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The Journal of Neuroscience, August 6, 2008, 28(32):8074-8085; doi:10.1523/JNEUROSCI.4904-07.2008
Previous Article | Next Article
Behavioral/Systems/Cognitive
Impaired Fear Extinction Learning and Cortico-Amygdala Circuit Abnormalities in a Common Genetic Mouse Strain
Kathryn Hefner,1 * Nigel Whittle,2 * Jaynann Juhasz,1 Maxine Norcross,1 Rose-Marie Karlsson,1 Lisa M. Saksida,3 Timothy J. Bussey,3 Nicolas Singewald,2 andAndrew Holmes1 1Section on Behavioral Science and Genetics, Laboratory for Integrative Neuroscience, National Institute on Alcoholism and Alcohol Abuse, National Institutes of Health, Rockville, Maryland 20852, 2Department of Pharmacology and Toxicology, Institute of Pharmacy and Center for Molecular Biosciences Innsbruck, University of Innsbruck, A-6020 Innsbruck, Austria, and 3Department of Experimental Psychology and Medical Research Council and Wellcome Trust Behavioural and Clinical Neuroscience Institute, University of Cambridge, Cambridge CB2 3EB, United Kingdom
Abstract
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Abstract
Introduction
Fear extinction is a form of new learning that results in the inhibition of conditioned fear. Trait deficits in fear extinction are a risk factor for anxiety disorders. There are few examples of naturally occurring animal models of impaired extinction. The present study compared fear extinction in a panel of inbred mouse strains. This strain survey revealed an impairment in fear extinction in 129/SvImJ (129S1). The phenotypic specificity of this deficit was evaluated by comparing 129S1 and C57BL/6J for one-trial and multitrial fear conditioning, nociception, and extinction of conditioned taste aversion and an appetitive instrumental response. 129S1 were tested for sensitivity to the extinction-facilitating effects of extended training, as well as D-cycloserine and yohimbine treatment. To elucidate the neural basis of impaired 129S1 fear extinction, c-Fos and Zif268 expression was mapped after extinction recall. Results showed that impaired fear extinction in 129S1 was unrelated to altered fear conditioning or nociception, and was dissociable from intact appetitive extinction. Yohimbine treatment facilitated extinction in 129S1, but neither extended extinction training nor D-cycloserine treatment improved 129S1 extinction. After extinction recall, 129S1 showed reduced c-Fos and Zif268 expression in the infralimbic cortex and basolateral amygdala, and elevated c-Fos or Zif268 expression in central nucleus of the amygdala and medial paracapsular intercalated cell mass, relative to C57BL/6J. Collectively, these data demonstrate a deficit in fear extinction in 129S1 associated with a failure to properly engage corticolimbic extinction circuitry. This common inbred strain provides a novel model for studying impaired fear extinction in anxiety disorders.
Key words: fear; extinction; anxiety; gene; prefrontal cortex; amygdala; intercalated cell masses
Introduction
Fear extinction is a form of learning in which the expression of a conditioned fear response is reduced after repeated experience of a conditioned stimulus in the absence of an unconditioned aversive stimulus (Pavlov, 1927). There is growing evidence that fear conditioning and fear extinction are independent forms of learning that are mediated by partially dissociable neural mechanisms (Kamprath and Wotjak, 2004
At the molecular level, extinction acquisition deficits are caused, for example, by upregulation of cyclin-dependent kinase 5 (Sananbenesi et al., 2007
2-adrenoreceptor antagonism (Cain et al., 2004
Fear extinction is readily quantifiable in laboratory rodents, providing important behavioral models for translational studies of anxiety disorders (Cryan and Holmes, 2005
Materials and Methods
Subjects. Subjects were male 129S1/SvImJ, A/J, BALB/cByJ, C57BL/6J, DBA/2J, and FVB/NJ strains. These strains were chosen on the basis of their frequent use in behavioral neuroscience, including as genetic backgrounds for mutants and inclusion as "group A" priority strains in the Mouse Phenome Project, an international effort to provide the biomedical research community with phenotypic data on the most commonly used mouse strains (www.jax.org/phenome). For experiments conducted at the National Institutes of Health, mice were obtained at8 weeks of age from The Jackson Laboratory and housed (two to four per cage) side-by-side in a temperature (22 ± 1°C)- and humidity (45 ± 15%)-controlled vivarium under a 12 h light/dark cycle (lights on, 6:00 A.M.). The IEG activation experiments were conducted in Innsbruck. These mice were obtained from Charles River and housed (four to five per cage) side-by-side in a temperature (22 ± 2°C)- and humidity (50–60%)-controlled vivarium under a 12 h light/dark cycle (lights on, 7:00 A.M.). The number of mice used in each experiment is given in the figure legends. All experimental procedures were approved by the National Institute on Alcohol Abuse and Alcoholism Animal Care and Use and Austrian Ethical Committees on Animal Care and Use (Bundesministerium für Wissenschaft und Forschung) and followed the National Institutes of Health guidelines outlined in Using Animals in Intramural Research and the local animal care and use committees.
