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The Journal of Neuroscience, September 15, 2000, 20(18):7059-7066
The Amygdala Modulates Memory Consolidation of Fear-Motivated Inhibitory Avoidance Learning But Not Classical Fear Conditioning
Ann E. Wilensky, Glenn E. Schafe, and Joseph E. LeDoux W. M. Keck Foundation Laboratory of Neurobiology, Center for Neural Science, New York University, New York, New York, 10003
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
Although the lateral and basal nuclei of the amygdala are believed to be essential for the acquisition of Pavlovian fear conditioning, studies using post-training manipulations of the amygdala in the inhibitory avoidance learning paradigm have recently called this view into question. We used the GABAA agonist muscimol to functionally inactivate these nuclei immediately after single-trial Pavlovian fear conditioning or single-trial inhibitory avoidance learning. Immediate post-training infusions of muscimol had no effect on Pavlovian conditioning but produced a dose-dependent effect on inhibitory avoidance. However, pre-training infusions dose-dependently disrupted Pavlovian conditioning. These findings indicate that the amygdala plays an essential role in the acquisition of Pavlovian fear conditioning and contributes to the modulation of memory consolidation of inhibitory avoidance but not of Pavlovian fear conditioning.
Key words: muscimol; memory; acquisition; consolidation; amygdala; inhibitory avoidance
INTRODUCTION
In Pavlovian or classical fear conditioning, a neutral conditioned stimulus (CS) acquires the capacity to elicit defensive responses after association with a noxious unconditioned stimulus (US). Considerable progress has been made in identifying the neural pathways that underlie this type of learning. Lesion, tract tracing, and electrophysiological studies collectively suggest that fear conditioning involves the transmission of sensory information about the CS and US to the lateral nucleus of the amygdala (LA), where alterations in synaptic transmission are thought to encode the key aspects of the learning (LeDoux et al., 1990
; Romanski et al., 1993
Although it is widely accepted that the plasticity underlying Pavlovian fear learning takes place in the amygdala, questions have been raised about the validity of this view (McGaugh et al., 1995
In the present study, we evaluated the possibility that pharmacological manipulations of the amygdala differentially affect memory consolidation of Pavlovian fear conditioning and inhibitory avoidance learning. We infused the GABAA agonist muscimol bilaterally into the LA and adjacent areas either before or immediately after single-trial Pavlovian fear conditioning. Additionally, we directly compared the effects of post-training infusions of muscimol on single-trial inhibitory avoidance learning and Pavlovian fear conditioning.
MATERIALS AND METHODS
Subjects. Subjects were adult male Sprague Dawley rats obtained from Hilltop Labs (Scottdale, PA). Rats were housed individually in plastic Nalgene cages (Nalge Nunc International, Rochester, NY) and maintained on a 12 hr light/dark cycle. Food and water were provided ad libitum throughout the experiment.
Surgery. Rats were given intra-amygdala cannula implants as previously described (Wilensky et al., 1999
Intracranial infusions. Rats were held in the experimenter's lap while dummy cannulas were replaced with 28 gauge infusion cannulas attached to 1.0 µl Hamilton (Reno, NV) syringes via polyurethane tubing. The tubing was back-filled with sesame oil, with a small air bubble separating the oil from the drug. Drugs were infused bilaterally by an infusion pump, and cannulas were left in place for an additional 1 min after infusion to allow diffusion of the drug away from the cannula tip before dummy cannula replacement. A total amount of 0.5 µl of drug or vehicle was infused into each amygdala. This amount was chosen on the basis of autoradiographic studies of the spread of muscimol (Martin, 1991
Apparatus. Pavlovian fear conditioning and testing for contextual conditioning took place in a Plexiglas conditioning chamber with a metal grid floor (model E10-10; Coulbourn Instruments, Lehigh Valley, PA) enclosed within a sound-attenuating chamber (model E10-20). Testing for auditory fear conditioning occurred in a distinct Plexiglas chamber (ENV-001; MedAssociates, Inc, Georgia, VT) fitted with a flat black Formica floor to minimize generalization to context (Schafe et al., 1999
Habituation, auditory fear conditioning, and testing. Behavioral procedures were conducted as previously described (Schafe et al., 1999
Rats were infused before training with either 0.5 µl of artificial CSF (ACSF) or one of five doses of muscimol in ACSF (4.4, 1.1, 0.44, 0.088, or 0.001 nmol/side in 0.5 µl). The highest dose was chosen because of its effectiveness in blocking multiple-trial Pavlovian fear conditioning (Muller et al., 1997
Rats were tested 24 hr later with three 30 sec tones (5 kHz, 75 dB; intertrial interval, 100 sec) and videotaped for later scoring. To measure baseline freezing to the tone testing chamber, the 30 sec period preceding the first tone was scored, as well as seconds freezing during each 30 sec tone. Data were analyzed with ANOVA and Scheffe's post hoc t tests. Differences were considered significant if p < 0.05.
