Relationships between the Prefrontal Cortex and the Basal Ganglia in the Rat: Physiology of the Cortico-Nigral Circuits

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The Journal of Neuroscience, June 1, 1999, 19(11):4674-4681

Relationships between the Prefrontal Cortex and the Basal Ganglia in the Rat: Physiology of the Cortico-Nigral Circuits
Nicolas Maurice¹, Jean-Michel Deniau², Jacques Glowinski¹, and Anne-Marie Thierry¹
¹ Chaire de Neuropharmacologie, Institut National de la Santé et de la Recherche Médicale U114, Collège de France, 75231 Paris Cedex 05, France, and ² Université Pierre et Marie Curie, Département de Neurochimie-Neuroanatomie, Institut des Neurosciences, Unité de Recherche Mixte 7624, 75230 Paris Cedex 05, France

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The prelimbic/medial orbital areas (PL/MO) of the rat prefrontal cortex are connected to substantia nigra pars reticulata(SNR) through three main circuits: a direct nucleus accumbens(NAcc)-SNR pathway, an indirect NAcc-SNR pathway involving theventral pallidum (VP) and the subthalamic nucleus (STN), and adisynaptic cortico-STN-SNR pathway. The present study was undertakento characterize the effect of PL/MO stimulation on SNR cells andto determine the contribution of these different pathways. Themajor pattern of responses observed in the SNR was an inhibitionpreceded by an early excitation and followed or not by a lateexcitation. The inhibition resulted from the activation of thedirect NAcc-SNR pathway because it disappeared after acute blockadeof the glutamatergic cortico-striatal transmission by CNQX applicationinto the NAcc. The late excitation resulted from the activationof the indirect NAcc-VP-STN-SNR pathway via a disinhibition ofthe STN because it disappeared after either CNQX application intothe NAcc or blockade of the GABAergic striato-pallidal transmissionby bicuculline application into the VP. The early excitation,which was markedly decreased after blockade of the cortico-STNtransmission by CNQX application into the STN, resulted from theactivation of the disynaptic cortico-STN-SNR pathway. Finally,the blockade of the cortico-STN-VP circuit by CNQX applicationinto STN or VP modified the influence of the trans-striatal circuitson SNR cells. This study suggests that, in the prefrontal cortex-basalganglia circuits, the trans-subthalamic pathways, by their excitatoryeffects, participate in the shaping of the inhibitory influenceof the direct striato-nigral pathway on SNRneurons.

Key words: basal ganglia circuits; prefrontal cortex; subthalamic nucleus; ventral striatum; nucleus accumbens; ventral pallidum; substantia nigra pars reticulata; in vivo single unit recordings; rat

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The substantia nigra pars reticulata (SNR) and the internal pallidum (GPi), or entopeduncular nucleus in the rat, are thetwo main output stations of the basal ganglia. Through these outputnuclei, information processed in the basal ganglia are directedto thalamic nuclei and pontomesencephalic structures. In currentworking models of basal ganglia (Alexander et al., 1986; Parentand Hazrati 1995a), the striatum is considered as a main inputstructure through which cortical information is transferred tothe SNR and GPi. The striatum, which receives excitatory afferentsfrom the entire cerebral cortex, projects to the SNR and GPi througha direct and an indirect pathway. The indirect pathway involvestwo tightly interconnected structures: the external segment ofthe globus pallidus and the subthalamic nucleus (STN). The STNalso receives direct inputs from motor and prefrontal areas ofthe cerebral cortex and is thus considered as an input structureof the basal ganglia (Berendse and Groenewegen, 1991; Parent andHazrati, 1995b). The neurons of this network are GABAergic, exceptthose of the STN, which areglutamatergic.

The convergent nature of the cortico-striatal projections and the subsequent striato-nigral and striato-pallidal pathwayshas long been emphasized (Percheron and Filion, 1991). However,there is now growing evidence that signals originating from functionallydistinct cortical areas are processed in separate striatal subterritoriesand remain segregated in the striato-pallido- and striato-nigro-thalamicpathways (Alexander et al., 1986; Groenewegen and Berendse, 1994;Deniau and Thierry, 1997). This led to the proposal cortico-basalganglia circuits are essentially organized in parallel channels(Alexander et al., 1986).

