Sensitivity to Instrumental Contingency Degradation Is Mediated by the Entorhinal Cortex and Its Efferents via the Dorsal Hippocampus

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The Journal of Neuroscience, December 15, 2002, 22(24):10976-10984

Sensitivity to Instrumental Contingency Degradation Is Mediated by the Entorhinal Cortex and Its Efferents via the Dorsal Hippocampus
Laura H. Corbit, Sean B. Ostlund, and Bernard W. Balleine
Department of Psychology University of California, Los Angeles, Los Angeles, California 90095

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Previous studies have shown that electrolytic lesions of the dorsal hippocampus render the instrumental performance of ratsinsensitive to selective degradation of the action-outcome contingency(Corbit and Balleine, 2000). In the present experiments, we soughtto replicate this finding and to examine the effects of excitotoxiclesions. In the first three experiments, rats with either electrolyticor NMDA lesions of the dorsal hippocampus and sham-lesioned controlswere trained to press two levers, each of which delivered a uniquefood outcome, before their sensitivity to outcome devaluationand degradation of the instrumental contingency was assessed.Although we were able to replicate our original finding that electrolyticlesions of the dorsal hippocampus render rats insensitive to selectivedegradation of the instrumental contingency, NMDA lesions of thedorsal hippocampus had no effect. Neither lesion had any detectableeffect on sensitivity to outcome devaluation. In experiment 4,we assessed the possibility that the effect of the electrolyticlesion resulted from damage to fibers originating in the retrohippocampalregion (including both entorhinal cortex and subiculum) by examiningthe impact of bilateral NMDA-induced lesions of the retrohippocampuson the same tasks. Importantly, this lesion produced a deficitsimilar to that observed after electrolytic hippocampal lesions.The final experiment used a disconnection procedure to assessmore directly whether damage to efferents from the retrohippocampalregion, rather than the dorsal hippocampus itself, can accountfor the observed deficit. The data from these tests suggest thatthe deficits observed previously after electrolytic hippocampallesions were the result of damage to entorhinalefferents.

Key words: entorhinal cortex; dorsal hippocampus; subiculum; instrumental conditioning; outcome devaluation; contingency degradation; reward; context

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Current behavioral evidence suggests that, in instrumental conditioning, animals encode the causal relationship between actionsand their consequences, as well as the current incentive valueof the instrumental outcome (Dickinson and Balleine, 1994; Balleineand Dickinson, 1998). Although the neural structures that mediatethese learning processes remain poorly understood, it has beensuggested that the hippocampus may be critical for the detectionof causal relationships in the environment and that removal ofthe hippocampus renders rats insensitive to changes in the instrumentalcontingency, resulting in behavior that is determined primarilyby event contiguity (Devenport, 1979, 1980; Devenport and Holloway,1980).

In a recent study, Corbit and Balleine (2000) examined the effects of hippocampal lesions on encoding the contingent relationshipbetween an instrumental action and its outcome. Rats were trainedto press two levers, one delivering sucrose and the other foodpellets. After this training, one of the instrumental contingencieswas degraded: in addition to the delivery of the sucrose and pelletoutcomes contingent on the performance of the instrumental responses,one of these two outcomes was also delivered noncontingently andin such a manner that the probability of the delivery of thatoutcome was the same whether the action was performed or not.In control rats, this manipulation was found to selectively decreaseresponding on the lever that delivered the same outcome as thatdelivered noncontingently. In contrast, rats with electrolyticlesions of the dorsal hippocampus did not show this effect butmaintained similar response rates on the two levers, indicatingthat their performance was relatively insensitive to contingencydegradation.

Although these data suggest that the hippocampus is involved in encoding the instrumental contingency, a possible concernis that this study used electrolytic lesions, which have beenshown to damage not only cell bodies but also fibers of passagewithin the lesioned region (Jarrard, 1993). As such, the deficitdescribed above could have been a result of damage to either cellsin the dorsal hippocampus or fiber pathways passing through thisregion.

Given this possibly, experiment 1 sought to replicate our original finding that electrolytic lesions of the hippocampus renderrats insensitive to contingency. Experiments 2 and 3 comparedthe impact of this lesion with the effects of cell body lesionsinduced by infusions of NMDA into the dorsal hippocampus. Thefinding that electrolytic but not NMDA lesions of the dorsal hippocampusimpair detection of changes in the instrumental contingency suggeststhat this deficit was a result of damage to fibers ofpassage.

The retrohippocampal region (i.e., the entorhinal cortex and subiculum) projects heavily through the areas lesioned in experiments1-3. As a consequence, experiment 4 investigated the effects ofNMDA lesions of the retrohippocampus on the sensitivity to contingencydegradation. Finally, experiment 5 used a disconnection procedureto determine the relative involvement of the entorhinal cortexand subiculum in this task and to relate the effects of selectivelesions of these structures directly to those obtained after electrolyticlesions of the dorsalhippocampus.

