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Proteome-wide covalent ligand discovery in native biological systems.
Backus, Keriann M; Correia, Bruno E; Lum, Kenneth M; Forli, Stefano; Horning, Benjamin D; González-Páez, Gonzalo E; Chatterjee, Sandip; Lanning, Bryan R; Teijaro, John R; Olson, Arthur J; Wolan, Dennis W; Cravatt, Benjamin F.
Afiliação
  • Backus KM; Department of Chemical Physiology, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Correia BE; Department of Chemical Physiology, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Lum KM; Department of Chemical Physiology, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Forli S; Department of Integrative Structural and Computational Biology, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Horning BD; Department of Chemical Physiology, The Scripps Research Institute. La Jolla, California 92307, USA.
  • González-Páez GE; Department of Molecular and Experimental Medicine, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Chatterjee S; Department of Molecular and Experimental Medicine, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Lanning BR; Department of Chemical Physiology, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Teijaro JR; Department of Immunology and Microbial Science, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Olson AJ; Department of Integrative Structural and Computational Biology, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Wolan DW; Department of Molecular and Experimental Medicine, The Scripps Research Institute. La Jolla, California 92307, USA.
  • Cravatt BF; Department of Chemical Physiology, The Scripps Research Institute. La Jolla, California 92307, USA.
Nature ; 534(7608): 570-4, 2016 06 23.
Article em En | MEDLINE | ID: mdl-27309814
Small molecules are powerful tools for investigating protein function and can serve as leads for new therapeutics. Most human proteins, however, lack small-molecule ligands, and entire protein classes are considered 'undruggable'. Fragment-based ligand discovery can identify small-molecule probes for proteins that have proven difficult to target using high-throughput screening of complex compound libraries. Although reversibly binding ligands are commonly pursued, covalent fragments provide an alternative route to small-molecule probes, including those that can access regions of proteins that are difficult to target through binding affinity alone. Here we report a quantitative analysis of cysteine-reactive small-molecule fragments screened against thousands of proteins in human proteomes and cells. Covalent ligands were identified for >700 cysteines found in both druggable proteins and proteins deficient in chemical probes, including transcription factors, adaptor/scaffolding proteins, and uncharacterized proteins. Among the atypical ligand-protein interactions discovered were compounds that react preferentially with pro- (inactive) caspases. We used these ligands to distinguish extrinsic apoptosis pathways in human cell lines versus primary human T cells, showing that the former is largely mediated by caspase-8 while the latter depends on both caspase-8 and -10. Fragment-based covalent ligand discovery provides a greatly expanded portrait of the ligandable proteome and furnishes compounds that can illuminate protein functions in native biological systems.
Assuntos

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Linfócitos T / Proteoma / Cisteína / Avaliação Pré-Clínica de Medicamentos / Bibliotecas de Moléculas Pequenas Tipo de estudo: Prognostic_studies Limite: Humans Idioma: En Ano de publicação: 2016 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Linfócitos T / Proteoma / Cisteína / Avaliação Pré-Clínica de Medicamentos / Bibliotecas de Moléculas Pequenas Tipo de estudo: Prognostic_studies Limite: Humans Idioma: En Ano de publicação: 2016 Tipo de documento: Article