Kling R, Lanig H, Clark T, Gmeiner P (2013)
Publication Language: English
Publication Type: Journal article, Original article
Publication year: 2013
Original Authors: Kling R.C., Lanig H., Clark T., Gmeiner P.
Publisher: Public Library of Science
Book Volume: 8
Article Number: e67244
Journal Issue: 6
DOI: 10.1371/journal.pone.0067244
Based on the recently described crystal structure of the β adrenergic receptor - G-protein complex, we report the first molecular-dynamics simulations of ternary GPCR complexes designed to identify the selectivity determinants for receptor-G-protein binding. Long-term molecular dynamics simulations of agonist-bound β2AR-Gα and D2R-Gα complexes embedded in a hydrated bilayer environment and computational alanine-scanning mutagenesis identified distinct residues of the N-terminal region of intracellular loop 3 to be crucial for coupling selectivity. Within the G-protein, specific amino acids of the α5-helix, the C-terminus of the Gα-subunit and the regions around αN-β1 and α4-β6 were found to determine receptor recognition. Knowledge of these determinants of receptor-G-protein binding selectivity is essential for designing drugs that target specific receptor/G-protein combinations. © 2013 Kling et al.
APA:
Kling, R., Lanig, H., Clark, T., & Gmeiner, P. (2013). Active-State Models of Ternary GPCR Complexes: Determinants of Selective Receptor-G-Protein Coupling. PLoS ONE, 8(6). https://doi.org/10.1371/journal.pone.0067244
MLA:
Kling, Ralf, et al. "Active-State Models of Ternary GPCR Complexes: Determinants of Selective Receptor-G-Protein Coupling." PLoS ONE 8.6 (2013).
BibTeX: Download