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The Journal of Neuroscience, January 15, 2001, 21(2):676-681
Amygdala Regulation of Nucleus Accumbens Dopamine Output is Governed by the Prefrontal Cortex
Mark E. Jackson and Bita Moghaddam Department of Psychiatry, Yale University School of Medicine, West Haven, Connecticut 06516
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
A dynamic interaction between the prefrontal cortex (PFC), amygdala, and nucleus accumbens (NAc) may be fundamental to regulation of goal-directed behavior by affective and cognitive processes. This study demonstrates that a mechanism for this triadic relationship is an inhibitory control by prefrontal cortex on accumbal dopamine release during amygdala activation. In freely moving rats, microstimulation of basolateral amygdala at intensities that produced mild behavioral activation produced an expected rapid increase in glutamate efflux in the prefrontal cortex and the nucleus accumbens shell region of the ventral striatum. However, during the stimulation, dopamine release increased only in the prefrontal cortex, not in the nucleus accumbens. An increase in accumbal dopamine release was observed during the stimulation if glutamate activation in the prefrontal cortex was inhibited at either presynaptic or postsynaptic levels. Some behaviors expressed during the stimulation were intensified in animals in which prefrontal cortex glutamate activation was blocked. In addition, these animals continued to express stimulus-induced behaviors after the termination of stimulation, whereas normal poststimulus behaviors such as ambulation and grooming were not displayed as frequently. Considering that dopamine neurotransmission in the nucleus accumbens is thought to play an integral role in goal-directed motor behavior, these findings suggest that the prefrontal cortex influences the behavioral impact of amygdala activation via a concomitant active suppression of accumbal dopamine release. Absence of this cortical influence appears to result in an aberrant pattern of behavioral expression in response to amygdala activation, including behavioral perseveration after stimulus termination.
Key words: AMPA; striatum; ventral tegmental area; metabotropic glutamate receptors; schizophrenia; motivation
INTRODUCTION
As components of the limbic system, the amygdala, nucleus accumbens (NAc), and prefrontal cortex (PFC) are involved in interdependent functional modalities that coordinate emotional and cognitive behavior. The amygdala is thought to mediate the processing and expression of emotional behavior (Davis, 1992
; LeDoux, 1992
Multidisciplinary lines of investigation have described close anatomical and functional interactions between these structures. For example, reciprocal projections between subregions of the amygdala and PFC (Kelley et al., 1982
To explore the mechanisms by which PFC can modulate the dynamic interaction between BLA and NAc, we focused on dopamine release in the NAc of awake animals as a behaviorally relevant functional output measure. The dopaminergic innervation of the NAc is strongly implicated in the mediation of goal-directed behavior (Kelley et al., 1986
MATERIALS AND METHODS
Animal preparation. All animal procedures were conducted in accordance with the National Institutes of Health Guide for the Care and Use of Laboratory Animals and were approved by the Yale University Animal Care and Use Committee. Male Sprague Dawley rats (280-350 gm) were anesthetized with halothane and placed in a stereotaxic frame with blunt ear bars. A small incision (7-10 mm) was made in the skin over the skull. The wound margin was infiltrated with lidocaine. Concentric microdialysis probes were implanted into the PFC [anteroposterior (AP), +3.2; lateral (L), 0.8; ventral (V), 5.3] and the NAc (AP, +1.4; L, 1.1; V, 8.3). A bipolar stainless steel electrode was implanted into the ipsilateral BLA (AP,
3.2; L, 5.0; V, 8.0). All coordinates are relative to bregma and according to the atlas of Paxinos and Watson (1982)
Drugs and chemicals. LY354740 and LY293558 were gifts from Eli Lilly (Indianapolis, IN). Stock solutions (10 mM in H20) were prepared and kept frozen. Before use, stock solutions were diluted in the perfusion solution to a concentration of 1 µM for LY354740 and 100 µM for LY293558.
Microdialysis procedure. Concentric microdialysis probes with an outer diameter of 330 µm and exposed tips of 3.0 mm (for PFC) and 2.0 mm (for NAc) were used. The perfusion solution contained (in mM): 145 NaCl, 2.7 KCl, 1.0 MgCl2, and 1.2 CaCl2. Probes were perfused at a flow rate of 0.5 µl/min during the recovery period and 2.5 µl/min during the experiment. Dialysis samples were collected every 2 min for glutamate and every 10 min for dopamine. The amount of dopamine and glutamate in the samples was measured by HPLC as described elsewhere (Bagley and Moghaddam, 1997
Experimental procedures. Microdialysis and behavioral data were collected between 11:00 A.M. and 1:00 P.M. and after animals had acclimated to their new environment for ~24 hr. Baseline samples were collected for 1 hr before BLA stimulation. Separate groups of animals were used for dopamine and glutamate microdialysis studies, but data were collected from both PFC and NAc of the same animal. All data presented here are for BLA stimulation-naïve rats; therefore, separate groups of rats were used for the control group (for either glutamate or dopamine measures) and experiments involving intra-PFC perfusion of LY354740 or LY293558. Perfusion solution containing either drug was perfused starting 1 hr before BLA stimulation.
