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The Journal of Neuroscience, March 15, 2001, 21(6):2143-2149
NMDA and AMPA Antagonist Infusions into the Ventral Striatum Impair Different Steps of Spatial Information Processing in a Nonassociative Task in Mice
Pascal Roullet1, 2, 3, Francesca Sargolini1, 2, 3, Alberto Oliverio1, and Andrea Mele1 1 Dipartimento di Genetica e Biologia Molecolare, Università di Roma "La Sapienza," I-00185, Rome, Italy, 2 Laboratoire d'Ethologie et Cognition Animale, Centre National de la Recherche Scientifique ERS 2041, 31062 Toulouse, France, and 3 Oasi Maria SS, 94018 Troina, Italy
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
Most of the research on ventral striatal functions has been focused on their role in modulating reward and motivation. More recently, a possible role of this structure in cognitive functions has been suggested. However, very little information is available on the involvement of the nucleus accumbens in the different stages of the consolidation process. In this study, the effect of focal injections of AP-5 and DNQX, competitive antagonists at the NMDA and AMPA receptors, respectively, was examined in a nonassociative task designed to estimate the ability of mice to react to spatial changes. The task consists of placing the animals in an open field containing five objects; after three sessions of habituation, their reactivity to object displacement was examined 24 hr later.
AP-5 injections administered after training impaired the ability of mice to detect the spatial novelty but did not affect response when injected 120 min after training or before testing. On the contrary, DNQX did not affect response when administered immediately or 120 min after training but did impair spatial discrimination when administered before training or testing. These data demonstrate a double dissociation between glutamate receptor subtypes, such that accumbens NMDA receptors are important for consolidation and not ongoing discrimination of spatial information, whereas AMPA receptors have an opposite role in these processes.
Key words: nucleus accumbens; glutamate; consolidation; spatial learning; DNQX; AP-5
INTRODUCTION
Most of the research on the functions of the nucleus accumbens (Nacc) has been focused on its role in modulating reward and motivation (Mogenson, 1987
). However, more recently a possible role of the basal ganglia in modulating cognitive functions has been emphasized (Graybiel, 1995
In particular, there is evidence of a possible role of the ventral striatum in processing spatial information (Annett et al., 1989
Limbic projections to the accumbens are thought to be mainly glutamatergic (Walaas and Fonnum, 1979
The purpose of this study was to investigate the possible involvement of NMDA and non-NMDA receptors located into the Nacc in the different aspects of spatial learning. The task we chose is a nonassociative task in which no explicit reward was present and in which no stimulus response association was required. It consists of placing mice in an open field containing five objects and, after three sessions of habituation, examining their reactivity to object displacement. Control animals usually show an increased exploration of the displaced object; this response is usually interpreted as an index of the ability of animals to detect and react to the spatial change (Poucet, 1989
MATERIALS AND METHODS
Animals. The subjects were CD1 outbred mice obtained from Charles River (Calco, Italy). At the time of surgery, they were ~9- to 10-weeks-old, and their weights ranged from 35 to 40 gm. On arrival, mice were housed in groups of five in standard breeding cages (21 × 21 × 12 cm) placed in a rearing room at a constant temperature (22 ± 1°C) with food and water available ad libitum. They were tested during the first half of the light period (between 9:00 A.M. and 2:00 P.M.).
Every possible effort was made to minimize animal suffering, and all procedures were in strict accordance with European community and Italian national laws and regulations on the use of animals in research and National Institutes of Health guidelines on animal care.
Surgery. Mice were anesthetized with chloral hydrate (400 mg/kg) and placed in a stereotaxic apparatus (David Kopf Instruments, Tujunga, CA) with mouse adapter and lateral bars. After placing the animals on the stereotaxic apparatus, the head skin was cut longitudinally and bilateral guide cannulae (0.5 mm in diameter), aimed at the core of the accumbens, were fixed on the calvarium with dental acrylic. The following coordinates with lambda and bregma in the same horizontal plane were used: anterior to bregma, +1.7 mm; lateral to midline, ±1 mm; ventral from the dura,
2 mm, according to Franklin and Paxinos (1997)
Reaction to novelty apparatus. The apparatus (Fig. 1) was a circular open field that was 60 cm in diameter with a 30-cm-high wall made of gray plastic material and a floor painted white and divided into sectors by black lines. The open field was placed into a soundproof cubicle and surrounded by a visually uniform environment except for a conspicuous striped pattern that was 30-cm-wide and 36-cm-high (alternating 1.5-cm-wide vertical white and black bars) attached to the wall of the field. The apparatus was illuminated by a red light (80 W) located on the ceiling. A video camera above the field was connected to a video recorder and a monitor.
