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Previous Article | Next Article
The Journal of Neuroscience, July 15, 2002, 22(14):5817-5822
BRIEF COMMUNICATION
Enhanced Inhibition of Synaptic Transmission by Dopamine in the Nucleus Accumbens during Behavioral Sensitization to CocaineCorinne Beurrier and Robert C. Malenka Nancy Pritzker Laboratory, Department of Psychiatry and Behavioral Sciences, Stanford University School of Medicine, Palo Alto, California 94304
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
Neural adaptations in the nucleus accumbens (NAc), a key component of the mesolimbic dopamine (DA) system, are thought to mediate several of the long-term behavioral sequelas of chronic in vivo exposure to drugs of abuse. Here, we examine whether the modulation of excitatory synaptic transmission by DA in the NAc shell is modified after chronic cocaine exposure that induced behavioral sensitization. The DA-induced inhibition of AMPA receptor-mediated synaptic responses was enhanced in cocaine-treated mice, an effect that was caused by activation of D1-like receptors. DA did not enhance NMDA receptor-mediated synaptic responses in saline- and cocaine-treated mice or in the dorsal striatum of control mice. We hypothesize that the enhanced inhibitory effects of DA on synaptic transmission in the NAc are one of a number of adaptations that contribute to a decrease in excitatory drive to NAc after exposure to drugs of abuse.
Key words: addiction; cocaine; dopamine; nucleus accumbens; striatum; synaptic transmission; glutamate; AMPA receptors; NMDA receptors
INTRODUCTION
The reinforcing effects of drugs of abuse are thought to be mediated in part by the release of dopamine (DA) in the mesolimbic dopaminergic pathway, which projects from A10 dopaminergic cell bodies within the ventral tegmental area to the nucleus accumbens (NAc) (Wise, 1998
). Thus, critical questions for understanding the neural mechanisms responsible for mediating the behavioral effects of drugs of abuse include (1) what are the effects of DA on synaptic transmission in the NAc and (2) how are these effects modified by chronic in vivo exposure to drugs of abuse? GABAergic medium spiny neurons are the major cell type in the NAc and receive glutamatergic inputs from cortical and subcortical limbic areas, including the hippocampus, prefrontal cortex, and amygdala (Groenewegen et al., 1999
MATERIALS AND METHODS
Treatment regimen and locomotor activity. Male C57BL/6 mice (22 d) were given intraperitoneal injections of either saline (0.9% NaCl) or saline with cocaine (15 mg/kg). Immediately after each injection, horizontal locomotor activity was monitored in open-field chambers (Med Associates Inc., St. Albans, VT) for 15 min. After an initial 2 d of receiving only saline injections, mice were randomly divided into groups that received five daily injections of either cocaine or saline. After 10-14 d without injections, both groups received cocaine injections, and locomotor activity was assessed. Brain slices were prepared from these animals on the following day. Some of these animals (10 of 31 saline animals; 10 of 43 cocaine animals) were included in our previous study on behavioral sensitization (Thomas et al., 2001
Electrophysiology. Sagittal slices of the NAc (200-250 µm) were prepared as described previously (Thomas et al., 2001
Cells were visualized with an upright microscope (Zeiss, Thornwood, NY), and whole-cell voltage-clamp recordings were made using an Axopatch 1D amplifier (Axon Instruments, Foster City, CA). Electrodes (5-8 M
) contained (in mM): 117 cesium gluconate, 2.8 NaCl, 20 HEPES, 0.4 EGTA, 5 TEA-Cl, 2.5 MgATP, and 0.25 MgGTP, pH 7.2-7.4 (285-295 mOsm). Field potential recordings were made using pipettes filled with 1 M NaCl. For perforated-patch experiments, amphotericin B (30 mg/ml) dissolved in DMSO was added to internal solution (0.02-0.03% final concentration) containing (in mM): 110 cesium gluconate, 2.8 NaCl, 20 HEPES, 0.4 EGTA, 5 TEA-Cl, and 20 CsCl. Experiments were begun only after series resistance had stabilized. Medium spiny neurons were identified by their morphology and high resting membrane potential (
75 to
Stainless steel bipolar microelectrodes were placed at the prelimbic cortex-NAc border to stimulate afferents, preferentially from the prelimbic cortex at a baseline frequency of 0.1 Hz. Neurons were voltage clamped at a membrane potential of
Drugs. All drugs were purchased from Sigma-RBI (St. Louis, MO) except cocaine hydrochloride (Stanford Health Services Pharmacy, Palo Alto, CA) and D-APV (Tocris Cookson, Ballwin, MO). Stock solutions of dopamine hydrochloride, R(+)-7-chloro-8-hydroxy-3-methyl-1-phenyl-2,3,4,5-tetrahydro-1H-3-benzazepine hydrochloride [R(+)-(+)-SCH-23390], 1-[2-(bis[4-fluorophenyl]methoxy)ethyl]-4-(3-phenylpropyl)piperazine-dihydrochloride (GBR-12909), and cocaine hydrochloride were made in water and applied through the superfusion medium. Sodium metabisulfite (final concentration, 50 µM) was added to the dopamine solution. Cocaine for in vivo injections was dissolved in NaCl (0.9%).
