Loss of Interhemispheric Connectivity in Patients with Lacunar Infarction Reflected by Diffusion-Weighted MR Imaging and Single-Photon Emission CT

Participants

We studied nine patients with multiple lacunar infarction (six men and three women; average age, 74 ± 8 years; range, 62–86 years) and poor cognitive levels as evaluated by mini-mental state examination (MMSE) (mean score, 17 ± 5; range, 10–23), and six healthy young adult volunteers (six men; average age, 30 ± 4 years; range, 25–35). Informed consent was obtained from every participant. Using a database of patients with multiple lacunar infarction in our laboratory, the study group was selected from persons who underwent brain SPECT and MR imaging within a 3-week interval. Every subject had a clinical history of repeat transient ischemic attack and hypertension and had multiple lacunae in the deep cerebral region around the perforating vessels revealed by routine T1- and T2-weighted MR imaging. We did not include patients with cortical lesions in order to eliminate the effect of direct cortical tissue damage.

Imaging Protocol

MR imaging data were acquired using a 1.5-T system (SignaHorizon, General Electric Yokokawa Medical Systems, Tokyo, Japan) at the maximum gradient strength of 23 mT/m and slew rate of 77 T/m per second with a quadrature head coil. A subject's head was carefully placed to ensure that the anterior-posterior commissure line was parallel to the axial gradient planes and axial sections. Routine MR imaging evaluation of 15 contiguous axial sections of the whole brain was performed using conventional spin-echo T1-weighted 420/10 (TR/TE) and fast spin echo T2-weighted 3500/100 (TR/TE_eff) images, with an echo train of 10, a field of view of 24 × 24 cm, an imaging matrix of 256 × 256, and a 6.5-mm section thickness with a 2.0-mm gap. For diffusion-weighted MR imaging, single-shot echo-planar imaging was used to obtain 12 to 14 contiguous axial 6500/120 sections, with a field of view of 24 × 24 cm, an imaging matrix of 128 × 128, and a 7.0-mm section with a 1.0-mm gap. The diffusion gradient pulses were applied with settings of b = 0 and b = 710 along the readout gradient axis (right to left, x-axis) and the phase gradient axis (anterior to posterior, y-axis), respectively; their duration was 25 milliseconds with a 29.2-millisecond gap.

SPECT data were acquired using a three-headed gamma camera Prism 3000 (Picker-Shimadzu International Inc, Kyoto, Japan), with low-energy high-resolution collimation and 5° projections over each 120° with 60 seconds of data collimation per projection, at 10 minutes after intravenous injection of 222 MBq of iodine-123 iodoamphetamine (¹²³I-IMP). After prefiltering the projection data with the standard 2D Butterworth filter, axial images parallel to the anterior-posterior commissure line were reconstructed with a 6.8-mm section thickness and a 1.0-mm gap. The reconstruction matrix of the SPECT scans was 128 × 128, and spatial resolution was 9 mm full width at half-maximum in the axial plane.

Determination of Diffusional Anisotropy

Three series of diffusion-weighted MR imaging data with a setting of b = 0 and b = 710 for each x- and y-axial direction were processed on an online computer system (Sun Sparc20) to create parametric ADC maps of each direction by using interactive data language software. For the calculation of ADC, the monoexponential intravoxel incoherent motion model (6) was used. Therefore, the ADC value of each direction can be determined in each pixel from the relative signal intensities by solving the following equations: where S is the signal intensity, b is the factor determined by the gradient strength, and each ADC_x and ADC_y is the ADC value in each axial direction. Region of interest (ROI) data of the ADC_x and ADC_y maps were extracted from the anterior and posterior parts of the corpus callosum and optic radiation (Fig 1). The ratio of ADC_x to ADC_y, namely, the anisotropic rate (AR) (AR = ADC_x/ADC_y × 100), was calculated as an index of diffusional anisotropy as in previous studies (15, 16). This index can be used to determine the main fiber orientation in a particular ROI. If the AR is greater than 1, the fibers are oriented in an x-axial direction; and if the AR is less than 1, the fibers are oriented in a y-axial direction.

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fig 1.

A representative level of calculated ADC maps. ROIs, placed on the anterior and posterior corpus callosum and optic radiation, are 100 to 200 pixels each and the same in contour between the two maps.

A, ADC

B, ADC

C, A scheme for regional data extraction from these maps.

Determination of ACV and Evaluation of the Relation to Neuronal Connectivity

For intersubject analysis, SPECT scans usually require normalization to counts in a certain reference area. In this study, the value of maximal counts measured in the visual cortex was used for normalization because there were no participants with reduced visual function in this study. Initially, brain uptake of greater than 80% of the maximal counts in the visual cortex was assumed to represent active cortical tissue and we defined it as the upper masking level. A lower masking level for eliminating pixels of white matter and CSF space from SPECT scans was also determined. After excluding scatter counts outside the brain, binary maps at the preliminary lower masking levels of 60%, 65%, and 70% of the maximal counts in the visual cortex of the subjects were created to determine which level results in a proportion of masked pixels closest to that of major white matter and CSF space, as has previously been calculated using manual thresholding of anatomic MR imaging (17). The ACV was thus defined as the regional ratio of the number of pixels above the 80% map to the number above the lower masking map as follows: The validity of this parameter was determined by testing whether these values eliminated partial volume effects using brain phantom (IB-10, Kyotokagaku-Hyohon, Kyoto, Japan) SPECT scans. SPECT scans were obtained using exactly the same protocol as in the human experiment described above, with ¹²³I-IMP concentration of gray matter and white matter of 7.8 MBq/530 mL and 2.2 MBq/300 mL (concentration rate = 2:1), respectively.

