(Stroke. 2000;31:1958.)
© 2000 American Heart Association, Inc.
Original Contributions |
Cerebral Blood Flow and Blood Volume Measured by Magnetic Resonance Imaging Bolus Tracking After Acute Stroke in Pigs
Comparison With [15O]H2O Positron Emission Tomography
From the PET-Center (M.S., A.G.) and the Department of Neuroradiology (L.R., C.G., L.Ø.), Aarhus University Hospital, Aarhus, Denmark; and the Department of Neurological Surgery (M.S.), Ehime University School of Medicine, Ehime, Japan.
Correspondence and reprint requests to Dr Masaharu Sakoh, MD, PhD, Department of Neurological Surgery, Ehime University School of Medicine, Shizukawa, Shigenobu-cho, Onsen-gun, Ehime 791-0295, Japan. E-mail sakoh{at}m.ehime-u.ac.jp
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Abstract |
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Background and Purpose—Early and accurate assessments of cerebral ischemia allow therapy to be tailored to individual stroke patients. We examined the feasibility of using a novel method for measuring cerebral blood flow (CBF) of ischemic tissue based on MRI after middle cerebral artery occlusion (MCAO). Moreover, the regional correlations between CBF and cerebral blood volume (CBV) were investigated in the regions with acute ischemic stroke.
Methods—CBF and CBV were measured before and after MCAO or reperfusion by positron emission tomography (PET) in 13 pigs. Just after the PET scans, CBF and CBV were measured by MR bolus tracking and were compared with results obtained by PET at 6 hours after permanent MCAO or reperfusion. The infarction was verified histologically.
Results—The MR method yielded parametric CBF and CBV maps with tissue contrast in good agreement with parametric PET images, which demonstrated hypoperfused and hyperperfused areas after MCAO or reperfusion. Both MRI and PET technology showed that CBF values below 60% of the contralateral value induced a reduction of CBV, which committed the tissue to infarction.
Conclusions—The novel MR method provides accurate measurement of CBF and CBV in acute stroke and hence gives useful information for planning the appropriate therapeutic intervention.
Key Words: cerebral blood flow • magnetic resonance imaging • stroke, acute • tomography, emission computed • pigs
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Introduction |
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TopAbstractIntroductionMaterials and MethodsResultsDiscussionReferencesIntroduction |
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Rapid MRI of the passage of a bolus of magnetic susceptibility contrast agent has recently become an important tool for assessing regional cerebral blood flow (CBF)1 2 and cerebral blood volume (CBV).3 4 In fact, absolute CBF values have been determined by means of MRI with introduction of an empirical normalization constant in animals5 and humans.6 Thus, this technique has gained widespread acceptance in the evaluation of hemodynamic changes in cerebral pathologies, especially stroke,7 migraine,8 and central nervous system tumors.9 For theoretical reasons, however, it is unknown whether this approach provides reliable measurements in the presence of pathological hemodynamics.2
In this study, we measured CBF and CBV using both positron emission tomography (PET) and dynamic susceptibility contrast (DSC)-MRI in combination with a newly developed technique for middle cerebral artery occlusion (MCAO) and reperfusion in pigs. The objective of this study was to determine whether rapid DSC-MRI could accurately measure relative CBF and CBV even in the presence of pathological hemodynamics. Moreover, we examined the regional correlations between CBF and CBV in the regions with acute ischemic stroke.
