High-throughput split-GFP antiviral screening assay against fusogenic paramyxoviruses.

IF 4.5 2区医学 Q1 PHARMACOLOGY & PHARMACY

Antiviral research Pub Date : 2025-07-21 DOI:10.1016/j.antiviral.2025.106242

Laura Vandemaele, Thibault Francken, Joost Schepers, Winston Chiu, Niels Cremers, Hugo Klaassen, Charlène Marcadet, Lorena Sanchez Felipe, Arnaud Marchand, Patrick Chaltin, Pieter Leyssen, Johan Neyts, Manon Laporte

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引用次数: 0

Abstract

The paramyxovirus family includes important pathogens such as measles and mumps viruses, as well as emerging pathogens with pandemic potential such as Nipah virus. Despite the threat to public health and the frequent identification of novel paramyxoviruses, no antiviral drugs are currently available. A hallmark of most paramyxoviruses is the induction of cell-cell fusion leading to syncytia formation. To facilitate antiviral drug discovery, we leveraged this trait and established a high-throughput split-green fluorescent protein (GFP) antiviral screening assay suitable for high-content imaging through the quantification of virus-induced GFP⁺ syncytia. The assay was validated with well-known broad-spectrum antiviral compounds against representative members of five different Paramyxovirinae genera. Using this split-GFP assay, a small-molecule repurposing library of approximately 3000 compounds was screened against recombinant Cedar virus, a nonpathogenic henipavirus. Two molecules were identified: Cathepsin Inhibitor 1 with henipavirus-specific activity and PF-543 with pan-paramyxovirus activity. Both molecules inhibit viral replication by blocking cell-cell fusion. The split-GFP assay presented here will enable the development of extensive drug discovery initiatives aimed at identifying much-needed pan-henipavirus/paramyxovirus inhibitors.

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高通量分裂- gfp抗融合副粘病毒筛选试验。

副粘病毒家族包括麻疹和腮腺炎病毒等重要病原体，以及尼帕病毒等具有大流行潜力的新出现病原体。尽管对公共卫生构成威胁，并且经常发现新型副粘病毒，但目前尚无抗病毒药物可用。大多数副粘病毒的一个特点是诱导细胞-细胞融合导致合胞体的形成。为了促进抗病毒药物的发现，我们利用这一特性，通过对病毒诱导的GFP+合胞体的定量分析，建立了适用于高含量成像的高通量分裂绿色荧光蛋白（GFP）抗病毒筛选试验。该试验与众所周知的广谱抗病毒化合物对五个不同副粘病毒属的代表成员进行了验证。利用这种分裂- gfp试验，筛选了一个含有约3000种化合物的小分子重组文库，以对抗重组雪松病毒（一种非致病性亨尼帕病毒）。鉴定出两个分子：具有亨尼帕病毒特异性活性的组织蛋白酶抑制剂1和具有泛副粘病毒活性的PF-543。这两种分子都通过阻断细胞-细胞融合来抑制病毒复制。这里提出的分裂- gfp测定将使广泛的药物发现倡议的发展，旨在确定急需的泛亨尼帕病毒/副粘病毒抑制剂。

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

Antiviral research 医学-病毒学

CiteScore

17.10

自引率

3.90%

发文量

157

审稿时长

34 days

期刊介绍： Antiviral Research is a journal that focuses on various aspects of controlling viral infections in both humans and animals. It is a platform for publishing research reports, short communications, review articles, and commentaries. The journal covers a wide range of topics including antiviral drugs, antibodies, and host-response modifiers. These topics encompass their synthesis, in vitro and in vivo testing, as well as mechanisms of action. Additionally, the journal also publishes studies on the development of new or improved vaccines against viral infections in humans. It delves into assessing the safety of drugs and vaccines, tracking the evolution of drug or vaccine-resistant viruses, and developing effective countermeasures. Another area of interest includes the identification and validation of new drug targets. The journal further explores laboratory animal models of viral diseases, investigates the pathogenesis of viral diseases, and examines the mechanisms by which viruses avoid host immune responses.