Acute and Chronic Dopamine Dynamics in a Nonhuman Primate Model of Recreational Cocaine Use

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The Journal of Neuroscience, September 15, 2000, 20(18):7109-7115

Acute and Chronic Dopamine Dynamics in a Nonhuman Primate Model of Recreational Cocaine Use
Charles W. Bradberry
Departments of Psychiatry and Laboratory Medicine, West Haven Veterans Administration Hospital and Yale University School of Medicine, West Haven, Connecticut 06516

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Using a model of recreational cocaine consumption, we have determined in four rhesus monkeys the impact of self-administeredcocaine on mesolimbic and sensorimotor striatal dopaminergic neurotransmission.The effects of cocaine repeated within a self-administration sessionand across multiple sessions over a 6 month period were determinedby the use of fixed-ratio self-administration and microdialysisprocedures. The exposure to cocaine was modest, with at most two0.5 mg/kg infusions permitted in each weekly session. Within acocaine self-administration session, acute tolerance to the abilityof cocaine to elevate extracellular striatal dopamine was observed.Over a period of 6 months of repeated self-administration, therewas a significant increase in the impact of a fixed dose on extracellulardopamine, indicating that neurochemical sensitization to the effectsof self-administered cocaine occurs in primates. A pronounceddopaminergic response to noncontingent cocaine was also observed,with no increases in extracellular dopamine in response to anunexpected saline substitution, indicating that the neurochemicalresponse to self-administered cocaine is primarily caused by directpharmacological effects of the drug rather than by conditioningto external environmental cues. These results highlight the contrastin time-dependent changes in neurochemical responsiveness to cocaine,depending on whether within-session or between-session comparisonsare made. They also demonstrate that recreational levels of cocaineconsumption can result in neurochemical sensitization, an enduringchange in brain function that may contribute toaddiction.

Key words: dependence; striatum; reward; relapse; psychostimulant; accumbens

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Dopamine (DA) neurotransmission is believed to play an essential role in cocaine reward (Roberts et al., 1977; Ritz et al.,1987; Wise and Bozarth, 1987; Volkow et al., 1997). The neuroadaptiveprocess in which the dopaminergic response to cocaine sensitizesafter chronic exposure has been proposed to cause excessive incentivesalience to be attributed to the act of drug taking and to stimuliassociated with drug taking, thereby contributing to addiction(Robinson and Berridge, 1993). Although animal models of druguse investigating the impact of cocaine exposure on dopaminergicfunction generally involve high-dose, frequent (e.g., daily) exposure,human patterns of cocaine consumption do not generally begin ascompulsive, high-dose bingeing. Rather, what begins as recreationaluse (e.g., on weekends) gradually progresses over time to becomethe focus of a user's energy andattention.

The goal of the present study was to develop and exploit a nonhuman primate self-administration model permitting in vivo measurementsof extracellular dopamine over a 6 month course of "moderate"chronic cocaine exposure mimicking human recreational consumption.Because there are considerable inherent differences between rodentand primate dopaminergic systems (Berger et al., 1991) and a greatersimilarity in brain metabolic responses to cocaine between humanand nonhuman primates (London et al., 1990; Pearlson et al., 1993),it is important that studies be done in primates to verify phenomena,such as sensitization, that have far-reaching implications forthe etiology of drugaddiction.

The questions about the effects of cocaine on extracellular mesolimbic DA addressed in the present study were as follows:(1) How do they change after repeated self-administration withina session? (2) How do they change with repeated exposure acrossa number of sessions? The first question addresses a potentialmechanism underlying subjective reports of tolerance after repeatedadministration in humans, a phenomenon that may contribute torepeated self-dosing of increasing amounts in an attempt to maintainthe desired effect (Jaffe, 1990). The second question relatesto whether a neurochemical sensitization develops in primates,evidence of which islacking.

The present drug administration paradigm was designed to model recreational weekend consumption in humans. This entailed aself-administration model of exposure, considered to be more naturalisticthan investigator-administered models of chronic exposure, witha one session per week frequency and a low amount (0.5 or 1.0mg/kg) of cocaine consumed. Extracellular DA from the mesolimbicand sensorimotor striatum was measured during the self-administrationsessions by the use of magnetic resonance-directed microdialysismethods.

