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Increased virulence of a mouse-adapted variant of influenza A/FM/1/47 virus is controlled by mutations in genome segments 4 5 7 and 8.

机译：适应小鼠的A / FM / 1/47流感病毒变异株的毒力增加受到基因组第4、5、7和8段突变的控制。

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To cause disease, influenza virus must possess several genetically determined abilities that mediate stages in pathogenesis. The virulent mouse-adapted variant A/FM/1/47-MA (FM-MA), derived from the avirulent A/FM/1/47 (FM) strain, had acquired mutations in genes that control virulence. The purpose of this study was to identify those genes that had mutated to result in increased virulence and to obtain viruses that differed in virulence because of differences in individual genome segments. The genes that had mutated to increase virulence were initially identified by genetic analysis of reassortants obtained by crossing FM-MA with the avirulent strain A/HK/1/68 (HK). FM-MA genome segments 4, 5, 7, and 8 were significantly associated with virulence, as determined by using the Wilcoxon ranked sum analysis. The role of FM-MA segments 4, 7, and 8 was confirmed by reintroduction of these genes into the parental strain, which also provided virus strains that differed in virulence because of mutations in individual genome segments. Segments 4, 7, and 8 were responsible for a 10(3.6)-fold increase in virulence that was proportioned 10(2.2)-, 10(0.7)-, and 10(0.8)-fold, respectively. The role of segment 5 could not be confirmed on transfer back into the parental strain because of reversion during preparation of such reassortants. The incidence of reversion was shown to be significantly associated with culturing of FM-MA in chicken embryo cells but was not associated with growth in MDCK cells. The genetic analysis of FM-MA suggests that adaptation to increased virulence is an incremental process that involves the acquisition of mutations in multiple genes, each of which plays an individual role in pathogenesis. The structural and functional properties of segments 4, 7, and 8 that control the virulence of FM-MA can now be determined by using viruses that differ in virulence because of mutations in these individual genome segments.

机译：为了引起疾病，流感病毒必须具有几种基因决定的能力来介导发病机理。衍生自无毒力A / FM / 1/47（FM）株的适应小鼠的强毒变体A / FM / 1 / 47-MA（FM-MA）在控制毒力的基因中获得了突变。这项研究的目的是鉴定那些突变后导致毒力增加的基因，并获得由于各个基因组片段的差异而导致毒力不同的病毒。最初，通过对FM-MA与无毒力菌株A / HK / 1/68（HK）杂交获得的重配子进行遗传分析，初步鉴定出已突变以增加毒力的基因。 FM-MA基因组片段4、5、7和8与毒力显着相关，这是通过使用Wilcoxon排名总和分析确定的。通过将这些基因重新引入亲本菌株，证实了FM-MA片段4、7和8的作用，该亲本菌株还提供了由于各个基因组片段的突变而导致毒力不同的病毒株。区段4、7和8导致毒力增加10（3.6）倍，分别成比例增加10（2.2）-，10（0.7）-和10（0.8）-倍。由于制备此类重配物时会发生逆转，因此无法确定区段5在转移回亲本菌株中的作用。逆转的发生率与鸡胚细胞中FM-MA的培养显着相关，但与MDCK细胞的生长无关。 FM-MA的遗传分析表明，适应增加的毒力是一个渐进的过程，涉及多个基因突变的获得，每个基因在发病机理中均起着各自的作用。现在可以通过使用由于这些单独的基因组片段中的突变而具有不同毒力的病毒来确定控制FM-MA毒力的片段4、7和8的结构和功能特性。

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期刊名称 Journal of Virology
作者
E G Brown;
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年(卷),期 1990(64),9
年度 1990
页码 4523–4533
总页数 11
原文格式 PDF
正文语种
中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;
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专利

1. MUTATIONS IN THE HEMAGGLUTININ AND MATRIX GENES OF A VIRULENT INFLUENZA VIRUS VARIANT, A/FM/1/47-MA, CONTROL DIFFERENT STAGES IN PATHOGENESIS [J] . Smeenk CA, Wright KE, Burns BF, Virus Research: An International Journal of Molecular and Cellular Virology . 1996,第2期

机译：致病性控制不同阶段的致病性流感病毒变异株A / FM / 1 / 47-MA的血凝素和基质基因突变
2. Single mutation at the amino acid position 627 of PB2 that leads to increased virulence of an H5N1 avian influenza virus during adaptation in mice can be compensated by multiple mutations at other sites of PB2. [J] . Li J, Ishaq M, Prudence M Virus Research: An International Journal of Molecular and Cellular Virology . 2009,第1a2期

机译：PB2氨基酸位置627的单个突变会导致H5N1禽流感病毒在小鼠适应过程中增加毒力，该突变可以通过PB2其他位点的多个突变来补偿。
3. The effect of mutations derived from mouse-adapted H3N2 seasonal influenza A virus to pathogenicity and host adaptation [J] . Eun-Ji Choi, Young Jae Lee, Jin-Moo Lee, PLoS One . 2020,第1期

机译：衍生自小鼠适应的H3N2季节性流感的突变的影响致病性和宿主适应性
4. Finding correlated mutations among RNA segments in H3N2 influenza viruses [C] . International Conference on Soft Computing and Intelligent Systems;SCIS;International Symposium on Advanced Intelligent Systems;ISIS . 2012

机译：寻找H3N2流感病毒RNA片段之间的相关突变
5. Characterization of Mutations in the Receptor Binding Site of Influenza A Viruses Determining Virus Host, Tissue, and Cell Tropisms Using Systems Biology Approaches [D] . Wen, Feng. 2018

机译：使用系统生物学方法测定病毒宿主，组织和细胞矫正性的流感病毒的受体结合位点中突变的表征
6. The influenza virus variant A/FM/1/47-MA possesses single amino acid replacements in the hemagglutinin controlling virulence and in the matrix protein controlling virulence as well as growth. [O] . C A Smeenk, E G Brown 1994

机译：流感病毒变体A / FM / 1 / 47-MA在血凝素中具有单个氨基酸替代物可控制毒力而在基质蛋白中则具有单个氨基酸替代物可控制毒力和生长。
7. Pattern of mutation in the genome of influenza A virus on adaptation to increased virulence in the mouse lung: Identification of functional themes [O] . Brown, E. G., Liu, H., Kit, L. Chang, 2001

机译：甲型流感病毒基因组突变模式。适应小鼠肺中增加的毒力：鉴定功能主题
8. Andes Virus M Genome Segment is Not Sufficient to Confer the Virulence Associated With Andres Virus in Syrian Hamsters. [R] . McElroy, A. K., Smith, J. M., Hooper, J. W., 2004

机译：安第斯山脉病毒m基因组片段不足以在叙利亚仓鼠中赋予与安德列斯病毒相关的毒力。

Increased virulence of a mouse-adapted variant of influenza A/FM/1/47 virus is controlled by mutations in genome segments 4 5 7 and 8.

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