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The Journal of Neuroscience, December 15, 1999, 19(24):10931-10939
Saccadic Dysmetria and Adaptation after Lesions of the Cerebellar Cortex
Shabtai Barash1, Armenuhi Melikyan1, Alexey Sivakov1, Mingsha Zhang1, Mitchell Glickstein2, and Peter Thier3 1 Department of Neurobiology, Weizmann Institute of Science, Rehovot 76100, Israel, 2 Department of Anatomy, University College London, London WC1E 6BT, United Kingdom, and 3 Sektion für Visuelle Sensomotorik, Neurologische Universitätsklinik Tübingen, 72076 Tübingen, Germany
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
We studied the effects of small lesions of the oculomotor vermis of the cerebellar cortex on the ability of monkeys to execute and adapt saccadic eye movements. For saccades in one horizontal direction, the lesions led to an initial gross hypometria and a permanent abolition of the capacity for rapid adaptation. Mean saccade amplitude recovered from the initial hypometria, although variability remained high. A series of hundreds of repetitive saccades in the same direction resulted in gradual decrement of amplitude. Saccades in other directions were less strongly affected by the lesions. We suggest the following. (1) The cerebellar cortex is constantly recalibrating the saccadic system, thus compensating for rapid biomechanical changes such as might be caused by muscle fatigue. (2) A mechanism capable of slow recovery from dysmetria is revealed despite the permanent absence of rapid adaptation.
Key words: saccades; saccadic eye movement; saccadic adaptation; fatigue; cerebellum; vermis; dysmetria; lesion; eye movement; recovery; recovery from brain damage; motor learning; cerebellar cortex
INTRODUCTION
Accurate saccadic eye movements are critical for directing the fovea to sites of interest in a given visual scene. The posterior vermis of the cerebellar cortex and its major output, the fastigial nucleus, are related to the control of saccadic accuracy and to saccadic adaptation (for review, see Leigh and Zee, 1990
; Botzel et al., 1993
If the fastigial nucleus is ablated with the cortex of the vermis (Ritchie, 1976
Two types of saccadic adaptation were traditionally thought to exist. Slow adaptation (days) is revealed in the recovery from extraocular muscle paresis (Kommerell et al., 1976
MATERIALS AND METHODS
Our general procedures were recently described in detail (Barash et al., 1998
Each monkey was tested postoperatively in two periods. The "early postlesion" period spanned the first two postlesion weeks (but saccadic dysmetria studies were limited to the first week). The "late postlesion" period spanned days 283-409 in monkey 1 and days 54-103 in monkey 2. Additional visuomotor tasks were tested that are not reported here.
Each of the two male Macaca fascicularis monkeys went through two surgical procedures. First, they were implanted with a scleral search coil (Judge et al., 1980
Recovery from the cerebellar lesion was very rapid. Within hours from completion of surgery, the monkeys behaved normally, and there were no overt neurological signs. For 1 week after surgeries, the monkeys were transferred to the chair to care for the wounds and for oral administration of analgesics and antibiotics. Beginning on the second day after the lesion surgery, while the monkeys were taken out of the cage for their medical care, the chairs were positioned in the experimental setup and the monkeys were given opportunity to perform saccade trials. Although the monkeys were not deprived of water or food, they were invariably willing to perform the task. These rather brief sessions allowed us to map saccadic dysmetrias before any recovery took place. Adaptation was not studied in the early postlesion period.
At the completion of the experiment (1 year and 3 months after the lesion surgery, respectively) the monkeys were deeply anesthetized by a lethal dose of Nembutal and perfused with saline, followed by fixative. The cerebellum was sectioned parasagittally, and the brainstem was sectioned horizontally in 60 µm sections and Nissl stained. Experimental procedures follow the United States National Institutes of Health Guidelines and Israeli law and were approved by the Animal Care and Use Committee of the Weizmann Institute.
RESULTS
The lesion-induced deficits in saccadic accuracy and adaptation that we observed were substantial primarily in one or both horizontal directions, whereas the vertical and other horizontal directions were less affected. In the first part of Results, we focus on the deficits in the directions strongly affected by the lesions.
Saccadic adaptation in the intact monkey
Saccadic adaptation, as observed before the cerebellar lesions, is illustrated in Figure 1. We used the procedure introduced by McLaughlin (1967)
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Figure 1. Examples of trials illustrating saccadic adaptation and extinction. Each panel shows the horizontal eye position and target position during trials from a block designed to study saccadic adaptation. Rightward saccades. A full record of saccade sizes in this block is shown in Figure 2B.