Extinction testing. Rats from the four groups with post-training infusions were presented with three 30 sec, 5 kHz, 75 dB tones every 24 hr until extinction criteria had been met. The extinction criteria, adapted from previously published protocols (Morgan et al., 1993
Contextual fear conditioning and testing. Habituation and training followed the protocol for auditory fear conditioning, except the US was raised to 2 mA to produce robust contextual learning. Training was followed by infusion of either 0.5 µl of 4.4 nmol of muscimol/side or ACSF. At testing, rats were returned to the conditioning chamber, allowed to acclimate for 5 min, and then observed and scored for freezing three times for 30 sec each, with 30 sec intervals between each scoring block. After ~10 min in the training chamber, rats were transferred to the testing chambers for auditory tone testing as described above.
Inhibitory avoidance training and testing. Procedures for inhibitory avoidance training were based on previously published work (Brioni et al., 1989
Rats trained with the 2 mA shock were videotaped during testing to measure freezing to the inhibitory avoidance apparatus. Rats were placed in the light chamber, allowed 10 sec to acclimate to the context, and then recorded for 2.5 min. Freezing data were collected for three 30 sec periods, separated by 30 sec intervals. After the freezing trials, the inhibitory avoidance testing began when the rats turned to face away from the door and continued as described above.
After inhibitory avoidance testing, the 4.4 and 0.001 nmol muscimol and the ACSF groups that received the 0.45 mA shock were trained in the auditory fear conditioning paradigm. Rats in the 4.4 nmol of muscimol/side and ACSF groups received post-training infusions of 4.4 nmol of muscimol/side and 0.5 µl of ACSF, respectively, and the remaining rats received pre-training infusions of 4.4 nmol of muscimol/side.
Histology. To verify infusion cannula tip locations, rats were anesthetized with an overdose of chloral hydrate (600 mg/kg, i.p.) and perfused transcardially with 10% buffered formalin. The brains were post-fixed in 30% sucrose in formalin and subsequently blocked, sectioned on a cryostat at 50-60 µm, and stained for Nissl using either 0.5% cresyl violet or 0.25% thionine. Sections were coverslipped with Permount and examined under light microscopy for tip penetration into the amygdala.
RESULTS
Pre-training functional inactivation of the amygdala dose-dependently impairs acquisition of auditory fear conditioning
Previous studies in our laboratory have shown that pre-training functional inactivation of LBA with high doses of muscimol disrupts acquisition of auditory and contextual fear conditioning (Muller et al., 1997
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Figure 1. Auditory Pavlovian fear conditioning: pre-training infusions. A, Outline of general procedures. B, Cannula tip placement for all animals included in the analysis (drawings adapted from Paxinos and Watson, 1997 p < 0.05). The intermediate dose (0.44 nmol, n = 8) also significantly differed from vehicle (*p < 0.05), whereas the lowest two doses (0.088 nmol, n = 5; 0.001 nmol, n = 5) did not. D, Mean ± SE percent freezing per group during each tone trial. All three trials show the same pattern of significance described in C.
