A conserved arginine with non-conserved function is a key determinant of agonist selectivity in α7 nicotinic ACh receptors.
Teresa Minguez-ViñasBeatriz Elizabeth NielsenDeborah K ShoemarkCecilia GottiRichard B SessionsAdrian J MulhollandCecilia BouzatSusan WonnacottTimothy GallagherIsabel BermudezAna Sofia F OliveiraPublished in: British journal of pharmacology (2021)
We conclude that the high mobility of the β3-strand arginine in the α7 nAChR influences agonist binding and possibly gating network and desensitisation. The findings have implications for rational design of subtype-selective nAChR agents.