Parallel Information Processing in the Dorsal Striatum: Relation to Hippocampal Function

QUICK SEARCH:

[advanced]

	Author:		Keyword(s):
Year:		Vol:		Page:

HOME | SEARCH | ARCHIVE | SUBSCRIBE | CONTACT | HELP

This Article

Abstract

Full Text (PDF)

Submit an eLetter

Alert me when this article is cited

Alert me when eLetters are posted

Alert me if a correction is posted

Citation Map

Services

Email this article to a friend

Similar articles in this journal

Similar articles in ISI Web of Science

Similar articles in PubMed

Alert me to new issues of the journal

Download to citation manager

Citing Articles

Citing Articles via HighWire

Citing Articles via ISI Web of Science (111)

Citing Articles via Google Scholar

Google Scholar

Articles by Devan, B. D.

Articles by White, N. M.

Search for Related Content

PubMed

PubMed Citation

Articles by Devan, B. D.

Articles by White, N. M.

Previous Article  |  Next Article

The Journal of Neuroscience, April 1, 1999, 19(7):2789-2798

Parallel Information Processing in the Dorsal Striatum: Relation to Hippocampal Function
Bryan D. Devan and Norman M. White
Department of Psychology, McGill University, Montreal, Quebec, Canada H3A 1B1

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
REFERENCES

We investigated the effects of localized medial and lateral CPu lesions and fornix/fimbria lesions on responses to a localcue and to behavior based on cognitive-spatial information inthe water maze. Rats were trained concurrently on the cue (visibleplatform) and spatial (submerged platform) components of the task,followed by a test in which responses to the two types of informationwere dissociated by a measure of competing response tendencies.Bilateral lesions of lateral CPu did not affect acquisition ofeither cue or spatial responding but produced a preference forthe spatial response on the competition test. Bilateral lesionsof the medial CPu retarded but did not prevent learning both componentsand produced a preference for the cue response on the competitiontest. The latter effect was accompanied by increased thigmotaxis(swimming in the periphery of the pool), primarily during theearly acquisition trials, which was attributed to an impairedability to respond to learned spatial information. Fornix/fimbrialesions prevented spatial but not cue learning and produced apreference for the cue response on the competition test. Asymmetriclesions (unilateral hippocampus and contralateral medial CPu)produced mild retardation of acquisition of both the cue and spatialtasks and a preference for the cue response on the competitiontest. These findings dissociate the functions of the lateral andmedial CPu and suggest that the hippocampus and medial CPu maybe parts of a system that promotes responding based on learnedcognitive-spatial information, particularly in competitive cue-placeresponsesituations.

Key words: dorsal striatum; medial CPu; lateral CPu; fornix/fimbria; hippocampal-striatal interactions; water maze; cue/place learning; competition test; asymmetric lesion; functional limbic circuit

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
REFERENCES

Studies of mnemonic function in rats frequently employ spatial or "place" cues to test cognitive forms of learning (Tolman,1948; O'Keefe and Nadel, 1978) and discrete cues to measure habitor stimulus-response (S-R) learning (Thorndike, 1911, 1933; Hull,1943). Evidence suggests that different neural systems contributeto each form of learning (Milner et al., 1968; Hirsh, 1974; O'Keefeand Nadel, 1978). Lesions of the dorsal striatum (caudate putamen;CPu) and hippocampus or fornix/fimbria were previously shown tohave opposite effects on behavior in cued and spatial versionsof the radial maze task (Packard et al., 1989; McDonald and White,1993). These findings are consistent with the hypothesis thata corticostriatal system mediates S-R habit formation, whereasa hippocampus-based system contributes to cognitive-spatial learning(Mishkin et al., 1984; Mishkin and Petri, 1984; Petri and Mishkin,1994).

Anatomical studies have shown that the dorsal striatum is a heterogeneous structure, both in terms of its intrinsic compartmentalizationof neurochemical constituents (Graybiel, 1990; Groves et al.,1995) and its regionally diverse connectivity with other cortical/subcorticalstructures (Alexander et al., 1986; McGeorge and Faull, 1989;Groenewegen et al., 1990). Behavioral studies further suggestthat the striatum is functionally differentiated (Winocur, 1974;Divac et al., 1978; Dunnett and Iversen, 1981, 1982a,b; Iversen,1984; Viaud and White, 1989; Pisa and Cyr, 1990; Reading et al.,1991; Hauber and Schmidt, 1993, 1994; Fricker et al., 1996). Lesionsof the lateral CPu disrupt sensorimotor function and S-R learning(Dunnett and Iversen, 1981, 1982a; White, 1989, 1997; Readinget al., 1991), whereas lesions of the medial CPu have been reportedto produce impairments on cognitive-spatial tasks (Whishaw etal., 1987; Columbo et al., 1989; Devan et al., 1996; Furtado andMazurek, 1996).

In the water maze, rats' ability to learn the location of a hidden (submerged) platform, a cognitive-spatial task, is impairedby fornix/fimbria (Sutherland and Rodriguez, 1989; Devan et al.,1996) or hippocampal (Morris et al., 1982; Sutherland et al.,1983) lesions, whereas acquiring the response of swimming directlyto a visible platform, an instance of S-R learning, is impairedby lateral CPu lesions (McDonald and White, 1994). Because lesionsconfined to the medial CPu impaired responses based on place cues(Devan et al., 1999), we compared the effects of separate medialand lateral CPu lesions with fornix/fimbria lesions on a combinedcue-place learning task in the water maze (McDonald and White,1994).

In the second experiment, we studied the relationship of the medial CPu to the hippocampus in the same water maze task usingasymmetric lesions consisting of damage to the hippocampus onone side of the brain and damage to the medial CPu on the otherside. This lesion preparation has been used to define routes ofserial information processing between other brain structures (Mishkin,1958, 1966; Horel and Keating, 1969, 1972; Olton, 1978; Gaffanand Harrison, 1987; Gaffan et al., 1988, 1989; Everitt et al.,1991; Sutherland and Hoesing, 1993; Gaffan and Parker, 1996; Florescoet al., 1997; Han et al., 1997).

  MATERIALS AND METHODS

Subjects. Ninety Long-Evans hooded rats weighing ~300-400 gm at the time of surgery were used. They were housed individuallyin hanging wire-mesh cages located in a temperature-controlledroom on a constant 12 hr light/dark cycle. All behavioral testingwas conducted during the light phase at approximately the sametime each day. Ad libitum food (Purina lab chow) and tap waterwere available in the home cage throughout theexperiments.

Experimental conditions. In experiment 1, rats were assigned to four bilateral lesion groups: lateral CPu (n = 15), medialCPu (n = 11), fornix/fimbria (n = 10), and a group of sham-operatedcontrols (n = 10). In experiment 2, rats were assigned to twounilateral lesion groups: medial CPu (n = 10) or hippocampus (n= 10), or to the asymmetric lesion condition (unilateral hippocampus-contralateralmedial CPu) (n = 12). There were also 12 sham-operatedcontrols.

