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Rapid discovery of repurposed drugs targeting SARS-CoV-2 spike HR1 by DNA-encoded library screening

Bioorganic Chemistry. 2026-02; 
Qingao Xue, Ze Liang, Yi Zhang, Fei Wang, Fulian Wang, Lili Liu, Guang Yang, Lei Yan
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Peptide Synthesis The peptide corresponding to the HR1 domain (residues 924–955) of the SARS-CoV-2 spike protein, with an N-terminal biotin tag, was custom-synthesized by GenScript (Nanjing, China) using standard solid phase Fmoc chemistry. Get A Quote

Abstract

The membrane fusion process mediated by the SARS-CoV-2 spike protein is a key therapeutic target. Its heptad repeat 1 (HR1) domain forms a conserved trimeric groove critical for forming the fusion-competent six-helix bundle with HR2. We used DNA-encoded library screening to identify small molecules binding HR1. Hits including Rabeprazole-related compound E (Rab RCE), Omeprazole, Alvimopan, and Olmesartan were characterized. Biophysical assays confirmed binding, while computational simulations revealed distinct interaction modes, with Alvimopan showing high predicted affinity. Cell-cell fusion assays demonstrated potent inhibitory activity for Olmesartan and Rab RCE. Notably, Rabeprazole and Rab RCE showed parti... More

Keywords

COVID-19; DNA-encoded library (DEL); HR1 domain; SARS-CoV-2; Small molecule; Spike protein; Viral entry inhibitor