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Figure 1. Schematic representation of the apparatus and the object configuration over successive sessions. A, The open field is initially empty (S1); in the three subsequent sessions (S2-S4), it is filled with objects in a particular configuration (B). In S5, two objects are displaced (spatial novelty) (C).
Five objects were simultaneously present in the open field: (1) a chromium-plated parallelepiped (7 × 4 × 4 cm) with holes irregularly distributed on the sides and the top; (2) a plastic cone on a transparent cylinder base (diameter of the section, 8 cm; height, 6 cm); (3) two gray iron rectangles (10 × 3 cm) forming a 90° angle, inserted on a rectangular plastic base (7 × 5 cm); (4) a black Plexiglas cylinder (height, 10 cm; diameter, 5 cm); and a (5) a black and gray spool (height, 9 cm; diameter of the top, 5 cm) on a square base (6 × 6 cm). The initial arrangement was a square with a central object (object E) as schematized in Figure 1.
Procedure. The first day, mice were individually submitted to four successive 6 min sessions, separated by a 3 min delay, during which the subjects were returned to their home cages. During session 1 (S1), the mice were placed into the empty open field to familiarize the animal with the apparatus and to record the baseline level of locomotor activity. During S2-S4, the objects were placed as shown in Figure 1.
On the second day (24 hr later), mice were submitted to only one 6 min session, with the objects displaced relative to the original arrangement (S5). The configuration was changed by moving two objects: object E replaced object A, which was itself displaced at the periphery of the apparatus so that the initial square arrangement was changed to a polygon-shaped arrangement.
Drug injections were performed at different time points: for experiment 1, the NMDA antagonist, (
The rationale for using these doses was based on previous studies and preliminary experiments in which they were demonstrated to be effective, when focally administered into the Nacc, in impairing spatial learning in the same task (Sargolini et al., 1999
Data collection and statistics. Data collection was performed using video recordings; the observer was always blind to treatment (Save et al., 1992
Statistical analyses were performed using an ANOVA with a within-between design. For the habituation, the repeated factor was session (three levels: S2, S3, S4) and the between factor was treatment (levels in experiment 1 were 0.0, 0.075, 0.15, and 0.3 of AP-5; levels in experiment 2 were 0.0, 0.001, and 0.005 of DNQX; levels in experiments 3 and 4 were controls, AP-5, and DNQX; levels in experiment 5 were controls and DNQX). The exploration of the different object categories in S4 and S5 expressed as absolute values was analyzed by repeated two-factors treatment [sessions (two levels), S4 and S5; object category (two levels), displaced objects (DO), and nondisplaced objects (NDO)] and between factor treatment (same levels than before). The re-exploration of the different object categories expressed as exploration in S5-S4 for each object category was analyzed using a within (object category, two levels) and between (treatment) design. Tukey honestly significant difference and/or simple effects post hoc comparison were used when appropriate.
Cannula placement verification. At the completion of the experiment, mice were killed by an overdose of chloral hydrate; brains were removed and frozen at
RESULTS
Cannula placement verification
Figure 2 shows a schematic representation of the cannula placements for all of the experiments. Histological analysis shows that the injection site is located in the Nacc core for the majority of mice. Only animals showing correct Nacc placements were included in the statistical analysis.
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Figure 2. Drawing of coronal sections from animals in all experiments. Each symbol represents the cannula placement. A, Immediate post-training AP-5 administrations. Filled triangles, saline; open circles, AP-5 at 0.07 µg/side; filled circles, AP-5 at 0.15 µg/side; filled diamonds, AP-5 at 0.3 µg/side. B, Immediate post-training DNQX administrations. Filled triangles, vehicle; open and filled circles, respectively, AMPA antagonist at 0.001 and 0.005 µg/side. C, Cannula placements for administrations of vehicle (filled triangles), AP-5 at 0.03 µg/side (open circles), and DNQX at 0.005 µg/side (filled circles) 120 min after training. D, Cannula placements for mice administered vehicle (filled triangles), AP-5 at 0.15 µg/side (open circles), and DNQX at 0.001 µg/side (filled circles) before testing. E, Cannula placements for mice administered vehicle (filled triangles) and DNQX at 0.001 µg/side (open circles) before training.