We have recently described in the rat the anatomo-functional organization of the prefrontal channel originating from the prelimbicand medial orbital areas (PL/MO). PL/MO areas send an excitatoryinput to a restricted territory of the ventral striatum, the coreof the nucleus accumbens (NAcc), which projects through a directand an indirect pathway to the dorsomedial part of the SNR (Deniauet al., 1994; Montaron et al., 1996; Maurice et al., 1997, 1998b).The indirect pathway involves the region of the ventral pallidum(VP), denominated lateral ventral pallidum (VPl) by Zahm (1989),and the medial part of the STN. In addition, the medial STN receivesa direct excitatory input from the prefrontal cortex and can thusbe also viewed as an input structure in this prefrontal channel(Berendse and Groenewegen, 1991; Maurice et al., 1998a).

The present study was undertaken to determine the contribution of the trans-striatal and trans-subthalamic circuits in theinfluence exerted by PL/MO areas on the activity of the SNR. Forthis purpose, the responses evoked in SNR cells by PL/MO stimulationwere characterized, and we investigated the effects of reversibleblockade of the synaptic transmission in the NAcc, the VP, orthe STN on theseresponses.

  MATERIALS AND METHODS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Experiments were performed on 37 adult male Sprague Dawley rats (weighing 275-300 gm; Charles River, Saint-Aubin les Elbeuf,France). Animals were anesthetized with ketamine (100 mg/kg, i.p.;supplemented by 50 mg/kg, i.m., injections; Imalgène 500; Rhône-Mérieux,Courbevoie, France) and fixed in a conventional stereotaxic headframe (Horsley Clarke Apparatus; Unimécanique, Epinay-sur-Seine,France). Body temperature was monitored by a rectal thermometerand maintained at 37°C with a homeothermic warming blanket (HarvardApparatus, Kent,UK).

Electrophysiological analysis. Single-unit activity of SNR cells was recorded extracellularly using glass micropipettes (6-10M $Omega$ ) filled with a 0.6 M sodium chloride solution containing 4%Pontamine Sky Blue. Action potentials of single neurons were amplifiedwith a World Precision Instruments (Hertfordshire, UK) DAM-5Adifferential preamplifier and displayed on a Tektronix (Marlow,UK) memory oscilloscope. Nigral neurons were identified as nondopaminergicon their classically defined electrophysiological characteristics:thin spikes (width, <2 msec) and ability to present high-frequencydischarge (>10 Hz) without a decrease in the spike amplitude (Bunneyet al., 1973; Deniau et al., 1978; Guyennet and Aghajanian, 1978).Spikes were separated from noise using a window discriminatorand sampled on-line thanks to a computer connected to a CED 1401interface (Cambridge Electronics Design, Cambridge, UK). Peristimulustime histograms were generated from 60 to 100 stimulation trialsusing 1 msec bins and plotted on a Hewlett-Packard plotter. Thecriterion used to establish the existence of an excitation wasan increase greater than 50% in the number of spikes comparedwith the prestimulus frequency, for at least three consecutivebins. The duration of an inhibitory response corresponds to thetime interval during which no spike wasobserved.

The electrical stimulation of the PL/MO areas, ipsilateral to the recording site in the SNR, was performed through a coaxialstainless steel electrode (diameter, 400 µm; tip-barrel distance,300 µm) positioned stereotaxically [anterior (A), 12.7; lateral(L), 0.6; height (H), 5.5 mm from the interaural line] accordingto the atlas of Paxinos and Watson (1986). Electrical stimuliconsisted of monopolar pulses of 0.6 msec width and 200-600 µAintensity delivered at a frequency of 1.4Hz.

At the end of each recording session, the tip of the stimulating electrode was marked by an electrical deposit of iron (15µA anodal, 20 sec) and observed on histological sections aftera ferri-ferrocyanide reaction. The tip of the recording electrodewas marked by iontophoretic ejection of Pontamine Sky Blue (8µA cathodal, 20 min), allowing the determination of the positionof the recorded cells. Brains were removed and fixed in a 10%formalin solution, and the positions of electrodes were microscopicallyidentified on serial frozen sections (100 µm) stained withsafranin.

