Limbic Thalamic Lesions, Appetitively Motivated Discrimination Learning, and Training-Induced Neuronal Activity in Rabbits

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The Journal of Neuroscience, September 15, 2002, 22(18):8212-8221

Limbic Thalamic Lesions, Appetitively Motivated Discrimination Learning, and Training-Induced Neuronal Activity in Rabbits
David M. Smith¹^,², John H. Freeman Jr⁴, Daniel Nicholson⁴, and Michael Gabriel¹^,²^,³
¹ Neuroscience Program, ² Beckman Institute Neuronal Pattern Analysis Group, and ³ Department of Psychology, University of Illinois, Urbana, Illinois 61801, and ⁴ Department of Psychology, University of Iowa, Iowa City, Iowa 52242

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

A substantial literature implicates the anterior and mediodorsal (limbic) thalamic nuclei and the reciprocally interconnectedareas of cingulate cortex in learning, memory, and attentionalprocesses. Previous studies have shown that limbic thalamic lesionsseverely impair discriminative avoidance learning and that theyblock development of training-induced neuronal activity in thecingulate cortex. The present study investigated the possibilitythat the limbic thalamus and cingulate cortex are involved inreward-based discriminative approach learning, wherein head-extensionresponses yielding oral contact with a drinking spout that wasinserted into the conditioning chamber after a positive conditionalstimulus (CS+) were reinforced with a water reward but responsesto the spout after a negative conditional stimulus (CS $-$ ) werenot reinforced. In this task, the rabbits learned primarily toomit their prepotent responses to the spout on CS $-$ trials. Acquisitionwas severely impaired in rabbits given limbic thalamic lesionsbefore training. As during avoidance learning, posterior cingulatecortical neurons of control rabbits developed learning-relatedneuronal responses to task-relevant stimuli, but this activitywas severely attenuated in rabbits with lesions. These resultssupport a general involvement of the cingulothalamic circuitryin instrumental approach and avoidance learning. The fact thatlearning consisted of response omission indicated that the cingulothalamicrole is not limited to acquisition or production of active behavioralresponses, such as locomotion. It is proposed that cingulothalamicneurons mediate associative attention, wherein enhanced neuronalresponses to stimuli associated with reinforcement facilitatethe selection and production of task-relevantresponses.

Key words: cingulate cortex; discrimination; approach; limbic thalamus; learning; attention; neuronal activity

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

A substantial experimental literature implicates the anterior and mediodorsal (MD) "limbic" nuclei of the thalamus and theirinterconnected cingulate cortical projection fields in processesof learning, memory, and attention (Victor et al., 1971; Isserhoffet al., 1982; Markowitsch, 1982; Beracochea et al., 1989; Squireet al., 1989; Bussey et al., 1996, 1997; Parker and Gaffan, 1997;Posner and DiGirolamo, 1998; Aggleton and Brown, 1999). Includedin the array of learning situations subserved by these cingulothalamicareas is discriminative instrumental avoidance learning, whereinrabbits learn to locomote in a wheel apparatus to avoid a shockin response to a tone [positive conditional stimulus (CS+)] andthey learn to ignore a different tone [negative conditional stimulus(CS $-$ )] that is not followed by shock. Cingulothalamic neuronsexhibit training-induced neuronal activity (TIA), insofar as theybecome more responsive, at brief latencies, to the CS+ than tothe CS $-$ during training (for review, see Gabriel, 1993). Lesionsof the limbic thalamus blocked avoidance learning and abolishedtraining-induced neuronal activity in the cingulate cortex (Gabrielet al., 1989).

Although these results indicate an important involvement of the cingulothalamic circuitry in discriminative avoidance learning,precise specification of the cingulothalamic contribution hasnot yet been achieved. For example, cingulothalamic involvementmay be limited to aversively motivated instrumental learning orto the production of particular classes of instrumental behavior,such as locomotion. Because the avoidance learning deficit wasevidenced by a failure to produce avoidance responses to the CS+,it is possible that the lesions disrupted the ability to initiatelocomotor responses oncue.

To address these issues, an instrumental discriminative approach task was implemented wherein water reward is earned by headextension and oral contact with a water spout that is insertedinto the experimental chamber after the CS+. No reward is givenfor spout contact responses made after the CS $-$ . In a previousstudy, cingulothalamic neurons exhibited training-induced activitysimilar to the activity seen during discriminative avoidance learning,suggesting common functions of these neurons in instrumental approachand avoidance learning (Freeman et al., 1996). The present studywas performed to determine whether limbic thalamic lesions wouldimpair approach learning and disrupt cingulate cortical neuronalresponses, as has been shown for discriminative avoidance learning.A positive outcome would implicate the cingulothalamic circuitryin a general associative function rather than a function specificto the avoidance learningtask.