  MATERIALS AND METHODS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Overview of experimental design. Acute within-session tolerance of the dopaminergic response to cocaine was examined by comparingthe first and second response to self-administered cocaine at0.5 mg/kg, with a 100 min time-out between infusions. DA levelsreturned to baseline between infusions, and the time into thesession was controlled for by conducting some studies in whichthe initial infusion of cocaine was withheld until the time inthe session when the second infusion would otherwise be occurring.Across-session sensitization was examined by regression of theaverage percent increase in DA over 10 min (after self-administrationof the initial cocaine infusion) versus the week into the study.To assess in a general sense the relative contribution of conditionedresponses in DA versus pharmacological effects of cocaine, DAlevels after saline substitution and noncontingent cocaine werecompared with those after self-administration ofcocaine.

Details of behavioral procedures. Microdialysis studies were conducted in rhesus monkeys restrained in a chair and trainedto self-administer cocaine intravenously. Four male animals wereused. They were restrained in a chair (Primate Products, RedwoodCity, CA) by a collar and placed in a behavioral chamber fittedwith an operant panel constructed from 1/4 inch aluminum to whichthe chair was attached. Med-Associates (East Fairfield, VT) softwareand hardware were used for all inputs and outputs and data collection.Animals were initially trained to lever press for food pelletsunder fixed ratio (FR) 10 (animals M103 and M32) or FR30 (animalsM47 and M49) lever response schedule of reinforcement for a minimumof 1 month, with animals exhibiting stimulus control as indicatedwith responding in the presence of a cue and little respondingin its absence. Subsequent to food training (with no strict criteria),a catheter was placed in the internal jugular that led to a vascularaccess port (Access Technologies, Skokie, IL) placed midscapula(Wojnicki et al., 1994), and animals were shifted to cocaine (i.e.,cocaine was now the reinforcer), with cocaine being signaled byan additional light of a different color on the operant panel.After switching to cocaine, food pellets or their cue were nolonger made available. The vascular access port allows percutaneousnonstressful access to the vasculature without the need for aprotective jacket and with reduced risk of infection because nothingis external to the skin. The device can be used daily for periodsof time well over a year (Wojnicki et al., 1994; Glowa et al.,1995). In our laboratory, with less frequent (biweekly) use, portshave been usable for up to 2 years. Maintenance of the ports consistsof a twice-weekly flushing with saline, locking with a solutionthat has a final concentration of 25% dextrose and 500 U/ml heparin.Animals quickly learned to lever press for cocaine under the sameFR contingency used for obtaining foodpellets.

Studies began at 10:00 A.M., although there was some variability (<30 min) between when an animal was first placed in a chair(immediately outside the home cage) and when the behavioral chamber(in a separate room) was closed, depending on how much difficultywas associated with attaching lines, etc. Animals were restrainedin a chair in the behavioral chamber with a house light on fora 60-90 min baseline period before presentation of the visualcue, during which microdialysis samples were collected. Duringthat time, no cue was presented, and lever pressing was recordedbut had no consequence. The visual cue indicating cocaine availabilitywas presented at the same time of day to each animal (11:30 A.M.for animals M103 and M32; 11:00 A.M. for animals M49 and M47).The visual cue was a horizontally placed pair of red and greenlights and indicated that the FR response would result in an infusionof a bolus of 0.5 mg/kg cocaine-HCl in 0.5 ml. The visual cuewas turned off as the infusion began at a flow rate of 16.3 ml/minover an 18 sec period. The 0.5 ml cocaine solution was loadedinto the line between the syringe and the vascular access port,and an excess volume (5 ml) was used to flush the cocaine dosecompletely into the animal, preventing the need to try and filljust the volume between the port and the catheter tip. This avoidedany "priming" that would result from slightly overfilling thatvolume. Visual inspection of a dye solution in a mock setup indicatedthat the loaded solution was infused into the animal beginning5 sec into the infusion and was essentially completely infusedby 10 sec into the infusion. After the infusion, a 100 min time-outbegan, during which no cues were presented and lever pressingwas recorded but had no consequences. After the time-out, thecue was presented again, with the second cue presentation andinfusion the same as thefirst.

