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Previous Article | Next Article
The Journal of Neuroscience, July 15, 2000, 20(14):5552-5563
Visual Responses of Neurons in the Middle Temporal Area of New World Monkeys after Lesions of Striate Cortex
Marcello G. P. Rosa1, 2, Rowan Tweedale1, and Guy N. Elston1 1 Vision, Touch, and Hearing Research Centre, The University of Queensland, QLD 4072, Australia, and 2 Department of Physiology, Monash University, VIC 3800, Australia
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
In primates, lesions of striate cortex (V1) result in scotomas in which only rudimentary visual abilities remain. These aspects of vision that survive V1 lesions have been attributed to direct thalamic pathways to extrastriate areas, including the middle temporal area (MT). However, studies in New World monkeys and humans have questioned this interpretation, suggesting that remnants of V1 are responsible for both the activation of MT and residual vision. We studied the visual responses of neurons in area MT in New World marmoset monkeys in the weeks after lesions of V1. The extent of the scotoma in each case was estimated by mapping the receptive fields of cells located near the lesion border and by histological reconstruction. Two response types were observed among the cells located in the part of MT that corresponds, in visuotopic coordinates, to the lesioned part of V1. Many neurons (62%) had receptive fields that were displaced relative to their expected location, so that they represented the visual field immediately surrounding the scotoma. This may be a consequence of a process analogous to the reorganization of the V1 map after retinal lesions. However, another 20% of the cells had receptive fields centered inside the scotoma. Most of these neurons were strongly direction-selective, similar to normal MT cells. These results show that MT cells differ in their responses to lesioning of V1 and that only a subpopulation of MT neurons can be reasonably linked to residual vision and blindsight.
Key words: marmoset; vision; extrastriate; receptive fields; blindsight; scotoma
INTRODUCTION
In primates, lesioning of occipital cortex leads to a scotoma, the extent of which corresponds to the affected portion of the visuotopic map in striate cortex (area V1) (Grüsser and Landis, 1992
). However, some visual functions remain within the affected visual field sector. For example, studies using forced-choice psychophysical tests have revealed that patients with V1 lesions can still orient toward stimuli presented within the scotoma and are even capable of correctly "guessing" some characteristics of these stimuli (Stoerig and Cowey, 1997
Interpretations of the sources of blindsight and residual vision are typically based on the activity of extrastriate visual areas, activated by thalamic routes that bypass V1. Lesions (Rodman et al., 1989
An important issue is whether the visuotopic organization of area MT is altered by long-term lesions of V1. Studies using retinal lesions have revealed a significant potential for plasticity in the visuotopic representations in cortex (Kaas et al., 1990
MATERIALS AND METHODS
Six marmosets (Callithrix jacchus) received a unilateral lesion of V1, whereas six nontreated animals, used for a previous study (Rosa and Elston, 1998
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Table 1. Animals and survival times after lesion Cortical lesions. The animals were anesthetized with intramuscular injections of ketamine (50 mg/kg) combined with xylazine (3 mg/kg). Additional doses of ketamine (5-10 mg) were used to maintain a surgical level of anesthesia (evaluated by monitoring the leg withdrawal and corneal reflexes). Injections of dexamethasone (0.4 mg/kg, i.m.) and atropine (0.15 mg/kg, i.m.) were also administered. Under sterile conditions, a craniotomy was made over the occipital pole of the right hemisphere, allowing access to V1. After removal of the dura mater, a suction probe was used to destroy V1, using previously published stereotaxic coordinates and visuotopic maps of this area as guides (Fritsches and Rosa, 1996
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Figure 1. Location and visuotopy of areas V1 and MT in the marmoset monkey, shown on lateral and medial (mirror-reversed) views of a right hemisphere. In the medial view, the banks of the calcarine sulcus were opened to reveal the part of V1 hidden therein. Isoeccentricity lines (2.5, 5, 10, 20, 40, and 60°) are indicated by thin dotted lines, and isopolar lines ( 45, +45, and HM) are indicated by thin continuous lines. The intended ablation (caudal to the plane shown by the thick dashed line) would remove the central representation of V1 up to 20-30° of eccentricity.
