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Attenuation of wild-type human influenza A virus by acquisition of the PA polymerase and matrix protein genes of influenza A/Ann Arbor/6/60 cold-adapted donor virus.

机译：通过获取甲型流感/ Ann Arbor / 6/60冷适应供体病毒的PA聚合酶和基质蛋白基因来减弱野生型人甲型流感病毒。

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Wild-type influenza A viruses can be attenuated for humans by the acquisition of genes from the A/Ann Arbor/6/60 cold-adapted (ca) donor virus. Six-gene reassortants, that is, viruses containing the hemagglutinin and neuraminidase surface glycoprotein genes of the wild-type virus and the six remaining RNA segments of the ca donor virus, are consistently attenuated for humans. During the production of a six-gene reassortant virus containing the surface glycoproteins of the A/Washington/897/80 (H3N2) wild-type virus, a reassortant virus was isolated that contained RNA segments 3 (coding for the polymerase PA protein) and 7 (coding for matrix [M] proteins) from the ca parent and all other genes from the wild-type virus. This reassortant virus is referred to as a two-gene reassortant. Because the gene or set of genes responsible for the attenuation of ca reassortant viruses has not been defined, we evaluated the two-gene reassortant for level of replication and level of virulence in ferrets and in humans, and we compared its characteristics to those of a six-gene reassortant virus derived from the same two parents. The two-gene reassortant virus infected each of 14 adult seronegative (serum hemagglutination inhibition titer of less than or equal to 1:8) volunteers when administered intranasally at a dose of 10(7) 50% tissue culture infectious doses, yet it did not produce illness. The level of replication of the two-gene reassortant virus in the upper respiratory tract was equivalent to that of the six-gene reassortant virus. This demonstrates that transfer of the A/Ann Arbor/6/60 ca PA polymerase and M genes is sufficient to confer the attenuation phenotype on wild-type influenza A viruses. In the context of previous observations, these results suggest that the A/Ann Arbor/6/60 ca donor virus PA polymerase gene plays a major role in the attenuation of ca reassortant viruses.

机译：通过从A / Ann Arbor / 6/60低温适应（ca）供体病毒中获取基因，可以减少人类的野生型A型流感病毒。六基因重组子，即含有野生型病毒的血凝素和神经氨酸酶表面糖蛋白基因以及ca供体病毒的六个剩余RNA片段的病毒，对于人类而言始终是减毒的。在生产包含A / Washington / 897/80（H3N2）野生型病毒表面糖蛋白的六基因重配病毒的过程中，分离出包含RNA片段3（编码聚合酶PA蛋白）的重配病毒。来自亲本的7个（编码基质[M]蛋白）和来自野生型病毒的所有其他基因。该重配病毒被称为两基因重配病毒。由于尚未确定导致ca重配株病毒减毒的基因或一组基因，因此我们评估了这两个基因重配株在雪貂和人类中的复制水平和毒力水平，并将其特征与白鼬的特征进行了比较。来自两个同父系的六基因重配病毒。当以10（7）50％组织培养感染剂量鼻内给药时，这种由两种基因组成的重组病毒可分别感染14名成人血清阴性（血清血凝抑制效价小于或等于1：8）志愿者，但没有感染。产生疾病。在上呼吸道中的两基因重组病毒的复制水平与六基因重组病毒的复制水平相同。这表明A / Ann Arbor / 6/60 ca PA聚合酶和M基因的转移足以赋予野生型A型流感病毒减毒表型。在先前的观察中，这些结果表明，A / Ann Arbor / 6/60 ca供体病毒PA聚合酶基因在减毒ca重组病毒中起主要作用。

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期刊名称 Journal of Clinical Microbiology
作者
M H Snyder; M L Clements; D De Borde; H F Maassab; B R Murphy;
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作者单位

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年(卷),期 1985(22),5
年度 1985
页码 719–725
总页数 7
原文格式 PDF
正文语种
中图分类微生物学;
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专利

1. Attenuation of wild-type human influenza A virus by acquisition of the PA polymerase and matrix protein genes of influenza A/Ann Arbor/6/60 cold-adapted donor virus. [J] . M H Snyder, M L Clements, D De Borde, Journal of Clinical Microbiology . 1985,第5期

机译：通过获取甲型流感/ Ann Arbor / 6/60冷适应供体病毒的PA聚合酶和基质蛋白基因来减弱野生型人甲型流感病毒。
2. Genetic mapping of the cold-adapted phenotype of B/Ann Arbor/1/66, the master donor virus for live attenuated influenza vaccines (FluMist (R)) [J] . Chen Zhongying, Aspelund Amy, Kemble George, Virology . 2006,第2期

机译：B / Ann Arbor / 1/66的冷适应表型的遗传作图，B / Ann Arbor / 1/66是减毒活疫苗的主要供体病毒（FluMist（R））
3. Genetic mapping of the cold-adapted phenotype of B/Ann Arbor/1/66, the master donor virus for live attenuated influenza vaccines (FluMist). [J] . Chen Z, Aspelund A, Kemble G, Virology . 2006,第2期

机译：B / Ann Arbor / 1/66的冷适应表型的遗传作图，B / Ann Arbor / 1/66是减毒活流感疫苗的主要供体病毒（FluMist）。
4. Analysis of promoter binding proteins of Ebp1 that is inhibitor protein of influenza virus RNA polymerase [C] . Mukai M., Honda A. Micro-NanoMechatronics and Human Science, 2009. MHS 2009 . 2009

机译：流行性感冒病毒RNA聚合酶抑制剂蛋白Ebp1的启动子结合蛋白分析
5. Virulence studies associated with influenza A/Ann Arbor/6/60. [D] . Sweet, Thersa Marie. 1998

机译：与甲型流感/安娜堡/ 6/60相关的毒力研究。
6. Evaluation of the genetic stability of the temperature-sensitive PB2 gene mutation of the influenza A/Ann Arbor/6/60 cold-adapted vaccine virus. [O] . J Treanor, M Perkins, R Battaglia, 1994

机译：评估A / Ann Arbor / 6/60型流感适应性疫苗病毒的温度敏感PB2基因突变的遗传稳定性。
7. Genetics of cold-adapted B/Ann Arbor/1/66 influenza virus reassortants: the acidic polymerase (PA) protein gene confers temperature sensitivity and attenuated virulence [O] . Armen M. Donabedian, Dan C. DeBorde, Hunein F. Maassab 1987

机译：冷适应B / ANNARBOR / 1/66流感病毒重新分配的遗传学：酸性聚合酶（PA）蛋白基因赋予温度敏感性和减毒毒力
8. Development of Live, Attenuated Cold-Adapted (CA) Influenza Vaccines. Annual Report October 25, 1985-October 24, 1986 [R] . Maassab, H. F. , DeBorde, D. C. 1986

机译：开发活的，减毒的冷适应（Ca）流感疫苗。年度报告1985年10月25日至1986年10月24日

Attenuation of wild-type human influenza A virus by acquisition of the PA polymerase and matrix protein genes of influenza A/Ann Arbor/6/60 cold-adapted donor virus.

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