After microdialysis studies began, each animal was permitted at most one session per week during which two infusions wouldbe available, separated by the 100 min time-out interval. In general,animals had a microdialysis session in which they received cocaineor had a "maintenance" cocaine self-administration session (witha single 0.5 mg/kg infusion) each week. Animals underwent studiesfor at least 3 months during which both infusions were 0.5 mg/kgcocaine, after which occasional saline substitutions or sessionswith no cue (or cocaine) presentation were conducted. This wasthe extent of cocaine exposure in each animal outside of the initialtraining with more traditional self-administration parameters(lower unit doses and more frequent infusions permitted). Thosesessions were 30 min in length, with one or two (consecutive)sessions in a given day. The amount of initial training each animalreceived was as follows: animal M103, 3 months of training withunit doses from 0.01 to 0.3 mg/kg and a total cumulative exposureover the training period of 80 mg/kg; animal M32, 1 month of trainingwith unit doses of 0.1-0.5 mg/kg and a total cumulative exposureof 6 mg/kg; and animals M49 and M47, 1 week of training each witha unit dose of 0.1 mg/kg and a total cumulative exposure of <3mg/kg. Animals were under stimulus control as indicated by responserates that increased by one to two orders of magnitude duringthe time of cue presentation (Bradberry et al., 2000).

When cocaine was administered noncontingently, it was infused at the usual times into the session but without any predictivevisual cues or the auditory cue of the infusion pump. Studiesin which saline was substituted for cocaine were conducted inexactly the same manner as those in which cocaine was administered,with the same visual cue presentation and FR response triggeringthe infusion pump with its associatedsound.

Microdialysis guide cannulae and probes. Details of the microdialysis procedures have been published (Bradberry et al., 2000).Probes were put in place the day before the experiment eitherunder light ketamine anesthesia (15 mg/kg) for animals M103 andM32 or without any ketamine by the use of a head-bolting procedurefor animals M47 and M49. After the probe is slowly lowered, aprotective molded plastic cap was put in place. On the study day,animals were restrained in the chair, the cap was removed, andinlet and outlet lines were attached to the probe. Probe placementswere in sites in which a probe had not been placed previously.There was usually just one probe in place, although occasionallytwo were placed. No apparent difference was ever noted betweenstudies in which two probes were in place as opposed to one. Placementorder varied between medial and lateral positions as well as betweendorsal and ventralplacements.

For the results from monkey M103 shown in Figure 1, the initial infusion of cocaine was given when samples were being collectedat 10 min intervals, with a perfusion rate set at 2 µl/min. Thesecond infusion was given after the perfusion rate was increasedto 5 µl/min, with samples collected at 2 min intervals. Thus,for this one animal, the second infusion was given with the microdialysisperfusion at a higher rate that was necessary for the rapid sampling.To permit a comparison, results from the second injection wereaveraged into 10 min bins. After changing the perfusion rate,there is no change in the actual mass of DA collected per unittime, making the comparison between the first and second injectionsfor this animal valid despite the different flow rates. Additionalstudies (see Fig. 2) in animal M103 in which both cocaine infusionswere done while the probe was being perfused at 5 µl/min showresults equivalent to those presented in Figure 1.

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Figure 1. Within-session tolerance of the extracellular DA response to self-administered cocaine in four different rhesus monkeys (M103, M32, M49, and M47), with responses collapsed across all striatal subdivisions. Initial studies were done in animal M103 with 10 min collection times, after which, for greater temporal detail, a 2 min sampling procedure was used. For animals M49 and M47, a time offset to compensate for dead volume in the outflow lines was incorporated; thus, the temporal pattern of the dopaminergic response for them is the most accurate. Cocaine was self-administered at t = 0. The second self-administration occurred 100 min after the first in the same session. Solid circles represent the first injection; open circles represent the second injection. The number of trials is as follows: M103, n = 4; M32, n = 5; M49, n = 14; M47, n = 9.

Data analysis. For the acute tolerance studies, data up to 20 min after cocaine were analyzed by two-way repeated measuresANOVA of extracellular levels expressed as a percent of a precuebaseline, defined as the mean of the three points preceding thecue (Robertson et al., 1991; Klitenick et al., 1992), with theorder of administration as a between-groups factor. For the chronicsensitization studies, Pearson's correlation was used to determinewhether the DA response showed progressive changes over time.Simple regression was run on the mean percent increase over 10min in response to the initial administration of cocaine in asession versus the week into the study. Each probe insertion wastreated as an individual statistical event, as individual neuronalrecordings are treated in electrophysiological studies (Schultzet al., 1993). Within each animal, responses were collapsed acrossall striatal regions. For evaluation of striatal regional differences,responses were collapsed across allanimals.

