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Membrane-Dependent Binding and Entry Mechanism of Dopamine into Its Receptor

Authors :
Giray Enkavi
Hanna Juhola
Tomasz Róg
Ilpo Vattulainen
Sami Rissanen
Agata Zak
Fabio Lolicato
Mariusz Kepczynski
Pekka A. Postila
Annina E. A. Saukko
Department of Physics
Materials Physics
Tampere University
Research group: Biological Physics and Soft Matter
Physics
Source :
ACS Chemical Neuroscience
Publication Year :
2020

Abstract

Synaptic neurotransmission has recently been proposed to function via either a membrane-independent or a membrane-dependent mechanism, depending on the neurotransmitter type. In the membrane-dependent mechanism, amphipathic neurotransmitters first partition to the lipid headgroup region and then diffuse along the membrane plane to their membrane-buried receptors. However, to date, this mechanism has not been demonstrated for any neurotransmitter-receptor complex. Here, we combined isothermal calorimetry measurements with a diverse set of molecular dynamics simulation methods to investigate the partitioning of an amphipathic neurotransmitter (dopamine) and the mechanism of its entry into the ligand-binding site. Our results show that the binding of dopamine to its receptor is consistent with the membrane-dependent binding and entry mechanism. Both experimental and simulation results showed that dopamine favors binding to lipid membranes especially in the headgroup region. Moreover, our simulations revealed a ligand-entry pathway from the membrane to the binding site. This pathway passes through a lateral gate between transmembrane alpha-helices 5 and 6 on the membrane-facing side of the protein. All in all, our results demonstrate that dopamine binds to its receptor by a membrane-dependent mechanism, and this is complemented by the more traditional binding mechanism directly through the aqueous phase. The results suggest that the membrane-dependent mechanism is common in other synaptic receptors, too. publishedVersion

Details

Language :
English
Database :
OpenAIRE
Journal :
ACS Chemical Neuroscience
Accession number :
edsair.doi.dedup.....76cf69dd539d4fe50ae17f36f4dfadde