RESULTS
Long-lasting locomotor sensitization to cocaine in mice
To induce behavioral sensitization, we paired repeated cocaine injections with exposure of the animals to a distinct test environment. After 2 d of saline injections to habituate the animals to the activity box, the locomotor response to a fixed dose of cocaine (15 mg/kg) increased dramatically across days of testing (Fig. 1) (day 3 distance traveled: saline, 463.5 ± 31.1 cm, n = 31; cocaine, 1329.5 ± 111.1 cm, n = 43; day 7 distance traveled: saline, 484.6 ± 54.8 cm, n = 31; cocaine, 3843.9 ± 185.5 cm, n = 43; p < 0.0001). To test whether this procedure produced long-lasting locomotor sensitization, we administered a challenge dose of cocaine to both saline- and cocaine-treated groups 10-14 d after the last dose of the initial treatment regimen. Mice pretreated with cocaine showed a much greater locomotor response to cocaine than did saline-pretreated animals (Fig. 1) (cocaine, 4384.9 ± 212.8 cm, n = 43; saline, 1535.3 ± 159.1 cm, n = 31; p < 0.0001). These results indicate that the initial 5 d exposure to cocaine caused behavioral sensitization that lasted for
2 weeks.
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Figure 1. Repeated cocaine administration induces behavioral sensitization. Mean ± SEM acute locomotor activity in response to saline and cocaine injections is shown. Locomotor activity was monitored for 15 min immediately after each injection.
Increased inhibition of excitatory synaptic transmission by dopamine in sensitized mice
The NAc is commonly divided into two components, the shell and the core, which can be distinguished both anatomically and functionally (Zahm, 1999
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Figure 2. Chronic cocaine treatment enhances inhibitory actions of DA on AMPAR EPSCs. A, Summary graph of the effects of DA (75 µM) in saline (n = 12 cells, 8 mice) and cocaine-treated (n = 12 cells, 9 mice) mice. B, Sample experiments from saline (top) and cocaine-treated (bottom) mice displaying the effect of 20 µM DA. Sample traces were collected at the times indicated on the graph. Calibration: top, 50 msec, 100 pA; bottom, 50 msec, 200 pA. C, Summary graph of the effects of DA (20 µM) in saline (n = 9 cells, 7 mice) and cocaine-treated (n = 10 cells, 5 mice) mice. D, Magnitude of inhibition of AMPAR EPSCs by DA in saline and cocaine-treated mice (*p < 0.05).
Synaptic actions of DA in cocaine-treated mice are caused by D1-like receptors
DA receptors are commonly subdivided into two classes: (1) D1-like receptors (D1 and D5) and (2) D2-like receptors (D2, D3, and D4) (Sibley and Monsma, 1992
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Figure 3. The DA-induced depression of excitatory synaptic transmission in cocaine-treated mice is mediated by D1-like receptors. A, Summary graph showing effects of DA (20 µM) on field EPSPs in saline (n = 11 slices, 8 mice) and cocaine-treated (n = 28 slices, 20 mice) mice. Sample traces were collected at the times indicated on the graph. Calibration: 4 msec, 0.1 mV. B, Summary of experiments in which DA (20 µM) was applied to slices from cocaine-treated mice first in the absence and then in the presence of SCH-23390 (10 µM; n = 6 slices, 6 mice). fEPSP amplitudes were renormalized when SCH-23390 was applied to minimize possible effects of experimental drift.
