首页> 美国卫生研究院文献>Journal of Virology >The avian influenza virus nucleoprotein gene and a specific constellation of avian and human virus polymerase genes each specify attenuation of avian-human influenza A/Pintail/79 reassortant viruses for monkeys.
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The avian influenza virus nucleoprotein gene and a specific constellation of avian and human virus polymerase genes each specify attenuation of avian-human influenza A/Pintail/79 reassortant viruses for monkeys.

机译:禽流感病毒核蛋白基因以及禽和人类病毒聚合酶基因的特定群均确定了猴的禽-人甲型/尾巴/ 79型重组病毒的减弱。

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摘要

Reassortant viruses which possessed the hemagglutinin and neuraminidase genes of wild-type human influenza A viruses and the remaining six RNA segments (internal genes) of the avian A/Pintail/Alberta/119/79 (H4N6) virus were previously found to be attenuated in humans. To study the genetic basis of this attenuation, we isolated influenza A/Pintail/79 X A/Washington/897/80 reassortant viruses which contained human influenza virus H3N2 surface glycoprotein genes and various combinations of avian or human influenza virus internal genes. Twenty-four reassortant viruses were isolated and first evaluated for infectivity in avian (primary chick kidney [PCK]) and mammalian (Madin-Darby canine kidney [MDCK]) tissue culture lines. Reassortant viruses with two specific constellations of viral polymerase genes exhibited a significant host range restriction of replication in mammalian (MDCK) tissue culture compared with that in avian (PCK) tissue culture. The viral polymerase genotype PB2-avian (A) virus, PB1-A virus, and PA-human (H) virus was associated with a 900-fold restriction, while the viral polymerase genotype PB2-H, PB1-A, and PA-H was associated with an 80,000-fold restriction of replication in MDCK compared with that in PCK. Fifteen reassortant viruses were subsequently evaluated for their level of replication in the respiratory tract of squirrel monkeys, and two genetic determinants of attenuation were identified. First, reassortant viruses which possessed the avian influenza virus nucleoprotein gene were as restricted in replication as a virus which possessed all six internal genes of the avian influenza A virus parent, indicating that the nucleoprotein gene is the major determinant of attenuation of avian-human A/Pintail/79 reassortant viruses for monkeys. Second, reassortant viruses which possessed the viral polymerase gene constellation of PB2-H, PB1-A, and PA-H, which was associated with the greater degree of host range restriction in vitro, were highly restricted in replication in monkeys. Since the avian-human influenza reassortant viruses which expressed either mode of attenuation in monkeys replicated to high titer in eggs and in PCK tissue culture, their failure to replicate efficiently in the respiratory epithelium of primates must be due to the failure of viral factors to interact with primate host cell factors. The implications of these findings for the development of live-virus vaccines and for the evolution of influenza A viruses in nature are discussed.
机译:先前发现具有野生型人甲型流感病毒的血凝素和神经氨酸酶基因以及禽A / Pintail / Alberta / 119/79(H4N6)病毒的其余六个RNA片段(内部基因)的重配病毒在人类。为了研究这种减毒的遗传基础,我们分离了包含人流感病毒H3N2表面糖蛋白基因和禽流感或人流感病毒内部基因的各种组合的A / Pintail / 79 X A / Washington / 897/80流感重配病毒。分离出二十四种重组病毒,并首先评估其在禽类(原发性鸡肾[PCK])和哺乳动物(Madin-Darby犬肾[MDCK])组织中的感染力。与禽类(PCK)组织培养相比,具有两个特定病毒聚合酶基因星座的重配病毒在哺乳动物(MDCK)组织培养中表现出明显的宿主复制范围限制。病毒聚合酶基因型PB2-禽(A)病毒,PB1-A病毒和PA人(H)病毒具有900倍的限制性酶切,而病毒聚合酶基因型PB2-H,PB1-A和PA-与PCK中相比,H与MDCK中80,000倍的复制限制相关。随后评估了15种重配病毒在松鼠猴呼吸道中的复制水平,并鉴定了两个减毒的遗传决定因素。首先,具有禽流感病毒核蛋白基因的重配病毒与具有禽流感A病毒亲本的所有六个内部基因的病毒一样,在复制方面受到限制,这表明核蛋白基因是减缓禽-人A病毒感染的主要决定因素。 / Pintail / 79种针对猴子的重配病毒。第二,具有在体外与宿主范围限制程度更高相关的PB2-H,PB1-A和PA-H病毒聚合酶基因构象的重配病毒在猴中的复制受到高度限制。由于在猴中表达减毒方式的禽-人流感重配病毒在鸡蛋和PCK组织培养物中均复制到高滴度,因此它们不能在灵长类动物的呼吸道上皮中有效复制的原因一定是由于病毒因子无法相互作用与灵长类宿主细胞因子有关。讨论了这些发现对活病毒疫苗的开发以及自然界中甲型流感病毒的进化的意义。

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