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对禽-人重配甲型流感病毒A/华盛顿/897/80×A/针尾鸭/119/79在猴子和成年志愿者体内的评估。

Evaluation of avian-human reassortant influenza A/Washington/897/80 x A/Pintail/119/79 virus in monkeys and adult volunteers.

作者信息

Clements M L, Snyder M H, Buckler-White A J, Tierney E L, London W T, Murphy B R

出版信息

J Clin Microbiol. 1986 Jul;24(1):47-51. doi: 10.1128/jcm.24.1.47-51.1986.

Abstract

A reassortant influenza A virus was produced by mating an avian influenza A/Pintail/Alberta/119/79 (H4N6) virus with wild-type human influenza A/Washington/897/80 (H3N2) virus. The avian-human influenza A reassortant virus contained the genes coding for the hemagglutinin and neuraminidase surface antigens of the human influenza wild-type virus and the six other RNA segments (internal genes) of the avian influenza A virus donor. In the lower respiratory tract of squirrel monkeys, this avian-human influenza reassortant virus, like its avian influenza A parent virus, was restricted approximately 100-fold in replication compared with the wild-type human influenza A virus. Despite this restriction of replication, infection of monkeys with the avian-human influenza A reassortant virus induced resistance to wild-type human influenza A virus challenge. In comparison with the wild-type human influenza A virus, the avian-human influenza A reassortant was also fully attenuated when 10(5.5) to 10(7.5) 50% tissue culture infective doses were administered to susceptible adult volunteers. Attenuation was indicated by a more than 300-fold reduction in virus shedding and lack of reactogenicity. The reassortant virus did not spread to susceptible contacts and could not be isolated from the blood or stools of infected adults. The 50% human infectious dose was 10(6.2) 50% tissue culture infective dose, indicating that this reassortant virus is only slightly less infectious for adults than a similarly derived avian-human influenza A/Washington/80 X A/Mallard/78 reassortant virus. These findings suggest that the avian influenza A/Pintail/79 virus may be a satisfactory donor of attenuating genes for production of live, attenuated avian-human influenza A reassortant virus vaccines.

摘要

通过将甲型禽流感病毒A/针尾鸭/艾伯塔/119/79(H4N6)与野生型甲型人流感病毒A/华盛顿/897/80(H3N2)进行交配,产生了一种重配甲型流感病毒。禽-人甲型流感重配病毒包含编码人流感野生型病毒血凝素和神经氨酸酶表面抗原的基因,以及甲型禽流感病毒供体的其他六个RNA片段(内部基因)。在松鼠猴的下呼吸道中,这种禽-人甲型流感重配病毒与其甲型禽流感亲本病毒一样,与野生型甲型人流感病毒相比,其复制受到约100倍的限制。尽管复制受到这种限制,但用禽-人甲型流感重配病毒感染猴子可诱导对野生型甲型人流感病毒攻击的抵抗力。与野生型甲型人流感病毒相比,当向易感成年志愿者接种10(5.5)至10(7.5)个50%组织培养感染剂量的禽-人甲型流感重配病毒时,该病毒也完全减毒。病毒排出减少300倍以上且无反应原性表明了减毒。重配病毒未传播至易感接触者,且无法从感染成年人的血液或粪便中分离出来。50%人感染剂量为10(6.2)个50%组织培养感染剂量,这表明这种重配病毒对成年人的传染性仅略低于类似衍生的禽-人甲型流感病毒A/华盛顿/80×A/绿头鸭/78重配病毒。这些发现表明,甲型禽流感病毒A/针尾鸭/79病毒可能是生产减毒活禽-人甲型流感重配病毒疫苗的减毒基因的理想供体。

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本文引用的文献

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Virulence of avian influenza A viruses for squirrel monkeys.甲型禽流感病毒对松鼠猴的致病性
Infect Immun. 1982 Sep;37(3):1119-26. doi: 10.1128/iai.37.3.1119-1126.1982.

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