Using the original human SPECT scans, ROIs were specified in the superior and inferior frontal associative areas, the parietal associative area, and the temporal associative area, to exclude the primary sensorimotor area, mesial temporal lobe, or insula. These were then superimposed on the ACV maps (Fig 2). To determine whether these ACVs correlated with cognitive function, they were compared with the cognitive scores in the patient group. The ARs were then compared with these ACVs for all subjects to elucidate the relationship between the interhemispheric neuronal connectivity and cortical perfusion.

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fig 2.

A–D, A representative series of binary SPECT scans showing masking levels of 60% (A), 65% (B), and 70% (C) of the maximal counts and the original SPECT scan (D). As the masking level increased, the number of masked pixels of relatively low counts also increased

Statistical Analysis

Parametric variables were expressed as mean values ± SD. Regional differences between the ACVs within a group were compared using one-way analysis of variance corrected for multiple comparisons, and the intergroup differences between the ACVs as well as between the ARs were compared using unpaired two-tailed t-tests, with P < .05 representing statistical significance. Correlations between the ACV and MMSE scores within the patient group, and between the ACV and MR values of all subjects, were determined using linear regression analysis, also with P < .05 representing statistical significance.

Determination of the Lower Masking Level for ACV Based on Human SPECT Scans

Figure 3 and Table 1 show the process of how the best lower masking level was determined. As shown in Table 1, the masked volume ratio at the 70% level was close to the ratio previously reported (49.5%) (17), and we selected that as the lower masking level.

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fig 3.

An explanation of how the ACV, determined as the ratio of the number of pixels above the 80% masking level to the number above the 70% level, is validated. In this setting, the ACVs derived from the eight cortical areas should be homogeneous, because the actual tracer accumulation in the cortical area is uniform regardless of the regions.

A, Phantom MR image.

B, Phantom ¹²³I-IMP SPECT scan.

Validation of ACV by Phantom SPECT Scans

Figure 4 shows phantom SPECT scans depicting eight different ROIs in various cortical regions. As shown in Table 2, the coefficient of variance of the ratio of the number of pixels above the 80% level to the number above the 70% level in these ROIs was much smaller than that of the number of pixels themselves, indicating that it reflects actual tracer accumulation regardless of the cortical regions.

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fig 4.

A and B, A representation of regional data extraction from one of the original SPECT scans. ROIs are specified at the superior frontal lobe and the parietal lobe (A), and the inferior frontal lobe and the temporal lobe (B), so as not to include the primary sensorimotor area, mesial temporal lobe, or insula. The ROIs are superimposed on ACV maps

Comparisons of Regional ACV between Groups

In terms of regional ACV differences, the lowest ACVs were observed in the frontal associative areas of the patient group; however, regional ACV differences were not significant in either the patient or volunteer groups. When regional ACVs were compared between the groups, there were significant decreases in the patients' ACVs in the superior frontal region, inferior frontal region, and temporal lobe (P < .05). These results are presented in Table 3. In the patient group, furthermore, individual ACVs in the superior and inferior frontal regions correlated well with the cognitive score (superior frontal: r = .87, P < .05; inferior frontal: r = .73, P < .01). These results are shown in Figure 5.

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fig 5.

Correlations between the regional ACV and the MMSE scores. Individual ACVs in the superior and inferior frontal regions were well correlated with the MMSE score (superior frontal: r = .89, P < .05; inferior frontal, r = .71, P < .05).

Left upper, superior frontal.

Right upper, inferior frontal.

Left lower, parietal.

Right lower, temporal.

Comparisons of Regional Diffusional Anisotropy between Groups

In both groups, the AR was markedly larger in the corpus callosum than in the optic radiation, attributable to regional differences in diffusional anisotropy. Compared with the healthy group, however, there were significant decreases in the patients' ARs in the anterior and posterior parts of the corpus callosum (P < .05). Table 4 summarizes the regional ARs in both groups.

Relationship between Associative Cortical Activity and Neuronal Connectivity

Including the data of all participants, the AR in the anterior corpus callosum was strongly correlated with the frontal ACV (Fig 6) (superior frontal: r = .86, P < .0001; inferior frontal: r = .79, P < .0005). However, these correlations were insignificant within the group of patients with multiple lacunae, probably because of the limited number of patients in this study. No significant correlation was shown in the other combinations of the AR and the ACV.

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fig 6.

Correlations between the regional AR of the corpus callosum and the ACV of the frontal areas. The AR in the anterior corpus callosum is strongly correlated with the frontal ACVs (superior frontal: r = .86, P < .0001; inferior frontal: r = .79, P < .0005). However, there are insignificant trends toward correlation between the AR in the anterior corpus callosum and the frontal ACVs within the patient group.

Left upper, anterior corpus callosum versus superior frontal region.

Right upper, anterior corpus callosum versus inferior frontal region.

Left lower, posterior corpus callosum versus superior frontal region.

Right lower, posterior corpus callosum versus inferior frontal region.