Tractography of the Corpus Callosum in Huntington’s Disease

Owen Phillips; Cristina Sanchez-Castaneda; Francesca Elifani; Vittorio Maglione; Alba Di Pardo; Carlo Caltagirone; Ferdinando Squitieri; Umberto Sabatini; Margherita Di Paola

doi:10.1371/journal.pone.0073280

Abstract

White matter abnormalities have been shown in presymptomatic and symptomatic Huntington’s disease (HD) subjects using Magnetic Resonance Imaging (MRI) and Diffusion Tensor Imaging (DTI) methods. The largest white matter tract, the corpus callosum (CC), has been shown to be particularly vulnerable; however, little work has been done to investigate the regional specificity of tract abnormalities in the CC. Thus, this study examined the major callosal tracts by applying DTI-based tractography. Using TrackVis, a previously defined region of interest tractography method parcellating CC into seven major tracts based on target region was applied to 30 direction DTI data collected from 100 subjects: presymptomatic HD (Pre-HD) subjects (n = 25), HD patients (n = 25) and healthy control subjects (n = 50). Tractography results showed decreased fractional anisotropy (FA) and increased radial diffusivity (RD) across broad regions of the CC in Pre-HD subjects. Similar though more severe deficits were seen in HD patients. In Pre-HD and HD, callosal FA and RD were correlated with Disease Burden/CAG repeat length as well as motor (UHDRSI) and cognitive (URDRS2) assessments. These results add evidence that CC pathways are compromised prior to disease onset with possible demyelination occurring early in the disease and suggest that CAG repeat length is a contributing factor to connectivity deficits. Furthermore, disruption of these callosal pathways potentially contributes to the disturbances of motor and cognitive processing that characterize HD.

Citation: Phillips O, Sanchez-Castaneda C, Elifani F, Maglione V, Di Pardo A, Caltagirone C, et al. (2013) Tractography of the Corpus Callosum in Huntington’s Disease. PLoS ONE 8(9): e73280. https://doi.org/10.1371/journal.pone.0073280

Editor: Ya-Ping Tang, Louisiana State University Health Sciences Center, United States of America

Received: April 4, 2013; Accepted: July 18, 2013; Published: September 3, 2013

Copyright: © 2013 Phillips et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Funding: This work was supported by the Italian Ministry of Health GRANT 204/GR-2009-1606835. Also, support was provided by the European Commission: Marie Curie Fellowship for career development to CS (FP7-PEOPLE-2011-IEF). The authors are grateful for the support they received from the Italian Ministry of Health (Ricerca Corrente), by Telethon [GGP12218], European Huntington’s Disease Network for the Registry Study, by the Italian Association Huntington Research “Lega Italiana Ricerca Huntington” and by the Italian Association of HD Families “Associazione Italiana Corea di Huntington - Neuromed.” The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The authors are grateful to all patients for contributing to the work.

Competing interests: The authors have declared that no competing interests exist.

Introduction

Huntington’s disease (HD) is neurodegenerative process caused by CAG repeats in the protein Huntington (HTT) gene [1]. Despite our understanding of HD genetics, the pathogenesis that results in the phenotype remains unclear since disease progression seems to be influenced by factors other than simply the mutation length [2].

The typical HD phenotype is characterized by middle to late age of onset, and by early specific neurodegeneration of striatal neurons. Many studies have documented the deleterious effect HD has on the brain, (for review see: [3]). Furthermore, it has been shown that presymptomatic (Pre-HD) subjects may have brain atrophy up to 10 years before disease manifestation [4], [5]. However, less is known about the effects of HD on white matter (WM) fibers. As opposed to gray matter where a variety of cell bodies (neurons, astrocytes, and oligodendrocytes) and processes (axons, dendrites, and myelin) coexist, WM fibers are composed primarily of myelin and axons. Thus, data on WM modifications in HD can provide the clearest support for the hypothesized process of HD pathogenesis: such as breakdown of early and heavily myelinated fibers and/or axonal degeneration [6].

The corpus callosum (CC) is an ideal WM fiber to investigate. This is because the CC is the largest WM fiber tract in the brain and it contains more 200 million WM fibers that transfer information between the hemispheres. These fibers arise from pyramidal cells that are affected early in HD [7]. The fibers vary in size and age of myelination with larger and early myelinated fibers seen in posterior regions and smaller and late myelinating fibers found in anterior regions [8], [9]. Because of this, the CC has been extensively studied in a number of neurological and psychiatric disorders [10], [11], [12]. Therefore, analyzing CC structure may elucidate the pathological process and regional differences HD has on WM myelination and/or axonal damage. Furthermore, since few callosal fibers arise from cortico-striatal neurons, callosal changes can give a different view of the HD physiopathology.

Diffusion tensor imaging (DTI) is the most frequently magnetic resonance imaging (MRI) technique used to study WM fibers changes. DTI approach is a non-invasive technique, which uses the local water diffusion in the brain tissues to study microstructural aspects of WM anatomy [13]. Though the biological determinants of diffusion parameters are not yet fully understood, (for an in-depth discussion on diffusion imaging see [14]), it is agreed that it is a sensitive modality to microstructural tissue properties. Reductions in fractional anisotropy (FA) could reflect decreased numbers of fibers or indicate reduced axonal myelination [15]. Furthermore, axial diffusivity (AD), a measure of how fast diffusion occurs in the preferred direction, has been shown to be sensitive to the number of axons, as well as their coherence [16]. Increased AD is related to WM axonal atrophy likely associated with Wallerian degeneration although in some cases it may be attributed to increased fiber organization [17]. Radial diffusivity (RD) is a measure of how fast diffusion occurs in the perpendicular direction. Increased RD is thought to reflect reductions in myelination [18], [19], [20].

Recent DTI studies suggest that abnormalities in HD extend to WM tracts. Two such studies showed CC degeneration in HD patients [21], [22] with early degeneration of cortico-cortical connectivity [23] likely contributing to a deficit in associative cortical processing. Two others have suggested that Pre-HD subjects exhibit WM fibers deficits in the CC [24], [25] and motor cortico-striatal circuit connectivity. Furthermore, reduced CC density in the isthmus predicted the “HD development” index [24] and early changes in CC, thalamus, sensorimotor and prefrontal region correlated with clinical function [25]. As such, DTI data may be particularly useful in identifying early and progressive WM changes in HD.

A relatively new step in MRI callosal WM abnormalities investigations is to apply DTI-based tractography, which allows the precise mapping of CC tract anatomy within subjects. The tractography method used in this study has the advantage to not be sensitive to the confounds of voxel-based registrations [26]. Furthermore, it provides regional specificity in anatomical modifications within the CC, by incorporating WM connectivity information. DTI-based tractography, indeed, can map apparent connectivity of voxels in the CC to specific cortical areas, since callosal fibers keep the topology of the orbital–frontal–parietal–occipital lobes.

DTI-based tractography has been reliably used to examine WM in a large number of studies because it allows the investigator to address whether disturbances of WM connectivity occur within particular cortical networks [27], [28], [29], [30]. That is, because the diffusion tensor approximating local diffusion is determined by the local tissue architecture, it can be used to generate an in vivo visualization of WM tracts [31], [32], [33], [34]. Although some doubt exists that tractography may generate sufficiently reproducible neuro-anatomical detail for use in quantitative analyses, evidence supports that tracking results agree well with postmortem definitions [35], [36].