  RESULTS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Acute tolerance

In an examination of acute tolerance to repeated self-administration of cocaine, two 0.5 mg/kg infusions of cocaine-HCl weremade available within a session. A 100 min time-out separatedthe two infusions. Mean response rates after each cue presentationwere very consistent as indicated in Table 1, with the FR contingencyquickly reached. Figure 1 demonstrates the increase in extracellularDA (relative to the baseline preceding each injection) after thetwo injections within a session in four different animals. Table2 lists basal DA values for each group in Figure 1. For eachanimal (except M103 in which the first drug administration wasat a different microdialysis perfusion rate, see Materials andMethods), basal levels at the time of the first and second druginfusion did not differ significantly (p > 0.05) by paired t testcomparison. There is a significant reduction in the magnitudeof the response to the second dose in three out of the four animalsby two-way repeated measures ANOVA with injection order as a between-groupsfactor. Because a gradual sensitization of the dopaminergic responseto cocaine was seen between sessions (see below), only pairedinjections (i.e., both infusions occurred in the same session)were used for the analysis so that the amount of chronic cocaineexposure was always balanced for the first and second infusions.Figure 2 shows additional studies done at a later time on animalM103 in which both infusions were done with the same microdialysisperfusion rate, with results equivalent to those shown in Figure1. Additional studies to control for time into the session arediscussed below (Fig. 3).


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Table 1. Rates of response from the time of cue presentation to the time that contingency was reached for the self-administration of cocaine in studies presented in Figure 1


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Table 2. Basal values of DA in microdialysates

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Figure 2. Within-session tolerance in animal M103 determined with the same microdialysis perfusion rate (5 µl/min) throughout, indicating the validity of the results for this animal in Figure 1. (Fig. 1, top left, shows data from studies with different flow rates for the first and second infusions.) Solid circles represent the first injection; open circles represent the second injection (n = 4 trials). Basal DA levels were as follows: first infusion, 1.42 ± 0.53 fmol/µl; second infusion, 1.78 ± 0.60 fmol/µl; t₍₆₎ = $-$ 0.45, NS.

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Figure 3. Self-administration of an initial infusion of cocaine late in the session (at the time the second infusion would normally occur) does not result in a diminished response, indicating that the reduced response to the second infusion shown in Figures 1 and 2 is not an artifact of the time into the session. Solid circles represent an early first infusion; open circles represent a late first infusion. The number of trials is as follows: M103, n = 4 early infusions and 6 late infusions; M32, n = 6 early infusions and 5 late infusions; M49, n = 14 early infusions and 11 late infusions; M47, n = 10 early infusions and 11 late infusions.

Comparisons between ventromedial, central, and dorsolateral striatal regions (collapsed across all animals) in the presentstudy indicated acute tolerance in the central and ventromedialsubdivisions of the mesolimbic striatum but not in the dorsolateral(sensorimotor) striatum (Fig. 4).

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Figure 4. Subdivision of the striatum indicated no regional differences in the magnitude of tolerance seen between the first and second infusions of cocaine when responses were collapsed across animals. The number of trials is indicated on each panel.

Studies to control for the time into the session

Studies were done in each animal in which a cocaine infusion was not made available until late in the session, at the timethe second infusion would normally have occurred. For each animal,the response to an initial infusion of cocaine given late in thesession was not less than the response to an initial infusiongiven early in the session, indicating that the reduced responseto a second cocaine infusion relative to the first was not anartifact of the time into the session (Fig. 3). As can be seen,there is actually a trend in all animals (reaching significancein two) for the response to a first cocaine infusion administeredlate to be larger than the response to a first cocaine infusiongiven early; however, these sessions were done in the latter monthsof the studies, and the greater response is presumably a resultof a between-session sensitization of the dopaminergic responseto cocaine and demonstrates why only sessions with paired infusionsare presented in Figures 1 and 2.