Drug applications. Pharmacological blockade of the glutamatergic transmission in the NAcc and the VP or of the GABAergic transmissionin the VP was performed by local application of 6-cyano-7-nitroquinoxaline-2,3-dione(CNQX) and bicuculline, respectively. CNQX (500 µM; Research Biochemicals,Natwick, MA) and bicuculline (500 µM; Sigma, St Louis, MO) wereapplied through a microdialysis probe (CMA 102; MicrodialysisAB, Stockholm, Sweden; membranes, 0.5 × 2 mm). The probe was positionedstereotaxically into the NAcc (A, 10.7; L, 1.7; H, 2.1) or theVP (A, 8.7; L, 2.5; H, 1.4) according to the atlas of Paxinosand Watson (1986). At the beginning of each experiment, the probewas perfused with a Ringer's phosphate solution (in mM: NaCl,120; KCl, 4.8; CaCl₂, 1.2; MgCl₂, 1.2; NaH₂PO₄, 15.6) using aCMA 102 microinjection pump at a flow rate of 2 µl/min. When aSNR cell responding to PL/MO stimulation was recorded, a peristimulustime histogram (100 stimuli) corresponding to the control situationwas generated. Then, the antagonist solution was perfused. Theactivity of the same cell was continuously recorded and, eachfifth minute, its response to PL/MO stimulation was monitored,and a peristimulus time histogram was generated. The blockadeof synaptic transmission was considered to be effective when nigralresponses evoked by PL/MO stimulation were increased or decreasedby at least 50%. The tested drug was then washed out by perfusionwith the Ringer's phosphate solution, and the same cell was recordeduntil the recovery of the control response. The blockade of theglutamatergic transmission in the STN was performed by a 1 mindelivery of a saline solution containing CNQX (1 mM, pH 7.0; 0.3µl) through a cannula (diameter, 400 µm) stereotaxically positionedinto the STN (A, 5.2; L, 2.2; H, 1.7). Peristimulus time histogramsof nigral responses evoked by PL/MO stimulation were generatedbefore and after the receptor antagonist application, and thedata were analyzed as mentioned above. When more than one cellwas tested in the same animal, drug applications were separatedby at least 2 hr after the recovery of the control response inthe precedingcell.

Student's t test (two-tailed) was used to compare excitatory and inhibitory responses observed before and after drugapplication.

  RESULTS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Effects of PL/MO stimulation on the activity of SNR cells

Responses evoked by electrical stimulation of PL/MO areas were investigated in 156 SNR cells recorded in 11 rats. As shownin Figure 1 and Table 1, PL/MO stimulation induced, in 80 cells,an inhibition preceded or not by an early excitation and followedor not by a late excitation. In 30 cells (37.5%), responses consistedof an inhibition [latency (L), 20.2 ± 0.5 msec; duration (D),14.5 ± 1.0 msec] preceded by an early excitation (L, 8.6 ± 0.4msec) and followed by a late excitation (L, 37.8 ± 1.1 msec).In eight cells (10%), the inhibition (L, 19.3 ± 2.0 msec; D, 16.1± 2.5 msec) was not preceded by an early excitation but was followedby a late excitation (L, 36.6 ± 2.2 msec). In 32 cells (40%),the inhibition (L, 23.0 ± 0.6 msec; D, 24.9 ± 2.0 msec) was precededby an early excitation (L, 8.7 ± 0.4 msec) but was not followedby a late excitation. An inhibition without early or late excitationswas observed in 10 cells (12.5%; L, 22.9 ± 1.1 msec; D, 23.0 ±4.5 msec). Interestingly, the inhibition was significantly shorter(40.2%; p < 0.001) in cells with a late excitation (D, 14.6 ±0.8 msec) than in cells without a late excitation (D, 24.4 ± 1.8msec).

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Figure 1. Patterns of responses evoked by PL/MO stimulation within SNR cells. The inhibition is preceded by an early excitation and is followed (A) or not (B) by a late excitation; the inhibition is not preceded by an early excitation and is followed (D) or not (C) by a late excitation.


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Table 1. Characteristics of the responses evoked by PL/MO stimulation within SNR cells

All these responding cells were located in the dorsomedial part of the SNR (Fig. 2). Within this SNR region, no obvious topographicaldistribution of the cells with distinct types of responses couldbe observed. In addition, it should be noted that in 6 of the156 cells tested, an excitation with a mean latency of 25.4 ±1.7 msec was observed instead of an inhibition. Finally, cellswith no response to PL/MO stimulation (70 of the 156 cells tested)were mainly located more laterally and ventrally in the SNR.

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Figure 2. Localization of SNR cells that responded to PL/MO stimulation. Note that responding cells are located in the medial part of the SNR, whereas more laterally located cells do not respond to PL/MO stimulation (Not responding cells). Each dot represents a tested cell. Numbers indicate the distance, in millimeters, from the interaural line. cp, Cerebral peduncle; ml, medial lemniscus; SNC, substantia nigra pars compacta.