  MATERIALS AND METHODS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Experiment 1
Subjects and apparatus. The subjects were 20 experimentally naive adult male Long-Evans rats. Rats were housed singly andwere handled daily for 1 week before surgery. All procedures usedwere in accordance with standards established by the Associationfor Assessment and Accreditation of Laboratory Animal Care forthe care of experimental subjects. Training and testing took placein 12 operant chambers (Med Associates, East Fairfield, VT) housedwithin sound- and light-resistant shells. Each chamber was equippedwith a pump fitted with a syringe that delivered 0.1 ml of a 20%sucrose solution into a recessed magazine in the chamber. Eachchamber was also equipped with a pellet dispenser that deliveredone 45 mg Noyes pellet (formula A/I) when activated. The chamberscontained two retractable levers that could be inserted to theleft and right of the magazine and were illuminated by a 3 W,24 V house light mounted on the top center of the wall oppositethe magazine. Microcomputers equipped with the MED-PC program(Med Associates) controlled the equipment, delivered reinforcers,and recorded the lever presses and magazine entries whenappropriate.
Surgery and histology. At the time of surgery, rats weighed between 350 and 400 gm. The rats were anesthetized with sodiumpentobarbital (Nembutal; 50 mg/kg), treated with atropine (0.1mg), and then placed in a stereotaxic frame with the incisor baradjusted so that lambda and bregma werelevel.
Electrolytic lesions. Half of the subjects received electrolytic lesions of the dorsal hippocampus, and the other half receivedsham surgery that consisted of lowering the electrode into thehippocampus without running any current. Electrodes made frominsect pins (size 00) covered in epoxy-polyester varnish exceptfor 1 mm at the tip were lowered into four sites in the dorsalhippocampus [all coordinates relative to bregma (in mm): anteroposterior(AP), $-$ 2.8 and $-$ 4.2; mediolateral (ML), ±2.0 and ±3.0; dorsoventral(DV), $-$ 4.0). When the electrodes were in place, a 1 mA, 20 seccurrent was passed through the electrode. After surgery, the ratswere given 1 week to recover, during which they were handleddaily.
Histology. At the end of the experiment, the rats were killed with a lethal barbiturate overdose and perfused transcardiallywith 0.9% saline, followed by 10% Formalin solution. The brainswere stored in 10% Formalin solution for 48 hr and then transferredto a 25% sucrose-Formalin solution before 40 µm coronal sectionswere cut throughout the region of the hippocampus. The sliceswere stained with thionin and examined for placement and extentof the lesion, with the latter assessed by microscopic examinationof sections for areas of markedgliosis.
Procedure. After recovery from surgery, subjects were placed on a food deprivation schedule such that they received 15 gmof their maintenance diet daily to maintain them at ~85% of theirfree-feeding weight. During training, the rats were fed aftereach session. Rats had access ad libitum to tap water while inthe home cage. Each session started with the illumination of thehouse light and insertion of the levers when appropriate and endedwith the retraction of the levers and turning off of the houselight.
Magazine training. Initially, all subjects received two 30 min sessions of magazine training in which the two outcomes weredelivered on independent random time 60 sec schedules with theleverswithdrawn.
Lever training. The rats were first trained with continuous reinforcement (i.e., every action earned an outcome) for 1 d,after which they were placed on a random ratio (RR) 5 schedule(i.e., each action delivered an outcome with a probability of0.2). After 3 d of training, this was changed to a RR-10 (or aprobability of 0.1) schedule for 3 d and then to an RR-20 schedule(or a probability of 0.05) for an additional 3 d of training.The rats received two training sessions each day, one with eachaction-outcome pair. The training sessions were 30 min in duration,and the rats had a break of at least 30 min betweensessions.
Contingency degradation training. The instrumental contingency for one of the levers was degraded using a procedure pioneeredby Hammond (1980) but as modified in the experiments by Balleineand Dickinson (1998) and Corbit and Balleine (2000). At the endof training, each lever earned a unique outcome (pellets or a20% sucrose solution) with a fixed probability, that is, eachresponse had a 1-in-20 chance of delivering the appropriate outcome(p_(O/A) = 0.05). In subsequent sessions, in addition to beingearned by one of the actions, one of the outcomes was now alsodelivered noncontingently with the same probability in each secondwithout a response (i.e., p_{(O/no A)} = 0.05). For one lever, thefree reinforcer was the same as that which was earned by a responseon that lever. Thus, the experienced probability of the deliveryof that particular outcome (e.g., pellets) was the same whetheror not the rats performed that action, a procedure that shouldhave acted to degrade that action-outcome contingency. For theother lever, the free reinforcer was different from the earnedreinforcer. As such, the rats still had to respond to receivethe earned outcome, so this contingency was nondegraded. For halfof the rats in each lesion condition, the degraded contingencyinvolved pellet delivery, whereas for the remainder, it involvedthe delivery of the sucrose solution. The rats had two 20 mintraining sessions per day, one on each lever and hence one oneach contingency. The rats had a break of ~1 hr between sessions,and the order of the sessions was alternated each day. This trainingcontinued for 8d.
Contingency test. On the day after the final day of contingency training, rats in both groups received a choice extinctiontest. The test began with the insertion of the levers and theonset of the house light and ended 5 min later with the retractionof the levers and the offset of the house light. No outcomes werepresented during thissession.