Surgery. Each rat was handled for ~5 min/d for 3 d before surgery. All rats were given Xylazine analgesia (5 mg/kg, i.m.)and anesthetized with sodium pentobarbital (60 mg/kg, i.p.). Brainlesions were made using standard stereotaxic procedures. Flatskull stereotaxic coordinates were derived from the atlas of Paxinosand Watson (1986) using bregma of the skull surface as the referencepoint. The coordinates for dorsomedial CPu lesions were 0.7 mmanterior (A), 2.4 mm lateral (L), and 5.4 mm ventral (V). Thecoordinates for dorsolateral CPu lesions were 0.7 A, 3.4 L, and5.4 V. Coordinates for fornix/fimbria lesions were 1.5 mm posterior(P), 0.8 and 2.2 L, and 4.5 V. The hippocampus was damaged usingfour separate lesions at the following coordinates: (1) 3.8 P,2.0 L, 4.0 V; (2) 5.3 P, 3.5 L, 4.0 V; (3) 5.8 P, 5.0 L, 5.5 V;and (4) 5.8 P, 5.0 L, 7.5V.

CPu and hippocampus lesions were made by passing 3 mA of direct anodal current for 15 sec through an insulated nichrome electrodeexposed 0.8 mm at the tip. Fornix/fimbria lesions were made byradio frequency current (6 mA for 40 sec). The side of the unilaterallesions was counterbalanced within the appropriate groups. Shamanimals received identical surgical treatment to the lesionedanimals except that no electrode was lowered into the brain. Behavioraltesting began 2 weeks aftersurgery.

Apparatus. A white swimming pool measuring 172 cm in diameter and 63 cm in height was used. The pool was elevated 20 cm abovethe floor in a room that contained many stationary cues, includingwall posters, book shelves, and a computer rack. The pool wasfilled to a depth of 38 cm with 22°C water, made opaque by theaddition of 100 ml white nontoxic tempera paint before daily swimmingtrials.

Two platforms were used. The visible platform, used on cued trials, was constructed of wood (top surface, 12 × 12 cm). Blackand white terry cloth strips were permanently attached to thesides and top surface. The visible platform protruded 3 cm abovethe surface of the water when placed in the pool. The hidden platform,used on place trials, was constructed of Plexiglas with whiteterry cloth attached to the top surface (10 × 10 cm). The topof the hidden platform was submerged 1.5 cm below the surfaceof thewater.

A video camera mounted above the pool was used to make recordings of swim trials. The recordings were used to measure escapelatencies and peripheral pool time using a stopwatch.

Procedure. The cue-place water maze task was adapted from McDonald and White (1994). On the first 2 d of the experiment, therats were trained to swim to the visible platform located in thecenter of the northwest quadrant of the pool. Each daily trainingsession consisted of four trials on which each rat was releasedonce from each of the four start points. A trial began by placinga rat in the pool (facing the wall) at a randomly selected startposition and ended when the rat climbed onto the visible platform,or after 30 sec had elapsed. If the rat had not escaped after30 sec, it was gently guided to the platform by hand. Each ratwas left on the platform for 5 sec and then returned to its homecage, located in an adjoining room. For each rat there was a delayof 10-15 min between successive trials within a daily session.During the delay, the remaining rats in the counterbalanced squadwere run on the same trial. Thus, the intertrial interval variedslightly according to the rats' level of performance but was approximatelyequal for all rats within each trainingsession.

On the day after the first 2 d of training with the visible platform (eight trials), each rat received a four-trial sessionin which the visible platform was replaced with the submergedplatform at the same location. Identical training procedures wereused during these hidden platformtrials.

Subsequently, the 3 d sequence of two visible platform sessions followed by a hidden platform session was repeated two moretimes for a total of 36 trials (24 visible, 12 hidden) over atotal of 9 d. Escape latency (time to reach the available platform)and peripheral pool time (time spent swimming within 20 cm ofthe edge of the pool) were measured on these acquisitiontrials.

On day 10, the competition test was given. The visible platform was moved to the center of the southeast quadrant (oppositeto its location during the acquisition trials). Two trials weregiven from start positions equidistant to the center of the northwestand southeast quadrants. The video recordings were used to determinewhether the rats swam within 5 cm of the perimeter of the formerplatform location in the northwest quadrant before escaping tothe visible platform, now located in the southeastquadrant.

Histology. After behavioral testing, the rats were deeply anesthetized with an intraperitoneal injection of 1 ml of 30% chloralhydrate and perfused intracardially with 0.9% saline followedby 10% formol saline. The brains were removed from the skullsand stored in 10% formol saline for at least 1 week. Frozen coronalsections were cut at 30 µm through the lesion area, and everyfifth section was mounted on glass microscope slides. The mountedsections were stained with formol thionin (Donovick, 1974) andexamined with amicroscope.

Statistical analyses. Two-way mixed ANOVAs with lesion type as the between-groups factor and trial block as the repeated-measuresfactor (with conservative dfs) were computed for the escape latencyand peripheral pool time (thigmotaxis) measures of acquisitionperformance. Separate analyses were conducted for trial blockswith the visible and hidden platform. Significant interactionswere followed up by one-way ANOVAs of the group factor at eachlevel of the repeated-measures factor. This procedure is consideredto be a conservative way to test simple main effects involvingoverall sources with different error terms (Olson, 1988, p. 723).If a one-way ANOVA yielded significance then Scheffe's methodwas used to determine specific group differences. One-way ANOVAfollowed by Scheffe's post hoc test of lesion type were used toanalyze latency and thigmotaxis scores on the competition test.In addition, likelihood ratio and Pearson's $chi$ ² analyses of lesion type were conducted for the response categorymeasure.

  RESULTS

Experiment 1: bilateral lesions of CPu subregions and fornix/fimbria

Histology
The minimal and maximal extent of damage to the structures lesioned in each group is shown in Figure 1. The dorsolateral CPulesion primarily damaged the region of CPu underlying the corpuscallosum and bordering the external capsule. At a posterior level,this lesion spared the more lateral portion of CPu adjacent tothe external capsule. One animal in the dorsolateral CPu groupsustained extensive damage to the medial CPu and lateral septum;data from this animal were not included in the final statisticalanalyses. The dorsomedial lesion was localized to the portionof CPu underlying the corpus callosum and bordering the lateralventricles. This lesion did not produce any observable damageto the choroid plexus within the ventricles or to the lateralseptum. The lesion also spared the nucleus accumbens anteriorlyand ventromedial portions of CPu posteriorly.

View larger version (37K):
[in this window]
[in a new window]
Figure 1. Minimum (dark hatching) and maximum (light hatching) extent of damage to the fornix/fimbria, lateral CPu, and medial CPu.

Fornix/fimbria lesions included damage to the medial and lateral portions of the structure. Sparing of the lateral-ventraltips was observed in some cases. Occasional damage was observedin the triangular septal nucleus and dorsal hippocampus, alongwith minimal electrode tract damage to overlyingcortex.

