par Pasquereau, Sébastien;Galais, Mathilde 
;Bellefroid, Maxime ;Pachón Angona, Irene;Morot-Bizot, Stéphanie;Ismaili, Lhassane;Van Lint, Carine ;Herbein, Georges
Référence Scientific reports, 12, 1, page (20309)
Publication Publié, 2022-11-01
;Bellefroid, Maxime ;Pachón Angona, Irene;Morot-Bizot, Stéphanie;Ismaili, Lhassane;Van Lint, Carine ;Herbein, GeorgesRéférence Scientific reports, 12, 1, page (20309)
Publication Publié, 2022-11-01
Article révisé par les pairs
| Résumé : | A novel coronavirus, SARS-CoV-2, emerged in China at the end of 2019 causing a large global outbreak. As treatments are of the utmost importance, drugs with broad anti-coronavirus activity embody a rich and rapid drug discovery landscape, where candidate drug compounds could be identified and optimized. To this end, we tested ten small-molecules with chemical structures close to ferulic acid derivatives (FADs) (n = 8), caffeic acid derivatives (CAFDs) (n = 1) and carboxamide derivatives (CAMDs) (n = 1) for their ability to reduce HCoV-229E replication, another member of the coronavirus family. Among these ten drugs tested, five of them namely MBA112, MBA33, MBA27-1, OS4-1 and MBA108-1 were highly cytotoxic and did not warrant further testing. In contrast, we observed a moderate cytotoxicity for two of them, MBA152 and 5c. Three drugs, namely MBA140, LIJ2P40, and MBA28 showed lower cytotoxicity. These candidates were then tested for their antiviral propreties against HCoV-229E and SARS-CoV2 replication. We first observed encouraging results in HCoV-229E. We then measured a reduction of the viral SARS-CoV2 replication by 46% with MBA28 (EC50 > 200 µM), by 58% with MBA140 (EC50 = 176 µM), and by 82% with LIJ2P40 (EC50 = 66.5 µM). Overall, the FAD LIJ2P40 showed a reduction of the viral titer on SARS-CoV-2 up to two logs with moderate cytotoxicity which opens the door to further evaluation to fight Covid-19. |
