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1
Temperature-sensitive defect of mutants isolated from L cells persistently infected with Newcastle disease virus.从持续感染新城疫病毒的L细胞中分离出的突变体的温度敏感缺陷。
J Virol. 1973 Sep;12(3):472-80. doi: 10.1128/JVI.12.3.472-480.1973.
2
Selection of temperature-sensitive mutants during persistent infection: role in maintenance of persistent Newcastle disease virus infections of L cells.持续性感染期间温度敏感突变体的选择:在维持L细胞持续性新城疫病毒感染中的作用
J Virol. 1973 Sep;12(3):481-91. doi: 10.1128/JVI.12.3.481-491.1973.
3
Viral ribonuclei acid synthesis by Newcastle disease virus mutants isolated from persistently infected L cells: effect of interferon.从持续感染的L细胞中分离出的新城疫病毒突变体的病毒核糖核酸合成:干扰素的作用
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4
Temperature-sensitive mutants isolated from L cells persistently infected with Newcastle disease virus.从持续感染新城疫病毒的L细胞中分离出的温度敏感突变体。
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5
Cells persistently infected with Newcastle disease virus. II. Ribonucleic acid and protein synthesis in cells infected with mutants isolated from persistently infected L cells.持续感染新城疫病毒的细胞。II. 感染从持续感染的L细胞中分离出的突变体的细胞中的核糖核酸和蛋白质合成
J Virol. 1970 Jul;6(1):42-8. doi: 10.1128/JVI.6.1.42-48.1970.
6
Comparison of RNA polymerase associated with Newcastle disease virus and a temperature-sensitive mutant of Newcastle disease virus isolated from persistently infected L cells.与新城疫病毒以及从持续感染的L细胞中分离出的新城疫病毒温度敏感突变体相关的RNA聚合酶的比较。
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7
RNA-dependent DNA polymerase activity in preparations of a mutant of Newcastle disease virus arising from persistently infected L cells.源自持续感染的L细胞的新城疫病毒突变体制剂中的RNA依赖性DNA聚合酶活性。
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Temperature-sensitive mutants isolated from hamster and canine cell lines persistently infected with Newcastle disease virus.从持续感染新城疫病毒的仓鼠和犬类细胞系中分离出的温度敏感突变体。
J Virol. 1975 Nov;16(5):1332-6. doi: 10.1128/JVI.16.5.1332-1336.1975.

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Early stage of establishment of persistent Sendai virus infection: unstable dynamic phase and then selection of viruses which are tightly cell associated, temperature sensitive, and capable of establishing persistent infection.仙台病毒持续性感染建立的早期阶段:不稳定的动态期,随后选择与细胞紧密相关、温度敏感且能够建立持续性感染的病毒。
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7
Viruses isolated from cells persistently infected with vesicular stomatitis virus show altered interactions with defective interfering particles.从持续感染水疱性口炎病毒的细胞中分离出的病毒,与缺陷干扰颗粒的相互作用发生了改变。
J Virol. 1980 Nov;36(2):627-31. doi: 10.1128/JVI.36.2.627-631.1980.
8
Newcastle disease virus infection of L cells.新城疫病毒对L细胞的感染。
J Virol. 1974 Jul;14(1):162-9. doi: 10.1128/JVI.14.1.162-169.1974.
9
Selection of temperature-sensitive mutants during persistent infection: role in maintenance of persistent Newcastle disease virus infections of L cells.持续性感染期间温度敏感突变体的选择:在维持L细胞持续性新城疫病毒感染中的作用
J Virol. 1973 Sep;12(3):481-91. doi: 10.1128/JVI.12.3.481-491.1973.
10
Analysis of a viral agent isolated from multiple sclerosis brain tissue: characterization as a parainfluenzavirus type 1.从多发性硬化症脑组织中分离出的一种病毒病原体的分析:鉴定为1型副流感病毒。
J Virol. 1974 May;13(5):1037-45. doi: 10.1128/JVI.13.5.1037-1045.1974.