Cue-place acquisition
Figure 2 shows the escape latency data for each group. All groups learned to swim to the visible platform (connected symbols).However, rats with medial CPu lesions had longer latencies onthe early trials. A two-way mixed ANOVA revealed a significantinteraction between factors (F_(3,41) = 2.89; p < 0.05) as wellas significant main effects of group (F_(3,41) = 4.93; p < 0.01)and trial block (F_(1,41) = 202.51; p < 0.001). Post hoc testsrevealed a significant difference between the medial CPu and shamgroup on trial block 2 (p < 0.01). No other group differenceswere significant.

View larger version (25K):
[in this window]
[in a new window]
Figure 2. Mean escape latencies for each group in experiment 1. Connected symbols represent visible platform trial blocks (days 1-2, 4-5, and 7-8; four trials per block). Disconnected symbols represent hidden platform trial blocks (days 3, 6, and 9; four trials per block) and the competition test (day 10; two trials per block).

Mean escape latencies on the hidden platform trials are also shown in Figure 2 (days 3, 6, and 9). Rats with medial CPu lesionstook longer than sham-lesioned rats to escape on the first hiddenplatform session. In contrast, rats with fornix/fimbria lesionstook longer than shams to escape on the last hidden platform session.Analyses of the escape latency data for hidden platform trialsshowed a significant group by trial block interaction (F_(3,41)= 3.30; p < 0.05) as well as significant main effects of group(F_(3,41) = 3.79; p < 0.01) and trial block (F_(1,41) = 27.09; p< 0.001). Post hoc tests showed that the medial CPu group differedsignificantly from both the sham and lateral groups on trial block3 (p values < 0.05), whereas the fornix/fimbria group differedsignificantly from the sham and lateral CPu groups on trial block9 (p values < 0.01). Hence, lesions of the medial CPu retardedbut did not prevent place learning, whereas lesions of the fornix/fimbriablocked placelearning.
Figure 3 shows the mean percentage of time spent in the peripheral part of the pool (thigmotaxis) for each group. Rats withmedial CPu lesions tended to be more thigmotactic than the othergroups. A two-way mixed ANOVA on the visible platform means revealeda significant group by trial block interaction (F_(3,41) = 2.79;p < 0.01) as well as significant main effects of group (F_(3,41)= 8.34; p < 0.001) and trial block (F_(1,41) = 92.61; p < 0.0001).Post hoc tests showed significant differences between the medialCPu and all other groups (sham: blocks 1, 2 and 7, p values <0.05; lateral CPu: block 5, p < 0.05; fornix/fimbria: blocks 7and 8, p < 0.005). Analyses of the hidden platform means revealeda significant group by trial block interaction (F_(3,41) = 4.60;p > 0.05) in addition to significant main effects of group (F_(3,41)= 4.78; p < 0.01) and trial block (F_(1,41) = 52.70; p < 0.001).Post hoc tests showed significant differences between the medialCPu and all other groups on trial block 3 (p values < 0.05) butno group differences on trial blocks 6 or 9 (p values > 0.10).Thus, the rats with medial CPu lesions showed a greater tendencythan the rats in the other groups to swim in the peripheral partof the pool on the early trials.

View larger version (28K):
[in this window]
[in a new window]
Figure 3. Mean percentage of swim time spent in the peripheral portion of the pool for each group in experiment 1. Connected symbols represent visible platform trial blocks (days 1-2, 4-5, and 7-8; four trials per block). Disconnected symbols represent hidden platform trial blocks (days 3, 6, and 9; four trials per block) and the competition test (day 10; two trials per block).

Competition test
The mean escape latencies for each group on the competition test are shown in Figure 2 (day 10). Rats with fornix and medialCPu lesions escaped faster than controls and rats with lateralCPu lesions. A one-way ANOVA on the mean latencies averaged acrossthe two competition test trials revealed a significant group effect(F_(3,41) = 12.38; p < 0.001). Post hoc tests showed that the fornixand medial CPu groups had significantly longer latencies thanthe sham and lateral CPu groups (p values < 0.01).
The mean percentage of time spent in the peripheral part of the pool on the competition test is shown in Figure 3 (day 10).Rats with medial CPu lesions were more thigmotactic than the othergroups. A one-way ANOVA revealed a significant group effect (F_(3,41)= 12.38; p < 0.001). Post hoc tests showed that the medial CPugroup differed significantly from the sham, lateral CPu, and fornixgroups (p values < 0.05).
The rats' responses on the competition test were categorized as cue or place by examining the swim paths. If an animal swamfrom the start point to within 5 cm of the perimeter of the formerplatform location in the northwest quadrant before escaping tothe visible platform in the southeast quadrant on either competitiontest trial, it was labeled a place responder. If an animal didnot meet this criterion, it was labeled a cue responder. The numberof place and cue responders in each group is shown in Table 1.Compared to controls, the lateral CPu group showed a significantplace-response bias ( $chi$ ² = 3.89; p < 0.05), whereas both the fornix and medial CPu groupsshowed significant cue-response biases ( $chi$ ² = 5.93, p < 0.05; $chi$ ² = 9.24, p < 0.01, respectively). Additional tests revealed thatthe lateral CPu group differed significantly from both the fornix( $chi$ ² = 16.47; p < 0.0001) and medial CPu groups ( $chi$ ² = 21.27; p < 0.0001) but that the fornix and medial CPu groupsdid not differ significantly from each other ( $chi$ ² = 1.15; p > 0.20).


View this table:
[in this window]
[in a new window]
Table 1. Number of rats that swam to the former platform location (place responders) versus the new visible platform position (cue responders) on the competition test (day 10)

Figure 4 shows some representative swim paths of individual rats categorized as cue or place responders on the competitiontest. Escape latencies corresponding to each path are also shown.The differences in these latencies across response categories(cue or place) in the lesioned rats were minimal (Fig. 4: A vsB and C vs D) and not reliably predictable from response category(Fig. 4: E vs F). Hence, while latency provides an indicationof the rats' progress in acquiring the tasks early in training,it does not accurately reveal which of the two response tendenciespredominate in a given rat, as revealed by the competition test.

View larger version (23K):
[in this window]
[in a new window]
Figure 4. Representative swim paths of cue and place responders on the first trial of the competition test. The visible platform is in the bottom left quadrant, and the location of the platform during the preceding training trials is in the top right quadrant. Escape latencies for the trials illustrated are shown in each case. The rats with medial caudate putamen lesions (A, C) did not cross the former platform location, whereas the rats with lateral caudate putamen lesions (B, D) did. Differences between escape latencies (A, B and C, D) were small (1.7 and 1.3 sec, respectively). As illustrated in E and F, the escape latencies of control rats classified as cue responders were not necessarily shorter than those classified as place responders, even if the distance they had to swim was shorter.