Adaptation trials began in the same way as the control trials, but shortly after the saccade onset and while the saccadic movement was under way, the target was displaced from 15° to 20° eccentricity. Figure 1B shows the first adaptation trial. The saccade ends very close to the 15° location, where the target had been before the saccade, so that the eye position is 5° short of the target. McLaughlin (1967)
The pattern of visual stimulation in the adaptation trial illustrated in Figure 1C is identical to that of the trial of Figure 1B; the only difference is that, whereas Figure 1B shows the first adaptation trial in the displayed block, Figure 1C shows the 1000th consecutive adaptation trial. The monkey's responses are now very different. The eye overshoots the presaccadic position of the target, reflecting the monkey's recent experience with the previous 1000 adaptation trials. Thus, Figure 1C replicates McLaughlin's observation of a change in saccadic gain induced by the repeated intersaccadic target jump. Figure 2B shows the full record of the saccade sizes from the block illustrated in Figure 1. Saccade size increases very gradually during the adaptation trials.
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Figure 2. Saccadic adaptation is abolished by the cerebellar lesion. Panels show full records of saccade sizes for block of trials recorded at the days indicated above the panels. All movements are to the right. The two vertical lines in each panel indicate the beginning and end of adaptation trials. The scale of A and B is stretched twice relative to C and D.
Figure 1D shows a control saccade trial in which the target remains at its presaccadic position after the series of 1000 adaptation trials. Although the initial target position is the same as in the control trial of Figure 1A, the saccade now overshoots the target. The third group of trials was designed to study the extinction of adaptation. Figure 1D shows the first of these. Repetition of control trials leads to extinction of the adaptation; the monkey's saccades are recalibrated to their normal size (Fig. 1E). Figure 2B shows that extinction also occurs gradually, but more rapidly than acquisition of adaptation.
Abolition of adaptation
The vermian lesion permanently abolished rapid adaptation of the amplitudes of rightward saccades (Fig. 2). Figure 2, C and D, illustrates postlesion studies of saccadic adaptation. Although the procedures were identical to these of the prelesion studies illustrated in Figure 2, A and B, the results differ greatly. Adaptation is abolished. Despite 1000 adaptation trials, there is no increase in saccade size, nor is there any sign of extinction effects caused by the switch back from adaptation to control trials. These changes persist to the late postlesion phase, ~3 months and 1 year after the lesion. Thus, the abolition of adaptation is permanent.
Two additional effects of vermian lesions can be discerned in Figure 2. First, saccade end points are more variable after the lesion (note the difference in scale between Fig. 2A,B and C,D). Second, during these long series of adaptation trials, saccade size is continuously reduced. We will return to these effects below.
Saccadic hypometria
Figure 3 illustrates eye position records of ten 15° saccades in the most severely dysmetric direction for each monkey. Prelesion movements are swift and precise (Fig. 3A,D). Immediately after the lesion (day + 3), fixation is less precise and saccades are grossly dysmetric (Fig. 3B,E). After three months (monkey 2) and 1 year (monkey 1) recovery of average saccade amplitude is nearly complete, although now more variable than preoperatively (Fig. 3C,F). The gain in these early postlesion trials is, respectively, 79 and 65%. Early postlesion saccades are highly significantly different from both prelesion and late postlesion saccades (p < 10
6 in both monkeys). In contrast, the mean size of late postlesion saccades is not significantly different from prelesion (p = 0.55 and 0.24, respectively; all values by t test).
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Figure 3. Lesions of the oculomotor vermis induce gross dysmetria, but with time the dysmetria recovers. Saccades from prelesion period (A, D), early postlesion (day + 3) (B, E), and late postlesion (3 months, 1 year) (C, F). Monkey 1 (A-C), leftward saccades; monkey 2 (D-F), rightwards saccades. Ten saccades per panel. In trials early after the lesion, two and sometimes three saccades are needed to fixate the target (B, E). Whereas the mean saccade size recovers (C, F), the variability in both fixation and saccade size persists (B, C, E, F).
