Affiliation:
1. Faculty of Pharmacy University of Ljubljana Aškerčeva cesta 7 SI-1000 Ljubljana Slovenia
2. Department of Hematology Oncology and Cancer Immunology Charité – Universitätsmedizin Berlin Hindenburgdamm 30 D-12203 Berlin Germany
3. Pharmaceutical Institute Department of Pharmaceutical & Medicinal Chemistry University of Bonn An der Immenburg 4 D-53121 Bonn Germany
4. Department of Medicinal Chemistry College of Pharmacy University of Florida 32610 Gainesville FL USA
Abstract
AbstractBCL‐2, a member of the BCL‐2 protein family, is an antiapoptotic factor that regulates the intrinsic pathway of apoptosis. Due to its aberrant activity, it is frequently implicated in haematopoietic cancers and represents an attractive target for the development of therapeutics that antagonize its activity. A selective BCL‐2 inhibitor, venetoclax, was approved for treating chronic lymphocytic leukaemia, acute myeloid leukemia, and other haematologic malignancies, validating BCL‐2 as an anticancer target. Since then, alternative therapeutic approaches to modulate the activity of BCL‐2 have been explored, such as antibody‐drug conjugates and proteolysis‐targeting chimeras. Despite numerous research groups focusing on developing degraders of BCL‐2 family member proteins, selective BCL‐2 PROTACs remain elusive, as disclosed compounds only show dual BCL‐xL/BCL‐2 degradation. Herein, we report our efforts to develop BCL‐2 degraders by incorporating two BCL‐2 binding moieties into chimeric compounds that aim to hijack one of three E3 ligases: CRBN, VHL, and IAPs. Even though our project did not result in obtaining a potent and selective BCL‐2 PROTAC, our research will aid in understanding the narrow chemical space of BCL‐2 degraders.
Funder
Deutsche Forschungsgemeinschaft
Javna Agencija za Raziskovalno Dejavnost RS