Diffusion Tensor Imaging of the Spinal Cord: Insights From Animal and Human Studies

Diffusion tensor imaging (DTI) provides a measure of the directional diffusion of water molecules in tissues. The measurement of DTI indexes within the spinal cord provides a quantitative assessment of neural damage in various spinal cord pathologies. DTI studies in animal models of spinal cord injury indicate that DTI is a reliable imaging technique with important histological and functional correlates. These studies demonstrate that DTI is a noninvasive marker of microstructural change within the spinal cord. In human studies, spinal cord DTI shows definite changes in subjects with acute and chronic spinal cord injury, as well as cervical spondylotic myelopathy. Interestingly, changes in DTI indexes are visualized in regions of the cord, which appear normal on conventional magnetic resonance imaging and are remote from the site of cord compression. Spinal cord DTI provides data that can help us understand underlying microstructural changes within the cord and assist in prognostication and planning of therapies. In this article, we review the use of DTI to investigate spinal cord pathology in animals and humans and describe advances in this technique that establish DTI as a promising biomarker for spinal cord disorders

Characterization and Limitations of Diffusion Tensor Imaging Metrics in the Cervical Spinal Cord in Neurologically Intact Subjects

Purpose To characterize diffusion tensor imaging (DTI) metrics across all levels of the cervical spinal cord (CSC) and to study the impact of age and signal quality on these metrics. Materials and Methods DTI metrics were calculated for gray matter (GM) and white matter (WM) funiculi throughout the CSC (C1–T1) in 25 healthy subjects (22-85 years old). Signal-to-noise ratios (SNRs) and mean DTI metrics were measured for the upper (C1-3), middle (C4-6) and lower (C7-T1) cervical segments. Age-related changes in DTI metrics were analyzed for the individual segment groups. Results Fractional anisotropy (FA), mean diffusivity (MD) and transverse apparent diffusion coefficient (tADC) showed significant differences between GM and WM funiculi. Significant age-related changes were observed in FA in upper and middle CSC segments but not in the lower CSC. The median SNR was significantly lower in the middle and lower segment groups as compared to the upper levels, contributing to poor spatial resolution in these regions. Conclusion This study provides DTI data for GM and WM funiculi throughout the CSC. While DTI metrics may be used to define cord pathology, variations in metrics due to age and signal quality need to be accounted for before making definitive conclusions. J. Magn. Reson

Open-access quantitative MRI data of the spinal cord and reproducibility across participants, sites and manufacturers

Databases; Imaging techniques; Spinal cord diseasesBases de datos; Tècnicas de imagen; Enfermedades de la médula espinalBases de dades; Tècniques d'imatge; Malalties de la medul·la espinalIn a companion paper by Cohen-Adad et al. we introduce the spine generic quantitative MRI protocol that provides valuable metrics for assessing spinal cord macrostructural and microstructural integrity. This protocol was used to acquire a single subject dataset across 19 centers and a multi-subject dataset across 42 centers (for a total of 260 participants), spanning the three main MRI manufacturers: GE, Philips and Siemens. Both datasets are publicly available via git-annex. Data were analysed using the Spinal Cord Toolbox to produce normative values as well as inter/intra-site and inter/intra-manufacturer statistics. Reproducibility for the spine generic protocol was high across sites and manufacturers, with an average inter-site coefficient of variation of less than 5% for all the metrics. Full documentation and results can be found at https://spine-generic.rtfd.io/. The datasets and analysis pipeline will help pave the way towards accessible and reproducible quantitative MRI in the spinal cord

Open-access quantitative MRI data of the spinal cord and reproducibility across participants, sites and manufacturers

In a companion paper by Cohen-Adad et al. we introduce the spine generic quantitative MRI protocol that provides valuable metrics for assessing spinal cord macrostructural and microstructural integrity. This protocol was used to acquire a single subject dataset across 19 centers and a multi-subject dataset across 42 centers (for a total of 260 participants), spanning the three main MRI manufacturers: GE, Philips and Siemens. Both datasets are publicly available via git-annex. Data were analysed using the Spinal Cord Toolbox to produce normative values as well as inter/intra-site and inter/intra-manufacturer statistics. Reproducibility for the spine generic protocol was high across sites and manufacturers, with an average inter-site coefficient of variation of less than 5% for all the metrics. Full documentation and results can be found at https://spine-generic.rtfd.io/. The datasets and analysis pipeline will help pave the way towards accessible and reproducible quantitative MRI in the spinal cord

Age related changes in metabolite concentrations in the normal spinal cord.

