Allopregnanolone Enhances GABAergic Inhibition in Spinal Motor Networks

The neurosteroid allopregnanolone (ALLO) causes unconsciousness by allosteric modulation of γ-aminobutyric acid type A (GABAA) receptors, but its actions on the spinal motor networks are unknown. We are therefore testing the hypothesis that ALLO attenuates the action potential firing of spinal interneurons and motoneurons predominantly via enhancing tonic, but not synaptic GABAergic inhibition. We used video microscopy to assess motoneuron-evoked muscle activity in organotypic slice cultures prepared from the spinal cord and muscle tissue. Furthermore, we monitored GABAA receptor-mediated currents by performing whole-cell voltage-clamp recordings. We found that ALLO (100 nM) reduced the action potential firing of spinal interneurons by 27% and that of α-motoneurons by 33%. The inhibitory effects of the combination of propofol (1 µM) and ALLO on motoneuron-induced muscle contractions were additive. Moreover, ALLO evoked a tonic, GABAA receptor-mediated current (amplitude: 41 pA), without increasing phasic GABAergic transmission. Since we previously showed that at a clinically relevant concentration of 1 µM propofol enhanced phasic, but not tonic GABAergic inhibition, we conclude that ALLO and propofol target distinct subpopulations of GABAA receptors. These findings provide first evidence that the combined application of ALLO and propofol may help to reduce intraoperative movements and undesired side effects that are frequently observed under total intravenous anesthesia.

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Cholinergic Modulation of Sevoflurane Potency in Cortical and Spinal Networks In Vitro

Anesthesiology ◽

10.1097/01.anes.0000267598.65120.f2 ◽

2007 ◽

Vol 106 (6) ◽

pp. 1147-1155 ◽

Cited By ~ 17

Author(s):

Christian Grasshoff ◽

Berthold Drexler ◽

Harald Hentschke ◽

Horst Thiermann ◽

Bernd Antkowiak

Keyword(s):

Action Potential ◽

Gabaa Receptor ◽

Gabaa Receptors ◽

Receptor Function ◽

Action Potential Firing ◽

Newborn Mice ◽

Organophosphate Intoxication ◽

Spontaneous Action Potential ◽

Potential Firing ◽

Spontaneous Action

Background Victims of organophosphate intoxication with cholinergic crisis may have need for sedation and anesthesia, but little is known about how anesthetics work in these patients. Recent studies suggest that cholinergic stimulation impairs gamma-aminobutyric acid type A (GABAA) receptor function. Because GABAA receptors are major targets of general anesthetics, the authors investigated interactions between acetylcholine and sevoflurane in spinal and cortical networks. Methods Cultured spinal and cortical tissue slices were obtained from embryonic and newborn mice. Drug effects were assessed by extracellular voltage recordings of spontaneous action potential activity. Results Sevoflurane caused a concentration-dependent decrease in spontaneous action potential firing in spinal (EC50=0.17+/-0.02 mM) and cortical (EC50=0.29+/-0.01 mM) slices. Acetylcholine elevated neuronal excitation in both preparations and diminished the potency of sevoflurane in reducing action potential firing in cortical but not in spinal slices. This brain region-specific decrease in sevoflurane potency was mimicked by the specific GABAA receptor antagonist bicuculline, suggesting that (1) GABAA receptors are major molecular targets for sevoflurane in the cortex but not in the spinal cord and (2) acetylcholine impairs the efficacy of GABAA receptor-mediated inhibition. The latter hypothesis was supported by the finding that acetylcholine reduced the potency of etomidate in depressing cortical and spinal neurons. Conclusions The authors raise the question whether cholinergic overstimulation decreases the efficacy of GABAA receptor function in patients with organophosphate intoxication, thereby compromising anesthetic effects that are mediated predominantly via these receptors such as sedation and hypnosis.

