A model of the adrenergic β2 receptor and binding sites for agonist and antagonist

Vasoactive intestinal peptide (VIP) receptors and p-adrenergic receptors were investigated in rat Harderian gland membranes using '251-VIP and 125I-cyanopindolol(125I-CYP), respectively, as ligands. The receptor bindings were rapid, reversible, saturable, specific, and dependent on time, temperature

A modified concept of functioning of G-protein coupled receptors is presented, on the assumption that agonistic and antagonistic effects of drugs are related to their interaction with two separate receptor sites that exist simultaneously on a single receptor molecule and possess different ligand-spe

A combination of mutagenesis, computer modeling and immunoreactivity has been used to develop a structural model of a segment of the glutamate receptor (GluR), termed GluR3B, which is bound by receptor-activating autoantibodies. In this model, the GluR3B epitope is located in a reverse hairpin loop

## Abstract The 2.4 Å crystal structure of the __β__~2~‐adrenergic receptor (__β__~2~AR) in complex with the high‐affinity inverse agonist (−)‐carazolol provides a detailed structural framework for the analysis of ligand recognition by adrenergic receptors. Insights into agonist binding and the cor