Rapid Seizure-Induced Reduction of Benzodiazepine and Zn2+ Sensitivity of Hippocampal Dentate Granule Cell GABAA Receptors

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Volume 17, Number 19, Issue of October 1, 1997 pp. 7532-7540
Copyright ©1997 Society for Neuroscience

Rapid Seizure-Induced Reduction of Benzodiazepine and Zn²⁺ Sensitivity of Hippocampal Dentate Granule Cell GABA_A Receptors

Jaideep Kapur¹ and Robert L. Macdonald¹^,²
Departments of ¹ Neurology and ² Physiology, University of Michigan Medical Center, Ann Arbor, Michigan 48104-1687

ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
FOOTNOTES
REFERENCES

ABSTRACT

Fast synaptic inhibition in the forebrain is mediated primarily by GABA acting on GABA_A receptors (GABARs). GABARs are regulatedby numerous positive (barbiturates, benzodiazepines, and neurosteroids)and negative (picrotoxin, bicuculline, and Zn²⁺) allosteric modulators. The sensitivity of GABARs to GABA andto allosteric modulators changes gradually during normal development,during development of chronic epilepsy, and after prolonged exposureto GABAR agonists. Here we report the development of rapid functionalplasticity of GABARs occurring over 45 min of continuous seizures(status epilepticus) in rats. Seizures induced in rats by administrationof lithium followed by pilocarpine were readily terminated bythe benzodiazepine diazepam when administered early during theseizures (after 10 min of seizures). However, during status epilepticus,there was a substantial reduction of diazepam potency for terminationof the seizures. To determine whether the loss of sensitivityof the animals to diazepam was caused by an alteration of GABARfunctional properties, we obtained whole-cell GABAR currents fromhippocampal dentate granule cells isolated acutely from controlrats and from rats undergoing status epilepticus. GABAR propertieswere characterized by determining GABA sensitivity and the sensitivityof GABARs to regulation by benzodiazepines, barbiturates, andZn²⁺. When compared with those from naive controls, GABAR currentsfrom rats undergoing status epilepticus were less sensitive todiazepam and Zn²⁺ but retained their sensitivity to GABA and pentobarbital. Weconclude that the prolonged seizures of status epilepticus rapidlyaltered the functional properties of hippocampal dentate granulecell GABARs.
Key words: status epilepticus; seizures; GABA; diazepam; benzodiazepines; zinc; GABA_A receptors; pentobarbital; barbiturates; dentate gyrus; granule cells; hippocampus

INTRODUCTION

Fast inhibitory synaptic transmission in the CNS is mediated primarily by the neurotransmitter GABA interacting with postsynapticGABA_A receptors (GABARs). GABARs form chloride ion channels, andGABAR currents are regulated by numerous positive and negativeallosteric modulators, including barbiturates, benzodiazepines,neurosteroids, penicillin, picrotoxin, and bicuculline, and Zn²⁺. GABARs are pentameric combinations of several different familiesof GABAR subunits with multiple subunit subtypes of $alpha$ (1-6), $beta$ (1-4), $gamma$ (1-4), and $delta$ . GABAR pharmacological properties dependon their subunit subtype composition (Macdonald and Olsen, 1994).For example, the sensitivity of GABARs to benzodiazepines requiresthe presence of a $gamma$ subunit, and the relative affinity for manybenzodiazepine receptor agonists depends on the $alpha$ subtype incorporatedinto the receptor. In contrast, sensitivity to Zn²⁺ is reduced by the presence of a $gamma$ subunit, but relative sensitivityto Zn²⁺ also depends on the $alpha$ subtype incorporated into the receptor.GABAR functional properties have been shown to be modified undernormal and pathological conditions. GABAR properties change graduallyduring normal development, during development of chronic epilepsy,and after prolonged exposure to GABAR agonists and GABAR regulatorydrugs (Rabow et al., 1995).

Status epilepticus is a rapidly developing, prolonged epileptic state that occurs when a single seizure lasts at least 30min or intermittent seizures last at least 30 min between whichthe patient does not regain consciousness (Commission on Classificationand Terminology of the International League against Epilepsy,1981; DeLorenzo, 1990). During status epilepticus, seizures rapidlyalter brain function, allowing continuation of seizures. The hippocampal-parahippocampalcircuit contains neurons and synaptic connections that are wellsuited to the occurrence of rapid plasticity that facilitatesthe self-sustaining nature of prolonged status epilepticus (Lothmanet al., 1991). Prolonged hippocampal seizures reduce GABAR inhibition(Kapur et al., 1989, 1994; Sloviter, 1991), and this reductionof inhibition is correlated with the development of status epilepticus(Kapur and Lothman, 1989). The cellular mechanisms underlyingthis loss of GABAergic inhibition during status epilepticus seemto be postsynaptic, including reduced potency and efficacy ofGABA in activating chloride channels and diminished driving forcefor the GABAR currents (Kapur and Coulter, 1995). Thus one hypothesisexplaining the self-sustaining nature of status epilepticus isthat prolonged seizures produce a progressive reduction of GABARinhibition in the hippocampus that leads to the development ofstatus epilepticus.

In humans, status epilepticus is treated with benzodiazepines, including diazepam, lorazepam, and midazolam and with barbiturates,including phenobarbital and pentobarbital, all of which exertan anticonvulsant effect by acting on the GABARs (Macdonald andKelly, 1995). Interestingly, both in humans and in experimentalanimals, benzodiazepines are efficacious in early but not latestatus epilepticus, which in humans paradoxically responds tobarbiturates (Yaffe and Lowenstein, 1993). Thus both experimentalanimal and human data suggest that the functional properties ofhippocampal GABARs are rapidly modified during status epilepticus.We tested this hypothesis directly. The potency and efficacy ofbenzodiazepines in treating the early and late phases of statusepilepticus in rats were compared. Whole-cell GABAR currents inhippocampal dentate granule cells acutely isolated from rats undergoingstatus epilepticus were less sensitive to diazepam and Zn²⁺ compared with currents in naive litter mates but retained theirGABA and pentobarbital sensitivity. We conclude that prolongedseizures rapidly alter the functional properties of hippocampalGABARs.

