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Drug Repurposing: Deferasirox Inhibits the Anti-Apoptotic Activity of Mcl-1.

Authors :: Bourafai-Aziez A
Benabderrahmane M
Paysant H
Weiswald LB
Poulain L
Carlier L
Ravault D
Jouanne M
Coadou G
Oulyadi H
Voisin-Chiret AS
Sopková-de Oliveira Santos J
Sebban M
Source :: Drug design, development and therapy [Drug Des Devel Ther] 2021 Dec 15; Vol. 15, pp. 5035-5059. Date of Electronic Publication: 2021 Dec 15 (Print Publication: 2021).
Publication Year :: 2021
Abstract: Introduction: With the aim of repositioning commercially available drugs for the inhibition of the anti-apoptotic myeloid cell leukemia protein, Mcl-1, implied in various cancers, five molecules, highlighted from a published theoretical screening, were selected to experimentally validate their affinity toward Mcl-1.<br />Results: A detailed NMR study revealed that only two of the five tested drugs, Torsemide and Deferasirox, interacted with Mcl-1. NMR data analysis allowed the complete characterization of the binding mode of both drugs to Mcl-1, including the estimation of their affinity for Mcl-1. Biological assays evidenced that the biological activity of Torsemide was lower as compared to the Deferasirox, which was able to efficiently and selectively inhibit the anti-apoptotic activity of Mcl-1. Finally, docking and molecular dynamics led to a 3D model for the Deferasirox:Mcl-1 complex and revealed the positioning of the drug in the Mcl-1 P2/P3 pockets as well as almost all synthetic Mcl-1 inhibitors. Interestingly, contrary to known synthetic Mcl-1 inhibitors which interact through Arg263, Deferasirox, establishes a salt bridge with Lys234.<br />Conclusion: Deferasirox could be a potential candidate for drug repositioning as Mcl-1 inhibitor.<br />Competing Interests: The authors report no conflicts of interest in this work.<br /> (© 2021 Bourafai-Aziez et al.)