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首页> 外文期刊>Clinical and vaccine immunology: CVI >Virus-like particle vaccine containing hemagglutinin confers protection against 2009 H1N1 pandemic influenza
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Virus-like particle vaccine containing hemagglutinin confers protection against 2009 H1N1 pandemic influenza

机译:病毒样颗粒疫苗包含血凝素赋予预防2009H1N1大流行性流感

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Immunization of the world population before an influenza pandemic such as the 2009 H1N1 virus spreads globally is not possible with current vaccine production platforms. New influenza vaccine technologies, such as virus-like-particles (VLPs), offer a promising alternative. Here, we tested the immunogenicity and protective efficacy of a VLP vaccine containing hemagglutinin (HA) and M1 from the 2009 pandemic H1N1 influenza virus (H1N1pdm) in ferrets and compared intramuscular (i.m.) and intranasal (i.n.) routes of immunization. Vaccination of ferrets with VLPs containing the M1 and HA proteins from A/California/04/2009 (H1N1pdm) induced high antibody titers and conferred significant protection against virus challenge. VLP-vaccinated animals lost less weight, shed less virus in nasal washes, and had markedly lower virus titers in all organs tested than na?ve controls. A single dose of VLPs, either i.m. or i.n., induced higher levels of antibody than did two doses of commercial split vaccine. Ferrets vaccinated with split vaccine were incompletely protected against challenge; these animals had lower virus titers in olfactory bulbs, tonsils, and intestines, but lost weight and shed virus in nasal washes to a similar extent as na?ve controls. Challenge with heterologous A/Brisbane/59/07 (H1N1) virus revealed that the VLPs conferred minimal cross-protection to heterologous infection, as revealed by the lack of reduction in nasal wash and lung virus titers and slightly higher weight loss relative to controls. In summary, these experiments demonstrate the strong immunogenicity and protective efficacy of VLPs compared to the split vaccine and show that i.n. vaccination with VLPs has the potential for highly efficacious vaccination against influenza.
机译:免疫前的世界人口流感大流行,如2009年的H1N1病毒全球传播与当前是不可能的疫苗生产平台。疫苗技术,例如virus-like-particles(种),提供一种很有前途的的选择。和疫苗保护效果的车牌区域含血凝素(HA)和M12009年大流行H1N1流感病毒(H1N1pdm)肌内(坜)和雪貂和比较鼻内(i.n)的免疫途径。疫苗接种一种包含的雪貂M1和HA蛋白从加州/ / 04/2009(H1N1pdm)诱导抗体滴度高,赋予重要的防范病毒挑战。重量,就少了病毒在鼻腔冲洗,在所有器官的病毒滴度明显降低测试比娜?即时消息或i.n,诱导高水平的抗体比两剂商业分裂疫苗防止不完全的挑战;这些动物在嗅觉的病毒滴度较低灯泡、扁桃体和肠道,但失去了重量和病毒在鼻腔冲洗相似na程度?heterologous了布里斯班/ 59 /病毒(H1N1)显示一种授予最小跟踪不同的感染,如揭示了缺乏减少鼻清洗和肺病毒滴度和更高的重量相对于控制损失。实验证明了强大的免疫原性和相比一种保护效果分裂和显示i.n.疫苗接种疫苗一种有可能非常有效接种流感疫苗。

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