Chronic sensitization

To determine whether there were any progressive changes in the effects of cocaine over 6 months of repeated microdialysisstudies, a regression analysis of the mean percent increase (over10 min) in extracellular DA after self-administration of 0.5 mg/kgcocaine versus the week into the study was performed. Figure 5shows the pooled data for all four animals (top left), as wellas panels in which the dopaminergic response in each region isanalyzed separately for changes over time. The pooled responsescollapsed across all regions show a significant increase overtime in the dopaminergic response to cocaine. In analyzing regionsseparately, it is seen that in both mesolimbic subdivisions, aprogressive increase in the ability of cocaine to elevate extracellularcocaine over time occurs. However, in the dorsolateral sensorimotorsubdivision, sensitization was not seen.

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Figure 5. Progressive change in the cocaine-induced increase in extracellular DA over an extended time. Points represent the average increase relative to baseline during the 10 min after self-administration of an initial infusion of cocaine. Top left, Results collapsed across all animals and regions. Top right, bottom, Responses over time split by the subregion of the striatum. The two mesolimbic regions showed a significant increase in DA response over time, whereas the sensorimotor (dorsolateral) striatum did not.

In an examination of any individual differences between the animals, each animal was analyzed separately as shown in Figure6. As can be seen, in three out of the four animals, there wasa significant (p < 0.05) correlation between these two variables.Whether the lack of sensitization in the one animal is reflectiveof inherent variability in the neurochemical measurements or actualdifferences between individuals is difficult to specify with certaintybecause of the sample size.

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Figure 6. Changes in response to cocaine over time, determined in individual animals. Three (M103, M32, and M47) of the four animals showed a significant elevation in the effect of cocaine over time.

Regression of basal DA versus time indicated no progressive changes. Regression of basal DA versus the percent 10 min increaseshowed a significant negative correlation (R² = 0.14; p < 0.05; n = 36), suggesting that basal DA was to someextent predictive of the magnitude of the response to cocaine.However, this is more likely an artifact of the lower basal DAlevels in the ventromedial striatum that is also the most responsivestriatal subdivision (Bradberry et al., 2000). If each regionis examined separately, there was no trend toward a correlationof basal DA versus the percent 10 minincrease.

Chronic changes in behavior

The mean response rate for lever pressing (measured from the time of cue presentation to the time that contingency was reached)did not correlate with the time into the study for monkey M103(R² = 0.27, NS) or monkey M32 (R² < 0.01, NS) but did for both animals M47 (R² = 0.477; p < 0.05) and M49 (R² = 0.498; p < 0.05).

Dopaminergic impact of noncontingent cocaine and saline substitution

To determine whether the dopaminergic impact observed in response to self-administered cocaine is actually a conditioned responseassociated with training, we administered noncontingent cocaineat the usual time within a session as the self-administered cocaine.Figure 7 demonstrates that there was a pronounced dopaminergicimpact of noncontingent cocaine in each animal. Saline substitutiondata from Bradberry et al. (2000) are also presented in this figure,indicating no response to saline substitution (by one-way repeatedmeasures ANOVA) with all external cues normally associated withcocaine present (i.e., the visual cue offset and the auditorycue of the infusion pump).

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Figure 7. Dopaminergic response to noncontingent cocaine or surprise saline substitution. sal, Saline substitution; non-cont1, first noncontingent infusion; non-cont2, second noncontingent infusion. n = 2-4 trials per animal for noncontingent cocaine and 4-6 trials per animal for saline substitution.

  DISCUSSION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

These results demonstrate that in a primate model of recreational cocaine use, both acute tolerance to and chronic sensitizationof the impact of cocaine on extracellular striatal DA occur. Thephenomena of tolerance and sensitization have been implicatedin various aspects of psychostimulant dependency and relapse (Jaffe,1990; Robinson and Berridge, 1993; Schenk and Partridge, 1997;De Vries et al., 1998).

Acute tolerance

Tolerance to the subjective effects of repeated cocaine has consistently been seen in human laboratory studies by Fischmanand colleagues (Javaid et al., 1978; Foltin and Fischman, 1991,1992; Ward et al., 1997) and others (Ambre et al., 1988; Kumoret al., 1989). This phenomenon may contribute to binge patternsof consumption (Jaffe, 1990) because a user consumes progressivelylarger amounts to recapture the initial high obtained with thefirst dose. The present results suggest that tolerance to thesubjective effects of repeated cocaine could be caused by a reduceddopaminergic response to repeated cocaine. This presupposes thatincreased extracellular DA is a primary mediator of psychostimulant-inducedeuphoria. However, it has been noted that there is evidence conflictingwith this idea (Rothman and Glowa, 1995; Brauer et al., 1997;Berridge and Robinson, 1998). Although the present results areconsistent with a dopaminergic mediation of cocaine reward, itis correlative supportonly.