Magnetic resonance spectroscopy (MRS) studies have previously described metabolite changes associated with aging of the healthy brain and provided insights into normal brain aging that can assist us in differentiating age-related changes from those associated with neurological disease. The present study investigates whether age-related changes in metabolite concentrations occur in the healthy cervical spinal cord. 25 healthy volunteers, aged 23-65 years, underwent conventional imaging and single-voxel MRS of the upper cervical cord using an optimised point resolved spectroscopy sequence on a 3T Achieva system. Metabolite concentrations normalised to unsuppressed water were quantified using LCModel and associations between age and spinal cord metabolite concentrations were examined using multiple regressions. A linear decline in total N-Acetyl-aspartate concentration (0.049 mmol/L lower per additional year of age, p = 0.010) and Glutamate-Glutamine concentration (0.054 mmol/L lower per additional year of age, p = 0.002) was seen within our sample age range, starting in the early twenties. The findings suggest that neuroaxonal loss and/or metabolic neuronal dysfunction, and decline in glutamate-glutamine neurotransmitter pool progress with aging

White-matter abnormalities in brain during early abstinence from methamphetamine abuse

Previous studies revealed microstructural abnormalities in prefrontal white matter and corpus callosum of long-term abstinent chronic methamphetamine abusers. In view of the importance of the early abstinence period in treatment retention, we compared 23 methamphetamine-dependent subjects abstinent from methamphetamine for 7–13 days with 18 healthy comparison subjects. As certain metabolic changes in the brain first manifest after early abstinence from methamphetamine, it is also possible that microstructural white-matter abnormalities are not yet present during early abstinence. Using diffusion tensor imaging at 1.5 T, fractional anisotropy (FA) was measured in prefrontal white matter at four inferior–superior levels parallel to the anterior commissure–posterior commissure (AC–PC) plane. We also sampled FA in the corpus callosum at the midline and at eight bilateral, fiber-tract sites in other regions implicated in effects of methamphetamine. The methamphetamine group exhibited lower FA in right prefrontal white matter above the AC–PC plane (11.9% lower; p = 0.007), in midline genu corpus callosum (3.9%; p = 0.019), in left and right midcaudal superior corona radiata (11.0% in both hemispheres, p’s = 0.020 and 0.016, respectively), and in right perforant fibers (7.3%; p = 0.025). FA in left midcaudal superior corona radiata was correlated with depressive and generalized psychiatric symptoms within the methamphetamine group. The findings support the idea that methamphetamine abuse produces microstructural abnormalities in white matter underlying and interconnecting prefrontal cortices and hippocampal formation. These effects are already present during the first weeks of abstinence from methamphetamine and are linked to psychiatric symptoms assessed during this period

Cervical weakness and preterm birth: The structure and function of the internal cervical os