To our knowledge, no studies have been published using tractography to investigate regionally specific callosal WM abnormalities in HD and Pre-HD, in spite of the valuable information this approach can provide in terms of callosal WM connectivity modification.

The main aims of our study were 1) to explore the biological mechanism underlying callosal WM changes in a large cohort of subjects (25 HD patients and 25 Pre-HD, and 50 healthy subjects), we predicted that demyelination occurs prior to axonal degeneration in the CC; 2) to individuate a regional specificity in the CC changes, characteristic of the HD pathology, we predicted that the CC and each of the segments would be disturbed in HD with the most severe disturbances located in tracts with target regions in motor areas; 3) to investigate a possible association among genetic, cognitive, motor data and CC fiber values. We predicted that CAG repeat length would be negatively associated with CC microstructure. Lastly, we hypothesized that cognitive and motor scores in patients would be associated with CC fiber organization.

For these purposes, we used both DTI and DTI-based Tractography. We examined the CC in its entirety and segmented into its seven sub regions based on unique target areas: the orbital frontal (OF), anterior frontal (AF), superior frontal (SF), superior parietal (SP), posterior parietal (PP), temporal (Temp), and occipital (Occ). These tracts are easily identifiable using a multiple region of interest (ROI) approach in DTI data [37], [38].

Materials and Methods

Ethics Statement

The Santa Lucia Foundation Research Ethics Committee approved this study. All participants had the cognitive capacity to understand the research protocol and gave their oral and written consent. For those participants with disabling motor impairment, their proxies provided signature on the written informed consent. Consent was obtained according to the Declaration of Helsinki and the Santa Lucia Foundation Research Ethics Committee approved the study.

Subjects

Subject demographics and clinical assessments are outlined in Table 1. HD patients (n = 25) and Pre-HD subjects (n = 25), underwent a genetic test (abnormal CAG repeats ≥36) and were examined clinically by the same neurologist with expertise in HD. All individuals were assessed using the Unified Huntington’s Disease Rating Scale (UHDRS), which includes motor, cognitive, behavioral, and functional subscales [39]. Each section consists of a multistep subscale. The motor section measures eye movements, limb coordination, tongue impersistence and movement disorders (such as rigidity, bradykenisia, dystonia, chorea, and gait disturbances). A higher score means more motor impairment. The cognitive scale mainly evaluates executive function. A higher score means better cognitive performance. The behavioural section investigates the presence of depression, aggressiveness, obsessions/compulsions, delusions/hallucinations and apathy. A higher score means more impairment. The functional assessments include the HD functional capacity scale (HDFCS), the independence scale and a checklist of common daily tasks. All three scales mainly investigate independence in daily life activities. The HDFCS is reported as the total functional capacity (TFC) score (range 0–13) and is the only functional subscale with established psychometric properties (including inter-rater reliability and validity), which are based on radiographic measures of disease progression. Thus, the TFC score is used worldwide to determine patients’ HD stage. On the independence scale, the investigator indicates whether the patient can perform the task that evaluates independence level (range 10–100). The checklist (functional assessment) is summed by giving a score of 1 to all “yes” answers (range 0–25). Pre-HD are defined as those subjects whom the suspected clinical diagnosis is confirmed by DNA analysis, which revealed (CAG)(n) expansion into the range characteristic of Huntington disease (>40 repeats), but who do not have manifested Huntington’s disease symptoms yet defined by a total motor score of <5 in the UHDRS and cognitive and behavioural assessment within the normality. The Disease Burden index, a measure of disease severity, was used according to the already described formula (age×[CAG-35.5]), where CAG is the number of CAG repeats [40]. A higher score reflects increased disease severity. The Mini-Mental State Examination (MMSE) [41], which measures global cognitive functioning, was administered to Pre-HD subjects and HD patients. A lower score reflects greater impairment.

Download:

Table 1. Sociodemographic and clinical characteristics of patients and control subjects.

https://doi.org/10.1371/journal.pone.0073280.t001

Fifty individually healthy subjects were recruited from the community. Patients in the advanced stages of disease (Stages III and IV) and/or with traumatic brain injury or focal lesions were excluded.

MRI Data Acquisition

All MRI data was acquired on a 3 T Allegra MRI system (Siemens, Germany) using a birdcage head coil. Scans were collected in a single session, with the following pulse sequences: 1) proton density and T2-weighted double turbo spin echo (SE) acquired in transverse planes (time repetition [TR]: 4500 ms, time echo [TE]: 12 ms, time to inversion [TI]: 112 ms, field of view [FOV]: 230 × 172 mm, matrix: 320 × 240, slice thickness: 5 mm, number of slices: 24); 2) fluid-attenuated inversion recovery in the same planes as the SE sequence (TR/TE/TI: 8500/109/2000 ms; FOV: 230 × 168 mm, matrix: 256 × 256, slice thickness: 5 mm, number of slices: 24); 3) T1-weighted 3 D images, with partitions acquired in the sagittal plane, using a modified driven equilibrium Fourier transform [42] sequence (TE/TR/TI: 2.4/7.92/910 ms, flip angle: 15°, 1 mm3 isotropic voxels); and 4) diffusion-weighted volumes were also acquired using SE echo-planar imaging (TE/TR: 89/8500 ms, bandwidth: 2126 Hz/voxel, matrix: 128×128, 80 axial slices, voxel size: 1.8×1.8×1.8 mm) with 30 isotropically distributed orientations for the diffusion sensitizing gradients at a b value of 1000 s/mm2 and 6 b = 0 images. Scanning was repeated 3 times to increase the signal-to-noise ratio.

Images were visually inspected for gross anatomical abnormalities by 2 experienced observers (a neuropsychologist expert in neuroimaging and a neuroradiologist) blind to participant identities.

Images were also visually inspected for movement artifacts, which are a common source of concern while studying HD. Since movement can compromise CC tracking, we excluded subjects who had excessive movement in their scans.

DTI Processing

Diffusion-weighted images were processed with FMRIB’s Software Library (FSL 4.1 www.fmrib.ox.ac.uk/fsl/). The non-diffusion-weighted images were skull stripped using FSL’s Brain Extraction Tool (BET) (http://www.fmrib.ox.ac.uk/fsl/bet2/index.html), and used to mask all diffusion-weighted images [43]. Images were corrected for eddy current distortion, followed by FSL FLIRT for motion correction. After corrections, the DTI data was averaged and concatenated into 31 (1 B0+30 B1000) volumes. A diffusion tensor model was fitted at each voxel using Diffusion Toolkit, generating FA, AD, and RD maps. RD was defined as the average of the second and third eigenvalues of the diffusion tensor, while AD corresponded to the first eigenvalue.

Tractography

Tractography methods are outlined in more detail in [37], however, the tractography and ROI drawing was modified to use TrackVis, an interactive environment for fiber tracking reconstruction, display and analysis developed at the Harvard Medical School Martinos Center for Biomedical Imaging at Massachusetts General Hospital (www.trackvis.org). The FACT approach was used to reconstruct fiber paths. For details of the TrackVis tracking algorithm see [44]. A track angle threshold of 35° was used as well as an image mask based on the B0 image to restrict tracking to biologically plausible results.

