Evidence for Inhibition Mediated by Coassembly of GABAA and GABAC Receptor Subunits in Native Central Neurons

doi:10.1523/JNEUROSCI.1979-04.2004

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The Journal of Neuroscience, August 18, 2004, 24(33):7241-7250; doi:10.1523/JNEUROSCI.1979-04.2004

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Cellular/Molecular
Evidence for Inhibition Mediated by Coassembly of GABA_A and GABA_C Receptor Subunits in Native Central Neurons
Carol J. Milligan,¹^* Noel J. Buckley,¹^,2 Maurice Garret,³ Jim Deuchars,¹ and Susan A. Deuchars¹^*
¹School of Biomedical Sciences, University of Leeds, Leeds LS2 9NQ, United Kingdom, ²School of Biochemistry and Molecular Biology, University of Leeds, Leeds, LS2 9JT, United Kingdom, and ³Laboratoire de Neurophysiologie, Centre National de la Recherche Scientifique, Unité Mixte de Recherche 5543, Universitie de Bordeaux I, Bordeaux, France

Fast inhibition in the nervous system is commonly mediated byGABA_A receptors comprised of 2 ${alpha}$ /2 ${beta}$ /1 ${gamma}$ subunits. In contrast, GABA_Creceptors containing only ${rho}$ subunits ( ${rho}$ 1- ${rho}$ 3) have been predominantlydetected in the retina. However, here using reverse transcription-PCRand in situ hybridization we show that mRNA encoding the ${rho}$ 1 subunitis highly expressed in brainstem neurons. Immunohistochemistrylocalized the ${rho}$ 1 subunit to neurons at light and electron microscopiclevels, where it was detected at synaptic junctions. Applicationof the GABA_C receptor agonist cis-4-aminocrotonic acid (100-800µM) requires the ${rho}$ 1 subunit to elicit responses, whichsurprisingly are blocked independently by antagonists to GABA_A(bicuculline, 10 µM) and GABA_C [(1,2,5,6-tetrahydropyridin-4-yl)methylphosphinicacid (TPMPA); 40-160 µM] receptors. Responses to GABA_Cagonists were also enhanced by the GABA_A receptor modulatorpentobarbitone (300 µM). Spontaneous and evoked IPSPswere reduced in amplitude but never abolished by TPMPA, butwere completely blocked by bicuculline. We therefore testedthe hypothesis that GABA_A and GABA_C subunits formed a heteromericreceptor. Immunohistochemistry indicated that ${rho}$ 1 and ${alpha}$ 1 subunitswere colocalized at light and electron microscopic levels. Electrophysiologyrevealed that responses to GABA_C receptor agonists were enhancedby the GABA_A receptor modulator zolpidem (500 nM), which actson the ${alpha}$ 1 subunit when the ${gamma}$ 2 subunit is also present. Finally,coimmunoprecipitation indicated that the ${rho}$ 1 subunit formed complexesthat also contained ${alpha}$ 1 and ${gamma}$ 2 subunits. Taken together these separatelines of evidence suggest that the effects of GABA in centralneurons can be mediated by heteromeric complexes of GABA_A andGABA_C receptor subunits.

Key words: autonomic; bicuculline; brainstem; GABA; IPSP; preganglionic

Received July 10, 2003; revised June 28, 2004; accepted June 28, 2004.

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