Dissociable Neural Responses Related to Pain Intensity, Stimulus Intensity, and Stimulus Awareness within the Anterior Cingulate Cortex: A Parametric Single-Trial Laser Functional Magnetic Resonance Imaging Study

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The Journal of Neuroscience, February 1, 2002, 22(3):970-976

Dissociable Neural Responses Related to Pain Intensity, Stimulus Intensity, and Stimulus Awareness within the Anterior Cingulate Cortex: A Parametric Single-Trial Laser Functional Magnetic Resonance Imaging Study
Christian Büchel¹, Karin Bornhövd¹, Markus Quante², Volkmar Glauche¹, Burkhard Bromm², and Cornelius Weiller¹
¹ Cognitive Neuroscience Laboratory, Department of Neurology, and ² Department of Physiology, Hamburg University Medical School, Hamburg, D-20246 Germany

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Neuroimaging studies have demonstrated activations in the anterior cingulate cortex (ACC) related to the affective componentof pain, but not to stimulus intensity. However, it is possiblethat the low spatial resolution of positron emission tomography,as used in the majority of these studies, obscured areas codingstimulus intensity. We revisited this issue, using a parametricsingle-trial functional magnetic resonance imaging design, andinvestigated pain, stimulus intensity, and stimulus awareness(i.e., pain unrelated) responses within the ACC in nine healthyvolunteers. Four different stimulus intensities ranging from warmto painful (300-600 mJ) were applied with a thulium yttrium-aluminumgranate infrared laser in a randomized order and rated by thesubjects on a five point scale (P0-P4).
Pain-related regions in the ventral posterior ACC showed a response that did not distinguish between innocuous trials (P0and P1) but showed a positive linear relationship with the bloodoxygenation level-dependent contrast signal for painful trials(P2-P4). Regions in the dorsal anterior ACC along the cingulatesulcus differentiated between P0 (not perceived) and P1 but exhibitedno additional signal increase with P2; these regions are relatedto stimulus awareness and probably to cognitive processing. Mostimportantly, we identified a region in the dorsal posterior ACCshowing a response that discriminated between nonpainful trials(P0 and P1); therefor, this region was simply related to basicsensory processing and not to pain intensity. Stimulus-relatedactivations were all located adjacent to the cingulate motor area,highlighting the strategic link of stimulus processing and responsegeneration in the posteriorACC.

Key words: pain; single-trial fMRI; laser; neuroimaging; parametric; stimulus response function; affect; emotion; sensory coding; cingulate motor area; anterior cingulate cortex

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The anterior cingulate cortex (ACC) plays an important role in pain processing (Devinsky et al., 1995). Its pivotal role withinthe nociceptive system has been established in lesion studies(Foltz and White, 1968; Bouckoms, 1989; Talbot et al., 1995) andin numerous functional neuroimaging studies using positron emissiontomography (PET) (Jones et al., 1991; Talbot et al., 1991; Caseyet al., 1994; Craig et al., 1996; Rainville et al., 1997; Coghillet al., 1999; Casey, 2000) and functional magnetic resonance imaging(fMRI) (Davis et al., 1997; Porro et al., 1998; Ploghaus et al.,1999; Kwan et al., 2000; Sawamoto et al., 2000). The ACC receivesnociceptive inputs via medial thalamic nuclei (Vogt and Pandya,1987; Vogt et al., 1987) and has been shown to code affectivecomponents of painful stimuli (Craig et al., 1996; Rainville etal., 1997; Sawamoto et al., 2000). It is involved in working memory(Petit et al., 1998) and attentional processing (Gitelman et al.,1999; Peyron et al., 1999), and therefore is well suited to shiftattention toward pain. It is also involved in learning associationsbetween aversive and neutral stimuli in classical conditioning(LaBar et al., 1998; Ploghaus et al., 1999; Büchel and Dolan,2000), which is important to avoid future damage in a similarsituation, and it embodies higher motor areas [cingulate motorarea (CMA)] (Dum and Strick, 1996; Picard and Strick, 1996; Finket al., 1997), which are necessary for defensepreparation.