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Materials and Methods |
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TopAbstractIntroductionMaterials and MethodsResultsDiscussionReferencesIntroduction |
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Theory
MRI CBF Measurement
The following equation, introduced in detail by Østergaard and coworkers,2 was used to determine relative CBF by DSC-MRI of nondiffusible tracer bolus passage. In brief, the concentration CVOI(t) of an intravascular contrast agent within a given volume of interest (VOI) can be expressed as a function of time (t):
 | (1) |
PET CBF Measurement
The regional uptake of a diffusible tracer is described
by the equation introduced by Ohta et al12 :
 | (2) |
Animal Preparation and Experimental Protocol
The research project was approved by the Danish National
Committee for Animal Research Ethics (DanCARE). Thirteen female
country-bred Yorkshire pigs weighing 38 to 45 kg each were divided into
the following 2 groups: (1) permanent MCAO (n=8) and (2)
reperfusion after 2-hour MCAO (n=5). They had free access to water but
were deprived of food for 24 hours before the experiment. Pigs were
initially sedated by intramuscular injection of 20 mL of midazolam (5
mg/mL). After intravenous injection of a mixture of
fentanyl 1 mg, midazolam 50 mg, and pancuronium 4 mg, the pig was
intubated and artificially ventilated (Engstrøm Ventilator) with a
70% N2O–30% O2 mixture.
Anesthesia was maintained by continuous infusion of
fentanyl 0.1 mg ·
kg-1 ·
h-1, midazolam 1.25
mg · kg-1 ·
h-1, and pancuronium
bromide 0.2 mg ·
kg-1 ·
h-1 for the first 3 hours
during which surgery was performed. Thereafter, fentanyl 0.05 mg
· kg-1 ·
h-1, midazolam 1.25
mg · kg-1 ·
h-1, and pancuronium
bromide 0.2 mg ·
kg-1 ·
h-1 were used. Indwelling
femoral venous and arterial catheters were installed
surgically for injection of tracers and arterial blood
sampling. Isotonic saline (
100 mL/h) was administered
intravenously throughout the experiments. Rectal
temperature was kept at 38°C by means of a thermostatically
controlled heating blanket.
Focal cerebral ischemia was transorbitally induced by occlusion of the left proximal middle cerebral arteries (MCAs), generally consisting of 2 arteries, and the distal internal carotid artery (ICA). Bipolar coagulation or Sugita microclip (Mizuho; blade length 2 to 4 mm, blade width 0.8 mm, holding force 65 to 70 g) was used to induce permanent MCAO or transient MCAO, respectively. Reperfusion was accomplished by microsurgical removal of the microclips 2 hours after MCAO. The dura was closed with Neuro-Patch (Braun) and fibrin glue (Immuno) to avoid leakage of cerebrospinal fluid. The cavity of the orbit was filled with isotonic saline and gauze to avoid susceptibility artifacts in DSC-MRI.
PET studies were performed before and 1 and 6 hours after permanent MCAO. In the reperfusion experiments, PET studies were done before and 1 hour after MCAO, as well as 1 and 6 hours after reperfusion. CBF and CBV were measured in 13 and 9 (ie, 4 for permanent MCAO and 5 for reperfusion) pigs at each time, respectively. Just after the PET scans, relative CBF, CBV, and mean transit time (MTT) with DSC-MRI were measured in the pigs placed in the MRI scanner, ie, 7 hours after permanent MCAO or reperfusion; the elapsed time between PET and MRI was 1 hour. Then, digital subtraction angiography (DSA) was performed via a femoral catheter that was placed in an ascending pharyngeal artery (corresponding to the distal part of the ICA in humans) near the origin of the rete mirabile to verify the occlusion of the MCA after permanent MCAO and the patency of the MCA after reperfusion. At the end of the experiment, usually 10 to 12 hours after MCAO, histological examination was performed to verify the infarction.
Throughout the experiments, body temperature, blood pressure, heart rate, and expired-air carbon dioxide (CO2) levels were monitored continuously, and arterial blood samples were withdrawn and analyzed (ABL 300, Radiometer) every hour to monitor blood gases and whole-blood acid-base parameters. Disturbances in body fluid balance were corrected by appropriate procedures (eg, forced ventilation and/or changes in infusion rates) to maintain physiological parameters within the normal range.