Figure 1B shows the infusion cannula tip locations. These were mostly located in the LA, with a few just outside of the LBA. All cannulas <0.5 mm outside of the LBA were included in the analysis (Martin, 1991
Figure 1C shows the mean ± SE percent freezing averaged across all tones, whereas Figure 1D shows the results for each of the three trials. Baseline freezing scores for the 30 sec period before CS onset did not differ among groups [F(5,31) = 1.11; p > 0.05]. The mean ± SE percent baseline freezing for all animals infused before training was 4 ± 0.77%, indicating that fear did not generalize from the conditioning chamber to the testing chamber. In contrast, the ANOVA for freezing scores during CS presentation showed a significant effect of drug concentration [F(5,31) = 8.38; p < 0.001], with nonsignificant effects for trial [F(2,62) = 1.60] and drug-by-trial interaction [F(10,64) = 0.50]. Consistent with previous work in our laboratory (Muller et al., 1997
Post-training functional inactivation of the amygdala does not impair auditory fear conditioning
We next evaluated whether post-training functional inactivation of LBA with muscimol would affect single-trial auditory fear conditioning similarly to inhibitory avoidance learning (Brioni et al., 1989
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Figure 2. Auditory Pavlovian fear conditioning: post-training infusions. A, Outline of general procedures. B, Cannula tip placement for all animals included in analysis (Paxinos and Watson, 1997
Cannula tip placements were similar to those of the first experiment (Fig. 2B). One animal was excluded from the analysis because of cannula placement in the ventricles.
Figure 2C shows the mean ± SE percent freezing averaged across all tones, whereas Figure 2D shows the results for each of the three trials. Freezing scores for the 30 sec period before CS onset did not differ between groups [F(3,38) = 0.38; p > 0.05]. For freezing scores during the CS, the ANOVA showed a significant effect for trials [F(2,76) = 3.37; p < 0.05], in which trials 1 and 3 were significantly different (p < 0.05). However, no significant effect of drug [F(3,38) = 0.12] or drug-by-trial interaction [F(6,76) = 0.92] was observed. Thus, in contrast to the dose-dependent effect of muscimol on fear retention after pre-training infusions, groups receiving infusions of muscimol immediately after auditory fear conditioning did not differ from controls at any dose.
Another measure of the strength of conditioning is the rate at which the conditioned response extinguishes. If post-training intra-amygdala infusions of muscimol attenuated fear consolidation in a manner not observable after 24 hr, then one would expect muscimol-treated rats to extinguish more quickly than controls. To evaluate this possibility, rats from each post-training infusion group were tested for rate of extinction. The ANOVA revealed that groups did not differ significantly in the average number of days to reach extinction criterion [F(3,19) = 0.43; Fig. 2E]. Thus, although pre-training inactivation disrupts learning, post-training inactivation of the amygdala appears to have no effect on Pavlovian fear conditioning, measured both by freezing in the first three tone trials and by days required to reach extinction.
Post-training functional inactivation of the amygdala does not impair contextual fear conditioning
In the previous two experiments, we evaluated the impact of pre- or post-training functional inactivation of LBA on auditory fear conditioning and found that, unlike in the inhibitory avoidance literature, post-training infusions did not affect the learning. In the third experiment, we evaluated the effects of post-training amygdala inactivation on contextual fear conditioning. Contextual Pavlovian conditioning may parallel inhibitory avoidance learning more closely than auditory Pavlovian conditioning because of the associations with the context in each paradigm. This comparison is particularly relevant in light of a recent report (Vazdarjanova and McGaugh, 1999
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Figure 3. Contextual Pavlovian fear conditioning: post-training infusions. A, Outline of general procedures. Rats were tested for both contextual and auditory fear conditioning. B, Representative cannula tip placement of included animals (Paxinos and Watson, 1997
Figure 3B shows representative infusion cannula tip locations for all rats. Tips were located in or just outside of the LA.
Figure 3C shows the mean ± SE percent freezing averaged across all auditory trials, whereas Figure 3D shows the results for each individual tone. Overall freezing is higher than in experiment 2, presumably because of the higher US intensity. Consistent with the results of the second experiment, the ANOVA showed a significant effect for trial [F(2,42) = 4.54; p < 0.05] between trials 1 and 3 (p < 0.05). However, no significant effect of drug [F(1,21) = 0.06] or drug-by-trial interaction [F(2,42) = 1.19] was observed.