Experiment 2
The general procedures for this and the following experiments were identical to those described for experiment 1 unless otherwisenoted.
Subjects and apparatus. The subjects were 19 experimentally naive male rats that weighed between 450 and 500 gm at the timeofsurgery.
Surgery and histology: excitotoxic lesions. Half of the subjects received excitotoxic lesions of the dorsal hippocampus, andthe other half received sham surgery that consisted of loweringthe cannula into the hippocampus without injecting any neurotoxin.Small burr holes were drilled into the skull bilaterally, andcannulas (28 gauge) were lowered into four sites in the dorsalhippocampus [all coordinates relative to bregma (in mm): AP, $-$ 2.8and $-$ 4.2; ML, ±2.0 and ±3.0; DV, $-$ 4.0]. A 10 µl Hamilton syringewas mounted in an infusion pump (Harvard Apparatus, South Natick,MA) and connected to the injection cannulas with polyethylenetubing. Next, 0.4 µl of NMDA (20 mg/ml; Sigma, St. Louis, MO)was infused into the hippocampus at a rate of 0.1 µl/min. Fiveminutes was allowed after the infusion for diffusion before removalof the cannulas. After surgery, the rats were given 1 week torecover, during which they were handleddaily.
Procedure. The training and testing procedures were the same as described in experiment 1above.

Experiment 3
Subjects and apparatus. The subjects were 19 experimentally naive malerats.
Surgery and histology. The surgical and histological procedures for the electrolytic and excitotoxic lesions were as describedin experiments 1 and 2above.
Procedure. The magazine and lever training procedures used were identical to those described in experiment 1 above. The otherprocedures were generally similar, with the followingexceptions.
Contingency degradation training. Contingency degradation training continued for 4 d, at which point a reliable contingencyeffect was observed in the NMDA rats. The rats next received a5 min choice extinction test identical to that described in experiment1.
Retraining. After the contingency extinction test, the rats received 3 d of retraining (one session on each lever each day)to recover responding that decreased with the previoustest.
Devaluation extinction test. After the final day of retraining, all of the rats were given access ad libitum to one of thetwo outcomes for 1 hr in the home cage. Half of the rats in eachlesion condition received pellets (50 gm placed in a bowl in thehome cage), and the remaining rats received sucrose (50 ml ina drinking bottle fixed to the front of the home cage). Immediatelyafter the prefeeding, the rats were placed in the operant chambers.A 5 min choice extinction test was then conducted in which bothlevers were extended and the number of presses on each lever wascounted. No outcomes were delivered during thetest.

Experiment 4
Subjects and apparatus. The subjects were 24 experimentally naive adult female rats that weighed between 250 and 350 gm atthe time ofsurgery.
Surgery. The surgical and histological procedures generally followed those described in experiment 2 above, with the followingexceptions.
Excitotoxic lesions. Half of the subjects received excitotoxic lesions of the retrohippocampus, and the other half receivedsham surgery that consisted of lowering the cannula into the retrohippocampuswithout injecting any neurotoxin. The coordinates used were adaptedfrom Maren et al. (1997), who found that these lesions produceda deficit in context conditioning. Cannulas (28 gauge) were loweredinto six sites in the retrohippocampal region [all coordinatesrelative to bregma (in mm): AP, $-$ 6.8, 7.5, and 8.2; ML, ±5.0,±4.5, and ±4.5; DV, $-$ 7.0, $-$ 6.5, and $-$ 5.0]. Next, 0.4 µl of NMDA(20 mg/ml; Sigma) was infused into each site at a rate of 0.1µl/min following the procedures outlined in experiment 2 above.One subject in the sham group failed to recover from surgery (n=11).
Procedure. The magazine and lever training procedures were identical to those described in experiment 1 above. The other procedureswere generally similar with the followingexceptions.
Contingency degradation training. Contingency degradation training continued for 12 d. The rats next received a 5 min extinctiontest.
Devaluation extinction test and retraining. The devaluation extinction test was identical to that described in experiment3.

Experiment 5
Subjects and apparatus. The subjects were 30 experimentally naive femalerats.
Surgery: disconnection lesions. All subjects received unilateral electrolytic lesions of the dorsal hippocampus but were thendivided into three groups that received contralateral neurotoxiclesions of either the entorhinal cortex or subiculum or sham surgerythat consisted of lowering the cannula into one of these locationswithout injecting any neurotoxin. The electrolytic lesions wereproduced as in experiment 1, except that they were unilateral[left or right side was counterbalanced; all coordinates relativeto bregma (in mm): AP, $-$ 2.8 and $-$ 4.2; ML, ±2.0 and ±3.0; DV, $-$ 4.0].Cannulas (28 gauge) were then lowered into two sites in the contralateralentorhinal cortex (in mm: AP, $-$ 7.5 and $-$ 8.2; ML, ±4.5; DV, $-$ 6.5and 5.0) or subiculum (in mm: AP, $-$ 6.3 and $-$ 6.8; ML, ±5.0; DV, $-$ 6.0 and $-$ 4.0). Next, 0.4 µl of NMDA (20 mg/ml; Sigma) was infusedinto each site at a rate of 0.1 µl/min except in the sham-lesionedgroup. Five minutes was allowed after the infusion for diffusionbefore removal of the cannulas. After surgery, the rats were given1 week to recover, during which they were handleddaily.
Procedure. The magazine and lever training procedures were identical to those described in experiment 1 above. The other procedureswere generally similar, with the followingexceptions.
Contingency degradation training. Contingency degradation training continued for 3 d and was followed by a 5 min extinctiontest.