Summary and discussion
The results of this experiment reveal a dissociation between the effects of medial and lateral CPu lesions on the combinedcue-place task in the water maze. Lateral CPu lesions did notaffect acquisition rate but produced a significant place-responsebias on the competition test. This finding is consistent withthe results of a previous study (McDonald and White, 1994) andwith the hypothesis that lesions of the lateral CPu impair learnedresponding to local cues (i.e., S-Rlearning).
As shown both in the present study and by McDonald and White (1994), the deficit in responding to the local cue revealed bythe rats' responses on the competition test is not reflected intheir latencies on the cued training trials. Moreover, the strengthof the competition test finding may be influenced by the specifictraining parameters used. In a previous study (Devan et al., 1999),rats with lateral CPu lesions exhibited a weaker place-responsebias and a more subtle cue deficit than those in the present study.However, the rats in the previous study were fully trained onthe place response before receiving any cue training whereas inthe present study, and in the one by McDonald and White (1994),cue and place training were given concurrently. The 5 d delayimposed by intervening cue training in the Devan et al. (1999)study may have weakened spatial response tendencies resultingin more cue-directed responses on the competition test, thus maskingthe effect of lateral CPu lesions as presently and previously(McDonald and White, 1994) shown after contemporaneous experiencewith both types oftraining.
In contrast, lesions of the medial CPu increased escape latencies and thigmotaxis during acquisition and produced a cue-responsebias on the competition test. The latter result is consistentwith other reported cue enhancement effects (Mikulas, 1966; Winocur,1980; Mitchell et al., 1985; Mitchell and Hall, 1988; Devan etal., 1996) after CPulesions.
The present observations are consistent with those of previous experiments in showing that thigmotaxis tends to occur duringthe early trials of escape training (Devan et al., 1996, 1999).Devan et al. (1996, 1999) suggested that this form of lesion-inducedthigmotaxis may be caused by a transient deficit in initiatingresponses that move the animal away from the pool wall, towarda location defined by spatial cues. Such a difference could alsobe the source of the cue-response bias of these rats on the competitiontest. Hence, increased thigmotaxis and enhanced cue respondingmay both result from a common underlying cause, i.e., a weakenedtendency to respond to spatialcues.
Lesions of the fornix/fimbria also produced a cue-response bias in the present study, as previously shown by McDonald andWhite (1994). This bias is thought to be a reflection of the failureof rats with these lesions to acquire the cognitive-spatial informationrequired to perform the place response (O'Keefe and Nadel, 1978).
Although lesions of both the medial CPu and fornix/fimbria decreased the rats' tendency to swim to the hidden platform locationon the competition test, they may have done so for different reasons.This suggestion is partly based on differences in the effectsof the two lesions on the acquisition trials. Fornix/fimbria lesionscompletely blocked place learning, whereas medial CPu lesionsproduced only transient increases in escape latencies, accompaniedby thigmotaxis, on early cue and place acquisition trials. Thesefindings are consistent with the hypothesis that the fornix/fimbriadeficit is caused by impaired acquisition of cognitive-spatialinformation and that the medial CPu deficit may be caused by impairedacquisition of responses based on learned spatial information.The latter deficit is most clearly revealed in situations characterizedby competing place- and cue-based responsealternatives.

Experiment 2: unilateral and asymmetric lesions of medial CPu and hippocampus

Histology
The minimal and maximal extent of damage to the structure or structures lesioned in each group is shown in Figure 5. Unilaterallesions of the medial CPu were similar to the bilateral lesionsin the previous experiment. Unilateral lesions of the hippocampusincluded extensive damage to the rostrodorsal and posterior partsof the structure but typically spared the ventral part at thetemporal pole. The dentate gyrus and CA subfields (Ammon's horn)were damaged at both dorsal and posterior sites. In addition,the subiculum (including presubiculum and parasubiculum) was lesionedposteriorly with occasional damage extending more ventrally intothe entorhinal cortex. As shown in Figure 5, lesions in the asymmetricgroup were similar to those in the corresponding unilateral lesiongroups.

View larger version (76K):
[in this window]
[in a new window]
Figure 5. Minimum (dark hatching) and maximum (light hatching) extent of damage to the structures lesioned unilaterally in experiment 2. Although the reconstructions are illustrated within a single hemisphere, the side of lesion was counterbalanced within each group: unilateral-medial CPu, unilateral-hippocampus, and asymmetric (crossed-unilateral) lesion. Plates adapted from Swanson (1992).

Cue-place acquisition
Figure 6 shows the mean escape latencies for each group. All groups learned to swim to the visible platform, however, escapelatencies on these trials were slightly elevated in the asymmetriclesion group (Fig. 6, insets). A two-way mixed ANOVA revealeda significant group by trial block interaction (F_(3,40) = 2.77;p < 0.05), as well as significant main effects of group (F_(3,30)= 12.94; p < 0.0001) and trial block (F_(1,30) = 247.67; p < 0.00001).Post hoc tests revealed that the asymmetric lesion group differedfrom the sham (blocks 2, 4, 5, 7, and 8; p values < 0.05), unilateral-medialCPu (blocks 2, 5, 7, and 8; p values < 0.01), and unilateral-hippocampal(blocks 5, 7, and 8; p values < 0.01) groups. Because the meandifferences were on the order of 1 sec or less on trials blocks5, 7, and 8, the functional implications of these effects maybe of minor importance.

View larger version (31K):
[in this window]
[in a new window]
Figure 6. Mean escape latencies for each group in experiment 2. Connected symbols represent visible platform trial blocks (days 1-2, 4-5, and 7-8; four trials per block). Disconnected symbols represent hidden platform trial blocks (days 3, 6, and 9; four trials per block) and the competition test (day 10; two trials per block). Inset graphs illustrate significant group differences on visible trial blocks on an expanded ordinate: inset 1 (blocks 4 and 5) is expanded 3×; inset 2 (blocks 7 and 8) is expanded 5×.

The asymmetric lesion group also took longer than the shams to find the hidden platform (Fig. 6). A two-way mixed ANOVA revealeda significant effect of group (F_(3,40) = 7.07; p < 0.001) andtrial block (F_(1,40) = 30.99; p < 0.00001) but no significantinteraction between factors (F_(3,40) = 1.76; p > 0.10). Post hoctests revealed that the asymmetric group differed from the shamgroup (p < 0.001) but not from the unilateral-hippocampal or unilateral-medialCPu groups (p values > 0.05).
Figure 7 shows the mean percentage of time spent in the peripheral part of the pool for each group. Rats with asymmetric lesionswere more thigmotactic than controls. A two-way ANOVA on the datafor the visible platform sessions revealed a nonsignificant effectof group (F_(3,40) = 1.66; p > 0.10), a significant effect of trialblock (F_(1,40) = 116.74; p < 0.00001), and a significant groupby trial block interaction (F_(3,40) = 2.33; p < 0.05). Post hoctests showed that the asymmetric group differed significantlyfrom the sham group on trial block 2 (p < 0.05). Analyses of hiddenplatform sessions showed a significant effect of trial block (F_(1,40)= 33.28; p < 0.00001) but no effect of group or interaction betweenfactors (F values < 2.8; p values > 0.05).