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Figure 2. Extent of the V1 lesions and scotomas in four animals. For each case, the estimated extent of the scotoma (gray) is indicated on a view of the central 40° of the visual field (HM and VM). The receptive fields of V1 neurons used as the basis for this estimate, which were recorded at sites near the lesion border, are also illustrated (rectangles and ovals). The insets at the bottom of each diagram show a projection of the extent of the scotoma on an averaged map of marmoset V1 (from Fritsches and Rosa, 1996
Electrophysiological recordings: animal care and preparation. Each of the animals underwent a single recording session. The procedures for anesthetic induction and medication were the same as those described for the lesion surgery. A tracheotomy was performed, and a tracheal tube was inserted to enable artificial ventilation. The marmoset was placed on a thermostatically controlled heating pad, and its head was positioned in a stereotaxic frame. The cortex was exposed, and an acrylic well was constructed around the craniotomy, being secured to the skull by orthopedic screws. A rod attached to an adjustable arm (mounted on the stereotaxic frame) was positioned over the frontal midline and fixed to the acrylic well. This arrangement allowed the head to be supported without the need for stereotaxic bars and offered an unhindered field of vision. The well was then filled with silicone oil, and a picture of the cortical surface was taken for plotting of electrode penetration sites.
After all surgical procedures were completed, the animal was administered an intravenous infusion of a mixture of pancuronium bromide (0.1 mg · kg
1 · h
Protection of the cornea, dioptric correction, and control for eye movements. Administration of atropine (1%) and phenylephrine hydrochloride (10%) eye drops resulted in mydriasis and cycloplegia. Application of a hard contact lens with a curvature radius of 3.4-3.6 mm focused the left eye (contralateral to the lesion) on the surface of a translucent hemispheric screen (radius of 60 cm) and protected the cornea from desiccation. Repeated ophthalmoscopic inspections revealed that optic media quality remained stable throughout the recordings. The right eye was also covered with a contact lens for protection but was kept covered by an opaque metal shield, except for occasional checks (e.g., when a cell responded poorly to the left eye or when responses were sampled in the hemisphere contralateral to the lesion). A reversible ophthalmoscope was used to project the position of the optic disks and foveae onto the hemispheric screen. The horizontal meridian (HM) of the visual field was defined as a line connecting the centers of the left eye fovea and blind spot (Troilo et al., 1993
Electrophysiological recordings. The electrophysiological experiments consisted of three consecutive phases: (1) mapping of receptive fields in MT and surrounding areas, using hand-held stimuli; (2) mapping of receptive fields in V1, in tissue immediately surrounding the lesion, using hand-held stimuli; and (3) Quantitative analysis of single-unit responses at selected recording sites, using stimuli presented within and outside the estimated boundaries of the scotoma.
In all three phases of the experiment, tungsten-in-glass microelectrodes with an exposed tip of 10 µm were inserted in the vertical stereotaxic plane. Amplification and filtering of the electrophysiological signal was achieved via an AM Systems Model 1800 Microelectrode AC amplifier (AM Systems, Everett, WA) and a 50 Hz eliminator (HumBug; Quest Scientific, Vancouver, Canada). The signal was further processed by a computer-based waveform discrimination system (SPS-8701; Signal Processing Systems, Adelaide, Australia; operated on a 133MHz Pentium computer), which allowed the isolation of single-unit spike trains with high temporal resolution.
