Mapping Quantitative Trait Loci for Seizure Response to a GABAA Receptor Inverse Agonist in Mice

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The Journal of Neuroscience, May 15, 1999, 19(10):3731-3738

Mapping Quantitative Trait Loci for Seizure Response to a GABA_A Receptor Inverse Agonist in Mice
Howard K. Gershenfeld¹, Paul E. Neumann², Xiaohua Li¹, Pamela L. St. Jean³, and Steven M. Paul⁴^,⁵
¹ Department of Psychiatry, University of Texas Southwestern Medical Center, Dallas, Texas 75235-8898, ² Department of Anatomy and Neurobiology, Dalhousie University, Halifax, Nova Scotia, Canada B3H 4H7, ³ Glaxo Wellcome Research, Inc., Research Triangle Park, North Carolina 27514, ⁴ Lilly Research Laboratory, Indianapolis, Indiana 46285, and ⁵ Departments of Psychiatry, Pharmacology and Toxicology, Indiana University School of Medicine, Indianapolis, Indiana 46202

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

To define the genetic contributions affecting individual differences in seizure threshold, a $beta$ carboline [methyl- $beta$ -carboline-3-carboxylate( $beta$ -CCM)]-induced model of generalized seizures was geneticallydissected in mice. $beta$ -CCM is a GABA_A receptor inverse agonist andconvulsant. By measuring the latency to generalized seizures after $beta$ -CCM administration to A/J and C57BL6/J mice and their progeny,we estimated a heritability of 0.28 ± 0.10. A genome wide screenin an F2 population of these parental strains (n = 273) mappedquantitative trait loci (QTLs) on proximal chromosome 7 [logarithmof the likelihood for linkage (LOD) = 3.71] and distal chromosome10 (LOD = 4.29) for seizure susceptibility, explaining ~22 and25%, respectively, of the genetic variance for this seizure trait.The best fitting logistic regression model suggests that the A/Jallele at each locus increases the likelihood of seizures approximatelythreefold. In a subsequent backcross population (n = 223), wemapped QTLs on distal chromosome 4 (LOD = 2.88) and confirmedthe distal chromosome 10 QTLs (LOD = 4.36). In the backcross,the C57BL/6J allele of the chromosome 10 QTL decreases the riskof seizures approximately twofold. These QTLs may ultimately leadto the identification of genes influencing individual differencesin seizure threshold in mice and the discovery of novel anticonvulsantagents. The colocalization on distal chromosome 10 of a $beta$ -CCMsusceptibility QTL and a QTL for open field ambulation and verticalmovement suggests the existence of a single, pleiotropic locus,which we have named Exq1.

Key words: quantitative trait locus (QTL); epilepsy; seizure; $beta$ -carboline; open field; individual differences

  INTRODUCTION

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Wide inter-individual differences (~12-fold) in seizure thresholds have been documented in humans as measured by the electricalstimulus dose needed to induce a seizure (Sackeim et al., 1991;Colenda and McCall, 1996). Despite intense investigations at themolecular, cellular, neural network, slice, and whole-brain levels(McNamara, 1992, 1994), the pathophysiology of paroxysmal dischargesand seizure threshold regulation are incompletely understood.Genetic factors contribute to a predisposition for seizures witha complex inheritance (Anderson et al., 1986; Berkovic et al.,1998). Recent conflicting results in mapping loci for juvenilemyoclonic epilepsy (Greenberg and Delgado-Escueta, 1993; Liu etal., 1995, 1996; Elmslie et al., 1996; Serratosa et al., 1996)have highlighted the problems in mapping loci for complex diseasessuch as epilepsy. These difficulties include (1) incomplete penetrance,(2) the presence of phenocopies, (3) genetic heterogeneity (differentloci giving rise to a single phenotype), (4) multigenic modesof inheritance, (5) gene interactions, and (6) environmental factors.These complexities render the mapping and positional cloning ofloci for complex behaviors challenging in humans. As an alternative,we have chosen to focus on a mouse model of drug-induced epilepsythat offers the advantages of planned matings and controlled environments.Rodent models have already demonstrated utility in mapping genesand quantitative trait loci (QTLs) for epilepsy (Applegate etal., 1989, 1990; Neumann and Seyfried, 1990; Neumann and Collins,1991; Rise et al., 1991; Frankel et al., 1994, 1995a,b; Frankel,1995; Noebels, 1996; Buck et al., 1997; Cox et al., 1997; Ferraroet al., 1997; Skradski et al., 1998).