Positron Emission Tomography
The pigs were positioned supine in the scanner (Siemens/CTI ECAT
EXACT HR) with the head in a custom-made headholder. CBF was estimated
by intravenous bolus injection of 800 MBq
[15O]H2O. Sequences of 21
(12, 6, and 3 samples during the first, second, and third minute,
respectively) arterial blood samples and 12 (6, 4, and 2
images per minute, respectively) PET brain images were then obtained.
CBV was measured by a single-breath inhalation (1 L) of 1200 MBq
[15O]CO, followed by 10-second breath-holding.
For all experiments, total radioactivity in blood samples was measured.
Brain image and arterial data were corrected for the
half-life of 15O (123 seconds). PET image data
were reconstructed for 3D images with 2D data acquisition mode,
providing 47 contiguous 3.2-mm slices using a Hanning filter with a
cutoff frequency of 0.5
pixel-1, resulting in a
spatial resolution of 4.6 mm full width at half maximum
(FWHM).13 Correction for attenuation was made on the basis
of a transmission scan.
Raw PET images were applied to the 3x3 uniform smoothing kernel. Then,
the 15O water data were fitted to Equation 2
by
nonlinear, least squares regression analysis of each image
voxel. CBV was determined by the ratio of cerebral and
arterial whole blood [15O]CO levels
after initial distribution (30 seconds) of the tracer.
Magnetic Resonance Imaging
The pigs were positioned supine in the scanner with the head in
a custom-made whole-body holder. Imaging was performed with a GE Signa
Horizon 1.0-T Imager (GE Medical Systems). After a sagittal scout, an
axial T1-weighted 3D gradient-echo sequence (time of repetition [TR]
8 ms, time of echo [TE] 1.5 ms, 20° flip angle) was acquired for
later coregistration of MRI and PET data. Then, a T2-weighted
fast-spin-echo sequence was obtained with TR/TE of 4000/105 ms. For
dynamic imaging of bolus passages, gradient-echo echo-planar imaging
(EPI) (TR/TE=1500/45 ms) was performed, starting 15 seconds before
injection. A 64x64 acquisition matrix was used with a 14x14-cm axial
field of view, leading to an in-plane resolution of 2.2x2.2
mm2, with a slice thickness of 5 mm and an
interslice gap of 2 mm. Six slices were obtained. In all
experiments, bolus injection of gadodiamide (0.1 mmol/kg;
OMNISCAN, Nycomed Imaging) was performed at a rate of 10 mL/s.
We used susceptibility contrast arising from compartmentalization of
the paramagnetic contrast agent14 for determining tissue
and arterial tracer levels. We assumed a linear
relation11 between paramagnetic contrast agent
concentration and the change in transverse relaxation rate,
R2, for determining tissue and
arterial tracer time concentration curves C(t) according to
the equation
 | (3) |
R2 (3 to 10 times that of gray and white
matter) after contrast injection.15 The integrated
area of the arterial input curve was in each measurement
normalized to the injected contrast dose (in millimoles per kilogram of
body weight) for comparisons within and among
animals.5
To determine CBF from Equation 1, the deconvolution was performed over
the range of measurements, where the arterial input values
exceeded the noise level (usually 15 seconds). Deconvolution
followed smoothing of raw image data by a 3x3 uniform smoothing
kernel. The maximum of the deconvolved response curve was assumed to be
proportional to CBF. CBV was determined by numerically integrating the
concentration time curve from bolus arrival to tracer
recirculation.16 Then, true MTT was determined from the
CBF and CBV values calculated above, because MTT=CBV/CBF. MRI CBF maps
were filtered with a 5-mm FWHM gaussian filter to make the spatial
resolution of PET and MRI maps as similar as possible using a
commercially available software package (ALICE; Hayden Image Processing
Solutions).