The experiment started with the qualitative study of receptive field extent and direction selectivity of neurons in MT. The protocol and techniques were the same as those used in our study of MT in normal marmosets (Rosa and Elston, 1998
Once the first phase of the experiment was deemed complete (typically after six to eight electrode tracks), additional electrode penetrations were aimed at the remnant part of V1, near the boundaries of the lesion. The aim of this phase of the experiment was to enable an estimation of the boundaries of the scotoma caused by the V1 lesion (in this paper, we use the word "scotoma" to refer to the region of the visual field that was originally represented in the ablated part of V1; this usage is justified on the basis of the symptoms experienced by humans and other primates after similar lesions). To obtain an estimate of the borders of the scotoma during the recording session, the electrode was moved from caudal to rostral, in rows perpendicular to the lesion border, until the first responses were obtained. Recordings were obtained at various depths, including in the calcarine sulcus and on the ventral surface. The borders of the scotoma were then estimated by drawing a line joining the inner boundaries of the receptive fields mapped at the recording sites nearest to the borders of the lesion. In some regions, the extent of the lesion was such that it reached the border between V1 and the second visual area (V2). This resulted in no responses along some parts of the perimeter of the lesion, indicating that, as in other monkeys (Cowey, 1964
In the third part of the experiments, the electrode was again aimed at MT, with the objective of quantitatively studying the single-unit responses to stimuli presented either inside or outside the scotoma. For these analyses, the spike trains processed by the SPS-8701 system were collected via a high-fidelity interface (ITC-16 Nubus; Instrutech Corp., Great Neck, NY) into a Macintosh Power PC 604e/120MHz computer (Apple Computers, Cupertino, CA), which also controlled visual stimulus generation. High-contrast drifting sine wave gratings were generated by a stimulus/data collection software package (A/DVance 3.55; McKellar Designs, Vancouver, British Columbia, Canada). These stimuli were presented on an Apple Multiple Scan 20 inch monitor (Apple Computers) located 60 cm from the eyes. The screen resolution was set to 1152 × 870 pixels, and the refresh rate was set to 75 Hz. The spatiotemporal characteristics of the stimuli were adjusted for each cell while qualitatively monitoring the responses of the cell to a full screen grating. After that, quantitative tests were performed to quantify the direction and speed sensitivities of the neuron in response to two types of stimulus: a drifting grating that nearly completely filled the estimated borders of the scotoma (the "inside" condition) and the same grating presented to the entire screen, except for the scotoma (the "outside" condition). In both conditions, the remaining part of the screen was presented with a nonmodulated gray, the luminance of which matched the average of the grating pattern. The gray pattern also covered a strip of the visual field that included the approximate borders of the scotoma, estimated as explained above. The width of this strip was 2° centrally but increased toward the periphery according to the known relationship between receptive field size and eccentricity in V1 (Fritsches and Rosa, 1996
Histology. At the end of the experiment, the animal was given a lethal dose of sodium pentobarbitone (100 mg/kg) and perfused transcardially with 0.9% saline, followed by 4% paraformaldehyde in 0.1 M phosphate buffer, pH 7.4. Once the brain was removed from the skull, it was placed into fixative with increasing concentrations of sucrose and sectioned into 40 µm coronal slices using a freezing microtome. Alternate series were stained for Nissl substance (with cresyl violet) and myelin (Schmued, 1990
Determination of the extent of the scotomas. For the purposes of data analysis, the determination of the extent of the scotomas caused by the lesions was based on a process of successive approximations, starting with the examination of histological sections through the remaining parts of V1. The limits of V1 were located using architectonic criteria (Gebhard et al., 1993
RESULTS
The main conclusions of this study can be summarized as follows. First, several weeks after unilateral V1 ablations, visually responsive neurons are found throughout MT ipsilateral to the lesion. Second, comparison between the extent and visuotopy of MT in normal animals and animals with V1 lesions allows the estimation of a "lesion projection zone", i.e., the part of MT in which cells are expected to be affected by the V1 lesion. In the lesion projection zone, threshold mapping of receptive field boundaries often reveals that the receptive fields are displaced beyond the borders of the scotoma. This results in a complex visual topography not seen in normal animals, including sudden jumps in receptive field position and receptive fields comprising two different parts of the visual field. Third, a subgroup of MT cells within the lesion projection zone retain receptive fields that are entirely or partially located within the borders of the scotoma. These cells alternate with cells showing "displaced" receptive fields, sometimes along the same electrode track, in an apparently nonsystematic way. Last, most neurons in MT remain strongly direction selective, both within and outside the lesion projection zone.
