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2型单纯疱疹病毒ICP4缺陷型突变体:分离与初步鉴定

Mutants defective in herpes simplex virus type 2 ICP4: isolation and preliminary characterization.

作者信息

Smith C A, Schaffer P A

出版信息

J Virol. 1987 Apr;61(4):1092-7. doi: 10.1128/JVI.61.4.1092-1097.1987.

Abstract

Vero cells were biochemically transformed with the gene encoding ICP4 of herpes simplex virus type 2 (HSV-2). These cells were used as permissive hosts to isolate and propagate HSV-2 mutants defective in this gene. Two mutants, designated hr259 and hr79, were isolated. Neither mutant grew in nontransformed Vero cells, but both grew to near wild-type levels in HSV-2 ICP4-expressing cells. hr259 contains a deletion of about 0.6 kilobases which eliminates the mRNA start site of the ICP4 gene. hr79 contains a mutation which maps by marker rescue to the portion of the ICP4 gene encoding the carboxy-terminal half of the protein. Although hr259 failed to generate any detectable ICP4 mRNA in nontransformed Vero cells, hr79 encoded an ICP4 mRNA which is wild type with respect to size. In nontransformed Vero cells infected with hr259, only ICP0, ICP6, ICP22, and ICP27 were readily detectable. In the case of hr79, a truncated form of ICP4 appeared to be made in addition to ICP0, ICP6, ICP22, and ICP27. Both hr259 and hr79 grew efficiently on cell lines transformed with the ICP4 gene of HSV-1 as evidenced by plating efficiencies and single-burst experiments. Similarly, cells transformed with the ICP4 gene of HSV-2 served as efficient hosts for the growth of d120, HSV-1 ICP4 deletion mutant.

摘要

用编码单纯疱疹病毒2型(HSV - 2)ICP4的基因对非洲绿猴肾细胞(Vero细胞)进行生化转化。这些细胞用作允许性宿主来分离和繁殖该基因缺陷的HSV - 2突变体。分离出了两个突变体,命名为hr259和hr79。这两个突变体在未转化的Vero细胞中均不生长,但在表达HSV - 2 ICP4的细胞中均生长至接近野生型水平。hr259包含约0.6千碱基的缺失,该缺失消除了ICP4基因的mRNA起始位点。hr79包含一个通过标记拯救定位到ICP4基因编码该蛋白质羧基末端一半部分的突变。尽管hr259在未转化的Vero细胞中未能产生任何可检测到的ICP4 mRNA,但hr79编码的ICP4 mRNA在大小方面是野生型的。在感染hr259的未转化Vero细胞中,仅易于检测到ICP0、ICP6、ICP22和ICP27。就hr79而言,除了ICP0、ICP6、ICP22和ICP27外,似乎还产生了一种截短形式的ICP4。通过平板接种效率和单步生长实验证明,hr259和hr79在用HSV - 1的ICP4基因转化的细胞系上均能高效生长。同样,用HSV - 2的ICP4基因转化的细胞作为d120(HSV - 1 ICP4缺失突变体)生长的有效宿主。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3889/254068/5f177b4c9763/jvirol00095-0157-a.jpg

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