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伪狂犬病病毒疫苗株Bartha的gIII包膜蛋白编码基因含有一个影响蛋白定位的突变。

The gene encoding the gIII envelope protein of pseudorabies virus vaccine strain Bartha contains a mutation affecting protein localization.

作者信息

Robbins A K, Ryan J P, Whealy M E, Enquist L W

机构信息

Central Research & Development Department, E. I. du Pont de Nemours & Co., Inc., Wilmington, Delaware 19898.

出版信息

J Virol. 1989 Jan;63(1):250-8. doi: 10.1128/JVI.63.1.250-258.1989.

Abstract

Pseudorabies virus (PRV) vaccine strain Bartha has a diminished capacity to cause disease and harbors a variety of mutations affecting virulence. It has been reported that PRV Bartha produces virions with reduced amounts of the major envelope glycoprotein gIII. One hypothesis was that this phenotype was due to reduced expression of the gIII gene. In this report, we demonstrate that the reduced amount of gIII in virions was not mediated at the level of transcription, but rather reflected a defect in protein localization. We describe experiments with gene replacement technology to prove that the expression defect was closely linked to the gIII gene itself. Using pulse-chase experiments, we found a defect similar to that observed for certain signal sequence mutations of PRV Becker gIII. The Bartha gIII protein was translated, but was inefficiently introduced into the membrane protein export pathway. Consequently, only a fraction of the primary Bartha gIII translation product was glycosylated and matured. The remaining fraction stayed presumably in the cytoplasm, where it never became glycosylated or inserted into cell or virus membranes. The result was that Bartha-infected cells produced virions with reduced amounts of gIII in their envelopes. Comparison of the DNA sequence of the promoter and amino-terminal coding regions of Becker and Bartha gIII genes revealed a single base pair difference in Bartha, changing codon 14 of the signal sequence from a leucine (CTC) to a proline (CCC) codon. We suggest that the signal sequence mutation is responsible for the apparent reduced expression phenotype of this attenuated strain. This mutation represents, to our knowledge, the first reported natural signal sequence mutation in a herpesvirus glycoprotein.

摘要

伪狂犬病病毒(PRV)疫苗株Bartha致病能力减弱,携带多种影响毒力的突变。据报道,PRV Bartha产生的病毒粒子中主要包膜糖蛋白gIII的含量减少。一种假说是这种表型是由于gIII基因表达降低所致。在本报告中,我们证明病毒粒子中gIII含量的减少不是在转录水平介导的,而是反映了蛋白质定位的缺陷。我们描述了用基因替换技术进行的实验,以证明表达缺陷与gIII基因本身密切相关。通过脉冲追踪实验,我们发现了一个与PRV Becker gIII某些信号序列突变所观察到的缺陷相似的缺陷。Bartha gIII蛋白被翻译,但低效地进入膜蛋白输出途径。因此,只有一部分初级Bartha gIII翻译产物被糖基化并成熟。其余部分可能留在细胞质中,在那里它从未被糖基化或插入细胞或病毒膜中。结果是,受Bartha感染的细胞产生的病毒粒子包膜中gIII含量减少。对Becker和Bartha gIII基因启动子和氨基末端编码区的DNA序列比较显示,Bartha中有一个单碱基对差异,将信号序列的第14个密码子从亮氨酸(CTC)变为脯氨酸(CCC)密码子。我们认为,信号序列突变是这种减毒株明显的表达降低表型的原因。据我们所知,这种突变是疱疹病毒糖蛋白中首次报道的天然信号序列突变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c38f/247679/6d2e9463916c/jvirol00068-0270-a.jpg

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