Identification of the Highly Active, Species Cross-Reactive Complex I Inhibitor BAY-179

Jeffrey Mowat; Alexander H M Ehrmann; Sven Christian; Carolyn Sperl; Stephan Menz; Judith Günther; Roman C Hillig; Marcus Bauser; Wolfgang Schwede

doi:10.1021/acsmedchemlett.1c00666

Identification of the Highly Active, Species Cross-Reactive Complex I Inhibitor BAY-179

ACS Med Chem Lett. 2022 Feb 18;13(3):348-357. doi: 10.1021/acsmedchemlett.1c00666. eCollection 2022 Mar 10.

Authors

Jeffrey Mowat¹, Alexander H M Ehrmann², Sven Christian¹, Carolyn Sperl¹, Stephan Menz¹, Judith Günther¹, Roman C Hillig¹, Marcus Bauser¹, Wolfgang Schwede¹

Affiliations

¹ Pharmaceuticals R&D, Bayer AG, 13342 Berlin, Germany.
² Pharmaceuticals R&D, Bayer AG, 42113 Wuppertal, Germany.

Abstract

Mitochondria are key regulators of energy supply and cell death. Generation of ATP within mitochondria occurs through oxidative phosphorylation (OXPHOS), a process which utilizes the four complexes (complex I-IV) of the electron transport chain and ATP synthase. Certain oncogenic mutations (e.g., LKB1 or mIDH) can further enhance the reliance of cancer cells on OXPHOS for their energetic requirements, rendering cells sensitive to complex I inhibition and highlighting the potential value of complex I as a therapeutic target. Herein, we describe the discovery of a potent, selective, and species cross-reactive complex I inhibitor. A high-throughput screen of the Bayer compound library followed by hit triaging and initial hit-to-lead activities led to a lead structure which was further optimized in a comprehensive lead optimization campaign. Focusing on balancing potency and metabolic stability, this program resulted in the identification of BAY-179, an excellent in vivo suitable tool with which to probe the biological relevance of complex I inhibition in cancer indications.