GPCR Inhibitors Have Antiviral Properties against JC Polyomavirus Infection.

IF 3.8 3区 医学 Q2 VIROLOGY
Viruses-Basel Pub Date : 2024-09-30 DOI:10.3390/v16101559
Amanda L Sandberg, Avery C S Bond, Lucas J Bennett, Sophie E Craig, David P Winski, Lara C Kirkby, Abby R Kraemer, Kristina G Kelly, Samuel T Hess, Melissa S Maginnis
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Abstract

JC polyomavirus (JCPyV) infects the majority of the population and initially establishes a persistent but asymptomatic infection of the kidneys. In healthy individuals, the infection remains controlled by the host immune system, but for individuals experiencing prolonged immunosuppression, the infection can reactivate and spread to the brain, where it causes progressive multifocal leukoencephalopathy (PML), which is a fatal neurodegenerative disease. Currently, there are no approved therapies to treat PML, and affected individuals suffer rapid motor weakness and cognitive deterioration. To identify novel therapeutic treatments for JCPyV infection, receptor agonists/antagonists identified in a previously published drug screen were evaluated for their antiviral properties. Seven drugs were selected and validated using infectivity assays, and the mechanism of inhibition was further explored for G protein coupled receptor (GPCR)-associated inhibitors due to the role of the GPCR 5-hydroxytryptamine 2 receptors (5-HT2Rs) in JCPyV entry. The inhibitors cetirizine and paroxetine both reduced infection early in the JCPyV infectious cycle. Paroxetine specifically reduced viral internalization through altering the receptor density of 5-HT2CR, inhibiting β-arrestin recruitment to the receptor, and reducing MAPK signaling through ERK. These findings highlight the potential of receptor signaling and viral entry mechanisms as possible targets for antiviral drug development. Further, this research suggests that FDA-approved receptor agonists/antagonists currently used to treat other medical conditions could be repurposed into antivirals for the possible treatment of JCPyV infection and the fatal disease PML.

GPCR 抑制剂具有抗 JC 多瘤病毒感染的病毒特性
JC 多瘤病毒(JCPyV)会感染大多数人群,最初会在肾脏形成持续性无症状感染。对于健康人来说,宿主免疫系统仍能控制感染,但对于长期处于免疫抑制状态的人来说,感染会重新激活并扩散到大脑,在大脑中引起进行性多灶性白质脑病(PML),这是一种致命的神经退行性疾病。目前,治疗 PML 的疗法尚未获得批准,患者会迅速出现运动乏力和认知功能衰退。为了找出治疗 JCPyV 感染的新疗法,我们对之前发表的药物筛选中发现的受体激动剂/拮抗剂的抗病毒特性进行了评估。由于 GPCR 5-hydroxytryptamine 2 受体(5-HT2Rs)在 JCPyV 进入中的作用,我们进一步探索了 G 蛋白偶联受体(GPCR)相关抑制剂的抑制机制。西替利嗪和帕罗西汀抑制剂都能减少 JCPyV 感染周期早期的感染。帕罗西汀通过改变 5-HT2CR 的受体密度、抑制 β-restin 募集到受体以及通过 ERK 减少 MAPK 信号传导,特异性地减少了病毒的内化。这些发现凸显了受体信号转导和病毒进入机制作为抗病毒药物开发可能靶点的潜力。此外,这项研究还表明,目前用于治疗其他疾病的美国食品与药物管理局批准的受体激动剂/拮抗剂可以重新用于抗病毒药物,以治疗 JCPyV 感染和致命疾病 PML。
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来源期刊
Viruses-Basel
Viruses-Basel VIROLOGY-
CiteScore
7.30
自引率
12.80%
发文量
2445
审稿时长
1 months
期刊介绍: Viruses (ISSN 1999-4915) is an open access journal which provides an advanced forum for studies of viruses. It publishes reviews, regular research papers, communications, conference reports and short notes. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced. We also encourage the publication of timely reviews and commentaries on topics of interest to the virology community and feature highlights from the virology literature in the ''News and Views'' section. Electronic files or software regarding the full details of the calculation and experimental procedure, if unable to be published in a normal way, can be deposited as supplementary material.
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