Figure 3E shows the mean ± SE percent freezing averaged across all three context test periods, whereas Figure 3F shows the results for each individual period. As with auditory conditioning, the ANOVA detected no significant effects for group [F(1,21) = 0.86], trial [F(2,42) = 0.52], or group-by-trial [F(2,42) = 0.27]. Thus, in contrast to the finding of Vazdarjanova and McGaugh (1999)
Post-training functional inactivation of the amygdala impairs inhibitory avoidance learning but not Pavlovian fear conditioning
The results of the previous three experiments indicate that neural activity in the amygdala during but not immediately after training is required for acquisition of Pavlovian fear conditioning. In contrast, numerous studies have reported effects of post-training infusions of GABAergic drugs, including muscimol, on memory consolidation of inhibitory avoidance learning (Brioni et al., 1989
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Figure 4. Inhibitory avoidance learning: post-training infusions, 0.45 mA shock. A, Outline of general procedures. Inhibitory avoidance learning was followed by Pavlovian conditioning. B, Cannula tip placement for all animals included in the analysis (Paxinos and Watson, 1997
Figure 4B shows the infusion cannula tip locations, and again, tips were mostly located in the LA. Two animals were excluded from the analysis, one for cannula tip location in the ventricles and the other for an indeterminate cannula placement.
Figure 4, C and D, respectively, shows the mean ± SE latency to enter the dark chamber during training and for the difference between training and testing. The Kruskal-Wallis ANOVA on the difference scores showed a significant effect of group [H (df = 3; n = 47) = 9.76; p < 0.05] with a significant difference between the highest dose group and vehicle controls (p < 0.01) and between the highest dose group and the lowest dose group (p < 0.05). Consistent with previous work (Brioni et al., 1989
We next used rats that had been trained in the inhibitory avoidance task and retrained them in the auditory fear conditioning paradigm. One group of rats received muscimol (4.4 nmol) before training. The other two groups received an immediate post-training infusion of either ACSF or muscimol (4.4 nmol; Fig. 4A). In this manner, we were able to evaluate the impact of post-training functional inactivation of the amygdala on the two single-trial learning paradigms in the same animals with the same cannula placements.
Figure 4E displays freezing scores averaged across all tone trials, whereas Figure 4F shows the data for each of the three tone trials. Freezing scores for retrained rats were somewhat lower than those for naïve animals, which was expected because of previous exposure to the aversive US. The ANOVA showed a significant effect of drug [F(2,32) = 8.15; p < 0.01], with which the pre-infused group differed significantly from both post-infused groups (p < 0.05; Scheffe's test), a significant effect for trial [F(2,64) = 5.75; p < 0.01] between trials 1 and 2 (p < 0.05) and between trials 1 and 3 (p < 0.05), and no significant effect for group-by-trial [F(12,64) = 0.97]. Pre-training infusions of muscimol impaired fear conditioning, whereas rats infused after training did not differ from ACSF-infused controls (p > 0.05). Thus, consistent with our previous experiments, pre-training administration of muscimol into the LBA impaired fear acquisition, whereas, in contrast to inhibitory avoidance, post-training infusions did not affect retention of auditory fear conditioning.
Because we tested our rats at 48 hr in the inhibitory avoidance experiment and at 24 hr in the Pavlovian fear conditioning experiments, it may be argued that this difference is responsible for the different effects observed in the two paradigms. If true, then we would expect to observe impaired retention after 48 hr in rats given immediate post-training infusions of muscimol after Pavlovian conditioning. We therefore analyzed data at 48 hr from rats given extinction training in our second experiment (discussed above). The ANOVA showed no significant effects for drug [F(3,19) = 2.11], trial [F(2,38) = 2.12], or drug-by-trial interaction [F(6,38) = 0.41]. These results are identical to those found at 24 hr after training and fail to support the hypothesis that time of testing significantly affects the results of post-training GABAergic manipulations of the amygdala.
Finally, we addressed the question of whether the differences obtained using Pavlovian fear conditioning and inhibitory avoidance learning paradigms might be attributable to differences in foot shock intensity. For example, evidence suggests that parameters such as foot shock intensity can affect the ability of amnesic agents to interfere with memory, presumably by influencing the rate of memory consolidation (Ray and Bivens, 1968
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Figure 5. Inhibitory avoidance learning: post-training infusions, 2 mA shock. A, Outline of general procedures. B, Cannula tip placement for all animals included in the analysis (Paxinos and Watson, 1997
Figure 5B shows the infusion cannula tip locations, and again, tips were mostly located in the LA. One animal was excluded from the analysis because of damage throughout the LA.
