A role for a specific cholesterol interaction in stabilizing the Apo configuration of the human A(2A) adenosine receptor.

نویسندگان

  • Edward Lyman
  • Chris Higgs
  • Byungchan Kim
  • Dmitry Lupyan
  • John C Shelley
  • Ramy Farid
  • Gregory A Voth
چکیده

The function of G-protein-coupled receptors is tightly modulated by the lipid environment. Long-timescale molecular dynamics simulations (totaling approximately 3 mus) of the A(2A) receptor in cholesterol-free bilayers, with and without the antagonist ZM241385 bound, demonstrate the instability of helix II in the apo receptor in cholesterol-poor membrane regions. We directly observe that the effect of cholesterol binding is to stabilize helix II against a buckling-type deformation, perhaps rationalizing the observation that the A(2A) receptor couples to G protein only in the presence of cholesterol (Zezula and Freissmuth, 2008). The results suggest a mechanism by which the A(2A) receptor may function as a coincidence detector, activating only in the presence of both cholesterol and agonist. We also observed a previously hypothesized conformation of the tryptophan "rotameric switch" on helix VI in which a phenylalanine on helix V positions the tryptophan out of the ligand binding pocket.

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عنوان ژورنال:
  • Structure

دوره 17 12  شماره 

صفحات  -

تاریخ انتشار 2009