The role of bicarbonate in GABAA receptor‐mediated IPSPs of rat neocortical neurones.

Kaila, Kai; Voipio, Juha; Paalasmaa, Pekka; Pasternack, Michael; Deisz, Rudolf A.

doi:10.1113/jphysiol.1993.sp019634

Cited by 196 publications

(183 citation statements)

References 40 publications

Supporting

Mentioning

166

Contrasting

Unclassified

Order By: Relevance

“…As discussed in Section 9, this mechanism may play an important role in neonatal seizures (Dzhala et al, 2005(Dzhala et al, , 2010Nardou et al, 2009). Third, GABA A receptormediated depolarizations are contributed by HCO 3 − currents that have quite positive reversal potentials (−10 to −15 mV) (Staley et al, 1995;Lamsa and Kaila, 1997;Kaila et al, 1993Kaila et al, , 1997Rivera et al, 2005). Fourth, as discussed in Section 5.2.2, postsynaptic GABA A receptor activation can produce per se increases in extracellular K + concentration ([K + ] o ) (Barolet and Morris, 1991), a phenomenon that is known to depolarize neighboring nerve cells and to cause seizure activity (Zuckermann and Glaser, 1968).…”

Section: Gaba a Receptor-mediated Depolarizing Actionsmentioning

confidence: 96%

GABAergic synchronization in the limbic system and its role in the generation of epileptiform activity

Avoli¹,

Curtis²

2011

Progress in Neurobiology

227

253

View full text Add to dashboard Cite

GABA is the main inhibitory neurotransmitter in the adult forebrain, where it activates ionotropic type A and metabotropic type B receptors. Early studies have shown that GABA A receptormediated inhibition controls neuronal excitability and thus the occurrence of seizures. However, more complex, and at times unexpected, mechanisms of GABAergic signaling have been identified during epileptiform discharges over the last few years. Here, we will review experimental data that point at the paradoxical role played by GABA A receptor-mediated mechanisms in synchronizing neuronal networks, and in particular those of limbic structures such as the hippocampus, the entorhinal and perirhinal cortices, or the amygdala. After having summarized the fundamental characteristics of GABA A receptor-mediated mechanisms, we will analyze their role in the generation of network oscillations and their contribution to epileptiform synchronization. Whether and how GABA A receptors influence the interaction between limbic networks leading to ictogenesis will be also reviewed. Finally, we will consider the role of altered inhibition in the human epileptic brain along with the ability of GABA A receptor-mediated conductances to generate synchronous depolarizing events that may lead to ictogenesis in human epileptic disorders as well.

show abstract

Section: Gaba a Receptor-mediated Depolarizing Actionsmentioning

confidence: 96%

GABAergic synchronization in the limbic system and its role in the generation of epileptiform activity

Avoli¹,

Curtis²

2011

Progress in Neurobiology

227

253

View full text Add to dashboard Cite

show abstract

“…For instance, GABA A receptor channels mediate a significant net efflux of HCO 3 Ϫ under physiological conditions (32,33), and an increase in pH i induces an increase in the depolarizing bicarbonate current component in ionotropic GABAergic responses (34). Furthermore, the depolarizing action of HCO 3 Ϫ efflux by GABA A receptors drives a conductive net uptake of chloride, resulting in chloride-mediated positive shifts in GABA A receptor responses (35).…”

Section: Discussionmentioning

confidence: 99%

Mice with targeted Slc4a10 gene disruption have small brain ventricles and show reduced neuronal excitability