It is important to note that tractography is still an emerging technology and limitations such as the fact that fiber bundles are not reconstructed directly; instead trajectories are calculated through the data, which are (hopefully) largely parallel to nerve fibers. As such, interpretations of diffusion data should keep in mind that we cannot as of yet assert categorically that scores are being driven by a specific biological or physiological process [14].

Tractography of the CC was performed by manually drawing regions of interest on each individuals FA color map by a single expert (OP) who was blinded to subject age, gender, and diagnosis.

To determine intra-rater reliability, fiber tracts were identified in 10 randomly chosen brain volumes. Reliability was assessed using the intraclass correlation coefficient (2-way mixed for intra-rater). Statistical analyses were performed using SPSS 14.0. Excellent intra reliability was achieved for ROI placement as determined by computing the intra-class correlation coefficients for tract volume and mean FA, AD and RD (Table S1).

Tractography was performed using the two region-of-interest approach. One region was drawn on a midsagittal slice encompassing the entire CC, and seven separate regions of interest spanning both sides of the midline were used as target regions to segment the CC into distinct sections. All regions of interest were drawn according to specific anatomical landmarks and guidelines that were followed carefully and consistently for each individual; the ROI placements are described by [38]. Ordered from front to back the seven sections delineated were: orbital frontal (OF), anterior frontal (AF), superior frontal (SF), superior parietal (SP), posterior parietal (PP), temporal (Temp), and occipital (Occ). ROI locations and exclusion criteria are further detailed in [37]. Fibers that were clearly not part of the anatomical connectivity of the track were eliminated. FA, AD, and RD were calculated for each region by averaging all voxels over the entire tract, counting each voxel only once.

Statistical Analysis

Demographic differences were assessed using chi-square, independent sample t-tests or Anova as appropriate.

To test for callosal differences, a Multivariate Analysis of Variance (Manova) was applied to all three groups (healthy controls, HD patients and Pre-HD subjects). Sex and age were included as covariates in the model. After that, contrasts were run to individuate the significant difference between groups. To control for multiple comparisons, we used a False Discovery Rate (FDR) threshold p<0.05.

In order to investigate which early callosal changes in the course of pathology were related to clinical, cognitive and genetic aspects, we performed, correlations analysis between CAG repeat length, Disease burden, clinical scales (UHDRS-Motor, -Cognitive), and track measures. Track measures were limited to tract regions and measures already compromised in Pre-HD subjects (main analysis). Operationally we took in consideration only those tract regions and measures that were significantly different between healthy controls and Pre-HD subjects. From those tracts and measures, we extracted values both from the Pre-HD and HD groups. We included these extracted values in the correlational analysis together with the above-mentioned genetic, cognitive and clinical scores. Sex and age were included as covariates. To control for multiple comparisons, we used a False Discovery Rate (FDR) threshold p<0.05.

Results

Subject Demographic

Details are outlined in Table 1. Pre-HD subject and HD patients differed in age and CAG repetition length. Additionally, as expected, HD patients had significantly poorer performances with respect to all measures assessed by the UHDRS, and also a significantly higher score of Disease Burden.

Tractography Data

Statistical details for Manova analysis are provided in Table 2. Track measures are outlined in Table S2. Figure 1 further provides a graphical overview of the findings as well as an indication of significant results.

Download:

Figure 1. Corpus Callosum Tract Measures by Diagnosis.

Bar graphs show differences between CC FA, AD, and RD for the whole CC and the seven components of the CC as defined by the tract target region. The error bars represent the Standard Error Mean (SEM). Tracts: Whole corpus callosum (CC); orbital frontal (OF), anterior frontal (AF), superior frontal (SF), superior parietal (SP), posterior parietal (PP), temporal (Temp), and occipital (Occ).

https://doi.org/10.1371/journal.pone.0073280.g001

Download:

Table 2. Tractography Group Comparisons.

https://doi.org/10.1371/journal.pone.0073280.t002

FA.

Callosal FA analysis revealed a number of significant findings between healthy controls and Pre-HD subjects. Within the CC as a whole FA was lower in Pre-HD subjects as well as within the tracts connecting to the SP, and Occ regions. In FA comparisons between healthy controls and HD patients, reduced FA in patients was seen across the whole CC and within the tracts connecting to the OF, AF, SF, SP, and Occ regions. Finally, FA analyses between Pre-HD subjects and HD patients revealed reductions in HD patients across the whole CC and within the tracts connecting the OF, AF, SF, SP, and Occ regions.

AD.

HD patients exhibited higher AD compared to healthy controls across the whole CC and within the tracts connecting the OF, AF, SF, SP, PP, and Occ regions. The analyses between Pre-HD subjects and HD patients indicated higher AD in HD patients across the CC as a whole and within the tracts connecting the OF, AF, SP, PP and Occ regions.

RD.

RD analyses showed significant increases in Pre-HD subjects compared to healthy controls across the CC as a whole as well as within the tracts connecting the PP, and Occ regions. HD patients also showed increased RD compared to healthy controls across the CC as a whole and tracts within the OF, AF, SF, SP, PP and Occ regions. Finally, comparisons between Pre-HD subjects and HD patients showed increased RD in HD patients across the CC as a whole and within the tracts connecting the OF, AF, SF, SP, and Occ regions.

Correlations

Correlations between callosal measures, clinical scores and genetic value within Pre-HD subjects and HD patients were significant for CAG Repeat length, Disease Burden, UHDRSI, and UHDRS2. Scatterplots in Figure 2 display correlations between the whole CC FA and RD and CAG repeats, Disease Burden, UHDRSI and UHDRS2.

Download:

Figure 2. Significant Correlations between Corpus Callosum FA, RD and CAG Repeat Length, Disease Burden, UDRS1 & UDRS2.

https://doi.org/10.1371/journal.pone.0073280.g002

CAG Repeat length was negatively correlated with whole CC FA (r = –0.34, p<0.01), and Occ FA (r = –0.363, p<0.011). Positive correlations were found between the whole CC RD (r = 0.458, p<0.001) and Occ RD (r = 0.358, p<0.012).

Disease Burden was negatively correlated with FA of the whole CC (r = –0.334, p<0.02) and Occ (r = –0.319, p<0.027). Positive correlations with RD across the CC as a whole (r = 0.456, p<0.007) and the Occ (r = 0.323, p<0.025) were found.

UHDRS1 was negatively correlated with whole CC FA (r = –0.583, p<0.001), SP FA (r = –0.492, p<0.002) and Occ FA (r = –0.515, p<0.001). UHDRS1 was positively correlated with RD with the CC as a whole (r = 0.730, p<0.001) and Occ component (r = 0.559, p<0.001). UHDRS2 was positively correlated with whole CC FA (r = 0.619, p<0.001), and Occ FA (r = 0.481, p<0.001). UHDRS2 was negatively correlated with whole CC RD (r = –0.655, p<0.001) and Occ RD (r = –0.452, p<0.003).

