Integration of Perspective and Disparity Cues in Surface-Orientation-Selective Neurons of Area CIP

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Integration of Perspective and Disparity Cues in Surface-Orientation-Selective Neurons of Area CIP

Ken-Ichiro Tsutsui,¹^,³ Min Jiang,¹ Kazuo Yara,² Hideo Sakata,¹ and Masato Taira¹

¹Department of Physiology and ²Department of Neuropsychiatry, Nihon University School of Medicine, Tokyo 173-8610; and ³Japan Society for the Promotion of Science, Tokyo 102-8471, Japan

ABSTRACT

TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES

Tsutsui, Ken-Ichiro, Min Jiang, Kazuo Yara, Hideo Sakata, and Masato Taira. Integration of Perspective and Disparity Cues in Surface-Orientation-Selective Neurons of Area CIP. J. Neurophysiol. 86: 2856-2867, 2001. We investigated the effects of linear perspective and binocular disparity, as monocular and binocular depth cues, respectively,on the response of surface-orientation-selective (SOS) neuronsin the caudal part of the lateral bank of the intraparietal sulcus(area CIP). During the single-unit recording, monkeys were requiredto perform the delayed-matching-to-sample (successive same/differentdiscrimination) of discriminating surface orientation in stereoscopiccomputer graphics. Of 211 visually responsive neurons, 66 wereintensively tested using the solid-figure stereogram (SFS) ofa square plate with both disparity and perspective cues (D+P condition),and 62 of these were identified as SOS neurons for respondingselectively to the orientation of stimuli. All these neurons werefurther tested using a solid figure with perspective cues alone(P-only condition), and 58% (36/62) of these showed selectiveresponse to the orientation of the stimuli. Of the 62 SOS neurons,35 neurons were also tested using SFS with disparity cues alone(D-only condition) in addition to the D+P and P-only conditions.We classified these 35 neurons into four groups by comparing theresponse selectivity under the P-only and D-only conditions. Morethan one-half of these (19/35) were sensitive to both perspectiveand disparity cues (DP neurons), and nearly one-third (11/35)of these were sensitive to disparity cues alone (D neurons), buta few (2/35) were sensitive to perspective cues alone (P neurons).The remaining (3/35) neurons exhibited orientation selectivityonly when both cues were present. In DP neurons, the preferredorientation under the D+P condition was correlated to those underthe D-only and P-only conditions, and the response magnitude underthe D+P condition was greater than those under the D-only andP-only conditions, suggesting the integration of both cues forthe perception of surface orientation. However, in these neurons,the orientation tuning sharpness under the D+P and D-only conditionswas higher than that under the P-only condition, suggesting thedominance of disparity cues. After the single-unit recording experiments,muscimol was microinjected into the recording site to temporarilyinactivate its function. In all three effective cases out of sixmicroinjection experiments, discrimination of a three-dimensional(3D) surface orientation was impaired when disparity cues alonewere present. In only one effective case, when a relatively largeamount of muscimol was microinjected, discrimination of a 3D surfaceorientation was impaired even when both disparity and perspectivecues were present. These results suggest that linear perspectiveis an important cue for representations of a 3D surface of SOSneurons in area CIP, although it is less effective than binoculardisparity, and that both of these depth cues may be integratedin area CIP for the perception of surface orientation indepth.

	INTRODUCTION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

It was proposed by Gibson (1950) that our visual system utilizes various kinds of depth cues to perceive the three-dimensional(3D) shape of an object from two-dimensional (2D) retinal images.Visual depth is perceived not only with binocular cues of disparity,but also with monocular cues of linear perspective, texture gradient,and shading. Similarly, Marr (1982) postulated in his computationaltheory of vision that the description of the geometry of a visiblesurface by integrating various depth cues is a critical step invisual information processing for forming a representation ofa 3Dshape.

Many psychophysical studies have shown that in addition to binocular disparity, monocular depth cues, such as the linear perspectiveof contours (Clark et al. 1955; Freeman 1966; Olson 1974; Stevens1983) and texture gradients (Clark et al. 1956; Cutting and Millard1984; Flock and Moscatelli 1964; Goodenough and Gillam 1997; Gruberand Clark 1956), are also important for the perception of thesurface orientation. It was reported that such monocular depthcues interact with binocular depth cues during the perceptualprocess (Poom and Borjesson 1999).

In our previous studies, we identified surface-orientation-selective (SOS) neurons in the caudal part of the lateral intraparietalsulcus (area CIP) of the monkey and found that they are sensitiveto binocular disparity (Shikata et al. 1996). It was found thatthese neurons are sensitive to the gradients of disparity acrossthe surface and/or those along the contour, and that they integratethese disparity signals to represent 3D surface orientation (Tairaet al. 2000). It was shown by further study that some of theseSOS neurons are also sensitive to monocular cues for depth suchas linear perspective and texture gradient (Tsutsui et al. 1999);however, it is still unclear how the neural signals of monoculardepth cues are integrated with those of disparity cues to generatea representation of the 3D surface orientation in theseneurons.

In the present study, we compared the effects of monocular depth cues of linear perspective with those of binocular depthcues on the response of SOS neurons in area CIP by single-unitrecording experiments. We also examined the critical role of SOSneurons in the perception of 3D surface orientation by muscimolmicroinjection into the recording sites of theseneurons.