Strain survey of fear extinction. Fear extinction was assessed based on methods described previously (Izquierdo et al., 2006a
Twenty-four hours later, initial fear recall and within-session fear extinction were tested. Mice were placed in a novel context (black/white-checkered walls, solid-Plexiglas, opaque floor, cleaned with a 70% ethanol/30% water solution), housed in a different room from conditioning. After 180 s, there were 50 x 30 s CS presentations (5 s no-stimulus interval). Twenty-four hours later, extinction recall was tested using the same procedure as the previous day.
Freezing was measured as an index of fear (Blanchard and Blanchard, 1969
Behavioral specificity of extinction deficit in the 129S1 strain. On the basis of the strain comparison data revealing a marked deficit in fear extinction in the 129S1 strain, we next assessed the behavioral specificity of the deficit in this strain.
Fear conditioning. Failure of 129S1 to show extinction could result from either an extinction deficit per se or an inability of an intact extinction memory to overcome an excessive fear memory. We therefore examined whether impaired fear extinction in 129S1 mice was dissociable from an increase in fear. In one experiment, 129S1 (and for comparison, C57BL/6J) mice were conditioned using the same three tone–shock protocol described above and, 24 h later, tested for fear recall via average freezing over three CS presentations (Yang et al., 2008
Nociception. To exclude the possibility that increased pain perception could confound fear extinction, 129S1 (and for comparison, C57BL/6J) mice were tested on the hot plate and Von Frey tests. The hot plate test apparatus was a flat plate (Columbus Instruments) heated to 55°C on which the mouse was placed (Boyce-Rustay and Holmes, 2006
Extinction of appetitive instrumental response. We next evaluated extinction to a nonaversive, appetitively motivated form of learning. 129S1 (and for comparison, C57BL/6J) were tested for extinction of an instrumental response using a touchscreen-based operant system described previously [for details of apparatus, see Izquierdo et al. (2006b)
For the task proper, mice were required to respond to stimuli (1 x 2.8 cm2 white square per window) to obtain reward. Stimuli remained on the screen until a response was made, with 30 trials (5 s ITI) per session. Criterion was performing 30 trials within 12.5 min on each of five consecutive sessions. Next, extinction of the response was tested in sessions during which responses to the stimulus were no longer rewarded. Criterion was a two session average of 75% or more response omissions. The dependent measure was the number of trials to reach the acquisition and extinction criteria.
Extinction of conditioned taste aversion. To assess whether impaired fear extinction occurred in another test of extinction to an aversive learning event, 129S1 (and for comparison, C57BL/6J) were tested for extinction of a conditioned taste aversion (CTA) as described previously (Jacobson et al., 2006
Extinction was assessed over 13 daily sessions. The procedure was the same as for habituation days, except that mice were offered two tubes, one containing 0.5% saccharin and one containing water, for 40 min during each twice daily presentation, with the left/right side of the water- versus saccharin-containing tubes counterbalanced across days and experimental groups. A daily aversion index was calculated as fluid consumed from water-contained tube/total fluid consumed from both tubes; with an index score closer to 1.0 indicating maximum aversion.
