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用表达H3N2猪流感病毒血凝素和核蛋白的人腺病毒5重组病毒对断奶仔猪进行免疫保护。

Protection of weaned pigs by vaccination with human adenovirus 5 recombinant viruses expressing the hemagglutinin and the nucleoprotein of H3N2 swine influenza virus.

作者信息

Wesley Ronald D, Tang Min, Lager Kelly M

机构信息

Virus and Prion Diseases of Livestock Research Unit, National Animal Disease Center, USDA, Agricultural Research Service, P.O. Box 70, Ames, IA, 50010, USA.

出版信息

Vaccine. 2004 Sep 3;22(25-26):3427-34. doi: 10.1016/j.vaccine.2004.02.040.

Abstract

Swine influenza virus (SIV), subtype H3N2, is a recent reassortant virus that emerged in 1998 in North American swine causing severe respiratory and reproductive disease. In this study, two replication-defective adenovirus recombinants were developed as potential vaccines against H3N2 influenza viruses. Three groups of 3-week-old pigs (10 pigs per group) were vaccinated intramuscularly (IM) with the recombinants; one group was vaccinated with the recombinant adenovirus expressing the influenza virus H3 hemagglutinin (HA) protein, one group was vaccinated with the recombinant adenovirus expressing the nucleoprotein (NP), and one group was vaccinated with both recombinants in a mixture. Two additional control groups (10 pigs per group) were included in the animal trial. One control group was challenged with a virulent H3N2 field strain and one control group remained unchallenged. The results showed that pigs in the groups given the recombinant adenovirus expressing HA alone and HA plus NP developed high levels of virus-specific hemagglutination-inhibition (HI) antibody by 4 weeks post vaccination. Pigs in the group vaccinated with both recombinant viruses in a mixture were completely protected. Complete protection was shown by the lack of nasal shedding of virus following challenge and by the lack of lung lesions at 1 week following the challenge infection. Thus, replication-incompetent adenovirus vaccines given simultaneously to pigs are efficacious for SIV and have the additional advantage over commercial vaccines that suckling piglets have no pre-existing maternally-derived antibody to block early life vaccination.

摘要

H3N2亚型猪流感病毒(SIV)是一种最近出现的重配病毒,于1998年在北美猪群中出现,可引起严重的呼吸道和生殖系统疾病。在本研究中,开发了两种复制缺陷型腺病毒重组体作为针对H3N2流感病毒的潜在疫苗。将三组3周龄仔猪(每组10头)肌肉注射(IM)重组体进行免疫;一组用表达流感病毒H3血凝素(HA)蛋白的重组腺病毒进行免疫,一组用表达核蛋白(NP)的重组腺病毒进行免疫,一组用两种重组体的混合物进行免疫。动物试验中还包括另外两个对照组(每组10头猪)。一个对照组用强毒H3N2田间毒株进行攻毒,一个对照组不进行攻毒。结果显示,单独给予表达HA的重组腺病毒组以及给予HA加NP组的仔猪在接种疫苗后4周产生了高水平的病毒特异性血凝抑制(HI)抗体。用两种重组病毒混合物进行免疫的组的仔猪得到了完全保护。攻毒后鼻腔无病毒排出以及攻毒感染后1周肺部无病变表明获得了完全保护。因此,同时给予仔猪无复制能力的腺病毒疫苗对SIV有效,并且与商业疫苗相比具有额外优势,即哺乳仔猪不存在预先存在的母源抗体来阻断早期免疫接种。

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