	METHODS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Two male Japanese monkeys (Macaca fuscata) were used in the present study. Throughout the experiments, the monkeys were treatedin accordance with the National Institutes of Health Guide forCare and Use of Laboratory Animals. This project was approvedby the Ethical Committee of Nihon University School ofMedicine.

Apparatus

All stimuli used in the present study were generated by a graphics computer (SGI, Indigo2) and presented on a display (1,240× 1,024 pixels, 21 in.) with a liquid crystal polarized filter(NUvision). The display was placed 44 cm in front of the monkeyat eye level. The filter was switched at 120 Hz, whereby 60 frames/sof stimulus were presented to each eye. The monkey wore polarizedglasses to view these stimulistereoscopically.

Stimulus

Figure 1A shows samples of the binocularly presented stimuli used in the single-unit recording and the muscimol injectionexperiments. 1) Solid-figure stereogram (SFS) of a square platewith perspective cues (D+P condition, top row): this type of stimulushad perspective cues as well as disparity cues; therefore the2D shapes of fused images were dependent on their orientationin depth. 2) Solid figure (SF) with perspective cues alone (P-onlycondition, middle row): these were presented binocularly in thetask. This type of stimulus had perspective cues, but no binoculardisparity cues (i.e., 2D shape stimuli). 3) SFS with disparitycues alone (D-only condition, bottom row): this type of stimulushad binocular cues, but no perspective cues; therefore the 2Dshape of a fused image was the same (square) in all orientations.We used nine different orientations in the task: a plate in thefrontoparallel plane and plates of eight different orientationsthat were slanted 45° against the frontoparallel plane and rotatedevery 45° around the sagittal (Z) axis (see insets in Fig. 2).We defined the direction of slant as "tilt" following Stevens(1983), so that the tilt of the slanted plate ranged from 0 to315° at 45° intervals. In the muscimol injection experiments,2D shape stimuli (circle, triangle, square, and hexagon) wereused for 2D shape discrimination, which was the control task (2D-shapecondition). The 2D shape stimuli were presented binocularly inthe task.

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Fig. 1. A: stimulus sets used in the single-unit recording experiments. Solid figure stereogram (SFS) of a plate in 0° tilt (left column) and in 270° tilt (right column) under the D+P (top row), P-only (middle row), and D-only (bottom row) conditions. The figure on the left is for the left eye, and that on the right is for the right eye (see METHODS for details). B: schematic illustration indicating the location of the caudal part of the lateral bank of the intraparietal sulcus (area CIP). The intraparietal sulcus (ips), lunate sulcus (lu), and the parietooccipital sulcus (po) are unfolded. Area CIP is located between areas LIP and V3A. C: single-unit recording sites were superimposed on the trace of the frontoparallel section of the left hemisphere of one monkey. Small dots indicate the points where SOS neurons were recorded.

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Fig. 2. Responses of a typical surface-orientation-selective (SOS) neuron with sensitivity to perspective cues. A: responses to 9 different orientations under the D+P condition. The two-dimensional (2D) shape of the fused image changed in accordance with the linear perspective. B: responses to 9 different orientations under the P-only condition in which all stimuli were presented with zero disparity so that the linear perspective was the only cue for surface orientation. Insets indicate the stimuli presented: solid lines represent the orthographic projection of the simulated plate onto the frontoparallel plane, dashed lines schematically represent the orientation of the surface in depth caused by binocular disparity, and arrow represents the surface normal. The numbers at the top left of the rasters indicate the tilt (the orientation in the frontoparallel plane of the axis around which the surface was rotated). In the present study, the slant of the surface (the angle between the line of sight and the surface normal) was fixed at 45°. Cor. indicates the plate in the frontoparallel screen. Rasters and histograms are aligned to the stimulus onset (dashed line). Bold underline denotes the stimulus presentation period (750 ms). Note that preferred orientations of this neuron are similar under both conditions although the response magnitude is much higher under the D+P condition. This neuron also responded selectively under the D-only condition (not shown) and was classified as a DP neuron.

The size of these stimuli was 6.3 × 6.3° when they were in the frontoparallel orientation and was of minimum thickness (1dot on the display, 0.0385 × 0.0385°). The fixation point andthe center of the stimulus were presented at a distance of 44cm from the monkey at eye level. The simulated distance for theperspective cues of the stimuli was the same as the optical distance.Pure red was chosen as the color of the stimuli to prevent ghoststimuli from appearing inappropriately in the eye when the filterwas switched. All stimuli were rendered without shading or texture,and the background of the stimulus wasblack.

Behavioral task

We used a GO/NO-GO-type delayed-matching-to-sample (DMTS) task, or successive same/different discrimination, in which themonkey had to judge whether the surface orientations of successivelypresented sample and test stimuli were the same or different.The difference in tilt angles between a pair of sample and teststimuli in a trial ranged from 0 to 180° at 45° intervals, becausethe sample and test stimuli were chosen from a stimulus set consistingof nine orientations. The time sequence of the task is as follows.When a small fixation spot (0.2° diam) appeared, the monkey pressedthe key and fixated on the spot. The monkey had to fixate on thespot until it released the key at the end of the trial. The presentationtime of sample and test stimuli was 1 s or 750 ms, and the delayperiod (time interval between sample stimulus offset and teststimulus onset) was 2 s. If the surface orientation of the samplestimulus was the same as that of the test stimulus, the monkeyhad to release the key as soon as possible after the color ofthe fixation spot changed (GO trial); however, if the surfaceorientations were different, the monkey had to withhold key releasefor 1.5 s after the color change of the fixation spot until thefixation spot was turned off (NO-GO trial). The monkey was rewardedfor the appropriate key release in both GO and NO-GO trials (symmetricalreinforcement). In the muscimol injection experiments, a 2D shapediscrimination task was performed as the control task in additionto the surface orientation discrimination tasks. The sample andtest stimuli were chosen from a 2D shape stimulus set, which consistedof a circle, triangle, square, and hexagon. The monkey had todiscriminate whether the shapes of the sample and test stimuliwere the same ordifferent.