Amygdala stimulation. Stimulation current was provided by a constant current source (Grass, Quincy, MA) driven by a pulse stimulator (Grass). The stimulation was delivered as a train of short bursts (0.5 msec monophasic pulses delivered at 200 pulses/sec for 20 msec, 5 pulses per burst) delivered at 1 sec interburst intervals for a total duration of 10 min.
Behavioral rating. During microdialysis studies, animals were rated for the 10 min periods before, during, and after BLA stimulation. Animals received a score of "0" for absence or "1" for presence of each of the following behaviors: ambulation, defined as movement about the cage; freezing, defined as an alert posture without movement; sniffing, defined as exploratory sniffing of the cage environment; mouth movement, defined as vacuous chewing motions of the mouth without food in the mouth; and jaw tremor, defined as a rapid quivering of the jaw, often resulting in an audible grinding noise. Note that because behaviors were scored if they persisted for at least 30 sec during each 10 min epoch, seemingly contradictory behaviors (i.e., ambulation and freezing) could be observed in the same animal during the same epoch. Animals were scored only once every 10 min for a behavior even if it was exhibited repeatedly and for a duration longer than 30 sec. The scores are presented as the percentage of animals exhibiting defined behaviors for each experimental group. It should be emphasized that because a number of manipulations had to be performed immediately next to the animal (e.g., timed collection of microdialysis samples, turning the stimulator on/off, switching the perfusion solution to a drug-containing one, etc.), the rater was not blind to these manipulations.
Data analysis. All dialysis values given are expressed as percentages of baseline ± SEM. The average concentration of three dialysis samples immediately before stimulation was defined as baseline. Within-group analysis of the main effect of stimulation was performed by using one-way ANOVA with time as the repeated measure. Between-group analysis was performed by using ANOVA with Bonferroni post hoc comparison of means. Behavioral data were analyzed by nonparametric Kruskal-Wallis ANOVA.
Histology. At the end of each experiment, animals were anesthetized with chloral hydrate. The location of the stimulating electrode was marked by passing a 5 mA current through the electrode for 30 sec. Animals were then perfused intracardially with saline followed by 10% buffered formalin. Brains were removed and stored in formalin. Fixed brains were cut at 250 µm intervals, and sections were stained with cresyl violet. Probe placements were verified for all data presented this study and are demonstrated on Figure 1.
RESULTS
Effects of BLA stimulation on glutamate efflux in PFC and NAc
Stimulus parameters, glutamate response in PFC and NAc, and probe and electrode positions are summarized in Figure 1. Electrical stimulation of the BLA produced significant increases in extracellular glutamate in the PFC. This increase was immediate, peaked within 4 min of the beginning of the stimulation period, and persisted above baseline levels for >20 min. BLA stimulation also produced a significant increase in extracellular glutamate in the NAc. The magnitude of this increase was smaller than that observed in the PFC.
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Figure 1. Placements of electrode and microdialysis probes, depiction of stimulus parameters, and glutamate efflux during BLA stimulation. Locations of electrode tips ( ) and lines representing the active surface of microdialysis probes for all animals used in the study are illustrated. Electrode placement was ipsilateral to microdialysis probes in all experiments, but in different rats, placements were made randomly in either the left or right hemisphere. a, Electrode placements were confined to the basolateral amygdala complex. b, PFC probe placements were primarily in infralimbic/prelimbic regions of the medial PFC. c, NAc probe placements were along the border of the shell and medial core. d, BLA stimulation consisted of brief bursts of 50 µA current pulses over a period of 10 min. e, BLA stimulation significantly increased glutamate efflux in the PFC (F = 4.53; p < 0.01; n = 15). f, BLA stimulation also increased glutamate efflux in the NAc (F = 1.69; p < 0.05; n = 10).
Effects of BLA stimulation on dopamine efflux in PFC and NAc
In the PFC, BLA stimulation produced a significant increase in extracellular dopamine levels (Fig. 2), which returned to baseline during the next 40 min. In contrast to the PFC, there was no significant increase in dopamine efflux in the NAc during the period of BLA stimulation. A significant delayed increase was observed after the BLA stimulation was terminated. Dopamine levels in the NAc gradually returned to baseline during the next 50 min.