To assess unconditioned saccharin preference, an additional experiment was conducted in naive mice. Mice were tested as above with the exception that LiCl was replaced with saline, and saccharin preference was measured on days 8–10 only.
Behavioral and pharmacological influences on fear extinction in 129S1. We next conducted a series of experiments to test whether the extinction deficit in 129S1 mice was rescued by behavioral or pharmacological manipulations.
Extended massed-trial extinction. To examine whether 129S1 mice would demonstrate extinction over an extended massed-trial extinction protocol, mice were tested on a 100 trial extinction protocol followed by a 50 trial extinction recall protocol.
Effects of D-cycloserine treatment. Systemic treatment with the NMDAR partial agonist D-cycloserine facilitates fear extinction in rodents and has proven to be effective as an adjunct to exposure therapy in human anxiety disorders (Davis et al., 2006
Effects of yohimbine treatment. Systemic treatment with the
Extinction-related cortico-amygdala IEG activation. We next sought to identify neural correlates of the extinction deficit in 129S1 using IEG expression as a marker for neuronal activity (Singewald, 2007
For IEG analysis, mice were deeply anesthetized with an overdose of sodium pentobarbital (200 mg/kg) and transcardially perfused with 20 ml of 0.9% saline followed by 20 ml of 4% paraformaldehyde in 0.1 mol/L PBS, pH 7.4. Brains were then removed and postfixed at 4°C overnight in 4% paraformaldehyde in PBS. Coronal sections (50 µm) were cut with a vibratome (Ted Pella) and collected in immunobuffer. The sections were processed for (1) c-Fos immunoreactivity as described previously (Singewald et al., 2003
Fear-related cortico-amygdala IEG activation. To test for possible strain differences in immediate-early gene activation after fear recall per se, an additional control experiment was conducted. 129S1 and C57BL/6J mice were conditioned as above for extinction-related immediate-early gene analysis and, 24 h later, exposed to 1 x 30 s tone presentation before being killed and processed for immediate-early gene analysis 2 h later, as above.
Statistics. The effects of strain x tone-trial/block, session, or day on freezing, instrumental responses, or taste aversion index were analyzed using two-factor ANOVA, with repeated measures for tone-trial/block, session, or day, followed by Bonferroni's post hoc analysis. In the presence of a significant interaction in this initial strain profile, within-session strain profiles were either analyzed via separate repeated-measures ANOVA. Effects of strain and condition on IEG expression after fear recall were analyzed using unpaired t tests. Effects of strain by condition on IEG expression after fear recall were analyzed using two-factor ANOVA followed by Bonferroni's post hoc analysis. Correlations between freezing during extinction recall and number of c-Fos and Zif268 cells were performed using the Spearman's coefficient test. The threshold for statistical significance was set at p < 0.05 (statistical results below this threshold are not described).
Results
Strain survey of fear extinction
There was a significant strain x tone-trial/block interaction for freezing during conditioning (F(15,186) = 3.43; p < 0.01), extinction (F(45,558) = 2.67; p < 0.01), and extinction recall (F(45,558) = 1.86; p < 0.01) sessions. For clarity, the profiles of each of the six strains are presented separately in Figure 1. During conditioning, all strains showed a significant increase in freezing across trials (all p < 0.01) with the exception of A/J, which had high baseline freezing. During extinction, DBA/2J, FVB/NJ, BALB/cByJ, and C57BL/6J showed a significant decrease in freezing across trial-blocks (all p < 0.01). Neither A/J nor 129S1 showed a significant decrease in freezing during the extinction session. All strains (all p < 0.01) except 129S1 displayed a significant decrease in freezing during the extinction recall session.
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Figure 1. Survey of fear extinction across inbred strains. All strains except 129S1 showed a significant reduction in conditioned fear over at least one extinction session. Cond, Conditioning; Ext recall, extinction recall. n = 7–14/strain. *p < 0.05, significant change over trials. Data in Figures 1
Behavioral specificity of extinction deficit in the 129S1 strain
Fear conditioning
There were no differences between 129S1 and C57BL/6J in fear recall after either 3x tone–shock (Fig. 2A, right) or 1x tone–shock (Fig. 2A, left) conditioning protocols.