  RESULTS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Histology

No recovery problem or weight loss was observed after surgery in any of the lesion groups. In all electrolytically lesionedrats (experiments 1 and 3), damage to the dorsal hippocampus wasbilateral and complete, except at the rostral and caudal extremesand with some sparing of tissue on the lateral edges of the lesions.Figure 1, left, summarizes the maximum and minimum damage resultingfrom the lesions for the rats included in the behavioral analysis.No systematic damage to the overlying cortex was observed in eithergroup. All rats receiving excitotoxic hippocampal lesions (experiments2 and 3) had complete bilateral lesions of the dorsal hippocampus,except at the rostral and caudal extremes. Figure 1, middle, summarizesthe maximum and minimum damage from the lesions. The lesions weregenerally consistent between rats. Inspection of the stained tissuedid not reveal damage to areas outside the hippocampus in theregion of the lesion. In general, these neurotoxic lesions weresimilar to those obtained with an electrolytic procedure, althoughthe latter produced damage to axonal tracts passing through thedorsal hippocampus, and, if anything, electrolytic lesions sparedmore tissue at the lateral and rostral extremes of the region,whereas NMDA infusions produced a more complete lesion.

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Figure 1. Line drawings of coronal sections from the brains of subjects with the maximum (dark gray) and minimum (light gray) damage resulting from electrolytic lesions of dorsal hippocampus (A), NMDA lesions of dorsal hippocampus (B), and NMDA lesions of retrohippocampal region (C). Starting from the top, sections for the hippocampal lesions are taken from the following points in the AP plane (relative to bregma, in mm): $-$ 2.56, $-$ 3.14, $-$ 3.60, $-$ 4.16, and $-$ 4.52. Sections for the entorhinal lesions are taken from the following points: $-$ 6.30, $-$ 7.04, $-$ 7.64, $-$ 8.0, and $-$ 8.72. Drawings are from Paxinos and Watson (1998).

All rats receiving excitotoxic lesions of the retrohippocampus (experiment 4) had complete bilateral damage of the medialentorhinal cortex and limited yet reliable damage to the lateralentorhinal cortex, subiculum proper, subicular cortices (presubiculumand parasubiculum), and the caudal aspect of the dentate gyrus.Figure 1, right, summarizes the maximum and minimum damage fromthe lesions. The lesions were generally consistent betweenrats.

In experiment 5, unilateral lesions of the dorsal hippocampus were consistent across lesion groups and were similar in extentof damage to electrolytic lesions in experiments 1 and 3 (Fig.2, left). Contralateral NMDA lesions of the subiculum producedsubstantial damage to the ventral subiculum. These lesions wereoften narrow, preserving the medial and lateral portions of theventral subiculum in several rats. In addition, the coordinateswere chosen to minimize the risk of overlap; thus, the most posterioraspect of the ventral structure remained intact in several rats.Animals with large lesions also had limited damage of the presubiculum(Fig. 2, middle), extending rostrally in some rats to the ventralhippocampal fields (dentate gyrus and CA1). Contralateral NMDAlesions of the entorhinal cortex (Fig. 2, right) were generallylimited to the medial entorhinal cortex but often included somedamage to the presubiculum and parasubiculum. Additional investigationwould be needed to determine the individual contribution of thepresubiculum and parasubiculum in contingency learning. As shownin Figure 2, there was no overlap in the minimal or maximal damageof the subicular and entorhinal lesions.

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Figure 2. Line drawings of horizontal sections from the brains of subjects with the maximum (dark gray) and minimum (light gray) damage resulting from unilateral electrolytic lesions of the dorsal hippocampus (left) and contralateral (middle) NMDA lesions of subiculum or NMDA lesions of entorhinal cortex (right). Each section is marked with its position in the DV plane (millimeters relative to bregma). Drawings are from Paxinos and Watson (1998).

Experiment 1

Training
No effect of the lesion on the acquisition of lever pressing was observed. The two groups acquired the lever press responsein the same number of days. Furthermore, no difference in therate of lever pressing between the lesion [mean responses perminute (M) = 33.43; SE = 5.33] and sham (M = 43; SE = 4.40) groupswas evident at the end of initial training (F_(1,18) = 1.961; p> 0.05).

Contingency degradation training
Figure 3, left, shows the effects of contingency degradation across 2 d blocks of training. Inspection of the figure suggeststhat, across days, at least in the sham group, the rats showedsensitivity to the degradation of the instrumental contingency,performing more responses on the lever for which the contingencyhad not been degraded. The statistical analysis of the contingencytraining data revealed a main effect of contingency (F_(1,18) =4.482; p < 0.05), a main effect of training day (F_(3,54) = 5.573;p < 0.01), but no main effect of group (F < 1). Examination ofFigure 3 suggests that the hippocampal rats were not sensitiveto the degradation of the instrumental contingency; however, thegroup × contingency interaction failed to reach significance (F_(1,18)= 2.00; p > 0.05). None of the other interactions were significant.

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Figure 3. Mean lever presses per minute across 2 d blocks of contingency degradation training are depicted at left. For each group, one of the action-outcome contingencies had been degraded, whereas the other remained nondegraded. Right, Lever responses for electrolytically and sham-lesioned rats in a two-lever choice extinction test after the selective degradation of one of the instrumental contingencies. Error bars represent the SE of the difference of the mean (±1 SED) for the within-subjects variable in each group.