View larger version (27K):
[in this window]
[in a new window]
Figure 7. Mean percentage of swim time spent in the peripheral portion of the pool for each group in experiment 2. Connected symbols represent visible platform trial blocks (days 1-2, 4-5, and 7-8; four trials per block). Disconnected symbols represent hidden platform trial blocks (days 3, 6 and 9; four trials per block) and the competition test (day 10; two trials per block).

Competition test
The mean escape latencies for each group on the competition test are shown in Figure 6 (day 10), whereas the mean percentagesof peripheral pool time are shown in Figure 7 (day 10). One-wayANOVAs computed for each measure failed to reveal any significantgroup differences (escape latency, F_(3,40) = 0.94, p > 0.40; peripheralpool time, F_(3,40) = 2.14, p > 0.10).
The number of place and cue responders in each group, defined using the same criteria as in experiment 1, is shown in Table2. The asymmetric lesion group showed a significant cue-responsebias in comparison to controls ( $chi$ ² = 4.44; p < 0.05). In contrast, the unilateral-medial CPu andunilateral-hippocampal groups did not differ from the sham orasymmetric lesion groups (p values > 0.09).


View this table:
[in this window]
[in a new window]
Table 2. Number of rats that swam to the former platform location (place responders) versus the new visible platform position (cue responders) on the competition test (day 10)

Summary and discussion
In this experiment, asymmetric lesions of the hippocampus and medial CPu impaired escape learning on both visible and hiddenplatform trials, increased thigmotaxis (peripheral pool time)on early trials, and produced a significant cue-response biason the competition test. Unilateral lesions of the hippocampusor medial CPu had none of these effects. Hence, these findingsshow a synergistic effect when the two forms of unilateral damagewere combined to produce asymmetriclesions.
On the early acquisition trials, the effects of asymmetric lesions were similar to (but not the same as) those of bilateralmedial CPu lesions in experiment 1; both lesion groups exhibitedincreased escape latencies and increased thigmotaxis, especiallyon the early trials. As already suggested, this pattern of effectsmay be caused by an impaired ability to learn to initiate theappropriate response of swimming to the platform location on thebasis of cognitive-spatialinformation.
On the later acquisition trials, the increased latencies of the asymmetric lesion group resembled those of the fornix/fimbriagroup in experiment 1, although the deficit was not as severein the asymmetric as in the fornix/fimbria group (Figs. 2 and5, compare block 9). Thus, whereas bilateral fornix/fimbria lesionsappeared to prevent learning the location of the hidden platformalmost completely, the asymmetric lesion produced only a partialdeficit of this type. This is consistent with the hypothesis thatmedial CPu lesions do not impair acquisition of the spatial informationrequired to locate the hiddenplatform.
On the competition test, the asymmetric lesioned rats exhibited a clear cue-response bias, resembling both the medial CPuand fornix/fimbria groups in experiment 1. Based on the hypothesizedeffects of the two lesions, this bias may have been caused bydisruption of the flow of information between the two structuresthat is required to initiate a learned response to spatial-cognitiveinformation in the presence of a competing local cue, the visibleplatform.

  DISCUSSION

The results of experiment 1 suggest that the medial and lateral subregions of the CPu are functionally heterogeneous and mayinteract competitively at a behavioral level when inconsistentresponse alternatives are available. The findings also indicatethat under similar behavioral conditions the hippocampal systemmay interact competitively with the lateral CPu and cooperativelywith the medial CPu. In experiment 2, the effects of the asymmetriclesions suggest that this cooperative interaction may be basedon serial information processing within a functional neural circuitthat includes (but is not limited to) both hippocampus and medialCPu.

Previous experiments using different versions of the radial arm maze task (Packard et al., 1989; McDonald and White, 1993,1995) showed that large lesions of the dorsal striatum (includingparts of both medial and lateral subregions) produced differentbehavioral effects from lesions of the fornix/fimbria or hippocampus.It was suggested that the two structures may mediate differentkinds of mnemonic functions that may compete for behavioral expressionin certain situations. A similar conclusion was suggested by theresults of a study of place versus response learning on a crossmaze task (Packard and McGaugh, 1996) involving temporary inactivationof lateral CPu or hippocampus. The present findings are consistentwith this interpretation, but they suggest that it may apply onlyto the lateral CPu. In contrast, the medial CPu subregion of thedorsal striatum may interact cooperatively with the hippocampalsystem, mediating the behavioral expression of certain hippocampus-dependentmnemonicfunctions.

Lesions of the medial CPu have been reported to produce impairments in acquisition and retention of both place and cue tasksin the water maze (Whishaw et al., 1987; Devan et al., 1996).The latter findings cannot be attributed to a selective deficitin cognitive-spatial learning because, as in the present study,cue navigation was also compromised to some extent, and thigmotaxiswas present. The fact that impairments of both place and cue acquisitionafter medial CPu lesions are accompanied by transient increasesin thigmotaxis (as also reported by Devan et al., 1996, 1999)suggests that the behavioral impairment may be related to a deficiencyin learned response initiation, such as that previously shownto occur on simple reaction time tasks after medial but not lateralCPu lesions (Brown and Robbins, 1989; Hauber and Schmidt, 1994).Moreover, as shown in the acquisition trials of the present experiment,rats with medial CPu lesions can acquire information about spatial/placecues and express such information when it provides the only possiblesolution to a task. This spared function may be mediated by allocorticaland/or neocortical output to the pyramidal motor system. As shownin the competition test, however, when an alternative solutioninvolving local cues is available, rats with medial CPu damagetend to respond to those cues rather than to the cognitive-spatialinformation they have acquired (see also, Whishaw et al., 1987).

Differences in the anatomical connections of the lateral and medial CPu are consistent with the proposed functional dissociationbetween these two parts of the dorsal striatum. The lateral CPureceives descending projections primarily from sensorimotor neocortex(McGeorge and Faull, 1989) and ascending dopaminergic input fromthe substantia nigra pars compacta (Heimer et al., 1995). Thesepatterns of connectivity combined with the results of severalstudies involving lesions and post-training manipulation of memoryconsolidation functions (Packard and White, 1991; White and Viaud,1991; McDonald and White, 1994; Packard and McGaugh, 1996) suggestthat this striatal subregion may specialize in S-R habit formation(for review, see White, 1989, 1997).

In contrast, the patterns of connectivity and the present lesion findings suggest that the medial CPu may contribute to thecontrol of behavior by the cognitive-spatial functions of otherstructures afferent to it. The medial CPu receives input fromseveral mesocortical and allocortical areas (see introductoryremarks), including the hippocampal formation. In the presentstudy, asymmetric lesions of the hippocampus and medial CPu producedeffects similar to bilateral but not unilateral lesions of thesestructures. Because the asymmetric lesions did not affect directinterhemispheric connections through the commissures, it is likelythat the lesion effects resulted specifically from the disconnectionof ipsilateral connections, that is, efferent hippocampal projectionsto medial CPu on the hippocampus lesion side, and both hippocampalafferents and medial CPu efferents on the medial CPu lesionside.

