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Previous Article | Next Article
The Journal of Neuroscience, January 15, 2003, 23(2):510-517
Correlation between Brain Reorganization, Ischemic Damage, and Neurologic Status after Transient Focal Cerebral Ischemia in Rats: A Functional Magnetic Resonance Imaging Study
Rick M. Dijkhuizen1, 2, Aneesh B. Singhal2, Joseph B. Mandeville1, Ona Wu1, Elkan F. Halpern3, Seth P. Finklestein4, Bruce R. Rosen1, and Eng H. Lo2 1 Athinoula A. Martinos Center for Biomedical Imaging, Department of Radiology, and 2 Neuroprotection Research Laboratory, Departments of Radiology and Neurology, Massachusetts General Hospital, Harvard Medical School, Charlestown, Massachusetts 02129, 3 Data Analysis Group, Department of Radiology, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts 02114, and 4 ViaCell Neuroscience Inc., Worcester, Massachusetts 01605
ABSTRACT
TOP
ABSTRACT
Introduction
The pattern and role of brain plasticity in stroke recovery has been incompletely characterized. Both ipsilesional and contralesional changes have been described, but it remains unclear how these relate to functional recovery. Our goal was to correlate brain activation patterns with tissue damage, hemodynamics, and neurologic status after temporary stroke, using functional magnetic resonance imaging (fMRI). Transverse relaxation time (T2)-weighted, diffusion-weighted, and perfusion MRI were performed at days 1 (n = 7), 3 (n = 7), and 14 (n = 7) after 2 hr unilateral middle cerebral artery occlusion in rats. Functional activation and cerebrovascular reactivity maps were generated from contrast-enhanced fMRI during forelimb stimulation and hypercapnia, respectively. Before MRI, rats were examined neurologically. We detected loss of activation responses in the ipsilesional sensorimotor cortex, which was related to T2 lesion size (r =
0.858 on day 3, r =
Key words: brain ischemia; neuronal plasticity; recovery of function; hemodynamics; magnetic resonance imaging; rats
Introduction
Stroke is the leading cause of disability in modern society, yet most stroke patients show some, albeit variable, functional recovery over time. This restoration of function is commonly thought to be associated with brain plasticity (Lee and van Donkelaar, 1995
; Seil, 1997
Animal stroke models allow reproducible and correlative studies on stroke recovery. With the use of contrast-enhanced functional magnetic resonance imaging (fMRI) in a rat stroke model, we recently described (1) loss of activation in the ipsilesional sensorimotor cortex and (2) a shift of predominantly widespread contralesional responses at 3 d after stroke to increased perilesional and more restricted contralesional activity at 14 d after stroke (Dijkhuizen et al., 2001
A major question that remains unanswered is the functional significance of the pattern of brain reorganization and its relationship to the extent of ischemic damage. In our previous study, which involved a model of permanent focal cerebral ischemia, we were unable to detect statistically significant correlations between the profile of brain activation and the degree of ischemic damage and neurologic dysfunction (Dijkhuizen et al., 2001
Materials and Methods
Experimental protocols were institutionally approved in accordance with the NIH Guide for the Care and Use of Laboratory Animals.
Stroke induction. Rats were anesthetized with 1-1.5% halothane in N2O/O2 (70:30) under spontaneous respiration. Body temperature was monitored continuously and maintained at 37°C with a thermostatically controlled heating pad. Transient focal cerebral ischemia was induced by 2 hr occlusion of the right middle cerebral artery with an intraluminal filament in adult male Sprague Dawley rats (250-350 gm) (Longa et al., 1989
Neurologic examination. At 24 hr, 3 d, and 14 d after onset of stroke, the animal's neurologic status was evaluated using the grading system as described by others (Bederson et al., 1986
MRI. In three separate groups of animals, MRI experiments were performed at 1 d (n = 7) (group "day 1"), 3 d (n = 7) (group "day 3"), and 14 d after stroke (n = 7) (group "day 14").
Rats were tracheotomized and ventilated mechanically with 1% halothane in O2/air (1:1). The right femoral artery was catheterized for monitoring of arterial blood pressure and blood gases. The right femoral vein and jugular vein were cannulated for administration of anesthetic agent and magnetic resonance contrast agent, respectively. Thin copper wires were inserted just underneath the skin on opposite sides of each forelimb at the level of the wrist. Next, rats were paralyzed by an intravenous bolus of pancuronium (2 mg/kg) followed by continuous infusion (2 mg · kg
1 · h
-chloralose (40 mg · kg
MRI was done on a 2.0 T magnet system (Varian Instruments, Palo Alto, CA) using a 3 cm surface radiofrequency coil that was developed in-house. Body temperature, blood pressure, and blood gases were controlled carefully and maintained at normal values during the MRI experiments.