MATERIALS AND METHODS
Whole animal experiments. Status epilepticus was induced in Sprague Dawley rats of both sexes (230-255 gm; Harlan SpragueDawley, Indianapolis, IN) by intraperitoneal injection of LiClat 3 mEq/kg followed 20 hr later by pilocarpine at 50 mg/kg (Honcharet al., 1983). After pilocarpine injection, the rats were observedcontinuously for occurrence of behavioral seizures. The time toonset of behavioral seizures was recorded, and behavioral seizureswere observed. Behavioral seizures evoked by lithium and pilocarpinewere as described by Racine (1972). Seizure termination was definedas the absence of forelimb clonus or falling, facial twitching,and stop-and-stare activity. Additionally, resumption of normalbehavior within 30 min of drug injection was assessed. Diazepamwas administered 10 or 45 min after pilocarpine injection. Thefraction of rats that stopped having seizures within 5 min ofdiazepam injection was plotted against the log of diazepam dose.The data were fitted to a sigmoidal dose-response curve with themaximum fixed to 100% and the minimum to 0%. The ED₅₀ values werederived from the equation that best fit the data.

Cell isolation. Cells were isolated from rats undergoing 45 min of seizures or from controls consisting of naive rats or saline-injectedanimals of the same age. All experiments were performed on dentategranule cells isolated according to the method described originallyby Kay and Wong (1986) and later modified by Coulter et al. (1990).The brain was dissected free, and the region containing the hippocampuswas blocked and chilled in an oxygenated 1,4-piperazinediethanesulfonicacid (PIPES)-buffered medium (4°C) for 1 min. The PIPES buffersolution contained (in mM) NaCl, 120; KCL, 2.5; CaCl₂, 1.5; MgCl₂,1; D-glucose, 25; and PIPES, 20, pH 7.0. After blot drying, thebrain was mounted on a vibratome stage, and 500 µm coronal sectionscontaining the hippocampus were cut. The sections were allowedto recover in oxygenated (95% 0₂/5% CO₂) PIPES buffer for 30-60min. Hippocampal sections were then incubated with oxygenatedSigma type XXIII (Sigma, St. Louis, MO) protease enzyme in thebuffer at 32°C for 30-45 min. The dentate gyrus was dissectedout and cut into 0.5 mm cubes that were triturated in a cold (4°C)PIPES-buffered medium in fire-polished glass pipettes to isolateneurons. The isolated neurons were plated on poly-L-lysine-coated35 mm polystyrene petri dishes (Corning, Corning, NY), and therecordings were made within 1 hr of isolation.

Whole-cell recording. Whole-cell GABAR currents were recorded from hippocampal dentate granule cells acutely isolated from28- to 35-d-old rats using the technique described by Hamill etal. (1981). The extracellular recording solution consisted of(in mM) NaCl, 142; CaCl₂, 1.0; KCl, 8; MgCl₂, 6; glucose, 10;and HEPES, 10, pH-adjusted to 7.4; osmolarity was 310-320 mOsm(all reagents from Sigma). Glass recording patch pipettes werefilled with a solution consisting of the following (in mM): Trizmaphosphate (dibasic), 115; Trizma base, 30; EGTA, 11; MgCl₂, 2;and CaCl₂, 0.5, pH 7.35. Recording pipettes also contained ATP(2 mM) unless otherwise specified. All recordings were obtainedat room temperature (24°C). With a bathing solution containinga chloride concentration of 164 mM and whole-cell recording pipettescontaining a 5 mM chloride ion solution, the chloride ion concentrationgradient produced a chloride ion equilibrium potential (E_Cl) of $-$ 76 mV. Granule cells were voltage-clamped to 0 mV, and thus,application of GABA produced outward currents. Patch pipettes(resistance of 6-10 M $Omega$ ) were pulled on a Flaming-Brown P-87 pullerby a four-stage pull. Currents were recorded with an Axopatch1-D amplifier and low-pass filtered at 2 kHz with an eight poleBessel filter before digitization, storage, and display. Currentswere displayed on a Gould 2400S chart recorder, and peak whole-cellcurrents were measured manually from the chart paper. Currentswere also recorded on a hard disk using the Axotape program (AxonInstruments) (digitized at 208 Hz) and on a videocassette taperecorder (Sony SL-HF360) via a digital audio processor (Sony PCM-501ES; 14 bit, 44 kHz).

Drug application. GABA, pentobarbital, and ZnCl₂ dissolved in extracellular solution were applied to neurons using a modifiedU-tube "multipuffer" rapid application system (Greenfield andMacdonald, 1996) with the tip of the application pipette placed100-200 µm from the cell. Diazepam was dissolved first in dimethylsulfoxide(DMSO) and then diluted in extracellular buffer with the finalDMSO dilution being at least 1:50,000. GABA, diazepam, pentobarbital,and ZnCl₂ were obtained from Sigma.

Data analysis. The magnitude of the enhancement or inhibition of GABAR current by a drug was measured by dividing the peakamplitude of GABAR current elicited in the presence of a givenconcentration of the drug and GABA by the peak amplitude of controlcurrent elicited by GABA alone and by multiplying the fractionby 100 to express it as percent control. Thus the control responsewas 100%. Peak GABAR currents at various drug concentrations werefitted to a sigmoidal function using a four parameter logisticequation (sigmoidal concentration-response) with a variable slope.The equation used to fit the concentration-response relationshipwas:

where I was the GABAR current at a given GABA concentration, and I_(max) was the maximal GABAR current. Maximal current andconcentration-response curves were obtained after pooling datafrom all neurons tested for GABA and for all drugs. The curve-fittingalgorithm minimized the sum of the squares of the actual distanceof points from the curve. Convergence was reached when two consecutiveiterations changed the sum of squares by <0.01%. The curve fitwas performed on an IBM-compatible personal computer using theprogram Prism (Graph Pad, San Diego, CA). All data are presentedas mean ± SEM.

RESULTS

Benzodiazepine treatment of brief and prolonged seizures
Behavioral seizures began 3-5 min after the injection of pilocarpine. Behavioral seizures during lithium- and pilocarpine-inducedstatus epilepticus were characterized by immobility, repetitivechewing, head nodding, vibrisal twitching, forelimb clonus withor without rearing, and falling as described previously (Racine,1972; Walton and Treiman, 1988). Four rats were not treated withan anticonvulsant drug, and they continued to have seizures for2 hr. After 10 min of seizures, diazepam (20 mg/kg) terminatedseizures in all treated animals (n = 3). However, after 45 minof seizures (status epilepticus), diazepam (20 mg/kg) terminatedthe seizures in none of the animals (n = 3). Seizure terminationwas defined as the absence of behavioral convulsion, facial twitching,and stop-and-stare activity. Additionally, resumption of normalbehavior within 30 min of drug injection was assessed.

