Subcellular distribution of GABAB receptor homo- and hetero-dimers

GBRs (GABAB receptors; where GABA stands for γ-aminobutyric acid) are G-protein-coupled receptors that mediate slow synaptic inhibition in the brain and spinal cord. In vitro assays have previously demonstrated that these receptors are heterodimers assembled from two homologous subunits, GBR1 and GB...

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Published inBiochemical journal Vol. 388; no. 1; pp. 47 - 55
Main Authors VILLEMURE, Josée-France, ADAM, Lynda, BEVAN, Nicola J., GEARING, Katy, CHÉNIER, Sébastien, BOUVIER, Michel
Format Journal Article
LanguageEnglish
Published Portland Press Ltd 15.05.2005
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Summary:GBRs (GABAB receptors; where GABA stands for γ-aminobutyric acid) are G-protein-coupled receptors that mediate slow synaptic inhibition in the brain and spinal cord. In vitro assays have previously demonstrated that these receptors are heterodimers assembled from two homologous subunits, GBR1 and GBR2, neither of which is capable of producing functional GBR on their own. We have used co-immunoprecipitation in combination with bioluminescence and fluorescence resonance energy transfer approaches in living cells to assess directly the interaction between GBR subunits and determine their subcellular localization. The results show that, in addition to forming heterodimers, GBR1 and GBR2 can associate as stable homodimers. Confocal microscopy indicates that, while GBR1/GBR1 homodimers are retained in the endoplasmic reticulum and endoplasmic reticulum–Golgi intermediate compartment, both GBR2/GBR2 homodimers and GBR1/GBR2 heterodimers are present at the plasma membrane. Although these observations shed new light on the assembly of GBR complexes, they raise questions about the potential functional roles of GBR1 and GBR2 homodimers.
Bibliography:1Present address: AstraZeneca R&D Montreal, 7171, Frederick-Banting, Ville St-Laurent, QC, Canada H4S 1Z9.
3Holder of the Hans Selye Chair in molecular and cell biology and a Canada Research Chair in signal transduction and molecular pharmacology.
ISSN:0264-6021
1470-8728
DOI:10.1042/BJ20041435