Habituation
Table 1 shows the mean time of contact in S2, S3, and S4 with all five objects for each experiment. No major differences among groups were observed with regard to overall object exploration in S2, S3, and S4 when drugs were administered after training in experiments 1-4. Moreover, all groups showed a similar decrease in the time spent exploring the objects over sessions. The ANOVA revealed only a significant session effect but no drug effect and no session-drug interaction. Pretraining focal administrations of DNQX reduced the overall time spent by the animals exploring the objects only in experiment 5. It is worthwhile to note, however, that AMPA receptor blockade did not affect the habituation pattern of the mice. The ANOVA revealed a significant effect of drug (F(1,12) = 15.2; p = 0.0021) and sessions (F(2,24) = 36.5; p = 0.0001) but no interaction (F(2,24) = 0.14; p = 0.86). Table 1 shows the mean time of contact with the two object categories, DO and NDO, before spatial change in S4; control as well as drug-injected groups explored the two categories for a similar amount of time.
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Table 1. Mean duration of contact (± SEM) with the objects before and after spatial change in the different experimental groups Experiment 1: effect of post-training AP-5 administration into the nucleus accumbens on detection of spatial change
Table 1 shows the mean time spent in contact with the different object categories in S5 by saline- and drug-injected animals. Mice injected with saline immediately after training explored DO more than NDO. The difference in the time spent exploring the two categories of objects was reduced in a dose-dependent manner by focal administrations of AP-5 after training. Mice injected with the lower dose explored DO significantly more than NDO, whereas animals treated with the two higher doses showed no significant difference between the two object categories.
Figure 3 represents the effect of post-trial AP-5 administrations on the exploration of the two categories of objects, expressed as difference between S5 and S4. AP-5 injections decrease the re-exploration of DO without affecting NDO. The one-between one-within analysis revealed a significant effect of the object category (F(1,33) = 39.887; p = 0.0001) and a significant interaction between drug and object category (F(1,33) = 10.731; p = 0.0001) but no significant drug effect (F(3,33) = 0.537; p = 0.66).
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Figure 3. Experiment 1: Reactivity to spatial change of mice after immediate post-training focal administration of AP-5 into the nucleus accumbens. The histogram illustrates the mean time (± SEM) spent exploring the DO or NDO in S5 minus the time spent exploring the same class of objects in the last session of habituation (S4). *p < 0.05; DO versus NDO.
Experiment 2: effect of post-training DNQX administration into the nucleus accumbens on detection of spatial change
Table 1 shows absolute values for DO and NDO exploration in S5. S5 control animals as well as DNQX-injected mice spent more time in contact with DO compared with NDO. Post hoc analysis revealed a significant difference between the two categories in all groups.
Figure 4 represents the effect of immediate post-training DNQX administrations on DO-NDO exploration, expressed as the difference between S5 and S4. The one-between one-within factor analysis revealed a significant main object category effect (F(1,19) = 40.6; p = 0.0001) but no treatment effect (F(2,19) = 0.397; p = 0.6778) and no treatment-object category interaction (F(2,19) = 0.263; p = 0.7718).
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Figure 4. Experiment 2: Reactivity to spatial change of mice after immediate post-training focal administration of the AMPA antagonist DNQX into the nucleus accumbens. The histogram illustrates the mean time (± SEM) spent exploring the DO or NDO in S5 minus the time spent exploring the same class of objects in the last session of habituation (S4). *p < 0.05; DO versus NDO.
Experiment 3: effect of AP-5 and DNQX administration into the nucleus accumbens at 120 min after training on detection of spatial change
The absolute values for DO-NDO exploration in S5 after administrations of vehicle, NMDA antagonist, and AMPA antagonist 120 min after training are reported in Table 1. Control mice showed a higher level of DO exploration rather than NDO exploration. Focal administrations of AP-5 and DNQX did not impair this response.
Figure 5 represents the effects of AP-5 and DNQX injections administered 120 min after training on DO and NDO exploration, expressed as difference in two subsequent sessions (S5-S4). The ANOVA revealed a mean object category effect (F(1,23) = 91.087; p = 0.0001) but no significant treatment effect (F(2,23) = 0.231; p = 0.796) or interaction between the two factors (F(2,23) = 0.244; p = 0.785).
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Figure 5. Experiment 3: Reactivity to spatial change of mice after post-training focal administration of AP-5 at 0.03 µg/side and DNQX at 0.005 µg/side into the nucleus accumbens 120 min after S4. The histogram illustrates the mean time (± SEM) spent exploring the DO or NDO in S5 minus the time spent exploring the same class of objects in the last session of habituation (S4). *p < 0.05; DO versus NDO.
