| Literature DB >> 23094098 |
Katherine H Karlsgodt1, Tena Rosser, Evan S Lutkenhoff, Tyrone D Cannon, Alcino Silva, Carrie E Bearden.
Abstract
Neurofibromatosis (NF1) represents the most common single gene cause of learning disabilities. NF1 patients have impairments in frontal lobe based cognitive functions such as attention, working memory, and inhibition. Due to its well-characterized genetic etiology, investigations of NF1 may shed light on neural mechanisms underlying such difficulties in the general population or other patient groups. Prior neuroimaging findings indicate global brain volume increases, consistent with neural over-proliferation. However, little is known about alterations in white matter microstructure in NF1. We performed diffusion tensor imaging (DTI) analyses using tract-based spatial statistics (TBSS) in 14 young adult NF1 patients and 12 healthy controls. We also examined brain volumetric measures in the same subjects. Consistent with prior studies, we found significantly increased overall gray and white matter volume in NF1 patients. Relative to healthy controls, NF1 patients showed widespread reductions in white matter integrity across the entire brain as reflected by decreased fractional anisotropy (FA) and significantly increased absolute diffusion (ADC). When radial and axial diffusion were examined we found pronounced differences in radial diffusion in NF1 patients, indicative of either decreased myelination or increased space between axons. Secondary analyses revealed that FA and radial diffusion effects were of greatest magnitude in the frontal lobe. Such alterations of white matter tracts connecting frontal regions could contribute to the observed cognitive deficits. Furthermore, although the cellular basis of these white matter microstructural alterations remains to be determined, our findings of disproportionately increased radial diffusion against a background of increased white matter volume suggest the novel hypothesis that one potential alteration contributing to increased cortical white matter in NF1 may be looser packing of axons, with or without myelination changes. Further, this indicates that axial and radial diffusivity can uniquely contribute as markers of NF1-associated brain pathology in conjunction with the typically investigated measures.Entities:
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Year: 2012 PMID: 23094098 PMCID: PMC3477133 DOI: 10.1371/journal.pone.0047854
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Figure 1DTI diagram showing radial diffusion, axial diffusion and ADC as related to FA.
Demographics.
| Patients | Controls | Statistics | |
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| 24±4.93 | 22.66±4.54 | t(24) = .713, p = .483 |
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| 6/8 | 5/7 | X2 = .0038, p = .951 |
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| 96.79±8.68 | 109.62±9.78 | t(20) = 2.189, p = .0046 |
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| 14.21±2.12 | 15.00±2.28 | t(24) = -.613, p = .5459 |
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| X2 = .1806, p = .671 | ||
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| 7 | 5 | |
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| 5 | 1 | |
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| 2 | 0 | |
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| 0 | 3 | |
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| 0 | 3 |
IQ data was only available for 8/12 control subjects.
Race and ethnicity statistics were calculated for Caucasian vs non-Caucasian subjects.
Figure 2Gray and White Matter volumetric differences between groups.
Figure 3Voxelwise analysis of FA, at a threshold of p<.05 (left) and p<.005 (right).
Red colors reflect areas of decreased FA in the NF1 group.
Figure 4Voxelwise analysis of radial diffusion, at a threshold of p<.05 and p<.005.
Green colors reflect increased radial diffusion in the NF1 group.
Figure 5Voxelwise analysis of axial diffusion, at a threshold of p<.05 and p<.005.
Brown colors reflect increased axial diffusion in the NF1 group.
Figure 6Voxelwise analysis of ADC, at a threshold of p<.05 and p<.005.
Blue colors reflect increased ADC in the NF1 group.
Differences in Fractional Anisotropy (NF1 Patients vs. Controls).
| Region | Hemisphere | Patients | Controls | Statistics |
| Anterior Thalamic Radiation | L |
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| Anterior Thalamic Radiation | R |
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| Corticospinal Tract | L | .5567 (.0207) | .5654 (.0228) | t(24) = 1.01, p = .321;effect size = .390 |
| Corticospinal Tract | R | .5391 (.0182) | .5433 (.0187) | t(24) = 5.74, p = .572;effect size = .229 |
| Cingulate Bundle | L |
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| Cingulate Bundle | R | .5315 (.0374) | .5555 (.0300) | t(24) = 1.786, p = .087; effect size = .692 |
| Hippocampal Cingulum | L | .3305 (.0195) | .3379 (.0423) | t(24) = .591, p = .2815; effect size = .235 |
| Hippocampal Cingulum | R | .2968 (.0231) | .3093 (.0345) | t(24) = 1.10, p = .282;effect size = .432 |
| Forceps Major | L+R | .7215 (.0351) | .7349 (.0313) | t(24) = 1.023, p = .316; effect size = .402 |
| Forceps Minor | L+R | .5538 (.0186) | .5561 (.0278) | t(24) = 1.838, p = .078; effect size = .691 |
| Inferior fronto-occipital fasciculus | L | .4359 (.0184) | .4592 (.0215) | t(24) = 2.98, p = .0066; effect size = 1.02 |
| Inferior fronto-occipital fasciculus | R | .4329 (.0203) | .4567 (.0204) | t(24) = 2.97, p = .0066; effect size = 1.02 |
| Inferior longitudinal fasciculus | L | .4064 (.0139) | .4178 (.0257) | t(24) = 1.44, p = .164;effect size = .553 |
| Inferior longitudinal fasciculus | R | .4154 (.0175) | .4282 (.0203) | t(24) = 1.72, p = .098;effect size = .652 |
| Superior longitudinal fasciculus | L | .4400 (.0229) | .4550 (.0312) | t(24) = 1.41, p = .172;effect size = .543 |
| Superior longitudinal fasciculus | R | .4538 (.0273) | .4568 (.0208) | t(24) = .312, p = .754;effect size = .125 |
| Uncinate fasciculus | L | .4265 (.0216) | .4308 (.0259) | t(24) = 4.64, p = .647;effect size = .185 |
| Uncinate fasciculus | R | .4072 (.0196) | .4239 (.0260) | t(24) = 1.87, p = .074;effect size = .70 |
Region of interest based FA analysis.
Radial and Axial Diffusion and ADC: NF1 Patients vs. Controls.
| Tract | Measure | Patients | Controls | Statistics |
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| Axial | .001190 (2.67×10−5) | .001180 (2.74×10−5) | t(24) = .9817, p = .3361 | |
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| Axial | .001175 (3.09×10−5) | .001162 (3.25×10−5) | t(24) = .996, p = .3292 | |
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| Axial | .001260 (4.11×10−5) | .001249 (2.87×10−5) | t(24) = .803, p = .430 | |
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| Axial | .001267 (5.47×10−5) | .001252 (3.65×10−5) | t(24) = .808, p = .427 | |
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Supplementary ROI analysis testing radial diffusion, axial diffusion, and ADC in regions with significant FA findings.