  MATERIALS AND METHODS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Subjects and surgical procedures. The subjects were 28 male New Zealand White rabbits (Myrtle's Rabbitry, Thompson Station,TN). Seven days after arrival in the Beckman Institute vivarium,the rabbits were placed on a moderately restricted diet (one cupof Purina rabbit chow daily) to control obesity. After 1-2 weeksfor recovery from surgery, the rabbits were placed on a restrictedregimen of 100 ml of water daily. They were given at least 1 weekto adjust to this regimen beforetraining.

Bilateral electrolytic lesions of the anterior and mediodorsal thalamic nuclei were induced in 15 rabbits. The electrodesused for making the lesions were stainless steel insect pins insulatedwith Epoxylite, with 0.80-0.90 mm of the insulation removed fromthe tip. Four bilateral sites were chosen for the lesions to producemaximal damage in the target nuclei. The coordinates chosen resultedin four lesions: one each in the anterior and posterior regionsof the anterior nuclear complex, one in the anterodorsal regionof the MD nucleus, and one in the posteroventral MD thalamic nucleus.The stereotaxic coordinates (Girgis and Shih-Chang, 1981) anddurations of current passage were as follows: (1) anteroposterior(AP), 1.5 mm posterior to bregma; mediolateral (ML), 2.3 mm; dorsoventral(DV), 8.4 mm; 35 sec; (2) AP, 2.5 mm; ML, 2.3 mm; DV, 8.1 mm;40 sec; (3) AP, 3.5 mm; ML, 1.4 mm; DV, 8.7 mm; 35 sec; and (4)AP, 4.5 mm; ML, 1.6 mm; DV, 9.2 mm; 55sec.

During surgery, six fixed-position stainless steel microelectrodes were implanted intracranially in all rabbits for the recordingof neuronal (multiple-unit) activity during training. Detailsof electrode fabrication and implantation were given previously(Gabriel et al., 1995). The target sites for recording electrodeswere as follows: (1) anterior cingulate cortex, AP, 3.5 mm anteriorto bregma; ML, 0.8 mm; DV, 3.5 mm; (2) posterior cingulate cortex,AP, 4.0 mm posterior to bregma; ML, 0.8 mm; DV, 1.5 mm; (3) thebasolateral (BL) nucleus of the amygdala, AP, 0.5 mm posteriorto bregma; ML, 5.5 mm; DV, 13.25 mm; and (4) the medial divisionof the medial geniculate (MG) nucleus, AP, 7.5 mm posterior tobregma; ML, 5.0 mm; DV, 9.0 mm. Control rabbits underwent surgicalprocedures similar to rabbits with lesions but had recording electrodesimplanted in the MD thalamic nucleus (AP, 4.6 mm posterior tobregma; ML, 1.5 mm; DV, 8.0 mm) and the anteroventral (AV) thalamicnucleus (AP, 2.0 mm posterior to bregma; ML, 2.3 mm; DV, 7 mm)in addition to the other sites. Because insufficient data wereobtained from the amygdalar and thalamic sites, only the behavioraldata and cingulate cortical neuronal data are reportedhere.

Discriminative approach training. The rabbits were given daily training sessions in an apparatus designed for the administrationof discriminative approach training. The instrumental responsewas head extension and oral contact with a drinking spout. Theexperiment was conducted while the rabbits occupied a cubicalchamber that provided electrical shielding and sound attenuation.Within the chamber, rabbits occupied a Plexiglas rabbit restrainerthat allowed free head movement. Two pure tones (1 or 8 kHz; duration,500 msec; 85 dB at 20 µN/m²; rise time, 3 msec) were assigned in a counterbalanced manneras the CS+ and the CS $-$ . During training, the onset of the CS+was followed after 4 sec by insertion of a drinking spout throughan opening in the chamber wall. Head extension of ~4 cm was requiredfor the rabbits to reach the spout. Water reward (3 ml in 2 sec)was delivered during oral contact with the spout. Spout contactresponses were detected by a grounding circuit. CS $-$ presentationwas also followed by spout presentation and spout contact responseswere recorded, but no reward was delivered. Instead, spout contactresponses were followed immediately by retraction of thespout.

Acclimation and preliminary training. Before training, rabbits were given daily sessions for acclimation to the conditioningchamber and spout presentations. In these sessions, 60 spout presentationswere given at irregular intervals until the rabbits reached acriterion of at least 45 spout contact responses in a session.After acclimation, the rabbits received two preliminary trainingsessions during which baseline neuronal data were recorded forcomparison with later training sessions. In the first preliminarytraining session, the tones to be used as conditional stimuliwere presented 60 times each in an irregular sequence withoutspout presentation or water reward. In the second session, thetone conditional stimuli were presented 60 times each with thewater spout presented in an explicitly unpaired manner. The rabbitscould obtain water reward for spout contact responses. After preliminarytraining, the rabbits received daily training sessions consistingof 120 trials (60 trials each with the CS+ and CS $-$ , presentedin an irregular sequence). The intertrial interval was 8, 13,18, 23, or 28 sec, with these values occurring in an irregularorder. Training continued until the rabbits reached a criterionin which the percentage of spout contact responses on CS+ trialsexceeded the percentage of spout contact responses on CS $-$ trialsby at least 50%. This discriminative performance had to be achievedin two consecutive training sessions. On the last day of trainingbefore they were killed, all rabbits were given access to waterad libitum for 15 min in the training apparatus to assess possiblemotivational effects oflesions.