A detailed diazepam dose-response (fraction of animals becoming seizure free) analysis was performed using a total of 30 rats.Increasing doses of diazepam from 2 to 20 mg/kg were administeredafter 10 min of seizures; five rats were treated with diazepamat 2 mg/kg, and three rats each were treated with diazepam at7.5, 10, and 20 mg/kg. After 45 min of seizures, three rats eachwere treated with diazepam at 20, 30, 50, and 100 mg/kg. At highdoses of diazepam (50 and 100 mg/kg), behavioral seizures seemedterminated, but rats were extremely sedated, and resumption ofnormal activity did not occur. The dose-response data were fitto a sigmoidal dose-response relationship, and the ED₅₀ valuesfor diazepam control of behavioral seizures after 10 and 45 minof seizures were derived. The dose-response curve showed thatthe ED₅₀ for diazepam-induced termination of seizures shiftedfrom 4.2 mg/kg when administered after 10 min of continuous seizuresto 40 mg/kg when administered after 45 min of continuous seizures(Fig. 1).
Fig. 1. Diazepam was effective in controlling brief (10 min) seizures but lost efficacy after prolonged (45 min) seizures. Seizureswere induced in 70-150 gm rats by intraperitoneal injection ofLiCl at 3 mEq/kg followed 16-24 hr later by intraperitoneal injectionof pilocarpine at 50 mg/kg. Behavioral seizures started within1-5 min in all rats. Diazepam was administered 10 min (filledboxes, solid line; n = 14) or 45 min (filled circles, dashed line;n = 12) after pilocarpine injection. The percent of rats thatstopped having seizures within 5 min of diazepam injection wasplotted against the log of the diazepam dose. The data were fittedto a sigmoidal dose-response curve with the maximum fixed to 100%and the minimum to 0%. The ED₅₀ values were derived from the equationthat best fit the data.
[View Larger Version of this Image (21K GIF file)]

Because diazepam exerts its anticonvulsant effect primarily by enhancing GABAergic inhibition by acting on GABARs (Macdonaldet al., 1992), we hypothesized that seizures altered the functionalproperties of GABARs. The seizures could potentially alter themodulation of GABAR by various drugs, such as enhancement by benzodiazepines,barbiturates, and neurosteroids and antagonism by penicillin,picrotoxin, bicuculline, and Zn²⁺. We characterized GABAR currents recorded from acutely isolatedhippocampal dentate granule cells, their potentiation by benzodiazepinesand barbiturates, and their inhibition by Zn²⁺.