Most studies, including those manipulating pain affect with hypnosis (Rainville et al., 1997) or those investigating an illusionleading to pain (Craig et al., 1996), have only found evidencefor affective or pain-related processing within the ACC. So far,simple sensory coding of stimulus intensity in the ACC has notbeen observed, and in a recent review, Peyron et al. (2000) hadto conclude that there is no evidence "favoring a role of ACCin coding stimulusintensity."

It should be noted that only few previous imaging studies allowed the identification of stimulus intensity-related responses,because they used at least two stimulus intensities below painthreshold (Casey et al., 1996; Tölle et al., 1999). This conceptwas taken further by a parametric PET study that allowed assessmentof the relationship between brain activity and pain intensity(Coghill et al., 1999). In this study, linear regression analysisrevealed pain intensity-related activation in the ACC. All ofthese studies used PET; therefore a response profile indicativeof sensory processing in a small region might have been obscuredby neighboring pain-relatedactivations.

We revisited this issue with event-related fMRI in combination with a thulium yttrium-aluminum granate (YAG) infrared laserthat delivers very brief heat stimuli, in a parametric design,with four different stimulus intensities ranging from warm topainful. This allowed us to assess individual blood oxygenationlevel-dependent (BOLD) responses as a function of stimulus andpain intensity and to plot a stimulus response function (SRF)for each region similar to the study by Coghill et al. (1999).

We focused on two distinct shapes of this function: (1) an immediate linear increase discriminating between low, innocuousintensities, indicative of sensory-discriminative processing,and (2) an initial plateau followed by a linear increase onlyat higher, painful intensities (i.e., a step function with nodiscrimination of nonpainful warm stimuli and an increase forpainful stimuli, indicative of painprocessing).

  MATERIALS AND METHODS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Subjects. A total of 10 healthy subjects (7 male, 3 female) with a mean age of 28.1 years (range 24-42 years) were recruitedfrom the University of Hamburg; subjects gave their written informedconsent to participate in the study, which was approved by thelocal Ethics Committee. One subject had to be excluded from thestudy because of an exceedingly high pain threshold and poor pain-discriminationability. The remaining nine subjects (six male, three female;one left-handed) were free to withdraw from the study at anytime.

During scanning, two investigators stayed with the subject in the scanner room. One investigator applied the laser stimulito the dorsum of the left hand and the other investigator documentedthe rating of eachstimulus.

Laser stimulator. A thulium YAG laser (Baasel Lasertech, Starnberg, Germany) was used to apply computer-controlled brief radiantpulses to the skin of the subjects. The thulium laser emits near-infraredradiation (wavelength of 1.96 µm, spot diameter of 5 mm, pulseduration of 1 msec) with a penetration depth of 360 µm into humanskin. The laser stimulus allows a precise restriction of the emittedheat energy to the termination area of primary nociceptive afferents(20-570 µm) without damaging the epidermis or affecting the subcutaneoustissue (Spiegel et al., 2000). In addition, the temperature risein the superficial skin after laser stimuli is fast enough toelicit activations of thinly myelinated A $delta$ nociceptors and unmyelinatedCnociceptors.

Experimental protocol and pain rating. In a single fMRI session, 100 nociceptive stimuli were delivered to the dorsum of theleft hand. Interstimulus intervals were randomized in an intervalbetween 8 and 12 sec to minimize pain anticipation (Bromm andTreede, 1991). The stimulation site was changed slightly aftereach stimulus to avoid nociceptor sensitization and fatigue. Stimulationintensity was randomized between 300 and 600 mJ (300 to 400 to500 to 600 mJ). At 4 sec after the laser stimulus, a tone (1 kHzsine, 500 msec) signaled the subjects to rate the perceived painintensity by giving signs with their right hand. Showing a closedhand indicated a pain intensity rating of zero (P0); one finger(thumb) indicated a pain intensity of one (P1); two, three, orfour fingers indicated a pain intensity of P2, P3, and P4, respectively.The intensities were defined as follows: P0, no stimulus perceived;P1, a clear, warm but not painful sensation; P2, P3, and P4, increasinglypainful sensations, comparable to a pinprick. P4 was defined asthe most intensive pain stimulus of the study. Volunteers wereexposed to all pain intensities and trained with this rating scaleinside the MR scanner for 20 min before scanning. In addition,the individual pain threshold was derived psychophysically ineach subject before scanning by three series of stimuli ascendingin steps of 30 mJ, from below sensation threshold to 90 mJ abovepain threshold, and back again to below sensation threshold. Datapertaining to this prescanning pain threshold estimation werelost for two subjects, because of a computer failure. Becauseof the low intersubject variability of the individual pain thresholdin previous behavioral studies, we decided to use fixed energylevels for all subjects to simplify the paradigm and the dataanalysis (Bromm and Lorenz, 1998).

