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人巨细胞病毒的细胞质包裹需要衣壳蛋白pp28在装配区室中的定位后功能。

Cytoplasmic envelopment of human cytomegalovirus requires the postlocalization function of tegument protein pp28 within the assembly compartment.

作者信息

Seo Jun-Young, Britt William J

机构信息

Department of Microbiology, University of Alabama School of Medicine, and Department of Pediatrics, Children's Hospital, 1600 7th Ave. South, Birmingham, AL 35233, USA.

出版信息

J Virol. 2007 Jun;81(12):6536-47. doi: 10.1128/JVI.02852-06. Epub 2007 Mar 28.

Abstract

The assembly of herpesvirus remains incompletely defined due to the structural complexity of these viruses. Although the assembly of the capsid of these large DNA viruses is well studied and reasonably well conserved for all members of this diverse family of viruses, the cytoplasmic processes of tegumentation and envelopment are not well understood. The virion of the largest human herpesvirus, human cytomegalovirus (HCMV), contains over 70 virus-encoded proteins that are incorporated during a nuclear and cytoplasmic phase of assembly. Envelopment of this virus requires the function of at least one tegument protein, pp28, the product of the UL99 open reading frame. However, the role of pp28 in the envelopment of HCMV remains undefined. We have generated a pp28 mutant virus that encodes only the first 50 amino acids (aa) of this 190-aa virion protein. This virus is replication impaired and is defective in virus assembly. Characterization of both intracellular and extracellular virions from cells infected with this viral mutant indicated that the decrease in production of infectious virus was secondary to a defect in envelopment and the accumulation of tegumented, noninfectious intracellular particles. Image analysis using fluorescence recovery after photobleaching indicated that the pp28 mutant protein encoded by this virus failed to efficiently accumulate in the virus assembly compartment (AC). Our results suggest that pp28 must accumulate in the AC for efficient envelopment of the particle and provide evidence for a direct role of this tegument protein in the late stages of assembly, such as envelopment.

摘要

由于疱疹病毒结构复杂,其组装过程仍未完全明确。尽管这些大型DNA病毒衣壳的组装已得到充分研究,且在这个多样的病毒家族所有成员中相当保守,但衣壳化和包膜化的细胞质过程仍未被充分理解。最大的人类疱疹病毒——人巨细胞病毒(HCMV)的病毒粒子含有70多种病毒编码蛋白,这些蛋白在组装的核内和细胞质阶段被整合进去。该病毒的包膜化需要至少一种衣壳蛋白pp28(UL99开放阅读框的产物)发挥作用。然而,pp28在HCMV包膜化过程中的作用仍不明确。我们构建了一种pp28突变病毒,它仅编码这种190个氨基酸的病毒粒子蛋白的前50个氨基酸。这种病毒复制受损,在病毒组装方面存在缺陷。对感染这种病毒突变体的细胞产生的细胞内和细胞外病毒粒子的特性分析表明,感染性病毒产量的下降是由于包膜化缺陷以及衣壳化的非感染性细胞内颗粒的积累所致。使用光漂白后荧光恢复的图像分析表明,这种病毒编码的pp28突变蛋白未能有效地在病毒组装区室(AC)积累。我们的结果表明,pp28必须在AC中积累才能有效地包裹病毒粒子,并为这种衣壳蛋白在组装后期(如包膜化)的直接作用提供了证据。

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