Differential effect of acute versus persistent insect-specific flavivirus infection on superinfection exclusion of West Nile, Zika and chikungunya viruses in RNAi-competent and -deficient mosquito cells

IF 4.5 2区 医学 Q1 INFECTIOUS DISEASES One Health Pub Date : 2025-06-01 Epub Date: 2024-12-24 DOI:10.1016/j.onehlt.2024.100960
Wessel Willemsen , Nick Helmes , Gijs J. Overheul , Marleen Henkens , Ruben Spruijt , Ronald P. van Rij , Monique M. van Oers , Gorben P. Pijlman , Jelke J. Fros
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Abstract

Millions of people are annually infected by mosquito-transmitted arboviruses including dengue virus (DENV), West Nile virus (WNV), Zika virus (ZIKV) and chikungunya virus (CHIKV). Insect-specific flaviviruses (ISFs), which only infect mosquitoes and cannot replicate in vertebrates, can offer a potential one health strategy to block the transmission of arboviruses by reducing the mosquito's susceptibility for subsequent arbovirus infections through superinfection exclusion (SIE). Most SIE studies focus on acute ISF infections in RNAi-deficient Aedes albopictus C6/36 cells. Because ISFs are known to persistently infect mosquitoes, acute infections in C6/36 cells may not accurately reflect natural interactions between ISFs and arboviruses. To study the underlying mechanisms for SIE, we persistently infected C6/36 and RNAi-competent Aedes aegypti Aag2 cells with the ISF Binjari virus (BinJV) and a BinJ-ZIKV chimera that contains the ZIKV prME structural genes. SIE of WNV, ZIKV and CHIKV by BinJV was more pronounced in acute than in persistently infected cells and much stronger in acutely infected C6/36 cells compared to Aag2 cells. The viability of RNAi-deficient mosquito cells was severely reduced upon acute ISF infection, which correlated to the observed SIE. However, persistently infected mosquito cells still inhibited subsequent arbovirus replication. Moreover, RNAi-competent Aag2 cells were better protected against ZIKV superinfection when they were pre-infected with BinJ-ZIKV as compared to BinJV. Therefore, acute ISF infections and strong cytopathic effects in RNAi-deficient cells augment SIE, while in persistently infected cells SIE is established through RNAi-dependent and independent mechanisms. This highlight the importance of using more representative in vitro models.
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急性和持续性昆虫特异性黄病毒感染对rnai阳性和缺陷型蚊子细胞排除西尼罗河、寨卡和基孔肯雅病毒重复感染的差异影响
每年有数百万人感染蚊子传播的虫媒病毒,包括登革热病毒(DENV)、西尼罗河病毒(WNV)、寨卡病毒(ZIKV)和基孔肯雅病毒(CHIKV)。昆虫特异性黄病毒(ISFs)只感染蚊子,不能在脊椎动物中复制,它可以通过重复感染排斥(SIE)降低蚊子对后续虫媒病毒感染的易感性,从而提供一种潜在的单一卫生策略来阻止虫媒病毒的传播。大多数SIE研究集中在缺乏rnai的白纹伊蚊C6/36细胞中的急性ISF感染。由于已知isf会持续感染蚊子,因此C6/36细胞中的急性感染可能无法准确反映isf与虫媒病毒之间的自然相互作用。为了研究SIE的潜在机制,我们用ISF宾贾里病毒(BinJV)和含有ZIKV原结构基因的BinJV -ZIKV嵌合体持续感染C6/36和RNAi-competent埃及伊蚊Aag2细胞。BinJV对WNV、ZIKV和CHIKV的SIE在急性感染细胞中比在持续感染细胞中更明显,在急性感染的C6/36细胞中比在Aag2细胞中强得多。急性ISF感染后,rnai缺陷蚊子细胞活力严重降低,这与观察到的SIE相关。然而,持续感染的蚊子细胞仍然抑制随后的虫媒病毒复制。此外,与BinJV相比,RNAi-competent Aag2细胞被BinJV -ZIKV预感染时,对ZIKV重复感染具有更好的保护作用。因此,在rnai缺陷细胞中,急性ISF感染和强烈的细胞病变作用增强了SIE,而在持续感染的细胞中,SIE是通过rnai依赖和独立机制建立的。这突出了使用更具代表性的体外模型的重要性。
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来源期刊
One Health
One Health Medicine-Infectious Diseases
CiteScore
8.10
自引率
4.00%
发文量
95
审稿时长
18 weeks
期刊介绍: One Health - a Gold Open Access journal. The mission of One Health is to provide a platform for rapid communication of high quality scientific knowledge on inter- and intra-species pathogen transmission, bringing together leading experts in virology, bacteriology, parasitology, mycology, vectors and vector-borne diseases, tropical health, veterinary sciences, pathology, immunology, food safety, mathematical modelling, epidemiology, public health research and emergency preparedness. As a Gold Open Access journal, a fee is payable on acceptance of the paper. Please see the Guide for Authors for more information. Submissions to the following categories are welcome: Virology, Bacteriology, Parasitology, Mycology, Vectors and vector-borne diseases, Co-infections and co-morbidities, Disease spatial surveillance, Modelling, Tropical Health, Discovery, Ecosystem Health, Public Health.
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