Receptive field mapping
In a previous study (Rosa and Elston, 1998
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Figure 3. Visuotopic organization of MT in a normal marmoset. Top left, Lateral view of the marmoset brain with the location of MT shown in gray. Middle left, Magnified view of graphically "unfolded" MT, with the locations of recording sites obtained at five successive rostrocaudal levels indicated by horizontal line segments. Bottom left, Reconstructed visuotopy of MT, based on the correlation between these recording sites and the receptive fields illustrated on the right. In the right diagram, receptive fields from the same rostrocaudal level are connected in sequences that correspond to sites progressing from dorsal to caudal in the cortex (e.g., 1-8, 9-15, etc.). For clarity, not every recording site or receptive field obtained in this case is illustrated (Rosa and Elston, 1998
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Figure 4. Recording sites and receptive fields in MT of an animal with a V1 lesion (case #7). The sections (left of each panel) correspond to a plane slightly tilted from coronal. The MT cortex is shown magnified, with the location of recording sites obtained in an electrode penetration (circles and crosses) indicated. Black circles indicate cells with weakly or nonhabituating responses, white circles indicate cells with strongly habituating responses, and crosses indicate cells that did not respond to the stimuli used. The borders of MT are indicated by dashed lines. The locations of these electrode penetrations, projected to two-dimensional maps of MT, are indicated by the dotted lines in the top left diagrams. The diagrams on the right of each panel illustrate a portion of the animal's visual field, with the extent of the scotoma shown in gray and receptive fields indicated by rectangles or ovals. The preferred direction of motion of each cell is indicated next to its designation (cell h responded equally well to movement in all directions).
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Figure 5. Recording sites and receptive fields in MT of an animal with a V1 lesion (case #4). In the right diagram, the receptive fields are indicated using different line patterns only for clarity. Other conventions as in Figure 4.
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Figure 6. Recording sites and receptive fields in MT of an animal with a V1 lesion (case #6).
The recording sites and receptive fields illustrated in the left panel of Figure 4 exemplify a common result observed in the mapping experiments; the receptive fields avoid the interior of the scotoma, instead representing portions of the visual field immediately outside its borders. The first receptive fields mapped in this track (fields 1-6) follow the normal pattern of representation in MT, moving from the lower field toward the upper field, with some overlap. However, once the lower limit of the scotoma is reached (field 6), this pattern is disrupted. The receptive fields mapped in the next four recording sites (fields 7-10) essentially re-represent the same sector of the visual field represented by field 6. They are followed by a nonoverlapping receptive field around the upper edge of the scotoma (field 11) and an unresponsive neuron (indicated by the x along the penetration). The penetration is completed with two recording sites yielding receptive fields near the vertical meridian (fields 12, 13) and two unresponsive layer 6 cells. Several characteristics of this track are unusual compared with those obtained in normal animals. First, neurons at five consecutive sites (fields 6-10), covering over 1 mm of cortex, re-represent the same region at the lower edge of the scotoma. Second, an electrode movement of as little as 200 µm is sufficient to yield nonoverlapping fields (fields 10, 11). Finally, there are several sites at which neurons do not respond to any of the stimuli used. A variant of this pattern in shown in Figure 6 (left panel) in which the receptive fields follow a broad arc along the lower edge of the scotoma (fields 1-6) and then jump to its upper edge within 240 µm (recording sites and fields 6, 7).