The cervix is integral to the maintenance of pregnancy and timely delivery of the baby. Mechanical failure of the cervix resulting in spontaneous preterm birth presents with collapse of the internal os, yet little is known about why the cervix behaves in this way. This may in part be due to research being technically limited and/or limited to punch biopsies of the distal cervix that did not include tissue from the internal os. The aim of this thesis was to re-evaluate cervical anatomy using novel laboratory and imaging methods to gain further insight into the structure of the cervix and how this may influence function during pregnancy. To achieve this, whole cervical samples were obtained from women undergoing hysterectomy for benign pathology. Uterine tissue was subsequently fixed and analysed using 2D and 3D histological methods. Cervical anatomy was characterised using markers for smooth muscle and collagen and analysed using computer-assisted quantification methods. Sequential tissue slices were then reconstructed to produce 3D models of the proximal, middle and distal cervix. High-resolution diffusion-tensor imaging was used to determine whether complex cervical anatomy could be visualised using radiological methods. Tissue was assessed using quantitative and qualitative diffusion methods, and directly compared to immunohistochemically stained tissue. The results obtained demonstrated that diffusion-tensor imaging accurately assessed cervical anatomy and provided further detail in terms of fibre volume, density and organisation. Ex vivo endoscopic ultrasound was used to assess whether current, established medical imaging technology could discern cervical smooth muscle and collagen fibres. Although this method could be used to identify gross anatomical structures, it was not an appropriate method to identify cervical microanatomy. The results described in this thesis provide further insight into how the cervix resists intrauterine forces throughout pregnancy, and then dilates and effaces to allow for delivery of a fetus. Diffusion-tensor imaging accurately assessed cervical anatomy, which may have implications for in vivo characterisation of cervical remodelling during pregnancy and identifying those at risk of delivering early. Finally, observations in this thesis encourage continued re-examination of the cervix using high-resolution imaging to provide insight into function and to develop strategies to discern cervical insufficiency from other known causes of preterm birth

Development of an MRI Template and Analysis Pipeline for the Spinal Cord and Application in Patients with Spinal Cord Injury

