Identifying the proteins to which small-molecule probes and drugs bind in cells.

نویسندگان

  • Shao-En Ong
  • Monica Schenone
  • Adam A Margolin
  • Xiaoyu Li
  • Kathy Do
  • Mary K Doud
  • D R Mani
  • Letian Kuai
  • Xiang Wang
  • John L Wood
  • Nicola J Tolliday
  • Angela N Koehler
  • Lisa A Marcaurelle
  • Todd R Golub
  • Robert J Gould
  • Stuart L Schreiber
  • Steven A Carr
چکیده

Most small-molecule probes and drugs alter cell circuitry by interacting with 1 or more proteins. A complete understanding of the interacting proteins and their associated protein complexes, whether the compounds are discovered by cell-based phenotypic or target-based screens, is extremely rare. Such a capability is expected to be highly illuminating--providing strong clues to the mechanisms used by small-molecules to achieve their recognized actions and suggesting potential unrecognized actions. We describe a powerful method combining quantitative proteomics (SILAC) with affinity enrichment to provide unbiased, robust and comprehensive identification of the proteins that bind to small-molecule probes and drugs. The method is scalable and general, requiring little optimization across different compound classes, and has already had a transformative effect on our studies of small-molecule probes. Here, we describe in full detail the application of the method to identify targets of kinase inhibitors and immunophilin binders.

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عنوان ژورنال:
  • Proceedings of the National Academy of Sciences of the United States of America

دوره 106 12  شماره 

صفحات  -

تاریخ انتشار 2009