Pathohistological Protocol
Each pig was transcardially perfused with 1 L of Sørensen’s
phosphate buffer (0.15 mol/L) containing 0.1% sodium sulfide, followed
by 5 L of buffer containing 4% paraformaldehyde during
exsanguination via the left atrium. After storage for 2 days in
buffered 30% sucrose, the brains were removed and cut into coronal
9-mm slabs with a custom-made slicer. These slabs, which closely
matched the orientation of the PET images, were frozen and cut in the
coronal plane into 100-µm-thick slices by a sliding microtome. From
each slab, 1 slice was Timm stained for detection of zinc sulfides and
another slice was Nissl stained for neuronal cell bodies with toluidine
blue on gelatin-coated slides. The slices were analyzed to
verify the infarction histologically and to bring into
registration the anatomically defined brain morphology with the PET and
MRI images in the same plane.
Region-of-Interest Protocol
The ischemic regions were defined with the isocontour
setting of ECAT 7 software (Electronic Catalog Corp) as regions with
CBF that were reduced at least 2 SDs relative to the contralateral CBF
values measured 1 hour after MCAO. Regions of interest (ROIs) were
selected from these isocontour maps; the ROIs were encircled by
freehand tracing within the zone of reduced CBF (Figure 1
). Three sequential slices (9.6 mm)
with the largest ischemic regions were obtained so that the
ischemic core, detected by the greatest reduction of CBF, was
included. One set of ROIs consisted of the entire ischemic
region, the ischemic cortex, and the ischemic core in
each pig. Another set of ROIs was obtained by superimposition of the
ROIs of the MCAO side onto the contralateral side of the brain, ie, the
MCA region, the cortex, and the white matter. The set of ROIs, once
defined for each pig, was used in all subsequent PET studies. The set
of ROIs selected by PET was coregistered in the DSC-MRI in each pig by
Register (Montreal Neurological Institute, McGill University).
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Data Analysis
Statistical analysis was performed by 1-way
repeated-measures ANOVA to determine whether
physiological parameters and/or
absolute values for CBF and CBV measured by PET differed significantly
with time. A P value of 0.05 was used for statistical
significance throughout this report. Pixel maps of CBF and CBV (at
similar anatomic locations) generated with PET and MRI were compared on
a regional basis for the ischemic regions. For the assessment
of correlation between DSC-MRI and PET parameter values,
Spearman’s test was used. Linear least squares regression
analysis was performed with the ratio of each variable for
the ischemic regions in relation to the contralateral value to
determine the slope and y intercept of the fit. The
statistical significance of the difference between slopes estimated by
linear regression was determined by Student’s t test.
Moreover, differences between coefficients of correlation after MCAO
and reperfusion were measured for CBF and CBV.
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Results |
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TopAbstractIntroductionMaterials and MethodsResultsDiscussionReferencesIntroduction |
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General Physiological Variables
All general physiological variables were in the normal range under baseline conditions (Table 1
). Most variables remained
stable and did not significantly differ before and 6 hours after
permanent MCAO or reperfusion, although plasma glucose concentration
was increased 6 hours after permanent MCAO. In addition,
physiological variables did not differ between
PET and MRI studies.
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Angiographic and Pathohistological Study
After permanent MCAO, the MCAs of 8 pigs angiographically
showed complete occlusion. The infarction was verified
histologically in 7 of 8 brains. Six of these 7 brains
had infarction that included both the ischemic core and the
ischemic cortex, but 1 brain had infarction only in the
ischemic core. One brain had no infarction because of the
collateral flow supplied from the anterior cerebral artery, despite
complete occlusion of the MCA.
Reperfusion 2 hours after MCAO was found angiographically to have provided for complete recanalization of the MCA in 5 pigs. Four of the 5 brains had an infarction. Three of these 4 brains showed that the infarction included both the ischemic core and the ischemic cortex, but 1 brain had infarction only in the ischemic core. One brain had no infarction.
PET Study
The absolute values of CBF and CBV were divided into 2 groups on
the basis of the tissue damage, ie, infarction or noninfarction in the
ischemic core and the ischemic cortex, as shown in
Table 2. MCAO induced a
significant reduction of CBF in the ischemic core and cortex as
soon as 1 hour after occlusion, whereas CBV was significantly decreased
in the infarcted ischemic core and cortex only at 6 hours after
MCAO. During the MCAO, the ischemic regions with CBV values
above the baseline were spared from infarction. Reperfusion 2 hours
after MCAO restored CBF and CBV to normal levels after an initial
excessive rise in CBF, whereas the saved tissue due to the reperfusion
did not show the excessive rise in CBF (Table 2).