Brief-latency CS-elicited neuronal responses. The neuronal signals were fed from each electrode to field-effect transistors(FETs) that served as high-impedance source followers. The FETswere affixed to a connector that mated with a connector affixedto the rabbit's skull. This arrangement minimized the length ofthe conduction pathway (~2.5 cm) from the recording sites to thefirst stage of signal amplification. The FET outputs were fedto a preamplifier appropriate for unit recording (gain of 40,000;half-amplitude cutoffs at 500 and 8000 Hz). The records were subjectedto a second stage of active bandpass filtering (half-amplitudecutoffs at 600 and 8000 Hz; roll-off at 18 dB/octave). The recordswere then fed to Schmitt triggers with thresholds set on eachchannel to allow triggering at a mean rate of 110-190 spikes persecond. With these settings, several of the larger spikes weresampled on each channel. In addition, the bandpass filter outputswere half-wave rectified and integrated, and the outputs of theintegrators were sampled. The Schmitt trigger data provided anindex of the firing frequency of the larger spikes, whereas theintegrated activity measured the voltage fluctuations of the entirerecord, including activity below the triggering thresholds. Schmitttrigger pulses were counted, and the integrator signals were digitizedon each trial (CS presentation). Digital values were sampled every10 msec. Sampling was performed for 1.0 sec, beginning 0.3 secbefore CS onset to 0.7 sec after CS onset. The spike counts andintegrator values provided an index of brief-latency multiunitresponses to the CS+ and CS $-$ .

Collection of the brief-latency neuronal data used automatic and experimenter-controlled screening methods to ensure thatthe records did not contain noise related to spontaneous movementsof the subject (Foster et al., 1980). For example, electronicnoise detection eliminated trials accompanied by noise just beforethe CS or within 400 msec of CS onset, and data analysis was limitedto the 400 msec period after CS onset, a time empirically establishedto precede behavioral response [conditioned response (CR)]-relatednoise (Foster et al., 1980).

Long-latency neuronal responses. In addition to the brief-latency data described above, methods were used in this study toobtain measures of neuronal activity beyond the 400 msec epochthroughout the duration of the trial when the rabbits' CR-relatedmovement could occur. Records containing discrete neuronal spikeswere sampled at a rate of 25 kHz using the Discovery Program ofBrainWave Systems (now DataWave Technologies). The program storedto disk all spike waveforms that exceeded a preset voltage threshold,as well as the time of occurrence of each spike. Recording began300 msec before CS onset and continued throughout the trial untilthe subject made a spout contact response or until 5 sec afterCS onset in the case of trials with no response. The recordingthresholds were set to record the largestspikes.

Standard spike sorting procedures (Payne et al., 1995) were used to exclude non-neuronal (noise) waveforms. Multiunit recordscontaining spikes from three to five neurons throughout the fullduration of the trials were analyzed. Studies in progress areexamining the single-unit correlates of discriminative approachlearning. Preliminary results have been presented in abstractform previously (Burhans et al., 2001).

Histology. After the completion of training, the animals were killed via an overdose of sodium pentobarbital, followed bytranscardial perfusion with normal saline and 10% formalin. Thebrains were frozen and sectioned at 40 µm, and the sections werephotographed while still wet (Fox and Eichman, 1959). After drying,the sections were stained with a metachromatic Nissl and myelinstain using formol thionin (Donovick, 1974). Photographs and stainedsections were used to verify recording electrode locations. Lesionsize was estimated by drawing damaged regions on photocopied imagesfrom the atlas of Girgis and Shih-Chang (1981). Nine sectionswere photocopied from 1.5 to 5.5 mm posterior to bregma. A gridwith squares that subtended 0.25 mm² of tissue was overlaid on the photocopied drawings. The numberof squares covering damaged tissue was divided by the total numberof squares covering the region of interest, yielding an estimateof the percentage of limbic thalamic tissue destroyed. Three rabbitswere found to have <50% of limbic thalamic tissue destroyed andwere therefore excluded from the analyses. With these exclusions,a total of 13 control rabbits and 12 rabbits with lesions wereretained for additional analysis. The mean damage score for the12 rabbits with lesions was 90.17% of the total limbic thalamus(range of 69-100%). The mean damage scores for individual nucleiwere as follows: AD, 85.33%; AV, 80.17%; anteromedial, 83.92%;and MD, 94.92%. The smallest and largest lesions are depictedin Figure 1.

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Figure 1. Coronal sections showing the smallest (gray) and largest (white) lesions. Anterior cingulate cortical Area 24b and posterior cingulate cortical Area 29c/d recording sites are indicated by asterisks. Coordinates are shown in millimeters from bregma.

