Human respiratory organoids sustained reproducible propagation of human rhinovirus C and elucidation of virus-host interaction

人类呼吸道类器官能够持续、可重复地扩增人鼻病毒C,并阐明病毒与宿主的相互作用。

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作者:Cun Li #,Yifei Yu #,Zhixin Wan,Man Chun Chiu,Jingjing Huang,Shuxin Zhang,Xiaoxin Zhu,Qiaoshuai Lan,Yanlin Deng,Ying Zhou,Wei Xue,Ming Yue,Jian-Piao Cai,Cyril Chik-Yan Yip,Kenneth Kak-Yuen Wong,Xiaojuan Liu,Yang Yu,Lin Huang,Hin Chu,Jasper Fuk-Woo Chan,Hans Clevers,Kwok Yung Yuen,Jie Zhou

Abstract

The lack of a robust system to reproducibly propagate HRV-C, a family of viruses refractory to cultivation in standard cell lines, has substantially hindered our understanding of this common respiratory pathogen. We sought to develop an organoid-based system to reproducibly propagate HRV-C, and characterize virus-host interaction using respiratory organoids. We demonstrate that airway organoids sustain serial virus passage with the aid of CYT387-mediated immunosuppression, whereas nasal organoids that more closely simulate the upper airway achieve this without any intervention. Nasal organoids are more susceptible to HRV-C than airway organoids. Intriguingly, upon HRV-C infection, we observe an innate immune response that is stronger in airway organoids than in nasal organoids, which is reproduced in a Poly(I:C) stimulation assay. Treatment with α-CDHR3 and antivirals significantly reduces HRV-C viral growth in airway and nasal organoids. Additionally, an organoid-based immunofluorescence assay is established to titrate HRV-C infectious particles. Collectively, we develop an organoid-based system to reproducibly propagate the poorly cultivable HRV-C, followed by a comprehensive characterization of HRV-C infection and innate immunity in physiologically active respiratory organoids. The organoid-based HRV-C infection model can be extended for developing antiviral strategies. More importantly, our study has opened an avenue for propagating and studying other uncultivable human and animal viruses.

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