Discussion

This study adds four main findings to the HD literature. One, greater RD in Pre-HD subjects compared to healthy controls, adds support to the hypothesis that demyelination occurs prior to disease onset in the CC revealing abnormal structural connectivity. Two, increased RD appears to occur earlier in occipital and posterior parietal tracks compared to other regions. These tracts are associated with motor and visual systems early involved in HD. Three, structural connectivity of the CC is correlated with motor and cognitive scores in patients (UHDRS1 and UHDRS2 scores), which indicates that the fibers play an important functional role. Further, this indicates that the diffusivity differences between healthy controls and patients reflect connectivity impairments both at structural and functional level. Four, increased Disease Burden and CAG repeat length is associated with altered CC microstructure suggesting a strong genetic basis for WM impairments.

Using a validated ROI approach for identifying the CC and its major sub regions [37], [38], we were able to examine highly localized changes of WM connectivity in the CC. We used FA, AD and RD to assess track structure. Significant differences were found between Pre-HD subjects and healthy controls for FA and RD. This result is similar to a recent study which used a related method [25], and found increased apparent diffusion coefficient (ADC) across the whole CC tract, though they did not find FA differences and did not examine AD/RD. Our finding of decreased FA may have to do with varying acquisition strategies or subject demographics. As axial and radial measures make up the FA value, significant RD increases but not significant AD increases indicate myelin impairment in Pre-HD stages may be the driving factor in decreased FA. Three previous studies using varying DTI methods found similar RD increases in Pre-HD subjects compared to healthy controls [23], [24], [45]. Our result of increased RD supports the previous research. Further evidence for impaired myelin in HD comes from a DTI study on a HD mouse model [46], which found thinner myelin sheaths and increased myelin periodicity.

When comparing Pre-HD subjects and HD patients, results indicate significant deterioration with disease progression characterized by both increased AD and RD across the whole CC. This suggests that the CC may be susceptible to both axonal damage and demyelination as the disease progresses. Previous studies have also revealed the negative effect HD has on the CC [21], [23], [24], [25].

However, although it is likely HD progression results in increased demyelination, we are not yet able to discern whether abnormal brain development in Pre-HD subjects contributed to their reduced myelination or whether disease progression results in demyelinated fibers. Previous work has suggested that abnormal brain development may contribute to the pathogenesis of HD as a precursor to the neurodegenerative process. Also, it may be some combination of abnormal brain development and pathogenesis that is contributing to the connectivity deficits [47]. Future longitudinal studies on Pre-HD subjects will be needed to elucidate this hypothesis.

Regional analysis of the CC revealed increases in RD in the tracts connecting parietal and occipital regions in Pre-HD subjects compared to healthy controls. It is likely the functions of the tracts are closely tied to the regions they connect with and both the motor and visual systems show early impairment in HD. For example, cortical thickness is reduced in occipital and parietal lobe regions in Pre-HD subjects [48] and cortical thickness has been shown to correlate with connectivity properties of WM tracts [29], [49]. Moreover, decreased FA was seen in the SP and Occ tracts, which, taken together support a possible posterior to anterior gradient for disease progression [23], [50], [51]. Finally, it has also been suggested [23] that metabolic dysfunction and alterations in energetics [52] seen in HD may influence the CC. Our regionally specific results of early changes in the Occ, PP, SP tracts add possible support to this hypothesis as these tracts are associated with motor and visual systems and are therefore subject to high energetic demands.

In the current study, we also found correlations between global motor & cognitive (UHDRS1 & UHDRS2) scores and CC connectivity. This relationship was observed across the CC as a whole and within specific sub regions (SP, and Occ) for FA and RD. This suggests that the CC may play an important functional role in HD symptoms. Furthermore, because diffusivity is associated with decreased motor and cognitive abilities, it supports the conclusion that WM diffusion differences between patients and healthy controls reflects abnormal structural and eventually functional connectivity between cortical regions connected by the CC. The correlations with RD indicate that decreased fiber myelination likely results in reduced global motor and cognitive scores. An earlier paper on HD patients also found a correlation between motor scores and the body of the CC using MD/RD [22] that was localized to premotor and supplementary motor cortices. The possible important role for the CC in clinical symptoms of HD is further supported by the significant relationship between cognitive measures and reductions in FA and increased RD shown by Rosas et al. [23].

However the full picture can be more complex. As CC connectivity is correlated with Disease Burden as well, which is a measure of disease severity, it is possible that connectivity deficits in the CC do not play a particularly focal role in motor and cognitive changes associated with HD. Rather, the CC may play a more general role in explaining the cognitive symptoms of HD. Importantly though, as reported previously [23], the cognitive symptoms of HD have not been adequately explained by cortico-striatal dysfunction alone. This indicates a possible district role for the CC and in general of WM in HD symptoms.

We also investigated the role CAG repeats may play in CC connectivity. We found a significant (though weak) correlation between CAG repeat length and connectivity across the CC as a whole that was driven by increased RD. This finding indicates less myelination in subjects with higher CAG repeats. However, Disease Burden showed a stronger correlation with CC connectivity, indicating that CAG repeats have an increasingly negative effect on the CC as the subject ages. This genetic basis for WM alterations was not found in two previous diffusion CC studies [22], [23], where CAG repeat length did not correlate with diffusivity measures. Again, this may have to do with the increased sensitivity of tractography to elucidate the microstructural changes in WM or varying subject demographics.

In conclusion, the CC is made up of thousands of WM fibers and we have shown, using a DTI-tractography method, a regional callosal variation in diffusivity measures between Pre-HD subjects and healthy control subjects. These structural connectivity impairments are present before a subject is clinically defined as having HD. Impairments appear to start in motor and visual tracts and proceed to encompass most of the CC in a posterior to anterior direction. And although the biological role of this connectivity change is still not fully understood [14], and caution should be used in the interpretation of diffusion findings [53], it is likely demyelination occurs early and later includes axonal damage with disease progression. Furthermore, abnormal CC structural connectivity is correlated with motor and cognitive scores (UHDRS1 & 2), suggesting an important functional role for these callosal tracts.

Supporting Information

Table S1.

Intra-rater Reliablity Coefficient.

https://doi.org/10.1371/journal.pone.0073280.s001

(DOC)

Table S2.

Tractography Data.

https://doi.org/10.1371/journal.pone.0073280.s002

(DOC)

Author Contributions

Conceived and designed the experiments: MD OP US. Performed the experiments: MD OP CSC FE VM ADP CC FS. Analyzed the data: OP MD. Wrote the paper: OP MD.