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Propofol and Sevoflurane Depress Spinal Neurons In Vitro via Different Molecular Targets

Anesthesiology ◽

10.1097/00000542-200411000-00017 ◽

2004 ◽

Vol 101 (5) ◽

pp. 1167-1176 ◽

Cited By ~ 51

Author(s):

Christian Grasshoff ◽

Bernd Antkowiak

Keyword(s):

Spinal Cord ◽

Action Potential ◽

Gabaa Receptors ◽

Molecular Targets ◽

Glycine Receptors ◽

Spinal Neurons ◽

Action Potential Firing ◽

Spontaneous Action Potential ◽

Potential Firing ◽

Spontaneous Action

Background The capacity of general anesthetics to produce immobility is primarily spinally mediated. Recently, compelling evidence has been provided that the spinal actions of propofol involve gamma-aminobutyric acid type A (GABAA) receptors, whereas the contribution of glycine receptors remains uncertain. The relevant molecular targets of the commonly used volatile anesthetic sevoflurane in the spinal cord are largely unknown, but indirect evidence suggests a mechanism of action distinct from propofol. Methods The effects of sevoflurane and propofol on spontaneous action potential firing were investigated by extracellular voltage recordings from ventral horn interneurons in cultured spinal cord tissue slices obtained from embryonic rats (embryonic days 14-15). Results Propofol and sevoflurane reduced spontaneous action potential firing of neurons. Concentrations causing half-maximal effects (0.11 microm propofol, 0.11 mm sevoflurane) were lower than the median effective concentration immobility (1-1.5 microm propofol, 0.35 mm sevoflurane). At higher concentrations, complete inhibition of action potential activity was observed with sevoflurane but not with propofol. Effects of sevoflurane were mediated predominantly by glycine receptors (45%) and GABAA receptors (38%), whereas propofol acted almost exclusively via GABAA receptors (96%). Conclusions The authors' results suggest that glycine and GABAA receptors are the most important molecular targets mediating depressant effects of sevoflurane in the spinal cord. They provide evidence that sevoflurane causes immobility by a mechanism distinct from the actions of the intravenous anesthetic propofol. The finding that propofol acts exclusively via GABAA receptors can explain its limited capacity to depress spinal neurons in the authors' study.

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Development of Ionic Currents Underlying Changes in Action Potential Waveforms in Rat Spinal Motoneurons

Journal of Neurophysiology ◽

10.1152/jn.1998.80.6.3047 ◽

1998 ◽

Vol 80 (6) ◽

pp. 3047-3061 ◽

Cited By ~ 125

Author(s):

Bao-Xi Gao ◽

Lea Ziskind-Conhaim

Keyword(s):

Action Potential ◽

Cell Voltage ◽

Ionic Currents ◽

Repetitive Firing ◽

Delayed Rectifier ◽

Ionic Mechanism ◽

Spinal Motoneurons ◽

Action Potential Firing ◽

Voltage Gated ◽

Potential Firing

Gao, Bao-Xi and Lea Ziskind-Conhaim. Development of ionic currents underlying changes in action potential waveforms in rat spinal motoneurons. J. Neurophysiol. 80: 3047–3061, 1998. Differentiation of the ionic mechanism underlying changes in action potential properties was investigated in spinal motoneurons of embryonic and postnatal rats using whole cell voltage- and current-clamp recordings. Relatively slow-rising, prolonged, largely Na+-dependent action potentials were recorded in embryonic motoneurons, and afterdepolarizing potentials were elicited in response to prolonged intracellular injections of depolarizing currents. Action potential amplitude, as well as its rates of rise and repolarization significantly increased, and an afterhyperpolarizing potential (AHP) became apparent immediately after birth. Concurrently, repetitive action potential firing was elicited in response to a prolonged current injection. To determine the ionic mechanism underlying these changes, the properties of voltage-gated macroscopic Na+, Ca2+, and K+ currents were examined. Fast-rising Na+ currents ( I Na) and slow-rising Ca2+ currents ( I Ca) were expressed early in embryonic development, but only I Na was necessary and sufficient to trigger an action potential. I Na and I Ca densities significantly increased while the time to peak I Na and I Ca decreased after birth. The postnatal increase in I Na resulted in overshooting action potential with significantly faster rate of rise than that recorded before birth. Properties of three types of outward K+ currents were examined: transient type-A current ( I A), noninactivating delayed rectifier-type current ( I K), and Ca2+-dependent K+ current ( I K(Ca)). The twofold postnatal increase in I K and I K(Ca) densities resulted in shorter duration action potential and the generation of AHP. Relatively large I A was expressed early in neuronal development, but unlike I K and I K(Ca) its density did not increase after birth. The three types of K+ channels had opposite modulatory actions on action potential firing behavior: I K and I A increased the firing rate, whereas I K(Ca) decreased it. Our findings demonstrated that the developmental changes in action potential waveforms and the onset of repetitive firing were correlated with large increases in the densities of existing voltage-gated ion channels rather than the expression of new channel types.