Effect of CNQX application into the NAcc on nigral responses evoked by PL/MO stimulation

The effect of a blockade of the glutamatergic cortico-striatal transmission by application of CNQX into the NAcc was examinedin 13 SNR cells (eight rats) exhibiting a response to PL/MO stimulation.In control conditions, these cells presented the following patternsof responses: excitation-inhibition-excitation (four cells), excitation-inhibition(six cells), inhibition only (two cells), and inhibition-excitation(onecell).

In all these cells, the inhibition disappeared 8-25 min after the beginning of CNQX application (Fig. 3). In eight cells heldlong enough, the recovery of the inhibition occurred 25-65 minafter the cessation of CNQX application. In addition, the lateexcitatory response observed in five cells in control conditionswas markedly reduced under CNQX, with the maximal effect (63-97%decrease; p < 0.001) being observed 10-25 min after the beginningof the drug application (Fig. 3). In the three cells held longenough, the recovery of the late excitatory response was observed40-65 min after the cessation of drug application. In contrast(Fig. 3), the CNQX treatment did not modify the early excitationthat preceded the inhibition (10 cells).

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Figure 3. Effect of CNQX application into the NAcc on the response evoked by PL/MO stimulation in an SNR cell. From top to bottom, The response exhibited a triphasic excitation-inhibition-excitation sequence in control conditions; under CNQX application into the NAcc, the early excitation was not affected, the inhibition disappeared, and the late excitation was markedly decreased. The maximal effect was observed 10 min after the beginning of CNQX application, and the recovery of the inhibition and of the late excitation occurred 40 min after the cessation of CNQX application. Each poststimulus time histogram represents 100 superimposed sweeps. Arrow indicates the stimulation artifact.

Effect of bicuculline application into the VP on nigral responses evoked by PL/MO stimulation

Bicuculline was applied into the VP to block the GABAergic transmission of the NAcc-VP pathway. The effect of bicucullineon the responses evoked by PL/MO stimulation was examined in 10cells (eight rats). In control conditions, PL/MO stimulation inducedan inhibition preceded by an early excitation and followed bya late excitation. In 9 of these 10 cells, bicuculline markedlyreduced the late excitation, with the maximal effect (70-100%decrease; p < 0.001) being observed 8-35 min after the beginningof the drug application (Fig. 4). In eight cells held long enough,the recovery of the late excitation occurred 40-75 min after thecessation of bicuculline application. Interestingly, the disappearanceof the late excitation was associated with a significant increasein the duration of the inhibition (control conditions: D, 15.8± 0.5 msec; bicuculline treatment: D, 24.4 ± 2.8 msec; mean increase,54%; p < 0.01) without a significant change of the latency (control:L, 20.7 ± 0.6 msec; bicuculline: L, 21.3 ± 0.6 msec). Finally,bicuculline treatment did not affect the early excitatory response(Fig. 4).

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Figure 4. Effect of bicuculline application into the VP on the response evoked by PL/MO stimulation in an SNR cell. From top to bottom, The response exhibited a triphasic excitation-inhibition-excitation sequence in control conditions; under bicuculline application into the VP, the early excitation was not modified, the duration of the inhibition was slightly increased, and the late excitation was markedly decreased. The maximal effect was observed 10 min after the beginning of bicuculline application, and the recovery of the late excitation occurred 60 min after the cessation of bicuculline application. Each poststimulus time histogram represents 100 superimposed sweeps. Arrow indicates the stimulation artifact.

Effect of CNQX application into the VP on nigral responses evoked by PL/MO stimulation

CNQX was applied into the VP to block the glutamatergic input from the STN and thus to investigate the possible influenceof the subthalamo-pallidal loop on nigral responses evoked byPL/MO stimulation. In control conditions, the patterns of responsesobserved in the six SNR cells tested (four rats) were as follows:excitation-inhibition-excitation (five cells) and inhibition-excitation(one cell). In all cells, CNQX treatment markedly enhanced thelate excitatory response (Fig. 5). The duration of the late excitationincreased from 13.0 ± 1.7 msec (control conditions) to 31.2 ±2.8 msec (under CNQX; p < 0.001), although its latency was slightlydecreased (control: L, 37.5 ± 1.1 msec; CNQX: L, 34.0 ± 1.0 msec;p < 0.05). The maximal effect (67-410% increase in the numberof spikes during the excitatory period) occurred 15-35 min afterthe beginning of CNQX application, and a recovery of the responsewas observed 70-85 min after the cessation of the drug applicationin the three cells held long enough. Interestingly, this CNQXtreatment slightly reduced the duration of the inhibition (control:D, 13.8 ± 1.2 msec; CNQX: D, 10.5 ± 1.0 msec; p < 0.05). Finally,the CNQX application did not significantly modify the early excitatoryresponse recorded in control conditions (five cells).

