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用于研究猫冠状病毒有前途抑制剂的 RNA 复制子系统。

An RNA replicon system to investigate promising inhibitors of feline coronavirus.

机构信息

Institute of Virology and Immunology (IVI), Bern and Mittelhäusern, Switzerland.

Department of Infectious Diseases and Pathobiology, Vetsuisse Faculty, University of Bern, Bern, Switzerland.

出版信息

J Virol. 2024 Feb 20;98(2):e0121623. doi: 10.1128/jvi.01216-23. Epub 2024 Jan 18.

Abstract

Feline infectious peritonitis (FIP) is a fatal feline disease, caused by a feline coronavirus (FCoV), namely feline infectious peritonitis virus (FIPV). We produced a baby hamster kidney 21 (BHK) cell line expressing a serotype I FCoV replicon RNA with a green fluorescent protein (GFP) reporter gene (BHK-F-Rep) and used it as an screening system to test different antiviral compounds. Two inhibitors of the FCoV main protease (M), namely GC376 and Nirmatrelvir, as well as the nucleoside analog Remdesivir proved to be effective in inhibiting the replicon system. Different combinations of these compounds also proved to be potent inhibitors, having an additive effect when combined. Remdesivir, GC376, and Nirmatrelvir all have a 50% cytotoxic concentration (CC50) more than 200 times higher than their half-maximal inhibitory concentrations (IC50), making them important candidates for future studies as well as clinically implemented drug candidates. In addition, results were acquired with a virus infection system, where whole fetus 4 (Fcwf-4) cells were infected with a previously described recombinant GFP-expressing FIPV (based on the laboratory-adapted serotype I FIPV strain Black) and treated with the most promising compounds. Results acquired with the replicon system were comparable to the results acquired with the virus infection system, demonstrating that we successfully implemented the FCoV replicon system for antiviral screening. We expect that this system will greatly facilitate future screens for anti-FIPV compounds and provide a non-infectious system to study and evaluate drug-resistant mutations that may emerge in the FIPV genome.IMPORTANCEFIPV is of great significance in the cat population around the world, causing 0.3%-1.4% of feline deaths in veterinary practices (2). As there are neither effective preventive measures nor approved treatment options available, there is an urgent need to identify antiviral drugs against FIPV. Our FCoV replicon system provides a valuable tool for drug discovery . Due to the lack of cell culture systems for serotype I FCoVs (the serotype most prevalent in the feline population) (2), a different system is needed to study these viruses. A viral replicon system is a valuable tool for studying FCoVs. Overall, our results demonstrate the utility of the serotype I feline coronavirus replicon system for antiviral screening as well as to study this virus in general. We propose several compounds representing promising candidates for future clinical trials and ultimately with the potential to save cats suffering from FIP.

摘要

猫传染性腹膜炎 (FIP) 是一种致命的猫科疾病,由猫冠状病毒 (FCoV) 引起,即猫传染性腹膜炎病毒 (FIPV)。我们生产了一株表达 I 型 FCoV 复制子 RNA 与绿色荧光蛋白 (GFP) 报告基因的幼仓鼠肾 21 细胞系(BHK-F-Rep),并将其用作筛选系统来测试不同的抗病毒化合物。两种 FCoV 主蛋白酶 (M) 的抑制剂,即 GC376 和 Nirmatrelvir,以及核苷类似物瑞德西韦,被证明能有效抑制复制子系统。这些化合物的不同组合也被证明是有效的抑制剂,联合使用时有相加作用。瑞德西韦、GC376 和 Nirmatrelvir 的细胞半数毒性浓度 (CC50) 均比其半最大抑制浓度 (IC50) 高 200 倍以上,这使它们成为未来研究以及临床实施药物候选物的重要候选物。此外,我们还使用全胎 4 (Fcwf-4) 细胞感染先前描述的表达 GFP 的重组 FIPV(基于实验室适应的 I 型 FIPV 株 Black)的病毒感染系统获得了结果,并使用最有前途的化合物进行了处理。复制子系统获得的结果与病毒感染系统获得的结果相当,表明我们成功地将 FCoV 复制子系统用于抗病毒筛选。我们预计该系统将极大地促进未来针对抗 FIPV 化合物的筛选,并提供一个非感染性系统来研究和评估可能在 FIPV 基因组中出现的耐药突变。重要性FIPV 在全世界的猫群中具有重要意义,导致兽医实践中 0.3%-1.4%的猫死亡(2)。由于既没有有效的预防措施也没有批准的治疗方法,因此迫切需要确定针对 FIPV 的抗病毒药物。我们的 FCoV 复制子系统为药物发现提供了有价值的工具。由于缺乏 I 型 FCoV(在猫群中最常见的血清型)的细胞培养系统(2),因此需要一种不同的系统来研究这些病毒。病毒复制子系统是研究 FCoV 的有价值的工具。总体而言,我们的结果证明了 I 型猫冠状病毒复制子系统在抗病毒筛选以及一般研究该病毒方面的实用性。我们提出了几种代表有前途的候选物的化合物,用于未来的临床试验,最终有可能拯救患有 FIP 的猫。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0249/10878086/24e479358f04/jvi.01216-23.f001.jpg

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