Inhibition of SARS-CoV-2 main protease by allosteric drug-binding
Author:
Günther SebastianORCID, Reinke Patrick Y. A.ORCID, Fernández-García YaizaORCID, Lieske Julia, Lane Thomas J., Ginn Helen M., Koua Faisal H. M., Ehrt Christiane, Ewert Wiebke, Oberthuer Dominik, Yefanov Oleksandr, Meier Susanne, Lorenzen Kristina, Krichel Boris, Kopicki Janine-DeniseORCID, Gelisio Luca, Brehm Wolfgang, Dunkel Ilona, Seychell Brandon, Gieseler Henry, Norton-Baker Brenna, Escudero-Pérez Beatriz, Domaracky Martin, Saouane Sofiane, Tolstikova Alexandra, White Thomas A., Hänle Anna, Groessler Michael, Fleckenstein Holger, Trost Fabian, Galchenkova Marina, Gevorkov Yaroslav, Li Chufeng, Awel Salah, Peck Ariana, Barthelmess Miriam, Schlünzen Frank, Xavier P. Lourdu, Werner Nadine, Andaleeb Hina, Ullah Najeeb, Falke Sven, Srinivasan Vasundara, Franca Bruno Alves, Schwinzer Martin, Brognaro Hévila, Rogers Cromarte, Melo Diogo, Zaitsev-Doyle Jo J., Knoska Juraj, Peña Murillo Gisel E., Mashhour Aida Rahmani, Guicking Filip, Hennicke Vincent, Fischer Pontus, Hakanpää Johanna, Meyer Jan, Gribbon Phil, Ellinger Bernhard, Kuzikov Maria, Wolf Markus, Beccari Andrea R., Bourenkov Gleb, Stetten David von, Pompidor Guillaume, Bento Isabel, Panneerselvam Saravanan, Karpics Ivars, Schneider Thomas R., Garcia Alai Maria Marta, Niebling Stephan, Günther Christian, Schmidt Christina, Schubert Robin, Han Huijong, Boger Juliane, Monteiro Diana C. F., Zhang Linlin, Sun Xinyuanyuan, Pletzer-Zelgert Jonathan, Wollenhaupt Jan, Feiler Christian G., Weiss Manfred S., Schulz Eike-Christian, Mehrabi Pedram, Karničar Katarina, Usenik Aleksandra, Loboda Jure, Tidow Henning, Chari Ashwin, Hilgenfeld RolfORCID, Uetrecht CharlotteORCID, Cox Russell, Zaliani Andrea, Beck Tobias, Rarey Matthias, Günther Stephan, Turk DusanORCID, Hinrichs WinfriedORCID, Chapman Henry N., Pearson Arwen R., Betzel Christian, Meents AlkeORCID
Abstract
AbstractThe coronavirus disease (COVID-19) caused by SARS-CoV-2 is creating tremendous health problems and economical challenges for mankind. To date, no effective drug is available to directly treat the disease and prevent virus spreading. In a search for a drug against COVID-19, we have performed a massive X-ray crystallographic screen of two repurposing drug libraries against the SARS-CoV-2 main protease (Mpro), which is essential for the virus replication and, thus, a potent drug target. In contrast to commonly applied X-ray fragment screening experiments with molecules of low complexity, our screen tested already approved drugs and drugs in clinical trials. From the three-dimensional protein structures, we identified 37 compounds binding to Mpro. In subsequent cell-based viral reduction assays, one peptidomimetic and five non-peptidic compounds showed antiviral activity at non-toxic concentrations. We identified two allosteric binding sites representing attractive targets for drug development against SARS-CoV-2.
Publisher
Cold Spring Harbor Laboratory
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