GABAR currents recorded from acutely isolated hippocampal dentate granule cells
Whole-cell voltage-clamp recordings were made from dentate granule cells (Kay and Wong, 1986; Oh et al., 1995) acutely isolatedfrom control rats or from same-age rats who had 45 min of continuousseizures (status epilepticus). When access was initially establishedin granule cells from control rats, GABAR currents evoked by 10µM GABA increased slightly and became stable in 2-4 min (run-up)(Fig. 2A). The stable response compared with the first responseincreased 174 ± 47% (n = 4) (Fig. 3). In contrast, GABAR currentsevoked from hippocampal neurons from animals undergoing statusepilepticus required 10 min to stabilize (Fig. 2B), and the run-upwas substantially larger (374 ± 66%; n = 5; p < 0.05) (Fig. 3).
Fig. 2. Stabilization of GABAR currents after access. GABAR currents elicited immediately on access from dentate granule cells. Traceswere from two neurons, the top from a cell isolated from a controlanimal and the bottom from an animal undergoing status epilepticus.The durations of GABA application were indicated by horizontalbars. Two minutes elapsed between each GABA application. A, GABARcurrents elicited from hippocampal dentate granule cells isolatedfrom control animals rapidly increased to a relatively stableamplitude. B, GABAR currents elicited from hippocampal dentategranule cells isolated from animals undergoing status epilepticustook longer to stabilize and showed a greater increase in amplitude.
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Fig. 3. Run-up of GABAR currents after access. Granule cell GABAR peak currents were normalized to the initial current evoked by 10µM GABA after access. Means ± SEMs of peak normalized GABAR currentsfrom five neurons from animals undergoing status epilepticus andfour neurons from control animals were plotted.
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Once stable responses to 10 µM GABA were obtained, GABA was applied to granule cells at concentrations ranging from 1 to 1000µM (Fig. 4). For each of the groups, data from individual cellswere pooled and fitted to a sigmoidal logistic equation. In neuronsfrom control animals, the mean GABA EC₅₀ for GABARs was 50 ± 20µM (n = 17), similar to that in neurons from animals undergoingstatus epilepticus, 33 ± 14 µM (n = 9; p > 0.05). The maximalGABAR current in cells from control animals was 962 ± 109 pA (n= 19), similar to that in cells from animals undergoing statusepilepticus, 820 ± 188 pA (n = 9). Thus after status epilepticus,there was increased run-up of GABAR currents after initial access,but once stable currents had been obtained, the potency and efficacyof GABA on dentate granule cell GABARs was similar to those inneurons from control animals. Modulation of GABAR currents wasstudied in dentate granule cells isolated from control rats andfrom those undergoing status epilepticus after stabilization ofcurrents.
Fig. 4. GABA concentration dependency. GABA concentration and normalized GABAR peak current relationships were plotted for 17 neuronsisolated from control animals and for 9 neurons isolated fromanimals undergoing status epilepticus. Concentration-responsedata were obtained after stabilization of currents. Each pointrepresented the mean of normalized peak currents, and the errorbars showed SEMs. The line was the best fit of data to a sigmoidalfunction. The EC₅₀ and I_max were derived from the equation forthe sigmoidal function that best fitted the data.
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Diazepam enhancement of GABAR currents
In hippocampal dentate granule cells from control animals, when 10 µM GABA was coapplied with 300 nM diazepam, GABAR currentswere enhanced in all neurons by 68 ± 10% (n = 6) (Fig. 5A). Incontrast, in dentate granule cells from animals undergoing statusepilepticus, 300 nM diazepam inconsistently enhanced 6 or 10 µMGABA-evoked GABAR currents by 10 ± 6% (n = 5; p < 0.001; groupedt test) (Fig. 5B).
Fig. 5. Diazepam enhancement of GABAR currents in dentate granule cells from control animals and in cells isolated from rats after45 min of seizures. Diazepam at 300 nM enhanced GABAR currentin dentate granule cells from control animals but did not enhancecurrent in cells isolated from rats after 45 min of seizures.The traces are from two different neurons. Horizontal bars showedthe duration of application of the drug. A, Diazepam (300 nM)was applied with 10 µM GABA to a dentate granule cell from a controlanimal. B, Diazepam (300 nM) was applied with 6 µM GABA to a granulecell isolated from a rat after status epilepticus. A lower concentrationof GABA was used to compensate for a small leftward shift of theGABA concentration-response curve in cells from animals undergoingstatus epilepticus (equipotent GABA concentration).
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Diazepam concentration-response curves were obtained for enhancement of GABAR currents from neurons from both naive animalsand from animals subjected to status epilepticus. In neurons fromnaive animals, 1 or 3 µM diazepam elicited maximal enhancementof GABAR currents, whereas in neurons from rats undergoing statusepilepticus, 3 µM diazepam elicited more enhancement of GABARcurrents than did 1 µM diazepam. Because diazepam causes a leftwardshift of the GABA concentration-response curve, the same amountof diazepam will cause more enhancement of GABAR currents if appliedwith a lower GABA concentration. Additionally, the GABA EC₅₀ wasslightly (but not statistically significantly) left-shifted ingranule cells acutely isolated from rats undergoing status epilepticuswhen compared with the value in controls. In this situation, itwas important to use equipotent and not equal GABA concentrations.In four neurons from rats undergoing status epilepticus, varyingconcentrations of diazepam were coapplied with 6 µM (instead of10 µM) GABA; however the diazepam EC₅₀ and maximal enhancementin these experiments were similar to those with diazepam coappliedwith 10 µM GABA. The data from these experiments were pooled.In neurons from control animals, 1 µM diazepam enhanced GABARcurrents by 92 ± 6% (n = 6), but in neurons from animals undergoingstatus epilepticus, 3 µM diazepam only enhanced GABAR currentsby 51 ± 8% (n = 5; p < 0.05; grouped t test) (Fig. 6). The EC₅₀for diazepam enhancement of GABAR currents in neurons from controlanimals was 195 ± 12 nM, and the EC₅₀ in neurons from animalsundergoing status epilepticus was 4.4 ± 0.25 µM (Fig. 6). Thusthe prolonged seizures of status epilepticus reduced the potencyand efficacy of diazepam for enhancement of granule cell GABARcurrents.
Fig. 6. Diazepam concentration-dentate granule cell GABAR current enhancement relationships. Diazepam concentration-response curveswere obtained for neurons isolated from control animals (filledboxes, solid line; n = 9) and for neurons isolated from animalsundergoing status epilepticus (filled circles, dashed line; n= 12). Higher concentrations of diazepam inhibited GABAR currentas reported previously (De Deyn and Macdonald, 1988).
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Zn²⁺ inhibition of GABAR currents
Because Zn²⁺ modulation of recombinant GABAR currents varies inversely with benzodiazepine sensitivity (Draguhn et al., 1990;Smart et al., 1991), Zn²⁺ inhibition of granule cell GABAR currents was studied. Zn²⁺ was less potent in inhibiting GABAR currents recorded from granulecells isolated from animals undergoing status epilepticus thanfrom control granule cells. In neurons from control animals, GABARcurrents were inhibited 59 ± 4% (n = 8) by 100 µM Zn²⁺ (Fig. 7A), but in neurons isolated from animals undergoing statusepilepticus, the inhibition was reduced to 39 ± 6% (n = 6; p <0.05; grouped t test) (Fig. 7B).
Fig. 7. Zn²⁺ inhibition of GABAR currents in dentate granule cells from control animals and from animals undergoing status epilepticus.Zn²⁺ (100 µM) inhibited GABAR currents in dentate granule cells fromcontrol animals more than it did in granule cells from animalsundergoing status epilepticus. The traces are from two differentneurons. Zn²⁺ (100 µM) was coapplied with 30 µM GABA. Horizontal bars showthe duration of application of the drug. A, Traces from a dentategranule cell isolated from a control animal. B, Traces from agranule cell isolated from an animal undergoing status epilepticus.
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Zn²⁺, ranging in concentration from 1 to 1000 µM, was coapplied with GABA to define the mechanism of the reduced Zn²⁺ block (Fig. 8). In dentate granule cells from control rats, GABARcurrents were reduced by Zn²⁺ in a concentration-dependent manner with an IC₅₀ of 30 ± 3.6µM (n = 12). In dentate granule cells isolated from animals undergoingstatus epilepticus, the IC₅₀ of Zn²⁺ inhibition of GABAR currents was 123 ± 15 µM (n = 10; p < 0.01;grouped t test). The maximal inhibition of GABAR currents by Zn²⁺ was unchanged (78 ± 3% in neurons from control animals and 90± 16% in neurons from animals undergoing status epilepticus).Thus the prolonged seizures of status epilepticus reduced thepotency of Zn²⁺ without altering the efficacy of inhibition of granule cell GABARcurrents.
Fig. 8. Zn²⁺ concentration-dentate granule cell GABAR current reduction relationships. Zn²⁺ concentration-dentate granule cell GABAR current inhibition relationshipswere obtained from neurons isolated from control animals (filledboxes, solid line; n = 12) and from neurons isolated from animalsundergoing status epilepticus (filled circles, dashed line; n= 12). The lines were the best fit of the data to a sigmoidalfunction. The IC₅₀ and Hill slope (n_H) were derived fromthe equation for the sigmoidal function that best fitted the data.
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Pentobarbital enhancement of GABAR currents
In neurons from control animals, GABAR currents elicited by 10 µM GABA were enhanced 77 ± 7% (n = 6) by 30 µM pentobarbital(Fig. 9A), whereas in neurons from animals undergoing status epilepticus,GABAR currents elicited by 10 µM GABA were enhanced 62 ± 11% (n= 3) by 30 µM pentobarbital (Fig. 9B) (p > 0.05; grouped t test).
Fig. 9. Pentobarbital enhancement of GABAR currents from dentate granule cells from control animals and from cells isolated from animalsundergoing status epilepticus. Pentobarbital (30 µM) equally enhancedGABAR currents in dentate granule cells from control animals andin granule cells from animals undergoing status epilepticus. Thetraces are from two different neurons. Pentobarbital (30 µM) wascoapplied with 10 µM GABA. Horizontal bars show the duration ofapplication of the drug. A, Traces from a dentate granule cellisolated from a control animal. B, Traces from a granule cellisolated from an animal undergoing status epilepticus.
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Concentration-response curves were obtained by coapplying 1-300 µM pentobarbital with 10 µM GABA to neurons obtained fromcontrol animals and from animals undergoing status epilepticus(Fig. 10). In dentate granule cells from control animals, the pentobarbitalEC₅₀ was 42 ± 15 µM (n = 6), and in neurons from animals undergoingstatus epilepticus, the pentobarbital EC₅₀ was not significantlydifferent (36 ± 8 µM; n = 6) (Fig. 10). Maximal enhancement ofGABAR currents by pentobarbital in neurons from control rats (190± 55%) and in neurons from animals undergoing status epilepticus(158 ± 20%) were not significantly different (p > 0.05; groupedt test). Thus, the prolonged seizures of status epilepticus didnot alter the efficacy or potency of pentobarbital enhancementof GABAR currents in dentate granule cells.
Fig. 10. Pentobarbital concentration-dentate granule cell GABAR current enhancement relationships. Pentobarbital concentration-dentategranule cell GABAR current enhancement relationships were obtainedfor neurons isolated from control animals (filled boxes, solidline; n = 7) and for neurons isolated from animals undergoingstatus epilepticus (filled circles, dashed line; n = 6). The lineswere the best fit of the data to a sigmoidal function. The EC₅₀and Hill slope were derived from the equation for the sigmoidalfunction that best fitted the data.
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DISCUSSION

