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The Journal of Neuroscience, February 1, 2002, 22(3):1126-1136
Dissociable Effects of Lidocaine Inactivation of the Rostral and Caudal Basolateral Amygdala on the Maintenance and Reinstatement of Cocaine-Seeking Behavior in Rats
Kathleen M. Kantak1, Yolanda Black1, Eric Valencia1, Kristen Green-Jordan1, and Howard B. Eichenbaum2 1 Laboratory of Behavioral Neuroscience and 2 Cognitive Neurobiology Laboratory, Department of Psychology, Boston University, Boston, Massachusetts 02215
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
Cocaine addiction is a chronically relapsing brain disease, but its neural basis is not yet well understood. Clinical reports underscore the possible importance of associative processes for regulating at least some aspects of cocaine addiction. The present study reports the effects of reversible lidocaine-induced inactivation of rostral basolateral amygdala (rBLA) and caudal basolateral amygdala (cBLA) regions on the maintenance and reinstatement of drug-seeking behavior in rats trained to self-administer 1 mg/kg cocaine under a second order schedule of drug delivery. Both regions of the basolateral amygdala were investigated because they have dissociable effects on cognitive task performance. Results demonstrated that after self-administration training and a period of extinction and abstinence, lidocaine inactivation of the rBLA and cBLA attenuated the reinstatement of drug-seeking behavior induced by cocaine-associated cues examined in conjunction with a single priming injection of cocaine. In contrast, lidocaine inactivation of only the rBLA blocked reinstatement of drug-seeking behavior induced by cocaine-associated cues examined alone. Additional differences were shown during cocaine maintenance testing where inactivation of only the cBLA attenuated drug-seeking behavior. Drug intake was not altered. Thus, the rBLA and cBLA appear to selectively and dissociably regulate drug-seeking behavior under conditions of cocaine abstinence (cue-induced reinstatement) and repeated cocaine use (maintenance), respectively. These findings suggest that the basolateral amygdala may be more functionally heterogeneous than commonly thought for regulating drug-seeking behavior. The basis for this dissociation might be related to neuroanatomical connections of the rBLA and cBLA with segregated, but parallel, corticostriatalpallidothalamic circuits.
Key words: caudal basolateral amygdala; cocaine; drug cues; drug prime; lidocaine; maintenance; reinstatement; rostral basolateral amygdala
INTRODUCTION
Cocaine addiction is a chronically relapsing brain disease. Clinical reports suggesting a link between limbic and cortical structures in mediating drug use and craving underscore the possible importance of associative processes for regulating some aspects of drug addiction. Imaging studies demonstrate that craving induced by cocaine-associated cues in abstinent addicts produces specific changes in patterns of activation in the amygdala, anterior cingulate, basal ganglia, dorsolateral prefrontal cortex, and cerebellum (Grant et al., 1996
; Maas et al., 1998
An associative conditioning process involving mechanisms within the basolateral amygdala is thought to underlie the salience of cues associated with cocaine self-administration, which induce drug-seeking behavior in laboratory animals (Whitelaw et al., 1996
We used a model of maintenance and reinstatement that relies on second-order scheduling of drug and conditioned stimulus cues for maintaining high rates of performance (Spealman et al., 1999
MATERIALS AND METHODS
Subjects
Male Crl(WI)BR rats (Wistar rats; Charles River Breeding Labs, Portage, MI) were housed in individual hanging plastic cages (24 × 22 × 20 cm) within a temperature- (21-23°C) and light-controlled (on at 8:00 A.M.; off at 8:00 P.M.) vivarium. Between experimental sessions, the rats had continuous access to water in their home cages. To maintain body weight at ~85% of adjusted ad libitum values throughout the duration of the study (from 338 ± 7 to 417 ± 7 gm), ~16 gm of food was provided each day. The policies and procedures set forth in the National Institutes of Health Guide for the Care and Use of Laboratory Animals were followed.Apparatus
Eight experimental chambers (model ENV-008CT; Med Associates, East Fairfield, VT) were each equipped with two response levers positioned 8 cm to the left and right of a center mounted food receptacle. Connected to the food receptacle was a pellet dispenser, which delivered 45 mg food pellets (Traditional Formula; Noyes, Lancaster, NH). A white stimulus light was mounted 7 cm above each lever. Each chamber was outfitted with a single channel fluid swivel and spring leash assembly that were connected to a counterbalanced arm assembly (Med Associates). A sound-attenuating cubicle (model ENV-018 M; Med Associates) equipped with an overhead light to provide general illumination, a fan to provide ventilation, and an 8speaker to provide sound stimuli enclosed each chamber. Motor-driven syringe pumps (model PHM-100; Med Associates) were used for drug delivery and were located outside the sound-attenuating cubicle. A 486 AT-compatible computer programmed in Medstate Notation and connected to an interface (Med Associates) controlled experimental events.
