Characterization of [³H]Quisqualate Binding to Recombinant Rat Metabotropic Glutamate 1a and 5a Receptors and to Rat and Human Brain Sections

Abstract: Abstract:We have investigated the binding properties of [ 3 H]quisqualate to rat metabotropic glutamate (mGlu) 1a and 5a receptors and to rat and human brain sections. Saturation isotherms gave K D values of 27 Ϯ 4 and 81 Ϯ 22 nM for mGlu1a and mGlu5a receptors, respectively. Several compounds inhibited the binding to mGlu1a and mGlu5a receptors concentration-dependently. (S)-4-Carboxyphenylglycine, (S)-4-carboxy-3-hydroxyphenylglycine, and (R,S)-1-aminoindan-1,5-dicarboxylic acid, which completely inhibited [… Show more

“…The measured affinity for quisqualate was similar for myc-mGluR1 and myc-mGluR1mut-i1/i3 (mGluR1 K D 75.9 Ϯ 31.6 nM, mGluR1mut-i1/i3 K D 78.1 Ϯ 26.6 nM, n ϭ 6; Fig. 3, A and B) although lower than previously reported (24), presumably because of the presence of the tag close to agonist binding site. To examine the impact of caveolin-1 binding on receptor association with lipid rafts, HEK293 cells expressing myc-mGluR1mut-i1/i3 were incubated with GPT/pyruvate alone or challenged with 1 mM glutamate for 5 min; DRMs were prepared from control and glutamate-treated cells, and receptor localization was examined by immunoblot.…”

Agonist-dependent Signaling by Group I Metabotropic Glutamate Receptors Is Regulated by Association with Lipid Domains

“…The measured affinity for quisqualate was similar for myc-mGluR1 and myc-mGluR1mut-i1/i3 (mGluR1 K D 75.9 Ϯ 31.6 nM, mGluR1mut-i1/i3 K D 78.1 Ϯ 26.6 nM, n ϭ 6; Fig. 3, A and B) although lower than previously reported (24), presumably because of the presence of the tag close to agonist binding site. To examine the impact of caveolin-1 binding on receptor association with lipid rafts, HEK293 cells expressing myc-mGluR1mut-i1/i3 were incubated with GPT/pyruvate alone or challenged with 1 mM glutamate for 5 min; DRMs were prepared from control and glutamate-treated cells, and receptor localization was examined by immunoblot.…”

Agonist-dependent Signaling by Group I Metabotropic Glutamate Receptors Is Regulated by Association with Lipid Domains

“…Concentrationresponse curves for these FRET signals yielded EC 50 values of 1.3 mM for quisqualate and 22.6 mM for glutamate (Fig. 4C), which parallels in vitro functional assays of the mGluR1 (45).…”

“…The concentration-response curve for the agonist quisqualate gave an EC 50 (median effective concentration) value of 1.05 mM (Fig. 3D), which is compatible with mGluR1 pharmacology (44,45). The increase in FRET between fluorescent proteins placed in the intracellular loops of the subunits is compatible with the assumed activation mechanism of class C receptors that involves a rearrangement of the two subunits within the receptor dimer (46)(47)(48).…”

Sequential Inter- and Intrasubunit Rearrangements During Activation of Dimeric Metabotropic Glutamate Receptor 1

“…The results of the experiments conducted with the chimeric receptors indicate that also for mGluR3 and mGluR1a, as for other GPCRs (25,40), the coupling to the G-protein is involved in determining the affinity of the receptors toward their agonist (but see other reports (41,42)). Therefore, we suggest that depolarization causes a conformational change that affects the intracellular loops that couple to the G-protein, thereby regulating the likelihood of the receptors to couple to their corresponding G-protein.…”

The Metabotropic Glutamate G-protein-coupled Receptors mGluR3 and mGluR1a Are Voltage-sensitive