Eye movement recording

The movement of the right eye was monitored using an infrared eye movement recording system (RMS). The trial was canceledimmediately when the eye position exceeded the limit of 1° fromthe fixation spot. The eye movement during each trial was alsomonitored off-line to confirm that small saccades or vergenceeye movements did not occur. Please refer to our recent paper(Taira et al. 2000) for a detailed description of eye movementrecording.

Single-unit recording

Before the single-unit recording, an atlas of the stereotaxic magnetic resonance image (MRI) of the brain of each monkey wasconstructed. For head fixation, a halo-like metal ring was implantedin each monkey's skull, and a microelectrode recording chamberwas stereotaxically implanted in the opening of the skull overthe parietal cortex under pentobarbital sodium anesthesia. Afterrecovery from the surgery, extracellular single-unit recordingswere carried out in the lateral bank of the intraparietal sulcususing tungsten microelectrodes. Since the recording chamber wasimplanted stereotaxically, the penetration track of the electrodecould be accurately superimposed on the stereotaxic MRI brainmap.

Single-unit activity was recorded during the performance of the DMTS task under three conditions (D+P, P-only, and D-only)in a blocked manner. Each block consisted of 45 trials, in whicheach of 9 different surface orientations was presented as a samplestimulus for every 9 trials in a random order. Test stimuli wereselected so that 22 or 23 trials became GO trials and the remainingones became NO-GO trials in one block. The recording procedurewas as follows. We first tested the response of the neurons toa flat wooden plate held by the experimenter. If a neuron appearedto be selective to the surface orientation, it was further testedusing the computer-generated stimuli during the monkey's performanceof the DMST task, first under the D+P condition. If the neurondid not clearly exhibit selectivity as determined by the experimenter'svisual inspection of rasters displayed on-line, it was discardedbefore completing the entire sequence (45 successful trials) ofthe D+P condition. All neurons recorded under the D+P conditionwere further recorded under the P-only condition. If the single-unitactivity could be maintained in good isolation, the activity wasfurther recorded under the D-onlycondition.

Analysis of neuronal activity

In the present study, neuronal responses to the sample stimulus in successful trials only were analyzed. To examine whethera neuron was visually responsive, neuronal activities in the prestimulus(500 ms) and stimulus (1 s or 750 ms) periods under the D+P conditionwere compared using the Student's t-test (P < 0.05) for each orientation.If the activities during the prestimulus and stimulus periodswere different at least for one orientation, the neuron was classifiedas visually responsive. For visually responsive neurons, theirselectivity to surface orientation under each condition was testedby comparing the activities during the stimulus period of eightorientations, excluding frontoparallel orientation, using theRayleigh test (Mardia 1972). If a neuron responded selectivelyunder the D+P condition, it was classified as an SOSneuron.

To estimate the preferred orientation and tuning sharpness of each SOS neuron under each condition, we transferred the responsefrequency for eight different orientations into vectors (_{0, 1 ... 7}for 0, 45 ... 315° tilt) so that the vector angle corresponded tothe surface tilt and the vector length corresponded to the responsefrequency. The preferred orientation (tilt) was obtained by calculatingthe direction of the sum vector ( $Sigma$ ). This method of calculatingthe preferred orientation is mathematically the same as the methodof fitting a sinusoidal function to a discharge rate, as describedby Georgopoulos et al. (1982). For the index of the tuning sharpness,we used the angular deviation S, which is equivalent to the standarddeviation in linear statistics. The angular deviation S was calculatedusing

<IT>R</IT><IT>=‖&Sgr; </IT><IT><A><AC>r</AC><AC>&cjs1164;</AC></A></IT><IT>‖ &cjs0823; &Sgr; ‖</IT><IT><A><AC>r</AC><AC>&cjs1164;</AC></A></IT><IT>‖</IT>

<IT>S</IT><IT>=</IT>(<IT>180&cjs0823; &pgr;</IT>)[<IT>2</IT>(<IT>1−</IT><IT>R</IT>)]<SUP><IT>1&cjs0823; 2</IT></SUP>

where | $Sigma$ $r$ | is the length of the sum vector, $Sigma$ | $r$ | is the sum of each vector's length, and S is the angular deviation indegrees.

Neurons recorded under all three (D+P, P-only, and D-only) conditions were classified according to their selectivity underthe three conditions (Table 1). If a neuron responded selectivelyunder the D+P and P-only conditions but not under the D-only condition,it was classified as a P neuron, that is, it is sensitive to perspectivecues alone. If a neuron responded selectively under the D+P andD-only conditions but not under the P-only condition, it was classifiedas a D neuron, that is, sensitive to disparity cues alone. Ifa neuron responded selectively under all three conditions, itwas classified as a DP neuron, that is, it is sensitive to bothdisparity and perspective cues.