There are at least four possible functional links between the hippocampal formation and the dorsomedial striatum. First, althoughdirect projections from the CA1 subfield of the hippocampus andsubiculum project primarily to the ventral striatum via the fornix/fimbria(Heimer and Wilson, 1975; Groenewegen et al., 1987; Brog et al.,1993), Groenewegen et al. (1987) have shown that subicular afferentsalso reach the most medial, ventral, rostral and caudal partsof the CPu. Second, the perirhinal cortex projects to the dorsalhippocampal CA1 field (Liu and Bilkey, 1996), to the entorhinalcortex (Amaral and Witter, 1995), and to the nucleus accumbens/medialCPu (McGeorge and Faull, 1989; Vaudano et al., 1990; Burwell etal., 1995), and hippocampal output from the entorhinal cortexreaches the nucleus accumbens and medial CPu (Krayniak et al.,1981; Sørensen and Witter, 1983; Swanson and Köhler, 1986). Third,hippocampal output may influence striatal function through connectionswith the posterior cingulate cortex, which projects strongly tothe medial CPu (Domesick, 1969; McGeorge and Faull, 1989). Finally,the hippocampal formation projects to sectors of the medial prefrontalcortex (Swanson, 1981; Swanson and Köhler, 1986; Jay et al.,1989; Sesack et al., 1989; Jay and Witter, 1992; Condé et al.,1995), which in turn project to the ventral and dorsomedial striatum(Gerfen, 1984; McGeorge and Faull, 1989; Groenewegen et al., 1990).

The possibility that spatial information may be conveyed to the medial CPu via one or more of these indirect routes is supportedby reports that bilateral lesions of the entorhinal/perirhinalcortex (Schenk and Morris, 1985; Nagahara et al., 1995), perforantpath (Skelton and McNamara, 1992), posterior cingulate cortex(Sutherland et al., 1988; Sutherland and Hoesing, 1993), and medialprefrontal cortex (Sutherland et al., 1982; Kolb et al., 1994)all impair the ability to learn the location of a hidden platformin the water maze. Furthermore, Floresco et al. (1997) found thattemporary asymmetric lesions of the ventral hippocampus and prelimbiccortex selectively disrupted performance of a delayed win-shifttask involving spatial cues, but had no effect on a random foragingtask. Temporary disconnection of the ventral hippocampus and nucleusaccumbens had an opposite pattern of effects. Thus, differentlimbic circuits may mediate different kinds of functional interactionsbetween the hippocampal formation and thestriatum.

In conclusion, the present results provide empirical evidence for a dissociation between medial and lateral subregions ofthe CPu and for different behavioral interactions between theseCPu subregions and the hippocampal system. These interactionscan be competitive or cooperative, depending on: (1) at a behaviorallevel, the type or types of information available in a particularlearning task and (2) at a neural level, the subregion of dorsalstriatum that is engaged by this information. The findings alsosuggest that the medial and lateral regions of the CPu can functionin parallel and with some degree of independence, based on theirfunctionally segregated corticostriatal connections. The lateralCPu may contribute to S-R-based behavior and the medial CPu, aspart of a system that includes the fornix/fimbria and hippocampus,may contribute to behavior based on cognitive-spatial forms ofinformationprocessing.

  FOOTNOTES

Received Oct. 16, 1998; revised Jan. 13, 1999; accepted Jan. 20, 1999.

This work was supported by grants from the Medical Research Council of Canada and Fonds pour lat Formation de Chercheurs etl'Aide à la Rechereche, province de Quebec to N.M.W., and a HydroQuebec/McGill Major Fellowship to B.D.D. We thank Peter Walletfor assistance with animal testing, Emily Goad and Janet Raymondfor assistance with histology, and Dr. Robert McDonald for helpfuldiscussions.
Correspondence should be addressed to Dr. Bryan Devan at his presentaddress.

Dr. Devan's present address: The Krasnow Institute for Advanced Study, George Mason University, Mail Stop 2A1, Fairfax, VA22030-4444.

Parts of this paper were reported in abstract form on October 27, 1997 at the Annual Meeting of the Society for Neuroscience,New Orleans,LA.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
REFERENCES

