Reappraisal of the Motor Role of Basal Ganglia: A Functional Magnetic Resonance Image Study

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The Journal of Neuroscience, April 15, 2003, 23(8):3432

Reappraisal of the Motor Role of Basal Ganglia: A Functional Magnetic Resonance Image Study
Takayuki Taniwaki¹^,^*, Akira Okayama¹^,²^,^*, Takashi Yoshiura³, Yasuhiko Nakamura³, Yoshinobu Goto¹, Jun-ichi Kira², and Shozo Tobimatsu¹
Departments of ¹ Clinical Neurophysiology, ² Neurology, and ³ Clinical Radiology, Graduate School of Medical Sciences, Kyushu University, Fukuoka 812-8582, Japan

  ABSTRACT

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

The importance of the basal ganglia in controlling motor function is well known. However, neuroimaging studies have failedto show either movement-rate dependence or different activationpatterns caused by self-initiated (SI) and externally triggered(ET) movements in the basal ganglia-thalamo-motor loop. We hereinreport the functional magnetic resonance image (fMRI) mappingof sequential left-hand finger movements at five different ratesunder SI and ET conditions. Significant movement-rate dependencewas found in the whole right basal ganglia-thalamo-motor looponly during the SI task. Network analysis also showed strong interactionswithin this loop during SI movement, whereas interactions werepresent only from the premotor cortex to the putamen via the sensorimotorcortex during the ET task. Furthermore, psychophysiological interactionanalysis confirmed the different modulation between the two tasksin the putamen. fMRI provides evidence that the basal ganglia-thalamo-motorloop plays a key role in controlling the rate of sequential fingermovements in SI movement but not in ETmovement.

Key words: basal ganglia; fMRI; motor control; self-initiated movement; externally triggered movement; movement rate; path analysis

  Introduction

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

The role of the basal ganglia in controlling motor function remains enigmatic despite considerable advances in the understandingof the pathophysiology of movement disorders (Brooks, 2000). Thebasal ganglia have been assumed to control the velocity of movementpartly because of the bradykinesia seen in patients with Parkinson'sdisease (PD) (Hallett and Khoshbin, 1980) and electrophysiologicalstudies in nonhuman primates (Georgopoulos et al., 1983; Mitchellet al., 1987; Hamada et al., 1990). Previous imaging studies,however, failed to show a correlation between movement rate andactivity of the basal ganglia (Blinkenberg et al., 1996; Sadatoet al., 1996; Jenkins et al., 1997). These findings provide evidencethat basal ganglia do not play a significant role in the decisionof movement rate (Brooks, 1995, 2000). The tasks used in previousstudies were externally cued movements rather than self-pacedsequential movements. PD patients experience great difficultyin volitional sequential movements (Benecke et al., 1987), althoughexternal cues improve their performance (Georgiou et al., 1994).Consequently, the basal ganglia seem to be activated more by sequentialor internally cued movement than by repetitive or externally cuedmovement. Non-dominant hand movement caused a greater recruitmentof striatum than that of dominant hand in sequential finger movement(Mattay et al., 1998). Thus, the effects of sequential and internallycued movement in the non-dominant hand must be investigated toelucidate the physiological role of the basal ganglia in movementrate and volitionalmovement.

Discrepancies in the performance of PD patients suggest that the basal ganglia may be differently involved in self-initiated(SI) and externally triggered (ET) movements (Benecke et al.,1987; Georgiou et al., 1994). Electrophysiological studies inmonkeys have suggested that the basal ganglia-supplementary motorarea (SMA) projection is more involved in SI movement, whereasthe cerebellum-lateral premotor cortex (PM) projection is moreimportant in ET movement (Romo and Schultz, 1987; Mushiake etal., 1991; Middleton and Strick, 2000). However, only a few imagingstudies have reported the differential activation of the basalganglia between SI and ET movements (Menon et al., 1998; Cunningtonet al., 2002). Neither study investigated the function of thecortico-subcortical loops, nor did they describe the role of basalganglia in the movement. Thus, the role of the basal ganglia inSI movement remainsunknown.

