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首页> 外文期刊>The Lancet >Development of adenoviral-vector-based pandemic influenza vaccine against antigenically distinct human H5N1 strains in mice.
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Development of adenoviral-vector-based pandemic influenza vaccine against antigenically distinct human H5N1 strains in mice.

机译:针对小鼠中抗原性不同的人类H5N1株的基于腺病毒载体的大流行性流感疫苗的开发。

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INTRODUCTION: Avian H5N1 influenza viruses currently circulating in southeast Asia could potentially cause the next pandemic. However, currently licensed human vaccines are subtype-specific and do not protect against these H5N1 viruses. We aimed to develop an influenza vaccine and assessed its immunogenicity and efficacy to confer protection in BALB/c mice. METHODS: We developed an egg-independent strategy to combat the avian influenza virus, because the virus is highly lethal to chickens and the maintenance of a constant supply of embryonated eggs would be difficult in a pandemic. We used a replication-incompetent, human adenoviral-vector-based, haemagglutinin subtype 5 influenza vaccine (HAd-H5HA), which induces both humoral and cell-mediated immune responses against avian H5N1 influenza viruses isolated from people. FINDINGS: Immunisation of mice with HAd-H5HA provided effective protection from H5N1 disease, death, and primary viral replication (p<0.0001) against antigenically distinct strains of H5N1 influenza viruses. Unlike the recombinant H5HA vaccine, which is based on a traditional subunit vaccine approach, HAd-H5HA vaccine induced a three-fold to eight-fold increase in HA-518-epitope-specific interferon-gamma-secreting CD8 T cells (p=0.01). INTERPRETATION: Our findings highlight the potential of an Ad-vector-based delivery system, which is both egg-independent and adjuvant-independent and offers stockpiling options for the development of a pandemic influenza vaccine.
机译:简介:目前在东南亚流行的禽H5N1流感病毒有可能引起下一次大流行。但是,当前许可的人类疫苗是亚型特异性的,不能抵抗这些H5N1病毒。我们旨在开发一种流感疫苗,并评估其免疫原性和在BALB / c小鼠中提供保护的功效。方法:我们开发了一种不依赖卵子的策略来对抗禽流感病毒,因为该病毒对鸡具有高度致死性,并且在大流行中很难维持恒定数量的胚卵。我们使用了一种无复制能力的,基于人类腺病毒载体的血凝素亚型5型流感疫苗(HAd-H5HA),该疫苗可诱导针对从人分离的禽类H5N1流感病毒的体液免疫和细胞介导的免疫反应。结果:用HAd-H5HA免疫小鼠可有效抵抗H5N1流感病毒的抗原性不同株,从而免受H5N1疾病,死亡和原代病毒复制(p <0.0001)的侵害。与基于传统亚单位疫苗方法的重组H5HA疫苗不同,HAd-H5HA疫苗可诱导HA-518表位特异性干扰素-γ分泌的CD8 T细胞增加三倍至八倍(p = 0.01) )。解释:我们的发现强调了基于Ad载体的传递系统的潜力,该系统既不依赖卵又不依赖佐剂,为大流行性流感疫苗的开发提供了储存选择。

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