Energy Landscapes Reveal Agonist Control of G Protein-Coupled Receptor Activation via Microswitches.
Oliver FleetwoodPierre MatriconJens CarlssonLucie DelemottePublished in: Biochemistry (2020)
Agonist binding to G protein-coupled receptors (GPCRs) leads to conformational changes in the transmembrane region that activate cytosolic signaling pathways. Although high-resolution structures of different receptor states are available, atomistic details of allosteric signaling across the membrane remain elusive. We calculated free energy landscapes of β2 adrenergic receptor activation using atomistic molecular dynamics simulations in an optimized string of swarms framework, which shed new light on how microswitches govern the equilibrium between conformational states. Contraction of the extracellular binding site in the presence of the agonist BI-167107 is obligatorily coupled to conformational changes in a connector motif located in the core of the transmembrane region. The connector is probabilistically coupled to the conformation of the intracellular region. An active connector promotes desolvation of a buried cavity, a twist of the conserved NPxxY motif, and an interaction between two conserved tyrosines in transmembrane helices 5 and 7 (Y-Y motif), which lead to a larger population of active-like states at the G protein binding site. This coupling is augmented by protonation of the strongly conserved Asp792.50. The agonist binding site hence communicates with the intracellular region via a cascade of locally connected microswitches. Characterization of these can be used to understand how ligands stabilize distinct receptor states and contribute to development drugs with specific signaling properties. The developed simulation protocol can likely be transferred to other class A GPCRs.
Keyphrases
- molecular dynamics simulations
- molecular docking
- high resolution
- transcription factor
- signaling pathway
- randomized controlled trial
- epithelial mesenchymal transition
- reactive oxygen species
- genome wide
- dna methylation
- binding protein
- oxidative stress
- small molecule
- single molecule
- molecular dynamics
- cell proliferation
- pi k akt
- endoplasmic reticulum stress