Recombination and amino acid point mutations in VP3 exhibit a synergistic effect on increased virulence of rMDPV.

IF 5.5 1区 农林科学 Q1 IMMUNOLOGY Virulence Pub Date : 2024-12-01 Epub Date: 2024-06-13 DOI:10.1080/21505594.2024.2366874
Jianye Wang, Wanmei Li, Xiaoyan Gong, Zhixian Wang, Yu Wang, Jueyi Ling, Zhiwei Jiang, Guoqiang Zhu, Yufeng Li
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Abstract

Recombinant Muscovy duck parvovirus (rMDPV) is a product of genetic recombination between classical Muscovy duck parvovirus (MDPV) and goose parvovirus (GPV). The recombination event took place within a 1.1-kb DNA segment located in the middle of the VP3 gene, and a 187-bp sequence extending from the P9 promoter to the 5' initiation region of the Rep1 ORF. This resulted in the alteration of five amino acids within VP3. Despite these genetic changes, the precise influence of recombination and amino acid mutations on the pathogenicity of rMDPV remains ambiguous. In this study, based on the rMDPV strain ZW and the classical MDPV strain YY, three chimeric viruses (rZW-mP9, rZW-mPR187, and rYY-rVP3) and the five amino acid mutations-introduced mutants (rZW-g5aa and rYY-5aa(ZW)) were generated using reverse genetic technology. When compared to the parental virus rZW, rZW-g5aa exhibited a prolonged mean death time (MDT) and a decreased median lethal dose (ELD50) in embryonated duck eggs. In contrast, rYY-5aa(ZW) did not display significant differences in MDT and ELD50 compared to rYY. In 2-day-old Muscovy ducklings, infection with rZW-g5aa and rYY-5aa(ZW) resulted in mortality rates of only 20% and 10%, respectively, while infections with the three chimeric viruses (rZW-mP9, rZW-mPR187, rYY-rVP3) and rZW still led to 100% mortality. Notably, rYY-rVP3, containing the VP3 region from strain ZW, exhibited 50% mortality in 6-day-old Muscovy ducklings and demonstrated significant horizontal transmission. Collectively, our findings indicate that recombination and consequent amino acid changes in VP3 have a synergistic impact on the heightened virulence of rMDPV in Muscovy ducklings.

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VP3 中的重组和氨基酸点突变对增强 rMDPV 的毒力具有协同作用。
重组鸭副粘病毒(rMDPV)是经典鸭副粘病毒(MDPV)和鹅副粘病毒(GPV)基因重组的产物。重组事件发生在位于 VP3 基因中间的 1.1-kb DNA 片段以及从 P9 启动子延伸到 Rep1 ORF 的 5' 起始区的 187-bp 序列中。这导致了 VP3 中五个氨基酸的改变。尽管发生了这些基因变化,但重组和氨基酸突变对 rMDPV 致病性的确切影响仍不明确。本研究以 rMDPV 株系 ZW 和经典 MDPV 株系 YY 为基础,利用反向遗传技术生成了三种嵌合病毒(rZW-mP9、rZW-mPR187 和 rYY-rVP3)和五个氨基酸突变引入的突变体(rZW-g5aa 和 rYY-5aa(ZW))。与亲本病毒 rZW 相比,rZW-g5aa 的平均死亡时间(MDT)延长,胚胎鸭蛋的中位致死剂量(ELD50)降低。相比之下,rYY-5aa(ZW)与 rYY 相比,在 MDT 和 ELD50 方面没有显著差异。在 2 日龄的中华秋沙鸭中,感染 rZW-g5aa 和 rYY-5aa(ZW) 的死亡率分别仅为 20% 和 10%,而感染三种嵌合病毒(rZW-mP9、rZW-mPR187、rYY-rVP3)和 rZW 的死亡率仍为 100%。值得注意的是,含有 ZW 株 VP3 区域的 rYY-rVP3 在 6 日龄的麝香鸭中的死亡率为 50%,并表现出显著的水平传播。总之,我们的研究结果表明,VP3 的重组和随之而来的氨基酸变化对提高 rMDPV 在麝香鸭中的毒力具有协同作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Virulence
Virulence IMMUNOLOGY-MICROBIOLOGY
CiteScore
9.20
自引率
1.90%
发文量
123
审稿时长
6-12 weeks
期刊介绍: Virulence is a fully open access peer-reviewed journal. All articles will (if accepted) be available for anyone to read anywhere, at any time immediately on publication. Virulence is the first international peer-reviewed journal of its kind to focus exclusively on microbial pathogenicity, the infection process and host-pathogen interactions. To address the new infectious challenges, emerging infectious agents and antimicrobial resistance, there is a clear need for interdisciplinary research.
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