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Table 1. Classification of SOS neurons recorded under three conditions

Muscimol microinjection

After the single-unit recording experiments, the muscimol microinjection experiments were performed on the same monkeys. Wemicroinjected muscimol using an injection-recording device (astainless steel microinjection cannula containing a Teflon-coatedtungsten wire that serves as a unit recording electrode; Crist).The tip of the microinjection cannula and that of the electrodewere about 1 mm apart. The cannula was attached to the electrodemanipulator and inserted into the recording site. To confirm thatthe tip of the cannula was in area CIP, extracellular single-unitrecordings were carried out through an attached electrode. A totalof 15-20 µg of muscimol (5 µg/µl) was injected over a period of10 min. Immediately after the completion of the microinjection,the monkeys were required to perform thetask.

In the muscimol microinjection experiments, the monkeys were required to perform the DMTS task under three conditions (D+P,D-only, and 2D-shape). The time course of the trial was the sameas that in the unit recording experiments (1-s or 750-ms stimuluspresentation and 2-s delay). One session consisted of three blocksof different conditions in a random order. In three of six casesof microinjection experiments, a block consisted of 18 trials.In the other three cases, a block lasted until the number of correcttrials reached 18 trials, and then it was switched to anotherblock. The duration of one session was approximately 15 min. Betweenblocks, five practice trials of the stimulus condition of thefollowing block were inserted, to avoid the effect of changingthe stimulus condition on the monkeys' performance. Before themicroinjection, the monkeys were required to perform the taskof two sessions as the control. After the microinjection, theywere required to perform one session every 30 min during the first2 h, one session after 3 h, and two sessions after 24h.

Histology

After completion of the muscimol microinjection experiments, the monkeys were sacrificed and the entire brain was removedfrom the skull and soaked in 20% formaline. After the formalinefixation, 50-µm-thick sections were cut along the frontal planein both hemispheres of two monkey brains. One in every two sectionswas stained with thionine to trace the penetrations. The unitrecording sites and muscimol injection sites were determined indirectlyfrom the relative positions of the penetrations to the anatomicallandmarks, as well as from the stereotaxic lesions made afterperforming all the experimental sessions. The recording and injectionsites were superimposed at 2-mm intervals on the trace of thefrontal section of the left hemisphere of one monkey (Figs. 1Cand 6A, see details in the figure legend). The plotting by thishistological method and those by stereotaxic MRI method did notdiffer by more than 1mm.

	RESULTS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

We recorded 211 visually responsive neurons in area CIP (Fig. 1B), and 66 of these were tested for orientation selectivitywith a complete test routine (9 orientations × 5 repetitions)using a SFS of a square plate with both disparity and perspectivecues (D+P condition). [We discarded neurons when they appearedto be nonselective to surface orientation in the initial examination(see METHODS for details concerning the recording procedure).Therefore there might be a sampling bias in selecting 66 neuronsto be examined with a complete test routine.] Of these 66 neurons,62 were identified as SOS neurons, as they responded selectively(Rayleigh test, P < 0.05) to the surface orientation. The meanangular deviation S (index for tuning sharpness; see METHODS fordetails) for SOS neurons (n = 62) was 68.5°, and that for non-SOSneurons (n = 4) was 79.4°. For each SOS neuron, the preferredorientation under the D+P condition was calculated by transferringthe response frequency for eight different orientations into vectorsand calculating the direction of the sum vector. These preferredorientations of SOS neurons were distributed randomly (Rayleightest, P > 0.10).

To examine the effect of linear perspective cues on the response of SOS neurons, we tested their response to the solid figurewith perspective cues alone (P-only condition). Figure 2 showsresponses of a typical SOS neuron sensitive to linear perspectivecues. Under the D+P condition (Fig. 2A), this neuron respondedmost vigorously to the surface tilted 315° and also respondedwith a high discharge rate to those tilted 0 and 45° (preferredorientation: 358.7°). Under the P-only condition (Fig. 2B), thisneuron showed almost the same orientation selectivity (preferredorientation: 5.7°) as that under the D+P condition, but its responsewas much weaker. Thus this neuron appeared to be sensitive toboth perspective and disparity cues. Of all the SOS neurons, 58%(36/62) showed orientation selectivity under the P-only condition,suggesting their sensitivity to perspectivecues.

To examine the effect of binocular disparity cues on the response of SOS neurons, 35 of 62 SOS neurons were further testedusing stimuli with disparity cues alone (D-only condition) inaddition to the D+P and P-only conditions. Figure 3 shows responsesof a typical SOS neuron with sensitivity to binocular disparitycues. Under the D+P condition (Fig. 3A), this neuron respondedvigorously to surfaces tilted 0, 270, and 315° (preferred orientation:323.3°). Under the D-only condition (Fig. 3B), this neuron showedalmost the same orientation selectivity (preferred orientation:313.6°) as that under the D+P condition, and its magnitude ofresponse was almost the same. Thus this neuron did not appearto be sensitive to perspective cues. Of all the SOS neurons tested,86% (30/35) showed orientation selectivity under the D-only condition,suggesting their sensitivity to disparity cues. This populationwas significantly higher ( $chi$ ² test, P < 0.01) than that of neurons selective under the P-onlycondition (58%, 36/62).