La moelle épinière est un organe fondamental du corps humain. Étant le lien entre le cerveau et le système nerveux périphérique, endommager la moelle épinière, que ce soit suite à un trauma ou une maladie neurodégénérative, a des conséquences graves sur la qualité de vie des patients. En effet, les maladies et traumatismes touchant la moelle épinière peuvent affecter l’intégrité des neurones et provoquer des troubles neurologiques et/ou des handicaps fonctionnels. Bien que de nombreuses voies thérapeutiques pour traiter les lésions de la moelle épinière existent, la connaissance de l’étendue des dégâts causés par ces lésions est primordiale pour améliorer l’efficacité de leur traitement et les décisions cliniques associées. L’imagerie par résonance magnétique (IRM) a démontré un grand potentiel pour le diagnostic et pronostic des maladies neurodégénératives et traumas de la moelle épinière. Plus particulièrement, l’analyse par template de données IRM du cerveau, couplée à des outils de traitement d’images automatisés, a permis une meilleure compréhension des mécanismes sous-jacents de maladies comme l’Alzheimer et la Sclérose en Plaques. Extraire automatiquement des informations pertinentes d’images IRM au sein de régions spécifiques de la moelle épinière présente toutefois de plus grands défis que dans le cerveau. Il n’existe en effet qu’un nombre limité de template de la moelle épinière dans la littérature, et aucun ne couvre toute la moelle épinière ou n’est lié à un template existant du cerveau. Ce manque de template et d’outils automatisés rend difficile la tenue de larges études d’analyse de la moelle épinière sur des populations variées. L’objectif de ce projet est donc de proposer un nouveau template IRM couvrant toute la moelle épinière, recalé avec un template existant du cerveau, et intégrant des atlas de la structure interne de la moelle épinière (e.g., matière blanche et grise, tracts de la matière blanche). Ce template doit venir avec une série d’outils automatisés permettant l’extraction d’information IRM au sein de régions spécifiques de la moelle épinière. La question générale de recherche de ce projet est donc « Comment créer un template générique de la moelle épinière, qui permettrait l’analyse non biaisée et reproductible de données IRM de la moelle épinière ? ». Plusieurs contributions originales ont été proposées pour répondre à cette question et vont être décrites dans les prochains paragraphes. La première contribution de ce projet est le développement du logiciel Spinal Cord Toolbox (SCT). SCT est un logiciel open-source de traitement d’images IRM multi-parametrique de la moelle épinière (De Leener, Lévy, et al., 2016). Ce logiciel intègre notamment des outils pour la détection et la segmentation automatique de la moelle épinière et de sa structure interne (i.e., matière blanche et matière grise), l’identification et la labellisation des niveaux vertébraux, le recalage d’images IRM multimodales sur un template générique de la moelle épinière (précédemment le template MNI-Poly-AMU, maintenant le template PAM50, proposé içi). En se basant sur un atlas de la moelle, SCT intègre également des outils pour extraire des données IRM de régions spécifiques de la moelle épinière, comme la matière blanche et grise et les tracts de la matière blanche, ainsi que sur des niveaux vertébraux spécifiques. D’autres outils additionnels ont aussi été proposés, comme des outils de correction de mouvement et de traitement basiques d’images appliqués le long de la moelle épinière. Chaque outil intégré à SCT a été validé sur un jeu de données multimodales. La deuxième contribution de ce projet est le développement d’une nouvelle méthode de recalage d’images IRM de la moelle épinière (De Leener, Mangeat, et al., 2017). Cette méthode a été développée pour un usage particulier : le redressement d’images IRM de la moelle épinière, mais peut également être utilisé pour recaler plusieurs images de la moelle épinière entre elles, tout en tenant compte de la distribution vertébrale de chaque sujet. La méthode proposée se base sur une approximation globale de la courbure de la moelle épinière dans l’espace et sur la résolution analytique des champs de déformation entre les deux images. La validation de cette nouvelle méthode a été réalisée sur une population de sujets sains et de patients touchés par une compression de la moelle épinière. La contribution majeure de ce projet est le développement d’un système de création de template IRM de la moelle épinière et la proposition du template PAM50 comme template de référence pour les études d’analyse par template de données IRM de la moelle épinière. Le template PAM50 a été créé à partir d’images IRM tiré de 50 sujets sains, et a été généré en utilisant le redressement d’images présenté ci-dessus et une méthode de recalage d’images itératif non linéaire, après plusieurs étapes de prétraitement d’images. Ces étapes de prétraitement incluent la segmentation automatique de la moelle épinière, l’extraction manuelle du bord antérieur du tronc cérébral, la détection et l’identification des disques intervertébraux, et la normalisation d’intensité le long de la moelle. Suite au prétraitement, la ligne centrale moyenne de la moelle et la distribution vertébrale ont été calculées sur la population entière de sujets et une image initiale de template a été générée. Après avoir recalé toutes les images sur ce template initial, le template PAM50 a été créé en utilisant un processus itératif de recalage d’image, utilisé pour générer des templates de cerveau. Le PAM50 couvre le tronc cérébral et la moelle épinière en entier, est disponible pour les contrastes IRM pondérés en T1, T2 et T2*, et intègre des cartes probabilistes et atlas de la structure interne de la moelle épinière. De plus, le PAM50 a été recalé sur le template ICBM152 du cerveau, permettant ainsi la tenue d’analyse par template simultanément dans le cerveau et dans la moelle épinière. Finalement, plusieurs résultats complémentaires ont été présentés dans cette dissertation. Premièrement, une étude