Wisconsin Card Sorting Revisited: Distinct Neural Circuits Participating in Different Stages of the Task Identified by Event-Related Functional Magnetic Resonance Imaging

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The Journal of Neuroscience, October 1, 2001, 21(19):7733-7741

Wisconsin Card Sorting Revisited: Distinct Neural Circuits Participating in Different Stages of the Task Identified by Event-Related Functional Magnetic Resonance Imaging
Oury Monchi¹^,², Michael Petrides², Valentina Petre¹, Keith Worsley¹^,³, and Alain Dagher¹
¹ McConnell Brain Imaging Centre and ² Cognitive Neuroscience Unit, Montreal Neurological Institute, and ³ Department of Mathematics and Statistics, McGill University, Montréal, Québec, H3A 2B4 Canada

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The Wisconsin Card Sorting Task (WCST) has been used to assess dysfunction of the prefrontal cortex and basal ganglia. Previousbrain imaging studies have focused on identifying activity relatedto the set-shifting requirement of the WCST. The present studyused event-related functional magnetic resonance imaging (fMRI)to study the pattern of activation during four distinct stagesin the performance of this task. Eleven subjects were scannedwhile performing the WCST and a control task involving matchingtwo identical cards. The results demonstrated specific involvementof different prefrontal areas during different stages of taskperformance. The mid-dorsolateral prefrontal cortex (area 9/46)increased activity while subjects received either positive ornegative feedback, that is at the point when the current informationmust be related to earlier events stored in working memory. Thisis consistent with the proposed role of the mid-dorsolateral prefrontalcortex in the monitoring of events in working memory. By contrast,a cortical basal ganglia loop involving the mid-ventrolateralprefrontal cortex (area 47/12), caudate nucleus, and mediodorsalthalamus increased activity specifically during the receptionof negative feedback, which signals the need for a mental shiftto a new response set. The posterior prefrontal cortex responsewas less specific; increases in activity occurred during boththe reception of feedback and the response period, indicatinga role in the association of specific actions to stimuli. Theputamen exhibited increased activity while matching after negativefeedback but not while matching after positive feedback, implyinggreater involvement during novel than routineactions.

Key words: basal ganglia; caudate nucleus; fMRI; prefrontal cortex; set-shifting; Wisconsin card sorting

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The Wisconsin Card Sorting Task (WCST) has been used to investigate deficits in executive function in humans (Milner, 1963;Nelson, 1976; Stuss et al., 2000). The subject is asked to matchtest cards to reference cards according to the color, shape, ornumber of stimuli on the cards. Feedback is provided after eachmatch, enabling the subject to acquire the correct rule of classification.After a fixed number of correct matches, the rule is changed withoutnotice, and the subject must shift to a new mode of classification.Thus, the WCST measures cognitive flexibility, that is the abilityto alter a behavioral response mode in the face of changing contingencies(set-shifting).

Patients with lesions of the prefrontal cortex (PFC) are impaired at card sorting (Milner, 1963; Nelson 1976; Stuss et al.,2000). The basal ganglia also play a role in WCST performanceas shown by impairments observed in patients with Parkinson'sdisease (Bowen et al., 1975; Lees and Smith, 1983; Gotham et al.,1988), consistent with the strong anatomical connections betweenthe PFC and basal ganglia (Alexander et al., 1986; Middleton andStrick, 1994). Alexander et al. (1986) proposed the existenceof parallel cortical basal ganglia loops, each comprising a specificlocation in the cortex, basal ganglia, and thalamus. There isevidence that the nature of the deficit is different in Parkinson'sdisease than after PFC lesions (Rogers et al., 1998), althoughthe specific roles of PFC and basal ganglia remainunclear.