Figure 5C shows the mean ± SE percent freezing averaged across all three context test periods, whereas Figure 5D shows the results for each individual test period. Freezing during the test periods was very low (averages were <10%), and the ANOVA detected no significant effects for group [F(1,13) = 1.23], trial [F(2,26) = 2.24], or group-by-trial interaction [F(2,26) = 2.15]. Therefore, any differences in avoidance latencies between muscimol-treated and vehicle groups cannot be attributed to differences in freezing.
Figure 5, E and F, shows the mean ± SE latency to enter the dark chamber during training and the difference between training and testing. Mann-Whitney U tests showed a significant effect of group on the difference scores (adjusted Z =
2.8; p < 0.01). Thus, even when shock intensity and duration were matched to those used in our Pavlovian fear conditioning experiments, we found a strong modulatory effect on inhibitory avoidance learning with post-training functional inactivation of the amygdala. Collectively, the results of all of our experiments strongly favor the hypothesis that fundamental differences exist with respect to the involvement of the amygdala in memory consolidation of Pavlovian fear conditioning and inhibitory avoidance learning.
DISCUSSION
Although a considerable amount of progress has been made in understanding the neural basis of fear conditioning, the exact role of the amygdala still remains controversial (Cahill et al., 1999
One possible resolution of this controversy is that both views are correct; namely, that in Pavlovian fear conditioning the amygdala serves as the site of plasticity underlying fear learning, whereas in inhibitory avoidance learning the amygdala serves to modulate the strength of aversive memory elsewhere. The experiments in the present paper were designed to test this possibility by directly comparing post-training pharmacological manipulations of the amygdala in both paradigms. Although pre-training functional inactivation of the LBA with muscimol dose-dependently impaired Pavlovian fear conditioning, immediate post-training inactivation had no effect. In contrast, post-training inactivation of the LBA consistently impaired inhibitory avoidance learning. These results are consistent with those of previous studies in which intra-amygdala administration of AP-5 impaired Pavlovian fear conditioning if given before, but not immediately after, training (Maren et al., 1996b
Procedural differences exist between Pavlovian fear conditioning and inhibitory avoidance learning that may account for the different role of the amygdala in each paradigm. In the former, the animal is presented with tones (CS) and shocks (US) independent of its behavior. However, inhibitory avoidance learning is an example of instrumental learning, in which shock delivery is contingent on the animal's response. It is thus likely that the ability to affect one kind of learning and not the other with post-training manipulations of the amygdala reflects differences in the relative complexity of the neural network underlying each type of learning. Indeed, a number of lesion studies have implicated the entorhinal and parietal cortex in late memory phases of inhibitory avoidance learning (Izquierdo et al., 1997
In experiment 3, we found that post-training functional inactivation of the LBA did not affect contextual Pavlovian fear conditioning. This finding stands in contrast to one recent report (Vazdarjanova and McGaugh, 1999
Another, potentially more substantive, difference between the two sets of experiments lies in the drugs used to inactivate the amygdala. Although both muscimol and lidocaine reversibly inactivate the amygdala, muscimol agonizes the ionotropic GABAA receptor to inhibit neural transmission, whereas lidocaine is believed to inhibit transmission by inactivating Na+ channels using the cAMP signaling pathway (Onozuka et al., 1993
The results of the present study clearly indicate that amygdala inactivation differentially affects inhibitory avoidance and Pavlovian conditioning and that pre-training, but not post-training, functional inactivation of the LBA impairs acquisition of Pavlovian fear conditioning to both contextual and auditory stimuli (Muller et al., 1997
FOOTNOTES Received April 21, 2000; revised June 27, 2000; accepted June 28, 2000.
This research was supported in part by National Institute of Mental Health Grants RO1 MH46516, KO2 MH00956, and R37 MH38774 and by a grant from the W. M. Keck Foundation to New York University. We thank Karim Nader for helpful comments about this manuscript and Nicole Nadel and Annemieke Schoute for assistance with the histology.
A.E.W. and G.E.S. contributed equally to this work.
Correspondence should be addressed to Dr. Joseph E. LeDoux, Center for Neural Science, New York University, 4 Washington Place, Room 809, New York, NY 10003. E-mail: ledoux{at}cns.nyu.edu.
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