Image acquisition. MR scanning was performed on a 1.5 T MR scanner (Siemens Vision, Erlangen, Germany). In a single session,375 volumes (25 contiguous, axial, 3-mm-thick slices each; 1 mmgap) were acquired using a gradient echo echo-planar imaging (EPI)T2*-sensitive sequence (repetition time, 2800 msec; echo time,60 msec; flip angle, 90°; matrix, 64 × 64; field of view, 210× 210 mm). A standard head coil was used and packed with foampads. Subjects were blindfolded during the experiment. For displaypurposes, a high-resolution (1 × 1 × 1 mm voxel size) T₁-weightedstructural MRI was acquired for each volunteer using a three-dimensionalfast low angle shotsequence.

Image processing and statistical analysis. Image processing and statistical analysis were performed using SPM99 (Friston etal., 1995b; Worsley and Friston, 1995) (http://www.fil.ion.ucl.ac.uk/spm).All volumes were realigned to the first volume (Friston et al.,1995c), spatially normalized (Friston et al., 1995a) to a standardEPI template (Evans et al., 1993), and finally smoothed usinga 6 mm full width at half maximum isotropic Gaussian kernel. Dataanalysis was performed by modeling the different trials ("perceivedpain intensity P0, P1, P2, P3, P4") as $delta$ functions convolved witha set of two basis functions, modeling an early response peakingat 5 sec after application of the painful stimulus and a secondbasis function peaking at 9 sec (expected peak for the motor component).The basis functions were the canonical hemodynamic response function(HRF) as implemented in SPM99. Voxelwise regression coefficientsfor all regressors were estimated using least squares within SPM99(Friston et al., 1995c).

Specific effects were tested with appropriate linear contrasts of the regression coefficients (parameter estimates), resultingin a t statistic for each voxel. These t statistics constitutea statistical parametric map (SPM). SPMs are interpreted by referringto the probabilistic behavior of Gaussian random fields (Worsley,1994). Data were analyzed for each subject individually and witha fixed-effects model to make inferences about the entire groupof subjects (Friston et al., 1999).

Because of strong a priori hypotheses of pain-related responses in the ACC, the threshold was set to p < 0.001 (uncorrected).The T₁-weighted structural volume was coregistered to the functionalscans by normalizing it to a T₁-weighted template in the samespace as the T₂* EPI template used to normalize the functionaldataset.

  RESULTS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Behavioral data

The correlation coefficient between perceived intensity and applied stimulus intensity were 0.72, 0.67, 0.81, 0.72, 0.70,0.82, 0.80, 0.69, and 0.75 in individual subjects. Figure 1 showsthe relationship between average pain rating and applied stimulusintensity. The average pain rating was linearly related to laserenergy (average pain rating = laser energy × 0.84-0.15), wherelaser energy is 300, 400, 500, and 600 mJ.

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Figure 1. Relationship between applied stimulus energy (x-axis) and average rating (P0-P4; y-axis). Each plotted data point refers to the mean rating for each energy level and each subject (i.e., nine data points for each energy level). The average pain rating was linearly related to laser energy (average pain rating = laser energy × 0.84-0.15), where laser energy is 300, 400, 500, and 600 mJ.

On average, a P0 rating was associated with a mean intensity of 333.5 ± 5.7 mJ; P1 was associated with a mean intensity of375.6 ± 11.3 mJ, P2 was associated with a mean intensity of 446.0± 9.5 mJ, P3 was associated with a mean intensity of 527.2 ± 7.5mJ, and P4was associated with a mean intensity of 577.4 ± 5.3mJ. Perceived intensity was linearly related to laser energy (appliedenergy = pain rating × 63.9 + 324), where rating is from 0 to4. The pain threshold during MRI scanning (average of mean intensityassociated with P1 and P2) was 410 ± 28mJ.

fMRI data

The main aim of the study was the characterization of areas activated by painful stimuli by their relationship to stimulusintensity and pain in the ACC (Büchel et al., 1998). Activationsoutside the ACC are beyond the scope of this paper and will bereported elsewhere. Treating differently rated trials as differentconditions allowed us to analyze the relationship between stimulusproperties (pain and intensity) and BOLDsignal.