The tracks illustrated in Figure 5 and in the right panels of Figures 4 and 6 demonstrate that not all receptive fields of neurons in MT of lesioned animals avoid the scotoma. For example, in the track shown in the left panel of Figure 5, two receptive fields (fields 7, 8) have boundaries entirely restricted to the scotoma. Indeed, the visuotopic organization revealed by this track resembles that obtained in control animals, with the receptive fields moving gradually from the lower to the upper field. This is not, however, the typical result; more often than not, neurons with receptive fields located entirely inside the scotoma alternate with neurons with displaced fields, often in the same track. This results in a somewhat disorganized representation compared with that of normal animals. For example, in the track illustrated in the right panel of Figure 5, two cells with receptive fields partially overlapping the lower boundary of the scotoma (a, b) are followed, within 150 µm, by a cell with a non-overlapping receptive field (c) representing a small pocket of spared visual field near the fovea [although no penetrations were aimed at this part of V1 (Fig. 2), the existence of this spared region was confirmed by both the presence of responsive V2 cells covering that part of the visual field and histological reconstruction]. The sequence of receptive fields centers then "backtracks," such that four consecutive cells with receptive fields located in the scotoma (d, g) are observed. After that, the normal lower-to-upper quadrant gradient is resumed (fields h-k). Essentially the same pattern was found in the sequence shown in Figure 4 (right). Finally, the track illustrated in the right panel of Figure 6 illustrates alternation between cells with peripheral receptive fields inside the scotoma and those with displaced receptive fields; four cells with receptive fields that follow the normal MT visuotopic gradient (a-d) are followed by a cell with a split receptive field (e), responding to stimulation of both the upper and lower edges of the scotoma. The receptive fields of the following three cells then zigzag between the interior of the scotoma (g) and its upper edge (f, h) before resuming the normal topography and approaching the upper vertical meridian (i-n). There were no clear differences between animals that could be related to the degree of V2 involvement in the lesion. Each of the six cases yielded evidence of both visuotopic reorganization and residual responses inside the scotoma.
Percentages of neurons with different response properties
To assess the changes in the responses of MT cells compared with control animals, it was first necessary to estimate the sectors of MT likely to have originally represented the same part of the visual field as the ablated portion of V1. For simplicity, we will refer to these sectors of MT as the lesion projection zones. The procedure for estimating the prelesion visuotopic maps of MT, and hence the lesion projection zones, is illustrated for three animals in the left column of Figure 7. The estimated "control" location of isoeccentricity and polar lines (Rosa and Elston, 1998
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Figure 7. Left, Estimates of the "normal" (prelesion) visuotopic organization of MT in three animals. The estimated locations of isoeccentricity and isopolar lines are shown, based on the averaged map of MT in six normal animals. The recording sites shown as black circles were used as a guide in regions outside the lesion projection zones. The dashed lines are estimates only. Right, Arrow diagrams indicating the displacement of visuotopic coordinates for individual recording sites. In these diagrams, the extent of the lesion projection zones is shown in gray. For cells within the lesion projection zones, an arrow connects the location of the recording site (circle) to the point of the estimated prelesion map corresponding to the location of the receptive field center. An arrow terminating outside the map indicates a receptive field center in the ipsilateral hemifield. For cells outside the lesion projection zones, this is indicated by a line segment without an arrowhead. The crosses indicate the location of nonresponsive neurons. In view of the density of recordings in the central representation of case #4, for clarity some recording sites are not included in the arrow diagram (top right).
The arrow diagrams shown in the right column of Figure 7 provide an intuitive view of the extent of receptive field displacement for each recording site in three animals. The arrows and lines connect the position of each recording site to the location in the visuotopic map corresponding to the geometric center of the neuronal receptive field recorded therein. Thus, the longer the arrow, the farther the receptive field center is from its predicted position (Calford et al., 1999
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Figure 8. Top, Extent of visuotopic "reorganization" within and outside the lesion projection zones, estimated as illustrated in Figure 7. For sites outside the lesion projection zone (black bars), this indicates the error in estimate attributable to sparse sampling and the normal receptive field scatter. The radius of the point-image size (mean + 2 SD) in normal marmoset MT is indicated by the arrow. Bottom, Percentages of neurons with different functional characteristics in terms of direction selectivity (left) and habituation (right).