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Zolpidem Activation of Alpha 1-Containing GABAA Receptors Selectively Inhibits High Frequency Action Potential Firing of Cortical Neurons

Frontiers in Pharmacology ◽

10.3389/fphar.2018.01523 ◽

2019 ◽

Vol 9 ◽

Cited By ~ 2

Author(s):

Elena Neumann ◽

Uwe Rudolph ◽

Daniel E. Knutson ◽

Guanguan Li ◽

James M. Cook ◽

...

Keyword(s):

Action Potential ◽

Gabaa Receptors ◽

High Frequency ◽

Cortical Neurons ◽

Action Potential Firing ◽

Potential Firing

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Enhancing the function of alpha5-subunit-containing GABAA receptors promotes action potential firing of neocortical neurons during up-states

European Journal of Pharmacology ◽

10.1016/j.ejphar.2013.01.034 ◽

2013 ◽

Vol 703 (1-3) ◽

pp. 18-24 ◽

Cited By ~ 11

Author(s):

Berthold Drexler ◽

Stefan Zinser ◽

Shengming Huang ◽

Michael M. Poe ◽

Uwe Rudolph ◽

...

Keyword(s):

Action Potential ◽

Gabaa Receptors ◽

Action Potential Firing ◽

Neocortical Neurons ◽

Up States ◽

Potential Firing

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Faculty Opinions recommendation of Silent synapses generate sparse and orthogonal action potential firing in adult-born hippocampal granule cells.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.729075669.793547388 ◽

2018 ◽

Author(s):

Linda Overstreet-Wadiche

Keyword(s):

Action Potential ◽

Granule Cells ◽

Action Potential Firing ◽

Silent Synapses ◽

Potential Firing

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Zinc Enhances the Inhibitory Effects of Strychnine-Sensitive Glycine Receptors in Mouse Hippocampal Neurons

Journal of Neurophysiology ◽

10.1152/jn.00500.2007 ◽

2007 ◽

Vol 98 (6) ◽

pp. 3666-3676 ◽

Cited By ~ 8

Author(s):

Hai Xia Zhang ◽

Liu Lin Thio

Keyword(s):

Action Potential ◽

Action Potentials ◽

Hippocampal Neurons ◽

Neuronal Excitability ◽

Hippocampal Slices ◽

Glycine Receptors ◽

Inhibitory Effects ◽

Action Potential Firing ◽

Embryonic Mouse ◽

Potential Firing

Although extracellular Zn2+ is an endogenous biphasic modulator of strychnine-sensitive glycine receptors (GlyRs), the physiological significance of this modulation remains poorly understood. Zn2+ modulation of GlyR may be especially important in the hippocampus where presynaptic Zn2+ is abundant. Using cultured embryonic mouse hippocampal neurons, we examined whether 1 μM Zn2+, a potentiating concentration, enhances the inhibitory effects of GlyRs activated by sustained glycine applications. Sustained 20 μM glycine (EC25) applications alone did not decrease the number of action potentials evoked by depolarizing steps, but they did in 1 μM Zn2+. At least part of this effect resulted from Zn2+ enhancing the GlyR-induced decrease in input resistance. Sustained 20 μM glycine applications alone did not alter neuronal bursting, a form of hyperexcitability induced by omitting extracellular Mg2+. However, sustained 20 μM glycine applications depressed neuronal bursting in 1 μM Zn2+. Zn2+ did not enhance the inhibitory effects of sustained 60 μM glycine (EC70) applications in these paradigms. These results suggest that tonic GlyR activation could decrease neuronal excitability. To test this possibility, we examined the effect of the GlyR antagonist strychnine and the Zn2+ chelator tricine on action potential firing by CA1 pyramidal neurons in mouse hippocampal slices. Co-applying strychnine and tricine slightly but significantly increased the number of action potentials fired during a depolarizing current step and decreased the rheobase for action potential firing. Thus Zn2+ may modulate neuronal excitability normally and in pathological conditions such as seizures by potentiating GlyRs tonically activated by low agonist concentrations.