de validation de la répétabilité et reproductibilité de mesures de l’aire de section de la moelle épinière a été menée sur une population de patients touchés par la sclérose en plaques. Les résultats démontrent une haute fiabilité des mesures ainsi que la possibilité de détecter des changements très subtiles de l’aire de section transverse de la moelle, importants pour mesurer l’atrophie de la moelle épinière précoce due à des maladies neurodégénératives comme la sclérose en plaques. Deuxièmement, un nouveau biomarqueur IRM des lésions de la moelle épinière a été proposé, en collaboration avec Allan Martin, de l’Université de Toronto. Ce biomarqueur, calculé à partir du ratio d’intensité entre la matière blanche et grise sur des images IRM pondérées en T2*, utilise directement les développements proposés dans ce projet, notamment en utilisant le recalage du template de la moelle épinière et les méthodes de segmentation de la moelle. La faisabilité d’extraire des mesures de données IRM multiparamétrique dans des régions spécifiques de la moelle épinière a également été démontrée, permettant d’améliorer le diagnostic et pronostic de lésions et compression de la moelle épinière. Finalement, une nouvelle méthode d’extraction de la morphométrie de la moelle épinière a été proposée et utilisée sur une population de patients touchés par une compression asymptomatique de la moelle épinière, démontrant de grandes capacités de diagnostic (> 99%). Le développement du template PAM50 comble le manque de template de la moelle épinière dans la littérature mais présente cependant plusieurs limitations. En effet, le template proposé se base sur une population de 50 sujets sains et jeunes (âge moyen = 27 +- 6.5) et est donc biaisée vers cette population particulière. Adapter les analyses par template pour un autre type de population (âge, race ou maladie différente) peut être réalisé directement sur les méthodes d’analyse mais aussi sur le template en lui-même. Tous le code pour générer le template a en effet été mis en ligne (https://github.com/neuropoly/template) pour permettre à tout groupe de recherche de développer son propre template. Une autre limitation de ce projet est le choix d’un système de coordonnées basé sur la position des vertèbres. En effet, les vertèbres ne représentent pas complètement le caractère fonctionnel de la moelle épinière, à cause de la différence entre les niveaux vertébraux et spinaux. Le développement d’un système de coordonnées spinal, bien que difficile à caractériser dans des images IRM, serait plus approprié pour l’analyse fonctionnelle de la moelle épinière. Finalement, il existe encore de nombreux défis pour automatiser l’ensemble des outils développés dans ce projet et les rendre robuste pour la majorité des contrastes et champs de vue utilisés en IRM conventionnel et clinique. Ce projet a présenté plusieurs développements importants pour l’analyse de données IRM de la moelle épinière. De nombreuses améliorations du travail présenté sont cependant requises pour amener ces outils dans un contexte clinique et pour permettre d’améliorer notre compréhension des maladies affectant la moelle épinière. Les applications cliniques requièrent notamment l’amélioration de la robustesse et de l’automatisation des méthodes d’analyse d’images proposées. La caractérisation de la structure interne de la moelle épinière, incluant la matière blanche et la matière grise, présente en effet de grands défis, compte tenu de la qualité et la résolution des images IRM standard acquises en clinique. Les outils développés et validés au cours de ce projet ont un grand potentiel pour la compréhension et la caractérisation des maladies affectant la moelle épinière et aura un impact significatif sur la communauté de la neuroimagerie.----------ABSTRACT The spinal cord plays a fundamental role in the human body, as part of the central nervous system and being the vector between the brain and the peripheral nervous system. Damaging the spinal cord, through traumatic injuries or neurodegenerative diseases, can significantly affect the quality of life of patients. Indeed, spinal cord injuries and diseases can affect the integrity of neurons, and induce neurological impairments and/or functional disabilities. While various treatment procedures exist, assessing the extent of damages and understanding the underlying mechanisms of diseases would improve treatment efficiency and clinical decisions. Over the last decades, magnetic resonance imaging (MRI) has demonstrated a high potential for the diagnosis and prognosis of spinal cord injury and neurodegenerative diseases. Particularly, template-based analysis of brain MRI data has been very helpful for the understanding of neurological diseases, using automated analysis of large groups of patients. However, extracting MRI information within specific regions of the spinal cord with minimum bias and using automated tools is still a challenge. Indeed, only a limited number of MRI template of the spinal cord exists, and none covers the full spinal cord, thereby preventing large multi-centric template-based analysis of the spinal cord. Moreover, no template integrates both the spinal cord and the brain region, thereby preventing simultaneous cerebrospinal studies. The objective of this project was to propose a new MRI template of the full spinal cord, which allows simultaneous brain and spinal cord studies, that integrates atlases of the spinal cord internal structures (e.g., white and gray matter, white matter pathways) and that comes with tools for extracting information within these subregions. More particularly, the general research question of the project was “How to create generic MRI templates of the spinal cord that would enable unbiased and reproducible template-based analysis of spinal cord MRI data?”