Author
Listed:
- Manon Laporte
(KU Leuven)
- Dirk Jochmans
(KU Leuven)
- Dorothée Bardiot
(CISTIM Leuven vzw)
- Lowiese Desmarets
(Université de Lille)
- Oliver J. Debski-Antoniak
(Utrecht University)
- Giulia Mizzon
(University of Heidelberg
Heidelberg Partner Site)
- Rana Abdelnabi
(KU Leuven
KU Leuven)
- Pieter Leyssen
(KU Leuven)
- Winston Chiu
(KU Leuven)
- Zhikuan Zhang
(University of Tokyo)
- Norimichi Nomura
(Kyoto University)
- Sandro Boland
(CISTIM Leuven vzw)
- Umeharu Ohto
(University of Tokyo)
- Yannick Stahl
(University of Heidelberg)
- Jurgen Wuyts
(CISTIM Leuven vzw)
- Steven Jonghe
(KU Leuven)
- Annelies Stevaert
(KU Leuven)
- Martijn J. Hemert
(Leiden University Medical Center)
- Brenda W. Bontes
(Leiden University Medical Center)
- Patrick Wanningen
(Leiden University Medical Center)
- G. J. Mirjam Groenewold
(Leiden University Medical Center)
- Aneta Zegar
(Jagiellonian University)
- Katarzyna Owczarek
(Jagiellonian University)
- Sanjata Joshi
(University of Lübeck)
- Mohamed Koukni
(CISTIM Leuven vzw)
- Philippe Arzel
(CISTIM Leuven vzw)
- Hugo Klaassen
(CISTIM Leuven vzw)
- Jean-Christophe Vanherck
(CISTIM Leuven vzw)
- Ilse Vandecaetsbeek
(CISTIM Leuven vzw)
- Niels Cremers
(KU Leuven)
- Kim Donckers
(KU Leuven)
- Thibault Francken
(KU Leuven)
- Tina Buyten
(KU Leuven)
- Jasper Rymenants
(KU Leuven)
- Joost Schepers
(KU Leuven)
- Krzysztof Pyrc
(Jagiellonian University)
- Rolf Hilgenfeld
(University of Lübeck)
- Jean Dubuisson
(Université de Lille)
- Berend-Jan Bosch
(Utrecht University)
- Frank Kuppeveld
(Utrecht University)
- Cecilia Eydoux
(Aix-Marseille Univ., CNRS, Faculté des Sciences Campus Luminy)
- Etienne Decroly
(Aix-Marseille Univ., CNRS, Faculté des Sciences Campus Luminy)
- Bruno Canard
(Aix-Marseille Univ., CNRS, Faculté des Sciences Campus Luminy)
- Lieve Naesens
(KU Leuven)
- Birgit Weynand
(KU Leuven)
- Eric J. Snijder
(Leiden University Medical Center)
- Sandrine Belouzard
(Université de Lille)
- Toshiyuki Shimizu
(University of Tokyo)
- Ralf Bartenschlager
(University of Heidelberg
Heidelberg Partner Site
German Cancer Research Center (DKFZ))
- Daniel L. Hurdiss
(Utrecht University)
- Arnaud Marchand
(CISTIM Leuven vzw)
- Patrick Chaltin
(CISTIM Leuven vzw
KU Leuven)
- Johan Neyts
(KU Leuven)
Abstract
The coronavirus membrane protein (M) is the main organizer of coronavirus assembly1–3. Here, we report on an M-targeting molecule, CIM-834, that blocks the assembly of SARS-CoV-2. CIM-834 was obtained through high-throughput phenotypic antiviral screening followed by medicinal-chemistry efforts and target elucidation. CIM-834 inhibits the replication of SARS-CoV-2 (including a broad panel of variants) and SARS-CoV. In SCID mice and Syrian hamsters intranasally infected with SARS-CoV-2, oral treatment reduced lung viral titres to nearly undetectable levels, even (as shown in mice) when treatment was delayed until 24 h before the end point. Treatment of infected hamsters prevented transmission to untreated sentinels. Transmission electron microscopy studies show that virion assembly is completely absent in cells treated with CIM-834. Single-particle cryo-electron microscopy reveals that CIM-834 binds and stabilizes the M protein in its short form, thereby preventing the conformational switch to the long form, which is required for successful particle assembly. In conclusion, we have discovered a new druggable target in the replication cycle of coronaviruses and a small molecule that potently inhibits it.
Suggested Citation
Manon Laporte & Dirk Jochmans & Dorothée Bardiot & Lowiese Desmarets & Oliver J. Debski-Antoniak & Giulia Mizzon & Rana Abdelnabi & Pieter Leyssen & Winston Chiu & Zhikuan Zhang & Norimichi Nomura & S, 2025.
"A coronavirus assembly inhibitor that targets the viral membrane protein,"
Nature, Nature, vol. 640(8058), pages 514-523, April.
Handle:
RePEc:nat:nature:v:640:y:2025:i:8058:d:10.1038_s41586-025-08773-x
DOI: 10.1038/s41586-025-08773-x
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