Multislice spin echo T2- [repetition time (TR) = 2000 msec; echo time (TE) = 40, 80 msec] and diffusion-weighted images (TR/TE = 2000/40 msec; b = 150, 850, 1550 sec/mm2; diffusion-encoding gradients in three directions) were acquired [field-of-view (FOV) = 25 × 25 mm2; 64 × 64 data matrix; nine 1.5 mm slices], from which we calculated two-dimensional maps of the T2 and the mean trace of the apparent diffusion coefficient (ADC) of tissue water, respectively (van Gelderen et al., 1994
Multislice contrast-enhanced MRI (single-shot gradient recalled EPI; TR/TE = 2000/22 msec; 510 time points; FOV = 25 × 25 mm2; 32 × 32 data matrix, zero-filled to 64 × 64; nine 1.5 mm slices) was performed after the injections of MION. Cerebral blood volume (CBV)-weighted images were calculated as described previously (Hamberg et al., 1996
Cerebrovascular reserve capacity was assessed by acquiring CBV-weighted images as described above, during 10 min inhalation of 5% CO2 in balanced O2 (after 10 min of breathing with 100% O2). We characterized the plateau CO2-induced CBV change (
CBVmax[CO2]) as the mean CBV change between 2 and 10 min after onset of 5% CO2 inhalation.
Data analysis. Lesion volumes were calculated from the multislice T2 datasets with use of the image analysis software package Alice (Hayden Image Processing Group, Boulder, CO). T2 lesion volume was defined as the ipsilateral parenchymal brain volume with T2 values higher than the mean + 2 SD of the T2 in contralateral tissue.
The total area of significant forelimb stimulation-induced CBV responses was calculated in each hemisphere with Alice. The laterality index, which expresses relative activity in the contralateral hemisphere as compared with the ipsilateral hemisphere, was defined as (C
ROI analyses were performed on MRI parameters (i.e., T2, ADC, CBFi, CBV,
All values are expressed as mean ± SD. Statistical comparisons were performed using one-way ANOVA (with repeated measures where appropriate) with post hoc Tukey test for multiple comparisons and paired Student's t test. For correlation analyses we applied the Pearson product moment correlation test (and linear regression) or the Spearman rank order correlation test (and ordinal logistic regression). To separate the possible confounding effects of the time after stroke from any independent relationship of laterality index and neurologic status, we used multiple linear and ordinal logistic modeling. p values of <0.05 were considered significant.
Results
Neurologic status
Animals demonstrated neurologic deficits at all time points after stroke; however, functional scores significantly improved over 14 d (Table 1).
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Table 1. Neurologic scores and T2 lesion volumes at 1, 3, and 14 d after 2 hr middle cerebral artery occlusion Ischemic damage
MRI revealed unilateral lesions in the middle cerebral artery territory, generally involving the lateral cortex and striatum (Fig. 1). Lesions were characterized by a reduced ADC and increased T2 (Fig. 1, top panel). Because our study involved a model of transient occlusion of the middle cerebral artery, ischemia was followed by reperfusion. In fact, we detected moderate hyperperfusion at 24 hr after stroke (Fig. 1, top panel). After 3 d, ADC values had pseudonormalized in large parts of the lesion (Fig. 1, middle panel). T2 and perfusion parameters continued to be high as compared with contralateral. At day 14, there was mild hyperperfusion in the lesion, and ADC and T2 values were elevated (Fig. 1, bottom panel). T2 lesion volumes are given in Table 1. Depending on the extent of the lesion, ADC, T2, and perfusion were mildly to severely affected in the forelimb region of the sensorimotor cortex (i.e., M1/S1fl) in the ipsilesional hemisphere.
