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Published May 7, 2021 | Supplemental Material + Submitted + Published
Journal Article Open

X-ray screening identifies active site and allosteric inhibitors of SARS-CoV-2 main protease

Günther, Sebastian ORCID icon
Reinke, Patrick Y. A. ORCID icon
Fernández-García, Yaiza ORCID icon
Lieske, Julia
Lane, Thomas J.
Ginn, Helen M. ORCID icon
Koua, Faisal H. M. ORCID icon
Ehrt, Christiane ORCID icon
Ewert, Wiebke
Oberthuer, Dominik
Yefanov, Oleksandr ORCID icon
Meier, Susanne
Lorenzen, Kristina
Krichel, Boris
Kopicki, Janine-Denise ORCID icon
Gelisio, Luca ORCID icon
Brehm, Wolfgang
Dunkel, Ilona
Seychell, Brandon
Gieseler, Henry
Norton-Baker, Brenna
Escudero-Pérez, Beatriz ORCID icon
Domaracky, Martin ORCID icon
Saouane, Sofiane ORCID icon
Tolstikova, Aleksandra ORCID icon
White, Thomas A.
Hänle, Anna
Groessler, Michael
Fleckenstein, Holger ORCID icon
Trost, Fabian ORCID icon
Galchenkova, Marina
Gevorkov, Yaroslav ORCID icon
Li, Chufeng ORCID icon
Awel, Salah ORCID icon
Peck, Ariana ORCID icon
Barthelmess, Miriam ORCID icon
Schlünzen, Frank
Lourdu Xavier, Paulraj ORCID icon
Werner, Nadine
Andaleeb, Hina
Ullah, Najeeb
Falke, Sven ORCID icon
Srinivasan, Vasundara ORCID icon
Alves França, Bruno ORCID icon
Schwinzer, Martin
Brognaro, Hévila
Rogers, Cromarte
Melo, Diogo
Zaitsev-Doyle, Joanna J.
Knoska, Juraj ORCID icon
Peña-Murillo, Gisel E. ORCID icon
Rahmani Mashhour, Aida
Hennicke, Vincent ORCID icon
Fischer, Pontus ORCID icon
Hakanpää, Johanna
Meyer, Jan ORCID icon
Gribbon, Philip ORCID icon
Ellinger, Bernhard ORCID icon
Kuzikov, Maria
Wolf, Markus
Beccari, Andrea R.
Borenkov, Gleb
von Stetten, David ORCID icon
Pompidor, Guillaume
Bento, Isabel ORCID icon
Panneerselvam, Saravanan
Karpics, Ivars
Schneider, Thomas R.
Garcia-Alai, Maria Marta
Niebling, Stephan ORCID icon
Günther, Christian
Schmidt, Christina
Schubert, Robin ORCID icon
Han, Huijong ORCID icon
Boger, Juliane
Monteiro, Diana C. F. ORCID icon
Zhang, Linlin
Sun, Xinyuanyuan
Pletzer-Zelgert, Jonathan
Wollenhaupt, Jan ORCID icon
Feiler, Christian G. ORCID icon
Weiss, Manfred S. ORCID icon
Schulz, Eike-Christian
Mehrabi, Pedram
Karničar, Katarina
Usenik, Aleksandra ORCID icon
Loboda, Jure ORCID icon
Tidow, Henning ORCID icon
Chari, Ashwin ORCID icon
Hilgenfeld, Rolf ORCID icon
Uetrecht, Charlotte ORCID icon
Cox, Russell ORCID icon
Zaliani, Andrea ORCID icon
Beck, Tobias
Rarey, Matthias ORCID icon
Günther, Stephan ORCID icon
Turk, Dusan ORCID icon
Hinrichs, Winfried ORCID icon
Chapman, Henry N. ORCID icon
Pearson, Arwen R. ORCID icon
Betzel, Christian ORCID icon
Meents, Alke ORCID icon

Abstract

The coronavirus disease (COVID-19) caused by SARS-CoV-2 is creating tremendous human suffering. To date, no effective drug is available to directly treat the disease. In a search for a drug against COVID-19, we have performed a high-throughput X-ray crystallographic screen of two repurposing drug libraries against the SARS-CoV-2 main protease (M^(pro)), which is essential for viral replication. 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 that bind to M^(pro). In subsequent cell-based viral reduction assays, one peptidomimetic and six 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.