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MRI Study
Relative CBF, CBV, and MTT maps obtained by DSC-MRI and
T2-weighted MRI after MCAO or reperfusion are shown in Figure 2. It is evident that CBF mapping by
DSC-MRI was closely correlated to CBF images obtained by PET, even in
terms of the different level and volume of ischemia or
hyperperfusion. MTT clearly showed a hemodynamic
compromise, particularly on mild ischemia, in which CBF and CBV
were not completely proportional as MTT=CBV/CBF. T2-weighted imaging
showed an obvious tissue injury 7 hours after reperfusion in all 4 pigs
with infarction (corresponding to 9 hours after MCAO) in relation to
the severity of ischemia, whereas the tissue injury was not yet
obvious on T2-weighted images even at 7 hours after permanent MCAO
despite the severity of ischemia shown in Figure 2.
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Regional Correlation Between MRI and PET of CBF and CBV
Measurement
The regional correlations of CBF and CBV measured by DSC-MRI and
PET are illustrated in Figures 3A and 3B.
The values obtained by DSC-MRI for CBF and CBV were significantly
correlated to those obtained by PET during both permanent MCAO and
reperfusion (CBF: r2=0.96,
P<0.01, df=38; CBV:
r2=0.85, P<0.01,
df=30). For CBV, however, DSC-MRI detected values lower than
PET, especially in severely ischemic territory.
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Regional Correlation Between CBF and CBV With PET and MRI
The regional correlations between CBF and CBV obtained by PET are
illustrated in Figure 4A. The regional
estimates of CBF and CBV were significantly correlated after MCAO
(pooled data for 1 and 6 hours:
r2=0.89, P<0.01,
df=38). In contrast, after reperfusion, CBF was less well
related to CBV (r2=0.33,
P<0.05, df=14). The correlations between CBF and
CBV differed significantly between permanent MCAO and reperfusion
(z=3.49, P<0.001), and pairwise comparison of
the slope showed a significant difference (t=2.21,
P<0.05, df=41). After MCAO, CBV remained above
the contralateral value until CBF fell to <70% of the contralateral
level. On the other hand, CBF values below 60% of the contralateral
value were accompanied by a linear decline in CBV. The reduction of CBV
was greater 6 hours after permanent MCAO
(r2=0.93, P<0.01,
df=11) than 1 hour after MCAO
(r2=0.89, P<0.01,
df=26), especially in severely ischemic territory,
although the difference failed to be statistically significant.
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The regional correlations between relative CBF and CBV obtained by
DSC-MRI are illustrated in Figure 4B. The estimates were
significantly correlated 7 hours after MCAO
(r2=0.91, P<0.01,
df=23), whereas after reperfusion, relative CBF was less
well related to CBV (r2=0.35,
P<0.05, df=14); the correlations between CBF and
CBV differed significantly between permanent MCAO and reperfusion
(z=3.26, P<0.001). DSC-MRI also showed that
relative CBV increased at relative CBF values above 70% of the
contralateral value 7 hours after MCAO, whereas relative CBV decreased
at CBF values below 60% of the contralateral value.
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Discussion |
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TopAbstractIntroductionMaterials and MethodsResultsDiscussionReferencesIntroduction |
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The extent of the time window for therapy of acute ischemic stroke depends on the magnitude of residual flow and varies from person to person.7 17 18 19 20 Thus, a diagnostic procedure that assesses the magnitude of residual flow allows therapy as a function of time to be tailored to individual patients with acute ischemic stroke. PET has enabled researchers to follow the dynamics of cerebral blood flow and metabolism leading to infarction after stroke, but the technology is of limited use in clinical practice and frequently not available in acute situations.19 21 22 23 24 On the other hand, recent results by Østergaard et al1 2 5 6 indicate that DSC-MRI can be used to measure relative and absolute CBF rates in the intact brain of humans or animals. In clinical practice, CBF measurements with MRI, feasible in combination with pathophysiological tomography such as diffusion-weighted imaging, would be of great benefit to patients with acute ischemic stroke.7 Therefore, it is important to know whether abnormal hemodynamics disrupt the reliability of MRI measurements.