Fitting canonical HRFs (see Materials and Methods for details) to the data yields a regression coefficient indicating themagnitude of the response for each trial type (P0-P4). This magnitudeof the regression coefficient plotted as a function of ratingis the SRF (see Fig. 3, middle column).

The rating scale used is linear with respect to stimulus intensity as defined by the energy level of the laser (Fig. 1). However,the scale is deliberately nonlinear with respect to pain. P0 andP1 were both defined as nonpainful, whereas P2-P4 were linearlyrelated to increasing painintensity.

Essentially, we found three different SRFs: (1) Some areas showed a significantly higher BOLD signal for P1 compared withP0 but no additional signal increase with P2-P4. Given that P0was used to code stimuli that were not perceived, this simplestep function discriminates between perceived and nonperceivedstimuli without any additional pain or intensity discriminationand is related to stimulus perception (i.e., attentional and workingmemory processing) (Fig. 2a). (2) Some areas showed a linear relationshipbeginning at P0 (i.e., distinguished well between P0, P1, andP2). This SRF differentiates between different stimulus intensities,although some (P0 and P1) were perceived as nonpainful. Signalchanges in these regions are therefore related to stimulus intensity(Fig. 2b). (3) Other SRFs showed an initial plateau (i.e., didnot differentiate between P0, P1, and sometimes P2) but showeda linear relationship for P2-P4. Given the definition of our pain-ratingscale, in which P2 was defined as clearly painful and P0 and P1were defined as nonpainful, this type of SRF is indicative ofareas coding pain intensity (Fig. 2c).

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Figure 2. Different SRFs. The SRF in a shows a higher BOLD signal for P1 (stimulus perceived, but not painful) compared with P0 (stimulus not perceived), but no additional signal increase with P2-P4 (low level, mid-level, and high level of pain). This step function discriminates between perceived and unperceived stimuli without any additional pain or intensity discrimination and seems to be linked to stimulus awareness and possibly to cognitive processing (e.g., working memory or attention). The SRF in b shows a linear relationship beginning at P0 and differentiates well between stimulus intensities, although some (P0 and P1) were perceived as nonpainful. This SRF is related to stimulus intensity. The SRF depicted in c shows an initial plateau (i.e., does not differentiate between P0 and P1 but shows a linear relationship for P2-P4). According to our pain-rating scale, in which P2 was defined as clearly painful and P0 and P1 were not painful, this SRF is related to pain intensity.

Areas showing a stimulus perception-related SRF

Regions with such an SRF were identified by a contrast comparing P1 with P0. To further exclude regions that also show differencesbetween P2 and P1, this contrast was exclusively masked with thecontrast P2 > P1 at p < 0.001. In simple words, this masked contrastreveals areas that show a significant difference between P1 andP0 but not between P1 and P2. Areas showing such an SRF were foundin an area in the dorsal anterior ACC (aACC) (y = 21-36 mm) coveringthe cingulate sulcus (Fig. 3a, blue areas and middle plot). Table1 summarizes the significance and location of these results.As indicated in Figure 3, we use the nomenclature of Kwan et al.(2000) to describe subregions in the ACC. They divide the ACCinto the aACC and the posterior part (pACC).