In the present study, we have genetically dissected the variation in seizure response to a $beta$ carboline convulsant, methyl- $beta$ -carboline-3-carboxylate( $beta$ -CCM). $beta$ -CCM binds to GABA_A receptors and exerts an effect oppositeto benzodiazepines (i.e., acts as an inverse agonist) to reduceGABA-mediated chloride ion conductance at low concentrations (Imet al., 1995; Barnard et al., 1998). The latter reduces postsynapticGABAergic inhibitory activity (Tunnicicliff and Raess, 1991; Olsenand Avoli, 1997). $beta$ -CCM is a convulsant when administered to chickens,mice, rats, rabbits, and baboons (Croucher et al., 1984; Pradode Carvalho et al., 1984; Chapman et al., 1985, 1987; Massottiet al., 1985).

In mice, convulsant doses of $beta$ -CCM induce a single brief (10 sec) convulsion of cortical origin with rapid propagation tothe hippocampus (Prado de Carvalho et al., 1983). We and othershave previously demonstrated large differences among inbred mousestrains in their sensitivity to $beta$ carboline convulsants with asignificant heritable component (Kosobud and Crabbe, 1990; Martinet al., 1991, 1992, 1994; Mathis et al., 1995; Chapouthier etal., 1998). We have focused in particular on the sensitive A/Jand resistant C57BL/6J strains, which differ markedly in theirseizure susceptibility to various chemical convulsants (Kosobudand Crabbe, 1990). Recently, segments of chromosomes 4, 9, and13 have been provisionally mapped as affecting $beta$ -CCM-induced seizures(Martin et al., 1995; Clement et al., 1996). Here, we report theresults of a genome-wide search for QTLs influencing susceptibilityto $beta$ -CCM in intercross and backcross populations derived fromA/J and C57BL/6J inbredmice.

  MATERIALS AND METHODS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Animals. Male and female A/J (A), C57BL/6J (B6), B6AF1, and F2 hybrid mice 7-8 weeks of age were obtained from Jackson Laboratory(Bar Harbor, ME). B6AF2 mice (F2; n = 273) were derived from anintercross of offspring of a cross between B6 females and A males.N2 mice (n = 220) were produced at the University of Texas SouthwesternMedical Center (UTSW) from a backcross of B6AF1 females and Amales. All mice of the same strain and gender were housed in groupsof four to five animals with food and water ad libitum. Animalswere maintained under a 12 light/dark cycle with lights on at6 A.M. F2 mice were identified by ear notching at 7-8 weeks ofage followed by 10 d of adaptation previous to phenotyping. N2mice were ear-notched at 4 weeks of age and tested at 7-8 weeksof age. Mice were tested individually and weighed on the day oftesting. Before testing for response to $beta$ -CCM, mice were subjectedto sequential testing in behavioral paradigms: exploratory behaviorin an open field (O-F) and light-dark (L-D) transitions, exceptfor the backcross offspring, which were not tested in the L-Dtransition test. The results of these studies (exploratory behaviorin an O-F and L-D transitions of the F2 hybrids) were reportedelsewhere (Gershenfeld and Paul, 1997; Gershenfeld et al., 1997).All experiments followed the NIH Guide for the Care and Use ofLaboratory Animals.