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Figure 5. Effect of CNQX application into the VP on the response evoked by PL/MO stimulation in an SNR cell. From top to bottom, The response exhibited a triphasic excitation-inhibition-excitation sequence in control conditions; under CNQX application into the VP, the early excitation was not significantly modified, the inhibition was still observed, and the late excitation was markedly increased. The maximal effect was observed 20 min after the beginning of CNQX application, and the recovery of the late excitation occurred 75 min after the cessation of CNQX application. Note that the duration of the inhibition and the latency of the late excitation were decreased under CNQX. Each poststimulus time histogram represents 100 superimposed sweeps. Arrow indicates the stimulation artifact.

Effect of CNQX application into the STN on nigral responses evoked by PL/MO stimulation

The effect of blockade of the glutamatergic cortico-subthalamic transmission by CNQX injection into the STN was examined ineight SNR cells (six rats) exhibiting a response to PL/MO stimulation.In control conditions, the responses evoked by PL/MO stimulationconsisted of an inhibition preceded by an early excitation (eightcells) and followed (six cells) or not (two cells) by a late excitation.In all cases, the CNQX injection markedly decreased the earlyexcitation (Fig. 6). The maximal effect (52-91%) was observed5-10 min after the drug application, and the recovery of the responseoccurred 35-50 min later in the five cells held long enough (Fig.6). In addition, CNQX increased the duration of the inhibition(control: D, 20.0 ± 3.8 msec; CNQX: D, 44.5 ± 9.8; p < 0.05) andinduced a disappearance of the late excitation (six cells).

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Figure 6. Effect of CNQX application into the STN on the response evoked by PL/MO stimulation in an SNR cell. From top to bottom, The response exhibited a triphasic excitation-inhibition-excitation sequence in control conditions; under CNQX application into the STN, the early excitation was markedly decreased, the duration of the inhibition was increased, and the late excitation disappeared. The maximal effect was observed 10 min after the CNQX application, and the recovery occurred 50 min after CNQX application. Each poststimulus time histogram represents 100 superimposed sweeps. Arrow indicates the stimulation artifact.

  DISCUSSION

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Our results indicate that the electrical stimulation of PL/MO areas of the rat prefrontal cortex induces in the SNR complexpatterns of responses composed of an inhibition preceded or notby an early excitation and followed or not by a tardive excitation.These patterns of responses are similar to those described afterstimulation of the sensorimotor frontal agranular cortex in therat (Fujimoto and Kita, 1993; Ryan and Sanders, 1994). The presentpharmacological data allowed the determination of the respectivecontribution of the trans-striatal and trans-subthalamic circuitsin the nigral responses evoked by PL/MO stimulation (Fig. 7).

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Figure 7. Schematic representation of the pathways involved in the SNR responses to prefrontal cortical stimulation. Broken and solid lines represent glutamatergic and GABAergic pathways, respectively. Bottom, Example of a complex response evoked in an SNR cell by stimulation of PL/MO areas of the prefrontal cortex. The early excitation is caused by the activation of the disynaptic cortico-STN-SNR pathway, the inhibition results from the activation of the direct NAcc-SNR pathway, and the late excitation involves the indirect NAcc-VP-STN-SNR pathway, which operates via disinhibition of the STN.