. Several original contributions have been made to answer this question and to enable template-based analysis of spinal cord MRI data. The first contribution was the development of the Spinal Cord Toolbox (SCT), a comprehensive and open-source software for processing multi-parametric MRI data of the spinal cord (De Leener, Lévy, et al., 2016). SCT includes tools for the automatic segmentation of the spinal cord and its internal structure (white and gray matter), vertebral labeling, registration of multimodal MRI data (structural and non-structural) on a spinal cord MRI template (initially the MNI-Poly-AMU template, later the PAM50 template), co-registration of spinal cord MRI images, as well as the robust extraction of MRI metric within specific regions of the spinal cord (i.e., white and gray matter, white matter tracts, gray matter subregions) and specific vertebral levels using a spinal cord atlas (Lévy et al., 2015). Additional tools include robust motion correction and image processing along the spinal cord. Each tool included in SCT has been validated on a multimodal dataset. The second contribution of this project was the development of a novel registration method dedicated to spinal cord images, with an interest in the straightening of the spinal cord, while preserving its topology (De Leener, Mangeat et al., 2017). This method is based on the global approximation of the spinal cord and the analytical computation of deformation fields perpendicular to the centerline. Validation included calculation of distance measurements after straightening on a population of healthy subjects and patients with spinal cord compression. The major contribution of this project was the development of a framework for generating MRI template of the spinal cord and the PAM50 template, an unbiased and symmetrical MRI template of the brainstem and full spinal cord. Based on 50 healthy subjects, the PAM50 template was generated using an iterative nonlinear registration process, after applying normalization and straightening of all images. Pre-processing included segmentation of the spinal cord, manual delineation of the brainstem anterior edge, detection and identification of intervertebral disks, and normalization of intensity along the spinal cord. Next, the average centerline and vertebral distribution was computed to create an initial straight template space. Then, all images were registered to the initial template space and an iterative nonlinear registration framework was applied to create the final symmetrical template. The PAM50 covers the brainstem and the full spinal cord, from C1 to L2, is available for T1-, T2- and T2*-weighted contrasts, and includes probabilistic maps of the white and the gray matter and atlases of the white matter pathways and gray matter subregions. Additionally, the PAM50 template has been merged with the ICBM152 brain template, thereby allowing for simultaneous cerebrospinal template-based analysis. Finally, several complementary results, focused on clinical validation and applications, are presented. First, a reproducibility and repeatability study of cross-sectional area measurements using SCT (De Leener, Granberg, Fink, Stikov, & Cohen-Adad, 2017) was performed on a Multiple Sclerosis population (n=9). The results demonstrated the high reproducibility and repeatability of SCT and its ability to detect very subtle atrophy of the spinal cord. Second, a novel biomarker of spinal cord injury has been proposed. Based on the T2*-weighted intensity ratio between the white and the gray matter, this new biomarker is computed by registering MRI images with the PAM50 template and extracting metrics using probabilistic atlases. Additionally, the feasibility of extracting multiparametric MRI metrics from subregions of the spinal cord has been demonstrated and the diagnostic potential of this approach has been assessed on a degenerative cervical myelopathy (DCM) population. Finally, a method for extracting shape morphometrics along the spinal cord has been proposed, including spinal cord flattening, indentation and torsion. These metrics demonstrated high capabilities for the diagnostic of asymptomatic spinal cord compression (AUC=99.8% for flattening, 99.3% for indentation, and 98.4% for torsion). The development of the PAM50 template enables unbiased template-based analysis of the spinal cord. However, the PAM50 template has several limitations. Indeed, the proposed template has been generated with multimodal MRI images from 50 healthy and young individuals (age = 27+/- 6.5 y.o.). Therefore, the template is specific to this particular population and could not be directly usable for age- or disease-specific populations. One solution is to open-source the templategeneration code so that research groups can generate and use their own spinal cord MRI template. The code is available on https://github.com/neuropoly/template. While this project introduced a generic referential coordinate system, based on vertebral levels and the pontomedullary junction as origin, one limitation is the choice of this coordinate system. Another coordinate system, based spinal segments would be more suitable for functional analysis. However, the acquisition of MRI images with high enough resolution to delineate the spinal roots is still challenging. Finally, several challenges in the automation of spinal cord MRI processing remains, including the robust detection and identification of vertebral levels, particularly in case of small fields-of-view. This project introduced key developments for the analysis of spinal cord MRI data. Many more developments are still required to bring them into clinics and to improve our understanding of diseases affecting the spinal cord. Indeed, clinical applications require the improvement of the robustness and the automation of the proposed processing and analysis tools. Particularly, the detection and segmentation of spinal cord structures, including vertebral labeling and white/gray matter segmentation, is still challenging, given the lowest quality and resolution of standard clinical MRI acquisition. The tools developed and validated here have the potential to improve our understanding and the characterization of diseases affecting the spinal cord and will have a significant impact on the neuroimaging community