In this study, we investigated the regional cerebral activation by functional magnetic resonance image (fMRI) during sequentialleft-hand finger movements at five different rates in SI or ETmovement. We focused on motor-related regions, particularly thebasal ganglia-thalamo-motor loop. The aims of the present studywere (1) to study the correlation between the activity of thebasal ganglia and rates of sequential finger movements duringSI and ET movements; (2) to construct a functional network toaccount for correlation in the basal ganglia-thalamo-motor loop;and (3) to compare the functional network model of SI movementwith that of ET movement to elucidate the physiological role ofthe basalganglia.

  Materials and Methods

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ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

Participants. Ten healthy male volunteers (age range, 24-29 years) participated in the study. All subjects were strongly right-handedas assessed by a modified version of the Edinburgh handednessinventory (Oldfield, 1971). All subjects gave informed writtenconsent.

Experimental design. We showed the subjects how to move each finger with changing movement rates. They were required to practicethe task before the scan until they were able to perform it atconstant amplitude without error. They were also instructed tokeep their eyes closed during MRI. The activation paradigm consistedof a sequential movement performed with the left hand. To performthis task, the subjects had to (1) make finger-to-thumb oppositionmovements in the order of index, middle, ring, and little finger;(2) open and clench the fist twice; (3) complete finger-to-thumbopposition in the opposite order (i.e., little, third, middle,and index finger); (4) open and clench the fist twice again; and(5) repeat the same series of movements during the 40 sec of dataacquisition (Sabatini et al., 2000). Each finger-to-thumb oppositionmovement and a pair of open and clench the fist movements wascounted as a single movement. In the SI task, movement rates wereset at very slow (as slow as possible), slow, moderate (comfortablepace), fast, very fast (as fast as possible). During the practicesession, movement rates were ~0.5 Hz at very slow and near 4.0Hz at very fast in most of the subjects. In the ET task, therefore,movement rates were set at 0.5, 1, 2, 3, or 4 Hz. Subjects pacedtheir movements in response to a metronome, which consisted ofa clicking sound at precise time intervals and was delivered binaurallyto the subject via air conduction through a pair of plastic tubes2.5 m in length. During the rest condition, subjects lay downwhile listening to the metronome used in the ET session. Movementswere performed for 40 sec (activation) at a constant rate, followedby 40 sec of rest (baseline), and were switched by a voice signal.Movement rate conditions were presented in pseudorandom orderwithin an imaging series. As a consequence, there were a totalof five baseline/activation (five different rates) cycles perimaging series. Four consecutive imaging series (two SI and twoET) were conducted per subject. Finger movements were analyzedvisually through a TV monitor, and exact movement rates weredetermined.

fMRI methods. Images were acquired on a 1.5 tesla Magnetom SYMPHONY (Siemens, Enlangen, Germany) whole-body MRI system equippedwith a circular polarized volume head coil. Initially, a set oflocalized images was acquired to position the image slice. Foreach session, 100 EPI multislice data sets were acquired (echotime 50 msec; repetition time 4 sec; flip angle 90°; acquisitiontime for the whole paradigm, 400 sec). Each multislice data setcontained 32 transverse slices (slice thickness 3.0 mm; interslicegap 1.0 mm; matrix 64 × 64; field of view 23 cm). All images wereanalyzed using Statistical Parametric Mapping 99 Software (WellcomeDepartment of Cognitive Neurology, London, UK) (Friston et al.,1995). The first three data sets of each time series were discarded,and the remaining EPI volumes were then realigned to the firstvolume. Data sets (one SI and one ET from each subject) were thenchosen for their high quality as demonstrated by small motioncorrections (<1 mm along each axis). The images were spatiallynormalized to a standard template and smoothed with a Gaussiankernel of 8 mm full-width at half-maximum. The design matrix wasset using the box-car reference waveform (40 sec epoch). The timeseries in each voxel were high-pass filtered (160 sec cutoff)and scaled to a grand mean of 100 over voxels and scans withineach session. Using a parametric approach, three different rate-responserelationships could be identified: (1) categorical on-off responsesbased on the difference between finger movement and resting conditionsregardless of movement rate (zero order term), (2) linear responsesin parallel with movement rate (first order term), and (3) nonlinearrelationships (second order term) (Buchel et al., 1996, 1998).