本文引用的文献

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Cells persistently infected with newcastle disease virus: I. Properties of mutants isolated from persistently infected L cells.持续感染新城疫病毒的细胞:I. 从持续感染的L细胞中分离出的突变体的特性。
J Virol. 1969 Sep;4(3):244-51. doi: 10.1128/JVI.4.3.244-251.1969.
2
Interference between viable strains of Newcastle disease virus.新城疫病毒活毒株之间的干扰
J Bacteriol. 1961 Dec;82(6):979-83. doi: 10.1128/jb.82.6.979-983.1961.
3
Studies on mixed infection with Newcastle disease virus. II. The occurrence of Newcastle disease virus heterozygotes and study of phenotypic mixing involving serotype and thermal stability.新城疫病毒混合感染的研究。II. 新城疫病毒杂合子的出现及涉及血清型和热稳定性的表型混合研究。
Virology. 1959 Dec;9:649-70. doi: 10.1016/0042-6822(59)90155-2.
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Loss of viral receptors in homologous interference by ultraviolet-irradiated Newcastle disease virus.紫外线照射的新城疫病毒同源干扰中病毒受体的丧失
Virology. 1959 Mar;7(3):315-27. doi: 10.1016/0042-6822(59)90201-6.
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Homologous interference by ultraviolet-inactivated Newcastle disease virus.紫外线灭活的新城疫病毒的同源干扰作用
Virology. 1957 Aug;4(1):72-96. doi: 10.1016/0042-6822(57)90044-2.
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Noninfectious forms of Newcastle disease and influenza viruses; studies on noninfectious virus occurring within cells that are producing fully infectious virus.新城疫病毒和流感病毒的非感染性形式;对在产生完全感染性病毒的细胞内出现的非感染性病毒的研究。
Virology. 1955 Dec;1(5):516-32. doi: 10.1016/0042-6822(55)90040-4.
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Complementation between temperature-sensitive mutants of Sindbis virus.辛德毕斯病毒温度敏感突变体之间的互补作用。
Virology. 1966 Oct;30(2):214-23. doi: 10.1016/0042-6822(66)90097-3.
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Isolation and characterization of conditional-lethal mutants of Sindbis virus.辛德毕斯病毒条件致死突变体的分离与鉴定。
Virology. 1966 Oct;30(2):204-13. doi: 10.1016/0042-6822(66)90096-1.
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A radiobiological study of the development of Newcastle disease virus.新城疫病毒发育的放射生物学研究。
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10
Studies on the RNA polymrase of some temperature-sensitive mutants of Semliki Forest virus.对一些辛德毕斯病毒温度敏感突变体的RNA聚合酶的研究。
Virology. 1969 Sep;39(1):107-17. doi: 10.1016/0042-6822(69)90352-3.

从持续感染新城疫病毒的L细胞中分离出的突变体的温度敏感缺陷。

Temperature-sensitive defect of mutants isolated from L cells persistently infected with Newcastle disease virus.

作者信息

Preble O T, Youngner J S

出版信息

J Virol. 1973 Sep;12(3):472-80. doi: 10.1128/JVI.12.3.472-480.1973.

DOI:10.1128/JVI.12.3.472-480.1973
PMID:4795830
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC356653/
Abstract

The temperature-sensitive defects of virus mutants isolated from L cells persistently infected with Newcastle disease virus (NDV) were analyzed. Genetic grouping of the mutants by complementation tests was attempted by using several different methods, including yield analysis, RNA synthesis, and heterozygote formation at 42 to 43 C, the nonpermissive temperature. In each case, specific interference prevented detection of complementation. This interference was shown to occur prior to or at the level of virus RNA synthesis. Temperature-shift experiments with five different NDV(pi) clones showed that virus replication begun at 37 C could not be completed at the nonpermissive temperature. The activity of the NDV-specific RNA-dependent RNA polymerase in the cytoplasm of infected chicken embryo cells was not stable and could not be demonstrated directly. However, indirect measurement of RNA polymerase activity at the nonpermissive temperature was accomplished by studying the kinetics of virus-specific RNA synthesis in infected cells after temperature shift. Two types of response were obtained: with three NDV(pi) clones, virus-specific RNA synthesis ceased immediately upon transfer of infected cells to 42 to 43 C, whereas in cells infected with two other NDV(pi) clones, RNA synthesis continued for several hours at this temperature. These results suggested that there may be two types of ts defects in NDV(pi), both associated with virus-specific RNA polymerase activity.

摘要

对从持续感染新城疫病毒(NDV)的L细胞中分离出的病毒突变体的温度敏感性缺陷进行了分析。尝试通过几种不同方法,包括产量分析、RNA合成以及在42至43°C(非允许温度)下杂合子形成,对突变体进行互补试验遗传分组。在每种情况下,特异性干扰都阻止了互补作用的检测。这种干扰显示发生在病毒RNA合成之前或该水平。对五个不同的NDV(pi)克隆进行温度转换实验表明,在37°C开始的病毒复制在非允许温度下无法完成。感染鸡胚细胞细胞质中NDV特异性RNA依赖性RNA聚合酶的活性不稳定,无法直接证明。然而,通过研究温度转换后感染细胞中病毒特异性RNA合成的动力学,在非允许温度下间接测量了RNA聚合酶活性。获得了两种类型的反应:对于三个NDV(pi)克隆,感染细胞转移到42至43°C后,病毒特异性RNA合成立即停止,而在感染其他两个NDV(pi)克隆的细胞中,RNA合成在该温度下持续数小时。这些结果表明,NDV(pi)可能存在两种类型的温度敏感缺陷,均与病毒特异性RNA聚合酶活性有关。