Development of optimized drug-like small molecule inhibitors of the SARS-CoV-2 3CL protease for treatment of COVID-19

Nature communications, Apr 2022 | 13 (1), 1891

DOI: 10.1038/s41467-022-29413-2

Development of optimized drug-like small molecule inhibitors of the SARS-CoV-2 3CL protease for treatment of COVID-19

Liu, Hengrui ; Iketani, Sho ; Zask, Arie ; Khanizeman, Nisha ; Bednarova, Eva ; Forouhar, Farhad ; Fowler, Brandon ; Hong, Seo Jung ; Mohri, Hiroshi ; Nair, Manoj S ; Huang, Yaoxing ; Tay, Nicholas E S ; Lee, Sumin ; Karan, Charles ; Resnick, Samuel J ; Quinn, Colette ; Li, Wenjing ; Shion, Henry ; Xia, Xin ; Daniels, Jacob D ; Bartolo-Cruz, Michelle ; Farina, Marcelo ; Rajbhandari, Presha ; Jurtschenko, Christopher ; Lauber, Matthew A ; McDonald, Thomas ; Stokes, Michael E ; Hurst, Brett L ; Rovis, Tomislav ; Chavez, Alejandro ; Ho, David D ; Stockwell, Brent R

PRODUCTS USED

NGS

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ABSTRACT

The SARS-CoV-2 3CL protease is a critical drug target for small molecule COVID-19 therapy, given its likely druggability and essentiality in the viral maturation and replication cycle. Based on the conservation of 3CL protease substrate binding pockets across coronaviruses and using screening, we identified four structurally distinct lead compounds that inhibit SARS-CoV-2 3CL protease. After evaluation of their binding specificity, cellular antiviral potency, metabolic stability, and water solubility, we prioritized the GC376 scaffold as being optimal for optimization. We identified multiple drug-like compounds with

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PRODUCTS USED

NGS

Genes

Oligo Pools

NGS Target Enrichment Solutions

Variant Libraries

Synthetic Controls

Antibody Discovery