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A pan-coronavirus fusion inhibitor targeting the HR1 domain of human coronavirus spike
Author(s) -
Shuai Xia,
Lei Yan,
Wei Xu,
Anurodh Shankar Agrawal,
Abdullah Algaissi,
ChienTe K. Tseng,
Qian Wang,
Lanying Du,
Wenjie Tan,
Ian A. Wilson,
Shibo Jiang,
Bei Yang,
Lu Lu
Publication year - 2019
Publication title -
science advances
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.928
H-Index - 146
ISSN - 2375-2548
DOI - 10.1126/sciadv.aav4580
Subject(s) - coronavirus , virology , covid-19 , spike (software development) , fusion , coronavirus infections , severe acute respiratory syndrome coronavirus , spike protein , computational biology , biology , medicine , computer science , infectious disease (medical specialty) , outbreak , disease , software engineering , pathology , linguistics , philosophy
Continuously emerging highly pathogenic human coronaviruses (HCoVs) remain a major threat to human health, as illustrated in past SARS-CoV and MERS-CoV outbreaks. The development of a drug with broad-spectrum HCoV inhibitory activity would address this urgent unmet medical need. Although previous studies have suggested that the HR1 of HCoV spike (S) protein is an important target site for inhibition against specific HCoVs, whether this conserved region could serve as a target for the development of broad-spectrum pan-CoV inhibitor remains controversial. Here, we found that peptide OC43-HR2P, derived from the HR2 domain of HCoV-OC43, exhibited broad fusion inhibitory activity against multiple HCoVs. EK1, the optimized form of OC43-HR2P, showed substantially improved pan-CoV fusion inhibitory activity and pharmaceutical properties. Crystal structures indicated that EK1 can form a stable six-helix bundle structure with both short α-HCoV and long β-HCoV HR1s, further supporting the role of HR1 region as a viable pan-CoV target site.

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