Seizure testing. Mice were tested for their vulnerability to seizures induced by $beta$ -CCM (Research Biochemicals, Natick, MA)at 10 weeks of age in the F2 hybrids and at 7-8 weeks of age inthe backcross offspring. $beta$ -CCM was dissolved in 0.1N HCl (100µl/mg $beta$ -CCM) and diluted in saline to a final concentration of1 mg/ml. $beta$ -CCM (5 mg/kg) was administered intraperitoneally ina volume of 0.1 ml/20 gm body weight. The animals received $beta$ -CCMat least 10 min after being isolated in individual cages. Preliminarydose and time-response studies indicated that 5 mg/kg was theoptimal dose and that 10 min was the optimal observation periodfor $beta$ -CCM-induced seizures. Nonseizing animals were assigned avalue of 600 sec. Thus, mice were observed for the following dependentvariables: (1) seizure susceptibility dichotomized as either susceptible(seizure occurred) or resistant (absence of a seizure) and (2)latency of seizures (measured in seconds). Generalized, myoclonicseizures were defined as motor behavior consisting of tonic andclonic alternations, accompanied by a loss of the rightingreflex.

DNA preparation and genotyping. DNA was prepared and genotyped as described previously (Gershenfeld and Paul, 1997). Briefly,DNA was genotyped by PCR with MapPair primers (Research Genetics,Huntsville, AL). Initially, a panel of 102 approximately equallyspaced CA repeat microsatellite DNA markers were selected (Dietrichet al., 1992, 1996), providing a whole genome screen at a spacingof ~14cm.

Exploratory behavior in an open field. O-F behavior was performed and analyzed as described previously (Gershenfeld et al.,1997), except that the backcross offspring were tested at UTSWfor O-F in a newer apparatus (Opto-Varimex-3, Columbus Instruments,Columbus, OH; 730 lux at cage floor). The dimensions of the squarefield were 43 × 43 × 30.5 cm, and the vertical sensor was positioned8 cm above the cage floor. Briefly, O-F behavior consisted ofthree consecutive 5 min epochs (e1, e2, e3) (15 min total), andthe following dependent measures were assessed: (1) initial totaldistance (TDe1), the distance travelled or ambulated during theinitial 5 min epoch, epoch 1; (2) habituated total distance (TDe3),the distance travelled or ambulated during the last 5 min epoch,epoch 3; and (3) vertical movements (VM15), the sum of verticalmovements (rearings) during the first trial of 15min.

Statistical analysis. The presence or absence of seizures was treated as a dichotomous, nominal variable. Latency to seizurewas measured as a continuous variable. The genetic component ofthe variance in the F2 generation and its error (i.e., the broadsense heritability) were estimated as described (Falconer, 1963).Analysis of components of the means was performed as describedpreviously (Neumann et al., 1993). Because no suitable transformationof the latency-to-seizure trait variable could be found (to obtaina normal distribution and equalize the variances among groups),the data were subsequently analyzed nonparametrically. By rankordering the latency-to-seizure variable, the "ceiling effect"of arbitrarily assigning nonseizing mice a value of 600 sec wasmitigated.

Overall differences in latency to seizure and percentage of animals with a myoclonic seizure were compared across gender,strain, and generation by nonparametric tests for significantdifferences with Mann-Whitney U, Kruskal-Wallis, and $chi$ ² tests (Statview 4.5 and SuperAnova, Abacus Concepts and JMP 3.02,SASInstitute).

For linkage detection, we initially used $chi$ ² tests of independence between markers and seizure susceptibility (i.e., the presenceor absence of seizure), which are inherently model-free. For single-pointlinkage of seizure latency and a marker, the seizure latency valueswere rank-ordered and analyzed by the Kruskal-Wallis test forthe F2 population and the Mann-Whitney U tests for the backcross(N2) population (Sokal and Rohlf, 1995). The Mapmaker/QTL (Landeret al., 1987; Paterson et al., 1991; Lincoln and Lander, 1992)and Map Manager QTLb21 (Manly, 1998) programs were used to confirm,localize, and estimate the percentage of the phenotypic varianceexplained for each QTL. For interpreting the seizure linkage results,we used the empirically derived statistical threshold criteriagenerated from permutation tests on the data (shuffling randomlythe genotypes and phenotypes 10,000 times) (Churchill and Doerge,1994; Manly, 1998). These empirically derived threshold definitionsfor suggestive and significant linkage correspond to the establishedp values based on the number of times that one would be expectedto find such a result at random under the more stringent assumptionof a dense marker map genome scan (Lander and Kruglyak, 1995).Suggestive linkage thresholds define a level at which just oneoccurrence at random in a genome scan would be expected, whereasthe significant linkage threshold would be surpassed statistically0.05 times in a genome scan. For the F2 population, the permutationsof the ranked seizure latency determined the thresholds for suggestiveand significant linkage as logarithm of the likelihood for linkage(LOD) scores of 2.3 and 3.7, respectively. For the N2 population,the threshold values for suggestive and significant linkage wereLOD scores of 1.4 and 2.7, respectively. Finally, the data weremodeled by stepwise linear and nominal logistic regression tofind the best fitting model and to obtain odds ratios (Kleinbaum,1994; Sokal and Rohlf, 1995). For interpreting the exploratorybehavioral traits' linkage results, we used the published guidelines(Lander and Kruglyak, 1995). The percentage of the genetic componentof the variance explained by a QTL was estimated by dividing thepercentage of the phenotypic variance explained by the estimatedheritability. Epistatic interactions were examined by linear regressionanalysis, testing for statistical interactions among mapped locias described (Cheverud and Routman, 1995).