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Figure 3. Activations in the ACC (p < 0.001) overlaid on a structural T₁-weighted MRI used for spatial normalization. Laser-evoked responses and their locations are depicted in a. Three sagittal slices through the ACC are shown from x = $-$ 3 mm to x = 3 mm. The dashed white line indicates the vertical line through the anterior commissure (VAC). Regions showing different SRFs are color-coded. Stimulus intensity-related areas are shown in red, pain intensity-related areas are shown in green, and cognitive processing-related areas are shown in blue. The top row shows an area in the dorsal pACC with a stimulus intensity-related (red) SRF. The middle row shows the cognitive processing-related step function response of a region in the cingulate sulcus of the aACC (blue). The bottom row shows the SRF of a pain intensity-related area in the ventral pACC (green). (Figure legend continues.)(Figure legend continued.) The middle column shows the individual SRF for each region. Fitting canonical HRFs (see Materials and Methods for details) to the data yields a regression coefficient indicating the magnitude of the response for each trial type (P0-P4). This magnitude (±SEM) plotted as a function of rating is the SRF. In the right column, adjusted data in each region are plotted in bins of 2 sec as a function of peristimulus time separately for P0-P4. In b, the motor-evoked hemodynamic response in the CMA is plotted. Additional motor-evoked responses were observed in the SMA.


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Table 1. Activations in the anterior cingulate cortex

Areas showing a stimulus intensity-related SRF

To identify regions showing intensity-related BOLD signal changes, we used a contrast modeling a linear signal increase forP0-P3. The most prominent linear relationship of the BOLD signalwith stimulus intensity in the low stimulus range (P0-P2) wasobserved in the posterior part of the cingulate sulcus. Apartfrom a linear relationship at low stimulus intensities, this areashowed a ceiling effect (i.e., a slight decrease rather than anincrease in the BOLD signal) when moving from P3 to P4 (Fig. 3a,red areas and top plot).

Areas showing a pain-related SRF

To identify regions showing a pain-related BOLD signal, we used a contrast modeling a linear signal increase for P1-P4, withoutsignificant difference between P0 and P1. Areas showing a linearrelationship between BOLD signal and pain were found in the perigenualACC and in the pACC (Table 1) (Fig. 3a, green areas and bottomplot). Inspection of the spatial distribution of stimulus intensity-and pain-related response functions revealed that the peak ofthe pain-related activations was lateralized to the right (i.e.,contralateral to the stimulated hand). A clear anterior-posteriordistribution was observed for pain- and attention-related areas,with pain-related areas covering the pACC (i.e., posterior tothe attention-related aACC activations). The stimulus intensity-relatedareas were found dorsally to the pain-related activations in thepACC, again posterior to the unspecific activations in the cingulatesulcus of the aACC (Fig. 3a).

To test for differences in shape, a second-order polynomial (y = b₁x² + b₂x + b₃) was fitted to the SRF and the second-order coefficients(b₁) were compared using a paired t test. The pain-related SRF(x = 3, y = 6, z = 48) was significantly different from the stimulusintensity-related SRF (x = $-$ 3, y = 3, z = 51; t₍₈₎ = 1.9; p <0.05) and the stimulus perception-related SRF (x = $-$ 3, y = 21,z = 45; t₍₈₎ = 2.4; p < 0.05).

Motor responses

To identify regions that show motor-related activation, we contrasted the basis functions coding pain responses with thosecoding motor responses pooled over all stimulus intensities. Apartfrom the left (contralateral to the moving hand) primary motorcortex, motor-related responses were observed in the dorsal pACC,posterior to the pain-related activations. With regard to previousmotor studies, these activations enclose the supplementary motorarea (SMA) and the CMA (Fink et al., 1997; Petit et al., 1998;Kwan et al., 2000) (Fig. 3b).

  DISCUSSION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Using a laser pain stimulus in combination with a parametric event-related fMRI design, we have characterized regions in theACC according to their SRF as (1) stimulus perception-related,(2) stimulus intensity-related, or (3) pain-related. The ACC showedall three response types: a BOLD signal in the perigenual ACCand ventral pACC was related to pain intensity, whereas aACC signalchanges were unspecific and most likely related to working memoryand attentional processes. More importantly, we have characterizeda dorsal pACC region in the cingulate sulcus coding stimulus intensity.Motor-related activations were found immediately posterior tothe pain- and stimulus-related ACC activations in the SMA andCMA.

Pain stimulus

The thulium YAG laser is the ideal stimulation device for event-related fMRI studies of pain. It delivers brief (1 msec) stimuliwith defined energy levels and only activates nociceptors andnot the vibrotactile sensory system. In recent magnet encephalographystudies, it was shown that vibrotactile stimuli evoke very shortlatency responses in the primary somatosensory cortex, whereaswith the laser, the latencies of the evoked responses in the SI[and secondary somatosensory cortex (SII)] were almost three timeslonger, without the initial short-latency component, highlightingthe ability of the laser to exclusively stimulate nociceptors(Ploner et al., 2000; Timmermann et al., 2001).