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Figure 1. Multislice ADC and T2 maps (3 adjacent slices are shown) and single-slice CBFi maps (same slice position as the left image of the ADC and T2 maps) at 1 d (top panel), 3 d (middle panel), and 14 d (bottom panel) after 2 hr middle cerebral artery occlusion. Each panel represents data from a single animal. Below the CBFi maps is an outline of a coronal rat brain section centered 0.7 mm from bregma [reproduced from Paxinos and Watson (1997)
Cerebrovascular reactivity
To test cerebrovascular reactivity, we applied a CO2 challenge and measured CBV changes in the brain. Results are shown in Figure 2. Inhalation of 5% CO2 raised the arterial PCO2 from 37.0 ± 2.3 to 53.6 ± 5.1 mmHg, resulting in a clear CBV increase in the contralesional hemisphere. At 1 d after transient focal ischemia, the CO2-induced CBV response was lowered significantly throughout most of the ipsilesional hemisphere. After 3 d, we found an enhanced CBV response in the ipsilesional parietal cortex. In M1/S1fl, at the border of the lesion, CBV changes were not significantly different as compared with contralesional. After 14 d, CO2-induced CBV changes were subnormal in the ipsilesional hemisphere, but this was not significant for M1/S1fl. Correlation analyses did not show any significant relationship between CO2-induced
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Figure 2. Plateau CBV change (
Cerebral activation responses
Figure 3 shows T2-weighted images overlaid by statistical activation maps and graphs of the time course of CBV changes in M1/S1fl for the different animal groups. Images, maps, and graphs represent data averaged across animals. Stimulation of the unimpaired forelimb invariably resulted in a significant activation-induced CBV response in M1/S1fl in the unaffected, contralesional hemisphere (i.e., contralateral to the stimulated limb) (Fig. 3). The stereotaxic coordinates of the center of the focus of activation on stimulation of the unimpaired limb were 0.1 ± 1.1 mm anterior, 3.7 ± 0.2 mm lateral, and 1.7 ± 0.3 mm ventral to bregma (averaged over all 21 animals), which corresponds to S1fl according to Paxinos and Watson (1997)
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Figure 3. Averaged T2-weighted images of coronal rat brain slices overlaid by statistical activation maps, calculated from the averaged activation-induced cerebral CBV changes (n = 7) (data are averaged across animals). The map of p values has been color-coded corresponding to the degree of significance (see bars below images). The graphs show the mean of the averaged time course of CBV changes (averaged across six on-off periods for each forelimb) in an ROI (5 voxels) in ipsilesional (right) and contralesional (left) M1/S1fl (mean ± SD; n = 7). Top row, 24 hr after stroke; middle row, 3 d after stroke; bottom row, 14 d after stroke. Right, Unimpaired forelimb stimulation (represented by the green bars in the graphs) induced significant activation responses in the contralateral (right) M1/S1fl at all time points. Stimulation of the left, impaired forelimb (represented by the blue bars in the graphs) resulted in diminished responsiveness in the right, ipsilesional M1/S1fl at 24 hr and 3 d after stroke. However, clear responses were found in the contralesional hemisphere. After 14 d, activation responses were predominantly in ipsilesional M1/S1fl. Infarction areas are characterized by increased T2-weighted signal intensity.
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Figure 4. Laterality indices during stimulation of the left, impaired (gray bars) and right, unimpaired forelimb (white bars) at 1, 3, and 14 d after 2 hr middle cerebral artery occlusion (mean ± SD; n = 7). The negative laterality indices during impaired forelimb stimulation at days 1 and 3 represent the enhanced relative activity in the contralesional hemisphere (i.e., ipsilateral to the stimulated forelimb) as compared with the ipsilesional hemisphere. At 14 d after stroke, the laterality index was near baseline, indicating that bulk activation was in the ipsilesional hemisphere (i.e., contralateral to the stimulated forelimb). *p < 0.05; #p = 0.052.
Correlation analyses
Correlation analyses demonstrated that changes in activation patterns were related to extent of ischemic damage. We found significant relationships between lesion size and impaired forelimb stimulation-induced
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Figure 5. Relationship between lesion volume and plateau CBV change ( ), and 14 d (
) after 2 hr middle cerebral artery occlusion (n = 7 for each time point). *p < 0.05.
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Table 2. Correlation between activation parameters (impaired forelimb stimulation-induced
Discussion
Both ipsilesional and contralesional brain reorganization are known to occur after stroke. The main finding of this study is that the degree of shift of activation balance toward the contralesional hemisphere early after stroke increases with the extent of tissue injury and that functional recovery is associated mainly with preservation or restoration of activation in the ipsilesional hemisphere.