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Fig. 3. Responses of a typical SOS neuron with sensitivity to disparity cues. A: responses to 9 different orientations under the D+P condition. B: responses to 9 different orientations under the D-only condition in which all stimuli were presented without linear perspective so that the disparity was the only cue for surface orientation. The 2D fused image of each stimulus was always square under the D-only condition. Conventions are the same as those in Fig. 2. This neuron showed nonselective response under the P-only condition (not shown) and was classified as a D neuron. Note that preferred orientations and discharge rates of this neuron are similar under both conditions.

Classification of SOS neurons

Thirty-five SOS neurons tested under three conditions were classified into four groups according to their selectivity undereach condition (Table 1). Two major types are shown in Fig. 4.

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Fig. 4. Two major types of SOS neuron. A: DP (disparity and perspective) neuron. B: D (disparity) neuron. Responses under the D+P, P-only, and D-only conditions are shown in the top, middle, and bottom rows, respectively. For each condition, only responses to the most preferred and the diagonal orientations are shown, although responses to nine orientations were recorded. The 2D shape of the fused image changed in accordance with the linear perspective under the D+P and P-only conditions, but it was always the same (square) under the D-only condition. Other conventions are the same as those in Fig. 2.

The largest group (19/35, 54%) consists of neurons responding selectively under all three conditions, suggesting their sensitivityto both disparity and perspective cues (DP neuron). The neuronwhose responses are shown in Fig. 4A is an example of this type.This typical DP neuron responded selectively to the surface tilted225° under the D+P condition (top row), P-only condition (middlerow), and D-only condition (bottom row). The figure shows thatthe response was greatly enhanced under the D+P condition in thesame orientation. This may be due to the summation of responsesto disparity and perspective cues. The average response of allDP neurons to the preferred orientations was significantly higherunder the D+P condition (50.7 ± 5.2 spikes/s, mean ± SE) thanunder the D-only condition (37.9 ± 4.7, Student's t-test, P <0.01) and the P-only condition (31.2 ± 3.5; Student's t-test,P < 0.001).

The second largest group (11/35, 31%) consists of neurons responding selectively under the D+P and D-only conditions but notunder the P-only condition, suggesting their sensitivity to disparitycues alone (D neuron). The neuron whose responses are shown inFig. 4B is an example of this type. This typical D neuron respondedto the surface tilted 270° under the D+P condition (top row) andthe D-only condition (bottom row) with almost the same responsemagnitude. However, it showed only a weak and nonselective responseunder the P-only condition (middle row). The average responsesof all D neurons to the preferred orientations under the D+P condition(45.7 ± 6.7 spikes/s) and the D-only condition (34.6 ± 5.6) werenot significantly different (Student's t-test, P > 0.10).

In contrast to DP and D neurons, only a few (6%, 2/35) neurons were classified as P neurons for responding selectively underthe D+P and P-only conditions but not under the D-only condition.Furthermore, in these neurons, the selectivity under the P-onlycondition was relatively low (just above the significant levelof P = 0.05). The remaining three neurons (9%, 3/35) did not showselectivity either under the P-only or D-only condition, showingresponse selectivity only under the D+Pcondition.

Concerning the location of neurons, these four types of neuron were uniformly distributed in area CIP, and there was no differencein the distribution according to the type ofneuron.

Interaction between linear perspective and binocular disparity cues

To examine the interaction between linear perspective and binocular disparity cues in SOS neurons, relationships of preferredorientations under the three different conditions wereanalyzed.

For SOS neurons sensitive to perspective cues (DP and P neurons, 21/35), we plotted the preferred orientation under the P-onlycondition versus that under the D+P condition (Fig. 5A). The correlationof preferred orientations under the two conditions was positivebut not sufficiently strong to reach statistical significance(circular-circular regression, r = 0.343, P > 0.10). However,the distribution of the preferred orientation difference was significantlyconcentrated to <45° ( $chi$ ² test, P < 0.05; Fig. 5B), showing that preferred orientationsunder these two conditions tend to coincide to some extent. Furthermore,when we restrict the sample to DP neurons (n = 19), the preferredorientations under the two conditions were significantly correlated(circular-circular regression, r = 0.432, P < 0.05).

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Fig. 5. A: plot of the preferred orientation of perspective-sensitive (DP and P) neurons under the P-only condition (ordinate) against that under the D+P condition (abscissa).

, P neurons;

, DP neurons. B: the distribution of the preferred orientation difference between the 2 conditions in these neurons.

, P neurons;

, DP neurons. C: plot of the preferred orientation of disparity-sensitive (DP and D) neurons under the D-only condition (ordinate) against that under the D+P condition (abscissa). $triangle$ , D neurons;

, DP neurons. D: the distribution of the preferred orientation difference between the 2 conditions in these neurons.

, D neurons;

, DP neurons. E: plot of the preferred orientation of DP neurons under the P-only condition (ordinate) against D-only condition (abscissa). F: the distribution of the preferred orientation difference between the 2 conditions in these neurons.

For SOS neurons sensitive to disparity cues (DP and D neurons, 30/35), we plotted the preferred orientation under the D-onlycondition against that under the D+P condition (Fig. 5C). Thepreferred orientations under the two conditions were well correlated(circular-circular regression, r = 0.760, P < 0.01), and the distributionof the preferred orientation difference was significantly concentratedto <45° ( $chi$ ² test, P < 0.01; Fig. 5D), showing that the preferred orientationunder the D-only condition had a strong tendency to coincide withthat under the D+P condition. For DP neurons (n = 19), the circular-circularregression coefficient was r = 0.888 (P < 0.001), whereas thatof D neurons (n = 11) was r = 0.596 (P < 0.05).