Open-access quantitative MRI data of the spinal cord and reproducibility across participants, sites and manufacturers

In a companion paper by Cohen-Adad et al. we introduce the spine generic quantitative MRI protocol that provides valuable metrics for assessing spinal cord macrostructural and microstructural integrity. This protocol was used to acquire a single subject dataset across 19 centers and a multi-subject dataset across 42 centers (for a total of 260 participants), spanning the three main MRI manufacturers: GE, Philips and Siemens. Both datasets are publicly available via git-annex. Data were analysed using the Spinal Cord Toolbox to produce normative values as well as inter/intra-site and inter/intra-manufacturer statistics. Reproducibility for the spine generic protocol was high across sites and manufacturers, with an average inter-site coefficient of variation of less than 5% for all the metrics. Full documentation and results can be found at https://spine-generic.rtfd.io/. The datasets and analysis pipeline will help pave the way towards accessible and reproducible quantitative MRI in the spinal cord

Mechanisms of spinal cord degeneration and repair in multiple sclerosis: A 3T MRI study of the spinal cord

The spinal cord is a clinically eloquent structure, commonly affected in multiple sclerosis (MS) and spinal neuroaxonal loss is an important cause of non-remitting, disability progression. Neuroaxonal loss in MS is likely to be multifactorial and caused by several disease pathways. In contrast, repair and adaptive mechanisms can ameliorate disability following clinical relapses. This thesis has explored some of these clinically relevant disease mechanisms by combining single-voxel proton spectroscopy (MRS) and Q-space imaging (QSI), two advanced MRI techniques, which have increased pathological specificity for neurodegeneration and myelin, and allow quantification of metabolites that reflect biological mechanisms, to study spinal neurodegeneration and repair in MS. In persons with early primary progressive MS (PPMS), spinal MRS and QSI exhibited increased sensitivity for detection of early disease changes than more conventional measures such as spinal cord atrophy and correlated with clinical disability measures suggesting these measures are functionally relevant. Region of interest analysis of the relationship between QSI indices in spinal white matter tracts and clinical scores which reflect the motor or sensory functions conveyed within those tracts, suggests a strong structure-function relationship exists between axonal integrity and disability. In persons with relapsing remitting MS (RRMS), with recent (within 4 weeks) symptoms suggestive of spinal cord relapse, serial imaging with spinal MRS and QSI over 6 months reflected clinical changes over that time. Specifically, rising spinal concentrations of total N-acetyl-aspartate (tNAA) and restriction of QSI-derived perpendicular diffusivity, which I hypothesise reflect, restoration of mitochondrial function and remyelination, respectively, underlie clinical recovery. Within the RRMS cohort, MRS and QSI measures at baseline were predictive of clinical outcomes at 6 months; elevated baseline spinal glutamate-glutamine (Glx), myo-inositol (Ins) and total creatine (tCr) concentrations and increased QSI-derived perpendicular diffusivity predicted poor outcomes and may reflect important mechanisms of disability progression such as; demyelination, neurodegeneration, astrogliosis and altered neuronal metabolism. Taken together the results suggest that mechanisms of disability following spinal cord relapse are complex and glutamate excitotoxicity, gliosis and axonal metabolic dysfunction may be important determinants of residual disability following relapses. This work suggests that newer, quantitative MRI techniques when applied to the spinal cord are sensitive markers of disease activity and progression and could be useful in monitoring therapies that aim to prevent neurodegeneration and enhance remyelination in MS