Conclusions
This study demonstrated that the prolonged seizures of status epilepticus reduced the potency but not the efficacy of thebenzodiazepine diazepam in terminating seizures. Diazepam andZn²⁺ sensitivity of hippocampal dentate granule cell GABARs were rapidlyand selectively altered by the prolonged seizures. In contrast,the GABA and barbiturate sensitivities of GABARs were unaffected.These findings demonstrate a novel form of rapidly developingfunctional plasticity of GABARs and may explain in part the observationthat status epilepticus becomes more difficult to treat the longerits duration at the time treatment begins.

Diazepam loses effectiveness in the treatment of status epilepticus
This study demonstrated that the prolonged seizures of status epilepticus reduced the ability of diazepam to terminate statusepilepticus. This refractoriness to diazepam resulted from theloss of diazepam potency but not of diazepam efficacy. This phenomenonof refractoriness to diazepam has been reported previously inhumans (Yaffe and Lowenstein, 1993) and rats (Walton and Treiman,1988). Several possible mechanisms can be hypothesized to explainthe loss of diazepam effectiveness in the treatment of prolongedseizures of status epilepticus; seizures may become more intense,there may be enhanced excitatory transmission, or there may bealtered inhibition. Past studies indicate that the hippocampusis involved in the generation of status epilepticus (Lothman etal., 1991; VanLandingham and Lothman, 1991; Kapur and Macdonald,1996), and hippocampal GABAergic inhibition is altered duringstatus epilepticus (Kapur and Lothman, 1989; Kapur et al., 1989;Kapur and Coulter, 1995). These studies suggested that refractorinessof seizures to diazepam may result from altered GABAR functionin the hippocampus. The experiments reported here support thealtered GABAR function hypothesis.

The principal limitation of the whole-animal experiments was that no electroencephalogram (EEG) was recorded during the inductionand treatment of status epilepticus. This was of concern becausebrief limbic seizures may occur in rats without behavioral change(Walton and Treiman, 1988; Lothman et al., 1989). Thus behaviorallya rat may appear seizure free but may still be having electrographicseizures after treatment. To circumvent this difficulty, we usedan additional criterion, resumption of normal behavior within30 min, to define termination of status epilepticus. Our conclusionthat status epilepticus in rats can be controlled with diazepamafter brief seizures but that after prolonged seizures the ratsbecome refractory to the same dose of diazepam was supported byseveral previous studies (Morrisett et al., 1987; Walton and Treiman,1988) that used combined EEG and behavioral observations. Thesepublished studies documented that diazepam at 20 mg/kg terminateslithium- and pilocarpine-induced status epilepticus 10 min afterthe onset of seizures but not 45 min after the onset. We wantedto determine whether this loss of effectiveness of diazepam interminating prolonged seizures represented a loss of efficacyor a loss of potency of diazepam. The current study suggests thatthis was caused by a loss of potency.

Plasticity of GABAR function during status epilepticus
During status epilepticus, GABAR-mediated inhibition in the hippocampus is reduced both in the CA1 region and in the dentategyrus (Kapur and Lothman, 1989; Sloviter, 1991; Kapur and Coulter,1995). One proposed mechanism for the reduction in inhibitionis a specific alteration in the functional properties of GABARs(Kapur and Coulter, 1995). This study demonstrates directly thattwo functional properties of GABARs, diazepam enhancement andZn²⁺ inhibition of GABAR currents, were altered by the prolonged seizures.This plasticity of GABARs in the hippocampus may play a role inthe pathogenesis and treatment of status epilepticus. Seizuresin the hippocampus reduce GABAergic inhibition, and these findingsdemonstrate that this is in part because of changes in GABAR function.The reduction of diazepam sensitivity of dentate granule cellGABARs parallels the loss of effectiveness of diazepam in thetreatment of experimental status epilepticus. It is possible thatchanges in the diazepam sensitivity of dentate granule cell GABARsreflect reduction of diazepam sensitivity in the treatment ofstatus epilepticus. Additionally, pentobarbital sensitivity ofGABARs on dentate granule cells isolated from animals undergoingstatus epilepticus was preserved. This suggested that status epilepticusalters specific properties of GABARs rather than causing a generalizeddysfunction of the receptor.

In the present study, we wanted to study allosteric modulation of GABARs by diazepam, Zn²⁺, and pentobarbital. To study the effect of the prolonged seizuresof status epilepticus on allosteric modulation of GABAR currents,it was necessary to obtain comparable baseline GABAR currentsin granule cells from controls and from animals undergoing statusepilepticus. This was achieved by using the conventional patch-clamptechnique used to record whole-cell GABAR currents, which alloweddialysis of intracellular contents including chloride ions withthe contents of the pipette. Increased run-up observed in cellsisolated from rats undergoing status epilepticus was consistentwith the previous report of intracellular chloride loading inneurons after status epilepticus (Kapur and Coulter, 1995). Presumablyin the present study, after access was established, the high intracellularchloride ion concentration was replaced by the pipette solutioncontaining lower chloride ion and permeant phosphate anion concentrationsthat caused the currents to increase.

A potential confounding factor in the study using acutely isolated neurons was that the procedure itself may alter the functionalproperties of GABARs. It was also possible that neurons in animalsundergoing status epilepticus were selectively vulnerable to theisolation procedure. Additionally, inclusion of EGTA in the recordingpipette would buffer any Ca²⁺-dependent changes in GABAR function (Chen and Wong, 1991; DeKoninck and Mody, 1996). However, excluding EGTA from the recordingpipette resulted in rapid run-down of GABAR currents, and therefore,it was necessary to include EGTA in the recording pipettes toperform these experiments (Chen and Wong, 1991). This cell isolationprocedure has been used repeatedly in the past to study GABARs(Akaike et al., 1985; Coulter et al., 1990; Oh et al., 1995) andepileptic neurons (Mody et al., 1992), and the results of thestudy were similar to those obtained in more intact preparations(Walton and Treiman, 1988; Kapur and Lothman, 1989).