  RESULTS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Segregation analysis

A/J mice were more susceptible to $beta$ -CCM-induced myoclonic seizures than B6 mice in both latency to seizure and proportionof tested mice that seized (p < 0.0001) (Table 1). The parentalstrains differed in effect size by 1 SD in their latency to $beta$ -CCM-inducedseizures. Preliminary experiments with the parental strains at7 and 10 weeks (data not shown) showed no difference in seizurefrequency or latency to seizure between age groups.


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Table 1. Seizure frequency and latency in parental, F1, F2 hybrid, and backcross mice injected with $beta$ -CCM

Seizure resistance showed partial dominance. The F1 hybrids were less susceptible than the theoretical midparental (m) valuesfor both seizure frequency and latency but were more susceptiblethan B6 mice without reaching statistical significance. The broadsense heritability of seizure latency was estimated in the F2hybrids to be 0.28 ± 0.10; however, this estimate makes the falseassumption of a normal distribution of the data. Analysis of thecomponents of the means was consistent with a simple model ofthe mode of inheritance requiring no interaction parameters. Theparameters m (0.45), a (0.23), and d ( $-$ 0.12) were calculated fromthe seizure frequencies in the B6, A, and F1 populations. Thepredicted seizure frequencies in the F2 (m + d/2 = 0.39) and N2(m + a/2 + d/2 = 0.51) were not significantly different from theobserved values (36 and 51%).

Linkage analysis of seizure susceptibility in intercross offspring

From the phenotypic rankings of the latency-to-seizure trait, F2 animals within the lowest and highest (17% tails) of thedistribution ("phenotypic extremes") were selected for initialgenotyping. We mapped loci using a three-stage strategy. In stageI, $chi$ ² tests of independence between markers and seizure susceptibilitywere calculated from a genome-wide screen on the phenotypic extremes.Six peak marker loci (D1Mit353, D7Mit78, D8Mit69, D10Mit14, D15Mit11,and D18Mit4) were identified with $chi$ ² tests surpassing a relatively low threshold of statistical significance(p = 0.05), which was selected to limit type II errors (Elston,1994). In the second stage, flanking DNA markers surrounding thesix stage I candidate loci were selected and genotyped on theextremes. Then, we merged this genotype data on the seizure phenotypicextremes with our previous genotype data on the behavioral traits'phenotypic extremes, creating a pooled dataset. With this enlargeddataset, the Mapmaker/QTL computer program was used to localizeand model these potential QTLs. Only two loci located on chromosomes7 and 10 met the "suggestive" level of significance criteria forLOD cutoff thresholds for linkage. In stage III, we "genotyped"the entire F2 population with markers in the regions of interest.This step reduced errors attributable to assumptions implicitin modeling the whole distribution from non-normally distributedpopulations with missing data. Finally, the F2 data were reanalyzedwith the single point nonparametric statistics (Sokal and Rohlf,1995), Mapmaker/QTL, and logisticregression.

D7Mit308 on proximal chromosome 7 displayed association with seizure susceptibility ( $chi$ ² = 14.8, p = 0.006, 2 df; n = 267) and seizure latency (Table2, Fig. 1A).