Experiment 4: effect of pretest AP-5 and DNQX administration into the nucleus accumbens on detection of spatial change
Table 1 shows the mean time of contact with DO and NDO in S5. Control mice explored DO more than NDO. Pretest administrations of the NMDA antagonist did not affect the amount of time spent exploring DO and NDO in S5 as well as the difference between the two object categories. On the contrary, pretest DNQX injections decreased exploration of both DO and NDO as well as the difference between DO and NDO.
Figure 6 represents the effects of focal administrations of vehicle and drugs immediately before the test, expressed as a difference in the exploration of the two object categories in the two subsequent sessions. The ANOVA revealed a significant object category effect (F(1,20) = 60.458; p = 0.0001), a mean drug effect (F(2,20) = 8.519; p = 0.002), and a significant interaction between the two factors (F(2,20) = 8.653; p = 0.002).
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Figure 6. Experiment 4: Reactivity to spatial change of mice after pretest focal administration of AP-5 at 0.015 µg/side and DNQX at 0.001 µg/side into the nucleus accumbens. The histogram illustrates the mean time (± SEM) spent exploring the DO or NDO in S5 minus the time spent exploring the same class of objects in the last session of habituation (S4). *p < 0.05; DO versus NDO.
Experiment 5: effect of pretraining DNQX administration into the nucleus accumbens on detection of spatial change
Table 1 shows the mean time of contact with DO and NDO in S5. Pretraining DNQX administration induced a decrease in the time spent exploring DO but increased the time spent exploring NDO, thus reducing the difference in object category exploration observed in control mice.
Figure 7 shows the effects of pretraining vehicle and DNQX administrations expressed as a difference between S5 and S4 for the two object categories. The ANOVA revealed a main drug effect (F(1,12) = 5.2; p = 0.04), a main object effect (F(1,12) = 66.36; p = 0.0001), and an interaction between the two main effects (F(1,12) = 57.1; p = 0.001).
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Figure 7. Experiment 5: Reactivity to spatial change of mice after pretraining focal administration of DNQX at 0.001 µg/side into the nucleus accumbens. The histogram illustrates the mean time (± SEM) spent exploring the DO or NDO in S5 minus the time spent exploring the same class of objects in the last session of habituation (S4). *p < 0.05; DO versus NDO.
DISCUSSION
The results presented in this paper confirm and extend earlier studies on the involvement of glutamate receptors located within the Nacc in processing spatial information (Maldonado-Irizarry and Kelley, 1995
There is considerable evidence suggesting an involvement of the Nacc in spatial learning (Annett et al., 1989
Previous studies have indicated an involvement of Nacc in memory consolidation on the basis of the impairing effects induced by post-trial temporary lesions with TTX or blockade of D2 dopamine receptors, respectively, in passive avoidance tasks, and in the spatial version of the Morris water maze (Lorenzini et al., 1995
The purpose of this study was also to verify possible different roles of the two major classes of glutamate receptors, AMPA and NMDA, in the distinct stages of memory formation. We have recently demonstrated an involvement of both glutamate receptors classes located in this structure in the acquisition of spatial information (Usiello et al., 1998
It has been demonstrated in the rat that the core rather than the shell subregion of the accumbens is involved in processing of spatial information (Maldonado-Irizarry and Kelley, 1995
The task we used in this study, modified from Poucet (1989)
The Nacc is viewed as an interface between the limbic and the motor systems that acts to select the most appropriate behavioral response (Mogenson, 1987
Even if experimental evidence on the involvement of the Nacc in consolidation of spatial information is now accumulating, whether this structure plays a role in information storage or whether memory resides elsewhere is still unclear. Several studies have demonstrated plastic changes involving glutamatergic afference to the Nacc (Mulder et al., 1997
Finally, it should be noted that deafferentation studies and pharmacological manipulation of the Nacc (Floresco et al., 1996
FOOTNOTES Received Oct. 18, 2000; revised Dec. 22, 2000; accepted Jan. 4, 2001.
This study was supported in part by the 40% Ministero dell'Universitá e della Ricerca Scientifica e Tecnologica grants "Farmacologia dell'apprendimento e della memoria" and "Neurobiologia delle tossicodipendenze e dei meccanismi di gratificazione naturale" and by a grant from the University of Rome "La Sapienza" (A.O.).
Correspondence should be addressed to Andrea Mele, Dipartimento di Genetica e Biologia Molecolare, Università di Roma "La Sapienza," Ple. Aldo Moro, 5, I-00185, Rome, Italy. E-mail: Andrea.Mele{at}uniroma1.it.
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