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三种甲型H2大流行性流感减毒活疫苗候选株在小鼠和雪貂体内的评估。

Evaluation of three live attenuated H2 pandemic influenza vaccine candidates in mice and ferrets.

作者信息

Chen Grace L, Lamirande Elaine W, Cheng Xing, Torres-Velez Fernando, Orandle Marlene, Jin Hong, Kemble George, Subbarao Kanta

机构信息

Laboratory of Infectious Diseases, NIAID, NIH, Bethesda, Maryland, USA.

出版信息

J Virol. 2014 Mar;88(5):2867-76. doi: 10.1128/JVI.01829-13. Epub 2013 Dec 26.

Abstract

UNLABELLED

H2 influenza viruses have not circulated in humans since 1968, and therefore a significant portion of the population would be susceptible to infection should H2 influenza viruses reemerge. H2 influenza viruses continue to circulate in avian reservoirs worldwide, and these reservoirs are a potential source from which these viruses could emerge. Three reassortant cold-adapted (ca) H2 pandemic influenza vaccine candidates with hemagglutinin (HA) and neuraminidase (NA) genes derived from the wild-type A/Japan/305/1957 (H2N2) (Jap/57), A/mallard/6750/1978 (H2N2) (mal/78), or A/swine/MO/4296424/2006 (H2N3) (sw/06) viruses and the internal protein gene segments from the A/Ann Arbor/6/60 ca virus were generated by plasmid-based reverse genetics (Jap/57 ca, mal/78 ca, and sw/06 ca, respectively). The vaccine candidates exhibited the in vitro phenotypes of temperature sensitivity and cold adaptation and were restricted in replication in the respiratory tract of ferrets. In mice and ferrets, the vaccines elicited neutralizing antibodies and conferred protection against homologous wild-type virus challenge. Of the three candidates, the sw/06 ca vaccine elicited cross-reactive antibodies and provided significant protection against the greatest number of heterologous viruses. These observations suggest that the sw/06 ca vaccine should be further evaluated in a clinical trial as an H2 pandemic influenza vaccine candidate.

IMPORTANCE

Influenza pandemics arise when novel influenza viruses are introduced into a population with little prior immunity to the new virus and often result in higher rates of illness and death than annual seasonal influenza epidemics. An influenza H2 subtype virus caused a pandemic in 1957, and H2 viruses circulated in humans till 1968. H2 influenza viruses continue to circulate in birds, and the development of an H2 influenza vaccine candidate is therefore considered a priority in preparing for future pandemics. However, we cannot predict whether a human H2 virus will reemerge or a novel avian H2 virus will emerge. We identified three viruses as suitable candidates for further evaluation as vaccines to protect against H2 influenza viruses and evaluated the immune responses and protection that these three vaccines provided in mice and ferrets.

摘要

未标记

自1968年以来,H2流感病毒未在人类中传播,因此,如果H2流感病毒再次出现,很大一部分人群将易受感染。H2流感病毒继续在全球禽类宿主中传播,这些宿主是这些病毒可能出现的潜在来源。通过基于质粒的反向遗传学产生了三种重配的冷适应(ca)H2大流行性流感疫苗候选株,其血凝素(HA)和神经氨酸酶(NA)基因分别来源于野生型A/日本/305/1957(H2N2)(Jap/57)、A/野鸭/6750/1978(H2N2)(mal/78)或A/猪/密苏里州/4296424/2006(H2N)(sw/06)病毒,内部蛋白基因片段来源于A/安阿伯/6/60 ca病毒(分别为Jap/57 ca、mal/78 ca和sw/06 ca)。这些疫苗候选株表现出温度敏感性和冷适应的体外表型,并且在雪貂呼吸道中的复制受到限制。在小鼠和雪貂中,这些疫苗引发中和抗体并提供针对同源野生型病毒攻击的保护。在这三种候选疫苗中,sw/06 ca疫苗引发交叉反应性抗体,并对最多数量的异源病毒提供显著保护。这些观察结果表明,sw/06 ca疫苗应作为H2大流行性流感疫苗候选株在临床试验中进一步评估。

重要性

当新型流感病毒引入对新病毒几乎没有预先免疫力的人群时,就会发生流感大流行,并且通常导致比年度季节性流感流行更高的发病率和死亡率。H2亚型流感病毒在1957年引发了一次大流行,并且H2病毒在人类中传播至1968年。H2流感病毒继续在鸟类中传播,因此,开发H2流感疫苗候选株被认为是为未来大流行做准备的优先事项。然而,我们无法预测人类H2病毒是否会再次出现或新型禽类H2病毒是否会出现。我们鉴定出三种病毒作为进一步评估为预防H2流感病毒疫苗的合适候选株,并评估了这三种疫苗在小鼠和雪貂中提供的免疫反应和保护作用。

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