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Table 2. QTL mapping summary and mean comparisons at mapped loci by genotype

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Figure 1. QTL likelihood plots on the F2 population for (A) chromosome 7 and (B) chromosome 10 and on the N2(B6AF1xA/J) backcross population for (C) chromosome 4 and (D) chromosome 10 from Mapmaker/QTL analyses. Logarithm of the likelihood ratio for linkage (LOD) score is plotted against map distance in centimeters for the traits of seizure latency, rank-ordered (), average of three trials of light $left-right-arrow$ dark transitions (AvgLD, $black-square$ ), initial O-F total distance ambulated (TDe1, $black-triangle$ ), habituated O-F total distance ambulated (TDe3, [tridf]), and O-F vertical movements (VM15, $black-diamond$ ). For the F2 hybrids with 2 df, the published threshold values for suggestive and significant linkage are LOD = 2.8 and LOD = 4.3, respectively, whereas the empirically derived threshold values from 10,000 permutations for the ranked latency to seizure gave values of 2.3 and 3.7, respectively. For the N2(B6AF1xA/J) cross with 1 df, the published threshold values for suggestive and significant linkage are LOD = 1.9 and LOD= 3.3, respectively, whereas the empirically derived values for the ranked latency to seizure gave values of 1.4 and 2.7. These QTL plots used the genotyping of 11 and 12 DNA markers for chromosome 7 and 10 in the F2 hybrids, whereas the backcross offspring used the genotyping of 7 and 10 DNA markers for chromosomes 4 and 10, respectively.

D10Mit180 on distal chromosome 10 was associated with seizure susceptibility ( $chi$ ² = 15.77, p = 0.004, 2 df; n = 271) and seizure latency (Table2, Fig. 1B). The B allele for the potential QTL near D10Mit180displayed near completedominance.

The best-fitting logistic regression model suggests that the A allele at the D7Mit308 locus increases the likelihood of seizures~3.3-fold, and the A allele at the D10Mit180-linked locus increasesthe likelihood of seizure by ~2.7-fold (Table 3). The contributionof these QTLs to the phenotypic variance was estimated similarlyfrom stepwise linear regression and Mapmaker/QTL (Table 2), whereeach locus individually accounted for 5-7% of the phenotypic variation.Together the two loci explain 11-12% of the phenotypic variationand roughly 40% of the genetic variation in the F2 generation.No epistatic interactions were detected between these loci. Noadditional QTLs were mapped in models that fix the identifiedQTL or in models that included only susceptible mice (n = 98).


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Table 3. Logistic regression model estimates of intercross offspring^a

Linkage analysis of seizure susceptibility in backcross offspring

The chromosome 10 QTL was robustly confirmed in the backcross offspring. D10Mit237, which is located ~4 cm distal to D10Mit180,displayed significant association with seizure susceptibility( $chi$ ² = 19.30, 1 df, p < 0.0001; n = 214) and seizure latency (Table2, Fig. 1D).

A genome-wide scan with 102 markers in the backcross mapped only one other QTL at the suggestive level of statistical significance.D4Mit68 on distal chromosome 4 was associated with seizure susceptibility( $chi$ ² = 10.3, 1 df, p = 0.0013; n = 217) and seizure latency (Table2, Fig. 1C).

The best fitting logistic regression model suggests that the B allele at the D4Mit68-linked locus increased the likelihoodof resistance by 2.3-fold, and the B allele at the D10Mit237-linkedlocus increased it by 2.8-fold (Table 4). Each locus accountedfor 6-9% of the phenotypic variance (Table 2). Together thesetwo loci explained ~11.8% of the phenotypic variance. The chromosome7 locus mapping in the F2 hybrids and the previously mapped loci(Martin et al., 1995; Clement et al., 1996) on chromosomes 9 and13 could not be confirmed. No statistical epistatic interactionswere detected, and no additional QTLs were mapped in models thatfix the identified QTL.