References

1. Macdonald ME, Ambrose CM, Duyao MP, Myers RH, Lin C, et al. (1993) A Novel Gene Containing a Trinucleotide Repeat That Is Expanded and Unstable on Huntingtons-Disease Chromosomes. Cell 72: 971–983.
- View Article
- Google Scholar
2. Persichetti F, Carlee L, Faber PW, McNeil SM, Ambrose CM, et al. (1996) Differential expression of normal and mutant Huntington’s disease gene alleles. Neurobiol Dis 3: 183–190.
- View Article
- Google Scholar
3. Esmaeilzadeh M, Ciarmiello A, Squitieri F (2011) Seeking brain biomarkers for preventive therapy in Huntington disease. CNS Neurosci Ther 17: 368–386.
- View Article
- Google Scholar
4. Duff K, Beglinger LJ, Paulsen JS (2008) “Pre-symptomatic” Huntington’s disease. Handb Clin Neurol 89: 589–598.
- View Article
- Google Scholar
5. Tabrizi SJ, Langbehn DR, Leavitt BR, Roos RA, Durr A, et al. (2009) Biological and clinical manifestations of Huntington’s disease in the longitudinal TRACK-HD study: cross-sectional analysis of baseline data. Lancet Neurol 8: 791–801.
- View Article
- Google Scholar
6. Bartzokis G, Lu PH, Tishler TA, Fong SM, Oluwadara B, et al. (2007) Myelin breakdown and iron changes in Huntington’s disease: pathogenesis and treatment implications. Neurochem Res 32: 1655–1664.
- View Article
- Google Scholar
7. Sach M, Winkler G, Glauche V, Liepert J, Heimbach B, et al. (2004) Diffusion tensor MRI of early upper motor neuron involvement in amyotrophic lateral sclerosis. Brain 127: 340–350.
- View Article
- Google Scholar
8. Aboitiz F, Scheibel AB, Fisher RS, Zaidel E (1992) Fiber composition of the human corpus callosum. Brain Res 598: 143–153.
- View Article
- Google Scholar
9. Aboitiz F, Montiel J (2003) One hundred million years of interhemispheric communication: the history of the corpus callosum. Braz J Med Biol Res 36: 409–420.
- View Article
- Google Scholar
10. Luders E, Di Paola M, Tomaiuolo F, Thompson PM, Toga AW, et al. (2007) Callosal morphology in Williams syndrome: a new evaluation of shape and thickness. Neuroreport 18: 203–207.
- View Article
- Google Scholar
11. Di Paola M, Luders E, Di Iulio F, Cherubini A, Passafiume D, et al. (2010) Callosal atrophy in mild cognitive impairment and Alzheimer’s disease: different effects in different stages. Neuroimage 49: 141–149.
- View Article
- Google Scholar
12. Tomaiuolo F, Carlesimo GA, Di Paola M, Petrides M, Fera F, et al. (2004) Gross morphology and morphometric sequelae in the hippocampus, fornix, and corpus callosum of patients with severe non-missile traumatic brain injury without macroscopically detectable lesions: a T1 weighted MRI study. J Neurol Neurosurg Psychiatry 75: 1314–1322.
- View Article
- Google Scholar
13. Pierpaoli C, Barnett A, Pajevic S, Chen R, Penix LR, et al. (2001) Water diffusion changes in Wallerian degeneration and their dependence on white matter architecture. Neuroimage 13: 1174–1185.
- View Article
- Google Scholar
14. Jones DK, Knosche TR, Turner R (2012) White matter integrity, fiber count, and other fallacies: The do’s and don’ts of diffusion MRI. Neuroimage.
15. Konrad A, Winterer G (2008) Disturbed structural connectivity in schizophrenia primary factor in pathology or epiphenomenon? Schizophr Bull 34: 72–92.
- View Article
- Google Scholar
16. Takahashi M, Ono J, Harada K, Maeda M, Hackney DB (2000) Diffusional anisotropy in cranial nerves with maturation: quantitative evaluation with diffusion MR imaging in rats. Radiology 216: 881–885.
- View Article
- Google Scholar
17. Hasan KM, Sankar A, Halphen C, Kramer LA, Brandt ME, et al. (2007) Development and organization of the human brain tissue compartments across the lifespan using diffusion tensor imaging. Neuroreport 18: 1735–1739.
- View Article
- Google Scholar
18. Concha L, Gross DW, Wheatley BM, Beaulieu C (2006) Diffusion tensor imaging of time-dependent axonal and myelin degradation after corpus callosotomy in epilepsy patients. Neuroimage 32: 1090–1099.
- View Article
- Google Scholar
19. Song SK, Sun SW, Ramsbottom MJ, Chang C, Russell J, et al. (2002) Dysmyelination revealed through MRI as increased radial (but unchanged axial) diffusion of water. Neuroimage 17: 1429–1436.
- View Article
- Google Scholar
20. Schmierer K, Wheeler-Kingshott CA, Tozer DJ, Boulby PA, Parkes HG, et al. (2008) Quantitative magnetic resonance of postmortem multiple sclerosis brain before and after fixation. Magn Reson Med 59: 268–277.
- View Article
- Google Scholar
21. Muller HP, Glauche V, Novak MJ, Nguyen-Thanh T, Unrath A, et al. (2011) Stability of white matter changes related to Huntington’s disease in the presence of imaging noise: a DTI study. PLoS Curr 3: RRN1232.
- View Article
- Google Scholar
22. Bohanna I, Georgiou-Karistianis N, Sritharan A, Asadi H, Johnston L, et al. (2011) Diffusion tensor imaging in Huntington’s disease reveals distinct patterns of white matter degeneration associated with motor and cognitive deficits. Brain Imaging Behav 5: 171–180.
- View Article
- Google Scholar
23. Rosas HD, Lee SY, Bender AC, Zaleta AK, Vangel M, et al. (2010) Altered white matter microstructure in the corpus callosum in Huntington’s disease: implications for cortical “disconnection”. Neuroimage 49: 2995–3004.
- View Article
- Google Scholar
24. Di Paola M, Luders E, Cherubini A, Sanchez-Castaneda C, Thompson PM, et al.. (2012) Multimodal MRI Analysis of the Corpus Callosum Reveals White Matter Differences in Presymptomatic and Early Huntington’s Disease. Cereb Cortex.
25. Dumas EM, van den Bogaard SJ, Ruber ME, Reilman RR, Stout JC, et al. (2012) Early changes in white matter pathways of the sensorimotor cortex in premanifest Huntington’s disease. Hum Brain Mapp 33: 203–212.
- View Article
- Google Scholar
26. Alexander DC, Pierpaoli C, Basser PJ, Gee JC (2001) Spatial transformations of diffusion tensor magnetic resonance images. IEEE Trans Med Imaging 20: 1131–1139.
- View Article
- Google Scholar
27. Phillips OR, Nuechterlein KH, Clark KA, Hamilton LS, Asarnow RF, et al. (2009) Fiber tractography reveals disruption of temporal lobe white matter tracts in schizophrenia. Schizophr Res 107: 30–38.
- View Article
- Google Scholar
28. Wakana S, Caprihan A, Panzenboeck MM, Fallon JH, Perry M, et al. (2007) Reproducibility of quantitative tractography methods applied to cerebral white matter. Neuroimage 36: 630–644.
- View Article
- Google Scholar
29. Phillips OR, Clark KA, Woods RP, Subotnik KL, Asarnow RF, et al. (2011) Topographical relationships between arcuate fasciculus connectivity and cortical thickness. Hum Brain Mapp 32: 1788–1801.
- View Article
- Google Scholar
30. Weinstein M, Ben-Sira L, Levy Y, Zachor DA, Ben Itzhak E, et al. (2011) Abnormal white matter integrity in young children with autism. Hum Brain Mapp 32: 534–543.
- View Article
- Google Scholar
31. Conturo TE, Lori NF, Cull TS, Akbudak E, Snyder AZ, et al. (1999) Tracking neuronal fiber pathways in the living human brain. Proc Natl Acad Sci U S A 96: 10422–10427.
- View Article
- Google Scholar
32. Ashburner J, Friston KJ (2000) Voxel-based morphometry–the methods. Neuroimage 11: 805–821.
- View Article
- Google Scholar
33. Catani M, Howard RJ, Pajevic S, Jones DK (2002) Virtual in vivo interactive dissection of white matter fasciculi in the human brain. Neuroimage 17: 77–94.
- View Article
- Google Scholar
34. Wakana S, Jiang H, Nagae-Poetscher LM, van Zijl PC, Mori S (2004) Fiber tract-based atlas of human white matter anatomy. Radiology 230: 77–87.
- View Article
- Google Scholar
35. Catani M, Jones DK, Donato R, Ffytche DH (2003) Occipito-temporal connections in the human brain. Brain 126: 2093–2107.
- View Article
- Google Scholar
36. Jellison BJ, Field AS, Medow J, Lazar M, Salamat MS, et al. (2004) Diffusion tensor imaging of cerebral white matter: a pictorial review of physics, fiber tract anatomy, and tumor imaging patterns. AJNR Am J Neuroradiol 25: 356–369.
- View Article
- Google Scholar
37. Lebel C, Caverhill-Godkewitsch S, Beaulieu C (2010) Age-related regional variations of the corpus callosum identified by diffusion tensor tractography. Neuroimage 52: 20–31.
- View Article
- Google Scholar
38. Huang H, Zhang J, Jiang H, Wakana S, Poetscher L, et al. (2005) DTI tractography based parcellation of white matter: application to the mid-sagittal morphology of corpus callosum. Neuroimage 26: 195–205.
- View Article
- Google Scholar
39. Huntington Study Group (1996) Unified Huntington’s Disease Rating Scale: reliability and consistency. Mov Disord 11: 136–142.
- View Article
- Google Scholar
40. Penney JB, Vonsattel JP, MacDonald ME, Gusella JF, Myers RH (1997) CAG repeat number governs the development rate of pathology in Huntington’s disease. Ann Neurol 41: 689–692.
- View Article
- Google Scholar
41. Folstein MF, Folstein SE, McHugh PR (1975) “Mini-mental state”. A practical method for grading the cognitive state of patients for the clinician. J Psychiatr Res 12: 189–198.
- View Article
- Google Scholar
42. Deichmann R, Schwarzbauer C, Turner R (2004) Optimisation of the 3D MDEFT sequence for anatomical brain imaging: technical implications at 1.5 and 3 T. Neuroimage 21: 757–767.
- View Article
- Google Scholar
43. Smith SM (2002) Fast robust automated brain extraction. Hum Brain Mapp 17: 143–155.
- View Article
- Google Scholar
44. Wedeen VJ, Wang RP, Schmahmann JD, Benner T, Tseng WY, et al. (2008) Diffusion spectrum magnetic resonance imaging (DSI) tractography of crossing fibers. Neuroimage 41: 1267–1277.
- View Article
- Google Scholar
45. Stoffers D, Sheldon S, Kuperman JM, Goldstein J, Corey-Bloom J, et al. (2010) Contrasting gray and white matter changes in preclinical Huntington disease: an MRI study. Neurology 74: 1208–1216.
- View Article
- Google Scholar
46. Xiang Z, Valenza M, Cui L, Leoni V, Jeong HK, et al. (2011) Peroxisome-proliferator-activated receptor gamma coactivator 1 alpha contributes to dysmyelination in experimental models of Huntington’s disease. J Neurosci 31: 9544–9553.
- View Article
- Google Scholar
47. Nopoulos PC, Aylward EH, Ross CA, Mills JA, Langbehn DR, et al. (2011) Smaller intracranial volume in prodromal Huntington’s disease: evidence for abnormal neurodevelopment. Brain 134: 137–142.
- View Article
- Google Scholar
48. Rosas HD, Salat DH, Lee SY, Zaleta AK, Pappu V, et al. (2008) Cerebral cortex and the clinical expression of Huntington’s disease: complexity and heterogeneity. Brain 131: 1057–1068.
- View Article
- Google Scholar
49. Kochunov P, Glahn DC, Lancaster J, Thompson PM, Kochunov V, et al. (2011) Fractional anisotropy of cerebral white matter and thickness of cortical gray matter across the lifespan. Neuroimage 58: 41–49.
- View Article
- Google Scholar
50. Rosas HD, Koroshetz WJ, Chen YI, Skeuse C, Vangel M, et al. (2003) Evidence for more widespread cerebral pathology in early HD: an MRI-based morphometric analysis. Neurology 60: 1615–1620.
- View Article
- Google Scholar
51. Rosas HD, Hevelone ND, Zaleta AK, Greve DN, Salat DH, et al. (2005) Regional cortical thinning in preclinical Huntington disease and its relationship to cognition. Neurology 65: 745–747.
- View Article
- Google Scholar
52. Browne SE (2008) Mitochondria and Huntington’s disease pathogenesis: insight from genetic and chemical models. Ann N Y Acad Sci 1147: 358–382.
- View Article
- Google Scholar
53. Wheeler-Kingshott CA, Cercignani M (2009) About “axial” and “radial” diffusivities. Magn Reson Med 61: 1255–1260.
- View Article
- Google Scholar

