Multiple Sclerosis Clinical Trial
— ENERGYSEPOfficial title:
Exploring in Vivo the Energetic Origin of Neurodegeneration in Multiple Sclerosis: a Ultra-high Field Sodium Imaging, Phosphorus Spectroscopy and Diffusion-weighted Spectroscopy Study.
Verified date | August 2020 |
Source | Institut National de la Santé Et de la Recherche Médicale, France |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
In multiple sclerosis (MS), the sequence of events leading to irreversible neuro-axonal
degeneration, which is a major determinant of clinical disability, is poorly understood.
Recently, the key role of neuronal energy dysfunction in driving axonal degeneration has been
highlighted. In the neuronal injury pathway triggered by inflammation and myelin disruption,
multiple adaptive changes force the neuron to a temporary condition of "virtual hypoxia",
characterized by a mismatch between energy demand and supply. If this condition of energy
dysregulation is not reversed within an appropriate time-window, neurons enter an
irreversible axonal degeneration.
Two key questions on the relationship between early energy dysregulation and
neurodegeneration remain unanswered:
i) whether brain energy dysfunction measured at a given time point can predict the subsequent
occurrence of neurodegeneration; ii) to what extent and for how long neurons can bear this
"virtual hypoxia" before undergoing structural damage.
Tracking the "energetic signature" of MS and defining its temporal distance from irreversible
damage is essential for the development of neuroprotective therapies.The recent optimization
of innovative magnetic resonance (MR)-based techniques such as sodium (23Na) MRI, phosphorus
MR spectroscopy (31P-MRS), and diffusion-weighted 1H MRS (DW-MRS) has allowed the generation
of promising in vivo data on cellular energy dysregulation in MS.
The main objective of this project is to explore whether MR-derived metrics of energy
dysregulation predict MR-derived parameters of cortical neurodegeneration developing over 2
years, as reflected by cortical atrophy. To address this key question, the Investigators will
use a combination of 23Na MRI, 31P MRS, and DW-MRS associated with advanced MRI sequences to
explore energy dysregulation in the sensorimotor region, and measurements of cortical atrophy
in the same area after 24 months in 40 patients with either relapsing-remitting or
progressive MS and 15 age- and gender-matched healthy controls.
The Investigators will also test whether MR-derived metrics of energy dysregulation at study
entry correlate, both cross-sectionally and longitudinally, with: i) global cortical atrophy;
ii) functional cortical reorganization resulting from the condition of energy dysregulation,
which precedes the occurrence of structural damage; iii) cortical demyelination and
remyelination; iv) clinical, neuropsychological and biological measures.
Status | Not yet recruiting |
Enrollment | 55 |
Est. completion date | March 15, 2024 |
Est. primary completion date | September 15, 2022 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 18 Years to 55 Years |
Eligibility |
Inclusion Criteria for MS: 1. RR-MS patients with a disease duration of less than 10 years: - 18-55 years - clinically defined RR-MS according to the 2017 revised McDonald's criteria (MS diagnostic criteria 2017) - disease duration <10 years - ability to understand the research objectives and the procedure details, and to sign the informed consent - affiliation with the French National Health Insurance, Universal Medical Coverage (CMU) or any equivalent 2. Patients with progressive MS (primary or secondary) of less than 10 years: - 18-55 years - clinically defined progressive MS according to the 2017 revised McDonald's criteria - disease duration <10 years from the beginning of the progressive phase - ability to understand the research objectives and the procedure details, and to sign the informed consent - affiliation with the French National Health Insurance, Universal Medical Coverage (CMU) or any equivalent Inclusion Criteria for healthy controls: - 18-55 years (matched with patients) - no known general pathologies - ability to understand the research objectives and the procedure details, and to sign the informed consent - affiliation with the French National Health Insurance, Universal Medical Coverage (CMU) or any equivalent Exclusion Criteria for MS: - Pregnant or breastfeeding women - Last infusion of cyclophosphamide, mitoxantrone or