首页> 美国卫生研究院文献>Journal of Virology >Four viral genes independently contribute to attenuation of live influenza A/Ann Arbor/6/60 (H2N2) cold-adapted reassortant virus vaccines.
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Four viral genes independently contribute to attenuation of live influenza A/Ann Arbor/6/60 (H2N2) cold-adapted reassortant virus vaccines.

机译:四个病毒基因独立地导致活流感A /安娜堡/ 6/60(H2N2)冷适应的重配病毒疫苗的减毒。

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摘要

Clinical studies previously demonstrated that live influenza A virus vaccines derived by genetic reassortment from the mating of influenza A/Ann Arbor/6/60 (H2N2) cold-adapted (ca) donor virus with epidemic wild-type influenza A viruses are reproducibly safe, infectious, immunogenic, and efficacious in the prevention of illness caused by challenge with virulent wild-type virus. These influenza A reassortant virus vaccines also express the ca and temperature sensitivity (ts) phenotypes in vitro, but the genes of the ca virus parent which specify the ca, ts, and attenuation (att) phenotypes have not adequately been defined. To identify the genes associated with each of these phenotypes, we isolated six single-gene substitution reassortant viruses, each of which inherited only one RNA segment from the ca parent virus and the remaining seven RNA segments from the A/Korea/1/82 (H3N2) wild-type virus parent. These were evaluated in vitro for their ca and ts phenotypes and in ferrets, hamsters, and seronegative adult volunteers for the att phenotype. We found that the polymerase PA gene of the ca parent specifies the ca phenotype and that the PB2 and PB1 genes independently specify the ts phenotype. The PA, M, PB2, and PB1 genes of the ca donor virus each contribute to the att phenotype. The finding that four genes of the ca donor virus contribute to the att phenotype provides a partial explanation for the observed phenotypic stability of ca reassortant viruses following replication in humans.
机译:先前的临床研究表明,通过对A / Ann Arbor / 6/60(H2N2)冷适应(ca)供体病毒与流行的野生型A型流感病毒进行交配而通过基因重组而得的活A型流感病毒疫苗具有可复制的安全性,具有传染性,免疫原性,可有效预防由强毒野生型病毒引起的疾病。这些甲型流感病毒重配病毒疫苗还在体外表达ca和温度敏感性(ts)表型,但是尚未明确定义ca病毒母体的指定ca,ts和减毒(att)表型的基因。为了鉴定与这些表型相关的基因,我们分离了6种单基因替代重配病毒,每种病毒仅从ca亲本病毒中继承了一个RNA片段,而从A / Korea / 1/82中继承了其余7个RNA片段( H3N2)野生型病毒亲本。在体外评估它们的ca和ts表型,在雪貂,仓鼠和血清阴性的成年志愿者中评估att表型。我们发现,ca亲本的聚合酶PA基因指定了ca表型,而PB2和PB1基因独立地指定了ts表型。 ca供体病毒的PA,M,PB2和PB1基因均与att表型有关。 ca供体病毒的四个基因促成att表型的发现为在人类复制后观察到的ca重配病毒的表型稳定性提供了部分解释。

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