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1.
SARS-CoV-2 hijacks neutralizing dimeric IgA for enhanced nasal infection and injury (preprint)
Biao Zhou; Runhong Zhou; Jasper Fuk-Woo Chan; Jianwei Zeng; Qi Zhang; Shuofeng Yuan; Li Liu; Rémy Robinot; Sisi Shan; Jiwan Ge; Hugo Yat-Hei Kwong; Dongyan Zhou; Haoran Xu; Chris Chung-Sing Chan; Vincent Kwok-Man Poon; Hin Chu; Ming Yue; Ka-Yi Kwan; Chun-Yin Chan; Na Liu; Chris Chun-Yiu Chan; Kenn Ka-Heng Chik; Zhenglong Du; Ka-Kit Au; Haode Huang; Hiu-On Man; Jianli Cao; Cun Li; Ziyi Wang; Jie Zhou; Youqiang Song; Man-Lung Yeung; Kelvin Kai-Wang To; David D. Ho; Lisa A. Chakrabarti; Xinquan Wang; Linqi Zhang; Kwok-Yung Yuen; Zhiwei Chen.
biorxiv; 2021.
Preprint in English | bioRxiv | ID: ppzbmed-10.1101.2021.10.05.463282

ABSTRACT

Robust severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) infection in nasal turbinate (NT) accounts for high viral transmissibility, yet whether neutralizing IgA antibodies can control it remains unknown. Here, we evaluated receptor binding domain (RBD)-specific monomeric B8-mIgA1 and B8-mIgA2, and dimeric B8-dIgA1 and B8-dIgA2 against intranasal SARS-CoV-2 challenge in Syrian hamsters. These antibodies exhibited comparably potent neutralization against authentic virus by competing with human angiotensin converting enzyme-2 (ACE2) receptor for RBD binding. While reducing viruses in lungs, pre-exposure intranasal B8-dIgA1 or B8-dIgA2 led to 81-fold more infectious viruses and severer damage in NT than placebo. Virus-bound B8-dIgA1 and B8-dIgA2 could engage CD209 as an alternative receptor for entry into ACE2-negative cells and allowed viral cell-to-cell transmission. Cryo-EM revealed B8 as a class II neutralizing antibody binding trimeric RBDs in 3-up or 2-up/1-down conformation. Therefore, RBD-specific neutralizing dIgA engages an unexpected action for enhanced SARS-CoV-2 nasal infection and injury in Syrian hamsters.


Subject(s)
Severe Acute Respiratory Syndrome
2.
SARS-CoV-2 hijacks neutralizing dimeric IgA for enhanced nasal infection and injury (preprint)
Biao Zhou; Runhong Zhou; Jasper Fuk-Woo Chan; Jianwei Zeng; Qi Zhang; Shuofeng Yuan; Li Liu; Rémy Robinot; Sisi Shan; Jiwan Ge; Hugo Yat-Hei Kwong; Dongyan Zhou; Haoran Xu; Chris Chan; Vincent Poon; Hin Chu; Ming Yue; Ka-Yi Kwan; Chun Yin Chan; Na Liu; Chris Chun-Yiu Chan; Kenn Ka-Heng Chik; Zhenglong Du; Ka-Kit Au; Haode Huang; Hiu-On Man; Jianli Cao; Cun Li; Ziyi Wang; Jie Zhou; Youqiang Song; Man Lung Yeung; Kelvin To; David Ho; Lisa Chakrabarti; Xinquan Wang; Linqi Zhang; Kwok-Yung Yuen; Zhiwei Chen.
researchsquare; 2021.
Preprint in English | PREPRINT-RESEARCHSQUARE | ID: ppzbmed-10.21203.rs.3.rs-923755.v1

ABSTRACT

Robust severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) infection in nasal turbinate (NT) accounts for high viral transmissibility, yet whether neutralizing IgA antibodies can control it remains unknown. Here, we evaluated receptor binding domain (RBD)-specific monomeric B8-mIgA1 and B8-mIgA2, and dimeric B8-dIgA1 and B8-dIgA2 against intranasal SARS-CoV-2 challenge in Syrian hamsters. These antibodies exhibited comparably potent neutralization against authentic virus by competing with human angiotensin converting enzyme-2 (ACE2) receptor for RBD binding. While reducing viruses in lungs, pre-exposure intranasal B8-dIgA1 or B8-dIgA2 led to 81-fold more infectious viruses and severer damage in NT than placebo. Virus-bound B8-dIgA1 and B8-dIgA2 could engage CD209 as an alternative receptor for entry into ACE2-negative cells and allowed viral cell-to-cell transmission. Cryo-EM revealed B8 as a class II neutralizing antibody binding trimeric RBDs in 3-up or 2-up/1-down conformation. Therefore, RBD-specific neutralizing dIgA engages an unexpected action for enhanced SARS-CoV-2 nasal infection and injury in Syrian hamsters.


Subject(s)
Severe Acute Respiratory Syndrome
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