Figure 4 documents both the hypometria and recovery more thoroughly. The figure shows histograms of saccade size for all the control saccades in the affected directions recorded in this study (464 and 1443 saccades, respectively, in the two monkeys). The data of the late postlesion recovery was collected over 39 experimental days (22 d in monkey 1 and 17 d for monkey 2). There were no systematic differences among days. Early postlesion saccades are highly significantly different from both prelesion and late postlesion saccades (p < 10
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Figure 4. Histograms of saccade size documentating postlesion hypometria and recovery. A-C, Monkey 1; D-F, monkey 2. A and D represent prelesion period; B and E show early postlesion period; C and F show late postlesion period. Saccades in same directions as Figure 1. All appropriate control saccades recorded in this study are included. Thick vertical lines represent means of distributions. Values on each panel show mean ± SD of gain (in percents).
Despite their entirely recovered mean amplitude, late postlesion saccades remain abnormal. They are also slower, the maximal saccadic velocity being reduced from 622 ± 29 °/sec in the prelesion period to 553 ± 41 °/sec in the late postlesion period in monkey 1 and from 641 ± 47 °/sec to 620 ± 52 °/sec in monkey 2. Both differences are significant with p < 10
Postlesion continuous reduction of saccade size: fatigue?
A second, unexpected effect of the lesions was a continuous reduction in saccade amplitude over long blocks of identical saccades (Fig. 2). This slow reduction is continuous throughout the block, regardless of whether trials are of the adaptation or extinction stages. The continuous reduction was somewhat more pronounced in monkey 2 than in monkey 1, although it was clearly present in both. The continuous reduction in amplitude might result from the monkey's increasing fatigue that is presumably caused by repeating the same movement over and over. The cerebellar area ablated in our monkeys may thus normally serve to counteract fatigue-related saccadic inaccuracy.
We tested whether the continuous reduction might be caused by the unnatural pattern of visual stimulation that occurs in the adaptation paradigm. To evaluate whether the continuous reduction is indeed specific to blocks of adaptation trials, we tested monkey 2 in a control experiment in which the adaptation trials were replaced by trials with a single 20° saccade. Before and after the 20° saccades, there were groups of 15° saccade trials, just as in the adaptation studies. Saccade size is continuously reduced in these control conditions as well (Fig. 5A). The continuous reduction is particularly apparent when the 15° saccades at the beginning and the end of the block are compared directly. Figure 5B is a histogram of the first 100 15° saccades in the block, and Figure 5C is a histogram of the last 100 trials. Mean saccade size drops from 15.2 to 14.1°. The difference is highly significant (p < 10
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Figure 5. In the absence of saccadic adaptation, prolonged effort induces saccadic errors. A, Record of saccade size in the format of Figure 4; however, instead of adaptation trials, the monkey makes 200 control saccades. Saccades become smaller during the block. B, Histogram of first 100 trials; C, histogram of last 100 trials (1501-1600). D-F, Same format for monkey 3 who has an intact cerebellum. There is no analogous decrease in saccade size.
Accuracy of saccades in other directions
Saccade accuracy was most strongly affected in one of the four cardinal directions for each of the two monkeys; leftward for monkey 1 and rightward for monkey 2. In both animals, the direction opposite the one that was most severely affected was more mildly hypometric. The vertical dysmetrias for both animals are much smaller. Vertical hypermetria might reflect the presence of residual cortex deep in the sulci (see next section, Histological reconstruction). Table 1 presents the relevant measurements of saccade amplitude in each of the four directions. Recovery was virtually complete for the most severely affected directions. The more mild dysmetrias showed less long-term recovery. Because saccades in the present study were to targets at 15° eccentricity, a dysmetria of <10% represents an error, which would still leave the target within the fovea. The 20 and 32% dysmetrias represent 3 and 5° errors, which may be more powerful stimuli for initiating a long-term recalibration of saccade amplitude.
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Table 1. Impact of lesions on saccades in different directions Histological reconstruction
Figures 6 and 7 illustrate parasagittal sections through the center of the lesions (for review, see Madigan and Carpenter, 1971
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Figure 6. Histological sections through the lesion of monkey 1. Sections are 60-µm-thick, Nissl stained. The calibration mark shown in section 1 is valid for all sections. Section numbers in the block are specified. Every 12th section is shown; that is, the distance between displayed sections is 0.72 mm.
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Figure 7. Histological sections through the lesion of monkey 2. Sections are 60-µm-thick, Nissl stained. The scale bar shown in section 2 is valid for all sections. Section numbers in the block are specified. Every 12th section is shown; that is, the distance between displayed sections is 0.72 mm.
