Energy substrate availability as a determinant of neuronal resting potential, GABA signaling and spontaneous network activity in the neonatal cortex <i>in vitro</i>

Holmgren, Carl; Mukhtarov, Marat; Malkov, Anton; Popova, Irina; Bregestovski, Pìotr; Zilberter, Yuri

doi:10.1111/j.1471-4159.2009.06506.x

Cited by 78 publications

(125 citation statements)

References 86 publications

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“…S1A), in agreement with previously reported data (22). This early depolarizing action of GABA is not prevented by addition of the alternate energy substrate pyruvate (Table S1), in contrast to recent observations in both neocortex (11) and hippocampus (26).…”

Section: Gaba Switch Occurs Normally In Nicotinic Acetylcholine Recepcontrasting

confidence: 50%

Non–cell-autonomous factor induces the transition from excitatory to inhibitory GABA signaling in retina independent of activity

Barkis

Ford²,

Feller³

2010

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

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During development, the effect of activating GABA A receptors switches from depolarizing to hyperpolarizing. Several environmental factors have been implicated in the timing of this GABA switch, including neural activity, although these observations remain controversial. By using acutely isolated retinas from KO mice and pharmacological manipulations in retinal explants, we demonstrate that the timing of the GABA switch in retinal ganglion cells (RGCs) is unaffected by blockade of specific neurotransmitter receptors or global activity. In contrast to RGCs in the intact retina, purified RGCs remain depolarized by GABA, indicating that the GABA switch is not cell-autonomous. Indeed, purified RGCs cocultured with dissociated cells from the superior colliculus or cultured in media conditioned by superior collicular cells undergo a normal switch. Thus, a diffusible signal that acts independent of local circuit activity regulates the maturation of GABAergic inhibition in mouse RGCs.A lthough GABA is the principal inhibitory neurotransmitter in the mature CNS, it is a robust source of excitation during development that is important for many developmental processes (1-4). The transition from excitatory to inhibitory action of GABA has been observed in a number of neural circuits and in many vertebrate species (5, 6) and the primary mechanisms underlying the switch are fairly well understood (7-11; reviewed in refs. 12-14). However, whether the timing of the GABA switch is modulated by local circuit activity (8,(15)(16)(17)(18) or occurs independent of activity (19,20) and is therefore intrinsic to developmental program of the cell remains controversial.Retinal ganglion cells (RGCs) undergo a switch in their response to GABA during the first two postnatal weeks of development (21-23). In vivo recordings in zebrafish demonstrate that the timing of the GABA switch is critical for the timing of the development of light responses (24) and therefore might be linked to the onset of visual experience. Chronic blockade of GABA A receptors (GABA A Rs) in turtle retina prevents the normal maturation of spontaneous firing patterns termed retinal waves and the maturation of adult-like chloride gradients, implicating early GABA signaling in the normal maturation of inhibitory circuits in retina (15). Based on these results, it has been proposed that the maturation of GABAergic inhibition is influenced by local network activity and is critical for the cessation of retinal waves (25).Here we explore factors that influence the timing of the GABA switch in mouse RGCs. By using three different preparations, we test whether the timing of the GABA switch is regulated by (i) local circuit activity in the retina, (ii) an intrinsic developmental program, or (iii) a diffusible, non-cell autonomous factor that operates independent of retinal activity. Results GABA Switch Occurs Normally in Nicotinic Acetylcholine Receptor-KORetinas. The timing of the GABA switch in retinal neurons in the ganglion cell layer (GCL) was determined by calcium imagi...

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Section: Gaba Switch Occurs Normally In Nicotinic Acetylcholine Recepcontrasting

confidence: 50%

Non–cell-autonomous factor induces the transition from excitatory to inhibitory GABA signaling in retina independent of activity

Barkis

Ford²,

Feller³

2010

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

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“…GABAmediated excitation during early development is a central component of this concept because GABAergic synapses are formed before glutamatergic contacts (Ben-Ari et al, 2007) showing that an interference with intracellular Cl Ϫ accumulation at an immature stage perturbs both the proper morphological maturation of neurons and their functional synapse development (Cancedda et al, 2007;Pfeffer et al, 2009). Therefore, an absence of GABA-mediated excitation (Rheims et al, 2009;Holmgren et al, 2010) (Yuste and Katz, 1991;Owens et al, 1996;Yamada et al, 2004). This seems to be plausible, since a broad-spectrum antagonist of VGCCs abolished the responses almost completely (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…Sagittal slices (300 m) comprising the occipital cortex were cut on a vibratome and stored for at least 1 h before their use at room temperature in artificial CSF (ACSF) containing the following (in mM): 125 NaCl, 4 KCl, 10 glucose, 1.25 NaH 2 PO 4 , 25 NaHCO 3 , 2 CaCl 2 , and 1 MgCl 2 , bubbled with 5% CO 2 /95% O 2 , pH 7.4. In subsets of experiments, an energy substrate-enriched ACSF (eACSF) was used containing (in mM): 126 NaCl, 3.5 KCl, 1.2 NaH 2 PO 4 , 25 NaHCO 3 , 1.3 MgCl 2 , 2 CaCl 2 , 5 choline chloride, 5 glucose, 2 DL-sodium ␤-hydroxybutyrate, 5 sodium pyruvate, pH 7.4 (Holmgren et al, 2010).…”