Alexander GE, DeLong MR, Strick PL (1986) Parallel organization of functionally segregated circuits linking basal ganglia and cortex. Annu Rev Neurosci 9:357-381[ISI][Medline].
Amaral DG, Witter MP (1995) Hippocampal formation. In: The rat nervous system, Ed 2 (Paxinos G, ed), pp 443-493. San Diego: Academic.
Brog JS, Salyapongse A, Deutch AY, Zahm DS (1993) The patterns of afferent innervation of the core and shell in the "accumbens" part of the rat ventral striatum: immunohistochemical detection of retrogradely transported fluoro-gold. J Comp Neurol 338:255-278[ISI][Medline].
Brown VJ, Robbins TW (1989) Elementary processes of response selection mediated by distinct regions of the striatum. J Neurosci 9:3760-3765[Abstract].
Burwell RD, Witter MP, Amaral DG (1995) Perirhinal and postrhinal cortices of the rat: a review of the neuroanatomical literature and comparison with findings from the monkey brain. Hippocampus 5:390-408[ISI][Medline].
Colombo PJ, Davis HP, Volpe BT (1989) Allocentric spatial and tactile memory impairments in rats with dorsal caudate lesions are affected by preoperative behavioral training. Behav Neurosci 103:1242-1250[Medline].
Condé F, Maire-Lepoivre E, Audinat E, Crépel F (1995) Afferent connections of the medial frontal cortex of the rat. II. Cortical and subcortical afferents. J Comp Neurol 352:567-593[ISI][Medline].
Devan BD, Goad EH, Petri HL (1996) Dissociation of hippocampal and striatal contributions to spatial navigation in the water maze. Neurobiol Learn Mem 66:305-323[ISI][Medline].
Devan BD, McDonald RJ, White NM (1999) Effects of medial and lateral caudate-putamen lesions on place- and cue-guided behaviors in the water maze: relation to thigmotaxis. Behav Brain Res, in press.
Divac I, Markowitsch HJ, Pritzel M (1978) Behavioral and anatomical consequences of small intrastriatal injections of kainic acid in the rat. Brain Res 151:523-532[ISI][Medline].
Domesick VB (1969) Projections from the cingulate cortex in the rat. Brain Res 12:296-320[ISI][Medline].
Donovick PJ (1974) A metachromatic stain for neural tissue. Stain Technol 49:49-51[ISI][Medline].
Dunnett SB, Iversen SD (1981) Learning impairments following selective kainic acid-induced lesions within the neostriatum of rats. Behav Brain Res 2:189-209[Medline].
Dunnett SB, Iversen SD (1982a) Neurotoxic lesions of ventrolateral but not anteromedial neostriatum in rats impair differential reinforcement of low rates (DRL) performance. Behav Brain Res 6:213-226[Medline].
Dunnett SB, Iversen SD (1982b) Sensorimotor impairments following localized kainic acid and 6-hydroxydopamine lesions of the neostriatum. Brain Res 248:121-127[ISI][Medline].
Everitt BJ, Morris KA, O'Brien A, Robbins TW (1991) The basolateral amygdala-ventral striatal system and conditioned place preference: further evidence of limbic-striatal interactions underlying reward-related processes. Neuroscience 42:1-18[ISI][Medline].
Floresco SB, Seamans JK, Phillips AG (1997) Selective roles for hippocampal, prefrontal cortical, and ventral striatal circuits in radial-arm maze tasks with or without a delay. J Neurosci 17:1880-1890[Abstract/Free Full Text].
Fricker RA, Annett LE, Torres EM, Dunnett SB (1996) The placement of a striatal ibotenic acid lesion affects skilled forelimb use and the direction of drug-induced rotation. Brain Res Bull 41:409-416[ISI][Medline].
Furtado JCS, Mazurek MF (1996) Behavioral characterization of quinolinate-induced lesions of the medial striatum: relevance for Huntington's disease. Exp Neurol 138:158-168[ISI][Medline].
Gaffan D, Harrison S (1987) Amygdalectomy and disconnection in visual learning for auditory secondary reinforcement by monkeys. J Neurosci 7:2285-2292[Abstract].
Gaffan D, Parker A (1996) Interaction of perirhinal cortex with the fornix-fimbria: memory for objects and "object-in-place" memory. J Neurosci 16:5864-5869[Abstract/Free Full Text].
Gaffan EA, Gaffan D, Harrison S (1988) Disconnection of the amygdala from visual association cortex impairs visual reward-association learning in monkeys. J Neurosci 8:3144-3150[Abstract].
Gaffan D, Gaffan EA, Harrison S (1989) Visual-visual associative learning and reward-association learning: the role of the amygdala. J Neurosci 9:558-564[Abstract].
Gerfen CR (1984) The neostriatal mosaic: compartmentalization of corticostriatal input and striatonigral output systems. Nature 311:461-464[Medline].
Graybiel AM (1990) Neurotransmitters and neuromodulators in the basal ganglia. Trends Neurosci 13:244-254[ISI][Medline].
Groenewegen HJ, Berendse HW, Wolters JG, Lohman AHM (1990) The anatomical relationship of the prefrontal cortex with the striatopallidal system, the thalamus and the amygdala: evidence for a parallel organization. Prog Brain Res 85:95-118[Medline].
Groenewegen HJ, Vermeulen-Van der Zee E, te Kortxchot A, Witter MP (1987) Organization of the projections from the subiculum to the ventral striatum in the rat. A study using anterograde transport of Phaeseolus vulgaris leucoagglutinin. Neuroscience 23:103-120[ISI][Medline].
Groves PM, Garcia-Munoz M, Linder JC, Manley MS, Martone ME, Young SJ (1995) Elements of the intrinsic organization and information processing in the neostriatum. In: Models of information processing in the basal ganglia (Houk JC, Davis JL, Beiser DG, eds), pp 51-96. Cambridge: MIT.
Han JS, McMahan RW, Holland P, Gallagher M (1997) The role of an amygdalo-nigrostriatal pathway in associative learning. J Neurosci 17:3913-3919[Abstract/Free Full Text].
Hauber W, Schmidt WJ (1993) Discrete quinolinic acid lesions of the lateral but not of the medial caudate-putamen reversed haloperidol-induced catalepsy in rats. J Neural Transm 94:103-114[Medline].
Hauber W, Schmidt WJ (1994) Differential effects of lesions of the dorsomedial and dorsolateral caudate-putamen on reaction time performance in rats. Behav Brain Res 60:211-215[Medline].
Heimer L, Wilson RD (1975) The subcortical projections of the allocortex: Similarities in the neural associations of the hippocampus, the piriform cortex, and the neocortex. In: Golgi centennial symposium: perspectives in neurobiology (Santini M, ed), pp 177-193. New York: Raven.
Heimer L, Zahm DS, Alheid GF (1995) Basal ganglia. In: The rat nervous system, Ed 2 (Paxinos G, ed), pp 579-628. San Diego: Academic.
Hull CL (1943) In: Principles of behavior. New York: Appleton-Century-Crofts.
Hirsh R (1974) The hippocampus and contextual retrieval of information from memory: a theory. Behav Biol 12:421-444[ISI][Medline].
Horel JA, Keating EG (1969) Partial Klüver-Bucy syndrome produced by cortical disconnection. Brain Res 16:281-284[Medline].
Horel JA, Keating EG (1972) Recovery from a partial Klüver-Bucy syndrome in the monkey produced by disconnection. J Comp Physiol Psychol 79:105-114[Medline].
Iversen SD (1984) Behavioral aspects of the corticosubcortical interaction with special reference to frontostriatal relations. In: Cortical integration (Reinoso-Suárez F, Ajmone-Marsan C, eds), pp 237-254. New York: Raven.
Jay TM, Glowinski J, Thierry A-M (1989) Selectivity of the hippocampal projection to the prelimbic area of the prefrontal cortex in the rat. Brain Res 505:337-340[ISI][Medline].
Jay TM, Witter MP (1992) Distribution of hippocampal CA1 and subicular efferents in the prefrontal cortex of the rat by means of anterograde transport of Phaseolus vulgaris-leucoagglutinin. J Comp Neurol 313:574-586.
Kolb B, Buhrmann K, McDonald RJ, Sutherland RJ (1994) Dissociation of the medial prefrontal, posterior parietal, and posterior temporal cortex for spatial navigation and recognition memory in the rat. Cereb Cortex 6:664-680.