For SOS neurons sensitive to both disparity and perspective cues (DP neuron, 19/35), we plotted the preferred orientationunder the P-only condition versus that under the D-only condition(Fig. 5E). The correlation of the preferred orientations underthe two conditions was positive but did not reach statisticalsignificance (circular-circular regression, r = 0.273, P > 0.10).However, the population of neurons with the preferred orientationdifference of <90° (14/19) was significantly larger than thatwith the preferred orientation difference of more than 90° ( $chi$ ² test, P < 0.05; Fig. 5F), indicating that the preferred orientationsunder these two conditions tend to coincide to someextent.

To evaluate and compare the orientation tuning sharpness of SOS neurons under three different conditions, the angular deviationS, which corresponds to the standard deviation in normal distribution,was calculated (see METHODS for details concerning the calculationof the S value). For the perspective-cue-sensitive neurons (DPand P neurons), the mean S value under the P-only condition (76.1°)was significantly higher (Student's t-test, P < 0.01) than thatunder the D+P condition (68.4°), suggesting a broader orientationtuning under the P-only condition. For the disparity-cue-sensitiveneurons (DP and D neurons), the mean S value under the D-onlycondition (68.5°) and that under the D+P condition (69.3°) didnot differ significantly (Student's t-test, P > 0.10). For theneurons sensitive to both disparity and perspective cues (DP neuron),the mean S value under the P-only condition (76.3°) was significantlyhigher (Student's t-test, P < 0.01) than that under the D-onlycondition (68.0°) or that under the D+P condition (68.6°), suggestinga broader orientation tuning under the P-only condition in thisgroup. These data suggest that the orientation selectivity inmany SOS neurons tends to be relatively weak when only perspectivecues areavailable.

Muscimol microinjection

After the completion of the unit recording experiments, we microinjected muscimol into the caudal part of the lateral bankof the intraparietal sulcus (area CIP), where we recorded theresponses of SOS neurons (Fig. 6A), for the reversible functionalblock of this area.

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Fig. 6. A: muscimol injection sites were superimposed on the trace of the frontoparallel section of the left hemisphere of one monkey. $open circle$ , $triangle$ , and +, the injection points in 3 effective injection cases;

, those in 3 ineffective cases. In one case (+), muscimol was injected at 3 points along the lateral bank of IPS. Muscimol was injected at a single point in all other cases. B: time course of the success rate after muscimol injection in case 1. Only the performance level under the D-only condition decreased immediately after the injection and remained low for at least 3 h. It returned to the normal level on the next day (24 h). C: success rates before (

) and after (

) the injection in 3 positive cases. Graphs 1, 2, and 3 represent the success rates of cases indicated in the plot above by $open circle$ , $triangle$ , and +, respectively. * P < 0.05.

Out of six inactivation experiments, the performance of 3D surface orientation discrimination in the DMTS task was impairedin three cases (Fig. 6C). In one case (case 3), in which muscimolwas microinjected into three spots rostrocaudally along area CIP,the performance of 3D surface orientation discrimination underboth D-only and D+P conditions became significantly worse thanthat before microinjection, although 2D shape discrimination (seeMETHODS) was not affected. In two cases (cases 1 and 2), in whichmuscimol was microinjected into only one spot in area CIP, onlythe performance under the D-only condition was impaired aftermicroinjection.

Figure 6B shows the time course of the level of task performance after microinjection in case 1. The performance level underthe D-only condition decreased immediately after microinjectionand remained impaired for at least 3 h, then returned to the normallevel after 24 h. However, the ability to discriminate the 2Dshape was not impaired atall.

	DISCUSSION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

The present study demonstrates that linear perspective is effective as cues for 3D surface orientation in many SOS neuronsof area CIP, although they are less effective compared with binoculardisparity cues. It was also demonstrated that perspective cuesare integrated with disparity cues in many SOS neurons to generatethe representation of 3D surface orientation. Furthermore, theperformance of 3D surface orientation discrimination was impairedfollowing the inactivation of SOS neurons. These results stronglysupport the view that the activity of SOS neurons is a neuralcorrelate of the perception of 3D surfaceorientation.

Representation of 3D surface orientation in SOS neurons of area CIP

In the single-unit recording experiment, more than one-half (58%, 36/62) of all SOS neurons responded selectively to surfaceorientation under the P-only condition. This result suggests thatmany SOS neurons can encode the surface orientation with perspectivecues alone. However, perspective cues seem to be less importantthan disparity cues for SOS neurons, because the proportion ofperspective-sensitive neurons (58%, 36/62) was smaller than thatof disparity-sensitive neurons (86%, 30/35), and the proportionof neurons sensitive to perspective cues alone (P neuron, 2/35)was much smaller than that of neurons sensitive to disparity cuesalone (D neuron, 11/35). The finding that disparity cues are ofgreat importance is in line with the finding in our previous studiesthat the majority of SOS neurons are sensitive to binocular disparitycues (Shikata et al. 1996; Taira et al. 2000). On the other hand,it appears that monocular cues of linear perspective are incorporatedwith binocular disparity cues in area CIP to represent surfaceorientation, because the majority (19/35) of SOS neurons weresensitive to both disparity and perspective cues (DP neuron).In this type of neuron, summation of the effect of disparity andperspective cues was observed in the response magnitude; the responseto the preferred orientation was stronger under the D+P conditionthan under the D-only and P-only conditions (Fig. 4A). Since itis a general phenomenon in visual perception that the presenceof a larger number of cues enables clearer perception of visualfeatures, the activity of DP neurons may be strongly related tothe perception and judgment concerning 3D surfaceorientation.