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Table 4. Logistic regression model estimates of backcross offspring^a

Linkage analysis of behavioral phenotypes in backcross offspring

O-F behaviors in the backcross offspring were tested for association with marker loci on distal chromosome 10 because theco-localization of a seizure susceptibility QTL with a previouslyreported QTL for O-F exploratory (Gershenfeld et al., 1997) andfear-like (Gershenfeld and Paul, 1998) behaviors in B6AF2 hybridmice suggested the possibility of a single pleiotropic QTL (Fig.1B). D10Mit237 displayed significant association with O-F initial(TDe1) and habituated (TDe3) ambulation and O-F vertical movement(VM15) in the backcross population (Table 2, Fig. 1D). Consequently,we named this distal chromosome 10 locus Exq1 (exploratory andexcitability QTL) because it appears to affect both O-F exploratorybehavior (TDe1, TDe3, VM15) and $beta$ -CCM-induced seizure susceptibility.Exq1 explains 6-13% of the phenotypic variance and from 13-31%of the genetic variance for the various O-F exploratory traitslisted in the backcross population (Table 2). Consistent withthe observations in the F2 population (Gershenfeld et al., 1997),the B6 allele of Exq1 is an increasing allele for all the O-Ftraits in the backcross populations (Table 2).

  DISCUSSION

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

By using the GABA_A receptor inverse agonist $beta$ -CCM as a pharmacological probe, we examined the genetic basis of individualdifferences in seizure behavior in offspring derived from theA and B6 mice. In general, the A strain is a seizure-susceptiblestrain, and B6 mice are a seizure-resistant strain based on theirsusceptibility to nine chemoconvulsants (Kosobud and Crabbe, 1990).We selected this particular drug-induced paradigm as a model ofindividual differences in susceptibility to seizures, becauseprevious work had shown robust strain differences (Martin et al.,1991, 1993, 1994; Mathis et al., 1994, 1995) that reflect presumedgenetic differences in seizure threshold and "GABA inhibitorytone"(Tunnicicliff and Raess, 1991; Olsen and Avoli, 1997). Thedrug has been demonstrated to rapidly induce a single brief convulsionwithin 10 min, and the drug has behavioral activity for at least30 min after its injection (Prado de Carvalho et al., 1984). Bymeasuring the latency to seizure after a 5 mg/kg i.p. injectionwith $beta$ -CCM, we confirmed significant between-strain differencesand estimated a heritability of 0.28 ± 0.10 in this F2 population,similar to our previous findings from RI strains (Mathis et al.,1995). Genome wide screens mapped QTLs for seizure susceptibilityon proximal chromosome 7 and distal chromosome 10 in intercrossoffspring, and on distal chromosome 4 and distal chromosome 10QTL in backcross offspring. Only the QTL on chromosome 10 wasdetected in both the intercross and the backcross, probably becauseof dominance relationships. The confidence interval of the suggestiveQTL on distal chromosome 4 overlaps with that of a $beta$ -CCM susceptibilityQTL, Bis 1 (Martin et al., 1995). In the crosses reported here,we could not confirm the provisionally mapped QTLs on chromosomes9 or proximal 13, inferred as influencing $beta$ -CCM-induced seizures(Martin et al., 1995; Clement et al., 1996).

We have named the chromosome 7 QTL Bis 4 ( $beta$ -carboline-induced seizure 4). This QTL confirmed our previous suggestive locus(near Pmv15) from a recombinant inbred strain linkage analysis(Mathis et al., 1995), whereas the other potential QTLs may besmall effect loci or spurious loci secondary to limited statisticalpower (Neumann, 1992; Belknap et al., 1996). The broad, flat Bis4likelihood plot (Fig. 1A) has a large 1 LOD support interval rangingfrom 2 to 30 centimorgans (cM) and corresponds to human regions19q13, 11p15, and 15q11-q13. This interval contains several appealingcandidate genes: Atp1a3 (Na,K-ATPase 1a3), Atp1b3 (Na,K-ATPase1b3), Grik5 (glutamate receptor, kainate 5, $gamma$ 2), and Scn1b (voltage-gatedsodium channel, type I, $beta$ polypeptide). We cannot exclude as candidategenes the cluster of three GABA_A receptor subunits ( $alpha$ 5, $beta$ 3, gamma3)or the seizure susceptibility QTLSzf1 (Frankel et al., 1994) atroughly 28 cM. Human association studies for juvenile myoclonicepilepsy in this region have been equivocal (Sander et al., 1997),but mice deficient in the $beta$ 3 subunit have an increased susceptibilityto seizures (Homanics et al., 1997). The Bis4 QTL interval isprobably proximal to the Asp3 locus, which influenced audiogenicseizures (Neumann and Collins, 1991; Banko et al., 1997). In addition,we believe that Bis4 is probably distinct from Asp3, because previouswork has shown no correlation between $beta$ -CCM-induced seizures andaudiogenic seizures among 33 B10.D2 recombinant congenic strains(Martin et al., 1992).