Drugs
The drugs used were cocaine hydrochloride (gift from the National Institute on Drug Abuse, Bethesda, MD) and lidocaine hydrochloride (Sigma, St. Louis, MO). Cocaine was dissolved in a sterile 0.9% saline solution containing 3 IU of heparin/ml. Intravenous delivery of the 1.0 mg/kg cocaine training dose was accomplished by infusing a 2.67 mg/ml solution though a 20 cc filtered plastic syringe at a rate of 1.8 ml/min. To attain a dose of 1.0 mg/kg, infusion volume was adjusted for body weight, resulting in drug delivery times of ~4-5 sec in individual rats. The heparinized saline solution was used during saline substitution aspects of the study. Lidocaine, which was infused intracerebroventricularly, was dissolved in sterile 0.9% saline to make 2% (20 mg/ml), 6% (60 mg/ml), 11% (112 mg/ml), or 20% (200 mg/ml) solutions. The pH of all solutions, including saline, was 5.0. A total volume of 0.5 µl, resulting in lidocaine doses of 10, 30, 56, and 100 µg, respectively, was infused bilaterally into the rBLA or cBLA at a rate of 0.5 µl/1.2 min. A piece of PE-20 tubing was used to connect a 5 µl Hamilton syringe mounted on the syringe pump to a 28 gauge stainless steel infusion cannula that extended 1 mm beyond the tip of the guide cannula. The infusion cannula was left in place for 1 min after the infusion. Sterile 0.9% saline was used as the control vehicle for lidocaine infusions.Surgery and histology
Rats were anesthetized with intraperitoneal injections of 90 mg/kg ketamine plus 10 mg/kg xylazine. A catheter made from silicon tubing (inner diameter, 0.020 inches; outer diameter, 0.037 inches) was implanted into the right jugular vein as previously described (Kantak et al., 20002.0 mm, lateral (L) ±4.5 mm, dorsoventral (DV)
Self-administration training
Training baseline. Before surgery, rats were trained to press a lever under a fixed-ratio 1 (FR1) schedule of food pellet delivery. After food training was complete (rats rapidly pressed the lever for 50 pellets), right jugular vein catheters and guide cannulas were implanted. One week later, 2 hr cocaine self-administration sessions began. Rats were trained to self-administer 1.0 mg/kg cocaine under a FI 5 min (FR5:S) second-order schedule of drug delivery, as previously described (Kantak et al., 2000) sound and light cues. This aspect of training was included because it engenders reliable reinstatement of cue-induced drug-seeking behavior over repeated test sessions without any additional access to cocaine (Weiss et al., 2000
Cue-induced reinstatement of drug-seeking behavior
Using the training procedures described above, pilot work demonstrated that cocaine-associated cues alone were capable of reliably reinstating drug-seeking behavior for up to six test sessions spaced 3 d apart (unpublished findings). Therefore, cue-induced reinstatement test sessions were conducted every third day. Rats remained in their home cages on intervening days. To test for the discriminative control over second-order responding by the stimulus cues, the SCocaine prime plus cue-induced reinstatement of drug-seeking behavior
After completion of the cue-induced reinstatement procedure, test sessions were conducted in the same rats to examine cocaine prime plus cue-induced reinstatement of drug-seeking behavior. For this test, an intraperitoneal priming injection of 20 mg/kg cocaine, which produces maximal reinstatement of drug-seeking behavior in Wistar strain rats (Mantsch and Goeders, 1999Drug-seeking and drug-taking behavior under cocaine maintenance conditions
To directly examine the effects of lidocaine inactivation of the rBLA and cBLA on drug-taking behavior during repeated cocaine availability, three rats (n = 2 rBLA and n = 1 cBLA) used in the above reinstatement experiments and five experimentally naive rats (n = 2 rBLA and n = 3 cBLA) were examined under cocaine maintenance conditions. After establishing or reestablishing stable cocaine baselines and discrimination sessions were underway, rats from each group (n = 4) were bilaterally infused with saline, 10, 30, 56, or 100 µg lidocaine in a counterbalanced order 5 min before a cocaine self-administration test session. Each 1 hr test session was conducted 3 d apart, with discrimination sessions on intervening days. The S+ sound cue was presented throughout each test session, and the S+ light cue was presented during the brief stimulus, drug delivery, and 20 sec TO periods.Specificity of the behavioral effects of lidocaine