Pain intensity-related responses

We applied four different pain intensities (300, 400, 500, and 600 mJ), which were rated for intensity on a five-point ratingscale ranging from 0 to 4. The BOLD response was correlated withindividual ratings instead of the applied intensities, becausethis allowed us to accurately dissociate painful ( $>=$ P2) from nonpainful( $<=$ P1)events.

Activation of the ACC in pain studies has exclusively been linked with nociceptive or affective processing. This finding hasbeen derived by experimentally dissociating pain affect from stimulusintensity using hypnosis (Rainville et al., 1997) or using a painillusion (Craig et al., 1996). Other studies used multiple intensities(Coghill et al., 1999) and linear regression to find regions relatedto pain perception (Tölle et al., 1999), and still others investigateda very intense pain and the decay of this sensation over time(Porro et al., 1998). The location of the main activation relatedto pain processing in our study was found in a mid-cingulate regionslightly anterior to the anterior commissure (x = 3, y = 6, z= 48). This is close to an activation correlated with pain intensityin a previous fMRI study where the peak was located ventrally(x = 7, y = 6, z = 34) (Porro et al., 1998). This location isalso in accord with another recent fMRI study investigating painprocessing in the ACC (Kwan et al., 2000). A single neuron studyperformed in awake humans showed an SRF that was similar to thatfound in our study (Hutchison et al., 1999). Neurons in the ventralpACC showed no increase in firing rate with an increase in temperaturein the low (nonpainful) temperature range, but a marked increasewas seen in the painful range (46-50°C). The peak of our pain-relatedactivation also coincides with previous PET studies in which apain intensity- (x = $-$ 0.1, y = 11.5, z = 35.8) (Coghill et al.,1999) or pain threshold-related activation was found in the pACC(x = 6, y = 3, z = 43) (Tölle et al., 1999).

Stimulus intensity-related responses

Based on previous reports, we exclusively expected activations correlated with pain, because almost all studies have implicatedthe ACC in the affective coding of pain (Rainville et al., 1997;Sawamoto et al., 2000). However, our data clearly show that aregion in the dorsal pACC within the cingulate sulcus also exhibitsstimulus intensity-related BOLD responses that are not relatedto pain intensity, because BOLD responses in this region differentiatedwell between P0 and P1, which were both innocuous trials (Fig.3, red areas). Although previous studies have concentrated onaffective or pain-related responses in the ACC, this type of activationis not totally unexpected, considering that medial and intralaminarthalamic nuclei from which the ACC receives input (Vogt and Pandya,1987; Vogt et al., 1987) have shown intensity coding (Bushnelland Duncan, 1989). ACC neurons coding stimulus intensity havebeen found previously in the anesthetized rabbit (Sikes and Vogt,1992). Furthermore, clinical data from patients with anteriorcingulotomy (Davis et al., 1994) or deafferented anterior cingulate(Talbot et al., 1995) have also shown a diminished sensory codingability. The only other region showing a similar SRF in our studywas the primary sensory cortex. Similar to the SRF observed there,stimulus intensity-related responses in the ACC showed a ceilingeffect, or even a decrease, when moving from P3 to P4, suggestingan additional, possibly antinociceptive, mechanism initiated athigher stimulusintensities.

We can only speculate as to why stimulus intensity-related responses have not been found in previous functional neuroimagingstudies. One reason might be that subtle differences in SRFs areobscured by low spatial resolution in those PET studies that usedtwo or more innocuous stimulus conditions (Casey et al., 1996;Coghill et al., 1999; Tölle et al., 1999) or used averaging overthe entire ACC in a region of interest in fMRI (Sawamoto et al.,2000). Furthermore, in most studies, stimulus intensities havebeen chosen to detect pain but not stimulus intensity-relatedactivations (Kwan et al., 2000).

