Duck Plague Virus Tegument Protein Vp22 Plays a Key Role in the Secondary Envelopment and Cell-to-cell Spread

Overview

Journal Vet Res

Publisher Biomed Central

Specialty Veterinary Medicine

Date 2023 Jul 17

PMID 37461115

Authors

Liping Wu

Mingshu Wang

Anchun Cheng

Bin Tian

Juan Huang

Ying Wu

Qiao Yang

Xumin Ou

Di Sun

Shaqiu Zhang

Xinxin Zhao

Qun Gao

Yu He

Dekang Zhu

Shun Chen

Mafeng Liu

Renyong Jia

Affiliations

Soon will be listed here.

Abstract

Duck plague virus (DPV) is one of the major infectious and fatal diseases of geese, ducks, and other wild waterfowl. The DPV UL49 gene product VP22 is one of the most abundant tegument proteins. However, the role of the DPV VP22 is enigmatic to be clarified. In this study, we found deletion of the UL49 gene resulted in reduced viral growth curve and smaller plaque size in duck embryo fibroblast (DEF) cells, confirming that DPV VP22 is required for efficient viral growth in vitro. In addition, deletion of the UL49 gene inhibited the secondary envelopment of the virus, the release of viral particles, and the spread of viruses between cells. Our study signified the importance of VP22 for DPV secondary envelopment, release, cell-to-cell spread, and accumulation of viral RNA. These findings provide a basis for further study of the function of VP22 in DPV or other herpesviruses.

Citing Articles

Multiple functions of the herpesvirus UL14 gene product in viral infection.

Wan J, Wang M, Cheng A, Zhang W, Yang Q, Tian B Front Microbiol. 2024; 15:1483022.

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