There are clear functional subdivisions of the striatum based on anatomical connectivity (Yeterian and Van Hoesen, 1978; Russchenet al., 1985; Selemon and Goldman-Rakic, 1985; Lynd-Balta andHaber, 1994; Haber and McFarland, 1999). There is also enhancedresponsivity of the mesolimbic striatum to cocaine as indicatedby metabolic studies (Lyons et al., 1996) and to noncocaine rewardsas indicated in electrophysiological studies (Apicella et al.,1991). We have made comparisons previously between striatal areassubdivided into sensorimotor function (dorsolateral striatum)and mesolimbic function [ventromedial striatum, receiving orbitalprefrontal projections; central striatum, receiving dorsolateralprefrontal projections (Haber and McFarland, 1999)]. Those studiesdemonstrated enhanced responsiveness to cocaine in the ventromedialstriatum (Bradberry et al., 2000). Comparisons between striatalregions indicated acute tolerance in the central and ventromedialsubdivisions of the mesolimbic striatum but not in the dorsolateralsensorimotor striatum (Fig. 4). However, the lack of effect inthe dorsolateral region could be caused by reduced statisticalpower associated with fewer trials. There did not appear to belarge differences in the tolerance effect between theregions.

Most previous animal studies of tolerance to the effects of cocaine would more accurately be described as investigations ofchronic rather than acute tolerance, in which a greater amountof exposure than that used in the present study was required toinduce a state of tolerance over a number of days of repeated(or continuous) treatment (Hammer et al., 1997). There has beenone demonstration of acute neurochemical tolerance to cocainein rodents within a session of investigator-administered cocaine(Maisonneuve and Kreek, 1994). In that study, the exposure wassubstantially greater than that in the present study, both interms of the dose administered and the longer duration associatedwith the intraperitoneal route of administration (Nobiletti etal., 1994). The state of tolerance we have observed occurs whenthere is little, although measurable, plasma cocaine remainingfrom the first injection. On average, the remaining cocaine was5% of the peak levels measured 2 min after infusion (Bradberryet al., 2000).

Neurochemical sensitization

Although acute tolerance can easily be demonstrated and studied in the human laboratory, the second aspect of the presentfindings (i.e., neurochemical sensitization resulting from chronicself-administration of cocaine) is more difficult to study inhumans. There has been extensive work examining the neurochemicalimpact of chronic exposure to cocaine in the rodent (Kalivas andDuffy, 1990, 1993; Kalivas and Stewart, 1991; Segal and Kuczenski,1992; White et al., 1995; Robinson and Kolb, 1999). Neuroadaptiveprocesses underlying sensitization appear to involve excitatoryamino acid mechanisms (Wolf, 1998; Bonci and Malenka, 1999) aswell as morphological changes in neurons in brain regions involvedin the mediation of psychostimulant effects (Robinson and Kolb,1999). This is the first demonstration of neurochemical sensitizationin the primate, and the first demonstration of a sensitized neurochemicalresponse to self-administered cocaine that has been demonstratedin any species. There are reports of heightened behavioral responsesto self-administered cocaine in monkeys exposed previously topsychostimulants via self-administration. In particular, theywill initiate self-administration at lower unit doses (Wojnickiand Glowa, 1996). Repeated investigator administration of highdoses results in progressively exaggerated behavioral responses(Post et al., 1976; Farfel et al., 1992; Castner and Goldman-Rakic,1999). Also, there are reports of heightened behaviors and subjectivereports of elevated mood with controlled repeated administrationof amphetamine (Strakowski et al., 1996; Strakowski and Sax, 1998).

Because we have demonstrated previously enhanced responsiveness to cocaine in the ventromedial striatum (Bradberry et al.,2000), an issue of concern for the across-session studies is thepotential introduction of a regional bias via the choice of thesite order for placement. Placement order varied between medialand lateral positions as well as between dorsal ventral placements,and as can be seen in Figure 5, the distribution of ventromedialplacements was not skewed toward the later studies. Also apparentin Figure 5 is the observation that sensitization did not occurin the sensorimotor striatum. This regional divergence betweenthe sensorimotor and the mesolimbic striatum in vulnerabilityto sensitization has not been observed previously. However, thesedata (like the lack of tolerance in this region) should be interpretedcautiously because of the reduced statistical power attributableto the limited number of data points for dorsolateral striatalplacement.

