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和的实验性爬行动物沙粒病毒感染

Experimental Reptarenavirus Infection of and .

作者信息

Hetzel U, Korzyukov Y, Keller S, Szirovicza L, Pesch T, Vapalahti O, Kipar A, Hepojoki J

机构信息

Institute of Veterinary Pathology, Vetsuisse Faculty, University of Zürich, Zürich, Switzerland.

University of Helsinki, Department of Veterinary Biosciences, Faculty of Veterinary Medicine, Helsinki, Finland.

出版信息

J Virol. 2021 Mar 10;95(7). doi: 10.1128/JVI.01968-20. Epub 2021 Jan 13.

Abstract

Boid inclusion body disease (BIBD) causes losses in captive snake populations globally. BIBD is associated with the formation of cytoplasmic inclusion bodies (IBs), which mainly comprise reptarenavirus nucleoprotein (NP). In 2017, BIBD was reproduced by cardiac injection of boas and pythons with reptarenaviruses, thus demonstrating a causative link between reptarenavirus infection and the disease. Here, we report experimental infections of ( = 16) and ( = 16) with three reptarenavirus isolates. First, we used pythons ( = 8) to test two virus delivery routes: intraperitoneal injection and tracheal instillation. Viral RNAs but no IBs were detected in brains and lungs at 2 weeks postinoculation. Next, we inoculated pythons ( = 8) via the trachea. During the 4 months following infection, snakes showed transient central nervous system (CNS) signs but lacked detectable IBs at the time of euthanasia. One of the snakes developed severe CNS signs; we succeeded in reisolating the virus from the brain of this individual and could demonstrate viral antigen in neurons. In a third attempt, we tested cohousing, vaccination, and sequential infection with multiple reptarenavirus isolates on boas ( = 16). At 10 months postinoculation, all but one snake tested positive for viral RNA in lung, brain, and/or blood, but none exhibited the characteristic IBs. Three of the four vaccinated snakes seemed to sustain challenge with the same reptarenavirus; however, neither of the two snakes rechallenged with different reptarenaviruses remained uninfected. Comparison of the antibody responses in experimentally versus naturally reptarenavirus-infected animals indicated differences in the responses. In the present study, we experimentally infected pythons and boas with reptarenavirus via either intraperitoneal injection or tracheal instillation. The aims were to experimentally induce boid inclusion body disease (BIBD) and to develop an animal model for studying disease transmission and pathogenesis. Both virus delivery routes resulted in infection, and infection via the trachea could reflect the natural route of infection. In the experimentally infected snakes, we did not find evidence of inclusion body (IB) formation, characteristic of BIBD, in pythons or boas. Most of the boas (11/12) remained reptarenavirus infected after 10 months, which suggests that they developed a persistent infection that could eventually have led to BIBD. We demonstrated that vaccination using recombinant protein or an inactivated virus preparation prevented infection by a homologous virus in three of four snakes. Comparison of the antibody responses of experimentally and naturally reptarenavirus-infected snakes revealed differences that merit further studies.

摘要

蛇类包涵体病(BIBD)在全球范围内导致圈养蛇类种群数量减少。BIBD与细胞质包涵体(IBs)的形成有关,这些包涵体主要由爬行动物沙粒病毒核蛋白(NP)组成。2017年,通过向蟒和蚺心脏注射爬行动物沙粒病毒,成功复制出了BIBD,从而证明了爬行动物沙粒病毒感染与该疾病之间的因果关系。在此,我们报告了用三种爬行动物沙粒病毒分离株对16条蟒和16条蚺进行的实验性感染。首先,我们用8条蟒来测试两种病毒接种途径:腹腔注射和气管滴注。接种后2周,在脑和肺中检测到病毒RNA,但未检测到包涵体。接下来,我们通过气管对8条蟒进行接种。在感染后的4个月里,蛇出现了短暂的中枢神经系统(CNS)症状,但在安乐死时未检测到可检测到的包涵体。其中一条蛇出现了严重的CNS症状;我们成功地从该个体的脑中重新分离出病毒,并能在神经元中显示病毒抗原。在第三次尝试中,我们对16条蚺测试了同居、疫苗接种以及用多种爬行动物沙粒病毒分离株进行序贯感染。接种后10个月,除一条蛇外,所有蛇在肺、脑和/或血液中病毒RNA检测均呈阳性,但均未表现出特征性的包涵体。四只接种疫苗的蛇中有三只似乎能抵御同一爬行动物沙粒病毒的攻击;然而,用不同爬行动物沙粒病毒再次攻击的两条蛇均未保持未感染状态。对实验感染与自然感染爬行动物沙粒病毒的动物的抗体反应进行比较,结果表明反应存在差异。在本研究中,我们通过腹腔注射或气管滴注用爬行动物沙粒病毒对蟒和蚺进行了实验性感染。目的是通过实验诱导蛇类包涵体病(BIBD)并建立一个用于研究疾病传播和发病机制的动物模型。两种病毒接种途径均导致了感染,并且通过气管感染可能反映了自然感染途径。在实验感染的蛇中,我们在蟒或蚺中未发现蛇类包涵体病特征性的包涵体形成的证据。大多数蚺(11/12)在10个月后仍感染爬行动物沙粒病毒,这表明它们发生了持续性感染,最终可能导致BIBD。我们证明,使用重组蛋白或灭活病毒制剂进行疫苗接种可在四条蛇中的三条中预防同源病毒的感染。对实验感染和自然感染爬行动物沙粒病毒的蛇的抗体反应进行比较,发现了值得进一步研究的差异。

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