[ref1] 1. Macdonald ME, Ambrose CM, Duyao MP, Myers RH, Lin C, et al. (1993) A Novel Gene Containing a Trinucleotide Repeat That Is Expanded and Unstable on Huntingtons-Disease Chromosomes. Cell 72: 971–983.
View Article
Google Scholar

[2] View Article

[3] Google Scholar

[ref2] 2. Persichetti F, Carlee L, Faber PW, McNeil SM, Ambrose CM, et al. (1996) Differential expression of normal and mutant Huntington’s disease gene alleles. Neurobiol Dis 3: 183–190.
View Article
Google Scholar

[5] View Article

[6] Google Scholar

[ref3] 3. Esmaeilzadeh M, Ciarmiello A, Squitieri F (2011) Seeking brain biomarkers for preventive therapy in Huntington disease. CNS Neurosci Ther 17: 368–386.
View Article
Google Scholar

[8] View Article

[9] Google Scholar

[ref4] 4. Duff K, Beglinger LJ, Paulsen JS (2008) “Pre-symptomatic” Huntington’s disease. Handb Clin Neurol 89: 589–598.
View Article
Google Scholar

[11] View Article

[12] Google Scholar

[ref5] 5. Tabrizi SJ, Langbehn DR, Leavitt BR, Roos RA, Durr A, et al. (2009) Biological and clinical manifestations of Huntington’s disease in the longitudinal TRACK-HD study: cross-sectional analysis of baseline data. Lancet Neurol 8: 791–801.
View Article
Google Scholar

[14] View Article

[15] Google Scholar

[ref6] 6. Bartzokis G, Lu PH, Tishler TA, Fong SM, Oluwadara B, et al. (2007) Myelin breakdown and iron changes in Huntington’s disease: pathogenesis and treatment implications. Neurochem Res 32: 1655–1664.
View Article
Google Scholar