To determine if the reductions in drug-seeking behavior after lidocaine treatment were attributable to a nonspecific disruption in lever responding, a small group (n = 3) of the same rats as used in the reinstatement experiments (two from the cBLA group; one from the rBLA group) were examined for the effects of lidocaine on responding maintained by a FR5 schedule of food pellet delivery. No sound or light stimuli were used. After baseline responding was stable, rats were infused with 100 µg of lidocaine 5 min before a single 1 hr test session.Data analysis
For the self-administration studies, three dependent measures were calculated: (1) the total number of active lever responses emitted during the session (drug-seeking behavior), (2) the total number of inactive lever responses emitted during the session (non-specific responding), and (3) the total number of infusions earned during maintenance tests (drug-taking behavior) or the total number of infusion-paired light deliveries earned during reinstatement tests. Data from individual animals were averaged over the last three cocaine, saline, and extinction sessions and used to portray baseline performance. A series of single-factor (condition or dose) ANOVAs with repeated measures was performed for each brain site, and the Dunnett's t test was used for all post hoc comparisons. Paired t tests for dependent samples were used to compare the number of infusions earned during baseline sessions. For the food study, the number of active and inactive lever responses as well as pellets earned during baseline (averaged over the last three sessions) and after bilateral infusions of 100 µg lidocaine were calculated. The two conditions were compared by paired t tests for dependent samples.
RESULTS
Functional spread of lidocaine and histology
The volume of lidocaine required to inactivate >90% of neurons within a particular radius from the infusion site is governed by the spherical volume equation, V = 4/3
r3 (Tehovnik and Sommer, 1997
Based on the spherical volume equation, the functional spread of 0.5 µl lidocaine at each concentration is estimated to have been 0.49 mm from the infusion site in the present study. Consistent with this calculation, conduction analyses in the medulla or spinal cord show that 0.5 µl of lidocaine infused at fourfold different concentrations block an area with a radius of 0.45-0.50 mm from the infusion site (Sandkühler and Gebhart, 1984
Histological verification of bilateral placements was confirmed for 8 of 10 rats with cannulas aimed at the rBLA (Fig. 1, left). For every animal, cannulas were within 0.5 mm of the intended placement in the anterior-posterior position and within the rBLA anatomical range (Swanson, 1992
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Figure 1. Schematic representing coronal sections of the rat brain and cannula placements within the rostral (left) and caudal (right) regions of the basolateral amygdala. Circles indicate the location and diffusion of lidocaine and are drawn to scale. All drawings are based on the atlas of Swanson (1992)
Histological verification of bilateral placements was confirmed for 8 of 10 rats with cannulas aimed at the cBLA (Fig. 1, right). All cannulas were within 1.3 mm of the intended placement in the anterior-posterior position and within the cBLA anatomical range (Swanson, 1992
The above analyses indicate that there was a sufficient separation of placements from the rostral versus caudal BLA to delineate the two discrete regions of interest. Animals with cannulas that were not bilaterally positioned in the intended site were omitted from further analyses. Furthermore, for all rats included in the analyses, cannulas placements verify that lidocaine inactivation predominantly encompassed the region of interest. A representative photomicrograph of the extent of damage made by 22 gauge guide cannulas and a tract made by a 28 gauge infusion cannula is shown in Figure 2 for an rBLA-implanted rat.
