Facile synthesis of borofragments and their evaluation in activity-based protein profiling.

نویسندگان

  • Shinya Adachi
  • Armand B Cognetta
  • Micah J Niphakis
  • Zhi He
  • Adam Zajdlik
  • Jeffrey D St Denis
  • Conor C G Scully
  • Benjamin F Cravatt
  • Andrei K Yudin
چکیده

The discovery of enzyme inhibitors relies on synthetic methods that enable rapid and modular construction of small molecules. Heterocyclic fragments designed to maximize enthalpic interactions with their protein targets represent a particularly desirable class of molecules. Here we describe a reagent that enables straightforward construction of "borofragments", in which a heterocycle is separated from the boron center by two or three rotatable bonds. The stability of these molecules depends on the MIDA group which likely acts as a slow-release element under biological conditions. Borofragments can be used to discover inhibitors of enzymes that use catalytic oxygen nucleophiles. We have employed this method to identify inhibitors of ABHD10 and the predicted carboxypeptidase CPVL. This technique should be applicable to other classes of targets.

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عنوان ژورنال:
  • Chemical communications

دوره 51 17  شماره 

صفحات  -

تاریخ انتشار 2015