A general linear model was applied to reveal the voxel-wise effects of tasks (zero order term) and the changes in these effectsacross scans (first and second order). A statistical parametricalmap (SPM) of the F-static SPM{F} for the group data were generatedfor this general linear model. For group analysis, we used multi-subject,fixed-effect analysis. The threshold for significance was setat p < 0.05 corrected (F_(1,623.7) > 25.05). fMRI signal changewas calculated at the local maxima (the voxel with peak F value)in the activated regions within the basal ganglia-thalamo-motorloop from the conjunction analysis. For the voxels thus identified,the percentage signal changes were extracted for different orderterms per movement rate across each subject and were plotted againstthe rates of movement. Pearson's correlation coefficient was calculatedto examine a linear correlation between the movement rate andfMRI signal change at each assigned activatedregion.

Network analysis. To construct a functional network to account for correlation in the basal ganglia-thalamo-motor loop, interregionalcorrelation was calculated on the basis of data for the correlationbetween movement rate and fMRI signal change. Individual dataof signal changes from five different movement rates were cross-correlatedon a region by region basis using a Pearson product moment correlation.Each of the selected regions was centered on the stereotacticcoordinates of the local SPM{F} maximum detected in the relevantanatomical region [i.e., right putamen, right thalamus, SMA, rightsensory motor cortex (SMC), and right PM] as described above.The selected regions are presented in Table 2. The connectionsbetween these areas are based on the modified model reported previously(Grafton et al., 1994). The movement-related correlation matriceswere used to calculate path coefficients as defined in Figure4 using a path analysis, implemented with the software LISREL(Scientific Software, Chicago IL), as described previously (Graftonet al., 1994; McIntosh and Gonzalez-Lima, 1994; McIntosh et al.,1994). A maximum likelihood algorithm was used to fit parameters.Typical fits required only 4 or 14 iterations to obtain stablesolutions. The model fit was good because Bollen's fit index was0.938 in SI and 0.998 in ET, respectively (Bullmore et al., 2000).

Psychophysiological interaction analysis. To confirm the results of network analysis, psychophysiological interaction analysiswas used (Friston et al., 1997). The design matrix representeda factorial design in a parametric context with two factors (SIversus ET and five rates of movements). Movement rates were setas typical mirror symmetry (i.e., positive linear for SI and negativelinear for ET) between SI and ET. We selected a reference region,which showed significant positive linearity between movement ratesand signal change during SI in the design matrix as describedabove: the right putamen (x, y, z = 26, $-$ 6, 12; Z = 4.02; p <0.0001). The covariates consisted of the group effect (mirrorsymmetry between SI and ET) and signal change of the referenceregion. The analysis looked for the brain regions within SMA andright thalamus with activities that were modulated differentlyin SI compared with ET. Multi-subject, fixed-effect analysis wasused for group analysis. The resulting set of voxel values foreach contrast, constituting an SPM of the t-static SPM{t}, wastransformed to the unit normal distribution SPM{Z} and thresholdedat p = 0.05, corrected (Z > 4.80). If the activities in theseregions were modulated separately for the two tasks, there shouldbe an interaction in term of the difference in the regressionslope between the two tasks. Analysis of covariance (ANCOVA) wasused to compare the slope bytask.

  Results

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ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

Performance of subjects

In general, the subjects showed fairly good performance in SI movements. Very slow movements were performed at the frequencyof 0.64 ± 0.24 Hz (mean ± SD), slow movements at 1.02 ± 0.32 Hz,moderate movements at 1.79 ± 0.47 Hz, fast movements at 3.05 ±0.61 Hz, and very fast movements at 4.27 ± 0.73 Hz, respectively.ET movement rates were almost identical to the rate of the auditorytrigger (0.5 Hz trigger, 0.50 ± 0.00 Hz; 1.0 Hz trigger, 1.00± 0.01 Hz; 2.0 Hz trigger, 2.00 ± 0.04 Hz; 3.0 Hz trigger, 3.00± 0.03 Hz; 4.00 Hz trigger; 4.00 ± 0.04 Hz). The rates of theSI and ET movement were very similar without statistically significantdifferences (p = 0.438; two-way ANOVA with repeatedmeasures).