[17] View Article

[18] Google Scholar

[ref7] 7. Sach M, Winkler G, Glauche V, Liepert J, Heimbach B, et al. (2004) Diffusion tensor MRI of early upper motor neuron involvement in amyotrophic lateral sclerosis. Brain 127: 340–350.
View Article
Google Scholar

[20] View Article

[21] Google Scholar

[ref8] 8. Aboitiz F, Scheibel AB, Fisher RS, Zaidel E (1992) Fiber composition of the human corpus callosum. Brain Res 598: 143–153.
View Article
Google Scholar

[23] View Article

[24] Google Scholar

[ref9] 9. Aboitiz F, Montiel J (2003) One hundred million years of interhemispheric communication: the history of the corpus callosum. Braz J Med Biol Res 36: 409–420.
View Article
Google Scholar

[26] View Article

[27] Google Scholar

[ref10] 10. Luders E, Di Paola M, Tomaiuolo F, Thompson PM, Toga AW, et al. (2007) Callosal morphology in Williams syndrome: a new evaluation of shape and thickness. Neuroreport 18: 203–207.
View Article
Google Scholar

[29] View Article

[30] Google Scholar

[ref11] 11. Di Paola M, Luders E, Di Iulio F, Cherubini A, Passafiume D, et al. (2010) Callosal atrophy in mild cognitive impairment and Alzheimer’s disease: different effects in different stages. Neuroimage 49: 141–149.
View Article
Google Scholar

[32] View Article

[33] Google Scholar

[ref12] 12. Tomaiuolo F, Carlesimo GA, Di Paola M, Petrides M, Fera F, et al. (2004) Gross morphology and morphometric sequelae in the hippocampus, fornix, and corpus callosum of patients with severe non-missile traumatic brain injury without macroscopically detectable lesions: a T1 weighted MRI study. J Neurol Neurosurg Psychiatry 75: 1314–1322.
View Article
Google Scholar

[35] View Article

[36] Google Scholar

[ref13] 13. Pierpaoli C, Barnett A, Pajevic S, Chen R, Penix LR, et al. (2001) Water diffusion changes in Wallerian degeneration and their dependence on white matter architecture. Neuroimage 13: 1174–1185.
View Article
Google Scholar

[38] View Article

[39] Google Scholar

[ref14] 14. Jones DK, Knosche TR, Turner R (2012) White matter integrity, fiber count, and other fallacies: The do’s and don’ts of diffusion MRI. Neuroimage.

[ref15] 15. Konrad A, Winterer G (2008) Disturbed structural connectivity in schizophrenia primary factor in pathology or epiphenomenon? Schizophr Bull 34: 72–92.
View Article
Google Scholar

[42] View Article

[43] Google Scholar

[ref16] 16. Takahashi M, Ono J, Harada K, Maeda M, Hackney DB (2000) Diffusional anisotropy in cranial nerves with maturation: quantitative evaluation with diffusion MR imaging in rats. Radiology 216: 881–885.
View Article
Google Scholar

[45] View Article

[46] Google Scholar

[ref17] 17. Hasan KM, Sankar A, Halphen C, Kramer LA, Brandt ME, et al. (2007) Development and organization of the human brain tissue compartments across the lifespan using diffusion tensor imaging. Neuroreport 18: 1735–1739.
View Article
Google Scholar

[48] View Article

[49] Google Scholar

[ref18] 18. Concha L, Gross DW, Wheatley BM, Beaulieu C (2006) Diffusion tensor imaging of time-dependent axonal and myelin degradation after corpus callosotomy in epilepsy patients. Neuroimage 32: 1090–1099.
View Article
Google Scholar

[51] View Article

[52] Google Scholar

[ref19] 19. Song SK, Sun SW, Ramsbottom MJ, Chang C, Russell J, et al. (2002) Dysmyelination revealed through MRI as increased radial (but unchanged axial) diffusion of water. Neuroimage 17: 1429–1436.
View Article
Google Scholar

[54] View Article

[55] Google Scholar

[ref20] 20. Schmierer K, Wheeler-Kingshott CA, Tozer DJ, Boulby PA, Parkes HG, et al. (2008) Quantitative magnetic resonance of postmortem multiple sclerosis brain before and after fixation. Magn Reson Med 59: 268–277.
View Article
Google Scholar

[57] View Article

[58] Google Scholar

[ref21] 21. Muller HP, Glauche V, Novak MJ, Nguyen-Thanh T, Unrath A, et al. (2011) Stability of white matter changes related to Huntington’s disease in the presence of imaging noise: a DTI study. PLoS Curr 3: RRN1232.
View Article
Google Scholar

[60] View Article

[61] Google Scholar

[ref22] 22. Bohanna I, Georgiou-Karistianis N, Sritharan A, Asadi H, Johnston L, et al. (2011) Diffusion tensor imaging in Huntington’s disease reveals distinct patterns of white matter degeneration associated with motor and cognitive deficits. Brain Imaging Behav 5: 171–180.
View Article
Google Scholar

[63] View Article

[64] Google Scholar

[ref23] 23. Rosas HD, Lee SY, Bender AC, Zaleta AK, Vangel M, et al. (2010) Altered white matter microstructure in the corpus callosum in Huntington’s disease: implications for cortical “disconnection”. Neuroimage 49: 2995–3004.
View Article
Google Scholar

[66] View Article

[67] Google Scholar

[ref24] 24. Di Paola M, Luders E, Cherubini A, Sanchez-Castaneda C, Thompson PM, et al.. (2012) Multimodal MRI Analysis of the Corpus Callosum Reveals White Matter Differences in Presymptomatic and Early Huntington’s Disease. Cereb Cortex.

[ref25] 25. Dumas EM, van den Bogaard SJ, Ruber ME, Reilman RR, Stout JC, et al. (2012) Early changes in white matter pathways of the sensorimotor cortex in premanifest Huntington’s disease. Hum Brain Mapp 33: 203–212.
View Article
Google Scholar

[70] View Article

[71] Google Scholar

[ref26] 26. Alexander DC, Pierpaoli C, Basser PJ, Gee JC (2001) Spatial transformations of diffusion tensor magnetic resonance images. IEEE Trans Med Imaging 20: 1131–1139.
View Article
Google Scholar

[73] View Article

[74] Google Scholar

[ref27] 27. Phillips OR, Nuechterlein KH, Clark KA, Hamilton LS, Asarnow RF, et al. (2009) Fiber tractography reveals disruption of temporal lobe white matter tracts in schizophrenia. Schizophr Res 107: 30–38.
View Article
Google Scholar

[76] View Article

[77] Google Scholar

[ref28] 28. Wakana S, Caprihan A, Panzenboeck MM, Fallon JH, Perry M, et al. (2007) Reproducibility of quantitative tractography methods applied to cerebral white matter. Neuroimage 36: 630–644.
View Article
Google Scholar

[79] View Article

[80] Google Scholar

[ref29] 29. Phillips OR, Clark KA, Woods RP, Subotnik KL, Asarnow RF, et al. (2011) Topographical relationships between arcuate fasciculus connectivity and cortical thickness. Hum Brain Mapp 32: 1788–1801.
View Article
Google Scholar

