An Epilepsy-Related Region in the GABA<sub>A</sub> Receptor Mediates Long-Distance Effects on GABA and Benzodiazepine Binding Sites

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The GABA A receptor is a multisubunit protein that transduces the binding of a neurotransmitter at an intersubunit interface into the opening of a central ion channel. The structural components that mediate the steps involved in this action are poorly defined. A large amount of work has focused on clarifying the specific functions and interactions of residues believed to surround the GABA binding pocket. Here, we explored two charged residues (␤ 2 Asp163 and ␣ 1 Arg120), which have been suggested by homology models to participate in a salt-bridge interaction. When mutated to alanine, both single mutants, as well as the double mutant, increase EC 50-GABA , decrease the GABA binding rate, and accelerate deactivation and GABA unbinding rates. Double-mutant cycle analysis demonstrates that the effects of each alanine mutation on the GABA binding rate were additive and independent. In contrast, a significant coupling energy was found during an analysis of deactivation time constants. Using kinetic modeling, we further demonstrated that the GABA unbinding rates, in particular, are strongly coupled. These data suggest that ␤ 2 Asp163 and ␣ 1 Arg120 form a state-dependent salt bridge, interacting when GABA is bound to the receptor but not when the receptor is in the unbound state.

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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A State-Dependent Salt-Bridge Interaction Exists across the β/α Intersubunit Interface of the GABA_AReceptor

Laha

Wagner²

2011

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“…In general, it is believed that BZDs exert their allosteric effects by either shifting the GABA A R closed to open-state channel equilibrium (Downing et al, 2005;Rü sch and Forman, 2005;Campo-Soria et al, 2006) or altering the receptor's microscopic binding affinity for GABA (Twyman et al, 1989;Rogers et al, 1994;Lavoie and Twyman, 1996;Mellor and Randall, 1997;Thompson et al, 1999;Goldschen-Ohm et al, 2010). Regardless of the mechanism, BZD binding to the receptor is the initial perturbation that triggers structural rearrangements in the protein that result in modulation of GABA A R function.…”

Section: Introductionmentioning

confidence: 99%

Different Residues in the GABA_AReceptor Benzodiazepine Binding Pocket Mediate Benzodiazepine Efficacy and Binding

Morlock

Czajkowski²

2011

Benzodiazepines (BZDs) exert their therapeutic actions by binding to the GABA A receptor (GABA A R) and allosterically modulating GABA-induced chloride currents (I GABA ). A variety of ligands with divergent structures bind to the BZD site, and the structural mechanisms that couple their binding to potentiation of I GABA are not well understood. In this study, we measured the effects of individually mutating 22 residues throughout the BZD binding pocket on the abilities of eszopiclone, zolpidem, and flurazepam to potentiate I GABA . Wild-type and mutant ␣ 1 ␤ 2 ␥ 2 GABA A Rs were expressed in Xenopus laevis oocytes and analyzed using a two-electrode voltage clamp. GABA EC 50 , BZD EC 50 , and BZD maximal potentiation were measured. These data, combined with previous radioligand binding data describing the mutations' effects on BZD apparent binding affinities (J Neurosci 28:3490 -3499, 2008; J Med Chem 51:7243-7252, 2008), were used to distinguish residues within the BZD pocket that contribute to BZD efficacy and BZD binding. We identified six residues whose mutation altered BZD maximal potentiation of I GABA (BZD efficacy) without altering BZD binding apparent affinity, three residues whose mutation altered binding but had no effect on BZD efficacy, and four residues whose mutation affected both binding and efficacy. Moreover, depending on the BZD ligand, the effects of some mutations were different, indicating that the structural mechanisms underlying the ability of BZD ligands with divergent structures to potentiate I GABA are distinct.

“…Unlike the binding rate, we could not examine this directly, but instead we asked whether such a hypothesis could explain our observations using a kinetic model shown previously to account for multiple aspects of GABA A receptor behavior (Fig. 7A) (Jones et al, 1998;Wagner et al, 2004;Goldschen-Ohm et al, 2010).…”

Section: Role Of Arginines In Agonist and Antagonist Binding 653mentioning

confidence: 99%

Three Arginines in the GABA_AReceptor Binding Pocket Have Distinct Roles in the Formation and Stability of Agonist- versus Antagonist-Bound Complexes

Goldschen-Ohm

Wagner²,

Jones³

2011

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Binding of the agonist GABA to the GABA A receptor causes channel gating, whereas competitive antagonists that bind at the same site do not. The details of ligand binding are not well understood, including which residues interact directly with ligands, maintain the structure of the binding pocket, or transduce the action of binding into opening of the ion channel gate. Recent work suggests that the amine group of the GABA molecule may form a cation-bond with residues in a highly conserved "aromatic box" within the binding pocket. Although interactions with the carboxyl group of GABA remain unknown, three positively charged arginines (␣ 1 Arg67, ␣ 1 Arg132, and ␤ 2 Arg207) just outside of the aromatic box are likely candidates. To explore their roles in ligand binding, we individually mutated these arginines to alanine and measured the effects on microscopic ligand binding/unbinding rates and channel gating. The mutations ␣ 1 R67A or ␤ 2 R207A slowed agonist binding and sped unbinding with little effect on gating, demonstrating that these arginines are critical for both formation and stability of the agonist-bound complex. In addition, ␣ 1 R67A sped binding of the antagonist 2-(3-carboxypropyl)-3-amino-6-(4 methoxyphenyl)pyridazinium bromide (SR-95531), indicating that this arginine poses a barrier to formation of the antagonistbound complex. In contrast, ␤ 2 R207A and ␣ 1 R132A sped antagonist unbinding, indicating that these arginines stabilize the antagonist-bound state. ␣ 1 R132A also conferred a new longlived open state, indicating that this arginine influences the channel gate. Thus, each of these arginines plays a unique role in determining interactions with agonists versus antagonists and with the channel gate.