Section: Methodsmentioning

confidence: 99%

“…Despite the wealth of data supporting the hypothesis of a depolarizing/excitatory mode of GABA action during early development, this concept has been seriously questioned. Recently, it was reported that GABA-mediated depolarization in immature neocortical pyramidal cells could be due to an inadequate energy supply of the in vitro preparation (Rheims et al, 2009;Holmgren et al, 2010). More precisely, Rheims et al (2009) found that addition of the ketone body DL-␤-hydroxybutyrate to the extracellular medium abolished excitatory effects of GABA.…”

Section: Introductionmentioning

confidence: 99%

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GABA Depolarizes Immature Neocortical Neurons in the Presence of the Ketone Body β-Hydroxybutyrate

Kirmse¹,

Witte²,

Holthoff³

2010

J. Neurosci.

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A large body of evidence suggests that the neurotransmitter GABA undergoes a developmental switch from being predominantly depolarizing-excitatory to predominantly hyperpolarizing-inhibitory. Recently published data, however, point to the possibility that the presumed depolarizing mode of GABA action during early development might represent an artifact due to an insufficient energy supply of the in vitro preparations used. Specifically, addition of the ketone body DL-␤-hydroxybutyrate (␤HB) to the extracellular medium was shown to prevent GABA from exerting excitatory effects. Applying a complementary set of minimally invasive optical and electrophysiological techniques in brain slices from neonatal mice, we investigated the effects of ␤HB on GABA actions in immature cells of the upper cortical plate. Fluorescence imaging revealed that GABA-mediated somatic [Ca 2ϩ ] transients, that required activation of GABA A receptors and voltage-gated Ca 2ϩ channels, remained unaffected by ␤HB. Cell-attached current-clamp recordings showed that, in the presence of ␤HB, GABA still induced a membrane potential depolarization. To estimate membrane potential changes quantitatively, we used cell-attached recordings of voltage-gated potassium currents and demonstrated that the GABA-mediated depolarization was independent of supplementation of the extracellular solution with ␤HB. We conclude that, in vitro, GABA depolarizes immature cells of the upper cortical plate in the presence of the ketone body ␤HB. Our data thereby support the general concept of an excitatory-to-inhibitory switch of GABA action during early development.

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“…Although criticism [26][27][28] concerning the concept of depolarizing GABA has been largely invalidated in recent years [29][30][31][32][33] , supportive evidence from the intact mammalian brain is still lacking. In favour of a depolarizing GABA action in nonmammalian species in vivo, iontophoretic application of GABA or glycine was found to evoke somatic Ca 2 þ transients (CaTs) in spinal neurons of zebrafish larvae 34 .…”

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confidence: 99%

GABA depolarizes immature neurons and inhibits network activity in the neonatal neocortex in vivo

et al. 2015

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A large body of evidence from in vitro studies suggests that GABA is depolarizing during early postnatal development. However, the mode of GABA action in the intact developing brain is unknown. Here we examine the in vivo effects of GABA in cells of the upper cortical plate using a combination of electrophysiological and Ca 2 þ -imaging techniques. We report that at postnatal days (P) 3-4, GABA depolarizes the majority of immature neurons in the occipital cortex of anaesthetized mice. At the same time, GABA does not efficiently activate voltage-gated Ca 2 þ channels and fails to induce action potential firing. Blocking GABA A receptors disinhibits spontaneous network activity, whereas allosteric activation of GABA A receptors has the opposite effect. In summary, our data provide evidence that in vivo GABA acts as a depolarizing neurotransmitter imposing an inhibitory control on network activity in the neonatal (P3-4) neocortex.

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Energy substrate availability as a determinant of neuronal resting potential, GABA signaling and spontaneous network activity in the neonatal cortex in vitro

Cited by 78 publications

References 86 publications

Non–cell-autonomous factor induces the transition from excitatory to inhibitory GABA signaling in retina independent of activity

Non–cell-autonomous factor induces the transition from excitatory to inhibitory GABA signaling in retina independent of activity

GABA Depolarizes Immature Neocortical Neurons in the Presence of the Ketone Body β-Hydroxybutyrate

GABA depolarizes immature neurons and inhibits network activity in the neonatal neocortex in vivo

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