[82] View Article

[83] Google Scholar

[ref30] 30. Weinstein M, Ben-Sira L, Levy Y, Zachor DA, Ben Itzhak E, et al. (2011) Abnormal white matter integrity in young children with autism. Hum Brain Mapp 32: 534–543.
View Article
Google Scholar

[85] View Article

[86] Google Scholar

[ref31] 31. Conturo TE, Lori NF, Cull TS, Akbudak E, Snyder AZ, et al. (1999) Tracking neuronal fiber pathways in the living human brain. Proc Natl Acad Sci U S A 96: 10422–10427.
View Article
Google Scholar

[88] View Article

[89] Google Scholar

[ref32] 32. Ashburner J, Friston KJ (2000) Voxel-based morphometry–the methods. Neuroimage 11: 805–821.
View Article
Google Scholar

[91] View Article

[92] Google Scholar

[ref33] 33. Catani M, Howard RJ, Pajevic S, Jones DK (2002) Virtual in vivo interactive dissection of white matter fasciculi in the human brain. Neuroimage 17: 77–94.
View Article
Google Scholar

[94] View Article

[95] Google Scholar

[ref34] 34. Wakana S, Jiang H, Nagae-Poetscher LM, van Zijl PC, Mori S (2004) Fiber tract-based atlas of human white matter anatomy. Radiology 230: 77–87.
View Article
Google Scholar

[97] View Article

[98] Google Scholar

[ref35] 35. Catani M, Jones DK, Donato R, Ffytche DH (2003) Occipito-temporal connections in the human brain. Brain 126: 2093–2107.
View Article
Google Scholar

[100] View Article

[101] Google Scholar

[ref36] 36. Jellison BJ, Field AS, Medow J, Lazar M, Salamat MS, et al. (2004) Diffusion tensor imaging of cerebral white matter: a pictorial review of physics, fiber tract anatomy, and tumor imaging patterns. AJNR Am J Neuroradiol 25: 356–369.
View Article
Google Scholar

[103] View Article

[104] Google Scholar

[ref37] 37. Lebel C, Caverhill-Godkewitsch S, Beaulieu C (2010) Age-related regional variations of the corpus callosum identified by diffusion tensor tractography. Neuroimage 52: 20–31.
View Article
Google Scholar

[106] View Article

[107] Google Scholar

[ref38] 38. Huang H, Zhang J, Jiang H, Wakana S, Poetscher L, et al. (2005) DTI tractography based parcellation of white matter: application to the mid-sagittal morphology of corpus callosum. Neuroimage 26: 195–205.
View Article
Google Scholar

[109] View Article

[110] Google Scholar

[ref39] 39. Huntington Study Group (1996) Unified Huntington’s Disease Rating Scale: reliability and consistency. Mov Disord 11: 136–142.
View Article
Google Scholar

[112] View Article

[113] Google Scholar

[ref40] 40. Penney JB, Vonsattel JP, MacDonald ME, Gusella JF, Myers RH (1997) CAG repeat number governs the development rate of pathology in Huntington’s disease. Ann Neurol 41: 689–692.
View Article
Google Scholar

[115] View Article

[116] Google Scholar

[ref41] 41. Folstein MF, Folstein SE, McHugh PR (1975) “Mini-mental state”. A practical method for grading the cognitive state of patients for the clinician. J Psychiatr Res 12: 189–198.
View Article
Google Scholar

[118] View Article

[119] Google Scholar

[ref42] 42. Deichmann R, Schwarzbauer C, Turner R (2004) Optimisation of the 3D MDEFT sequence for anatomical brain imaging: technical implications at 1.5 and 3 T. Neuroimage 21: 757–767.
View Article
Google Scholar

[121] View Article

[122] Google Scholar

[ref43] 43. Smith SM (2002) Fast robust automated brain extraction. Hum Brain Mapp 17: 143–155.
View Article
Google Scholar

[124] View Article

[125] Google Scholar

[ref44] 44. Wedeen VJ, Wang RP, Schmahmann JD, Benner T, Tseng WY, et al. (2008) Diffusion spectrum magnetic resonance imaging (DSI) tractography of crossing fibers. Neuroimage 41: 1267–1277.
View Article
Google Scholar

[127] View Article

[128] Google Scholar

[ref45] 45. Stoffers D, Sheldon S, Kuperman JM, Goldstein J, Corey-Bloom J, et al. (2010) Contrasting gray and white matter changes in preclinical Huntington disease: an MRI study. Neurology 74: 1208–1216.
View Article
Google Scholar

[130] View Article

[131] Google Scholar

[ref46] 46. Xiang Z, Valenza M, Cui L, Leoni V, Jeong HK, et al. (2011) Peroxisome-proliferator-activated receptor gamma coactivator 1 alpha contributes to dysmyelination in experimental models of Huntington’s disease. J Neurosci 31: 9544–9553.
View Article
Google Scholar

[133] View Article

[134] Google Scholar

[ref47] 47. Nopoulos PC, Aylward EH, Ross CA, Mills JA, Langbehn DR, et al. (2011) Smaller intracranial volume in prodromal Huntington’s disease: evidence for abnormal neurodevelopment. Brain 134: 137–142.
View Article
Google Scholar

[136] View Article

[137] Google Scholar

[ref48] 48. Rosas HD, Salat DH, Lee SY, Zaleta AK, Pappu V, et al. (2008) Cerebral cortex and the clinical expression of Huntington’s disease: complexity and heterogeneity. Brain 131: 1057–1068.
View Article
Google Scholar

[139] View Article

[140] Google Scholar

[ref49] 49. Kochunov P, Glahn DC, Lancaster J, Thompson PM, Kochunov V, et al. (2011) Fractional anisotropy of cerebral white matter and thickness of cortical gray matter across the lifespan. Neuroimage 58: 41–49.
View Article
Google Scholar

[142] View Article

[143] Google Scholar

[ref50] 50. Rosas HD, Koroshetz WJ, Chen YI, Skeuse C, Vangel M, et al. (2003) Evidence for more widespread cerebral pathology in early HD: an MRI-based morphometric analysis. Neurology 60: 1615–1620.
View Article
Google Scholar

[145] View Article

[146] Google Scholar

[ref51] 51. Rosas HD, Hevelone ND, Zaleta AK, Greve DN, Salat DH, et al. (2005) Regional cortical thinning in preclinical Huntington disease and its relationship to cognition. Neurology 65: 745–747.
View Article
Google Scholar

[148] View Article

[149] Google Scholar

[ref52] 52. Browne SE (2008) Mitochondria and Huntington’s disease pathogenesis: insight from genetic and chemical models. Ann N Y Acad Sci 1147: 358–382.
View Article
Google Scholar

[151] View Article

[152] Google Scholar

[ref53] 53. Wheeler-Kingshott CA, Cercignani M (2009) About “axial” and “radial” diffusivities. Magn Reson Med 61: 1255–1260.
View Article
Google Scholar

[154] View Article

[155] Google Scholar

Figures

Abstract

Introduction

Materials and Methods

Ethics Statement

Subjects

MRI Data Acquisition

DTI Processing

Tractography

Statistical Analysis

Results

Subject Demographic

Tractography Data

FA.

AD.

RD.

Correlations

Discussion

Supporting Information

Table S1.

Table S2.

Author Contributions

References