Status epilepticus and chronic temporal lobe epilepsy have distinct effects on hippocampal GABARs
Studies investigating the role of GABAR-mediated inhibition in the hippocampus in kindling and other models of temporal lobeepilepsy are the most comparable with the current study. However,brief seizures of temporal lobe epilepsy and prolonged seizuresof status epilepticus are distinct phenomena. Close to 50% ofthose having an episode of status epilepticus have not previouslyexperienced a seizure (DeLorenzo et al., 1996). Epileptic seizuresare brief, and data from epilepsy monitoring units indicate thatthe majority of seizures spontaneously terminate within 10 min(Ramsay, 1993). In contrast, status epilepticus is a syndromeconsisting of a very prolonged seizure with continuous evolutionof neurological state, worsening cerebral metabolism, a steadyrise in core temperature, a rise in blood pressure, lactic acidosis,hyperglycemia (Meldrum and Horton, 1973), and increased catecholaminelevels (Simon et al., 1984). Hippocampal injury and neuronal lossoccur because of status epilepticus in humans (DeGiorgio et al.,1992; Nohria et al., 1994) and in most animal models of statusepilepticus (Meldrum et al., 1973; Clifford et al., 1987; Bertramand Lothman, 1993; Fujikawa et al., 1994; Sloviter et al., 1996),but whether individual brief seizures cause neuronal loss remainscontroversial (Bertram and Lothman, 1993; Cavazos et al., 1994;Watanabe et al., 1996). It is thus expected that status epilepticusand chronic temporal lobe epilepsy have different effects on hippocampaldentate granule cell GABARs.

In kindling, subconvulsive, electrical stimulation applied repeatedly to various regions of the brain evokes progressivelyprolonged behavioral and electrographic seizures that terminatein generalized tonic-clonic seizures. However there are importantdifferences between the gradual plasticity occurring during thekindling process and the rapidly evolving changes of status epilepticusreported here. Several studies have reported enhanced [³H]muscimol and [³H]benzodiazepine binding in hippocampal membranes (Shin et al.,1985) and specifically in the hippocampal dentate gyrus (McNamaraet al., 1980; Valdes et al., 1982). This increase in the hippocampaldentate granule cell GABARs after kindling was associated withan increase in the amplitude of miniature IPSCs and enhancementof paired pulse depression of kindled dentate gyrus (Otis et al.,1994). These long-term changes in GABAR-mediated inhibition inthe dentate gyrus were likely to be antiepileptic in nature. Thefindings of this study, however, do not contradict studies onthe kindling model. Although inhibitory neurotransmission in thedentate gyrus was enhanced during kindling and diminished duringstatus epilepticus, the changes in kindling were slower to developcompared with the rapid changes occurring during status epilepticus.

In electrical stimulation models of epilepsy, GABAR-mediated inhibition in the dentate gyrus was chronically reduced, butthis reduction was hypothesized to be caused by circuit rearrangementand dormancy of basket cells (Sloviter, 1991). Recently, Buhlet al. (1996) demonstrated enhanced Zn²⁺ sensitivity of hippocampal dentate granule cell GABARs afterkindling and suggested that this increased sensitivity resultedin a collapse of the augmented inhibition during seizures. Gibbset al. (1997) found increased GABAR density and enhanced GABARZn²⁺ sensitivity in another model of chronic temporal lobe epilepsy.Several important distinctions between these studies and thisreport pertain. First, the reduced diazepam sensitivity demonstratedhere has not been reported in the past. Second, the changes observedhere were acute, occurring over minutes, whereas previous reportsdocumented changes that were chronic, occurring over several weeks.Finally, previous studies reported increased Zn²⁺ sensitivity of hippocampal dentate granule cell GABARs, whereasthe current study reports diminished Zn²⁺ sensitivity of granule cell GABARs.

Possible molecular mechanisms for altered GABAR function
This rapid selective loss of benzodiazepine and Zn²⁺ sensitivity is a novel form of GABAR plasticity, and the underlying molecularbasis is unclear. Diminished benzodiazepine sensitivity with developmentof benzodiazepine tolerance occurred over a prolonged period oftime (Rabow et al., 1995). During development of cerebellar granulecells, benzodiazepine sensitivity of GABARs is lost during maturationin parallel with increasing expression of the $alpha$ 6 subtype in theGABAR. Similarly, development of tolerance to benzodiazepinesrequires chronic benzodiazepine administration.

This selective loss of benzodiazepine and Zn²⁺ sensitivity may result from altered structural composition or an altered stateof phosphorylation of GABARs. Diazepam sensitivity of GABARs requiresthe presence of the $gamma$ 2 subtype with a $beta$ subtype and either $alpha$ 1, $alpha$ 2, $alpha$ 3, or $alpha$ 5 subtypes (Pritchett et al., 1989; Macdonald andOlsen, 1994). Recombinant GABARs expressed without the $gamma$ 2 subtypeare highly sensitive to Zn²⁺ (IC₅₀ < 10 µM), whereas GABARs expressed with the $gamma$ 2 subtypewere relatively insensitive to Zn²⁺ (Draguhn et al., 1990; Smart et al., 1991). Thus one explanationfor acute reduction of diazepam sensitivity of hippocampal dentategranule cell GABARs after seizures would be a loss of the $gamma$ 2 subtypefrom the receptor; however this would not explain diminished Zn²⁺ sensitivity of these receptors. Another potential explanationfor diminished diazepam and Zn²⁺ sensitivity would be an altered $alpha$ subtype expression, because $alpha$ subtypes are known to alter both Zn²⁺ and diazepam sensitivity of the GABARs. For example, recombinantGABARs with the $alpha$ 4 or $alpha$ 6 subtype with a $beta$ subtype and a $gamma$ 2 subtypehave low diazepam and Zn²⁺ sensitivities (Saxena and Macdonald, 1996).

Seizures may alter GABAR function by other mechanisms such as posttranslational modification of GABARs or release of endogenousbenzodiazepine-like substances. Modification of GABARs by phoshorylationis well demonstrated (Lin et al., 1994; Macdonald and Olsen, 1994;Macdonald, 1995), and seizures are known to modulate activitiesof cAMP-dependent kinase, calcium- and calmodulin-dependent kinase,and calcium- and phospholipid-dependent kinase (Jope et al., 1992;Perlin et al., 1992). However, it remains to be shown that posttranslationalmodification can alter benzodiazepine and Zn²⁺ sensitivity of GABARs.

FOOTNOTES

Received March 7, 1997; revised June 24, 1997; accepted July 21, 1997.