Because of the large size of the lesions, some damage occurred to nontargeted structures. These included the midline thalamicnuclei (four rabbits) and the stria medullaris and habenula (sixrabbits). Separate ANOVA were computed for the number of sessionsrequired for the attainment of the learning criterion in thesetwo groups of rabbits. The data of each group were compared withthe data of the remainder of the rabbits with lesions. These analysesdid not yield significant between-group differences (p > 0.44and p > 0.21, respectively). Damage to the overlying hippocampalcommissure and dorsal subiculum occurred in three rabbits. Becausethe sample of subjects with this damage was small, we did notfeel that ANOVA would be appropriate. However, the hippocampaldamage was minimal (see Fig. 1, large lesion), and the subjectsthat sustained it were among the fastest learners in the groupwith lesions. Thus, the hippocampal damage did not contributeto the significant learning deficit found in subjects with lesions(see Results). Moreover, hippocampal damage in the form of fornixlesions had no impact on discriminative approach learning (Gabrielet al., 2001).

Analysis of data. Because the rabbits took varying numbers of training sessions to attain the criterion, the data of seventraining stages common to all subjects were analyzed. The stagesincluded the first and last training sessions and five equallyspaced sessions representing the second through the sixth trainingstages for each rabbit. Thus, the analysis included seven consecutivestages of training, each stage comprising one training session.The ordinal number of the training sessions (e.g., second session,third session, etc.) representing a given training stage variedamong the rabbits. For example, the fourth stage (i.e., the midpointof the seven stages) was represented by the fifth and the eighthtraining sessions for two rabbits that reached the criterion in10 and 16 sessions, respectively. Thus, each training stage wasdesignated in group data plots by the average of the session numberscomprising that stage (see Fig. 2). Five of the rabbits with lesionsfailed to attain the criterion. In these cases, training was discontinuedafter 45 sessions, and the data of these 45 sessions were dividedinto seven stages as describedabove.

For analysis of the behavioral data, the number of sessions required for attainment of the criterion and the percentage oftrials in which a spout contact CR occurred were analyzed. Theanalysis of CR percentage at each training stage was a factorial,repeated-measures ANOVA computed using the 2V program (BMDP StatisticalSoftware). The factors used were as follows: group (control andlesion), stimulus (CS+ and CS $-$ ), and training stage (seven levels,as described above). Corrections of the F tests attributable toviolations of sphericity were performed as needed following theprocedure of Huyhn and Feldt (1976). Factors yielding significantF ratios were further analyzed using simple effect tests followingprocedures described by Winer (1962).

Analyses of the brief-latency neuronal data had the same form as the analyses of the CR percentage with an additional orthogonalfactor, post-CS recording interval (40 consecutive 10 msec intervalsafter CS onset). The training stage factor in the analysis ofthe neuronal data had eight levels rather than seven, becauseit included the neuronal activity recorded during the preliminarytraining session with noncontingent tone and water reward presentations.The preliminary training data were not included in analyses ofthe behavioral results because spout presentations did not followCS presentations during preliminary training and no spout contactCRs were possible. The data of anterior and posterior cingulatecortex were analyzedseparately.

For the long-latency neuronal data, not all of the sessions provided usable multiunit records (i.e., records containing atleast 2500 readily isolated spikes). The best two records wereselected from among the first five training sessions to representan early training stage. None of the rabbits exhibited significantdiscriminative behavior during these sessions. The records selectedfor the late training stage included the criterial session anda second postcriterial training session, which occurred withinone or two sessions of the criterial session. Analysis of thelong-latency neuronal data took the same form as the analysisof the brief-latency data, except that the post-CS interval factorhad 43 levels (consecutive 100 msec intervals after CS onset).The analyses showed that the long-latency responses in the anteriorcingulate cortex were not significantly related to the trainingevents. Therefore, only the posterior cingulate cortical long-latencydata arepresented.

  RESULTS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Behavior

Behavior during acclimation and water consumption sessions
No differences between control rabbits and rabbits with lesions were found in the number of sessions required to attain theacclimation criterion before training (F_(1,23) = 0.096; p < 0.76),the number of responses made during the final acclimation session(F_(1,20) = 1.487; p < 0.24), or the amount of water consumed duringthe preliminary training sessions (F_(1,20) = 0.595; p < 0.45).Water consumption of control rabbits and rabbits with lesionsdid not differ significantly during the ad libitum access periodafter the completion of training (F_(1,15) = 1.408; p < 0.26).

First stage of training
Although there were no differences between groups before the initiation of training, rabbits with lesions approached the spoutafter its presentation less frequently than controls during thefirst session (stage) of training (p < 0.05). This reduced incidenceof the approach response was nondiscriminative, i.e., it occurredequally on CS+ and CS $-$ trials (Fig. 2). This effect was indicatedby simple effect tests after a significant interaction of thegroup and training stage factors (F_(6,138) = 3.36; p < 0.01).It is suggested that the initial experiences of spout presentationfollowed by nonreward produced an emotional response that disruptedthe approach response to the spout. Note that this interpretationis not in conflict with the finding (below) that the rabbits withlesions were severely retarded in learning to associate the CS $-$ with nonreward. The latter impairment was an associative (discriminative)failure and, thus, need not have involved any lesion-related changein emotionality.