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The thalamic low-threshold Ca 2+ potential: a key determinant of the local and global dynamics of the slow (<1 Hz) sleep oscillation in thalamocortical networks

Philosophical Transactions of The Royal Society A Mathematical Physical and Engineering Sciences ◽

10.1098/rsta.2011.0126 ◽

2011 ◽

Vol 369 (1952) ◽

pp. 3820-3839 ◽

Cited By ~ 14

Author(s):

Vincenzo Crunelli ◽

Adam C. Errington ◽

Stuart W. Hughes ◽

Tibor I. Tóth

Keyword(s):

Action Potential ◽

Slow Oscillation ◽

Global Dynamics ◽

Action Potential Firing ◽

Local And Global Dynamics ◽

Up States ◽

Potential Firing ◽

Low Threshold

During non-rapid eye movement sleep and certain types of anaesthesia, neurons in the neocortex and thalamus exhibit a distinctive slow (<1 Hz) oscillation that consists of alternating UP and DOWN membrane potential states and which correlates with a pronounced slow (<1 Hz) rhythm in the electroencephalogram. While several studies have claimed that the slow oscillation is generated exclusively in neocortical networks and then transmitted to other brain areas, substantial evidence exists to suggest that the full expression of the slow oscillation in an intact thalamocortical (TC) network requires the balanced interaction of oscillator systems in both the neocortex and thalamus. Within such a scenario, we have previously argued that the powerful low-threshold Ca 2+ potential (LTCP)-mediated burst of action potentials that initiates the UP states in individual TC neurons may be a vital signal for instigating UP states in related cortical areas. To investigate these issues we constructed a computational model of the TC network which encompasses the important known aspects of the slow oscillation that have been garnered from earlier in vivo and in vitro experiments. Using this model we confirm that the overall expression of the slow oscillation is intricately reliant on intact connections between the thalamus and the cortex. In particular, we demonstrate that UP state-related LTCP-mediated bursts in TC neurons are proficient in triggering synchronous UP states in cortical networks, thereby bringing about a synchronous slow oscillation in the whole network. The importance of LTCP-mediated action potential bursts in the slow oscillation is also underlined by the observation that their associated dendritic Ca 2+ signals are the only ones that inform corticothalamic synapses of the TC neuron output, since they, but not those elicited by tonic action potential firing, reach the distal dendritic sites where these synapses are located.

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pigkMutation underliesmachobehavior and affects Rohon-Beard cell excitability

Journal of Neurophysiology ◽

10.1152/jn.00355.2015 ◽

2015 ◽

Vol 114 (2) ◽

pp. 1146-1157 ◽

Cited By ~ 2

Author(s):

V. Carmean ◽

M. A. Yonkers ◽

M. B. Tellez ◽

J. R. Willer ◽

G. B. Willer ◽

...

Keyword(s):

Action Potential ◽

Sensory Neurons ◽

Sodium Current ◽

Genetic Defect ◽

Sensory Cells ◽

Loss Of Function ◽

Wild Type ◽

Action Potential Firing ◽

Potential Firing ◽

Touch Response

The study of touch-evoked behavior allows investigation of both the cells and circuits that generate a response to tactile stimulation. We investigate a touch-insensitive zebrafish mutant, macho (maco), previously shown to have reduced sodium current amplitude and lack of action potential firing in sensory neurons. In the genomes of mutant but not wild-type embryos, we identify a mutation in the pigk gene. The encoded protein, PigK, functions in attachment of glycophosphatidylinositol anchors to precursor proteins. In wild-type embryos, pigk mRNA is present at times when mutant embryos display behavioral phenotypes. Consistent with the predicted loss of function induced by the mutation, knock-down of PigK phenocopies maco touch insensitivity and leads to reduced sodium current (INa) amplitudes in sensory neurons. We further test whether the genetic defect in pigk underlies the maco phenotype by overexpressing wild-type pigk in mutant embryos. We find that ubiquitous expression of wild-type pigk rescues the touch response in maco mutants. In addition, for maco mutants, expression of wild-type pigk restricted to sensory neurons rescues sodium current amplitudes and action potential firing in sensory neurons. However, expression of wild-type pigk limited to sensory cells of mutant embryos does not allow rescue of the behavioral touch response. Our results demonstrate an essential role for pigk in generation of the touch response beyond that required for maintenance of proper INa density and action potential firing in sensory neurons.

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