We named the distal chromosome 10 locus Exq1 because it appears to affect O-F exploratory behavior (TDe1, TDe3, VM15), L-Dbehavior, and $beta$ -CCM-induced seizure behavior. Although the mostparsimonious explanation for the pleiotropic effects of distalchromosome 10 is a single locus, much higher resolution fine mappingwill be needed to exclude the possibility of two closely linkedloci. The steep QTL likelihood plots (Fig. 1) for Exq1 on thehabituated total distance (TDe3) in the backcross suggest a morediscrete localization of the locus to the telomeric-most 15 cM,corresponding to human chromosomes 12q11-14 and 12q24. If oneinterprets our strain differences as individual differences inmajor behavioral systems [where open field behavior reflects abehavioral inhibition system (Kagan et al., 1988; Gray and NcNaughton,1996; Gershenfeld et al., 1997), where $beta$ -CCM-induced seizuresinterrogates the "set point" of GABA neuronal inhibition (Nuttet al., 1992), and where the L-D paradigm reflects a "fear-like"system (Gershenfeld and Paul, 1997)], then a mechanistic understandingof the Exq1 gene product should be informative in understandingthe interrelationship among these higher order behaviors. We speculatethat this locus functions as a neuronal modulator (distinct fromthe known neurotransmitter and receptor complexes) because noknown candidate genes map to this region. Although conceivableneuromodulators abound, the list might include factors known toaffect GABA_A receptor function such as growth factors (Wan etal., 1997), protein kinases (Lin et al., 1996; McDonald and Moss,1997), neurosteroids (Paul and Purdy, 1992; Purdy et al., 1992;Lambert et al., 1996; Rupprecht et al., 1996), endogenous benzodiazapineligands (Polc, 1995; Wichlinski, 1996), and transcriptional factors(Berninger et al., 1995; Sadar et al., 1996; Ashiya and Grabowski,1997) differentially regulated between the two strains. The ultimatepositional cloning of this locus may clarify the etiological mechanism.From a therapeutic perspective, one might speculatively considerthe role of a dominantly acting locus as a "protective" allele,especially in "all or none" threshold behaviors such as seizures.It is possible that the effect of relatively modest genes on anunderlying threshold may be clinically significant. As developmentsin brain stem cells and vectors progress (Lawrence et al., 1995;O'Connor et al., 1997; Xiao et al., 1997; Zhang et al., 1997),one can imagine gene therapy for people with medication refractiveepilepsy, where one might overexpress a mixture of such protectiveloci as Exq1 in the susceptible individual's tissue to increasethe seizure threshold or lessen the spread of paroxysmal neuronaldischarges.

The distal chromosome 4 QTL interval mapped in the backcross confirms the previously mapped Bis 1 QTL near je (Martin, Clementet al., 1995). Two serotonin receptor gene subunits that map tothis region (Htr1da and Htr1db) have some plausibility as regulatorsof seizure threshold. A third candidate gene is the Slc9a1 (formerlyknown as NheI), which encodes a Na⁺/H⁺ exchange protein. The etiology of the slow-wave epilepsy mutantmouse was recently attributed to a Slc9a1 null mutation (Cox etal., 1997). The region of conserved synteny in humans correspondsto 1p36-32.