Foci of activation

To separate the regional activity within the same task but at different rate-response functions, a parametric approach basedon orthogonal basis functions up to the second order was used.In the study of categorical on-off response, both tasks causedsignificant activation at the right posterior putamen, right thalamus,SMA, right primary SMC, and right PM (Table 1; Figs. 1a,b, 2a,b).


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Table 1. Parametric analysis of rate-dependent BOLD effects

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Figure 1. Statistical parametric maps showing the sites of significant hemodynamic responses (threshold at p < 0.05, corrected). These areas are projected onto single sagittal, coronal, and transverse planes. a, b, Categorical on-off responses across all movement rates and subjects. c, d, Parametric responses characterized by linear effect. a, c, Self-initiated movement. b, d, Externally triggered movement. R, Right; L, left.

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Figure 2. Areas of subcortical activation (p < 0.05, corrected) located within the right putamen for self-initiated (a, c) and externally triggered movements (b, d). a, b, Categorical on-off responses across all movement rates and subjects. c, d, Parametric responses characterized by linear effect. R, Right; L, left.

A significant linear relationship between the measured hemodynamic responses and the movement rate was evident at the rightposterior putamen, right thalamus including the ventrolateraland ventroanterior nuclei, SMA, right SMC, and right PM duringthe SI task. In the ET task, a significant linear relationshipwas found only at the right SMC and right PM (Table 1; Figs.1c,d, 2c,d).

A significant nonlinear rate-response function was observed only at the cingulate cortex (F_(1,614) = 36.28; p < 0.001; x,y, z = $-$ 4, 8, 34) in the ETtask.

Movement rate and fMRI signal change

To confirm the linear relationship between the activation of the basal ganglia-thalamocortical loop and the rate of sequentialfinger movement, fMRI signal changes were plotted against therate of finger movement for activated areas identified from thefirst order term (Fig. 3). This was done for the right putamen,right thalamus, SMA, right SMC, and right PM during the SI task,and for the right SMC and right PM during the ET task. In otherstructures, the fMRI signal changes were plotted for the areasfrom the zero order term. During the SI task, a strong positivecorrelation was found at the right posterior putamen (r = 0.715;p < 0.001), right thalamus (r = 0.684; p < 0.001), and right SMC(r = 0.751; p < 0.001). A moderate positive correlation was observedat the SMA (r = 0.510; p < 0.001), whereas a weak positive correlationwas noted at the right PM (r = 0.393; p = 0.005). During the ETtask, a strong positive correlation was found at the right SMC(r = 0.721; p < 0.001) and right PM (r = 0.677; p < 0.001). Therewas a weak positive correlation at the right putamen (r = 0.313;p = 0.027). No significant linear correlation was found at theright thalamus (r = 0.034; p = 0.810) and SMA (r = 0.164; p =0.256).

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Figure 3. Relationship between finger movement rates and fMRI signal change across each subject. a-c, Self-initiated movement. d-f, Externally triggered movement. SMC, Sensorimotor cortex.

Functional network analysis

During the SI movement task, there was a strong positive correlation between movement rate and fMRI signal change within thebasal ganglia-thalamo-motor loop; therefore, this loop appearedto play a significant role in rate-dependent motor processing.To confirm this hypothesis, functional network analysis was performedwithin theloop.

