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皮钦德病毒温度敏感突变体的特性分析。

Characterization of temperature-sensitive mutants of Pichinde virus.

作者信息

Shivaprakash M, Harnish D, Rawls W

机构信息

Department of Microbiology, Stanford University, California 94305.

出版信息

J Virol. 1988 Nov;62(11):4037-43. doi: 10.1128/JVI.62.11.4037-4043.1988.

Abstract

The synthesis of viral proteins and S RNAs in cells infected with 12 temperature-sensitive (ts) mutants of Pichinde virus was characterized. The mutants could be divided into five groups on the basis of the patterns of radiolabeled proteins immunoprecipitated from infected-cell lysates. Markedly reduced nucleoprotein levels and undetectable amounts of glycoprotein precursor and L protein were synthesized at the nonpermissive temperature in cells infected with five of the mutants. Reduced but detectable amounts of the viral proteins were synthesized at the nonpermissive temperature in cells infected with a single mutant. Two mutants were associated with the intracellular accumulation of glycoprotein precursor, which was apparently not transported across the cell membrane in cells incubated at the nonpermissive temperature. The synthesis of viral proteins in cells infected with two mutants was indistinguishable from those produced by wild-type virus. Two additional mutants were associated with markedly reduced amounts of immunoprecipitable proteins in infected cells incubated at both the permissive and nonpermissive temperatures. Analysis of viral RNA with radiolabeled single-stranded cDNA probes representing complementary and genomic-sense sequences corresponding to the 3' region of S RNA revealed two basic patterns of viral RNA synthesis. At the nonpermissive temperature, the synthesis of complementary- and genomic-sense sequences and mRNA of the S RNA segment was markedly reduced in cells infected with representative members of these mutant groups, suggesting the presence of mutations altering transcriptase activity. Viral-complementary- and genomic-sense sequence and RNA synthesis, as well as nucleoprotein mRNA in cells, was detected in reduced amounts for mutants associated with reduced levels of proteins at both temperatures. Interestingly, RNA species larger than the S RNA segment were detected in cells infected with some of the mutants, especially those with putative transcriptase lesions. These molecules suggest a possible oligomeric intermediate in the synthesis of S RNA of Pichinde virus.

摘要

对感染皮钦德病毒12个温度敏感(ts)突变株的细胞中病毒蛋白和S RNA的合成进行了表征。根据从感染细胞裂解物中免疫沉淀的放射性标记蛋白模式,这些突变株可分为五组。在感染五个突变株之一的细胞中,在非允许温度下,核蛋白水平显著降低,糖蛋白前体和L蛋白的合成量无法检测到。在感染单个突变株的细胞中,在非允许温度下合成的病毒蛋白量减少但可检测到。两个突变株与糖蛋白前体的细胞内积累有关,在非允许温度下培养的细胞中,糖蛋白前体显然没有穿过细胞膜进行转运。感染两个突变株的细胞中病毒蛋白的合成与野生型病毒产生的蛋白合成没有区别。另外两个突变株与在允许温度和非允许温度下培养的感染细胞中可免疫沉淀蛋白的量显著减少有关。用代表与S RNA 3'区域相对应的互补和基因组意义序列的放射性标记单链cDNA探针分析病毒RNA,揭示了病毒RNA合成的两种基本模式。在非允许温度下,感染这些突变株代表成员的细胞中,S RNA片段的互补和基因组意义序列以及mRNA的合成显著减少,这表明存在改变转录酶活性的突变。对于在两个温度下与蛋白水平降低相关的突变株,病毒互补和基因组意义序列及RNA合成以及细胞中的核蛋白mRNA检测量减少。有趣的是,在感染一些突变株的细胞中检测到比S RNA片段更大的RNA种类,尤其是那些具有假定转录酶损伤的突变株。这些分子提示了皮钦德病毒S RNA合成中可能的寡聚中间体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/67c7/253833/240f7c99f123/jvirol00090-0135-a.jpg

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