virus (SIV) vaccines, multiple influenza subtypes as well as antigenic and genetic variants within subtypes continue to circulate in the swine population. One of the challenges to control and eliminate SIV is that the currently used inactivated influenza virus vaccines do not provide adequate cross-protection against multiple antigenic variants of SIV in the field. We previously generated a recombinant H3N2 swine influenza virus (SIV) based on the influenza A/SW/TX/4199-2/98 virus (TX98) containing an NS1 gene expressing a truncated NS1 protein of 126 amino acids, TX98-NS1Delta126 virus. This recombinant strain was demonstrated to be highly attenuated in swine and showed potential for use as a modified live-virus vaccine (MLV) after intratracheal application in pigs. However, this route of inoculation is not practical for vaccination in the field. In the present study, we first compared intramuscular and intranasal routes of application of the MLV, and found that the intranasal route was superior in priming the local (mucosal) immune response. Pigs were then vaccinated via the intranasal route and challenged with wild type homologous TX98 H3N2 virus, with a genetic and antigenic variant H3N2 SIV (influenza A/SW/CO/23619/99 virus, CO99) and a heterosubtypic H1N1 SIV (influenza A/SW/IA/00239/2004 virus, IA04). The intranasally vaccinated pigs were completely protected against homologous challenge. In addition, MLV vaccination provided nearly complete protection against the antigenic H3N2 variant CO99 virus. When challenged with the H1N1 IA04 virus, MLV vaccinated animals displayed reduced fever and virus titers despite minimal reduction in lung lesions. In vaccinated pigs, there was no serologic cross-reactivity by HI assays with the heterologous or heterosubtypic viruses. However, there appeared to be substantial cross-reactivity in antibodies at the mucosal level with the CO99 virus in MLV vaccinated pigs.
在美国,尽管有猪流感病毒(SIV)疫苗可用,但多种流感亚型以及亚型内的抗原和基因变体仍在猪群中传播。控制和消除SIV的挑战之一是,目前使用的灭活流感病毒疫苗不能对田间SIV的多种抗原变体提供足够的交叉保护。我们之前基于甲型流感病毒A/SW/TX/4199-2/98病毒(TX98)构建了一种重组H3N2猪流感病毒(SIV),该病毒含有一个表达126个氨基酸的截短NS1蛋白的NS1基因,即TX98-NS1Delta126病毒。该重组毒株在猪体内表现出高度减毒,并且在猪气管内接种后显示出作为改良活病毒疫苗(MLV)使用的潜力。然而,这种接种途径在田间疫苗接种中并不实用。在本研究中,我们首先比较了MLV的肌肉注射和鼻内接种途径,发现鼻内接种途径在启动局部(粘膜)免疫反应方面更具优势。然后通过鼻内途径对猪进行疫苗接种,并用野生型同源TX98 H3N2病毒、一种基因和抗原变体H3N2 SIV(甲型流感病毒A/SW/CO/23619/99病毒,CO99)和一种异源亚型H1N1 SIV(甲型流感病毒A/SW/IA/00239/2004病毒,IA04)进行攻毒。经鼻内接种疫苗的猪对同源攻毒具有完全保护作用。此外,MLV疫苗接种对抗原性H3N2变体CO99病毒提供了近乎完全的保护。当用H1N1 IA04病毒攻毒时,尽管肺部病变减少最小,但MLV疫苗接种的动物发热和病毒滴度降低。在接种疫苗的猪中,血凝抑制试验未显示与异源或异源亚型病毒有血清学交叉反应。然而,在MLV疫苗接种的猪中,粘膜水平的抗体似乎与CO99病毒有大量交叉反应。
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