First, we constructed the correlation matrix of fMRI signal changes. Among the activated areas, Table 2 shows the inter-regionalcross-correlation within the basal ganglia-thalamo-motor loopobtained from both tasks. Estimates of path coefficients duringSI and ET finger movements are summarized in Table 3. Regionalinteractions can be characterized by a path diagram as shown inFigure 4. In this diagram, the width of the arrows and the directionof arrowheads correspond to the strength of uni-directional coefficientsbut not bi-directional correlation. During SI finger movement,there was a strong positive interaction in the projection fromthe right putamen to the right thalamus. Moderate positive interactionswere found in the projection from the SMA to the right putamenand from the right thalamus to the right SMC. The overall patternof regional interactions showed a dramatic change during ET fingermovement. There was a strong positive interaction from the rightPM to the right SMC and a moderate interaction from the SMC tothe putamen. There were weak or no interactions among other structures.


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Table 2. Inter-regional correlation coefficients (Pearson product-moment correlation)


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Table 3. Path coefficients during two different tasks

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Figure 4. Results of LISREL parameter estimates during self-initiated and externally triggered movements. Positive coefficients (solid arrows) indicate interactions in which an increase of activity in one area is associated with an increase of activity in the other area. Negative coefficients (broken arrows) indicate an opposite interaction. Compared with externally triggered movement, self-initiated movement is associated with strong positive interaction of SMA-basal ganglia-thalamocortical projections to the SMC. Put, Right putamen; Thal, right thalamus; SMA, supplementary motor area; SMC, right sensorimotor cortex; PM, right premotor cortex.

Psychophysiological interaction analysis

Because parametric analysis showed a task-related difference in the right putamen, the right thalamus, and the SMA, psychophysiologicalinteraction analysis was performed among those regions. We demonstratedsignificant alteration in functional connectivity between theright putamen and SMA (x, y, z = 8, $-$ 14, 50; Z = 5.94) and alsobetween right putamen and the right thalamus (14, $-$ 10, 4; Z =5.06) (Fig. 5). A comparison of regression slope showed a differentfunctional relationship between the SMA and right putamen (p =0.0135 by ANCOVA) and also between the right putamen and the rightthalamus (p = 0.0055) during SI compared with ET (Fig. 5).

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Figure 5. SMA (a) and right thalamus (b) showing a significant increase in functional connectivity with right putamen in SI movement versus ET movement. R, Right; L, left. c, d, Scatterplots of the fMRI percentage signal changes in the right putamen (x, y, z = 26, $-$ 6, 12) versus SMA (8, $-$ 14, 50) (c) and the right putamen versus the right thalamus (14, $-$ 10, 4) (d) during SI () and ET ( $open circle$ ). Two regression lines (a solid line for SI and a broken line for ET) are overlaid in each group, and each line shows the percentage signal change per movement rate across each subject. Note that the slopes of regression lines are significantly different.

  Discussion

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

In an attempt to elucidate the motor role of the basal ganglia, we measured the regional activation of the basal ganglia-thalamo-motorloop using fMRI during sequential finger movements of SI and ETtasks. Our major new findings were as follows: (1) the signalintensity of the right posterior putamen increased in parallelwith the movement rate during the SI task; (2) path analysis basedon the rate-dependent fMRI signal changes showed strong interactionsin the basal ganglia-thalamo-motor loop during SI movement; and(3) interactions of the basal ganglia-thalamo-motor loop differedbetween SI and ET finger movements, which were confirmed by psychophysiologicalinteractionanalysis.

Putaminal activation and movement rate

Partly on the basis of the observation that PD patients have bradykinesia, it has been suggested that the basal ganglia playan important role in controlling the velocity of movements (Hallettand Khoshbin, 1980). One approach for determining whether specificbrain areas play a key role in mediating a specific function isto examine whether they show a significant correlation with thelevels of blood flow when such function is performed at differentintensities. Previous neuroimaging studies showed no correlationof lentiform regional cerebral blood flow (rCBF) with increasingmovement rates (Blinkenberg et al., 1996; Sadato et al., 1996;Jenkins et al., 1997). This suggests that the basal ganglia donot determine basic movement parameters (Brooks, 1995, 2000).Our current results showed that ET movement produced only weaklinear correlation between movement rate and activation of thebasal ganglia. In SI movement, however, we found a strong positivelinear relation between movement rate and putaminal activationfor the first time. This is consistent with the electrophysiologicaldata (Georgopoulos et al., 1983; Mitchell et al., 1987; Hamadaet al., 1990) and clinical observations in PD (Hallett and Khoshbin,1980) and supports the hypothesis that the basal ganglia playa significant role in determining the rate of SI sequentialmovement.