Additional Information

© 2021 American Association for the Advancement of Science. Received 20 November 2020; accepted 29 March 2021; Published online April 2, 2021. We acknowledge Deutsches Elektronen-Synchrotron (DESY, Hamburg, Germany), a member of the Helmholtz Association HGF, for the provision of experimental facilities. Parts of this research were carried out at PETRA III at beamline P11. Further MX data were collected at beamline P13 and P14 operated by EMBL. We thank the DESY machine group, in particular Mario Wunderlich, Kim Heuck, Arne Brinkmann, Olaf Goldbeck, Jürgen Haar, Torsten Schulz, Gunnar Priebe, Maximilian Holz, Björn Lemcke, Klaus Knaack, Oliver Seebauer, Philipp Willanzheimer, Rolf Jonas, and Nicole Engling. We thank Thomas Dietrich, Simon Geile, Filip Guicking, Heshmat Noei, and Tim Pakendorf from DESY, and Bianca Di Fabrizio and Sebastian Kühn from BNITM for assistance. This research was supported in part through the Maxwell computational resources operated at DESY. We acknowledge the use of the XBI biological sample preparation laboratory at European XFEL, enabled by the XBI User Consortium. We acknowledge financial support from the EXSCALATE4CoV EU-H2020 Emergency Project (101003551), the Cluster of Excellence "Advanced Imaging of Matter" of the Deutsche Forschungsgemeinschaft (DFG) - EXC 2056 - project ID 390715994, the Helmholtz Association Impulse and Networking funds (projects ExNet-0002 and InternLabs-0011 "HIR3X"), the Federal Ministry of Education and Research (BMBF) via projects 05K16GUA, 05K19GU4, 05K20BI1, 05K20FL1, 16GW0277 and 031B0405D), and the Joachim-Herz-Stiftung Hamburg (project Infecto-Physics). CE and MR acknowledge financial support from grant-No. HIDSS-0002 DASHH (Data Science in Hamburg - HELMHOLTZ Graduate School for the Structure of Matter). RC is supported by DFG grants INST 187/621-1 and INST 187/686-1. DT is supported by the Slovenian Research Agency (ARRS; research program P1-0048, Infrastructural program IO-0048). BS was supported by an Exploration Grant from the Boehringer Ingelheim Foundation. The Heinrich Pette Institute, Leibniz Institute for Experimental Virology was supported by the Free and Hanseatic City of Hamburg and the Federal Ministry of Health. CU and BK were supported by EU Horizon 2020 ERC StG-2017 759661, BMBF RTK Struktur 01KI20391, BMBF Visavix 05K16BH1 and the Leibniz Association SAW-2014-HPI-4 grant. Author Contributions: SeG, PR, YFG, WB, PG, ARB, RC, DT, AZ, HNC, ARP, CB, AM designed research. SeG, PR, TJL, WH, HNC, ARP, CB, AM wrote manuscript. SeG, PR, JL, FHMK, SM, WB, ID, BS, HGie, BNB, MB, PLX, NW, HA, NU, SF, BAF, MS, HB, JK, GEPM, ARM, FG, VH, PF, MW, ECS, PM, HT, TB participated in sample preparation. PR performed crystallization experiments. SeG, PR, JL, TJL, OY, SS, AT, MGr, HF, FT, MGa, YG, CFL, SA, AP, GB, DVS, GP, TRS, IB, SP performed X-ray data collection. TJL, HGin, DO, OY, LG, MD, TAW, FS, CR, DM, JZD, IK, CS, RS, HUH, DCFM contributed to X-ray data management. SeG, PR, JL, TJL, HGin, FHMK, WE, DO, AH, VS, JH, JM, JB, JW, CF, MSW, AC, DT, WH, AM performed X-ray data analysis. KL, BK, CU, RC performed and analyzed MS experiments. YFG, BEP, StG performed and analyzed antiviral activity assays. PG, BE, MK, MGA, SN, CG, LZ, XS, KK, AU, JL, RH performed and analyzed ligand binding studies and protein activity assays. CE, JPZ, MR performed computational binding studies. Competing Interests: MR is stakeholder of BioSolveIT GmbH, licensor of the software HYDE. Data and materials availability: The coordinates and structure factors for all described crystal structures of SARS-CoV-2 Mpro in complex with compounds are deposited in the PDB with accession codes 6YNQ, 6YVF, 7A1U, 7ABU, 7ADW, 7AF0, 7AGA, 7AHA, 7AK4, 7AKU, 7AMJ, 7ANS, 7AOL, 7AP6, 7APH, 7AQE, 7AQI, 7AQJ, 7AR5, 7AR6, 7ARF, 7AVD, 7AWR, 7AWS, 7AWU, 7AWW, 7AX6, 7AXM, 7AXO, 7AY7, 7B83 and 7NEV. Code used in this analysis has been previously published (10). The code for forcing adherence to the Wilson distribution is included in the Vagabond refinement package (https://vagabond.hginn.co.uk/) under a GPLv3 license. Compounds from the Fraunhofer IME Repurposing collection were obtained from the Fraunhofer Institute for Molecular Biology and Applied Ecology under a Material Transfer Agreement. Compounds from the Safe-in-man Library were kindly provided by Dompé Farmaceutici S.p.A. Other materials are available from SeG or AM upon request. This work is licensed under a Creative Commons Attribution 4.0 International (CC BY 4.0) license, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. To view a copy of this license, visit https://creativecommons.org/licenses/by/4.0/. This license does not apply to figures/photos/artwork or other content included in the article that is credited to a third party; obtain authorization from the rights holder before using such material.

Attached Files

Published - 642.full.pdf

Submitted - 2020.11.12.378422v2.full.pdf

Supplemental Material - abf7945-Guenther-SM.pdf

Supplemental Material - abf7945_Guenther_Reproducibility-Checklist.pdf

Supplemental Material - abf7945_Guenther_Table-S1.xlsx

Supplemental Material - abf7945_Guenther_Table-S3.pdf

Supplemental Material - abf7945_Guenther_Table-S4.xlsx

Supplemental Material - abf7945_Guenther_Table-S7.xlsx

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