Functional neuroimaging studies have confirmed the involvement of the PFC in set-shifting (Berman et al., 1995; Nagahama etal., 1996; Goldberg et al., 1998; Konishi et al., 1998, 1999a;Rogers et al., 2000; Nagahama et al., 2001). Basal ganglia involvementhas been less evident. Rogers et al. (2000), using positron emissiontomography (PET), reported increased activity in the caudate nucleusduring an attentional set-shifting task only during reversalsin the rule of classification, but not during the types of extra-dimensionalset-shifts that occur in the WCST. Moreover, the events duringset-shifting can be separated into those occurring at the pointof receiving negative feedback, indicating that the current setmust be changed, and those occurring while the action is performedunder the new attentional set. Thus far, brain imaging studiesof the WCST have not attempted to differentiate brain activitybetween these two aspects of set-shifting. In addition, thesestudies did not separate activity occurring during the momentof receiving positive feedback, indicating that the current setmust be maintained, and activity occurring when matching accordingto the current set. A computational model predicted the involvementof distinct corticostriatal loops during these four stages ofthe WCST (Monchi et al., 2000). Here, we used mixed-trials event-relatedfunctional magnetic resonance imaging (fMRI) to determine thespecific location and pattern of activation in the PFC and basalganglia during these four stages of theWCST.

  MATERIALS AND METHODS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Subjects. Eleven right-handed subjects (mean age, 24 years; range, 18-31 years; five males, six females) with no history ofneurological or psychiatric disorder participated in this study.All subjects gave informed consent to the protocol, which wasreviewed and approved by the Research Ethics Committee of theMontreal NeurologicalInstitute.

Cognitive task. A computerized version of the WCST was administered using stimulus presentation software (Media Control Function;Digivox, Montréal, Canada). Subjects were fully trained on thetask, using a personal computer, before the scanning session.During scanning, the computer display was projected onto a mirrorin the MRI scanner. Throughout this task, four fixed referencecards are present in a row on the top of the screen, displayingone red triangle, two green stars, three yellow crosses, and fourblue circles, respectively (Fig. 1). On each trial, a new testcard is presented in the middle of the screen below the referencecards. Subjects must then match the test card to one of the referencecards based on the color, shape, or number of the stimuli.

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Figure 1. Appearance of the computer monitor during the different events of the WCST task. WCST trials are shown on the left, control trials on the right. The top four cards (on the monitor) are the reference cards, and the bottom card is the test card. During the matching period, the subject chooses the reference card that matches the test card by moving the orange cursor beneath the cards using computer mouse buttons. In the WCST trials, a change in screen brightness during the feedback period indicates a correct or incorrect match. The four subtractions used for data analysis are also illustrated. A, Event 1 minus control event 5; B, event 2 minus control event 6; C, event 3 minus control event 5; D, event 4 minus control event 6 (see Materials and Methods).

Each trial consists of two periods. The first period starts with the presentation of a new test card. The subject then choosesone of the four reference cards by using two mouse buttons: theleft button to move a cursor to point to one of the referencecards, and the right button to confirm the selection. The lengthof each matching period depends on the subject's response time,which varied between 480 and 3910 msec for this experiment. Thesecond period of each trial starts as soon as the subject hasmade a selection and consists of feedback conveyed through a changein screen brightness lasting 1900 msec. An incorrect classificationis indicated by a dark screen during the feedback period (Fig.1A), whereas a correct classification is indicated by a brightscreen (Fig. 1C).

In addition, there were control trials during which the test card was identical with respect to color, shape, and number toone of the four reference cards. For these control trials, subjectswere asked to match the test card to the identical reference card,and the screen maintained its original brightness during the feedbackperiod (Fig. 1A,C). During a scanning session, the subjects performedfour types of trials: WCST trials that require matching accordingto color, shape, or number, and controltrials.

Each scanning session consisted of five runs. Blocks of each of the four trial types (the three WCST trials, and the controltrial) were presented in random order three times per run. Inthe WCST blocks, six correct matching responses in a row had tobe completed before a change in dimension occurred. The controlblock consisted of eight trials. The total number of individualtrials per run varied with subject performance because it dependson the number oferrors.

