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Establishing Drug Discovery and Identification of Hit Series for the Anti-apoptotic Proteins, Bcl-2 and Mcl-1.
Murray, James B; Davidson, James; Chen, Ijen; Davis, Ben; Dokurno, Pawel; Graham, Christopher J; Harris, Richard; Jordan, Allan; Matassova, Natalia; Pedder, Christopher; Ray, Stuart; Roughley, Stephen D; Smith, Julia; Walmsley, Claire; Wang, Yikang; Whitehead, Neil; Williamson, Douglas S; Casara, Patrick; Le Diguarher, Thierry; Hickman, John; Stark, Jerome; Kotschy, András; Geneste, Olivier; Hubbard, Roderick E.
Afiliación
  • Murray JB; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Davidson J; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Chen I; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Davis B; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Dokurno P; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Graham CJ; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Harris R; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Jordan A; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Matassova N; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Pedder C; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Ray S; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Roughley SD; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Smith J; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Walmsley C; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Wang Y; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Whitehead N; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Williamson DS; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
  • Casara P; Institut de Recherches Servier Oncology R&D Unit, Croissy Sur Seine 78290, France.
  • Le Diguarher T; Institut de Recherches Servier Oncology R&D Unit, Croissy Sur Seine 78290, France.
  • Hickman J; Institut de Recherches Servier Oncology R&D Unit, Croissy Sur Seine 78290, France.
  • Stark J; Institut de Recherches Servier Oncology R&D Unit, Croissy Sur Seine 78290, France.
  • Kotschy A; Servier Research Institute of Medicinal Chemistry, Budapest 1031, Hungary.
  • Geneste O; Institut de Recherches Servier Oncology R&D Unit, Croissy Sur Seine 78290, France.
  • Hubbard RE; Vernalis (R&D) Ltd., Granta Park, Abington, Cambridge CB21 6GB, U.K.
ACS Omega ; 4(5): 8892-8906, 2019 May 31.
Article en En | MEDLINE | ID: mdl-31459977
We describe our work to establish structure- and fragment-based drug discovery to identify small molecules that inhibit the anti-apoptotic activity of the proteins Mcl-1 and Bcl-2. This identified hit series of compounds, some of which were subsequently optimized to clinical candidates in trials for treating various cancers. Many protein constructs were designed to identify protein with suitable properties for different biophysical assays and structural methods. Fragment screening using ligand-observed NMR experiments identified several series of compounds for each protein. The series were assessed for their potential for subsequent optimization using 1H and 15N heteronuclear single-quantum correlation NMR, surface plasmon resonance, and isothermal titration calorimetry measurements to characterize and validate binding. Crystal structures could not be determined for the early hits, so NMR methods were developed to provide models of compound binding to guide compound optimization. For Mcl-1, a benzodioxane/benzoxazine series was optimized to a K d of 40 µM before a thienopyrimidine hit series was identified which subsequently led to the lead series from which the clinical candidate S 64315 (MIK 665) was identified. For Bcl-2, the fragment-derived series were difficult to progress, and a compound derived from a published tetrahydroquinone compound was taken forward as the hit from which the clinical candidate (S 55746) was obtained. For both the proteins, the work to establish a portfolio of assays gave confidence for identification of compounds suitable for optimization.

Texto completo: 1 Base de datos: MEDLINE Tipo de estudio: Diagnostic_studies Idioma: En Revista: ACS Omega Año: 2019 Tipo del documento: Article

Texto completo: 1 Base de datos: MEDLINE Tipo de estudio: Diagnostic_studies Idioma: En Revista: ACS Omega Año: 2019 Tipo del documento: Article