Pain-intensity-independent responses

Aside from ACC regions showing a relationship with stimulus or pain intensity, our study revealed a region in the aACC, withinthe cingulate sulcus, that showed a significant BOLD signal differencebetween P0 and P1 but no additional discrimination between P1,P2, P3, and P4. Similar SRFs were observed in the dorsolateralprefrontal cortex and the intraparietal sulcus. This "on-off"response profile is related to whether a stimulus was perceived(a rating of >P0). Alternatively, this SRF could be related tocoding of warmth, in accordance with the fact that primary afferentwarm fibers code intensity of warmth up to pain threshold andthen either a plateau or decrease in activity in the painrange.

Whenever a stimulus is consciously perceived, many cognitive processes will be initiated: (1) an exogenous shift of spatialattention to the stimulated site (Corbetta et al., 2000), (2)rating of intensity, and (3) keeping this rating in working memoryfor 4 sec as required in our task. This interpretation is in agreementwith a recent fMRI study on working memory-related responses inthe medial wall (Petit et al., 1998). Recent single-cell workin patients undergoing cingulotomy revealed attention-relatedactivation in aACC neurons (Davis et al., 2000), anterior to painresponsive neurons (Hutchison et al., 1999). The location of theseresponses is in close agreement with the peak of our binary responsefound in the aACC (x = $-$ 3, y = 21, z = 45). Recently, an elegantstudy directly investigated the effect of attention in the contextof pain processing using a full factorial design. In precise spatialagreement with regions showing an on-off SRF according to ourdata, the main effect of attention (regardless of whether thestimulus was noxious or innocuous) activated an area in the aACC(x = $-$ 2, y = 22, z = 40) (Peyron et al., 1999).

Motor

Our experiment explicitly comprised an abstract motor command with the contralateral hand, thus avoiding interference witha possible withdrawal reflex (Schouenborg et al., 1992). Contrastinglaser-evoked with motor-evoked signal changes, we found a largearea in the dorsal pACC located within the boundary of the CMAand the SMA (Devinsky et al., 1995; Dum and Strick, 1996; Finket al., 1997) (Fig. 3b, red areas).

In agreement with a previous study (Kwan et al., 2000), ACC subregions that were only activated by the motor task were locatedin close vicinity to pain- and stimulus intensity-related activations(Fig. 3b). Such a spatial configuration (i.e., affective and sensoryareas neighboring the response-generating motor areas) seems advantageous,because the generation of an adequate response requires as muchinformation about the painful stimulus aspossible.

Conclusion

Using event-related fMRI together with brief laser pain stimuli of different intensities, we were able to precisely characterizeregions within the ACC according to their individual SRF. Withrespect to pain-related processing, we confirmed previous studiesshowing pain-related regions in the perigenual ACC and the ventralpACC. Distinct from these pain-related regions, activations inthe dorsal aACC were found to code stimulus perception withoutadditional discrimination of pain or stimulus intensities. Thisresponse pattern is unrelated to pain processing per se but seemsto be associated with working memory or attention to pain. Mostinterestingly, we discovered an area in the dorsal pACC that showeda BOLD signal that was indicative of basic sensory processinginstead of affective painprocessing.

Response patterns in the ACC mirror those found in other cortical areas: SI showed a response profile indicating basic sensoryprocessing, SII and the anterior insula showed pain-related responses,and the dorsolateral prefrontal and parietal cortex showed a binary,stimulus perception-related response pattern. Thus, our data supportthe notion that through projections from all of those regionsthe ACC can integrate a wide range of pain-relevant informationand generate an adequate response through its motor areas situatedimmediately posterior to the laser-stimulus-relatedresponses.

  FOOTNOTES

Received Sept. 4, 2001; revised Oct. 24, 2001; accepted Oct. 25, 2001.

This work was supported by the Volkswagenstiftung. We thank the Physics and Methods group at the Cognitive Neuroscience Laboratoryin Hamburg, the technical staff at the Department of Neurophysiologyfor their support with the laser, and J. Lorenz, D. Gonzalo, A.Schnitzler, and U. Bingel for suggestions on a previous draftof thispaper.
Correspondence should be addressed to Dr. Christian Büchel, Neurologische Universitätsklinik, Haus B, Universitäts-KrankenhausEppendorf, Martinistrasse 52, D-20246 Hamburg, Germany. E-mail:buechel{at}uke.uni-hamburg.de.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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