Extinction test
As shown in Figure 3, right, it is clear that the two groups performed very differently on this test. Whereas the sham groupshowed a clear decrease in responding on the lever for which thecontingency had been degraded relative to the other lever, thiswas not true of the hippocampal rats, which appeared to performboth actions at comparable rates. The analysis of the extinctiontest data confirmed this description. This analysis revealed nomain effect of group (F_(1,18) < 1); there was, however, a maineffect of contingency (F_(1,18) = 9.224; p < 0.01). Importantly,there was a significant contingency × group interaction (F_(1,18)= 7.356; p < 0.01). Simple effects analysis revealed that, forthe sham group, there was a significant effect of contingencytreatment (F₍₉₎ = 7.026; p < 0.01). As seen in Figure 3, right,these rats performed fewer presses on the lever for which thecontingency had been degraded. However, for the lesion group,there was no difference in response rate on the two levers afterthe contingency treatment (F₍₈₎ = 1.586; p > 0.05).
These results provide additional evidence that electrolytic lesions of the dorsal hippocampus eliminate rats' sensitivityto the selective degradation of the instrumentalcontingency.

Experiment 2

Training
Analysis of the training data revealed that, although the two groups acquired the lever press response in the same numberof days, the lesioned rats responded at a higher rate (M = 39.93;SE = 4.53) at the end of training than did sham rats (M = 26.67;SE = 3.33), and this result was statistically significant (F_(1,17)= 5.853; p < 0.05).

Contingency degradation training
Inspection of Figure 4, left, suggests that, although response rates were numerically higher in the lesioned rats, the twogroups were both sensitive to the contingency manipulation. Analysisof the contingency training data supports this description, revealingno effect of group (F_(1,17) = 2.286; p > 0.05) and no effect ofday (F < 1). There was, however, a significant effect of contingency(F_(1,17) = 10.430; p < 0.01) and a day × contingency interaction(F_(7,119) = 4.940; p < 0.01), suggesting that the contingencyeffect grew larger across days. No other interactions reachedsignificance.

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Figure 4. Mean lever presses per minute across 2 d blocks of contingency degradation training are depicted at left. For each group, one action-outcome contingency had been degraded, whereas the other remained nondegraded. Right, Lever responses for NMDA- and sham-lesioned rats in a two-lever choice extinction test. Error bars represent ±1 SED for the within-subjects variable in each group.

Extinction test
As shown in Figure 4, right, both groups performed fewer responses on the lever for which the contingency had been degraded.Analysis of the extinction test data supports this claim, revealingno effect of group (F < 1), a significant effect of contingency(F_(1,17) = 11.58; p < 0.01), and no group × contingency interaction(F < 1). These data suggest that NMDA lesions of the dorsal hippocampusproduce little if any impairment in rats' sensitivity to the selectivedegradation of one action-outcome contingency. This result contrastsmarkedly with previous findings (Corbit and Balleine, 2000) (experiment1 above), which have shown that electrolytic lesions of the dorsalhippocampus render rats relatively insensitive to contingencydegradation. Given this discrepancy, a more direct comparisonof the effects of these two lesion types in a single experimentwas conducted in experiment3.

Experiment 3

Training
There was no difference between groups in acquisition of the lever press response. At the end of training, the electrolytically(M = 25.30; SE = 5.80) and NMDA (M = 27.27; SE = 4) lesioned ratswere responding at similar rates (F <1).

Contingency degradation training
Figure 5, left, displays the responses for the two groups across days of contingency degradation training. Inspection of thefigure suggests that the electrolytically lesioned rats are insensitiveto the contingency manipulation. In contrast, rats with NMDA lesionsof the hippocampus appear to show normal sensitivity to the contingencydegradation manipulation. Statistical analysis of the trainingdata reveals no effect of group (F < 1) but a significant effectof day (F_(3,51) = 5.23; p < 0.01) and contingency (F_(1,17) = 8.72;p < 0.01) and a day × group interaction (F_(3,51) = 11.51; p <0.01); however, despite the numerical trends, the group × contingencyinteraction failed to reach significance (F_(1,17) = 2.19; p >0.05). No other interactions were significant.

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Figure 5. Mean lever presses per minute for electrolytically and NMDA-lesioned rats after degradation of one action-outcome contingency across days of training (left). Right, Lever-press responses for the two groups in a two-lever choice extinction test. Error bars represent ±1 SED for the within-subjects variable in each group.

Extinction test
The data from the extinction test are displayed in Figure 5, right. As suggested by the figure, the rats with NMDA lesionsperformed fewer responses on the lever for which the contingencyhad been degraded previously relative to the other lever, whereasthe rats with electrolytic lesions responded similarly on thetwo levers. This description is supported by the statistical analysis,which revealed no effect of group (F < 1), a marginal effect ofcontingency (F_(1,17) = 3.91; p = 0.06), but importantly a group× contingency interaction (F_(1,17) = 5.93; p < 0.05). Subsequentanalysis revealed a contingency effect in the NMDA group but noeffect in the electrolytic group. These results confirm that electrolyticand NMDA lesions of the dorsal hippocampus produce different effectswith regard to sensitivity to degradation of the instrumentalcontingency, with electrolytic lesions producing a deficit andNMDA lesions having no apparent effect. Given this difference,it is important to more fully characterize the impact of NMDAlesions on instrumental learning, so the rats were next testedin an outcome devaluation procedure. Electrolytic lesions havebeen shown previously to have no effect on this form of learning(Corbit and Balleine, 2000); however, the possibility remainsthat NMDA lesions may produce differenteffects.