Previous neuroimaging studies have been performed using stereotyped finger-to-thumb oppositions (Sadato et al., 1996), fingertapping (Blinkenberg et al., 1996), or joystick movements (Jenkinset al., 1997), ranging in frequency from 0.25-4 Hz. The taskswere externally cued, nonsequential movements. The different tasksbetween the studies could explain the absence of rate-relatedactivation of the basal ganglia in the previous studies. Anotherimportant factor could be the anatomical difference of the activatedarea in the putamen. In our current results, the location of therate-related activation in the right putamen corresponds fairlywell with the posterior part of putamen related to somatomotorfunction (Alexander et al., 1990). Previous studies (Sadato etal., 1996; Jenkins et al., 1997), on the contrary, showed task-relatedactivation in the anterior part of putamen, which belongs to thenon-motor loop (Alexander et al., 1990).

Because our tasks were rather complicated, we speculated that not only the rate of movement but also the complexity of thetask could affect our results. Increasing sequence complexityshowed a positive correlation of rCBF in the anterior globus pallidus(GP), contralateral thalamus, pre-SMA, premotor cortex, parietalcortex, ipsilateral SMC, and cerebellum, but not in the contralateralSMC and posterior putamen (Boecker et al., 1998; Catalan et al.,1998; Haslinger et al., 2002). Thus, the activation of the contralateralposterior putamen, shown in our current results, is unlikely tobe caused by the complexity of the task. We conclude that a taskwith sequential and internally cued movement in the nondominanthand is useful to map the movement rate-dependent changes in thebasalganglia.

Basal ganglia-thalamo-motor loop

We investigated interactions among the basal ganglia-thalamo-motor loop during SI finger movements using path analysis. Thismethod has provided new insight into task-specific functionalnetworks (Grafton et al., 1994; McIntosh and Gonzalez-Lima, 1994;McIntosh et al., 1994). In addition, we used correlation databased on rate-dependent movement. This approach provides additionalinformation about brain physiology such as rhythm formation, motorpreparation, or motor execution that is not always apparent inthe results of categorical comparisons of fMRI data. At leastfive distinct parallel loops involving the basal ganglia are knownto exist (Alexander et al., 1990). These include a "motor" loopinvolving the SMA, primary motor cortex, putamen, GP, and ventrolateralthalamus. Recent studies in monkeys have shown that the motorloop appears to be divided into projections to (Middleton andStrick, 2000) or subloops in (Nakano et al., 2000) the SMC, SMA,and PM. These subloops arise from the cortical region, projectinto the internal part of the GP via the putamen, and finallyreturn to the cortex via the thalamus (Nakano et al., 2000). Onthe basis of this neuroanatomy, we constructed a modified functionalmodel of the reported network (Grafton et al., 1994) except forthe GP and subregions within the basal ganglia and thalamus, becausethe cluster of the right putamen was too large todiscriminate.

To our knowledge, we are the first to show a strong interaction in the whole loop during an SI task. There were strong positiveinteractions in the projection from the SMA to the putamen, fromthe putamen to the thalamus, and from the thalamus to the SMC.The SMA has been shown to be active during internally generatedautomated movements, movement preparation, movement sequencing,or performance of complex movements (Roland et al., 1980; Deiberet al., 1991; Halsband et al., 1993; Boecker et al., 1998). Thebasal ganglia can focus on and filter desired motor patterns duringmovement, optimizing them and inhibiting unwanted movements (Minkand Thach, 1991; Marsden and Obeso, 1994), and the SMC has beenthought to play a primary role in motor execution. Therefore,our results indicate that the SMA-putamen-thalamus-SMC pathwayplays a significant role in rate-dependent movement during SImovement. In other words, the basal ganglia-thalamo-motor loopappears to play a primary role in timing SImovement.