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Figure 2. Percentage of spout contact responses made to the CS+ (solid lines) and the CS $-$ (dashed lines) by control rabbits (gray lines) and rabbits with lesions (black lines). Because the rabbits took varying numbers of training sessions to attain the criterion, the data of several training stages common to all subjects are shown. For control rabbits, the seven stages included the first and last training sessions and five equally spaced sessions representing the second through the sixth training stages for each rabbit. Rabbits with lesions required approximately twice the number of training sessions to attain criterion than controls. The abscissa labels indicate the average session numbers used for each training stage. For example, if the second training stage comprised sessions 4, 5, 6, and 7, the average of the sessions used to obtain data for the second training stage would be 5.5.

Sessions required to attain the criterion
The rabbits with lesions exhibited a severe retardation of discriminative behavioral acquisition. The mean number of trainingsessions (33.3) required for attainment of the learning criterionby the rabbits with lesions was significantly greater than themean number of sessions (15.9) required by controls (F_(1,23) =16.44; p < 0.0001). Five of the 12 rabbits with lesions failedto reach the criterion within the 45 allotted sessions, and eightof the rabbits with lesions required >30 conditioning sessions.Only one of the 13 control rabbits required 30 training sessionsto reach the criterion. The extent of damage to the limbic thalamuswas significantly correlated with the number of sessions requiredto attain criterion (n = 12; r = +0.64; p < 0.01).

Performance during acquisition
The percentage of CRs performed by rabbits with lesions and controls during the seven stages of training are plotted in Figure2. The analysis of these data yielded a significant interactionof the group, stimulus, and training stage factors (F_(6,138) =2.58; p < 0.05). Simple effect tests showed that control rabbitsdeveloped significant discriminative responding (significantlymore frequent responding on CS+ trials than on CS $-$ trials; p <0.05) after an average of 8.5 sessions. The rabbits with lesionsdid not exhibit significant discrimination until after an averageof 25.8 conditioning sessions. Rabbits with lesions also respondedto the CS $-$ significantly more often than controls throughout training,to and including the next-to-last conditioning session (afteran average of 33.3 sessions; p < 0.05). During the last conditioningsession, rabbits with lesions responded to the CS $-$ at a rate equivalentto that of controls. Other than the aforementioned reduced overallresponsiveness exhibited in the first training session by rabbitswith lesions, no group differences were found with respect toresponses to the CS+, indicating that the lesion-induced deficitwas primarily one of failure to withhold spout contact responseson CS $-$ trials.

Brief-latency neuronal activity in the posterior cingulate cortex

The rabbits in the control group developed discriminative training-induced neuronal activity (greater neuronal firing in responseto the CS+ than to the CS $-$ ) and excitatory training-induced neuronalactivity (greater firing in response to the CS+ during trainingcompared with the firing to the CS+ during preliminary training)(Fig. 3, top row). A significant interaction of the group, trainingstage, and stimulus factors was found (spike frequency, F_(7,105)= 2.78; p < 0.05). The same interaction in the analysis of theintegrated activity approached significance (F_(7,105) = 2.04;p < 0.06). Control rabbits developed significant discriminativetraining-induced neuronal activity after an average of 6.0 conditioningsessions (p < 0.05). This discrimination persisted throughouttraining. Control rabbits first exhibited significant excitatorytraining-induced neuronal activity (spike frequency, p < 0.05)on average after 3.5 conditioning sessions. This activity remainedsignificant throughout the duration of training. None of theseeffects were significant in the rabbits with lesions (Fig. 3,bottom row).

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Figure 3. Average integrated unit activity in the posterior cingulate cortex of control rabbits (top row) and rabbits with lesions (bottom row) during preliminary training and seven equally spaced training stages. Each plot shows the average integrated unit activity, in the form of Z-scores normalized to pre-CS baseline, from CS onset for 400 msec in 10 msec intervals with the response to the CS+ (black bars) and CS $-$ (white bars). The numbers above each plot indicate the average of the ordinal numbers of the sessions that were averaged to obtain data for a given training stage. For example, if the second training stage comprised sessions 4, 5, 6, and 7, the average of the sessions used to obtain data for the second training stage would be 5.5.

Long-latency neuronal activity in the posterior cingulate cortex

Summary
Representative waveforms of the spikes contributing to the posterior cingulate cortical long-latency multiunit records areshown in Figure 4. The posterior cingulate cortical neurons ofcontrol rabbits developed long-latency training-induced neuronalresponses (Fig. 5, top row). These responses took the form ofanticipatory activity (increased firing beginning ~2 sec beforethe presentation of the drinking spout) and spout responses (adramatic increase in firing after spout insertion). These responseswere discriminative in that they were significantly greater onCS+ trials than on CS $-$ trials. This neuronal activity was significantlyattenuated in rabbits with lesions (Fig. 5, bottom row).