To study the pattern of activation during the different stages of the WCST, four experimental event periods and two controlevent periods were defined. These six events were: event 1, receivingnegative feedback, indicating that a shift is required; event2, matching after negative feedback, which is the execution ofthe first match after the set-shift; event 3, receiving positivefeedback, indicating that the current matching criterion mustcontinue to be used; event 4, matching after positive feedback,which is the execution of matching according to the current criterion;event 5, control feedback; event 6, control matching. Activityin the appropriate control period trials was subtracted from thatof the different experimental event periods of the color, shape,and number trials combined to generate the following four contrastsfor statistical analysis: (1) receiving negative feedback in theWCST minus control feedback (Fig. 1A); (2) matching after negativefeedback in the WCST minus control matching (Fig. 1B); (3) receivingpositive feedback in the WCST minus control feedback (Fig. 1C);and (4) matching after positive feedback in the WCST minus controlmatching (Fig. 1D).

fMRI scanning. Subjects were scanned using a 1.5T Siemens Vision MRI scanner (Siemens AG, Erlangen, Germany). Each scanningsession began with a high-resolution T1-weighted three-dimensionalvolume acquisition for anatomical localization (voxel size, 1× 1 × 1 mm³). This was followed by acquisitions of echoplanar T2*-weightedimages with blood oxygenation level-dependent (BOLD) contrast(TE, 50 msec; FA, 90°). Functional images were acquired in fiveruns in a single session. The volumes were acquired continuouslyevery 3.5 sec within each run, and the total number of volumesacquired varied from run to run (from 79 to 113) depending onthe subject's performance. Volumes contained 16 slices each of6 mm thickness (matrix size, 128 × 128 pixels; voxel size, 2.35× 2.35 × 6 mm³). The stimulus presentation and the scanning were synchronizedat the beginning of eachrun.

Data analysis. The first three frames in each run were discarded because the BOLD signal does not reliably reach steady stateduring those frames. Images from each run were first realignedusing the fourth frame as reference. They were then smoothed usinga 6 mm full-width half-maximum (FWHM) isotropic Gaussian kernel.The data analysis was performed using an in-house package (Worsleyet al., 2000) (available at http://www.bic.mni.mcgill.ca/users/keith/).The statistical analysis of the fMRI data was based on a linearmodel with correlated errors. The design matrix of the linearmodel was first convolved with a difference of two gamma hemodynamicresponse functions with a mean lag of 5.4 sec timed to coincidewith the acquisition of each slice (Glover, 1999). Drift was removedby adding polynomial covariates in the frame times, up to degreethree, to the design matrix. Because the response times of thesubjects in each trial varied, we were able to obtain BOLD signalat different time points for each type of trial, allowing us toreconstruct the previously defined six events. The correlationstructure was modeled as an autoregressive process of degree one(Bullmore et al., 1996). At each voxel, the autocorrelation parameterwas estimated from the least-squares residuals using the Yule-Walkerequations, after a bias correction for correlation induced bythe linear model. The autocorrelation parameter was first regularizedby spatial smoothing with a 15 mm FWHM Gaussian filter, then usedto "whiten" the data and the design matrix. The linear model wasthen re-estimated using least squares on the whitened data toproduce estimates of effects and their SEs. Then, the resultingeffects and standard effect files were spatially normalized bynonlinear transformation into the standard proportional stereotaxicspace of Talairach and Tournoux (1988) using the algorithm ofCollins et al. (1994).

In a second step, runs and then subject data were combined using another linear model for the session and subject effects,weighted inversely by the square of their SEs. A random effectsanalysis was performed by first estimating the ratio of the randomeffects variance to the fixed effects variance, then regularizingthis ratio by spatial smoothing with a 13 mm FWHM Gaussian filterfor the average over runs and a 10 mm FWHM Gaussian filter forthe average over subjects. The variance of the effect was estimatedthen by the smoothed ratio multiplied by the fixed effect varianceto achieve higher degrees offreedom.

The resulting T statistic images were thresholded using the minimum given by a Bonferroni correction and random field theoryto account for multiple comparisons (Worsley et al., 1996). Thethreshold was calculated on the basis of an estimated gray mattervolume of 600 cm³. For a single voxel, this yields a threshold of t > 4.70, whichcorresponds to p < 0.05 corrected. For statistical peaks belowthat threshold, significance was also assessed on the basis ofthe spatial extent of the cluster of contiguous voxels with p< 0.05 corrected using the method of Friston et al. (1995).

