Molecular insights into receptor binding of recent emerging SARS-CoV-2 variants

被引:0
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作者
Pengcheng Han
Chao Su
Yanfang Zhang
Chongzhi Bai
Anqi Zheng
Chengpeng Qiao
Qing Wang
Sheng Niu
Qian Chen
Yuqin Zhang
Weiwei Li
Hanyi Liao
Jing Li
Zengyuan Zhang
Heecheol Cho
Mengsu Yang
Xiaoyu Rong
Yu Hu
Niu Huang
Jinghua Yan
Qihui Wang
Xin Zhao
George Fu Gao
Jianxun Qi
机构
[1] CAS Key Laboratory of Pathogenic Microbiology and Immunology,Department of Biomedical Engineering
[2] Institute of Microbiology,College of Life Science and Technology
[3] Chinese Academy of Sciences,Department of Biomedical Sciences
[4] Emory University,College of Veterinary Medicine
[5] Southeast University,Institutes of Physical Science and Information Technology
[6] City University of Hong Kong,School of Laboratory Medicine and Life Science
[7] Laboratory of Protein Engineering and Vaccines,School of Life Sciences, Division of Life Sciences and Medicine
[8] Tianjin Institute of Industrial Biotechnology,Tsinghua Institute of Multidisciplinary Biomedical Research
[9] Chinese Academy of Sciences,undefined
[10] Shanxi Academy of Advanced Research and Innovation,undefined
[11] Central Laboratory,undefined
[12] Shanxi Province Hospital of Traditional Chinese Medicine,undefined
[13] University of the Chinese Academy of Sciences,undefined
[14] National Institute of Biological Sciences,undefined
[15] Shanxi Agricultural University,undefined
[16] Anhui University,undefined
[17] Wenzhou Medical University,undefined
[18] University of Science and Technology of China,undefined
[19] Tsinghua University,undefined
[20] CAS Key Laboratory of Microbial Physiological and Metabolic Engineering,undefined
[21] Institute of Microbiology,undefined
[22] Chinese Academy of Sciences,undefined
[23] CAS Center for Influenza Research and Early-Warning (CASCIRE),undefined
[24] Chinese Academy of Sciences,undefined
来源
Nature Communications | / 12卷
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摘要
Multiple SARS-CoV-2 variants of concern (VOCs) have been emerging and some have been linked to an increase in case numbers globally. However, there is yet a lack of understanding of the molecular basis for the interactions between the human ACE2 (hACE2) receptor and these VOCs. Here we examined several VOCs including Alpha, Beta, and Gamma, and demonstrate that five variants receptor-binding domain (RBD) increased binding affinity for hACE2, and four variants pseudoviruses increased entry into susceptible cells. Crystal structures of hACE2-RBD complexes help identify the key residues facilitating changes in hACE2 binding affinity. Additionally, soluble hACE2 protein efficiently prevent most of the variants pseudoviruses. Our findings provide important molecular information and may help the development of novel therapeutic and prophylactic agents targeting these emerging mutants.
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