Structure-inspired design of β-arrestin-biased ligands for aminergic GPCRs

John D. McCorvy,Kyle V. Butler,Brendan Kelly,Katie Rechsteiner,Joel Karpiak,Robin M. Betz,Bethany Lyn Kormos,Brian K. Shoichet,Ron O. Dror,Jian Jin,Bryan L. Roth

Structure-inspired design of β-arrestin-biased ligands for aminergic GPCRs

2018

John D. McCorvy
Kyle V. Butler
Brendan Kelly
Katie Rechsteiner
Joel Karpiak
Robin M. Betz
Bethany Lyn Kormos
Brian K. Shoichet
Ron O. Dror
Jian Jin
Bryan L. Roth

D2 dopamine receptor ligands biased for b-arrestin recruitment were developed based on a receptor homology model that identified conserved ligand contacts within the TM5 and EL2 regions as important for biased signaling.

Keywords:

Molecular biology
Biology
Arrestin
Dopamine receptor
Ligand
G protein-coupled receptor
Homology modeling
Receptor
Biochemistry
Cell biology

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