  RESULTS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

All 11 subjects completed 45 WCST conditions (five runs, nine conditions per run). They made on average 0.45 perseverativeerrors and 6.65 nonperseverative, or set-loss, errors during thescanning session. They made an average of 52.87 incorrect classificationsafter shifts in condition. We compared the BOLD signal that wasobtained during the trials requiring matching according to color,shape, and number (combined) with that obtained during the correspondingperiods in the control trials. As predicted, a network of structuresinvolving the PFC, basal ganglia, and thalamus showed relativelygreater activity during different stages of WCST performance thanduring corresponding control conditions (see Tables 1-4).

Receiving negative feedback

When activity during the period of receiving negative feedback (event 1) was compared with the control feedback condition(event 5) (Table 1), there were significant activity increases,bilaterally, in the mid-dorsolateral PFC (areas 46, 9/46) (Fig.2A), in the mid-ventrolateral PFC (area 47/12) (Fig. 2B), andin the posterior PFC at the most caudal part of the inferior frontalsulcus, namely at the junction of rostral area 6 with area 8Aand area 44 (Fig. 2C). There were also bilateral increases ofactivity in the caudate nucleus and the dorsal thalamus (Table1, Fig. 2D). These structures make up the prefrontal corticalbasal ganglia loops (Alexander et al., 1986). Significant activationwas also found, bilaterally, in the rostral anterior cingulatecortex (area 32), lateral premotor cortex (area 6), posteriorparietal cortex (areas 7 and 40), and prestriate cortex (area19). Relative to the control, there was a reduction in the BOLDsignal in the left medial frontal cortex (area 10), left motorcingulate region (area 24), left motor cortex (area 4), and bilateralputamen and posterior parietal cortex during the reception ofnegative feedback (Table 1).


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Table 1. Receiving negative feedback (event 1) minus control feedback (event 5)

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Figure 2. Location of prefrontal peaks. The top left panel displays the sites of the main prefrontal areas identified in the experiment on a cortical surface rendering of an MRI in standard stereotaxic space. The vertical blue lines indicate the anteroposterior level of the coronal sections in A and B. The horizontal blue lines indicate the dorsoventral level of the sections displayed in C and D. The focus in the mid-dorsolateral PFC is indicated by the red circle, in mid-ventrolateral PFC by the green circle, and in posterior PFC by the yellow circle. A, Coronal section through the mid-dorsolateral PFC peak at Y = +30 mm. B, Coronal section through the mid-ventrolateral PFC peak at Y = +22 mm. C, Horizontal section through the posterior PFC peak at Z = +30 mm. D, Horizontal section through the mid-ventrolateral PFC peak at Z = +4 mm. Note also caudate and thalamus activation. All activation peaks shown here occurred during receiving negative feedback (event 1) minus control feedback (event 5). Some of these PFC peaks also occur selectively in other subtractions, permitting their functional dissociation (see Discussion and Table 6). The anatomical MRI images shown in A-D are the average of the T1 acquisitions of the 11 subjects transformed into stereotaxic space. The color scale represents the T statistic. IFS, Inferior frontal sulcus; IPrS, inferior precentral sulcus.

Matching after negative feedback

When the period of matching after negative feedback (event 2) was compared with the control matching period (event 6) (Table2), the BOLD signal was greater in the left putamen (Fig. 3)and left posterior PFC (Fig. 2C). There were also increases inactivity in the posterior parietal cortex (area 7), prestriatecortex (area 19), and right lateral premotor cortex (area 6).A reduction in BOLD signal in the right restroplenial cortex (area30) was also observed.


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Table 2. Matching after negative feedback (event 2) minus control matching (event 6)

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Figure 3. Putamen activation while matching after a set-shift. Activation map of the subtraction: matching after positive feedback (event 2) minus control matching (event 6). Horizontal section at Z = +6 mm. The anatomical MRI is the average of the T1 acquisitions of the 11 subjects transformed into stereotaxic space.

Receiving positive feedback

When activity during the period of receiving positive feedback (event 3) was compared with the control feedback condition(event 5) (Table 3), there were significant increases in BOLDsignal in the right mid-dorsolateral PFC (areas 46, 9/46), posteriorPFC (area 8), restroplenial cortex (area 30), and left posteriorparietal cortex (area 40). A reduction in the BOLD signal in thelateral premotor cortex (area 6) was also observed.