This work was supported by United States Public Health Service Grants RO1 33300 (R.L.M.) and KO8 NS01748 (J.K.) and by a grantfrom the Epilepsy Foundation of America (J.K.). We thank NadiaEsmaiel and Eric M. Ortwig for assistance with the experiments.

Correspondence should be addressed to Dr. Jaideep Kapur, Neuroscience Laboratory Building, 1103 East Huron, Ann Arbor, Michigan48104-1687.

REFERENCES

Akaike N, Hattori K, Inomata N, Oomura Y (1985) Gamma-Aminobutyric-acid- and pentobarbitone-gated chloride currents in internally perfused frog sensory neurones. J Physiol (Lond) 360:367-386[Abstract/Free Full Text].
Bertram EH, Lothman EW (1993) Morphometric effects of intermittent kindled seizures and limbic status epilepticus in the dentate gyrus of the rat. Brain Res 603:25-31[Web of Science][Medline].
Buhl EH, Otis TS, Mody I (1996) Zinc-induced collapse of augmented inhibition by GABA in a temporal lobe epilepsy model. Science 271:369-373[Abstract].
Cavazos JE, Das I, Sutula TP (1994) Neuronal loss induced in limbic pathways by kindling: evidence for induction of hippocampal sclerosis by repeated brief seizures. J Neurosci 14:3106-3121[Abstract].
Chen QX, Wong RK (1991) Intracellular Ca₂₊ suppressed a transient potassium current in hippocampal neurons. J Neurosci 11:337-343[Abstract].
Clifford DB, Olney JW, Maniotis A, Collins RC, Zorumski CF (1987) The functional anatomy and pathology of lithium-pilocarpine and high-dose pilocarpine seizures. Neuroscience 23:953-968[Web of Science][Medline].
Commission on Classification and Terminology of the International League against Epilepsy (1981) Proposal for revised clinical and electroencephalographic classification of epileptic seizures. Epilepsia 22:489-501[Web of Science][Medline].
Coulter DA, Huguenard JR, Prince DA (1990) Differential effects of petit mal anticonvulsants and convulsants on thalamic neurones: GABA current blockade. Br J Pharmacol 100:807-813[Web of Science][Medline].
De Deyn PP, Macdonald RL (1988) Effects of non-sedative anxiolytic drugs on responses to GABA and on diazepam-induced enhancement of these responses on mouse neurones in cell culture. Br J Pharmacol 95:109-120[Web of Science][Medline].
DeGiorgio CM, Tomiyasu U, Gott PS, Treiman DM (1992) Hippocampal pyramidal cell loss in human status epilepticus. Epilepsia 33:23-27[Web of Science][Medline].
De Koninck Y, Mody I (1996) The effects of raising intracellular calcium on synaptic GABA_A receptor-channels. Neuropharmacology 35:1365-1374[Web of Science][Medline].
DeLorenzo RJ (1990) Status epilepticus: concepts in diagnosis and treatment. Semin Neurol 10:396-405[Web of Science][Medline].
DeLorenzo RJ, Hauser WA, Towne AR, Boggs JG, Pellock JM, Penberthy L, Garnett L, Ko D (1996) A prospective, population-based epidemiologic study of status epilepticus in Richmond, Virginia. Neurology 46:1029-1035[Abstract/Free Full Text].
Draguhn A, Verdorn TA, Ewert M, Seeburg PH, Sakmann B (1990) Functional and molecular distinction between recombinant rat GABA_A receptor subtypes by Zn²⁺. Neuron 5:781-788[Web of Science][Medline].
Fujikawa DG, Daniels AH, Kim JS (1994) The competitive NMDA receptor antagonist CGP 40116 protects against status epilepticus-induced neuronal damage. Epilepsy Res 17:207-219[Web of Science][Medline].
Gibbs JW, Shumate MD, Coulter DA (1997) Differential epilepsy-associated alterations in postsynaptic GABA_A receptor function in dentate granule and CA1 neurons. J Neurophysiol 77:1924-1938[Abstract/Free Full Text].
Greenfield Jr LJ, Macdonald RL (1996) Whole-cell and single-channel alpha1 beta1 gamma2S-GABA_A receptor currents elicited by a "multipuffer" drug application device. Pflügers Arch 432:1080-1090[Web of Science][Medline].
Hamill OP, Marty A, Neher E, Sakmann B, Sigworth FJ (1981) Improved patch-clamp techniques for high-resolution current recording from cells and cell-free membrane patches. Pflügers Arch 391:85-100[Web of Science][Medline].
Honchar MP, Olney JW, Sherman WR (1983) Systemic cholinergic agents induce seizures and brain damage in lithium-treated rats. Science 220:323-325[Abstract/Free Full Text].
Jope RS, Song L, Kolasa K (1992) Inositol trisphosphate, cyclic AMP, and cyclic GMP in rat brain regions after lithium and seizures. Biol Psychiatry 31:505-514[Web of Science][Medline].
Kapur J, Coulter DA (1995) Experimental status epilepticus alters GABA_A receptor function in CA1 pyramidal neurons. Ann Neurol 38:893-900[Web of Science][Medline].
Kapur J, Lothman EW (1989) Loss of inhibition precedes delayed spontaneous seizures in the hippocampus after tetanic electrical stimulation. J Neurophysiol 61:427-434[Abstract/Free Full Text].
Kapur J, Macdonald RL (1996) Status epilepticus: a proposed pathophysiology. In: The treatment of epilepsy (Shorvon S, Dreyfuss F, Fish D, Thomas D, eds), pp 258-268. Oxford: Blackwell Science.
Kapur J, Stringer JL, Lothman EW (1989) Evidence that repetitive seizures in the hippocampus cause a lasting reduction of GABAergic inhibition. J Neurophysiol 61:417-426[Abstract/Free Full Text].
Kapur J, Lothman EW, DeLorenzo RJ (1994) Loss of GABA_A receptors during partial status epilepticus. Neurology 44:2407-2408[Free Full Text].
Kay AR, Wong RK (1986) Isolation of neurons suitable for patch-clamping from adult mammalian central nervous systems. J Neurosci Methods 16:227-238[Web of Science][Medline].
Lin Y, Browning MD, Dudek EM, Macdonald RL (1994) Protein kinase C enhances recombinant bovine a1b1G2L GABA_A receptor whole-cell currents expressed in L929 fibroblasts. Neuron 13:1421-1431[Web of Science][Medline].
Lothman EW, Bertram EH, Bekenstein JW, Perlin JB (1989) Self-sustaining limbic status epilepticus induced by "continuous" hippocampal stimulation: electrographic and behavioral characteristics. Epilepsy Res 3:107-119[Web of Science][Medline].