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Figure 4. Spike overlays of the neurons contributing to the long-latency multiple-unit records of four representative rabbits. Two of the records were recorded in control rabbits (A, B), and two were recorded in rabbits with lesions (C, D). Spikes are shown for early (A, C) and late (B, D) training sessions. Recording thresholds are indicated by horizontal lines.

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Figure 5. Average multiunit spike frequency in the posterior cingulate cortex of control rabbits (top row) and rabbits with lesions (bottom row) at the beginning of training (Early) and at the end of training (Late). Each plot shows the average number of spikes per trial, in the form of Z-scores normalized to pre-CS baseline, from CS onset for 4.3 sec in 100 msec intervals with the response to the CS+ (black bars) and CS $-$ (white bars). CS onset occurred at 0 sec, and CS $-$ offset occurred at 0.5 sec. Spout presentation occurred 4 sec after CS onset and is indicated by an arrow.

Details of the analysis
The analysis yielded a significant three-way interaction of the training stage, stimulus, and group factors (F_(1,13) = 8.19;p < 0.05). The four-way interaction of group, training stage,stimulus, and 100 msec post-CS interval approached significance(F_(42,546) = 1.46; p < 0.051). Individual comparisons were performedon the mean values of the four-way interaction. The intervalsduring which significant effects were found are given in Table1.


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Table 1. The intervals, in milliseconds after tone onset, during which significant effects were found in the long-latency neuronal activity of the posterior cingulate cortex (Fig. 5)

Neuronal responses to spout presentation
The neuronal responses to the presentation of the spout were significantly attenuated in the rabbits with lesions during theearly and late stages of training compared with the responsesof controls (p < 0.05) (Fig. 5, 4000-4300 msec after CS onset).Control rabbits exhibited a training-induced increase in the neuronalresponse to the spout during CS+ trials and a training-induceddecrease in the neuronal response to the spout during CS $-$ trials(Fig. 5, top row). The neuronal responses on CS+ trials duringall three of the 100 msec intervals after spout presentation weresignificantly increased late in training relative to the earlytraining stage (all p < 0.05). In contrast, the neuronal responseson CS $-$ trials were significantly reduced during the first 100msec period after spout presentation late in training comparedwith their magnitude during the early training stage (p < 0.05).Rabbits with lesions exhibited a training-induced increase inthe neuronal response to the spout in only two of the 100 msecintervals on CS+ trials, and they exhibited no decline in responsesto the spout on CS $-$ trials. In both controls and rabbits withlesions, the neuronal responses to the spout were discriminative(significantly greater on CS+ trials than on CS $-$ trials; p < 0.05).

Anticipatory neuronal responses
Control rabbits exhibited a training-induced increase in anticipatory activity during the recording period preceding spoutpresentation (Fig. 5, top row, 2100-4000 msec after CS onset).In control rabbits, the neuronal firing frequency in this intervalwas significantly greater in 15 of the 19 100 msec intervals duringthe late training stage, compared with the early training stage(p < 0.05). This training-induced increase in anticipatory activityoccurred only on CS+ trials. Consistent with this, the anticipatoryactivity was discriminative (significantly greater firing on CS+trials than on CS $-$ trials). In controls, the neuronal firing onCS+ trials was significantly greater than on CS $-$ trials in 14of the 19 100 msec intervals from the 2100-4000 msec after CSonset (all p < 0.05). The finding of associative neuronal activityin anticipation of spout presentation is consistent with resultsfound in other laboratories (Hsieh et al., 1999; Sawamoto et al.,2000; Koyama et al., 2001). Anticipatory neuronal activity wassignificantly attenuated in rabbits with lesions. These rabbitsexhibited significantly increased firing from the early to thelate training stage on CS+ trials in just two of the 19 100 msecintervals preceding spout presentation, and the neuronal responsesduring CS+ trials were significantly greater than the responsesduring CS $-$ trials in only three of the 19 100 msec intervals inrabbits with lesions (p < 0.05).

Individual long-latency neuronal records
The findings described above were readily observable in the single-session neuronal records from individual rabbits (Fig.6). The records shown are representative of the full data set,indicating the development of discriminative spout responses andanticipatory responses in controls and attenuation of these effectsin rabbits with lesions.

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Figure 6. Representative individual posterior cingulate cortical multiunit records from three control rabbits and three rabbits with lesions. Data are shown for early and late training sessions for each rabbit. Each plot shows the spike frequency, in the form of Z-scores normalized to pre-CS baseline, from CS onset to 4.3 sec after CS onset, in 100 msec intervals. The solid and dashed lines show the responses to the CS+ and CS $-$ , respectively. CS onset occurred at 0 sec, and CS offset occurred at 0.5 sec. Spout presentation (arrow) occurred 4 sec after CS onset.

Brief-latency neuronal activity in the anterior cingulate cortex

In contrast to previous studies of discriminative avoidance learning (for review, see Gabriel, 1993), control rabbits didnot develop significant discriminative neuronal activity in theanterior cingulate cortex (interaction of the stage, stimulus,and group factors: spike frequency, F_(7,147) = 0.34, p < 0.95;integrated activity, F_(7,147) = 0.62, p < 0.73) (Fig. 7). Therabbits with lesions also did not develop discriminative neuronalactivity.