We assessed spatiotemporal characteristics of changes in brain activation patterns in relation to tissue, perfusion, and neurologic status after transient focal cerebral ischemia in rats. With the use of contrast-enhanced CBV-weighted fMRI, we detected distinct activation-induced responses in the contralesional hemisphere after stimulation of the impaired forelimb early after transient ischemia, which is in agreement with two previous studies in models of permanent cerebral ischemia (Abo et al., 2001
Correlation between loss of activation responses and ischemic damage
An important goal of this study was to correlate the pattern of brain reorganization with ischemic damage. Brain tissue status was assessed with T2- and diffusion-weighted MRI. Brain ADC values that are reduced acutely after stroke reflect cytotoxic edematous tissue (Moseley et al., 1990
In addition to the brain tissue status, we calculated relative CBFi and CBV with the use of dynamic and steady-state susceptibility contrast-enhanced MRI, respectively. Because we did not detect reduced perfusion levels at the examined time points (in fact, 2 hr middle cerebral artery occlusion in the rat was followed by chronic hyperperfusion), loss of detection of fMRI signals cannot be explained by insufficient distribution of the contrast agent. Still, altered CBF and CBV dynamics after temporary stroke may have affected the fMRI signal. Nevertheless, we did not detect a significant relationship between activation-induced
Correlation between brain reorganization and ischemic damage
Along with loss of activation responses in ipsilesional M1/S1fl, stroke led to augmented responsiveness in the contralesional hemisphere, characterized by a reduction of the laterality index. Enhanced contralesional activation has been described in earlier studies in stroke patients and animal models and appears to be strongest early after stroke (Cuadrado et al., 1999
We found significant correlations between the laterality index and the degree of brain injury. At day 1 the laterality index was correlated negatively with lesion size (there was a trend toward a significant relationship at day 14). Also, the laterality index was correlated with the degree of tissue damage in M1/S1fl, expressed by the local ADC and T2, at days 1 and 14 after stroke. The lack of correlation between the laterality index and the ADC and T2 at 3 d after stroke is most likely attributable to the pseudonormalization of ADC and partial recovery of T2 values at subacute stages, as a result of cellular lysis (Pierpaoli et al., 1993
The correlation between brain reorganization and ischemic tissue damage is in agreement with a recent fMRI study in patients with cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy, in which the motor cortex laterality index correlated with the relative N-acetylaspartate decrease in white matter, which was used as an index of axonal injury (Reddy et al., 2002
Correlation between brain reorganization and functional status
From the above it appears clear that changes in the pattern of activation are linked directly to the degree of ischemic injury. However, an important question is how cerebral reorganization is associated with functional recovery. Despite a significant negative relationship between laterality index and neurologic status when all data were grouped together, no significant correlations were found at the individual time points. The lack of a significant effect that was independent of the time after stroke prohibits any presumption of a causal relationship between a shift of sensorimotor activation patterns and restoration of forelimb function. Moreover, it should be mentioned that the behavioral test that we used provided an overall score of neurologic function and did not inform exclusively on sensorimotor function of the forelimb. A stronger relationship between brain reorganization and functional recovery may have been found when neural and functional measures were matched more specifically. Nonetheless, the trend of a negative association between laterality index and neurologic status is in line with earlier findings by others (Marshall et al., 2000
Concluding remarks
This study shows that the spatiotemporal pattern of shifts in cerebral activation after stroke is closely related to the degree of ischemic damage. Our results provide correlative evidence that good neurologic function is associated with a "normal" balance of activation in the cerebral hemispheres. Functional recovery seems to depend predominantly on preservation, reinstatement, or intrahemispheric shift of activation within the ipsilesional hemisphere. Although functional fields in the contralesional hemisphere may be involved in upholding and restoring function, acute contralesional activity appears to be mainly a direct response to the ischemic injury, without a clear functional significance. Finally, our results suggest that the application of fMRI in stroke patients can provide important prognostic information on functional outcome. This may aid in the selection of therapeutic strategies that could improve functional recovery after stroke.
FOOTNOTES Received May 28, 2002; revised Oct. 10, 2002; accepted Oct. 22, 2002.
This study was supported by National Institutes of Health Grants P50-NS10828, RO1-HL39810, P01-CA48729, P41-RR14075, RO1-NS38477, RO1-NS37074, and RO1-NS38731. This work was done during the tenure of fellowships from the American Heart Association, New England Affiliate, Inc. (R.M.D., A.B.S.).
Correspondence should be addressed to Dr. Rick M. Dijkhuizen, Image Sciences Institute, University Medical Center Utrecht, Bolognalaan 50, 3584 CJ Utrecht, The Netherlands. E-mail: rick{at}invivonmr.uu.nl.
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