Outcome devaluation
The results of the devaluation test are illustrated in Figure 6. As suggested by this figure, both the electrolytically andNMDA-lesioned groups were sensitive to outcome devaluation andto a similar degree, with both groups performing fewer responseson the lever for which the previously earned outcome had beendevalued. Statistical analysis confirms this suggestion, revealinga significant effect of devaluation (F_(1,17) = 4.763; p < 0.05).Although the figure suggests a numerically smaller effect in theNMDA rats, there was no effect of group (F < 1) and no devaluation× group interaction (F < 1). These results replicate the previousfinding that electrolytic hippocampal lesions have no effect onsensitivity to outcome devaluation and extend this result to NMDAlesions of the hippocampus.

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Figure 6. Mean lever presses per minute for electrolytically and NMDA-lesioned rats in a two-lever choice extinction test after devaluation of one instrumental outcome. Error bars represent ±1 SED for the within-subjects variable in each group.

Experiment 4

Training
Analysis of the training data revealed that, although the two groups acquired the lever press response in the same numberof days, the retrohippocampal rats responded at a higher rate(M = 31.17; SE = 2.07) at the end of training than the sham ratsdid (M = 21.57; SE = 2.2; F_(1,19) = 9.805; p < 0.01). Two shamrats failed to acquire the instrumental response and were excludedfrom the experiment (n =9).

Contingency degradation training
Two rats, one from the sham and one from the lesion group, were excluded from analysis of the contingency degradation becauseof equipment failure. The results from the remaining subjects(sham, n = 8; retrohippocampal, n = 11) are illustrated in Figure7, left. Inspection of Figure 7 suggests that, in general, theperformance of the sham rats was sensitive to the contingencymanipulation. In contrast, the retrohippocampal group respondedat generally higher rates and displayed no sensitivity to thecontingency manipulation, maintaining similar response rates onthe two levers. Confirming this description, the statistical analysisof the contingency training data revealed a significant main effectof contingency in the sham group (F_(1,17) = 3.33; p < 0.05) butno effect of contingency in the retrohippocampal group (F < 1),which, if anything, appeared to respond more on the lever withthe degraded contingency than on the other lever.

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Figure 7. Mean lever presses per minute across 3 d blocks for the sham and retrohippocampal lesioned rats after degradation of one action-outcome contingency across days of training (left). Right, Data from a two-lever choice extinction test. Error bars represent ±1 SED for the within-subjects variable in each group.

Extinction test
The test data displayed in Figure 7, right, suggest that the two groups performed very differently in the extinction test.Sham rats seemed to be sensitive to the contingency manipulation.The retrohippocampal rats, however, responded similarly on thetwo levers. The statistical analyses were conducted using orthogonalplanned comparisons derived from the pattern of results observedduring the contingency training phase. These tests established,first, that no contingency effect emerged in the retrohippocampalgroup; degradation of the instrumental contingency failed to influenceperformance, and responding was similar on the two levers (t₍₁₇₎= 0.45; p > 0.05). In contrast, the sham group was clearly sensitiveto degradation of the contingency; thus, although performancedid not differ from the retrohippocampal group on the nondegradedaction (t₍₁₇₎ = 0.70; p > 0.05), the responding of the sham ratswas reduced selectively and reliably on the lever the response-outcomecontingency of which was degraded relative to both the retrohippocampalgroup and to responding on the nondegraded lever (t₍₁₇₎ = 2.58;p < 0.05). This pattern of results provides clear evidence thatthe sham but not the retrohippocampus-lesioned rats were sensitiveto degradation of the instrumental contingency, an effect thatemerged both during training and in the extinctiontest.

Devaluation extinction test
Although the retrohippocampal rats were not sensitive to the contingency degradation, both they and the sham rats displayedsensitivity to outcome devaluation by responding less on the leverthat had previously earned the now devalued outcome (lesion, M= 36, SE = 17; sham, M = 12, SE = 4) relative to responding onthe other lever (lesion, M = 182, SE = 37; sham, M = 49, SE =16). Statistical analysis revealed a significant effect of group(F_(1,19) = 9.48; p < 0.01), with retrohippocampal rats performingmore responses overall. In addition, there was a significant effectof devaluation (F_(1,19) = 14.75; p < 0.01). Although there appearsto be a numerically smaller effect in the sham group, there wasno devaluation × group interaction (F_(1,19) = 2.59; p > 0.05).This result is important, because to perform accurately on thistest, rats must be able to discriminate between the two actionsand between the two outcomes. The selective performance of theretrohippocampal rats on this test means that neither a failureto discriminate between the two actions nor between the two outcomescan explain their lack of sensitivity to selective degradationof the instrumental contingency describedabove.