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Figure 2. Fear conditioning and nociception in 129S1 mice. A, Fear recall was no different between 129S1 (S1) and C57BL/6J (B6) after either 1x tone–shock conditioning (n = 15/strain) or 3x tone–shock conditioning (n = 15/strain). B, Nociceptive responses were no different between S1 and B6 in either the hot plate or von Frey tests (n = 11/strain).
Nociception
Neither hot plate response latencies (Fig. 2B, left) nor Von Frey responses (Fig. 2B, right) differed between 129S1 and C57BL/6J.Extinction of appetitive instrumental behavior
There was no significant effect of strain for trials to extinguish the instrumental behavior (129S1, 130 ± 18 trials; C57BL/6J, 120 ± 7 trials) (sessions 1–5 are shown in Fig. 3A). There was a significant effect of strain for trials to acquire an appetitively driven instrumental response behavior (F(1,18) = 4.70; p < 0.05) because of faster learning in 129S1 (8.7 ± 1.4 trials to criterion) than C57BL/6J (13.4 ± 1.6 trials to criterion).
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Figure 3. Extinction of an appetitive instrumental behavior and extinction of conditioned taste aversion in 129S1 mice. A, 129S1 (S1) and C57BL/6J (B6) showed similar rates extinction of an appetitively motivated instrumental response (n = 9–11/strain). B, 129S1 showed lesser initial expression of conditioned taste aversion and no reduction in the aversion over extinction sessions, compared with B6 (n = 9/strain).
Extinction of conditioned taste aversion
There was a significant strain by day interaction for aversion index during CTA extinction (F(12,192) = 2.92; p < 0.01). The aversion index in C57BL/6J was significantly higher than in 129S1 during the first two sessions (p < 0.01), and there was a significant decrease in the aversion index across sessions in C57BL/6J (F(12,96) = 17.26; p < 0.01) but not 129S1 (Fig. 3B). Malaise scores were no different between strains (129S1 = 0.58 ± 0.11; C57BL/6J = 0.47 ± 0.12). Unconditioned C57BL/6J showed a clear preference for saccharin over water (80 ± 4.4% preference), whereas unconditioned 129S1 showed no preference (49 ± 5.9% preference) (n = 7/strain).Behavioral and pharmacological influences on fear extinction in 129S1
Extended massed-trial extinction
129S1 showed no decrease in freezing over two sessions in an extended massed-trial protocol (Fig. 4A).
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Figure 4. Effects of behavioral and pharmacological manipulations on fear extinction in 129S1 mice. A, Extended massed-trial extinction did not reduce conditioned fear (n = 7). B, D-Cycloserine treatment during extinction did not reduce conditioned fear during extinction recall (n = 9/dose). C, Yohimbine treatment during extinction significantly reduced conditioned fear during extinction recall relative to vehicle treatment (n = 9–10/dose). *p < 0.05 versus vehicle.