Saccadic direction is thought to be systematically mapped onto the surface of the saccadic area of the vermis (Ron and Robinson 1973
DISCUSSION
Summary of results
We evaluated the effects of lesions that were restricted to the oculomotor posterior vermis as delineated by Noda (Fujikado and Noda, 1987
Speculation: two anatomically segregated processes of saccadic adaptation
Several aspects of our findings may look paradoxical. For instance, the increased variability of saccade size might seem to be a secondary effect of the dysmetria, but it persists even after the recovery. The following interpretation, although speculative, is consistent with all aspects of our data and also with previous studies in which the fastigial nucleus was ablated in addition to the vermis (Optican and Robinson, 1980
We propose that two processes adjust for the dysmetria. The two processes differ by the rate with which they adjust the saccadic gain (their "time constant"). A rapid process critically depends on functional posterior vermis cortex. A slow process is revealed in the absence of this region of cerebellar cortex; it might depend on the fastigial nuclei. In the intact cerebellum, the distinction between the two processes is obscured because both act in synergy to maintain saccadic accuracy with the rapid, cerebellar cortical process dominating the slower, noncortical.
Below, we shall examine how this proposition might relate to our data.
Hypometria is consistent with previous data
Our finding of hypometria, not hypermetria, is primarily consistent with previous studies. Buettner and Fuhry (1995)
Increase of variability
Takagi et al. (1998)
The increase in variability can be explained as failure of rapid but not slow adaptation. Slow adaptation acts as a high-pass filter. It corrects for slow gain errors and keeps the mean gain accurate (for sufficiently large samples). However, it fails to cope with high-frequency gain errors. These rapid errors of the gain present themselves as increased variability of saccade size.
Increase in saccade size variability was also observed after transient inactivation of the fastigial nuclei (Robinson et al., 1993
Is the recovery mediated by adaptation?
In the introductory remarks, we distinguished between traditional slow adaptation, induced by extraocular muscle paresis (Kommerell et al., 1976
Is the recovery from dysmetria mediated by any form of sensorimotor adaptation at all? The key feature of visuomotor adaptation is that it is invoked by vision; it is a process in which the precision of saccades is modified according to their visual outcome. If the gain modification was not based on vision, the precision of the recovery we observed would be remarkable. It is obvious that the large initial saccadic hypometria results in a significant loss of vision. During recovery, the monkey's vision is not restricted in any way. Therefore, the most likely possibility is that some form of sensorimotor adaptation mediates recovery.
Relationship to neurological studies
The accepted neurological sign of posterior vermis lesions is saccadic dysmetria (Leigh and Zee, 1990
Does the continuous reduction of saccade amplitude represent fatigue?
The role of rapid saccadic adaptation has been a matter of speculation since the procedure for inducing it was invented (McLaughlin, 1967
We suggest that the oculomotor vermis is continuously active in adjusting and calibrating the oculomotor system, a process that is reflected in rapid saccadic adaptation. This mechanism is specifically involved in preventing the continuous reduction caused by fatigue. Thus, rapid saccadic adaptation would be a continuously active process, highly valuable for our ability to continue to use visual perception at the end of the day.
Relationship to previous studies
Although the posterior vermis and the fastigial nucleus are known to be involved in saccadic adaptation, the conclusion is based on a small number of monkeys. Moreover, in all but one study (Takagi et al., 1998
These differences probably stem from various sources. The variability in saccade size may make the extent of adaptation harder to assess when studying smaller saccades and decreasing magnification as in Takagi et al. (1998)
Although there are important points of agreement, the data from the two studies cannot simply be pooled. The lesions in our two monkeys were bilateral but not perfectly symmetrical in our monkey 1. The exact damage to each side of this functional region is not established, because the functional midline may not be coextensive with the anatomical midline. Despite these reservations, the data from the two studies makes it clear that the posterior vermis regulates the amplitude of saccadic eye movements and is probably essential for the short-term adaptation.
FOOTNOTES Received May 4, 1999; revised Aug. 25, 1999; accepted Aug. 25, 1999.
This work was supported by a grant from the Germany-Israel Foundation for Scientific Research and Development.
Correspondence should be addressed to Dr. Shabtai Barash, Department of Neurobiology, Weizmann Institute of Science, Rehovot 76100, Israel. E-mail: shabtai.barash{at}weizmann.ac.il.
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