Role of the disynaptic cortico-subthalamo-nigral pathway

The cortico-subthalamic and subthalamo-nigral projections are glutamatergic and form asymmetrical synaptic contacts with theirtarget neurons in the STN and the SNR (Smith et al., 1998). Basedon the conduction time of these projections, it has been proposedthat short latency excitations evoked in SNR cells by stimulationof the sensorimotor cortex are mediated through the disynapticcortico-subthalamo-nigral pathway (Kita, 1994). Accordingly, theearly excitations evoked in the SNR by frontal agranular cortexstimulation are no longer observed after excitotoxic lesion ofthe STN (Ryan and Sanders, 1994). Our data indicate the existenceof a similar functional link between PL/MO areas and the medialSNR. Indeed, the latency of the early excitatory responses evokedby PL/MO stimulation in SNR cells is in the range of the conductiontime of the disynaptic cortico-subthalamo-nigral pathway, andPL/MO stimulation induces a short latency excitation in STN cellsprojecting to the SNR (Maurice et al., 1998b). In addition, theearly nigral excitatory responses evoked by PL/MO stimulationdisappeared after CNQX application into the STN but persistedafter the blockade of the cortico-NAcc transmission. This effectcannot be attributed to a diffusion of CNQX into the SNR because,in contrast to the reduced firing of nigral cells reported afterlocal application of glutamatergic antagonists into the SNR (Robledoand Féger, 1990), the spontaneous activity of SNR cells was notmodified (20.6 ± 3.4 Hz, before CNQX; 19.2 ± 2.2 Hz, underCNQX).

Role of the direct NAcc-SNR pathway

We have previously shown the existence of a functional link between the PL/MO areas and the NAcc neurons that innervate theSNR. Indeed, stimulation of PL/MO areas induces excitatory responsesin NAcc neurons projecting to the SNR (Montaron et al., 1996),and stimulation of the NAcc inhibits the activity of SNR cells(Deniau et al., 1994). The present data demonstrate that the inhibitoryresponses observed in SNR cells after PL/MO stimulation resultfrom the activation of the direct NAcc-SNR pathway: (1) the inhibitoryresponses have a latency compatible with the conduction time ofthe PL/MO-NAcc-SNR pathway and a duration similar to that observedafter NAcc stimulation (Deniau et al., 1994); (2) the inhibitoryresponses were observed in cells located in the dorsomedial partof the SNR, in agreement with the distribution of NAcc projections(Montaron et al., 1996); and (3) finally, the inhibitory responsesdisappeared after acute blockade of the glutamatergic cortico-striatalneurotransmission by CNQX application into the NAcc, althoughthey persisted after blockade of the striato-pallidal or cortico-subthalamictransmissions. It should be noted that the duration of CNQX applicationrequired to obtain a maximal effect in the SNR presented somevariability. This is likely to be related to the diffusion timenecessary for CNQX to produce a blockade of the synaptic transmissionin the whole NAcc territory involved in the PL/MO-NAcc-SNRcircuit.

Role of the indirect NAcc-SNR pathway

The indirect striato-nigral pathway, involving the external pallidum and the STN, has been proposed to exert an excitatoryinfluence on the SNR (Alexander et al., 1986). Activation of striato-pallidalneurons inhibits the tonic discharge of the GABAergic pallidalneurons that project to the STN and consequently should lead toa disinhibition of STN. In turn, disinhibition of STN would resultin an increased firing of SNR cells because STN-SNR projectionsare glutamatergic andexcitatory.

The present data, along with our previous study (Maurice et al., 1998a), demonstrate that the late excitatory responses thatfollow the inhibition evoked in SNR cells by PL/MO stimulationare a result of the activation of the indirect NAcc-SNR pathwayand result from the disinhibition of the STN. Indeed, the latenigral excitatory responses disappeared after blockade of eithercortico-NAcc transmission by CNQX application into the NAcc orNAcc-VP transmission by bicuculline application into the VP. Thesetreatments have also been shown to block the disinhibition ofSTN cells evoked by PL/MO stimulation (Maurice et al., 1998a).In addition, the latency of the late excitatory responses is inthe range of the conduction time of the multisynaptic circuitlinking the PL/MO areas to the SNR via the indirect basal gangliapathway (Montaron et al., 1996; Maurice et al., 1997, 1998a,b).

Role of the STN-VP-STN loop

The STN and pallidum are two tightly interconnected structures, and pallido-subthalamic connections are topographically organizedsuch that the GP and VP project to the STN region from which theyreceive an input (Groenewegen and Berendse, 1990; Smith et al.,1998). Electrophysiological data suggest that activation of STNcells projecting to the pallidum by cortical inputs leads to afeedback inhibition of the STN (Ryan and Clarke, 1991; Fujimotoand Kita, 1993). Confirming this hypothesis, we have recentlyshown that disinhibition of STN cells by PL/MO stimulation ismarkedly increased after blockade of the STN-VP glutamatergictransmission by CNQX application into the VP (Maurice et al.,1998a). The present data show that the late excitatory responsesinduced by PL/MO stimulation in SNR cells are also markedly increasedafter CNQX application into the VP. Together, these data indicatethat the VP-STN feedback circuit modulates the late excitatoryresponses of SNR cells to PL/MO stimulation and further confirmthat these late excitations result from the disinhibition of theSTN.

