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Structural Insights into the Role of β3 nAChR Subunit in the Activation of Nicotinic Receptors
Authors:Petros Giastas  Athanasios Papakyriakou  George Tsafaras  Socrates J. Tzartos  Marios Zouridakis
Affiliation:1.Department of Neurobiology, Hellenic Pasteur Institute, GR11521 Athens, Greece; (G.T.); (S.J.T.);2.Department of Biotechnology, Agricultural University of Athens, GR11855 Athens, Greece;3.Institute of Biosciences and Applications, NCSR “Demokritos”, GR15310 Athens, Greece;
Abstract:The β3 subunit of nicotinic acetylcholine receptors (nAChRs) participates in heteropentameric assemblies with some α and other β neuronal subunits forming a plethora of various subtypes, differing in their electrophysiological and pharmacological properties. While β3 has for several years been considered an accessory subunit without direct participation in the formation of functional binding sites, recent electrophysiology data have disputed this notion and indicated the presence of a functional (+) side on the extracellular domain (ECD) of β3. In this study, we present the 2.4 Å resolution crystal structure of the monomeric β3 ECD, which revealed rather distinctive loop C features as compared to those of α nAChR subunits, leading to intramolecular stereochemical hindrance of the binding site cavity. Vigorous molecular dynamics simulations in the context of full length pentameric β3-containing nAChRs, while not excluding the possibility of a β3 (+) binding site, demonstrate that this site cannot efficiently accommodate the agonist nicotine. From the structural perspective, our results endorse the accessory rather than functional role of the β3 nAChR subunit, in accordance with earlier functional studies on β3-containing nAChRs.
Keywords:nAChR, pentameric ligand gated ion channels, pentamers, principal binding site, complementary binding site, α    2 nAChR, α      3 nAChR, electrophysiology, molecular dynamics, crystal structure
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