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Figure 2. Representative photomicrograph of the extent of damage made by 22 gauge guide cannulas. In this example, the tips of the guide cannulas were bilaterally positioned 1 mm above the rostral basolateral amygdala at a level 2.0 mm posterior to bregma. A tract made by a 28 gauge infusion cannula is visible in the left hemisphere.
Cue-induced reinstatement of drug-seeking behavior
Rostral BLA
As shown in Figure 3 (top), cocaine maintained high rates of active lever responding that were clearly distinguished from saline performance during baseline discrimination sessions and from extinction performance during extinction sessions (F(2,10) = 42; p0.001). Responses on the inactive lever (Fig. 3, bottom) averaged
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Figure 3. Drug-seeking behavior after lidocaine inactivation of the rostral basolateral amygdala (n = 6). Responses on the active lever are shown on the top, and responses on the inactive lever are shown on the bottom for each phase of the experiment: discrimination baseline, extinction, drug cue-induced reinstatement, and drug prime plus drug cue-induced reinstatement conditions. Values are the mean ± SEM. S+ refers to the drug-associated cues, and S
After extinction training, S+ cues associated with cocaine availability reinstated drug-seeking behavior on the active lever to 68% of the cocaine baseline, whereas S
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Figure 4. Number of infusions earned or number of infusion-paired light deliveries earned after lidocaine inactivation of the rostral basolateral amygdala for each phase of the experiment: discrimination baseline, extinction, cue-induced reinstatement, and prime plus cue-induced reinstatement conditions (n = 6). Values are the mean ± SEM. S+ refers to the drug-associated cues, and S
Caudal BLA
The baseline performance profile in rats with cannulas aimed at the cBLA was similar to the profile observed in rats with cannulas aimed at the rBLA. Drug-seeking behavior on the active lever (Fig. 5, top) (F(2,8) = 14; p
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Figure 5. Drug-seeking behavior after lidocaine inactivation of the caudal basolateral amygdala (n = 5). Responses on the active lever are shown on the top, and responses on the inactive lever are shown on the bottom for each phase of the experiment: discrimination baseline, extinction, drug cue-induced reinstatement, and drug prime plus drug cue-induced reinstatement conditions. Values are the mean ± SEM. S+ refers to the drug-associated cues, and S
After extinction training, S+ cues associated with cocaine availability reinstated drug-seeking behavior on the active lever to 20% of the cocaine baseline in this group of rats, whereas S
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Figure 6. Number of infusions earned or number of infusion-paired light deliveries earned after lidocaine inactivation of the caudal basolateral amygdala for each phase of the experiment: discrimination baseline, extinction, drug cue-induced reinstatement, and drug prime + drug cue-induced reinstatement conditions (n = 5). Values are the mean ± SEM. S+ refers to the drug-associated cues, and S
Cocaine prime plus cue-induced reinstatement of drug-seeking behavior
Rostral BLA
After an intraperitoneal priming injection of 20 mg/kg cocaine, the conditioned S+ cocaine cues reinstated drug-seeking behavior on the active lever to 145% of the cocaine baseline (Fig. 3, top). Bilateral lidocaine infusions into the rBLA dose-dependently attenuated the reinstatement of drug-seeking behavior, with a significant reduction after 100 µg (F(4,16) = 3.3; pCaudal BLA
A cocaine priming injection in combination with the conditioned S+ cocaine cues reinstated drug-seeking behavior on the active lever to 35% of the cocaine baseline in this group of rats (Fig. 5, top). Bilateral lidocaine infusions into the cBLA dose-dependently attenuated the reinstatement of drug-seeking behavior, with significant reductions after 56 and 100 µg (F(4,12) = 3.3; p
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Table 1. Drug-seeking behavior during reinstatement tests and after various doses of lidocaine Drug-seeking and drug-taking behavior under cocaine maintenance conditions
Rostral BLA
During cocaine maintenance test sessions, bilateral lidocaine inactivation of the rBLA with doses up to 100 µg did not modify drug-seeking (p
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Figure 7. Drug-seeking (top) and drug-taking (bottom) behavior after lidocaine inactivation of the rostral basolateral amygdala (left) and caudal basolateral amygdala (right) during maintenance testing (n = 4 for each site). Values are the mean ± SEM.