Lothman EW, Bertram III EH, Stringer JL (1991) Functional anatomy of hippocampal seizures. Prog Neurobiol 37:1-82[Web of Science][Medline].
Macdonald RL (1995) Ethanol, gamma-aminobutyrate type A receptors, and protein kinase C phosphorylation. Proc Natl Acad Sci USA 92:3633-3635[Free Full Text].
Macdonald RL, Kelly KM (1995) Antiepileptic drug mechanisms of action. Epilepsia 36:S2-S12.
Macdonald RL, Olsen RW (1994) GABA_A receptor channels. Annu Rev Neurosci 17:569-602[Web of Science][Medline].
Macdonald RL, Twyman RE, Ryan-Jastrow T, Angelotti TP (1992) Regulation of GABA_A receptor channels by anticonvulsant and convulsant drugs and by phosphorylation. Epilepsy Res [Suppl] 9:265-277[Medline].
McNamara JO, Peper AM, Patrone V (1980) Repeated seizures induce long-term increase in hippocampal benzodiazepine receptors. Proc Natl Acad Sci USA 77:3029-3032[Abstract/Free Full Text].
Meldrum BS, Horton RW (1973) Physiology of status epilepticus in primates. Arch Neurol 28:1-9[Abstract/Free Full Text].
Meldrum BS, Vigouroux RA, Brierley JB (1973) Systemic factors and epileptic brain damage. Prolonged seizures in paralyzed, artificially ventilated baboons. Arch Neurol 29:82-87[Abstract/Free Full Text].
Mody I, Otis TS, Staley KJ, Kohr G (1992) The balance between excitation and inhibition in dentate granule cells and its role in epilepsy. Epilepsy Res [Suppl] 9:331-339[Medline].
Morrisett RA, Jope RS, Snead OC (1987) Effects of drugs on the initiation and maintenance of status epilepticus induced by administration of pilocarpine to lithium-pretreated rats. Exp Neurol 97:193-200[Web of Science][Medline].
Nohria V, Lee N, Tien RD, Heinz ER, Smith JS, DeLong GR, Skeen MB, Resnick TJ, Crain B, Lewis DV (1994) Magnetic resonance imaging evidence of hippocampal sclerosis in progression: a case report. Epilepsia 35:1332-1336[Web of Science][Medline].
Oh K-S, Lee C-J, Gibbs JW, Coulter DA (1995) Postnatal development of GABA_A receptor function in somatosensory thalamus and cortex: whole-cell voltage clamp recordings in acutely isolated rat neurons. J Neurosci 15:1341-1351[Abstract].
Otis TS, De Koninck Y, Mody I (1994) Lasting potentiation of inhibition is associated with an increased number of gamma-aminobutyric acid type A receptors activated during miniature inhibitory postsynaptic currents. Proc Natl Acad Sci USA 91:7698-7702[Abstract/Free Full Text].
Perlin JB, Churn SB, Lothman EW, DeLorenzo RJ (1992) Loss of type II calcium/calmodulin-dependent kinase activity correlates with stages of development of electrographic seizures in status epilepticus in rat. Epilepsy Res 11:111-118[Web of Science][Medline].
Pritchett DB, Sontheimer H, Shivers BD, Ymer S, Kettenmann H, Schofield PR, Seeburg PH (1989) Importance of a novel GABA_A subunit for benzodiazepine pharmacology. Nature 338:582-585[Medline].
Rabow LE, Russek SJ, Farb DH (1995) From ion currents to genomic analysis: recent advances in GABA_A receptor research. Synapse 21:189-274[Web of Science][Medline].
Racine RJ (1972) Modification of seizure activity by electrical stimulation. II. Motor seizure. Electroencephalogr Clin Neurophysiol 32:281-294[Web of Science][Medline].
Ramsay RE (1993) Treatment of status epilepticus. Epilepsia [Suppl 1] 34:S71-S81.
Saxena NC, Macdonald RL (1996) Properties of putative cerebellar GABA_A receptor isoforms. Mol Pharmacol 49:567-579[Abstract].
Shin C, Pedersen HB, McNamara JO (1985) $gamma$ -Aminobutyric acid and benzodiazepine receptors in the kindling model of epilepsy: a quantitative radiohistochemical study. J Neurosci 5:2696-2701[Abstract].
Simon RP, Aminoff MJ, Benowitz NL (1984) Changes in plasma catecholamines after tonic-clonic seizures. Neurology 34:255-257[Abstract/Free Full Text].
Sloviter RS (1991) Permanently altered hippocampal structure, excitability, and inhibition after experimental status epilepticus in the rat: the "dormant basket cell" hypothesis and its possible relevance to temporal lobe epilepsy. Hippocampus 1:41-66[Medline].
Sloviter RS, Dean E, Sollas AL, Goodman JH (1996) Apoptosis and necrosis induced in different hippocampal neuron populations by repetitive perforant path stimulation in the rat. J Comp Neurol 366:516-533[Web of Science][Medline].
Smart TG, Moss SJ, Xie X, Huganir RL (1991) GABA_A receptors are differentially sensitive to zinc: dependence on subunit composition. Br J Pharmacol 103:1837-1839[Web of Science][Medline].
Valdes F, Dasheiff RM, Birmingham F, Crutcher KA, McNamara JO (1982) Benzodiazepine receptor increases after repeated seizures: evidence for localization to dentate granule cells. Proc Natl Acad Sci USA 79:193-197[Abstract/Free Full Text].
VanLandingham KE, Lothman EW (1991) Self-sustaining limbic status epilepticus. I. Acute and chronic cerebral metabolic studies: limbic hypermetabolism and neocortical hypometabolism. Neurology 41:1942-1949[Abstract/Free Full Text].
Walton NY, Treiman DM (1988) Response of status epilepticus induced by lithium and pilocarpine to treatment with diazepam. Exp Neurol 101:267-275[Web of Science][Medline].
Watanabe Y, Johnson RS, Butler LS, Binder DK, Spiegelman BM, Papaioannou VE, McNamara JO (1996) Null mutation of c-fos impairs structural and functional plasticities in the kindling model of epilepsy. J Neurosci 16:3827-3836[Abstract/Free Full Text].
Yaffe K, Lowenstein DH (1993) Prognostic factors of pentobarbital therapy for refractory generalized status epilepticus. Neurology 43:895-900[Abstract/Free Full Text].

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The Role of an alpha �Subtype M2-M3 His in Regulating Inhibition of GABAA Receptor Current by Zinc and Other Divalent Cations
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[Abstract] [Full Text] [PDF]

D. H. Lowenstein and B. K. Alldredge
Status Epilepticus
N. Engl. J. Med., April 2, 1998; 338(14): 970 - 976.
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