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血清阴性成年志愿者中活禽-人重配甲型H3N2和H1N1流感病毒疫苗的评估。

Evaluation of live avian-human reassortant influenza A H3N2 and H1N1 virus vaccines in seronegative adult volunteers.

作者信息

Snyder M H, Clements M L, Betts R F, Dolin R, Buckler-White A J, Tierney E L, Murphy B R

出版信息

J Clin Microbiol. 1986 May;23(5):852-7. doi: 10.1128/jcm.23.5.852-857.1986.

Abstract

An avian-human reassortant influenza A virus deriving its genes coding for the hemagglutinin and neuraminidase from the human influenza A/Washington/897/80 (H3N2) virus and its six "internal" genes from the avian influenza A/Mallard/NY/6750/78 (H2N2) virus (i.e., a six-gene reassortant) was previously shown to be safe, infectious, nontransmissible, and immunogenic as a live virus vaccine in adult humans. Two additional six-gene avian-human reassortant influenza viruses derived from the mating of wild-type human influenza A/California/10/78 (H1N1) and A/Korea/1/82 (H3N2) viruses with the avian influenza A/Mallard/NY/78 virus were evaluated in seronegative (hemagglutination inhibition titer, less than or equal to 1:8) adult volunteers for safety, infectivity, and immunogenicity to determine whether human influenza A viruses can be reproducibly attenuated by the transfer of the six internal genes of the avian influenza A/Mallard/NY/78 virus. The 50% human infectious dose was 10(4.9) 50% tissue culture infectious doses for the H1N1 reassortant virus and 10(5.4) 50% tissue culture infectious doses for the H3N2 reassortant virus. Both reassortants were satisfactorily attenuated with only 5% (H1N1) and 2% (H3N2) of infected vaccines receiving less than 400 50% human infectious doses developing illness. Consistent with this level of attenuation, the magnitude of viral shedding after inoculation was reduced 100-fold (H1N1) to 10,000-fold (H3N2) compared with that produced by wild-type virus. The duration of virus shedding by vaccines was one-third that of controls receiving wild-type virus. At 40 to 100 50% human infectious doses, virus-specific immune responses were seen in 77 to 93% of volunteers. When vaccinees who has received 10(7.5) 50% tissue culture infectious doses of the H3N2 vaccine were experimentally challenged with a homologous wild-type human virus only 2 of 19 (11%) vaccinees became ill compared with 7 of 14 (50%) unvaccinated seronegative controls ( P < 0.025; protective efficacy, 79%). Thus, three different virulent human influenza A viruses have been satisfactorily attenuated by the acquisition of the six internal genes of the avian influenza A/Mallard/NY/78 virus. The observation that this donor virus can reproducibly attenuate human influenza A viruses indicates that avian-human influenza A reassortants should be further studied as potential live influenza A virus vaccines.

摘要

一种禽-人重配甲型流感病毒,其编码血凝素和神经氨酸酶的基因来自人甲型流感病毒A/华盛顿/897/80(H3N2),其六个“内部”基因来自禽甲型流感病毒A/绿头鸭/纽约/6750/78(H2N2)病毒(即六基因重配体),先前已证明作为成人活病毒疫苗是安全、有传染性、不传播且具有免疫原性的。另外两种由野生型人甲型流感病毒A/加利福尼亚/10/78(H1N1)和A/韩国/1/82(H3N2)与禽甲型流感病毒A/绿头鸭/纽约/78病毒交配产生的六基因禽-人重配甲型流感病毒,在血清阴性(血凝抑制效价小于或等于1:8)的成年志愿者中进行了安全性、感染性和免疫原性评估,以确定人甲型流感病毒是否可通过转移禽甲型流感病毒A/绿头鸭/纽约/78病毒的六个内部基因而可重复地减毒。对于H1N1重配病毒,50%人感染剂量为10^(4.9) 50%组织培养感染剂量,对于H3N2重配病毒为10^(5.4) 50%组织培养感染剂量。两种重配体均得到了满意的减毒,接种疫苗的感染者中分别只有5%(H1N1)和2%(H3N2)接受少于400 50%人感染剂量后发病。与这种减毒水平一致,接种后病毒脱落的程度与野生型病毒相比降低了100倍(H1N1)至10000倍(H3N2)。疫苗接种者病毒脱落的持续时间是接受野生型病毒的对照组的三分之一。在40至100 50%人感染剂量时,77%至93%的志愿者出现了病毒特异性免疫反应。当接受10^(7.5) 50%组织培养感染剂量H3N2疫苗的接种者用同源野生型人病毒进行实验性攻击时,19名接种者中只有2名(11%)发病,而14名未接种的血清阴性对照组中有7名(50%)发病(P<0.025;保护效力,79%)。因此,三种不同的致病性人甲型流感病毒通过获得禽甲型流感病毒A/绿头鸭/纽约/78病毒的六个内部基因得到了满意的减毒。这种供体病毒可重复地减毒人甲型流感病毒的观察结果表明,禽-人甲型流感重配体应作为潜在的甲型流感活病毒疫苗进行进一步研究。

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