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Figure 2. Dopamine release during BLA stimulation. BLA stimulation increased extracellular levels of dopamine in both the PFC (F = 6.09; p < 0.01; n = 10) and the NAc (F = 4.65; p < 0.01; n = 10). However, post hoc analysis revealed that NAc dopamine levels did not increase during the period of BLA stimulation when compared with baseline. Asterisks indicate significant differences from baseline (p < 0.05).
Effect of reduction of cortical glutamate activation during BLA stimulation on dopamine release in the NAc
To test the hypothesis that the PFC regulates the output of NAc dopamine during BLA stimulation, we repeated the above experiments while blocking stimulus-induced glutamatergic activation in the PFC. We used two strategies to inhibit PFC glutamate neurotransmission. The first was to infuse into the PFC the selective AMPA/kainate receptor antagonist LY293558 to block postsynaptic glutamate receptor activation. Because this (commonly used) approach produces an indiscriminate blockade of glutamate neurotransmission, we also used another pharmacological strategy that produces presynaptic inhibition of evoked glutamate release (Lovinger and McCool, 1995
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Figure 3. Effect of intra-PFC perfusion of mGluR2/3 agonist LY354740 on glutamate efflux in the PFC during BLA stimulation. Reverse dialysis of LY354740 (1 µM) reduced the glutamate efflux evoked by BLA stimulation (solid line; n = 7) as compared with control animals (dotted line; n = 15) (also depicted in Fig. 1). Two-way repeated-measures ANOVA revealed a significant difference between the groups (F = 12.04; p < 0.01). Asterisks indicate individual samples that were significantly different between groups (p < 0.05). [Of note, we were able to detect LY354740 levels in our HPLC system that were used to detect glutamate, and therefore we were able to confirm that LY354740 did not diffuse from the PFC to the NAc because, during the time that the compound was perfused into the PFC, it was not detected in the dialysate obtained from the probe implanted in the NAc (data not shown).]
In the subsequent experiments, either the AMPA receptor antagonist (LY293558, 100 µM) or the mGluR2/3 agonist (LY354740, 1 µM) was applied to the PFC while dopamine release was measured in both PFC and NAc (Fig. 4). In contrast to control animals in which no increase in NAc dopamine was observed during BLA stimulation, intra-PFC application of either compound resulted in an immediate increase in dopamine release in the NAc (Fig. 4a). In the case of LY293558, dopamine output remained elevated throughout the experiment. Local perfusion of LY354740 or LY293558 into the PFC had no significant effect on dopamine efflux in this region during BLA stimulation (Fig. 4b).
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Figure 4. Effects of local perfusion into PFC of mGluR2/3 agonist LY354740 (1 µM) and AMPA antagonist LY293558 (100 µM) on dopamine efflux in the NAc and PFC during BLA stimulation. Drug perfusion began at least 1 hr before BLA stimulation. a, BLA stimulation increased NAc dopamine efflux with either the mGluR2/3 agonist in the PFC (solid line, ) (F = 3.72; p < 0.01; n = 9) or the AMPA antagonist in the PFC (solid line,
) (F = 4.26; p < 0.01; n = 6). This increase was in contrast to the lack of immediate dopamine increase during BLA stimulation in control rats (dotted line) (also depicted in Fig. 2.). Asterisks indicate significant differences between the control and the other two groups (p < 0.05). b, In the PFC, dopamine increase was evoked by BLA stimulation in the presence of either the mGluR2/3 agonist (solid line,
Behavioral observations
All animals were in a rest/sleep position before the start of BLA stimulation (data not shown). At the onset of the stimulation, animals became fully alert and exhibited several stereotypical behaviors that are listed in Table 1. After the termination of the stimulus, the overall pattern of behavioral expression was different and included behaviors such as grooming and ambulation that were not observed during stimulation.
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Table 1. Behaviors observed during microdialysis sample collection in the 10 min periods during and after BLA stimulation The behaviors displayed by animals with intra-PFC application of LY354740 or LY293558 differed from control animals both during and after BLA stimulation (Table 1). Aberrant behaviors observed during the stimulation, such as mouth movement and jaw tremor, were observed in a significantly higher percentage of these animals. In addition, they continued to express these behaviors after the termination of the stimulus, whereas normal poststimulus behaviors such as ambulation and grooming were observed in significantly fewer animals.