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Table 3. Receiving positive feedback (event 3) minus control feedback (event 5)

Matching after positive feedback

Activity during matching after positive feedback (event 4) compared with the control matching condition (event 6) (Fig. 1D)yielded only three significant positive peaks, namely the lateralpremotor cortex (area 6), bilaterally, and the left posteriorparietal cortex (area 7) (Table 4). There was a reduction inBOLD signal in the right restroplenial cortex (area 30) and theright posterior parietal cortex (area 40).


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Table 4. Matching after positive feedback (event 4) minus control matching (event 6)

Receiving negative feedback relative to receiving positive feedback

To understand further the specificity of involvement of the different areas of the PFC and the basal ganglia in WCST performance,the change in BOLD signal was also examined by subtracting activityduring the period of receiving positive feedback (event 3) fromthe period of receiving negative feedback (event 1) (Table 5).Significantly greater BOLD signal was found bilaterally in themid-ventrolateral PFC (area 47/12), the caudate nucleus, and themediodorsal thalamus (Fig. 2D). These structures make up a prefrontalcortical basal ganglia loop originating in the mid-ventrolateralPFC (Alexander et al., 1986). Significant activation was alsofound using this contrast in the right prestriate cortex (area19), the left lateral premotor cortex (area 6), and the rightposterior parietal cortex (area 7). The reverse subtraction, receivingpositive feedback minus receiving negative feedback, did not giverise to any significant differences.


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Table 5. Receiving negative feedback (event 1) minus receiving positive feedback (event 3)

  DISCUSSION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

We used event-related fMRI to dissociate activity related to shifting versus maintaining an attentional set and to receivingfeedback versus selecting the appropriate action during the performanceof the WCST. First, there was a dissociation between the mid-ventrolateraland mid-dorsolateral prefrontal areas. Although both showed increasedactivity during set-shifting, only the mid-dorsolateral PFC alsoshowed increased activity during set maintenance. Second, therole in set-shifting of the posterior lateral PFC (Konishi etal., 1998, 1999a) was clarified and shown to be different fromthat of the mid-dorsolateral and mid-ventrolateral prefrontalareas. Third, consistent with clinical studies, the caudate andputamen were found to be involved in performance of thetask.

Differential prefrontal activity

After matching a card, the subject receives feedback that must be related to information in working memory about earlier trialsto decide whether to maintain or shift the current attentionalset. Thus, responding to either negative or positive feedbackinvolves monitoring the contents of working memory. In the presentstudy, receiving either type of feedback compared with the controlcondition was associated with increased signal in the mid-dorsolateralPFC (area 9/46) (Tables 1, 3, 6; Fig. 2A). This area has previouslybeen shown to be involved in monitoring information in workingmemory (Petrides et al., 1993a, 1993b), a finding that has beenreplicated several times with various types of stimulus material(for review, see Owen, 1997; Petrides, 2000). Moreover, in monkeys,lesions confined to the mid-dorsolateral PFC yield a severe andselective impairment in the monitoring of working memory withoutaffecting the maintenance of information in memory per se (Petrides,1991, 1995).


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Table 6. Frontal and basal ganglia activation during the WCST

In contrast to the mid-dorsolateral prefrontal region, the mid-ventrolateral prefrontal area 47/12 was significantly involvedwhile receiving negative feedback (Tables 1, 5, 6; Fig. 2B,D),that is, at the point necessitating a set-shift, but not whilereceiving positive feedback. In the monkey, shifting from a previouslyrelevant to a new response mode is impaired by lesions of theinferior prefrontal convexity (Iversen and Mishkin, 1970). Thispart of the PFC is architectonically and topographically comparablewith the human ventrolateral PFC (Petrides and Pandya, 1994).It can therefore be inferred that the mid-ventrolateral prefrontalactivity seen here is selectively related to the cognitive eventsinvolved in shifting attentional set. This difference in mid-dorsolateralversus mid-ventrolateral PFC involvement in the WCST is consistentwith a theoretical position that posits a major difference inthe role of the mid-dorsolateral PFC, which is necessary for themonitoring of information in working memory, as opposed to themid-ventrolateral PFC, which is considered to be involved in morebasic executive processing, such as the active comparison of stimuliheld in working memory (Petrides, 1994, 1996).