Comparison Between DSC-MRI and PET
In the present study, the relative CBF and CBV values obtained
with DSC-MRI were in good agreement with the results of PET in the
regions that were ischemic after MCAO. Moreover, with the same
degree of accuracy as PET, DSC-MRI documented that the
hemodynamic abnormalities of acute stroke included
changes in both CBF and CBV. Hence, the present results show that
cerebral ischemia can be reliably detected and characterized
with DSC-MRI, as proposed by previous reports.7 25 This
MRI technique for acute ischemic stroke could be improved with
more mathematical work, because the technique has far higher resolution
and less noise than the PET technique.5
Variability of Cerebral Ischemia: Relation Between CBF
and CBV
Classically, the phase of autoregulation in response to decreasing
perfusion pressure is characterized by rising CBV at constant CBF, but
when maximum vasodilation occurs, CBF falls while CBV remains constant.
Gibbs et al21 showed that the ratio CBF/CBV (ie, the
reciprocal of the expression for MTT) was an index of diminishing
cerebral perfusion pressure and hence residual perfusion reserve.
In the present study, DSC-MRI clearly demonstrated the
variability of cerebral ischemia after MCAO, as shown in Figure 1. Especially in the regions with mild ischemia (CBF
>30 mL · 100
g-1 ·
min-1 in the
ischemic cortex shown by PET), which might proceed to
infarction without reperfusion, the MTT maps displayed the compensatory
vasodilation in response to the reduced perfusion pressure and hence
were highly indicative of a flow-volume mismatch. In the regions with
more severe ischemia (CBF <30 mL · 100
g-1 ·
min-1), the MTT maps
showed an area at risk that leads to infarction; CBV declined in linear
proportion to the reduction of CBF. The CBF thresholds for the
reduction of CBV increased with time in acute ischemic regions,
in agreement with the findings of Kohno et al26 that the
CBF thresholds for diffusion abnormality increased with time. Thus, the
CBV maps could be a useful predictive tool for the viability of
ischemic tissue, because the ischemic regions with
decreased CBV proceeded to infarction in the present study,
and moreover, a reliable correlation was demonstrated between the
lesion volume of diffusion-weighted imaging and the CBV
map.7
On the other hand, in the regions with reperfusion, MTT was reduced or normal, although both CBF and CBV were increased. Interestingly, CBV and CBF were uncoupled, indicative of a potentially harmful vasoparalysis. T2-weighted MRI at this time often showed infarction. Hence, the ischemic tissue should be carefully assessed in combination with DSC-MRI to avoid attempts to recanalize vessels supplying spontaneously reperfused tissue. The determination of such variability would allow optimum therapy to be tailored to individual patients with acute stroke. For example, one testable hypothesis suggested by these data is that patients with a severe decrease of CBV (or CBF) would not benefit from thrombolytic therapy, whereas patients with an increase of CBV (or mild reduction of CBF) could benefit from thrombolytic therapy during the occlusion.