SI versus ET movements

Because patients with PD have difficulty especially with SI or volitional movements (Benecke et al., 1987), a potentiallypowerful method to investigate the motor function of the basalganglia is to examine the differences between SI and ET movements.Several imaging studies have examined the cerebral activationduring index finger extensions or arm movements that involvedSI or ET movements in neurologically normal subjects and showedno significant difference (Jahanshahi et al., 1995; Jenkins etal., 2000). A recent event-related fMRI study showed activationof the lentiform nucleus only during SI movement (Cunnington etal., 2002). Although the activation was bilateral, it was seenmore on the ipsilateral side, and the study failed to show clearactivation of the motor loop. Our network analysis was based onthe rate dependence; however, it showed that different systemsoperate during the two tasks. There were moderate to strong interactionsfrom the SMA to SMC via the putamen and thalamus on SI movement.In ET movement, apparent interaction was found only from the PMto SMC and from the SMC to putamen. Psychophysiological interactionanalysis confirmed the different modulation between the tasksin the basal ganglia. These results demonstrate that the basalganglia-thalamo-motor loop plays a significant role in SI movementbut not in ETmovement.

Many unit-recording studies in monkeys have been performed to compare SI and ET movements. Simple motor tasks caused movement-relatedactivity in the neurons of SMA, PM, and putamen during both SIand ET tasks. Pre-movement activities were observed mainly beforethe SI movement in SMA and putamen (Okano and Tanji, 1987; Romoet al., 1992). During the sequential movement, most of the SMAneurons were active in relation to SI during both pre-movementand movement periods, whereas PM neurons were more active in ET(Mushiake et al., 1991). Studies in the motor thalamus suggestedthat specific subcircuits within the basal ganglia-thalamocorticaland cerebella-thalamocortical pathways were clearly differentiatedby using SI and ET tasks (van Donkelaar et al., 1999, 2000). Therefore,strong interaction within the basal ganglia $-$ thalamo-motor loop,which was only seen in SI, indicates the internal movement generationprocess from preparation to execution. In contrast, the interactionfrom PM to SMC observed in ET suggests motor preparation and executionof the neuronal process through which the reception of stimulusis translated into the execution of amovement.

We may need further study on the effect of right-hand movements because of the limited generality of the use of the left hand.In conclusion, however, out results support the findings of non-primateelectrophysiological studies (Georgopoulos et al., 1983; Mitchellet al., 1987; Hamada et al., 1990; Mushiake and Strick, 1995;Middleton and Strick, 2000) by fMRI for the first time. Our dataalso clearly explain the dissociation between the two tasks inPD (Benecke et al., 1987; Georgiou et al., 1994; Martin et al.,1994). The combined use of sequential finger movement, fMRI, andpath analysis made it possible to visualize the functional networkof the basal ganglia motor loop and allowed us to accomplish invivo neuroimaging for movement disorders in which different activationpatterns of the basal ganglia-thalamo-motor loop are predictedby the results in vitro (Delong, 1990).

  FOOTNOTES

Received Sept. 20, 2002; revised Dec. 31, 2002; accepted Jan. 22, 2003.

^* T.T. and A.O. contributed equally to thiswork.

This research was supported by grants from the Ministry of Education, Science, Sports and Culture, Japan (No. 12670608), theCasio Science Promotion Foundation, the Japanese NeurologicalFoundation, and the Magnetism and Health Science Promotion Foundation.We thank Dr. Hideaki Kawabata (Department of Psychology, Facultyof Literature, Kagoshima University) and Dr. Naoko Kinukawa (Departmentof Medical Informatics, Graduate School of Medical Sciences, KyushuUniversity) for helpful comments on thismanuscript.

Correspondence should be addressed to Takayuki Taniwaki, Department of Clinical Neurophysiology, Neurological Institute, GraduateSchool of Medical Sciences, Kyushu University, 3-1-1, Maidashi,Fukuoka 812-8582, Japan. E-mail: ttaniwa{at}neuro.med.kyushu-u.ac.jp.

  References

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ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

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