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Figure 7. Average integrated unit activity in the anterior cingulate cortex of control rabbits (top row) and rabbits with lesions (bottom row) during preliminary training and seven equally spaced training stages. Each plot shows the average integrated unit activity, in the form of Z-scores normalized to pre-CS baseline, from CS onset for 400 msec in 10 msec intervals with the response to the CS+ (black bars) and CS $-$ (white bars). Numbers above each plot indicate the average number of conditioning sessions represented by that stage. For example, if the second training stage comprised sessions 4, 5, 6, and 7, the average of the sessions used to obtain data for the second training stage would be 5.5.

  DISCUSSION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Summary of findings and conclusions

Discriminative approach learning was severely retarded and posterior cingulate cortical training-induced discriminative neuronalactivity was severely attenuated in rabbits with limbic thalamiclesions.

Because the rabbits learned to approach drinking spouts before training, they did not learn this response during training.From the outset of training, the approach response was made directlyto spout presentation, with which the CS+ was redundant. As aresult, discriminative approach learning was expressed exclusivelyas learning to omit the highly overlearned approach response whenspout presentations were preceded by the CS $-$ and no reward wasforthcoming. The lesions disturbed this omission learning. Incontrast, cingulothalamic lesions in previous studies severelyimpaired the learning of active locomotor avoidance responsesto a CS+. Therefore, cue processing suffers in subjects with cingulothalamiclesions generally, whether they are required to perform activeresponses on cue (as during discriminative avoidance learning)or to omit responses on cue (as in the discriminative approachtask).

In addition to the impairment of omission learning, the data indicated for the first time a direct involvement of the cingulothalamiccircuitry in associative processes of appetitive instrumentallearning. This is shown by the slowly acquired but robust associativecoding of the reward-predictive CS+ in the posterior cingulatecortex and by the absence of this coding in the rabbits with lesions.As noted, the rabbits with lesions approached the spout on virtuallyevery CS+ trial. These responses were very likely mediated byneuronal coding of the drinking spout itself, a coding consolidatedto noncingulothalamic areas during the extensive previous experiencewith spouts. That such consolidation occurs during overtraininghas been indicated previously (Hart et al., 1997). It is likely,however, that the discriminative approach responses exhibitedafter eight training sessions by the control rabbits were dependenton the TIA in the posterior cingulatecortex.

In summary, past and present data support cingulothalamic involvement in the mediation of the following: (1) associationsbetween a CS+ and an aversive (foot shock) reinforcer for acquisitionof an active locomotory avoidance CR; (2) appetitively based CS+and reward associations subserving a head extension CR, and; (3)CS $-$ and nonreward associations subserving CR omission. These resultsthus add substantially to knowledge of the range of task and behavioralresponse characteristics to which cingulothalamic processing isrelevant.

Neural coding of response omission

Was the lesion-related impairment of response omission on CS $-$ trials supported in controls by TIA increments in response tothe CS $-$ ? Increments of the multiunit response to the CS $-$ werenot found in the anterior or posterior cingulate cortex. As noted,incremental coding occurred in response to the CS+ in the posteriorcingulate cortex, and associative coding of the spout was alsoincremented when spout presentation was preceded by the CS+. However,neural responses to the spout diminished with training when spoutpresentation was preceded by the CS $-$ . The combination of incrementalcoding on CS+ trials and decremental coding on CS $-$ trials is sufficientto account for the discriminative learning without recourse toincremental coding of the CS $-$ . Nevertheless, incremental codingof the CS $-$ may have occurred, possibly in areas other than theposterior cingulate cortex. Preliminary analyses suggest thatsingle cells exhibit incremental coding of the CS $-$ in anteriorcingulate cortex (Burhans et al., 2001). Indeed, even during avoidancelearning a small proportion (10%) of single cells throughout thecingulothalamic circuit exhibited CS $-$ specific firing in trainedrabbits, and 40% of responsive cells in the MD nucleus showedthis effect (Kubota et al., 1996). Thus, we cannot exclude thepossibility that the impaired approach learning in rabbits withlesions may have been attributable in part to interference withincremental coding of the CS $-$ .

The cingulothalamic circuit and associative attention

The foregoing observations are in keeping with a long-standing hypothesis that cingulothalamic neurons encode the associativesignificance of task-relevant stimuli. This encoding is expressedby the TIA that develops in response to the CS+ and CS $-$ (Gabrielet al., 1980). A recent elaboration holds that the discriminativeTIA subserves associative attention and retrieval of learned responses(Gabriel and Talk, 2001).