Functional considerations

The terminals from the striatal and subthalamic afferent pathways form convergent synaptic contacts with individual neuronsin the SNR (Smith et al., 1998). Accordingly, the present electrophysiologicalstudy shows that the trans-striatal and trans-subthalamic pathwaysrelated to PL/MO areas of the prefrontal cortex exert a convergingsynaptic influence on medial SNR cells. In addition, our dataindicate that the inhibition exerted by the direct NAcc-SNR pathwayon nigral cells is under the control of the trans-subthalamicpathways. The duration of this inhibition was decreased afterCNQX application into the VP, a treatment that blocks the feedbackSTN-VP-STN inhibitory loop and thus enhances the disinhibitionof the STN. In contrast, the duration of the inhibition was increasedafter bicuculline application into the VP, which blocks the disinhibitionof the STN and consequently the late excitatory responses in theSNR. A more prolonged lengthening of the inhibition was observedafter CNQX application into the STN, which blocks the cortico-subthalamicpathway. The marked lengthening of the inhibition cannot justbe explained by the concomitant disappearance of the late excitatoryresponses but is likely to result from an increased inhibitoryinfluence of the direct NAcc-SNR pathway. Because the VP receivesexcitatory inputs from the STN and sends GABAergic projectionsto the NAcc (Groenewegen et al., 1993), the blockade of the glutamatergicexcitatory inputs to STN might lead to a disinhibition of theNAcc and thus would facilitate the activation of the NAcc-SNRpathway by PL/MO stimulation. On the other hand, the presenceof metabotropic glutamate receptors of the group III (mGluR7)on GABAergic terminals in the SNR have recently been described(Kosinski et al., 1998). Assuming a presynaptic inhibitory influenceof mGluR7 on transmitter release (Conn and Pin, 1997), it canbe proposed that blockade of the activation of the glutamatergicsubthalamo-nigral pathway by CNQX application into the STN couldhave reduced the inhibitory effect of mGluR7 receptors on GABArelease, resulting in an increased inhibitory influence of thedirect NAcc-SNRpathway.

In motor circuits of the basal ganglia, the activation of the direct striato-nigral GABAergic pathway, by inhibiting the tonicallyactive GABAergic projection neurons of the SNR, leads to a disinhibitionof their target nuclei in thalamus and brainstem (Chevalier andDeniau, 1990). This disinhibitory process very likely increasesthe excitability of the frontal cortex and is central to the physiologyof the basal ganglia. It has been proposed that the trans-subthalamicpathways, by their excitatory influence on the SNR, participatein the spatio-temporal shaping of this disinhibitory process andthus contributes to the scaling of movements and inhibition ofcompeting motor programs (Mink and Thach, 1993). An imbalancebetween the direct striato-nigral and the trans-subthalamic pathwaysis considered to be responsible for motor disorders, such as akinesiaand dyskinesia (Albin et al., 1989; Chesselet and Delfs, 1996;Obeso et al., 1997). Similarly, in the PL/MO circuits of the basalganglia, the present data show that SNR cells receive a directinhibitory input from the NAcc and that the trans-subthalamicexcitatory pathways participate in the shaping of the dischargeof nigral output neurons. By analogy with motor circuits, it canbe proposed that an imbalance between these pathways could beresponsible for perturbation in prefrontal functions, such asperseveration and alterations in attentional and emotionalprocesses.

  FOOTNOTES

Received Jan. 19, 1999; revised March 18, 1999; accepted March 23, 1999.

This work was supported by Institut National de la Santé et de la Recherche Médicale. N.M. is a recipient of a fellowshipfrom the Ministère de l'Enseignement Supérieur et de la Recherche.We thank A. M. Godeheu and M. Saffroy for histological assistanceand L. Darracq for his advice in the microdialysistechnique.
Correspondence should be addressed to Dr. Anne-Marie Thierry, Chaire de Neuropharmacologie, Institut National de la Santéet de la Recherche Médicale U114, Collège de France, 11 placeMarcelin Berthelot, 75231 Paris Cedex 05,France.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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