The neural activity during the reception of feedback could be a result of the response to the rewarding or punishing valuesof the feedback stimulus as well as to the act of mentally shiftingset. Previous fMRI studies have implicated the orbitofrontal cortex(OFC) and ventral striatum in the reception of reward and punishment.For example, the passive reception of monetary gains or lossesactivated these regions, but not the mid-ventrolateral PFC ordorsal striatum (Breiter et al., 2001). In two other fMRI studies,the reception of reward or penalty during simple tasks not requiringset-shifting or learning also activated the lateral OFC but notthe mid-ventrolateral or dorsolateral PFC (Elliott et al., 2000;Zalla et al., 2000). However, a fMRI study of monetary rewardsand losses during a reversal learning task showed involvementof both lateral OFC and mid-ventrolateral PFC after negative feedback,which signaled both a monetary loss and a need for a shift instrategy (O'Doherty et al., 2001). These findings suggest thatthe OFC responds to emotionally salient feedback, whereas theventrolateral PFC is only involved if it is necessary to plana response to the negative feedback. We suggest that the lackof OFC involvement in our study is attributable to the lack ofemotional salience of the feedback in the WCST compared with theseotherparadigms.

Previous imaging studies of the WCST demonstrated increased activity in a posterior lateral prefrontal area during set-shiftinglocated at the most posterior part of the inferior frontal sulcus(Konishi et al., 1998, 1999a). This activity focus was also observedin the present study, but it could be clearly dissociated fromactivity in the mid-dorsolateral and mid-ventrolateral PFC. Thisposterior prefrontal region, at the junction of areas 44, 8A,and rostral 6, corresponds to the periarcuate region of the macaquemonkey cortex (Petrides and Pandya, 1994). Lesions confined tothe periarcuate region cause impairment in the selection of alternativeresponses on the basis of conditional rules (i.e., select responseX when stimulus A, but response Y when stimulus B) in monkeys(Halsband and Passingham, 1982; Petrides, 1982, 1987) and humans(Petrides, 1985, 1990). Importantly, this conditional learningdeficit can be dissociated from the impairment in monitoring ofworking memory caused by mid-dorsolateral prefrontal lesions (Petrides,1987).

In the present study, activation of this posterior lateral prefrontal region was found during the reception of both positiveand negative feedback, as well as during matching after negativefeedback. Thus, activation of this region, unlike the mid-dorsolateraland mid-ventrolateral cortex, was seen during the actual matchingresponses. This finding, taken in conjunction with those obtainedfrom lesion studies in monkeys and humans, suggests that the posteriorlateral prefrontal region may be involved in the selection ofthe appropriate response on the basis of the currently relevantrule rather than in the establishment or maintenance of therule.

Other imaging studies are consistent with this notion. When Konishi et al. (1999a) modified the WCST by explicitly informingsubjects of the dimensional shifts, they still detected transientBOLD activity bilaterally in the posterior prefrontal area atthe time of the shifts. Thus, this area is involved in establishingthe correct conditional response even when the rule does not haveto be determined by trial and error. Nagahama et al. (2001) alsofound a dissociation between posterior PFC and mid-dorsolateralPFC when comparing a reversal task to a set-shifting task designedso that the same responses were made to the same stimuli, butaccording to different rules. The posterior PFC was involved inboth conditions, but the mid-dorsolateral PFC was only activatedin the set-shifting task, suggesting that only the latter areaplayed a role in higher-level control of response set. Other imagingstudies have shown involvement of the same posterior PFC areain the inhibition of incorrect responses (Taylor et al., 1997;Konishi et al., 1999b) and in conditional visuomotor mapping (Toniand Passingham, 1999).

We also observed significant activation in the rostral anterior cingulate cortex bilaterally only during reception of negativefeedback. This is consistent with its proposed role in detectingthe occurrence of conflict between prediction and outcome (Bernset al., 1997; Carter et al., 1998) and in situations in whichan action must be selected from among competing alternatives (Pauset al., 1993). Finally, the posterior parietal cortex was activatedduring all phases of the task. Involvement of this area has beendescribed in previous PET studies of the WCST (Berman et al.,1995; Nagahama et al., 1996; Goldberg et al., 1998) and may accountfor impairments on the task seen in patients with focal parietallesions (Anderson et al., 1991).

