Abstract
Background and PurposeReactive oxygen species (ROS) are normally involved in cell oxidative stress but also play a role as cellular messengers in redox signalling; for example, modulating the activity of neurotransmitter receptors and ion channels. However, the direct actions of ROS on GABA(A) receptors were not previously demonstrated. In the present work, we studied the effects of ROS on GABA(A)1 receptor function.
Experimental ApproachGABA(A)1 receptors were expressed in oocytes and GABA-evoked responses electrophysiologically recorded in the presence or absence of ROS. Chemical protection of cysteines by selective sulfhydryl reagents and site-directed mutagenesis studies were used to identify protein residues involved in ROS actions.
Key ResultsGABA(A)1 receptor-mediated responses were significantly enhanced in a concentration-dependent and reversible manner by H2O2. Potentiating effects were attenuated by a free radical scavenger, lipoic acid or an inhibitor of the Fenton reaction, deferoxamine. Each 1 subunit contains only three cysteine residues, two extracellular at the Cys-loop (C-177 and C-191) and one intracellular (C-364) at the M3-M4 linker. Mutant GABA(A)1 receptors in which C-364 was exchanged by alanine were completely insensitive to modulation, implying that this site, rather than a cysteine in the Cys-loop, is essential for ROS modulation.
Conclusion and ImplicationsOur results show that the function of GABA(A)1 receptors is enhanced by ROS and that the intracellular C-364 is the sensor for ROS actions.