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温度敏感型狂犬病病毒突变体的生化特性

Biochemical characterization of temperature-sensitive rabies virus mutants.

作者信息

Saghi N, Flamand A

出版信息

J Virol. 1979 Jul;31(1):220-30. doi: 10.1128/JVI.31.1.220-230.1979.

Abstract

Biochemical characterization of 70 temperature-sensitive (ts) mutants of rabies virus has been done by following the appearance of viral proteins and RNA molecules in infected cells at both permissive and nonpermissive temperature. The presence or absence of the nucleocapsid protein (N) was demonstrated by treating infected cells with anti-N fluorescent antibodies. At 33 degrees C, all the mutants induced a fluorescence comparable to the wild type. At 39.6 degrees C, the mutants can be classified into three groups. Three mutants induced a fluorescence comparable to the wild type (F+ mutants); 54 mutants induced a faint fluorescence which was proportional to the multiplicity of infection and increased with time (F+- mutants). No fluorescence could be detected for the 13 remaining mutants (F- mutants). The synthesis of all viral proteins was shown to be normal for F+ mutants, indicating that transcription and replication of the virus were normal and that the ts lesion was located in a protein which is not directly required for those functions. The synthesis of all viral proteins was similarly decreased for F+- mutants and undetectable for the F- mutants. This suggests that the ts lesion affects the transcription and/or replication of the virus. By annealing techniques it was demonstrated that the F+- mutants were able to perform some amount of secondary transcription at nonpermissive temperature. No secondary transcription occurred with F- mutants. When detectable (i.e., at higher multiplicity of infection), primary transcription of F- mutants was normal.

摘要

通过观察狂犬病病毒70个温度敏感(ts)突变体在允许温度和非允许温度下感染细胞中病毒蛋白和RNA分子的出现情况,对其进行了生化特性分析。用抗N荧光抗体处理感染细胞,以证明核衣壳蛋白(N)的存在与否。在33℃时,所有突变体诱导的荧光与野生型相当。在39.6℃时,突变体可分为三组。三个突变体诱导的荧光与野生型相当(F+突变体);54个突变体诱导微弱荧光,其与感染复数成正比,并随时间增加(F+-突变体)。其余13个突变体未检测到荧光(F-突变体)。结果表明,F+突变体所有病毒蛋白的合成正常,这表明病毒的转录和复制正常,ts损伤位于那些功能不直接需要的一种蛋白质中。F+-突变体所有病毒蛋白的合成同样减少,而F-突变体则无法检测到。这表明ts损伤影响病毒的转录和/或复制。通过退火技术证明,F+-突变体能够在非允许温度下进行一定量的二级转录。F-突变体未发生二级转录。当可检测到时(即感染复数较高时),F-突变体的初级转录正常。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7a52/353438/f9a977a17917/jvirol00187-0231-a.jpg

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