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通过接种表达猪流感病毒血凝素和核蛋白的人腺病毒5重组病毒克服母源抗体干扰。

Overcoming maternal antibody interference by vaccination with human adenovirus 5 recombinant viruses expressing the hemagglutinin and the nucleoprotein of swine influenza virus.

作者信息

Wesley Ronald D, Lager Kelly M

机构信息

Virus and Prion Diseases of Livestock Research Unit, National Animal Disease Center, USDA, Agricultural Research Service, Ames, IA 50010, USA.

出版信息

Vet Microbiol. 2006 Nov 26;118(1-2):67-75. doi: 10.1016/j.vetmic.2006.07.014. Epub 2006 Jul 25.

DOI:10.1016/j.vetmic.2006.07.014
PMID:16939702
Abstract

Sows and gilts lack immunity to human adenovirus 5 (Ad-5) vectored vaccines so immunogens of swine pathogens can be expressed with these vaccines in order to immunize suckling piglets that have interfering, maternally derived antibodies. In this study 7-day-old piglets, that had suckled H3N2 infected gilts, were sham-inoculated with a non-expressing Ad-5 vector or given a primary vaccination with replication-defective Ad-5 viruses expressed the H3 hemagglutinin and the nucleoprotein of swine influenza virus (SIV) subtype H3N2. The hemagglutination inhibition (HI) titer of the sham-inoculated group (n = 12) showed continued antibody decay whereas piglets vaccinated with Ad-5 SIV (n = 23) developed an active immune response by the second week post-vaccination. At 4 weeks-of-age when the HI titer of the sham-inoculated group had decayed to 45, the sham-inoculated group and half of the Ad-5 SIV vaccinated pigs were boosted with a commercial inactivated SIV vaccine. The boosted pigs that had been primed in the presence of maternal interfering antibodies had a strong anamnestic response while sham-inoculated pigs did not respond to the commercial vaccine. Two weeks after the booster vaccination the pigs were challenged with a non-homologous H3N2 virulent SIV. The efficacy of the vaccination protocol was demonstrated by abrogation of clinical signs, by clearance of challenge virus from pulmonary lavage fluids, by markedly reduced virus shedding in nasal secretions, and by the absence of moderate or severe SIV-induced lung lesions. These recombinant Ad-5 SIV vaccines are useful for priming the immune system to override the effects of maternally derived antibodies which interfere with conventional SIV vaccines.

摘要

母猪和后备母猪对人腺病毒5(Ad-5)载体疫苗缺乏免疫力,因此猪病原体的免疫原可以用这些疫苗来表达,以便免疫具有干扰性母源抗体的哺乳仔猪。在本研究中,对已哺乳感染H3N2的后备母猪的7日龄仔猪,用无表达的Ad-5载体进行假接种,或用表达猪流感病毒(SIV)H3N2亚型的血凝素和核蛋白的复制缺陷型Ad-5病毒进行初次免疫。假接种组(n = 12)的血凝抑制(HI)效价显示抗体持续衰减,而接种Ad-5 SIV的仔猪(n = 23)在接种后第二周产生了活跃的免疫反应。在4周龄时,假接种组的HI效价降至45,此时对假接种组和一半接种Ad-5 SIV的猪用市售灭活SIV疫苗进行加强免疫。在母源干扰抗体存在的情况下预先免疫的加强免疫猪产生了强烈的回忆反应,而假接种猪对市售疫苗无反应。加强免疫两周后,用非同源的H3N2强毒SIV对猪进行攻毒。通过消除临床症状、从肺灌洗液中清除攻毒病毒、显著减少鼻分泌物中的病毒排出以及不存在中度或重度SIV诱导的肺部病变,证明了该免疫方案的有效性。这些重组Ad-5 SIV疫苗可用于启动免疫系统,以克服母源抗体对传统SIV疫苗的干扰作用。

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