Cortical basal ganglia loops and attentional set

There was significantly greater signal in the caudate and putamen during the WCST than the control task. The activation wasonly detected in negative feedback trials, consistent with otherimaging studies showing greater striatal activity during noveltasks (Berns et al., 1997; Jueptner et al., 1997). Our resultsmay appear to contradict the PET study of Rogers et al. (2000),who failed to find ventrolateral PFC or striatal activation relatedto shifting attention to a new stimulus dimension. This may bebecause the transient neural events associated with shifting dimensiononce during a 90 sec PET acquisition had relatively little effecton the total measuredradioactivity.

In our study, the activity in the caudate and putamen paralleled that in the frontal cortex. Comparing the reception of negativefeedback to control feedback showed a bilateral increase in activityin the caudate nucleus and mediodorsal thalamus, as well as inthe mid-dorsolateral and mid-ventrolateral PFC. These prefrontaland subcortical structures form the "cognitive" cortical basalganglia loop, as originally proposed by Alexander et al. (1986),who also suggested that the function of each loop was linked tothe function of the cortical area that belongs to it. Interestingly,when matching after negative feedback was compared with controlmatching, there was significant activation in the left putamenand left posterior lateral PFC, structures forming one of themotor loops of Alexander et al. (1986). Note that in control matching,the subjects made the same movements as when matching after negativefeedback. Thus, the observed activation reflects the involvementof the putamen and posterior lateral PFC in performing an actionaccording to a behavioral rule. By contrast, the caudate and mid-dorsalateraland mid-ventrolateral PFC were activated during the setting ofthe rule, but not during the actual choice of action accordingto thatrule.

This pattern of involvement of the basal ganglia is consistent with single cell recordings in animals. During visuomotor tasks,caudate neurons are most active during preparation for movement,whereas putamen neurons fire mostly in relation to movement (Rolls,1994). Moreover, the firing of these neurons is usually context-dependent(Rolls, 1994; Houk and Wise, 1995), meaning that a neuron willfire in relation to a particular cue or behavioral response onlywithin the context of a certain task. This context dependencyis a key feature of attentional set and is also observed in PFC(Wise et al., 1996).

There is evidence that striatal activity is modulated by selective attention. Boussaoud and Kermadi (1997) performed single-cellrecordings in the striatum of monkeys during a conditional visuomotortask. They found large numbers of cells responding to cues thatreoriented spatial attention, even before the specification ofthe appropriate motor response. PET experiments in humans confirmthe role of the basal ganglia in attention (Vandenberghe et al.,1996; Koski et al., 1999), and patient studies have demonstratedimpaired control of visual attention in Parkinson's disease (Wrightet al., 1990; Yamada et al., 1990) and after vascular lesionsof the basal ganglia (Sakashita, 1991).

The involvement of the caudate and putamen reported here possibly explains the deficit on the WCST reported in Parkinson'sdisease (Bowen et al., 1975; Lees and Smith, 1983; Gotham et al.,1988). The finding of striatal activation in the WCST is consistentwith the theory that the basal ganglia are involved in selectingthe relevant action among competing motor responses (Mink andThach, 1993). We propose, furthermore, that the basal gangliaare particularly important in determining attentional set andguiding action in response to behavioral rules, in conjunctionwith thePFC.

  FOOTNOTES

Received May 14, 2001; revised July 19, 2001; accepted July 20, 2001.

This work was supported by the Canadian Institutes for Health Research and the International Consortium for Human Brain Mapping,National Institutes of Health-National Institute of Mental Health.We thank P. Ahad for help with stimulus presentation software,J. Aston and C. Liao for help with data analysis, and A. Charil,A. Evans, P. Neelin, and B. Pike for usefuldiscussions.
Correspondence should be addressed to Dr. Alain Dagher, McConnell Brain Imaging Centre, Montreal Neurological Institute, 3801University Street, Montréal, Québec, H3A 2B4, Canada. E-mail:alain{at}bic.mni.mcgill.ca or oury{at}bic.mni.mcgill.ca.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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