Results of the analysis of correlation of the preferred orientations provide strong support for the notion that SOS neuronsutilize linear perspective cues to represent 3D surface orientation.Since the preferred orientations under the P-only condition tendedto coincide with those under the D+P condition in many of perspective-sensitiveneurons (Fig. 5, A and B), it was suggested that they do not simplyrespond to a 2D shape (trapezoid) in different orientations, butthat they extract the signal of 3D surface orientation from a2D contour viewed in a linear perspective. In other words, theseneurons interpreted the stimuli as the silhouette of a squareplate slanted in depth, rather than that of a frontoparallel trapezoid.The notion was also supported by the coincidence of the preferredorientations under the D-only and P-only conditions in neuronsthat are sensitive to both disparity and perspective cues (DPneurons, Fig. 5, E and F). Thus the nature of the perspective-sensitiveSOS neurons should be distinguished from that of neurons in othercortical areas, such as the inferior temporal cortex, selectiveto 2D shapes reported previously (Desimone et al. 1984; Fujitaet al. 1992; Gross et al. 1972; Kobatake and Tanaka 1994; Rollset al. 1977; Tanaka et al. 1991), in the sense that the perspective-sensitiveSOS neurons extract the signal of 3D surface orientation froma 2Dimage.

Results of the analysis of tuning sharpness also suggested that perspective cues have a weaker effect than disparity cueson the response of SOS neurons. In perspective-sensitive neurons,tuning was broader under the P-only condition than under the D+Pcondition (mean S value 76.1 and 68.4°, respectively), while indisparity-sensitive neurons, tuning sharpness under the D-onlycondition and that under the D+P condition were almost the same(mean S value 68.5 and 69.3°, respectively). Furthermore, in neuronssensitive to both disparity and perspective cues (DP neurons),tuning was broader under the P-only condition than under the D-onlycondition (mean S value 76.3 and 68.0°, respectively). These datasuggest that the orientation selectivity in many SOS neurons tendsto be relatively weak when only perspective cues are available.This relatively weak effect of perspective cues compared withthat of disparity cues may be partly responsible for the weakercoincidence of orientation preference between the P-only and D+Pconditions in perspective-sensitive neurons (Fig. 5, A and B)than that between the D-only and D+P conditions in disparity-sensitiveneurons (Fig. 5, C and D), and the relatively weak coincidenceof orientation preference between the D-only and P-only conditionsin DP neurons (Fig. 5, E and F).

The dominance of disparity cues over perspective cues in the response of SOS neurons is in good correspondence with psychophysicalfindings. Since the perspective cues are somewhat ambiguous comparedwith disparity cues, the judgment of a surface slant is oftenunstable when based only on perspective cues, and the judgmentis much more reliable when perspective cues are coupled with binoculardisparity cues (Clark et al. 1955; Olson 1974). However, it ispossible that we have underestimated the effect of perspectivecues in the present study. Since we binocularly presented theSF with perspective cues alone instead of monocularly presentingthem under the P-only condition, the power of perspective cuesmay have been weakened to some extent by conflicting with thoseof disparity cues, which provide information that the figure isin the frontoparallel orientation. This kind of cue conflict alwaysoccurs when we look at a painting or a photograph with both eyesopen. The sensation of a 3D space becomes slightly stronger whenwe look at them monocularly (Koenderink et al. 1994).

Area CIP and the perception of 3D surface orientation

In muscimol microinjection experiments, the ability to discriminate a 3D surface orientation was selectively impaired followingthe inactivation of SOS neurons in area CIP, while the abilityto discriminate a 2D shape remained intact. On the basis of thisobservation, it was suggested that a 3D surface orientation isa discrete perceptual entity and that its perception is directlyachieved by the activity of SOS neurons in areaCIP.

There were three effective cases out of six microinjection experiments (Fig. 6C). In the case of muscimol being microinjectedinto a relatively large area (case 3), discrimination of a 3Dsurface orientation was impaired under both the D+P and D-onlyconditions. However, in two of three effective cases in whichmuscimol was microinjected into only one spot in area CIP (cases1 and 2), discrimination of a 3D surface orientation was impairedonly under the D-only condition but not under the D+P condition.One possible interpretation of these results is that the muscimolmicroinjection into a single spot may have selectively inactivatedD neurons leading to a selective effect under the D-only condition.However, this interpretation is unlikely because the distributionsof DP and D neurons did not differ in area CIP. The response propertyof neurons in area CIP revealed by the single-unit recording experimentssuggests another possibility. The activity of the entire populationof SOS neurons may have been higher under the D+P condition thanunder the D-only condition, because the activity of DP neuronswas enhanced under the D+P condition. It is a general phenomenonin visual perception that the presence of a larger number of cuesenables easier perception of visual features. Under the D+P condition,in which whole population activity was relatively high, inactivationof a large number of neurons in area CIP with a relatively largeamount of muscimol may have been necessary to affect the performanceofdiscrimination.