Overall, 62% (86 of 139) of the recording sites estimated to be located within the lesion projection zones yielded cells with displaced receptive fields centered outside the scotoma. This percentage takes into consideration only the location of the geometric center of the receptive field; many of these receptive fields invaded the scotoma to some extent (Fig. 4, fields 8-10). Moreover, 20% (28 of 139) of the sites within the lesion projection zones yielded cells with receptive fields centered within the scotoma, whereas only 18% (25 of 139) yielded cells with spontaneous activity but did not respond to any of the stimuli used. This percentage of nonresponsive recordings was much higher (
2 = 130.6; DF = 1; p < 0.0001) than that observed outside the lesion projection zones (2%) or in MT of nonlesioned animals (<1%).
The proportions of unidirectional, bidirectional, and pandirectional cells inside and outside the lesion projection zones are illustrated in the bottom panel of Figure 8 (these percentages refer to the population of responsive neurons only). These distributions are not statistically different (
Quantitative assessment of response properties
For 36 neurons, we sought to confirm that responses can be evoked from stimulation of the region of the visual field inside the scotoma caused by the V1 lesion. As illustrated in Figure 9A, this was based on the presentation of drifting sine wave grating patterns that were either restricted to the scotoma (the inside condition) or the surrounding visual field (the outside condition). A ring of visual field surrounding the borders of the scotoma, as estimated during the experiment, was left nonstimulated in both situations. This procedure was chosen so that the assessment of the responsiveness of MT cells to stimulation of the visual field inside the scotoma was independent of the precision of the borders of hand-mapped MT receptive fields. Of the 36 cells, nearly half (17 of 36) showed no significant response to stimulation of the visual field inside the scotoma. This number includes some cells, such as cell 1 in Figure 9, that were not located in the lesion projection zone. Five other cells, all from one animal, were discarded because the size of the scotoma was overestimated during the experiment, and there was inadvertent stimulation of spared visual field in the inside condition. Thus, 13 of the cells unequivocally responded to stimulation restricted to the scotoma.
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Figure 9. Single-unit analysis of direction selectivity of MT neurons. A, Diagramatic view of the outside and inside conditions of stimulus presentation. The dashed line shows the extent of the scotoma in this case, and the grating pattern shows the portion of the visual field stimulated in each condition. B, Location of the (hand-mapped) receptive fields of 10 neurons in relation to the scotoma. C, Bidimensional reconstruction of MT, with the estimated extent of the lesion projection zone shown in gray and the recording sites indicated by circles. The other panels illustrate, for each cell, peristimulus time histograms of the activity in response to stimulation of the outside (top three rows) and inside (bottom three rows) of the scotoma. The histograms on the left represent the responses to stimulus movement in the preferred direction of motion of the cell, and those on the right, responses to movement in a direction 180° from that. The results of stimulation at three different speeds (10, 40, and 90°/sec) are illustrated. The polar plots summarize the direction selectivities, assessed with full-screen gratings.