Experiment 5

Training
No reliable difference in the rate of acquisition of the lever press response was observed between groups. In addition, bythe final day of instrumental training, the unilateral sham (M= 26.9; SE = 3.17), subicular (M = 31.17; SE = 3.70), and entorhinal(M = 27.87; SE = 4.5) groups showed no difference in rate of responding(F <1).

Contingency degradation training
Figure 8, left, shows the effects of contingency degradation across days of training. As the figure suggests, both unilateraland subiculum-lesioned rats showed sensitivity to the degradationof the instrumental contingency. In contrast, rats with entorhinallesions responded similarly on both levers, indicating that theywere insensitive to the contingency manipulation. Statisticalanalysis of the degradation training data revealed no effect ofgroup (F_(2,27) = 1.11; p > 0.05), a significant main effect ofcontingency (F_(1,27) = 7.32; p < 0.05), and a group × contingencyinteraction (F_(2,27) = 4.18; p < 0.05). Additional analysis ofthis interaction revealed a significant simple effect of contingencyin the unilateral sham group (F_(1,9) = 8.51; p < 0.05) and thesubicular group (F_(1,9) = 5.14; p < 0.05) but not in the entorhinalgroup (F_(1,9) = 1.05; p > 0.05).

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Figure 8. Mean lever presses per minute for the entorhinal (top), subiculum (center), and unilateral sham (bottom) lesioned rats after degradation of one action-outcome contingency across days of training (left). Right, Data from a two-lever choice extinction test. Error bars represent ±1 SED for the within-subjects variable in each group.

Extinction test
Inspection of Figure 8, right, shows that, when tested in extinction, both the unilateral sham and subicular groups respondedless on the lever for which the contingency had been degraded,whereas the entorhinal group responded similarly on the two levers.This pattern suggests that the sham and subicular groups but notthe entorhinal group were sensitive to the contingency manipulation.Analyses of the extinction data revealed a significant effectof contingency in the sham (F_(1,9) = 10.94; p < 0.01) and subicular(F_(1,9) = 5.26; p < 0.05) groups but not in the entorhinal group(F < 1). These results support the claim that the entorhinal cortexbut not the subiculum is essential for the detection of instrumentalcontingency and relate the deficit found after electrolytic lesionsof the dorsal hippocampus (experiments 1 and 3) directly to thatobtained with neurotoxic lesions of the retrohippocampal complex(experiment4).

  DISCUSSION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The aim of this study was to characterize further the role of the dorsal hippocampus in instrumental conditioning. Specifically,we sought to replicate the previous finding that electrolyticlesions of the dorsal hippocampus render rats insensitive to theselective degradation of the instrumental action-outcome contingencyand to extend this finding by investigating the effects of NMDAlesions of the dorsal hippocampus and of the retrohippocampalregion (i.e., entorhinal cortex and subiculum). Finally, a disconnectionprocedure was used to determine more precisely the relative involvementof the entorhinal cortex and subiculum in the detection of changesin the instrumental contingency and to assess whether the deficitsobserved after cell body lesions of these structures could accountfor the deficits observed after electrolytic lesions of the dorsalhippocampus.

The results of experiments 1 and 3 confirmed our original observations that electrolytic hippocampal lesions have no effecton the acquisition of instrumental performance but reduce thesensitivity of rats to the selective degradation of the instrumentalcontingency. Although these results tend to support the suggestionof Devenport and colleagues (Devenport, 1979; Devenport and Holloway,1980) that the hippocampus is critical for the detection of thecausal relationship between an action and outcome, this conclusionis challenged by the results of experiments 2 and 3, which demonstratedthat animals with NMDA lesions of the hippocampus were as sensitiveas sham-lesioned controls to contingency degradation. As a consequence,these results suggest that the original deficit observed afterelectrolytic lesions is more likely the result of damage to fiberspassing through the region of thelesion.

In our previous analysis (Corbit and Balleine, 2000), we suggested that the deficit in contingency sensitivity induced byelectrolytic lesions of the dorsal hippocampus was produced bya reduction in the ability of lesioned animals to calculate thebackground rate of reinforcement, i.e., the rate of reinforcementin the absence of an action. It is now widely accepted that thereduction in instrumental performance induced by noncontingentoutcome delivery is the product of a reduction in the relativevalidity of the instrumental action compared with the backgroundor context as a predictor of reward (Wagner et al., 1968; Dickinsonand Charnock, 1985; Colwill and Rescorla, 1986). As such, andon the basis of reports suggesting that hippocampal lesions inducedeficits in context conditioning (Honey and Good, 1993; Marenand Fanselow, 1997), we were led to the suggestion that the failureof hippocampal rats to adjust to degradation of the instrumentalcontingency was secondary to a deficit in context conditioning.Although we remain convinced that the deficit in contingency degradationobserved after electrolytic lesions reflects a deficit in contextconditioning, particularly given our repeated failure to findany lesion-induced deficit in outcome devaluation (Corbit andBalleine, 2000), the failure of excitotoxic lesions to replicatethis effect suggests that structures outside the dorsal hippocampusare more critically involved in thistask.