methylprednisolone realized less than 1 month before inclusion - last clinical relapse less than one month before inclusion - severe cardiac, pulmonary, hepatic, hematologic renal, gastrointestinal disease, or cancer - contraindications to MRI: claustrophobia, pace-maker implant, any surgical ferromagnetic clips, ocular implants, any intraocular or intracranial metallic fragments, any metallic objects able to concentrate the radiofrequency field, cochlear implants, cardiac or brain stimulators, any tattoos or permanent makeup on the face, renal failure (exclusion criterion for gadolinium injection) patients not willing to be informed of any possible cerebral malformations incidentally discovered at the MRI exam - severe renal failure (clearance of creatinine < 30ml/min) - history of allergic reactions to gadolinium salts - any other chronic neurological disorders associated - persons deprived of liberty by law or by administrative decision - Persons under legal protection Exclusion Criteria for healthy controls: - Pregnant or breastfeeding women - severe cardiac, pulmonary, hepatic, hematologic renal, gastrointestinal disease, or cancer - contraindications to MRI : claustrophobia, pace-maker implant, any surgical magnetic clips, ocular implants, any intraocular or intracranial metallic fragments, any metallic objects able to concentrate the radiofrequency field, cochlear implants, cardiac or brain stimulators, any tattoos or permanent makeup on the face - person not willing to be informed of any possible cerebral malformations incidentally discovered at the MRI exam - associated chronic neurological disorders - persons deprived of liberty by law or by administrative decision - Persons under legal protection |
Country | Name | City | State |
---|---|---|---|
n/a |
Lead Sponsor | Collaborator |
---|---|
Institut National de la Santé Et de la Recherche Médicale, France |
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Energy dysregulation in the whole brain with sodium imaging | Evaluation of the levels of total, intracellular and extracellular sodium quantified through 23Na MRI in the whole brain. | 0-12 months | |
Primary | Energy dysregulation in the motor-sensory region (MSR) with phosphorus spectroscopy | Evaluation of ATP and PCr concentrations measured through 31P MRS in a voxel centred on the left MSR | 0-12 months | |
Primary | Energy dysregulation in the motor-sensory region with diffusion-weighted spectroscopy | Evaluation of the ADC of tCr (Cr + PCr) measured through DW-MRS in a voxel centred on the left MSR. | 0-12 months | |
Primary | Neurodegeneration in the MSR after 24 months | Neurodegeneration after 24 months will be evaluated by the measurements of the following parameters: Evaluation of MSR cortical thickness after 24 months and relative change in MSR cortical thickness between study entry and 24 months measured with Freesurfer (https://surfer.nmr.mgh.harvard.edu). |
0-24 months | |
Secondary | Patient-specific profiles of energy dysregulation | The difference of MRI-derived metrics of energy dysregulation between patients and controls at study entry will be evaluated with 23Na MRI in the whole brain, and with 23Na MRI, 31P MRS and DW-MRS in the MSR | 0-12 months | |
Secondary | cortical demyelination and remyelination | Cortical demyelination at study entry will be measured by cross-sectional cortical magnetisation transfer ratio (MTR), and cortical remyelination after 12 months will be evaluated by the measurement of cortical MTR change over 12 months | 0-12 months | |
Secondary | neuro-axonal damage over time | Early axonal damage will be quantified through the NODDI-derived metrics | 0-12-24 months | |
Secondary | functional changes in brain connectivity | Changes in brain connectivity at study entry and after 12 and 24 months will be measured by resting-state functional MRI | 0-12-24 months | |
Secondary | serum markers of tissue damage | Serum neurofilaments, measured at study entry and at 12 and 24 months, will be used as a biomarker of acute and chronic neuronal lesions | 0-12-24 months | |
Secondary | physical and cognitive dysfunction | Neurologic disability will be evaluated by EDSS | 0-12-24 months | |
Secondary | physical and cognitive dysfunction | Neurologic disability will be evaluated by MFIS | 0-12-24 months | |
Secondary | physical and cognitive dysfunction | Neurologic disability will be evaluated by BICAMS | 0-12-24 months |
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