Author
Listed:
- Ningning Wang
(Nanjing Agricultural University)
- Weiwei Ji
(Nanjing Agricultural University)
- Houqi Jiao
(Nanjing Agricultural University
Nanjing Agricultural University)
- Michael Veit
(Free University Berlin)
- Ju Sun
(Chinese Academy of Sciences)
- Yanjun Wang
(Chinese Academy of Sciences)
- Xing Ma
(Nanjing Agricultural University)
- Yu Wang
(Nanjing Agricultural University)
- Yutong Wang
(Nanjing Agricultural University)
- Xin-xin Li
(Nanjing Agricultural University)
- Xiaoguang Zhang
(Nanjing Agricultural University)
- Jie Chen
(Nanjing Agricultural University)
- Jiayu Wei
(Nanjing Agricultural University)
- Ying Xu
(Nanjing Agricultural University)
- Dawei Guo
(Nanjing Agricultural University)
- Xiaofeng Zhai
(Nanjing Agricultural University)
- Andres Merits
(University of Tartu)
- Chang Li
(Chinese Academy of Agricultural Sciences)
- Félix A. Rey
(CNRS UMR 3569)
- Georgi M. Dobrikov
(Bulgarian Academy of Sciences)
- George F. Gao
(Chinese Academy of Sciences
University of Chinese Academy of Sciences
Zhejiang University)
- Shuijun Zhang
(Nanjing Agricultural University)
- Yuhai Bi
(Chinese Academy of Sciences
University of Chinese Academy of Sciences
Jinzhou Medical University
Early Warning and Pathogen Research on Emerging Infectious Diseases)
- Shuo Su
(Nanjing Agricultural University
Nanjing Agricultural University
Fudan University)
Abstract
Despite accumulating evidence that bat-derived coronaviruses often require intermediate hosts to facilitate transmission to humans1, the potential role of fur animals in zoonotic coronavirus spillovers has largely been overlooked2. Here we report the isolation and characterization of a previously undescribed mink respiratory coronavirus (MRCoV) from farmed minks with pneumonia. Notably, MRCoV uses angiotensin-converting enzyme 2 (ACE2) as an entry receptor and can infect mink, bat, monkey and human cells. Cryo-electron microscopy analyses revealed that the MRCoV receptor-binding domain (RBD) binds to the same interface on ACE2 receptors as the RBD of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) despite structural differences. We identify the key determinants on the RBD of MRCoV and ACE2 that confer efficient binding. HKU5-33S, a bat coronavirus closely related to MRCoV, uses ACE2 of the bat Pipistrellus abramus for cell entry and requires only two amino acid substitutions to adapt to mink ACE2. SARS-CoV-2 protease and polymerase inhibitors potently block MRCoV infection, thereby indicating a potential therapeutic strategy. Collectively, these findings enhance our understanding of coronavirus receptor dynamics and highlight their zoonotic potential. Given the risks posed by fur farms as reservoirs for emerging pathogens, our study underscores the need for enhanced surveillance to mitigate future coronavirus outbreaks.
Suggested Citation
Ningning Wang & Weiwei Ji & Houqi Jiao & Michael Veit & Ju Sun & Yanjun Wang & Xing Ma & Yu Wang & Yutong Wang & Xin-xin Li & Xiaoguang Zhang & Jie Chen & Jiayu Wei & Ying Xu & Dawei Guo & Xiaofeng Zh, 2025.
"A MERS-CoV-like mink coronavirus uses ACE2 as an entry receptor,"
Nature, Nature, vol. 642(8068), pages 739-746, June.
Handle:
RePEc:nat:nature:v:642:y:2025:i:8068:d:10.1038_s41586-025-09007-w
DOI: 10.1038/s41586-025-09007-w
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