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鸡和鸭中弗林蛋白酶作为高致病性禽流感病毒血凝素激活蛋白酶的保守表达及功能

Conserved Expression and Functionality of Furin between Chickens and Ducks as an Activating Protease of Highly Pathogenic Avian Influenza Virus Hemagglutinins.

作者信息

de Bruin Anja C M, Spronken Monique I, Bestebroer Theo M, Fouchier Ron A M, Richard Mathilde

机构信息

Department of Viroscience, Erasmus Medical Center, Rotterdam, the Netherlands.

出版信息

Microbiol Spectr. 2023 Mar 14;11(2):e0460222. doi: 10.1128/spectrum.04602-22.

Abstract

Highly pathogenic avian influenza viruses (HPAIVs) typically emerge from low-pathogenic avian influenza viruses (LPAIVs) of the H5 and H7 subtypes upon spillover from wild aquatic birds into poultry. The conversion from LPAIV to HPAIV is characterized by the acquisition of a multibasic cleavage site (MBCS) at the proteolytic cleavage site in the viral binding and fusion protein, hemagglutinin (HA), resulting in cleavage and activation of HA by ubiquitously expressed furin-like proteases. The ensuing HPAIVs disseminate systemically in gallinaceous poultry, are endotheliotropic, and cause hemorrhagic disease with high mortality. HPAIV infections in wild aquatic birds are generally milder, often asymptomatic, and generally not associated with systemic dissemination nor endotheliotropic. As MBCS cleavage by host proteases is the main virulence determinant of HPAIVs in poultry, we set out to determine whether cleavage of HPAIV HA by host proteases might influence the observed species-specific pathogenesis and tropism. Here, we sequenced, cloned, and characterized the expression and functionality of duck furin. The furin sequence was strongly conserved between chickens and ducks, and duck furin cleaved HPAIV and tetrabasic HA in an overexpression system, confirming its functionality. Furin was expressed ubiquitously and to similar extents in duck and chicken tissues, including in primary duck endothelial cells, which sustained multicycle replication of H5N1 HPAIV but not LPAIVs. In conclusion, differences in furin-like protease biology between wild aquatic birds and gallinaceous poultry are unlikely to largely determine the stark differences observed in species-specific pathogenesis of HPAIVs. HPAIV outbreaks are a global concern due to the health risks for poultry, wildlife, and humans and their major economic impact. The number of LPAIV-to-HPAIV conversions, which is associated with spillover from wild birds to poultry, has been increasing over recent decades. Furthermore, H5 HPAIVs from the A/goose/Guangdong/1/96 lineage have been circulating in migratory birds, causing increasingly frequent epizootics in poultry and wild birds. Milder symptoms in migratory birds allow for dispersion of HPAIVs over long distances, justifying the importance of understanding the pathogenesis of HPAIVs in wild birds. Here, we examined whether host proteases are a likely candidate to explain some differences in the degree of HPAIV systemic dissemination between avian species. This is the first report to show that furin function and expression is comparable between chickens and ducks, which renders the hypothesis unlikely that furin-like protease differences influence the HPAIV species-specific pathogenesis and tropism.

摘要

高致病性禽流感病毒(HPAIVs)通常由H5和H7亚型的低致病性禽流感病毒(LPAIVs)从野生水鸟传播到家禽后演变而来。从LPAIV转变为HPAIV的特征是在病毒结合和融合蛋白血凝素(HA)的蛋白水解切割位点获得一个多碱性切割位点(MBCS),导致HA被普遍表达的类弗林蛋白酶切割并激活。随后产生的HPAIVs在家鸡中全身扩散,具有嗜内皮性,并导致高死亡率的出血性疾病。野生水鸟感染HPAIV通常症状较轻,往往无症状,一般不伴有全身扩散和嗜内皮性。由于宿主蛋白酶对MBCS的切割是HPAIV在家禽中毒力的主要决定因素,我们着手确定宿主蛋白酶对HPAIV HA的切割是否会影响所观察到的物种特异性发病机制和嗜性。在此,我们对鸭类弗林蛋白酶的序列进行了测序、克隆,并对其表达和功能进行了表征。鸡和鸭的类弗林蛋白酶序列高度保守,并且鸭类弗林蛋白酶在过表达系统中能够切割HPAIV和四碱性HA,证实了其功能。类弗林蛋白酶在鸭和鸡的组织中普遍表达且程度相似,包括在原代鸭内皮细胞中,该细胞能支持H5N1 HPAIV的多轮复制,但不能支持LPAIVs的复制。总之,野生水鸟和家鸡之间类弗林蛋白酶生物学特性的差异不太可能在很大程度上决定HPAIVs在物种特异性发病机制中所观察到的显著差异。由于对家禽、野生动物和人类的健康风险及其重大经济影响,HPAIV疫情是一个全球关注的问题。近几十年来,与野生鸟类传播到家禽相关的LPAIV向HPAIV的转变数量一直在增加。此外,来自A/鹅/广东/1/96谱系的H5 HPAIVs一直在候鸟中传播,导致家禽和野生鸟类中疫情日益频繁。候鸟中较轻的症状使得HPAIVs能够远距离传播,这说明了了解HPAIVs在野生鸟类中发病机制的重要性。在此,我们研究了宿主蛋白酶是否可能是解释鸟类物种之间HPAIV全身扩散程度差异的一个因素。这是第一份表明鸡和鸭的类弗林蛋白酶功能和表达具有可比性的报告,这使得类弗林蛋白酶样差异影响HPAIV物种特异性发病机制和嗜性这一假设不太可能成立。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f59f/10100678/3c0722a3ee5f/spectrum.04602-22-f001.jpg

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