There were effective and ineffective cases of muscimol microinjection experiments, although the injection sites were almostthe same in all injection cases. One possible explanation forthis is that the behavioral task was not sufficiently sensitiveto detect a subtle change in perceptive ability caused by suchsmall amounts of muscimol. In the present study, the differencein tilt angles between a pair of sample and test stimuli in NO-GOtrials in the DMTS task ranged from 45 to 180° at 45 intervals(see METHODS). If the difference in tilt angles had been sufficientlysmall to be close to the threshold level of the monkey's orientationdiscrimination, we might have found some impairment in the three"ineffective"cases.

The main findings in muscimol microinjection experiments that a 3D surface orientation is a discrete perceptual entity andthat its perception is directly achieved by the activity of neuronsin area CIP are in good agreement with those in human studies.In positron emission tomography (PET) and fMRI studies with humansubjects, the caudal part of the intraparietal area, which seemsto correspond to the monkey area CIP, was activated while thesubjects discriminated a 3D surface orientation based on texturegradients (Shikata et al. 2001), or a 3D surface geometry (convex-concave)based on monocular cues of shading (Taira et al. 2001) or binocularcues of disparity (Taira et al. 1997). Neurological studies haveshown that 3D constructional apraxia occurs in patients with rightparietal lobe lesions (Critchley 1953; De Renzi 1982). These patientsshowed abnormalities in assembling blocks according to a 3D modeland drew a characteristic line drawing with no linear perspective.Furthermore, patients with parietal lesions were reported to exhibitsevere impairment in 3D perception (Holmes and Horrax 1919; Riddoch1917; Rothstein and Sacks 1972). It is notable that these patientsseem to have problems not only in stereopsis (use of binoculardisparity) but also in the use of monocular cues such as linearperspective andshadings.

Relations of area CIP to other cortical areas

The intraparietal area including area CIP is a part of the dorsal visual pathway and receives strong input from the V3-V3Acomplex, where columns based on binocular disparity tuning arefound (Adams 1997). Area CIP appears to receive binocular disparitysignals from this area. However, it is not yet determined fromwhich region area CIP receives information regarding monocularcues. The most plausible candidates are certain areas in the ventralvisual pathway. A group of neurons that selectively respondedto 2D shape, texture, or shading was identified in the inferotemporalcortex (Desimone et al. 1984; Fujita et al. 1992; Gross et al.1972; Kobatake and Tanaka 1994; Rolls et al. 1977; Tanaka et al.1991). The intraparietal area including area CIP appears to receiveinput from areas in the ventral visual pathway (Baizer et al.1991; Webster et al. 1994).

Recently, neurons representing 3D curvature of a surface were found in the lower bank of the superior temporal sulcus (STS)in the rostral temporal cortex (area TEs) (Janssen et al. 1999,2000a,b). This area appears to be interconnected with area CIP(Baizer et al. 1991). It is one of the objectives of future researchto reveal how area CIP and area TEs, one in the dorsal pathwayand the other in the ventral pathway, cooperate with each otherto represent 3D structures of objects. One characteristic of areaCIP may be its anatomically close location to the area relatedto hand manipulation movements. In the anterior part of the lateralbank of the intraparietal sulcus (area AIP), a group of neuronswas found to be related to hand manipulation movements, and manyof these neurons were visually sensitive to the axis and surfaceorientations of objects as well as to their shape (Murata et al.2000; Sakata et al. 1995; Taira et al. 1990). These neurons arelikely to receive information regarding axis and surface orientationsfrom area CIP neurons. As proposed in our previous studies (Sakataet al. 1997, 1998; Taira et al. 2000), area CIP seems to providea viewer-centered representation of 3D surfaces for the manipulationof objects. On the other hand, area TE seems to be more closelyrelated to object recognition, because a lesion in the inferiortemporal cortex causes severe impairment of object recognition(Dean 1976; Iwai and Mishkin 1969; Weiskrantz and Saunders 1984),and many neurons in area TE respond selectively to a complex 2Dshape and texture (Desimone et al. 1984; Fujita et al. 1992; Grosset al. 1972; Kobatake and Tanaka 1994; Rolls et al. 1977; Tanakaet al. 1991).

	ACKNOWLEDGMENTS

We thank Solidray Co., Ltd. for help in developing the computer programs for our experiment. MRIs of the monkey brains weretaken at the Laboratory for Magnetic Resonance Imaging and Spectroscopy,National Institute for Physiological Science and are availableon the Web at http://www.med.nihon-u.ac.jp/department/physiol1/.

Part of this study was supported by Grants-in-Aid for Scientific Research on Priority Areas (07244103, 10680768, 50179397)and a Grant-in-Aid for Japan Society for the Promotion of ScienceFellows (199900008) from the Ministry of Education, Science, Sportsand Culture, a Grant-in-Aid for Target-Oriented Research and Developmentin Brain Science from the Science and Technology Agency, and Grants-in-Aidfor Scientific Research (13680903) and for Scientific Researchon Priority Areas (13210126) from the Ministry of Education, Culture,Sports, Science andTechnology.

	FOOTNOTES

Address for reprint requests: M. Taira, Dept. of Physiology, Nihon University School of Medicine, 30-1 Ohyaguchi-kamimachi,Itabashi, Tokyo 173-8610, Japan (E-mail: masato{at}med.nihon-u.ac.jp).

Received 27 November 2000; accepted in final form 2 August 2001.

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