The incentive sensitization theory of addiction (Robinson and Berridge, 1993) presumes long-term neuroadaptations in brainregions mediating reward. The selective changes in the mesolimbicstriatum that we have observed support such changes in responseto intermittent low-dose exposure to cocaine in primates. Thisdemonstration that neurochemical sensitization does occur in thenonhuman primate lends substantial support for such an occurrencein humans, as does the work of Strakowski and colleagues (Strakowskiet al., 1996; Strakowski and Sax, 1998). A striking aspect ofthe present study is the relatively small amount of drug exposureper session as well as cumulative exposure needed to result inthe progressive changes in the brain response to self-administeredcocaine. Human patterns of consumption, particularly bingeing,can result in much higher levels of exposure than can the moderateones used in this study. Thus, although the magnitude of the sensitizationwe observed herein was small, it remains an open question whethera more aggressive exposure to cocaine resembling human binge patternsof consumption would result in more pronouncedchanges.

Behavioral sensitization

The present study also leaves unanswered whether the neurochemical sensitization we observed is linked to an altered behavioralresponse to the cocaine cue. Although response rates from twoof the animals did correlate with the time into the study, thoseanimals were operating under an FR30 schedule compared with anFR10 schedule for the other two, and because they were smaller(and younger) animals, their ability to reach the lever was moreawkward because of barriers to prevent them from reaching theirheads. Thus, it is possible that the increased response rate overtime in these animals represents increased skill via practiceas well as increases because of motivational factors. It wouldseem that rates of lever pressing per se are not well suited fora determination of behavioral sensitization (Howell and Morse,1989), unlike more complex primate behaviors that have been shownto sensitize in other studies (Farfel et al., 1992; Castner andGoldman-Rakic, 1999).

Contribution of conditioning

These studies also addressed the role of conditioning in the ability of self-administered cocaine to induce a dopaminergicresponse. Clearly, the pronounced effects of noncontingent cocaineand the lack of a conditioned response to a surprise substitutionof saline suggest that the direct pharmacological effects of cocainepredominate in the dopaminergic response. Although the responsesto noncontingent cocaine appear larger than those to self-administeredcocaine, it must be noted that these were the last studies conductedand that there was a hiatus in the weekly exposure to repeatedcocaine before conducting these studies, conditions one wouldmost predict to result in a sensitized response (Kalivas and Stewart,1991).

Summary

Using a nonhuman primate model of recreational cocaine use, we observed acute tolerance to the impact of repeated infusionsof self-administered cocaine on striatal extracellular DA. Thismay represent a neurochemical basis for the tolerance to the subjectiveeffects of cocaine seen in humans, a phenomenon that contributesto binge patterns of consumption (Jaffe, 1990). To the extentthat neurochemical sensitization may represent processes involvedin the switch from recreational to obsessive consumption (Robinsonand Berridge, 1993), the present results reinforce the dangerof enduring change in brain function from recreational cocaineuse that can put users at risk ofaddiction.

  FOOTNOTES

Received May 12, 2000; revised June 28, 2000; accepted July 6, 2000.

This work was supported by National Institutes of Health Grants DA 08073, DA 04060, and DA 10331 and by the Yale-VeteransAdministration Alcoholism Research Center. The excellent technicalassistance of Susan Rubino, Christopher Baccei, Rita Barrett-Larimore,Shawna Ellis, and Cindy Rodriguez is also gratefullyacknowledged.
Correspondence should be addressed to Dr. Charles W. Bradberry, Departments of Psychiatry and Laboratory Medicine, West HavenVeterans Administration Hospital and Yale University School ofMedicine, WHVA/116A2, 950 Campbell Avenue, West Haven, CT 06516.E-mail: charles.bradberry{at}yale.edu.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Ambre JJ, Belknap SM, Nelson J, Ruo TI, Shin SG, Atkinson Jr A (1988) Acute tolerance to cocaine in humans. Clin Pharmacol Ther 44:1-8[Web of Science][Medline].
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