Caudal BLA
In contrast to the rBLA, bilateral lidocaine inactivation of the cBLA during cocaine maintenance test sessions resulted in reductions in drug-seeking behavior (Fig. 7, top right). Significant reductions were observed after 56 and 100 µg (F(3,9) = 6.57; pSpecificity of the behavioral effects of lidocaine
To determine if the reductions in responding after infusion with 100 µg lidocaine were attributable to nonspecific disruption of responding in general, rats were trained on a FR5 schedule of food pellet delivery for 3 weeks and then bilaterally infused with 100 µg of lidocaine in a single test session (Fig. 8). There were no significant differences between baseline performance and performance after 100 µg of lidocaine in active lever responses (p
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Figure 8. Food-maintained responding after lidocaine inactivation of the basolateral amygdala (n = 3). Active lever responses are shown on the left, inactive lever responses in the middle, and number of pellets earned on the right. Values are the mean ± SEM.
DISCUSSION
The present study outlines a procedure in rats whereby a high degree of drug-seeking behavior was induced during maintenance testing and reinstated by drug-associated sound and light cues after a period of extinction and abstinence from cocaine self-administration. Factors contributing to robust levels of response reinstatement are use of multiple stimulus cues (See et al., 1999
Dissociable effects of lidocaine inactivation of the rBLA and cBLA
In the rBLA, a dose of lidocaine (10 µg) that fully blocked the expression of conditioned stimulus-reward learning in a conditioned cue preference cognitive task (Kantak et al., 2001
Although the cBLA is also involved in regulating conditioned stimulus-reward learning (Kantak et al., 2001
Although lidocaine infusions into the rBLA and cBLA effectively attenuated the reinstatement of drug-seeking behavior after a cocaine priming injection, a 5- to 10-fold higher concentration of lidocaine was required than the concentration needed to block the effects of cues presented alone. The reasons why a 10 µg lidocaine dose was ineffective in the cocaine priming tests are not entirely clear. The data in Table 1 suggest that differences in the time course of inactivation for 10, 56, and 100 µg doses cannot explain the ineffectiveness of 10 µg during cocaine priming tests because the time course for each dose was similar. The only difference between the two types of reinstatement tests was the injection of 20 mg/kg cocaine 25 min before lidocaine infusion during the priming tests. Although cocaine has an approximately fivefold greater affinity for the sodium channel than lidocaine in rat brain (Wilcox et al., 2001
Basis of dissociable effects
One explanation for the functional heterogeneity between the rBLA and cBLA in regulating drug-seeking behavior under maintenance and reinstatement conditions may be related to their connections with segregated, but parallel, corticostriatalpallidothalamic circuits (Gröenewegen et al., 1991
Drug-seeking versus drug-taking behavior
Although it is clear that the rBLA and cBLA may dissociably regulate drug-seeking behavior during maintenance and reinstatement, sites outside the basolateral amygdala must regulate drug-taking behavior. This conclusion is derived from the fact that this aspect of behavior was not altered by lidocaine inactivation of either the rBLA or cBLA. Whether drug-taking behavior involves regulation by other memory systems is not entirely clear at this time. However, given rats maintained enough responses after lidocaine infusions to keep drug-taking behavior constant as drug-seeking behavior decreased suggests that a conditioning process may be involved. One possibility is that contextual cues in the self-administration environment served to maintain drug-taking behavior, suggesting possible regulation of drug-taking behavior by a hippocampal-dependent memory system that, among other things, mediates associations between stimuli (Eichenbaum, 1997
Conclusions
Using a second-order schedule of cocaine delivery, dissociable control over drug-seeking behavior by the rBLA and cBLA was demonstrated. These findings extend previous investigations of the basolateral amygdala (Whitelaw et al., 1996
FOOTNOTES Received July 13, 2001; revised Nov. 9, 2001; accepted Nov. 14, 2001.
This research was supported by National Institute on Drug Abuse Grant DA11716 (K.M.K.) and National Institute on Mental Health Senior Scientist Award MH01475 (H.B.E.). We thank Katrina Gibson and Francisco Ugalde for technical assistance.
Correspondence should be addressed to Kathleen M. Kantak, Department of Psychology, Boston University, 64 Cummington Street, Boston, MA 02215. E-mail: kkantak{at}bu.edu.
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