The responses of 10 MT neurons, studied in two electrode penetrations, are illustrated in Figure 9. For each cell, a polar plot is illustrated, showing its selectivity in response to full-screen gratings crossing the screen in different directions. Confirming the results of the qualitative assessment described above, every responsive cell in these penetrations was found to have a significant direction bias. The panels in Figure 9 also illustrate peristimulus time histograms that reflect, for each cell, the results of stimulation of the visual field outside (top three rows) and inside (bottom three rows) the scotoma. The responses to gratings moving both in the optimal direction of the neuron (arrow pointing to the right) and a direction 180° from that (arrow pointing to the left) are illustrated. These results demonstrate that some neurons in MT show significant responses to stimulation of the visual field inside the scotoma and that these responses are typically direction-selective. Indeed, for some of the neurons (e.g., cells 4 and b) the responses to stimulation restricted to the scotoma can be stronger than those obtained by stimulating the visual field surrounding it. In most cases, the results of the quantitative tests were compatible with the location of the hand-mapped receptive fields. For example, cell 1 only responded to the outside condition, whereas cell 4 responded much more strongly to the inside condition. However, some discrepancies were observed, such as cell 2 responding to the inside condition despite having a hand-mapped receptive field that only touched the edge of the scotoma.
In the experiment shown in Figure 9 (but not in other cases), each cell was also systematically tested with stimuli drifting at different speeds (10, 40, and 90°/sec). Although the sample was small, the data do demonstrate that different cells in the lesion projection zone of MT are tuned to different velocities of stimuli presented within the scotoma. For example, cell b shows a strong response to the slow drifting (10°/sec) stimulus, whereas cells 3 and 4 are most strongly responsive to the fastest drifting (90°/sec) pattern.
DISCUSSION
Weeks after lesions of striate cortex, neurons in MT show two types of response properties with respect to receptive field location. Some cells remain responsive to stimulation of the region of the visual field originally represented in the ablated part of V1 (the scotoma), whereas others have receptive fields that appear displaced from their likely original location, so that they represent the visual field immediately surrounding the scotoma. There is also a significant increase in the proportion of cells that do not respond to stimuli such as bars and spots and in the proportion of cells which strongly habituate to repetitive stimulation. Among the responsive cells, the proportion of those with direction selectivity is unaltered.
Using a lesion paradigm similar to the one adopted here, Rodman et al. (1989)
The existence of cells in MT that respond to stimulation of the visual field inside the scotoma makes it plausible that activity of extrastriate areas can explain blindsight and the limited residual vision of primates (including human patients) with V1 lesions. However, some studies (Fendrich et al., 1992
A large proportion of cells in the lesion projection zones of MT have receptive fields that appear displaced from their expected location, toward the visual field immediately outside the scotoma. The validity of this conclusion, and in particular of our estimates of the proportions of cells in different functional categories, depend on the precision of our estimates of the lesion projection zones. However, we have demonstrated previously (Rosa and Elston, 1998
Psychophysical studies in patients rendered hemianopic because of a complete unilateral V1 lesion demonstrate that they have a limited conscious ability to distinguish between stimuli moving in different directions (Perenin, 1991
In summary, New World and Old World monkeys are similar in that a large fraction of MT cells continue to process visual information after removal of afferents from V1. Cells with receptive fields within the scotoma can be reasonably linked to residual vision and blindsight. At the same time, other neurons become sensitive to the region of the visual field that immediately surrounds the scotoma. It will be important to establish the time course of these changes and to determine to what extent they depend on the size of the V1 lesion. If, as we suspect, displaced receptive fields are the result of intrinsic connections from parts of MT that still receive V1 afferents, it is likely that they will be less common in subjects rendered hemianopic by complete ablation of V1, in which the callosal connections may be the only source of excitation from spared portions of the visual field.
FOOTNOTES Received March 27, 2000; revised May 4, 2000; accepted May 5, 2000.
This work was supported by Research Grant 990007 from the National Health and Medical Research Council. The technical assistance of Rita Collins and comments by Dr. T. Vidyasagar are gratefully acknowledged. This paper was written while M.G.P.R. was a Visiting Fellow at the Division of Psychology, Australian National University, Canberra. The use of the equipment and facilities of the Division of Psychology is gratefully acknowledged.
Correspondence should be addressed to Dr. Marcello Rosa at the above address. E-mail: marcello.rosa{at}med.monash.edu.au.
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