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Imaging the Interplay Between Axonal Damage and Repair in Multiple Sclerosis — INsIDER

Multiple Sclerosis (MS) Clinical Trial

Official title:
INsIDER: Imaging the Interplay Between Axonal Damage and Repair in Multiple Sclerosis

Clinical Trial Summary

This project is to: 1. Quantify differences in axonal integrity and organization in aMS versus naPMS patients. 2. Quantify changes in axonal integrity and organization in aMS versus naPMS patients over a two-year period. 3. Validate the combination of imaging parameters that best differentiate aMS versus naPMS patients using histopathology.

Clinical Trial Description

Multiple sclerosis (MS) is a chronic autoimmune disease of the central nervous system characterized by multifocal inflammatory infiltrates, microglial activation and degradation of oligodendrocytes, myelin and axons. Clinical MS categories exhibit variable amount of central nervous system (CNS) damage and repair, depending on numerous variables including genetic, immunological, pathological and environmental factors. Therefore, understanding the interplay between axonal damage (i.e. axonal demyelination/degeneration/loss/disorganization) and (ii) axonal repair (i.e. axonal remyelination/reorganization) in living MS patients may be the key to understand disease progression, to establish accurate disease monitoring criteria and to predict disease response to future reparative therapies. New in-vivo methods are necessary to elucidate the interplay between axonal damage and repair in the brain of living patients with MS. Advanced MRI (aMRI) permits a multifaced quantification of the various components of the axons and their organization. Neurite Orientation Dispersion and Density Imaging (NODDI) and Diffusion Kurtosis (DK) are new approaches in clinical research This study is to identify in vivo the specific neuropathological pattern of axonal damage and repair exhibited by active MS (aMS) and non-active progressive MS (naPMS) patient by leveraging the information provided by model-based diffusion metrics (NODDI, DK), Magnetization Transfer Imaging (MTI), Multi-echo Susceptibility-Based imaging (SBI), Myelin Water Imaging (MWI) and quantitative T1 relaxometry (qT1). These advanced MRI contrasts provide complementary and partially redundant information about the axonal structure and its organization (i.e. density and orientation of axons and dendrites in the brain tissue, axonal integrity and myelination, presence of myelin and iron, and brain tissue architecture). Therefore, their combination may prove high sensitivity and specificity to axonal damage and repair. This project has 3 main aims: Aim 1. Quantify differences in axonal integrity and organization in aMS versus naPMS patients. Aim 2. Quantify changes in axonal integrity and organization in aMS versus naPMS patients over a two-year period. Aim 3. Validate the combination of imaging parameters that best differentiate aMS versus naPMS patients using histopathology. ;

Study Design

Related Conditions & MeSH terms

Clinical Trial Details
NCT number NCT05177523
Study type Observational
Source University Hospital, Basel, Switzerland
Contact Cristina Granziera, Prof. Dr. med.
Phone +41 61-32 85 665
Email cristina.granziera@usb.ch
Status Recruiting
Phase
Start date September 4, 2018
Completion date September 2024
View Details
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