Jacobs

Ruusuvuori

Sipilä³

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

149

246

View full text Add to dashboard Cite

Members of the SLC4 bicarbonate transporter family are involved in solute transport and pH homeostasis. Here we report that disrupting the Slc4a10 gene, which encodes the Na ؉ -coupled Cl ؊ -HCO3 ؊ exchanger Slc4a10 (NCBE), drastically reduces brain ventricle volume and protects against fatal epileptic seizures in mice. In choroid plexus epithelial cells, Slc4a10 localizes to the basolateral membrane. These cells displayed a diminished recovery from an acid load in KO mice. Slc4a10 also was expressed in neurons. Within the hippocampus, the Slc4a10 protein was abundant in CA3 pyramidal cells. In the CA3 area, propionate-induced intracellular acidification and attenuation of 4-aminopyridineinduced network activity were prolonged in KO mice. Our data indicate that Slc4a10 is involved in the control of neuronal pH and excitability and may contribute to the secretion of cerebrospinal fluid. Hence, Slc4a10 is a promising pharmacological target for the therapy of epilepsy or elevated intracranial pressure.cerebrospinal fluid ͉ epilepsy ͉ ion transport ͉ knockout mouse ͉ pH regulation

show abstract

“…Loss of space clamp is expected to be even smaller in the proximal parts of the dendrites (also recorded at a 50 m distance from the soma) than at the AIS. In the present context, it is notable that, in the whole-cell clamp experiments in which the calculated somatic E GABA is Ϫ68 mV (corrected for intracellular bicarbonate; E Cl of Ϫ77 mV) (Kaila et al, 1993;Kaila, 1994;Farrant and Kaila, 2007), the DGCs were obviously able to cope with part of this minor imposed load (7 mM Cl Ϫ ) even in the somatic compartment, and, hence, the measured somatic E GABA is more negative (Ϫ74.2 mV, corresponding to 4.9 mM intracellular Cl Ϫ ). A similar deviation of the measured intracellular Cl Ϫ from the calculated passive distribution was observed in the neocortical layer 2/3 pyramidal neurons.…”

Section: Methodsmentioning

confidence: 99%

“…However, the mere absence of KCC2 cannot account for the strikingly positive E GABA values at the AIS, because in the complete absence of Cl Ϫ transport, E GABA would achieve a level close to and only slightly more depolarized than the resting membrane potential (Kaila et al, 1993;Farrant and Kaila, 2007). Thus, the depolarizing GABA A receptor-mediated response at the AIS requires the presence of a Cl Ϫ uptake mechanism.…”

Section: Introductionmentioning

confidence: 99%

GABAergic Depolarization of the Axon Initial Segment in Cortical Principal Neurons Is Caused by the Na–K–2Cl Cotransporter NKCC1

Khirug

Yamada²,

Afzalov³

et al. 2008

J. Neurosci.

264

269

View full text Add to dashboard Cite

GABAergic terminals of axo-axonic cells (AACs) are exclusively located on the axon initial segment (AIS) of cortical principal neurons, and they are generally thought to exert a powerful inhibitory action. However, recent work (Szabadics et al., 2006) indicates that this input from AACs can be depolarizing and even excitatory. Here, we used local photolysis of caged GABA to measure reversal potentials (E GABA ) of GABA A receptor-mediated currents and to estimate the local chloride concentration in the AIS compared with other cellular compartments in dentate granule cells and neocortical pyramidal neurons. We found a robust axo-somato-dendritic gradient in which the E GABA values from the AIS to the soma and dendrites become progressively more negative. Data from NKCC1 Ϫ/Ϫ and bumetanide-exposed neurons indicated that the depolarizing E GABA at the AIS is set by chloride uptake mediated by the Na-K-2Cl cotransporter NKCC1. Our findings demonstrate that spatially distinct interneuronal inputs can induce postsynaptic voltage responses with different amplitudes and polarities as governed by the subcellular distributions of plasmalemmal chloride transporters.

show abstract

The role of bicarbonate in GABAA receptor‐mediated IPSPs of rat neocortical neurones.

Cited by 196 publications

References 40 publications

GABAergic synchronization in the limbic system and its role in the generation of epileptiform activity

GABAergic synchronization in the limbic system and its role in the generation of epileptiform activity

Mice with targeted Slc4a10 gene disruption have small brain ventricles and show reduced neuronal excitability

GABAergic Depolarization of the Axon Initial Segment in Cortical Principal Neurons Is Caused by the Na–K–2Cl Cotransporter NKCC1

Contact Info

Product

Resources

About