Is the Relationship between Cortical and White Matter Pathologic Changes in Multiple Sclerosis Spatially Specific? A Multimodal 7-T and 3-T MR Imaging Study with Surface and Tract-based Analysis

Louapre, Céline; Govindarajan, Sindhuja T.; Giannì, Costanza; Cohen‐Adad, Julien; Gregory, Michael D.; Nielsen, A. Scott; Madigan, Nancy; Kinkel, Revere P.; Mainero, Caterina

doi:10.1148/radiol.2015150486

Cited by 13 publications

(8 citation statements)

References 39 publications

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“…Thirty-one patients (21 females; mean age = 42.4 ± 8.7 SD years) were prospectively recruited in the study from May 2010 to May 2013. This cohort is partly overlapping (31 out of 41 patients) with a cohort from a previously published study in which we found cortical areas characterized by longer q-T 2 * relative to a healthy matched population (Louapre et al, 2016, Louapre et al, 2015, Mainero et al, 2015). The remaining 10 MS subjects were not included due to the lack of NP evaluation at the time of the scanning procedure.…”

Section: Methodsmentioning

confidence: 59%

The association between intra- and juxta-cortical pathology and cognitive impairment in multiple sclerosis by quantitative T 2 * mapping at 7 T MRI

Louapre

Govindarajan

Giannì

et al. 2016

NeuroImage: Clinical

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Using quantitative T2* at 7 Tesla (T) magnetic resonance imaging, we investigated whether impairment in selective cognitive functions in multiple sclerosis (MS) can be explained by pathology in specific areas and/or layers of the cortex.Thirty-one MS patients underwent neuropsychological evaluation, acquisition of 7 T multi-echo T2* gradient-echo sequences, and 3 T anatomical images for cortical surfaces reconstruction. Seventeen age-matched healthy subjects served as controls.Cortical T2* maps were sampled at various depths throughout the cortex and juxtacortex. Relation between T2*, neuropsychological scores and a cognitive index (CI), calculated from a principal component analysis on the whole battery, was tested by a general linear model.Cognitive impairment correlated with T2* increase, independently from white matter lesions and cortical thickness, in cortical areas highly relevant for cognition belonging to the default-mode network (p < 0.05 corrected). Dysfunction in different cognitive functions correlated with longer T2* in selective cortical regions, most of which showed longer T2* relative to controls. For most tests, this association was strongest in deeper cortical layers. Executive dysfunction, however, was mainly related with pathology in juxtameningeal cortex. T2* explained up to 20% of the variance of the CI, independently of conventional imaging metrics (adjusted-R2: 52–67%, p < 5.10− 4).Location of pathology across the cortical width and mantle showed selective correlation with impairment in differing cognitive domains. These findings may guide studies at lower field strength designed to develop surrogate markers of cognitive impairment in MS.

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Section: Methodsmentioning

confidence: 59%

The association between intra- and juxta-cortical pathology and cognitive impairment in multiple sclerosis by quantitative T 2 * mapping at 7 T MRI

Louapre

Govindarajan

Giannì

et al. 2016

NeuroImage: Clinical

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“…Furthermore, there are similarities between the average anatomical distribution of GM atrophy and the distributions of both existing WM lesions ( Bodini et al, 2009 ; Muhlau et al, 2013 ; Riccitelli et al, 2012 ) and new WM lesions ( Battaglini et al, 2009 ; Bendfeldt et al, 2010 ). The relation of local GM atrophy to lesional and non-lesional damage in connected WM tracts has only been partially explored ( Bergsland et al, 2015 ; Louapre et al, 2016 ; Steenwijk et al, 2015 ) and further studies are needed to clarify this.…”

Section: Challenges Of Pathology Physiology and Treatment Effectsmentioning

confidence: 99%

Urgent challenges in quantification and interpretation of brain grey matter atrophy in individual MS patients using MRI

Amiri

Sitter

Bendfeldt³

et al. 2018

NeuroImage: Clinical

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Atrophy of the brain grey matter (GM) is an accepted and important feature of multiple sclerosis (MS). However, its accurate measurement is hampered by various technical, pathological and physiological factors. As a consequence, it is challenging to investigate the role of GM atrophy in the disease process as well as the effect of treatments that aim to reduce neurodegeneration. In this paper we discuss the most important challenges currently hampering the measurement and interpretation of GM atrophy in MS. The focus is on measurements that are obtained in individual patients rather than on group analysis methods, because of their importance in clinical trials and ultimately in clinical care. We discuss the sources and possible solutions of the current challenges, and provide recommendations to achieve reliable measurement and interpretation of brain GM atrophy in MS.

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“…Tracts of the limbic system, like the fornix, play crucial roles in aspects of cognition, memory, behavior, and reasoning (Catani & de Schotten, 2012), and they have been implicated in the above whole-brain analyses of MS. Given this relevance, limbic system tracts have been the focus in MS diffusion MRI studies assessed with either region of interest/atlas (Dineen, Bradshaw, Constantinescu, & Auer, 2012;Koenig et al, 2013;Mesaros et al, 2012;Van Geest et al, 2018) or tractography (Fink et al, 2010;Kern et al, 2015;Keser et al, 2017;Louapre et al, 2016;Syc et al, 2013), both targeted analyses that can have distinct advantages over whole-brain voxel-based methods (e.g., far fewer multiple comparisons and do not need intersubject registration for native space tractography). The majority of these DTI studies have been in patients with RRMS, but FA abnormalities in the limbic WM tracts, including the fornix, have also been demonstrated in primary progressive (PPMS; Bodini et al, 2009) and secondary progressive MS (SPMS) (Meijer et al, 2016).…”

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confidence: 99%

Diffusion tensor imaging tractography reveals altered fornix in all diagnostic subtypes of multiple sclerosis

et al. 2019

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Inflammation, demyelination, and axonal degeneration of white matter (WM) pathways are hallmarks of multiple sclerosis (MS;Bjartmar, Wujek, & Trapp, 2003). The progressive deterioration of specific WM tracts may cause disconnections between cortical/subcortical regions that are associated with particular cognitive impairments (Mesaros et al., 2012). Diffusion tensor imaging (DTI) is well suited to the virtual identification of WM pathways and can yield quantitative metrics that are sensitive to microstructural damage of WM,

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Is the Relationship between Cortical and White Matter Pathologic Changes in Multiple Sclerosis Spatially Specific? A Multimodal 7-T and 3-T MR Imaging Study with Surface and Tract-based Analysis

Cited by 13 publications

References 39 publications

The association between intra- and juxta-cortical pathology and cognitive impairment in multiple sclerosis by quantitative T 2 * mapping at 7 T MRI

The association between intra- and juxta-cortical pathology and cognitive impairment in multiple sclerosis by quantitative T 2 * mapping at 7 T MRI

Urgent challenges in quantification and interpretation of brain grey matter atrophy in individual MS patients using MRI

Diffusion tensor imaging tractography reveals altered fornix in all diagnostic subtypes of multiple sclerosis

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