It is known that NMDA-induced lesions differ from electrolytic lesions in that, although both kill cells in the region ofthe lesion, the latter also damages axonal fibers of passage (Jarrard,1993, 1995). It is possible, therefore, that the effects of electrolyticlesions of the dorsal hippocampus in our studies reflect damageto axons from a distal structure involved more directly in contextconditioning in this task. There are, in fact, several recentreports that context conditioning is not meditated solely by thehippocampus. For example, in fear conditioning, lesions or inactivationof the major cortical inputs to the hippocampus, including theperirhinal, postrhinal, and entorhinal cortices, produce deficitsin freezing conditioned to contextual cues (Corodimas and LeDoux,1995; Maren and Fanselow, 1997; Sacchetti et al., 1999; Bucciet al., 2000) (but see Phillips and LeDoux, 1995; Bannerman etal., 2001). In addition, lesions of the subiculum, the major sourceof subcortical output from the hippocampus, disrupt contextualfear conditioning (Maren, 1999). The involvement of these structuresin contextual learning suggests that they may play a role in thedetection of changes to the instrumentalcontingency.

Of those areas implicated in contextual learning, striatal projections from the entorhinal cortex (Totterdell and Meredith,1997) and subiculum (Groenewegen et al., 1987) travel throughthe alveus, a pathway adjacent to the dorsal hippocampus, beforeentering the fornix. It is likely, therefore, that the electrolytichippocampal lesions in experiments 1 and 3 disrupted this pathway,disconnecting circuits originating in the retrohippocampalregion.

In experiment 4, combined entorhinal and subicular lesions (i.e., retrohippocampal lesions) were found to render animals insensitiveto a change in the instrumental contingency. Furthermore, retrohippocampalrats showed normal sensitivity to selective outcome devaluation,a finding that indicates that the deficit in contingency degradationwas not secondary to any failure to discriminate between eitherthe outcomes or the two actions. Importantly, this is exactlythe pattern of deficits that was observed after electrolytic lesionsof the dorsal hippocampus (Corbit and Balleine, 2000).

The results of experiment 4 suggest, therefore, that the retrohippocampus is involved in the ability of rats to encode thecontingency between actions and their consequences. Nevertheless,these results do not allow us to determine the relative involvementof the entorhinal cortex and subiculum in this effect. In addition,the results of experiment 4, although suggestive, do not establishdefinitively that electrolytic lesions of the hippocampus causetheir effects by disrupting a pathway arising in the retrohippocampus.A disconnection procedure was used in experiment 5 to identifymore clearly the structures involved in the detection of instrumentalcontingency and to relate the effect of NMDA lesions of the entorhinalcortex and subiculum to the deficits observed after electrolyticlesions of the dorsalhippocampus.

Subjects in experiment 5 all received unilateral electrolytic lesions of the dorsal hippocampus and either sham surgery orNMDA lesions of either the contralateral entorhinal cortex orthe subiculum. Although these groups were indistinguishable duringthe instrumental training phase, only the unilateral sham andsubicular groups showed normal sensitivity to the selective degradationof the instrumental contingency. In contrast, the entorhinal groupwas insensitive to contingency degradation, performing similarlyon both levers throughout contingency training and in the extinctiontest. These results suggest not only that the entorhinal cortexis involved selectively in detecting changes in the contingencybetween actions and outcomes, but also that the disruption offibers originating in this structure can account for the effectsobserved after electrolytic lesions of the dorsalhippocampus.

Although it remains a possibility, as some authors have suggested, that the hippocampus plays a role in contextual discriminationboth in the free-operant situation (Freeman et al., 1996) andin response selection in certain tasks (Wise and Murray, 1999),as it stands, these data argue against a direct role for the dorsalhippocampus either in the formation of response-reward associationsor in the encoding of the causal relationship between an actionand its specific consequences in our instrumental conditioningtasks. Rather, the current experiments suggest that the deficitsin the detection of changes in the instrumental contingency thatwe reported previously after electrolytic lesions were most likelythe result of damage to efferents of the entorhinal cortex. Itshould be noted, however, that the effects of lesions of the ventralhippocampus have not been examined and that the role of this structureremainsunknown.

In summary, although electrolytic hippocampal lesions rendered animals relatively insensitive to changes in the instrumentalcontingency, this deficit did not appear to depend on the integrityof cell bodies within the dorsal hippocampus, because neurotoxichippocampal lesions produced no detectable deficit. The possibilitythat the original deficit was secondary to damage to fibers ofpassage rather than damage to the hippocampus itself was exploredby examining the effects of lesions of the retrohippocampal region.These lesions were found to produce a deficit similar to thatobserved after electrolytic hippocampal lesions with rats failingto adjust their responding after degradation of the action-outcomecontingency. Finally, the deficit observed after NMDA lesionsof the entorhinal cortex and electrolytic lesions of contralateraldorsal hippocampus supports the claim that it is a circuit originatingin the entorhinal cortex and passing through the alveus that iscritical for the detection of changes to the instrumentalcontingency.

  FOOTNOTES

Received June 27; revised Sept. 26; accepted Oct.1.

This work was supported by National Institute of Mental Health Grant MH 56446 (B.W.B.). We thank Sandra Cetl and Chris Park,who assisted with datacollection.

Correspondence should be addressed to Laura Corbit, Department of Psychology, University of California, Los Angeles, Box 951563,Los Angeles, CA 90095. E-mail: corbit{at}ucla.edu.

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MATERIALS AND METHODS
RESULTS
DISCUSSION
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