Several limitations should be considered in interpreting our findings. The sample populations represent crosses between justtwo strains of mice and may not be generalizable to other strains.The sample sizes of the F2 and backcross offspring populationswere relatively small, and hence QTLs with an effect of <5% ofthe phenotypic variance would not reach statistical significance.In general, the complexity of interpreting drug response patternsin populations derives from the multiple genetic factors affectingpharmacokinetics as well as pharmacodynamics. We cannot formallyrule out pharmacokinetic explanations because we did not measurebrain $beta$ -CCM levels. In this regard, strain differences in $beta$ -CCM-inducedseizures between the NIH:GP (an outbred population of Swiss mice)and a derived line NIH:N population were attributed to a pharmacokineticdifference at 4-6 weeks of age, whereas no such strain differencein susceptibility was detected at 8-10 weeks of age (Schweri etal., 1983b). Although the plasma t_1/2 of $beta$ -CCM in rats is short(~3 min) (Schweri et al., 1983a), experiments in mice have demonstratedactive drug effects in behavioral paradigms for at least 30 minafter injection at subconvulsant doses (Prado de Carvalho et al.,1984). However, it seems unlikely that pharmacokinetic differencescould explain our results because (1) we phenotyped animals at8-10 weeks of age, (2) the A and B6 lines differ for many chemoconvulsants(Kosobud and Crabbe, 1990), and (3) seizures usually occur withinthe first 6min.

The Bis4 and Exq1 QTLs reported here are likely to be distinct from previously mapped loci for various mouse seizure phenotypes(Neumann and Seyfried, 1990; Neumann and Collins, 1991, 1992;Rise et al., 1991; Frankel et al., 1994, 1995a,b; Miner and Marley,1995; Clement et al., 1996; Buck et al., 1997; Ferraro et al.,1997; Skradski et al., 1998), and our distal chromosome 4 QTLsupports the chromosomal assignment of Bis1 (Martin et al., 1995).Previous work on genetic correlations among inbred strains withchemoconvulsants (Kosobud and Crabbe, 1990) and the >80 discreteknockout transgenic strains presenting with seizures as a phenotype(Noebels, 1996) suggest a multiplicity of genes affecting seizuresusceptibility. The current mapping of distinct loci specificfor vulnerability to a GABA_A receptor inverse agonist model ofseizures underscores the emerging construct of multigenic, geneticallyheterogenous models of epilepsy, where each mouse model may uniquelyrepresent an underlying seizure mechanism (Anderson et al., 1986;Frankel et al., 1994; McNamara, 1992, 1994). We anticipate thatthe positional cloning and functional analysis of the loci influencing $beta$ -CCM-induced seizures will substantially contribute to our understandingof the basic cellular mechanisms affecting seizure vulnerability.Moreover, the positional cloning of the Exq1 locus with its presumedpleiotropic effects on seizure threshold, open-field, and fear-likebehaviors may provide insights into the pathophysiology of individualdifferences in CNSexcitability.

  FOOTNOTES

Received Oct. 9, 1998; revised March 2, 1999; accepted March 9, 1999.

Correspondence should be addressed to Dr. Howard Gershenfeld, Department of Psychiatry, University of Texas Southwestern MedicalCenter, Dallas, TX 75235-8898.
This project has been generously supported by a National Alliance for Research on Schizophrenia and Depression Young InvestigatorsAward (H.G.), the Southwestern Medical Foundation, National Institutesof Health Grant R01-MH58882 (H.G.), and the KZA Hope Fund. P.E.N.is a Canadian Medical Research Council Scholar. We thank C. B.Taylor, I. L. Weissman, and D. Baltimore for encouragement inthe larval stages of this project. We appreciated helpful conversationswith C. Mathis, J. Crawley, E. Ginns, R. Philibert, E. Remmers,N.Schork, E. Lander, W. Dietrich, W. Berrettini, R. Joho, S. Patel,and W. Frankel, our National Institutes of Health and Universityof Texas Southwestern Medical Center colleagues. We are gratefulto the the Whitehead/Massachusetts Institute of Technology MouseGenome Project, Research Genetics, K. Manly, and the Mouse GenomeInformatics Project for providing the infrastructure for thiswork.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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