DISCUSSION
Microstimulation of the BLA at intensities that produced relatively mild behavioral activation produced an expected increase in glutamate efflux in the PFC and NAc. However, dopamine release increased only in the PFC, and not in the NAc, during the stimulation. An increase in NAc dopamine release was observed if stimulus-induced activation of glutamate neurotransmission in PFC was blocked, suggesting that PFC exerts an inhibitory control on amygdala-evoked activation of dopamine output in the NAc. The PFC modulation of amygdala-NAc interaction is thought to provide an interface in which cognitive processes, such as on-line retention of internalized information, can influence amygdala-mediated motor behavior (Mogenson et al., 1980
Glutamatergic and behavioral response to BLA stimulation
In agreement with morphological studies describing glutamatergic projections from the BLA to PFC and NAc (Groenewegen and Berendse, 1990
The behaviors exhibited by animals during the BLA stimulation are consistent with the involvement of this region in the expression of fear and anxiety. These behaviors (e.g., freezing, jaw tremor) were quite distinct from behaviors observed after the session of stimulation (e.g., grooming, ambulation) which generally are considered behaviors that contribute to adaptation to external environment. The sustained increase in PFC glutamate efflux may be relevant to the poststimulus behavioral activation. The observation that a normal pattern of poststimulus behavioral expression was not observed in animals in which the increase in glutamate release was blocked by the mGluR2/3 agonist, or when postsynaptic glutamate activation was blocked by an AMPA antagonist, is consistent with a role for PFC glutamate in sustaining the poststimulus behavioral activation.
Dopamine response to BLA activation
BLA stimulation produced a robust increase in dopamine efflux in the PFC. This increase was not blocked by inhibiting glutamate release in the PFC during the stimulation. Thus, it is likely that the activation of dopamine release results from increased neuronal activity in the ventral tegmental area (VTA) in which mesoprefrontal dopamine cell bodies are localized, as opposed to presynaptic regulation of dopamine by glutamate at the terminal (PFC) level. Although convincing evidence for direct projections from BLA to VTA is generally lacking in rodents, indirect projections through other structures may lead to activation of these neurons during BLA stimulation.
Release of dopamine in the NAc did not increase during BLA stimulation, although a delayed increase, starting after the cessation of stimulation, was observed. This latter increase is consistent with a delayed increase in accumbal dopamine reported after exposure to stress (Puglisi-Allegra et al., 1991
The lack of a stimulus-locked increase in dopamine in the NAc was reversed after local perfusion of the mGluR2/3 agonist LY354740 and the AMPA/kainate antagonist LY293558 into the PFC. Assuming that LY354740 presynaptically inhibits stimulated glutamate release, an assumption supported by data presented in Figure 3, this finding indicates that activation of glutamate release in the PFC inhibits dopamine release in the NAc during BLA stimulation. Blockade of AMPA receptors in the PFC, which reduces the postsynaptic effects of BLA-mediated glutamate activation, produced a similar response, providing additional support that an increase in glutamate neurotransmission in the PFC downregulates dopamine release in NAc during BLA activation.
Through what mechanism might amygdala activation differentially regulate dopamine release in the PFC and NAc? Dopamine neurons localized in the VTA appear to receive target-specific input from afferent regions (Carr and Sesack, 2000
In contrast to the present findings, the general notion has been that PFC exerts an excitatory control over dopamine release in the NAc. This mechanism has been supported by studies showing that electrical stimulation of PFC (Taber and Fibiger, 1995
A previous study using in vivo voltammetry in anesthetized animals reported that NAc dopamine release increases during BLA activation (Floresco et al., 1998
Conclusions
Cortical modulation of information transfer from amygdala to NAc is considered essential for translation of cognitive and emotive processes into appropriate motor responding. PFC control has been considered to be primarily, if not exclusively, at the postsynaptic level, i.e., by direct activation of NAc output neurons (Pennartz et al., 1994
FOOTNOTES Received Aug. 21, 2000; revised Oct. 10, 2000; accepted Oct. 25, 2000.
This research was supported by National Institutes of Health Grants T32NS07224 (M.E.J.), K02MH01616 (B.M.), MH48404 (B.M.), MH44866 (B.M.), and the U.S. Veterans Administration Centers for Schizophrenia and Post-Traumatic Stress Disorder. We thank Barbara Adams and Karyn Groth for technical assistance.
Correspondence should be addressed to Bita Moghaddam, Department of Psychiatry, Yale University School of Medicine, 950 Campbell Avenue, VAMC 116A/2, West Haven, CT 06516. E-mail: bita.moghaddam{at}yale.edu.
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