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长期扩增的猪气道类器官为研究猪呼吸冠状病毒感染的发病机制和先天免疫提供了线索。

Long-Term Expanding Porcine Airway Organoids Provide Insights into the Pathogenesis and Innate Immunity of Porcine Respiratory Coronavirus Infection.

机构信息

State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institutegrid.38587.31, Chinese Academy of Agricultural Sciences, Harbin, China.

Key Laboratory of Animal Epidemiology of the Ministry of Agriculture and Rural Affairs, College of Veterinary Medicine, China Agricultural Universitygrid.22935.3f, Beijing, China.

出版信息

J Virol. 2022 Jul 27;96(14):e0073822. doi: 10.1128/jvi.00738-22. Epub 2022 Jun 28.

Abstract

Respiratory coronaviruses cause serious health threats to humans and animals. Porcine respiratory coronavirus (PRCoV), a natural transmissible gastroenteritis virus (TGEV) mutant with partial spike deletion, causes mild respiratory disease and is an interesting animal respiratory coronavirus model for human respiratory coronaviruses. However, the absence of robust models of porcine airway epithelium hinders an understanding of the pathogenesis of PRCoV infection. Here, we generated long-term porcine airway organoids (AOs) derived from basal epithelial cells, which recapitulate the airway complicated epithelial cellularity. Both 3D and 2D AOs are permissive for PRCoV infection. Unlike TGEV, which established successful infection in both AOs and intestinal organoids, PRCoV was strongly amplified only in AOs, not intestinal organoids. Furthermore, PRCoV infection in AOs mounted vigorous early type I and III interferon (IFN) responses and upregulated the expression of overzealous inflammatory genes, including pattern recognition receptors (PRRs) and proinflammatory cytokines. Collectively, these data demonstrate that stem-derived porcine AOs can serve as a promising disease model for PRCoV infection and provide a valuable tool to study porcine respiratory infection. Porcine respiratory CoV (PRCoV), a natural mutant of TGEV, shows striking pathogenetic similarities to human respiratory CoV infection and provides an interesting animal model for human respiratory CoVs, including SARS-CoV-2. The lack of an model recapitulating the complicated cellularity and structure of the porcine respiratory tract is a major roadblock for the study of PRCoV infection. Here, we developed long-term 3D airway organoids (AOs) and further established 2D AO monolayer cultures. The resultant 3D and 2D AOs are permissive for PRCoV infection. Notably, PRCoV mediated pronounced IFN and inflammatory responses in AOs, which recapitulated the inflammatory responses associated with PRCoV infection. Therefore, porcine AOs can be utilized to characterize the pathogenesis of PRCoV and, more broadly, can serve as a universal platform for porcine respiratory infection.

摘要

呼吸道冠状病毒对人类和动物的健康构成严重威胁。猪呼吸冠状病毒(PRCoV)是一种天然传染性胃肠炎病毒(TGEV)的突变株,具有部分刺突缺失,引起轻微的呼吸道疾病,是研究人类呼吸道冠状病毒的有趣动物呼吸道冠状病毒模型。然而,缺乏强健的猪呼吸道上皮模型阻碍了对 PRCoV 感染发病机制的理解。在这里,我们从基底上皮细胞中生成了长期的猪呼吸道类器官(AOs),这些类器官重现了呼吸道复杂的上皮细胞组成。3D 和 2D AOs 均允许 PRCoV 感染。与在 AOs 和肠道类器官中均能成功建立感染的 TGEV 不同,PRCoV 仅在 AOs 中强烈扩增,而不在肠道类器官中扩增。此外,PRCoV 在 AOs 中的感染引发了强烈的早期 I 型和 III 型干扰素(IFN)反应,并上调了过度活跃的炎症基因的表达,包括模式识别受体(PRRs)和促炎细胞因子。总之,这些数据表明,源自干细胞的猪 AOs 可作为 PRCoV 感染的有前途的疾病模型,并为研究猪呼吸道感染提供了有价值的工具。猪呼吸冠状病毒(PRCoV)是 TGEV 的天然突变株,与人类呼吸道冠状病毒感染具有显著的相似的发病机制,为包括 SARS-CoV-2 在内的人类呼吸道冠状病毒提供了一个有趣的动物模型。缺乏一种能够重现猪呼吸道复杂细胞组成和结构的模型是研究 PRCoV 感染的主要障碍。在这里,我们开发了长期的 3D 气道类器官(AOs),并进一步建立了 2D AO 单层培养物。由此产生的 3D 和 2D AOs 允许 PRCoV 感染。值得注意的是,PRCoV 在 AOs 中介导了明显的 IFN 和炎症反应,重现了与 PRCoV 感染相关的炎症反应。因此,猪 AOs 可用于表征 PRCoV 的发病机制,更广泛地说,可作为猪呼吸道感染的通用平台。

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