Krayniak PF, Meibach RC, Siegel A (1981) A projection from the entorhinal cortex to the nucleus accumbens in the rat. Brain Res 209:427-431[ISI][Medline].
Liu P, Bilkey DK (1996) Direct connection between perirhinal cortex and hippocampus is a major constituent of the lateral perforant path. Hippocampus 6:125-134[Medline].
McDonald RJ, White NM (1993) A triple dissociation of memory systems: Hippocampus, amygdala, and dorsal striatum. Behav Neurosci 107:3-22[ISI][Medline].
McDonald RJ, White NM (1994) Parallel information processing in the water maze: Evidence for independent memory systems involving dorsal striatum and hippocampus. Behav Neural Biol 61:260-270[ISI][Medline].
McDonald RJ, White NM (1995) Hippocampal and nonhippocampal contributions to place learning in rats. Behav Neurosci 109:579-593[Medline].
McGeorge AJ, Faull RLM (1989) The organization of the projection from the cerebral cortex to the striatum in the rat. Neuroscience 29:503-537[ISI][Medline].
Mikulas WL (1966) Effects of lights at the choice point on spatial alternation and position learning by normal rats and rats with bilateral lesions of the caudate nucleus. Psychonom Sci 5:275-276.
Milner B, Corkin S, Teuber H-L (1968) Further analysis of the hippocampal amnesic syndrome: 14-year follow-up study of H.M. Neuropsychologia 6:215-234[ISI].
Mishkin M (1958) Visual discrimination impairment after cutting cortical connections between the inferotemporal and striate areas in monkeys. Am Psychol 13:414.
Mishkin M (1966) Visual mechanisms beyond the striate cortex. In: Frontiers in physiological psychology (Russell RW, ed), pp 93-119. New York: Academic.
Mishkin M, Petri HL (1984) Memories and habits: some implications for the analysis of learning and retention. In: Neuropsychology of memory (Squire LR, Butters N, eds), pp 287-296. New York: Guilford.
Mishkin M, Malamut B, Bachevalier J (1984) Memories and habits: two neural systems. In: Neurobiology of learning and memory (Lynch G, McGaugh JL, Weinberger NM, eds), pp 65-77. New York: Guilford.
Mitchell JA, Hall G (1988) Learning in rats with caudate-putamen lesions: unimpaired classical conditioning and beneficial effects of redundant stimulus cues on instrumental and spatial learning deficits. Behav Neurosci 102:504-514[Medline].
Mitchell JA, Channell S, Hall G (1985) Response-reinforcer associations after caudate-putamen lesions in the rat: spatial discrimination and overshadowing-potentiation effects in instrumental learning. Behav Neurosci 99:1074-1088[Medline].
Morris RGM, Garrud P, Rawlins JNP, O'Keefe J (1982) Place navigation impaired in rats with hippocampal lesions. Nature 297:681-683[Medline].
Nagahara AH, Otto T, Gallagher M (1995) Entorhinal-perirhinal lesions impair performance of rats on two versions of place learning in the Morris water maze. Behav Neurosci 109:3-9[ISI][Medline].
O'Keefe J, Nadel L (1978) In: The hippocampus as a cognitive map. Oxford: Clarendon.
Olson CL (1988) In: Statistics: making sense of data. Dubuque: Wm. C. Brown.
Olton DS (1978) The function of septo-hippocampal connections in spatially organized behaviour. In: Functions of the septo-hippocampal system (Ciba Foundation Symposium 58), pp 327-342. New York: Elsevier/Excerpta.
Packard MG, McGaugh JL (1996) Inactivation of hippocampus or caudate nucleus with lidocaine differentially affects expression of place and response learning. Neurobiol Learn Mem 65:65-72[ISI][Medline].
Packard MG, White NM (1991) Dissociation of hippocampus and caudate nucleus memory systems by posttraining intracerebral injection of dopamine agonists. Behav Neurosci 105:295-306[ISI][Medline].
Packard MG, Hirsh R, White NM (1989) Differential effects of fornix and caudate nucleus lesions on two radial maze tasks: evidence for multiple memory systems. J Neurosci 9:1465-1472[Abstract].
Paxinos G, Watson C (1986) In: The rat brain in stereotaxic coordinates, Ed 2. San Diego: Academic.
Petri HL, Mishkin M (1994) Behaviorism, cognitivism and the neuropsychology of memory. Am Scientist 82:30-37.
Pisa M, Cyr J (1990) Regionally selective roles of the rat's striatum in modality specific discrimination learning and forelimb reaching. Behav Brain Res 37:281-292[ISI][Medline].
Reading PJ, Dunnett SB, Robbins TW (1991) Dissociable roles of the ventral, medial and lateral striatum on the acquisition and performance of a complex visual stimulus response habit. Behav Brain Res 45:147-161[ISI][Medline].
Schenk F, Morris RGM (1985) Dissociation between components of spatial memory in rats after recovery from the effects of retrohippocampal lesions. Exp Brain Res 58:11-28[ISI][Medline].
Sesack SR, Deutch AY, Roth RH, Bunney BS (1989) Topographical organization of the efferent projections of the medial prefrontal cortex in the rat: an anterograde tract-tracing study with Phaseolus vulgaris leucoagglutinin. J Comp Neurol 290:213-242[ISI][Medline].
Skelton RW, McNamara RK (1992) Bilateral knife cuts to the perforant path disrupt spatial learning in the Morris water maze. Hippocampus 2:73-80[ISI][Medline].
Sørensen KE, Witter MP (1983) Entorhinal efferents reach the caudato-putamen. Neurosci Lett 35:259-264[ISI][Medline].
Sutherland RJ, Hoesing JM (1993) Posterior cingulate cortex and spatial memory: A microlimnology analysis. In: The neurobiology of the cingulate cortex and limbic thalamus: a comprehensive handbook (Vogt BA, Gabriel M, eds), pp 461-477. Boston: Birkhauser.
Sutherland RJ, Rodriguez AJ (1989) The role of the fornix/fimbria and some related subcortical structures in place learning and memory. Behav Brain Res 32:265-277[ISI][Medline].
Sutherland RJ, Kolb B, Whishaw IQ (1982) Spatial mapping: definitive disruption by hippocampal or medial frontal cortical damage in the rat. Neurosci Lett 31:271-276[ISI][Medline].
Sutherland RJ, Whishaw IQ, Kolb B (1983) A behavioural analysis of spatial localization following electrolytic, kainate- or colchicine-induced damage to the hippocampal formation in the rat. Behav Brain Res 7:133-153[ISI][Medline].
Sutherland RJ, Whishaw IQ, Kolb B (1988) Contributions of cingulate cortex to two forms of spatial learning and memory. J Neurosci 8:1863-1872[Abstract].
Swanson LW (1981) A direct projection from Ammon's horn to prefrontal cortex in the rat. Brain Res 217:150-154[ISI][Medline].
Swanson LW (1992) In: Structure of the rat brain. Amsterdam: Elsevier.
Swanson LW, Köhler C (1986) Anatomical evidence for direct projections from the entorhinal area to the entire cortical mantle in the rat. J Neurosci 6:3010-3023[Abstract].
Tolman EC (1948) Cognitive maps in rats and men. Psychol Rev 55:189-208[ISI].
Thorndike EL (1911) In: Animal Intelligence. New York: Macmillan.
Thorndike EL (1933) A proof of the law of effect. Science 17:173-175.
Vaudano E, Legg CR, Glickstein M (1990) Afferent and efferent connections of temporal association cortex in the rat: a horseradish peroxidase study. Eur J Neurosci 3:317-330.
Viaud MD, White NM (1989) Dissociation of visual and olfactory conditioning in the neostriatum of rats. Behav Brain Res 32:31-42[ISI][Medline].
Whishaw IQ, Mittleman G, Bunch ST, Dunnett SB (1987) Impairments in the acquisition, retention and selection of spatial navigation strategies after medial caudate-putamen lesions in rats. Behav Brain Res 24:125-138[ISI][Medline].
White NM (1989) A functional hypothesis concerning the striatal matrix and patches: mediation of S-R memory and reward. Life Sci 45:1943-1957[ISI][Medline].
White NM (1997) Mnemonic functions of the basal ganglia. Curr Opin Neurobiol 7:164-169[ISI][Medline].
White NM, Viaud M (1991) Localized intracaudate dopamine D2 receptor activa