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Genomic Discovery and Structure-Activity Exploration of a Novel Family of Enzyme-Activated Covalent Cyclin-Dependent Kinase Inhibitors.
Davison, Jack R; Hadjithomas, Michalis; Romeril, Stuart P; Choi, Yoon Jong; Bentley, Keith W; Biggins, John B; Chacko, Nadia; Castaldi, M Paola; Chan, Lawrence K; Cumming, Jared N; Downes, Thomas D; Eisenhauer, Eric L; Fei, Fan; Fontaine, Benjamin M; Endalur Gopinarayanan, Venkatesh; Gurnani, Srishti; Hecht, Audrey; Hosford, Christopher J; Ibrahim, Ashraf; Jagels, Annika; Joubran, Camil; Kim, Ji-Nu; Lisher, John P; Liu, Daniel D; Lyles, James T; Mannara, Matteo N; Murray, Gordon J; Musial, Emilia; Niu, Mengyao; Olivares-Amaya, Roberto; Percuoco, Marielle; Saalau, Susanne; Sharpe, Kristen; Sheahan, Anjali V; Thevakumaran, Neroshan; Thompson, James E; Thompson, Dawn A; Wiest, Aric; Wyka, Stephen A; Yano, Jason; Verdine, Gregory L.
Afiliación
  • Davison JR; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Hadjithomas M; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Romeril SP; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Choi YJ; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Bentley KW; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Biggins JB; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Chacko N; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Castaldi MP; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Chan LK; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Cumming JN; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Downes TD; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Eisenhauer EL; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Fei F; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Fontaine BM; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Endalur Gopinarayanan V; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Gurnani S; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Hecht A; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Hosford CJ; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Ibrahim A; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Jagels A; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Joubran C; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Kim JN; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Lisher JP; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Liu DD; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Lyles JT; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Mannara MN; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Murray GJ; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Musial E; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Niu M; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Olivares-Amaya R; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Percuoco M; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Saalau S; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Sharpe K; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Sheahan AV; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Thevakumaran N; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Thompson JE; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Thompson DA; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Wiest A; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Wyka SA; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Yano J; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
  • Verdine GL; LifeMine Therapeutics, 30 Acorn Park Drive, Cambridge, Massachusetts 02140, United States.
J Med Chem ; 2024 Jul 30.
Article en En | MEDLINE | ID: mdl-39078366
ABSTRACT
Fungi have historically been the source of numerous important medicinal compounds, but full exploitation of their genetic potential for drug development has been hampered in traditional discovery paradigms. Here we describe a radically different approach, top-down drug discovery (TD3), starting with a massive digital search through a database of over 100,000 fully genomicized fungi to identify loci encoding molecules with a predetermined human target. We exemplify TD3 by the selection of cyclin-dependent kinases (CDKs) as targets and the discovery of two molecules, 1 and 2, which inhibit therapeutically important human CDKs. 1 and 2 exhibit a remarkable mechanism, forming a site-selective covalent bond to the CDK active site Lys. We explored the structure-activity relationship via semi- and total synthesis, generating an analog, 43, with improved kinase selectivity, bioavailability, and efficacy. This work highlights the power of TD3 to identify mechanistically and structurally novel molecules for the development of new medicines.
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Texto completo: 1 Bases de datos: MEDLINE Idioma: En Revista: J Med Chem Asunto de la revista: QUIMICA Año: 2024 Tipo del documento: Article País de afiliación: Estados Unidos
Texto completo
Imprimir
XML
PubMed Links
Buscar en Google

Texto completo: 1 Bases de datos: MEDLINE Idioma: En Revista: J Med Chem Asunto de la revista: QUIMICA Año: 2024 Tipo del documento: Article País de afiliación: Estados Unidos