Mechanism of Action of Compound-13: An α1-Selective Small Molecule Activator of AMPK

نویسندگان

  • Roger W. Hunter
  • Marc Foretz
  • Laurent Bultot
  • Morgan D. Fullerton
  • Maria Deak
  • Fiona A. Ross
  • Simon A. Hawley
  • Natalia Shpiro
  • Benoit Viollet
  • Denis Barron
  • Bruce E. Kemp
  • Gregory R. Steinberg
  • D. Grahame Hardie
  • Kei Sakamoto
چکیده

AMPK is a sensor of cellular energy status and a promising target for drugs aimed at metabolic disorders. We have studied the selectivity and mechanism of a recently described activator, C2, and its cell-permeable prodrug, C13. C2 was a potent allosteric activator of α1-complexes that, like AMP, also protected against Thr172 dephosphorylation. Compared with AMP, C2 caused only partial allosteric activation of α2-complexes and failed to protect them against dephosphorylation. We show that both effects could be fully restored by exchanging part of the linker between the autoinhibitory and C-terminal domains in α2, containing the equivalent region from α1 thought to interact with AMP bound in site 3 of the γ subunit. Consistent with our results in cell-free assays, C13 potently inhibited lipid synthesis in hepatocytes from wild-type and was largely ineffective in AMPK-knockout hepatocytes; its effects were more severely affected by knockout of α1 than of α2, β1, or β2.

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عنوان ژورنال:

دوره 21  شماره 

صفحات  -

تاریخ انتشار 2014