Neurotransmitter GABA activates muscle but not a7 nicotinic receptors

DIONISIO, L.; BERGÉ, I.; BRAVO, M.; ESANDI, M.C.; BOUZAT, C.

Sierra de la Ventana, Bs As.

Congreso; Congreso de la Sociedad Argentina de Biofísica; 2014

SAB

Cys-loop receptors are neurotransmitter-activated ion channels involved in synaptic and extrasynaptic transmission in the brain and are also present in non-neuronal cells. As GABAA and nicotinic receptors (nAChR) belong to this family, we explored by macroscopic and single-channel recordings if the inhibitory neurotransmitter GABA has the ability to activate excitatory nAChRs. GABA differentially activates nAChR subtypes. It activates muscle nAChRs, with maximal peak currents of about 10 % of those elicited by ACh and 15-fold higher EC50 with respect to ACh. At the single-channel level, the weak agonism is revealed by the requirement of 20-fold higher concentration of GABA for detectable channel openings, a major population of brief openings, and absence of clusters of openings when compared to ACh. Mutations at key residues of the principal binding-site face of muscle nAChRs (αY190 and αG153) affect GABA-activation similarly as ACh-activation whereas a mutation at the complementary face (εG57) shows a selective effect for GABA. Studies with subunit-lacking receptors show that GABA can activate muscle nAChRs through the α/δ interface. Interestingly, single-channel activity elicited by GABA is similar to that elicited by ACh in gain-of-function nAChR mutants associated to congenital myasthenic syndromes, which could be important in the progression of the disorders due to steady exposure to serum GABA. In contrast, GABA cannot elicit single-channel or macroscopic currents of α7 or the chimeric α7-5HT3A receptor, a feature important for preserving an adequate excitatory/inhibitory balance in the brain as well as for avoiding activation of nonneuronal receptors by serum GABA.