The idea of a cingulothalamic role in attention is based on multiple findings, including the TIA itself, the remarkable enhancementof TIA when nonsalient CSs are used (Sparenborg and Gabriel, 1990;Gabriel and Taylor, 1998; Harvey et al., 2000), and the resultsof brain imaging studies with human subjects (Pardo et al., 1990;Bench, 1993; Marshall et al., 1997; Petersen et al., 1998; Posnerand DiGirolamo, 1998; Mesulam et al., 2001)

Rapid and slow coding

No significant TIA was found in the anterior cingulate cortex in this study, and minimal, late TIA was found in a previousstudy of discriminative approach learning (Freeman et al., 1996).These results contrast with studies of discriminative avoidancelearning, wherein the multiunit records in anterior cingulatecortex exhibited robust TIA in the very early stages of acquisition(for review, see Gabriel, 1993). This rapid TIA is dependent onthe integrity of the amygdala (Poremba and Gabriel, 1997). Morerecently, rapid, early TIA was found to develop during discriminativeavoidance learning in the basolateral nucleus of the amygdalaand the medial division of the medial geniculate nucleus, as wellas in the anterior cingulate cortex (Duvel et al., 2001). Auditorycortical lesions abolished the rapid TIA in all of these areas,and rapid behavioral learning, while leaving slower neuronal codingand behavioral learning intact. These areas thus form a circuitthat is essential for rapid discriminative avoidancelearning.

The involvement of this rapid circuit in avoidance learning is consistent with the possibility (above) that incremental CS $-$ coding reinforced by aversive nonreward may also be mediated byprocesses of the anterior cingulate cortex and related areas.Note that the coding of the CS $-$ subserves the discriminative learningof CR omission, and failure of this coding promotes errors ofcommission as found here in the rabbits with lesions. These considerationsbring the present data into register with the growing body ofevidence indicating a role of the anterior cingulate cortex inprocessing of errors (Gemba et al., 1986; Gehring et al., 1993;Falkenstein et al., 1995; Luu et al., 2000).

In contrast to the rapid coding circuit, discriminative approach learning and coding of associative attention in posteriorcingulate cortex are slowly acquired. The amygdala is not involvedin this learning (Smith et al., 2001), although the amygdala isneeded for a more accelerated posterior cingulate coding duringdiscriminative avoidance learning (Poremba and Gabriel, 1997).These findings are in accord with the hypothesis (Gabriel, 1993)that the posterior cingulate cortex and related circuitry mediaterelatively gradual coding of consistent, repeating stimulus-reinforcementrelationships. Coding in this circuit may also be driven by off-linerehearsal and rehearsal-like processes that are tantamount toevent repetition (Freeman and Gabriel, 1999; Sutherland and McNaughton,2000). As mentioned, avoidance trials are coded in the posteriorcingulate cortex more rapidly than approach trials. However, bothmotivationally urgent and less urgent coding occurs in this circuitin a relatively gradual manner compared with the rapid codingcircuit.

Rapid and slow neural coding and memory: filtration of experience?

It is intriguing to consider the functional significance of the rapid and slow coding circuits. Our proposal begins with thenotion that the two circuits mediate different specializationsof the memory system (Gabriel and Talk, 2001; Gabriel et al.,2002). We suggest that the two circuits implement an experience-filteringprocess. Rapid coding ensures that details of immediate, novelexperience, and especially highly aversive novel experience suchas trials of avoidance conditioning, are stored for a relativelybrief time, measured in hours. In humans, processes of the anteriorcingulate and prefrontal cortex, and the related MD thalamic nucleus,mediate this coding. It allows, for example, recall of all ofthe events of the day at the end of the day. However, becauseit is specialized for the coding of novel events, such codingwill displace previously formed codes in this circuit. Repetitiveevents will be stored by this circuit on their initial occurrences,but repetition will not strengthen the stored code. Thus, thecircuit is not well organized for enduring storage of information.For example, without rehearsal, one is not able, typically, torecall all events on a particular day of the previous week. Generally,much information stored via the rapid coding mechanism provesto be of no significance, it is not rehearsed, and it is lost.The loss of irrelevant data are an important function of the experience-filteringprocess.

The more gradual and enduring coding that occurs in the posterior cingulate cortical circuit is, like the rapid coding circuit,driven by single inputs that are highly significant (such as highlyaversive or emotional experiences). However, these events arestored not because they are novel; rather, they are stored becausethey are rehearsed. Less significant events (such as trials ofdiscriminative approach learning) are coded in the slow circuitbecause they are repeated frequently. These "admission requirements"represent a barrier that "filters out" the coding of events thatare neither important, rehearsed, nor repeated, thus enablingonly significant experiences to achieve a consolidated statusinmemory.

  FOOTNOTES

Received Feb. 4, 2002; revised June 7, 2002; accepted June 10, 2002.

This work was supported by National Institutes of Health Grant NS36591, National Institute of Mental Health (NIMH) Grant MH58259,National Institute on Drug Abuse Grant DA11164, National ScienceFoundation Grant BIR95-04842 (M.G.), and NIMH Grant F31-MH12077(D.S.).

Correspondence should be addressed to Dr. Michael Gabriel, University of Illinois, Beckman Institute, 405 North Mathews, Urbana,IL 61801. E-mail: mgabriel{at}s.psych.uiuc.edu.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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