Effects of D-cycloserine
There was no significant effect of D-cycloserine treatment on freezing during extinction recall in 129S1 mice (Fig. 4B). D-Cycloserine treatment significantly reduced freezing during extinction recall in C57BL/6J mice (F(3,49) = 2.80, p = 0.05; vehicle, 72.0 ± 6.2%; 5 mg/kg, 50.7 ± 6.4%; 15 mg/kg, 52.6 ± 4.8%; 30 mg/kg, 53.1 ± 6.0%; p < 0.05, all doses vs vehicle; n = 12–14/dose).Effects of yohimbine
There was a significant effect of yohimbine treatment on freezing during extinction recall (F(2,26) = 5.16; p < 0.05). Mice previously treated with either 2.5 or 5.0 mg/kg showed significantly less freezing than vehicle-treated controls (Fig. 4C).Extinction-related cortico-amygdala IEG activation
129S1 showed significantly more freezing than C57BL/6J over the extinction recall session (129S1, 65.3 ± 1.6%; C57BL/6J, 4.5 ± 0.9%; t(13) = 12.58; p < 0.01) and the first tone presentation per se (129S1, 74.0 ± 5.4%; C57BL/6J, 23.8 ± 5.1%; t(13) = 6.72; p < 0.01). There was a significant strain by condition interaction for the number of c-Fos-positive cells in the infralimbic cortex (IL) (1.78 mm from bregma, F(1,19) = 34.55, p < 0.01; 1.54 mm from bregma, F(1,19) = 9.47, p < 0.01), the basolateral (F(1,19) = 38.43; p < 0.01) and central nucleus (F(1,19) = 15.72; p < 0.01) of the amygdala. Although all three regions show higher c-Fos expression after extinction recall relative to CS minus baseline control levels in both strains, after extinction recall 129S1 mice exhibited fewer c-Fos-positive cells in the infralimbic cortex (Fig. 5A) and basolateral amygdala (Fig. 5B), and more positive cells in the central amygdala (Fig. 5C) than C57BL/6J. The cingulate cortex (1.78 mm from bregma, F(1,19) = 68.24, p < 0.01; 1.54 mm from bregma, F(1,19) = 177.56, p < 0.01; 1.10 mm from bregma, F(1,19) = 143.48, p < 0.01), prelimbic cortex (1.78 mm from bregma, F(1,19) = 220.43, p < 0.01; 1.54 mm from bregma, F(1,19) = 149.06, p < 0.01), lateral amygdala (F(1,19) = 35.77; p < 0.01), medial posterodorsal (F(1,19) = 91.49; p < 0.01), medial posteroventral (F(1,19) = 58.73; p < 0.01), anterior cortical (F(1,19) = 47.57; p < 0.01), and posterolateral cortical (F(1,19) = 58.88; p < 0.01) regions all expressed significantly more c-Fos-positive cells after extinction recall than after CS minus baseline conditions but did not differ between strains (Table 1). No other brain regions examined were significantly affected by condition or strain (Table 1).
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Figure 5. c-Fos expression after extinction recall. A, 129S1 (S1) mice showed a lesser increase (relative to CS minus baseline) in c-Fos-positive cells in the IL than C57BL/6J (B6) after extinction recall. B, S1 mice showed a lesser extinction-related increase in c-Fos-positive cells in the BLA than B6 after extinction recall. C, S1 mice showed a greater increase in c-Fos-positive cells in CeA than B6 after extinction recall. D, The number of c-Fos-positive cells in IL (but not BLA or CeA) (see Results) was highly negatively correlated with freezing during extinction recall. n = 7–8/strain for extinction recall; n = 4/strain for baseline. cc, Correlation coefficient. Scale bars, 100 µm. **p < 0.01 129S1 versus B6; ##p < 0.01, #p < 0.05 versus baseline.
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Table 1. Strain differences in c-Fos expression in cortical and amygdaloid regions after extinction recall
There was a significant strain by condition interaction for the number of Zif268-positive cells in the infralimbic cortex (1.78 mm from bregma, F(1,19) = 30.74, p < 0.01; 1.54 mm from bregma, F(1,19) = 14.32, p < 0.01), the lateral (F(1,19) = 17.22; p < 0.01) and basolateral nuclei of the amygdala (F(1,19) = 33.97; p < 0.01), and the Imp ITC mass (F(1,19) = 23.80; p < 0.01). Although these five regions show higher Zif268 expression after extinction recall relative to CS minus baseline control levels in both strains, after extinction recall 129S1 mice exhibited fewer Zif268-positive cells in the infralimbic cortex (Fig. 6A) and lateral amygdala (Fig. 6B), and more positive cells in Imp (Fig. 7B) than C57BL/6J. The secondary motor (F(1,19) = 153.97; p < 0.01), cingulate cortex (1.78 mm from bregma, F(1,19) = 109.96, p < 0.01; 1.10 mm from bregma, F(1,19) = 8.88, p < 0.01), prelimbic cortex (1.78 mm from bregma, F(1,19) = 97.41, p < 0.01; 1.54 mm from bregma, F(1,19) = 77.67, p < 0.01), central nucleus (F(1,19) = 72.11; p < 0.01), Ilp ITC mass (F(1,19) = 34.25; p < 0.01), medial posterodorsal (F(1,19) = 155.19; p < 0.01), medial posteroventral (F(1,19) = 62.88; p < 0.01), and posterolateral cortical (F(1,19) = 49.56; p < 0.01) regions all expressed significantly more Zif268-positive cells after extinction recall than after CS minus baseline but did not differ between strains (Table 2). No other brain regions examined were significantly affected by condition or strain (Table 2).