Limitations in DSC-MRI
Delays in arrival of contrast agent may be interpreted as a
CBF decrease, and therefore collateral flow may not be
represented adequately.2 6 In the present
study, the region supplied previously by the MCAs was perfused via the
collateral flow from the anterior cerebral artery because the MCAs were
completely occluded, as shown by angiography. However, DSC-MRI gave the
same CBF result as PET, although more mathematical work could improve
this technique for ongoing use in the evaluation of patients with acute
ischemia, in whom tracer arrival delays may be more severe. In
contrast, CBV values obtained by DSC-MRI were underestimated, possibly
because the tissue concentration time curve may be delayed and
dispersed and difficult to distinguish from the second pass. Thus, the
area could be underestimated by our numerical integration routine. This
effect affects the PET CBV measurements less, because signals are
recorded over 3 minutes, allowing for slow tracer passage. The
underestimation of CBV may have caused MTT, ie, the CBV/CBF ratio, to
be underestimated by the same amount in the infarcted regions.
Another limitation with this technique is that all intravascular tracer methods require delivery of the tracer to the region of measurement. This limitation also applies to PET, of course. Thus, true CBF and CBV values may be larger than recorded simply because no tracer is reaching dilated but nonperfused blood vessels. However, the present study consistently identified the flow-volume mismatches, although the shortcoming could mask greater mismatches.
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Acknowledgments |
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This study was funded by Danish Medical Research Council grants (9305246, 9305247, 9601888, and 9802833) and the Institute of Experimental Clinical Research, University of Aarhus, Denmark. The authors thank Nycomed Imaging (Oslo, Norway) for providing the contrast agent for this study. We thank Dr Donald F. Smith (Aarhus, Denmark) for his contributions to the improvement of the manuscript, Dr Jens Christian Sørensen (Aarhus, Denmark) for the histological preparations, and the technicians of the PET and MRI centers for their skillful assistance. We are grateful for the helpful contribution and support of Professor Saburo Sakaki (Ehime, Japan) during this project.
Received February 8, 2000; revision received April 26, 2000; accepted May 18, 2000.
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Editorial Comment
Comparison With [15O]H2O Positron Emission Tomography
Center for Stroke Research, Department of Neurology, Henry Ford Health Sciences Center, Detroit, Michigan {hd1}
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TopAbstractIntroductionMaterials and MethodsResultsDiscussionReferencesIntroduction |
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Techniques that can provide fast and accurate measurements of cerebral blood flow (CBF) and blood volume (CBV) represent an important diagnostic tool for the evaluation of the acute stroke patient. They can yield information about the anatomic location and degree of cerebral ischemia and the success or failure of reperfusion, and they may be potentially useful for planning therapeutic interventions.
The early development of magnetic resonance methods to measure CBF and CBV utilized tracer compounds that were labeled with MR-sensitive nuclei (eg, 3H, 17O, and 19F). More recently, there has been a flurry of activity to develop CBF and CBV measurement techniques that use high-speed MRI methods to track the passage of a bolus of a magnetic susceptibility contrast agent or magnetic labeling of protons in arterial blood with radiofrequency pulses. However, most of these studies have focused on the theoretical and methodological aspects of the measurements; there have been few that actually attempt to validate the accuracy of the technique by comparing MRI-based CBF and CBV measurements with a well-accepted "gold standard" method.
The study by Sakoh et al uses MRI to measure CBF and CBV in a novel model of middle cerebral artery occlusion and reperfusion in pigs. Measurements obtained by using dynamic susceptibility contrast (DSC)-MRI were evaluated and compared with similar measurements obtained with positron emission tomography (PET) methods to determine whether DSC-MRI could provide accurate measurements of CBF and CBV in stroke. The results demonstrate good agreement between parametric maps of CBF and CBV obtained using the 2 methods, with infarction demonstrated in brain regions having CBF values <60% of contralateral levels. Highly significant regional correlations were detected between DSC-MRI and PET measures of CBF, and to a slightly lesser degree CBV, with DSC-MRI showing lower CBV values than PET.
This study offers new and original information about the accuracy of DSC-MRI measurements of CBF and CBV in acute stroke. Although such studies performed with experimental animal models of cerebral ischemia may not exactly reproduce the conditions encountered in human stroke, they will provide an essential link toward the eventual goal of performing these measurements in the clinical setting.
Received February 8, 2000; revision received April 26, 2000; accepted May 18, 2000.
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