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Memory Immune Responses against Pandemic (H1N1) 2009 Influenza Virus Induced by a Whole Particle Vaccine in Cynomolgus Monkeys Carrying Mafa-A1*052∶02

机译:携带Mafa-A1 * 052∶02的食蟹猴对全颗粒疫苗诱导的2009年H1N1大流行性流感病毒的记忆免疫反应

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摘要

We made an H1N1 vaccine candidate from a virus library consisting of 144 ( = 16 HA×9 NA) non-pathogenic influenza A viruses and examined its protective effects against a pandemic (2009) H1N1 strain using immunologically naïve cynomolgus macaques to exclude preexisting immunity and to employ a preclinical study since preexisting immunity in humans previously vaccinated or infected with influenza virus might make comparison of vaccine efficacy difficult. Furthermore, macaques carrying a major histocompatibility complex class I molecule, Mafa-A1*052∶02, were used to analyze peptide-specific CD8+ T cell responses. Sera of macaques immunized with an inactivated whole particle formulation without addition of an adjuvant showed higher neutralization titers against the vaccine strain A/Hokkaido/2/1981 (H1N1) than did sera of macaques immunized with a split formulation. Neutralization activities against the pandemic strain A/Narita/1/2009 (H1N1) in sera of macaques immunized twice with the split vaccine reached levels similar to those in sera of macaques immunized once with the whole particle vaccine. After inoculation with the pandemic virus, the virus was detected in nasal samples of unvaccinated macaques for 6 days after infection and for 2.67 days and 5.33 days on average in macaques vaccinated with the whole particle vaccine and the split vaccine, respectively. After the challenge infection, recall neutralizing antibody responses against the pandemic virus and CD8+ T cell responses specific for nucleoprotein peptide NP262-270 bound to Mafa-A1*052∶02 in macaques vaccinated with the whole particle vaccine were observed more promptly or more vigorously than those in macaques vaccinated with the split vaccine. These findings demonstrated that the vaccine derived from our virus library was effective for pandemic virus infection in macaques and that the whole particle vaccine conferred more effective memory and broader cross-reactive immune responses to macaques against pandemic influenza virus infection than did the split vaccine.
机译:我们从由144种(= 16 HA×9 NA)非致病性A型流感病毒组成的病毒库中制备了H1N1疫苗候选物,并使用免疫学上食蟹猕猴排除了先前存在的免疫力和之所以要进行临床前研究,是因为先前接种过流感病毒或感染了流感病毒的人中已有的免疫力可能使疫苗功效的比较变得困难。此外,携带主要组织相容性复杂的I类分子Mafa-A1 * 052∶02的猕猴被用于分析肽特异性CD8 + T细胞反应。用灭活的全颗粒制剂免疫而不添加佐剂的猕猴血清比用分体制剂免疫的猕猴血清显示出更高的针对疫苗株A / Hokkaido / 2/1981(H1N1)的中和效价。在用分裂疫苗免疫两次的猕猴血清中,针对大流行毒株A / Narita / 1/2009(H1N1)的中和活性达到与用全颗粒疫苗免疫一次的猕猴血清相同的水平。接种大流行性病毒后,在未接种猕猴的鼻样本中检测到该病毒,感染后6天,而在接种全颗粒疫苗和剖分疫苗的猕猴中分别检测到平均2.67天和5.33天。攻击感染后,在接种全颗粒疫苗的猕猴中,召回的抗大流行病毒的中和抗体反应和特异性结合于Mafa-A1 * 052∶02的核蛋白肽NP262-270的CD8 + T细胞反应比猕猴中接种分裂疫苗的人。这些发现表明,衍生自我们病毒库的疫苗对于猕猴中的大流行性病毒感染是有效的,并且与分离疫苗相比,全颗粒疫苗针对猕猴对大流行性流感病毒感染具有更有效的记忆和更广泛的交叉反应性免疫反应。

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