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Figure 6. Zif268 expression after extinction recall. A, 129S1 (S1) mice showed a lesser increase (relative to CS minus baseline) in Zif268-positive cells in the IL than C57BL/6J (B6) after extinction recall. B, S1 mice showed a lesser increase in Zif268-positive cells in LA than B6 after extinction recall. C, S1 mice showed a lesser increase in Zif268-positive cells in the BLA than B6 after extinction recall. D, Across strains, the number of Zif268-positive cells in IL (but not BLA or CeA) (see Results) was negatively correlated with freezing during extinction recall. n = 7–8/strain for extinction recall; n = 4/strain for baseline. cc, Correlation coefficient. Scale bar, 100 µm. **p < 0.01 129S1 versus B6; ##p < 0.01, #p < 0.05 versus baseline.
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Figure 7. Zif268-positive cells identified in the ITC masses of the amygdala after extinction recall. Representative illustration of anatomical definition of ITC mass nuclei labeled with Zif268 immunoreactivity. A, Anatomical definition of Zif268-expressing medial paracapsular ITC mass (Imp) and lateral paracapsular ITC mass (Ilp). Scale bar, 500 µm. B, 129S1 (S1) mice showed a greater increase (relative to CS minus baseline) in Zif268-positive cells in Imp (but not Ilp) (Table 1) than C57BL/6J (B6) after extinction recall. Scale bar, 100 µm. C, Across strains, the number of Zif268-positive cells in Imp was positively correlated with freezing during extinction recall. n = 7–8/strain for extinction recall; n = 4/strain for baseline. cc, Correlation coefficient; ic, internal capsule; LA, lateral nucleus; ec, external capsule; CeA, central nucleus; BLA, basolateral nucleus; opt, optic tract; Imp, medial paracapsular nucleus; Ilp, lateral paracapsular nucleus. **p < 0.01 129S1 versus B6; ##p < 0.01 versus baseline.
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Table 2. Strain differences in Zif268 expression in cortical and amygdaloid regions after extinction recall
Correlational analysis of the whole sample (i.e., both strains) revealed a significant negative correlation between percentage freezing during first tone presentation during extinction recall and the number of c-Fos-positive (–0.83, p < 0.01, 1.74 mm from bregma; –0.75, p < 0.01, 1.54 mm from bregma) (Fig. 5D) and Zif268-positive (–0.77, p < 0.01, 1.74 mm from bregma; –0.80, p < 0.01, 1.54 mm from bregma) (Fig. 6D) cells in the infralimbic cortex. Significant negative correlation was also observed between extinction recall freezing and c-Fos (–0.75; p < 0.01)- and Zif268 (–0.77; p < 0.01)-positive cells in the basolateral amygdala, as well as Zif268-positive cells in the lateral amygdala (–0.79; p < 0.01). Finally, there was a significant positive correlation between extinction recall freezing and the number of c-Fos-positive cells in the central amygdala (0.87; p < 0.01) and the number of Zif268-positive cells in the medial paracapsular ITC (0.80; p < 0.01) (Fig. 7C, Tables 1, 2). No other brain region correlated significantly with freezing during extinction recall.Fear-related cortico-amygdala IEG activation
129S1 and C57BL/6J did not significantly differ in freezing during fear recall (129S1, 55.2 ± 3.5%; C57BL/6J, 51.6 ± 5.2%; NS). There was no significant effect of strain on the number of either c-Fos- or Zif268-positive cells in any brain region examined (Table 3) (all NS) after fear recall.
