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Immunization with 1976 swine H1N1‐ or 2009 pandemic H1N1‐inactivated vaccines protects mice from a lethal 1918 influenza infection

机译:1976年猪H1N1或2009年大流行H1N1灭活疫苗的免疫保护小鼠免受致命的1918年流感病毒感染

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摘要

Please cite this paper as: Easterbrook et al. (2011) Immunization with 1976 swine H1N1‐ or 2009 pandemic H1N1‐inactivated vaccines protects mice from a lethal 1918 influenza infection. Influenza and Other Respiratory Viruses DOI: 10.1111/j.1750‐2659.2010.00191.x. >Background  Zoonotic infections with H1N1 influenza viruses that evolved initially from the 1918 virus (1918) and adapted to swine threatened a pandemic in 1976 (1976 swH1N1) and a novel reassortant H1N1 virus caused a pandemic in 2009–2010 (2009 pH1N1). Epidemiological and laboratory animal studies show that protection from severe 2009 pH1N1 infection is conferred by vaccination or prior infection with 1976 swH1N1 or 1918. >Objectives  Our aim was to demonstrate cross‐protection by immunization with 2009 pH1N1 or 1976 swH1N1 vaccines following a lethal challenge with 1918. Further, the mechanisms of cross‐protective antibody responses were evaluated. >Methods  Mice were immunized with 1976 swH1N1, 2009 pH1N1, 2009 seasonal trivalent, or 1918 vaccines and challenged with 1918. Cross‐reactive antibody responses were assessed and protection monitored by survival, weight loss, and pathology in mice. >Results and Conclusions  Vaccination with the 1976 swH1N1 or 2009 pH1N1 vaccines protected mice from a lethal challenge with 1918, and these mice lost no weight and had significantly reduced viral load and pathology in the lungs. Protection was likely due to cross‐reactive antibodies detected by microneutralization assay. Our data suggest that the general population may be protected from a future 1918‐like pandemic because of prior infection or immunization with 1976 swH1N1 or 2009 pH1N1. Also, influenza protection studies generally focus on cross‐reactive hemagglutination‐inhibiting antibodies; while hemagglutinin is the primary surface antigen, this fails to account for other influenza viral antigens. Neutralizing antibody may be a better correlate of human protection against pathogenic influenza strains and should be considered for vaccine efficacy.
机译:请将此论文引用为:Easterbrook等。 (2011)1976年H1N1或2009年大流行H1N1灭活疫苗的免疫接种可保护小鼠免受致命的1918年流感病毒感染。流感和其他呼吸道病毒DOI:10.1111 / j.1750-2659.2010.00191.x。 >背景 H1N1流感病毒的人畜共患性感染最初是从1918年(1918年)演变而来,并适应了猪的威胁,在1976年爆发了大流行(1976 swH1N1),而新型的重组H1N1病毒在2009-2010年引起了大流行。 (2009 pH1N1)。流行病学和实验室动物研究表明,接种1976年swH1N1或1918年接种过的疫苗或事先感染,可以预防2009年pH1N1严重感染。>目的我们的目的是证明通过用2009 pH1N1或1976 swH1N1免疫进行交叉保护。疫苗在1918年致死性攻击后进行。进一步,评估了交叉保护性抗体应答的机制。 >方法用1976 swH1N1、2009 pH1N1、2009季节性三价或1918疫苗免疫小鼠,并用1918攻击。通过小鼠的存活,减重和病理学评估交叉反应性抗体反应并监测其保护作用。 。 >结果和结论:1976 swH1N1或2009 pH1N1疫苗的免疫接种使小鼠免受了1918年的致死性攻击,这些小鼠没有体重减轻,肺脏的病毒载量和病理显着降低。保护可能是由于通过微中和试验检测到的交叉反应抗体。我们的数据表明,由于先前曾使用1976 swH1N1或2009 pH1N1进行了感染或免疫,因此可能会保护普通人群免于将来发生类似1918年的大流行。此外,流感防护研究通常集中于交叉反应抑制血凝反应的抗体。尽管血凝素是主要的表面抗原,但这不能解释其他流感病毒抗原。中和抗体可能是人类针对致病性流感病毒株的更好保护,因此应考虑疫苗功效。

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