The enhanced inhibition of excitatory transmission by DA in the cocaine-treated group could be explained by some modification of the D1-like DA receptors (e.g., increase in receptor number and/or function) or by a change in the DA transporters (DATs) that might influence the effective concentration of DA when it is applied to the slices (e.g., decrease in DAT number and/or function). To help distinguish between these possibilities, we examined whether the selective DAT inhibitor GBR-12909 (300 nM) enhanced the synaptic actions of DA. If it did, it would suggest that the level of DAT activity in our slices could limit the effective concentration of DA. However, in saline-treated mice, GBR-12909 (300 nM) did not significantly affect the synaptic depression elicited by DA (30 µM; n = 4; data not shown). These results indicate that DATs do not influence the effective concentration of exogenous DA achieved in the slices. Therefore, it is very unlikely that the enhanced inhibition of excitatory synaptic transmission by DA in cocaine-treated mice is caused by a reduction in DAT number and/or function.
Lack of a postsynaptic effect of DA on NMDAR-mediated EPSCs
It has been suggested that the inhibitory effects of D1 receptor activation in the NAc are the consequence of a DA-induced enhancement of NMDAR-mediated responses (Harvey and Lacey, 1997
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Figure 4. DA does not potentiate NMDAR EPSCs in either the NAc or dorsal striatum. A1, Example of an experiment in which DA (75 µM) was applied while simultaneously monitoring AMPAR EPSCs and NMDAR EPSCs at +40 mV. Note that application of D-APV (50 µM) had minimal effect on the measurement of the AMPAR EPSC but eliminated the NMDAR EPSC. A2, Top traces show the dual-component EPSC, the AMPAR EPSC obtained after application of D-APV, and the NMDAR EPSC obtained by subtraction of the two traces. Bottom traces show the dual-component EPSC before and after application of DA. Arrows show time points at which measurements were made. Calibration: 50 msec, 100 pA. B, Summary graph of the effects of DA (75 µM) on NMDAR EPSCs and AMPAR EPSCs in saline (n = 8 cells, 5 mice) and cocaine-treated (n = 15 cells, 9 mice) mice. C, Summary graph of the effects of DA (100 µM) on NMDAR EPSCs and AMPAR EPSCs recorded in slices from control mice using perforated-patch recording techniques (n = 5 cells, 4 mice). D, Summary graph of the effects of DA (30-75 µM) on NMDAR EPSCs and AMPAR EPSCs in dorsal striatum slices from control mice (n = 4 cells, 4 mice). E, Mean AMPAR/NMDAR ratio during baseline and at the end of DA application for experiments shown in B-D. In all cases, DA did not affect the AMPAR/NMDAR ratios.
Although the previous work in the NAc also used standard whole-cell recording techniques (Harvey and Lacey, 1997
DISCUSSION
A prominent rodent model for some key features of addiction is the long-lasting increase in the acute drug-induced locomotor response after repeated exposure to psychostimulants (Robinson and Berridge, 1993
We find that the presynaptic inhibitory action of DA is enhanced in cocaine-sensitized animals, and that this effect is mediated by a D1-like receptor, as found previously in control animals (Pennartz et al., 1992
Because DA has been reported to enhance NMDAR-mediated responses in both the NAc (Harvey and Lacey, 1997
The functional significance of the enhancement of the inhibitory synaptic actions of DA in the NAc shell after chronic in vivo cocaine exposure remains to be determined. We would suggest it is likely one of a number of modifications of synaptic and cellular function in the NAc contributing to behavioral sensitization. Interestingly, many of the reported effects of chronic in vivo cocaine exposure would be expected to decrease net excitatory drive to medium spiny neurons (Henry and White, 1991
FOOTNOTES Received March 29, 2002; revised May 1, 2002; accepted May 7, 2002.
This work was supported by grants from Fondation pour la Recherche Médicale (C.B.) and the National Institute on Drug Abuse (R.C.M.). We thank A. Bonci, D. Saal, and M. Thomas for helpful comments.
Correspondence should be addressed to Robert C. Malenka, Department of Psychiatry and Behavioral Sciences, 1201 Welch Road, Room P105, Stanford Medical Center, Palo Alto, CA 94304. E-mail: malenka{at}stanford.edu.
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