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Table 3. Absence of strain differences in c-Fos or Zif268 expression in cortical and amygdaloid regions after fear recall
Discussion
The major finding of the present study was the identification of a significant and selective impairment in fear extinction in a common inbred mouse strain, 129S1/SvImJ (129S1). This phenotype was associated with abnormal activation of a key prefrontal-amygdala pathway mediating fear extinction.Our initial strain survey was the broadest conducted to date and revealed marked differences in fear extinction across inbred strains. Although not the focus of our study, we observed strain differences in the acquisition and expression of conditioned fear per se, in line with previous reports comparing various strains (Paylor et al., 1993
Of the strains currently tested, the most striking extinction profile was exhibited by the 129S1 strain. 129S1 showed no apparent short-term extinction learning over 2 x 50 trial massed extinction sessions and no long-term extinction recall. Although A/J also showed poor within-session extinction, as previously reported (Owen et al., 1997
Fear extinction in 129S1 was not improved by providing additional massed extinction trials. Nor was it facilitated by treatment with the partial NMDAR agonist D-cycloserine. This differs from the extinction facilitating effects of D-cycloserine in conditioned freezing or fear-potentiated startle paradigms in C57BL/6J mice (Tomilenko and Dubrovina, 2007
Deficient fear extinction in 129S1 was associated with a striking alteration in the activation profile of a key prefrontal-amygdala circuit mediating fear extinction. This was assayed via expression of the IEG c-Fos, a surrogate marker for neuronal activation (Singewald, 2007
Impaired fear extinction in 129S1 was not associated with blunted IL activation alone, but instead reflected a circuit level failure. 129S1 showed lesser IEG expression than C57BL/6J in BLA (but not medial or cortical amygdala subnuclei) after extinction. They also showed lesser induction of Zif268, but not c-Fos, in LA. Although the functional significance of this subnuclei dissociation between the two IEGs is not clear, it is in full agreement with the finding of low Zif268, not c-Fos, expression in the LA of poor extinguishing C57BL/6J mice after extinction recall (Herry and Mons, 2004
The ITC cell masses of the amygdala are posited to be another important component of the extinction circuit (Paré et al., 2004
In summary, through a strain survey, we identified an inbred mouse strain, 129S1, with a marked deficit in fear extinction. The extinction deficit in this strain was dissociable from fear conditioning and extinction of an instrumental appetitive behavior, both of which were normal in 129S1. 129S1 were resistant to the extinction facilitating effects of extended massed training and treatment with D-cycloserine, but yohimbine treatment improved long-term extinction. Analysis of neural activation after extinction recall revealed hypoactivation of IL and BLA, differential activation of the ITCs, and hyperactivation of CeA in 129S1 relative to C57BL/6J. Although previous studies have produced fear extinction deficits by neuroanatomical lesions, gene mutations, and selected breeding, the 129S1 mouse is a naturally occurring example of impaired fear extinction and cortico-amygdala dysfunction in an animal model. This provides an opportunity to study sources of genetic variation driving differences in extinction. More generally, given the increasing convergence of rodent and human studies of emotional disorders and extinction in particular (Holmes and Hariri, 2003
Note added in proof. At the time the current article was going to press, two important studies were published further describing the role of the amygdala and ITC masses in rodent fear extinction (Herry et al., 2008
Footnotes
Received Oct. 30, 2007; revised June 5, 2008; accepted June 25, 2008.*K.H. and N.W. contributed equally to this work.
This work was supported by National Institute of Alcohol Abuse and Alcoholism Intramural Research Program Grant Z01-AA000411 and Fonds zur Förderung der Wissenschaftlichen Forschung Grant NFN-S102 (N.S.). We are grateful to Benjamin Palachick and Michael Feyder for technical assistance, Laura Jacobson for helpful advice on conditioned taste aversion methodology, and Francesco Ferraguti, Denis Pare, and Gregory Quirk for discussion of the ITC masses.
Correspondence should be addressed to Dr. Andrew Holmes, Section on Behavioral Science and Genetics, Laboratory for Integrative Neuroscience, National Institute on Alcohol Abuse and Alcoholism, 5625 Fishers Lane, Room 2N09, Rockville, MD 20852-9411. Email: holmesan{at}mail.nih.gov
Copyright © 2008 Society for Neuroscience 0270-6474/08/288074-12$15.00/0
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