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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT05388331
Other study ID # 22Neuro01
Secondary ID
Status Recruiting
Phase
First received
Last updated
Start date April 15, 2022
Est. completion date April 15, 2029

Study information

Verified date May 2022
Source Centre Hospitalier Universitaire de Nice
Contact Christine LEBNRUN-FRENAY
Phone 33 4 92 03 41 26
Email lebrun-frenay.c@chu-nice.fr
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

The Radiologically Isolated Syndrome (RIS) corresponds to the discovery of white matter (WM) abnormalities suggestive of multiple sclerosis (MS) by their location, size, and appearance, on the brain or spinal cord Magnetic Resonance Imaging (MRI). This imaging is performed for a reason other than for suspicion of demyelinating disease in subjects without a history of neurological symptoms and a strict routine clinical neurological examination. It was defined and named in 2009 (Okuda et al.) after publishing 3 case series (French, USA, Turkey). The Radiologically Isolated Syndrome Consortium (RISC) published a cohort of subjects with an extended follow-up after the first brain MRI of MS, with 34% presenting an event (clinical conversion) at five years, 51.2 % of these subjects showed an event at ten years. The patients who offer a higher risk of developing a first clinical demyelinating event were identified such as male sex, young age, the presence of oligoclonal bands (BOCs) in the Cerebrospinal Fluid (CSF), the presence of infratentorial lesions and spinal cord lesions on the first MRI suggestive of RIS. The location and morphology of the lesions appear to be decisive for studying the risk of conversion. Our first objective is to prospectively collect data to identify the subjects who present a higher risk of developing a first clinical demyelinating event and the progression of the disease in these subjects. Among the objectives of this worldwide cohort is the analysis of (1) environmental factors (Vit D, EBV, tobacco…), (2) MRI biomarkers, including atrophy, central veins signs, paramagnetic rings, and DTI. (3) digital biomarkers (4) oculography (5) biological markers To summarize, this cohort will allow for analyzing features in imaging, biology and the exploration of digital and oculographic characteristics to identify predictive factors of clinical evolution of a large cohort of subjects presenting WM abnormalities suggestive of multiple sclerosis.


Recruitment information / eligibility

Status Recruiting
Enrollment 1000
Est. completion date April 15, 2029
Est. primary completion date April 15, 2023
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria: - white matter T2 lesions suggestive of demyelination - asymptomatic - normal neurological exam Exclusion Criteria: - abnormal neurological exam, - suspicion of another disease explaining MRI lesions.

Study Design


Intervention

Other:
No intervention
No intervention

Locations

Country Name City State
France Nice University Hospital Nice

Sponsors (1)

Lead Sponsor Collaborator
Centre Hospitalier Universitaire de Nice

Country where clinical trial is conducted

France, 

Outcome

Type Measure Description Time frame Safety issue
Primary Identification of lesions T2-weighted sequence at the index scan number of T2-weighted sequence at inclusion
Primary Identification of lesions T2-weighted sequence at the index scan localisation of interest of T2 lesion (juxtacortical, periventricular, infratentorial, spinal cord) at inclusion
Primary Identification of lesions T1 sequence with and without Gd at the index scan. Lesions number at inclusion
Primary Identification of lesions T1 sequence with and without Gd at the index scan. localisation of interest at inclusion
Primary Radiological progression : new T2 lesions localisation of interest year 1
Primary Radiological progression : new contrast enhancing lesions Lesions number year 1
Primary Radiological progression : new contrast enhancing lesions localisation of interest year 1
Primary Brain atrophy measurement of global and regional grey matter volume measurement of global and regional white matter volume year 1
Primary Brain atrophy measurement of global and regional grey matter volume measurement of global and regional white matter volume year 2
Primary Brain atrophy measurement of global and regional grey matter volume measurement of global and regional white matter volume year 3
Primary Brain atrophy measurement of global and regional grey matter volume measurement of global and regional white matter volume year 4
Primary Brain atrophy measurement of global and regional grey matter volume measurement of global and regional white matter volume year 5
Primary Brain atrophy measurement of global and regional grey matter volume measurement of global and regional white matter volume MS onset assessed up to 2 years
Primary Radiological progression : new T2 lesions number of T2-weighted sequence year 2
Primary Radiological progression : new T2 lesions localisation of interest of T2 lesion year 2
Primary Radiological progression : new T2 lesions number of T2-weighted sequence year 3
Primary Radiological progression : new T2 lesions localisation of interest of T2 lesion year 4
Primary Radiological progression : new T2 lesions number of T2-weighted sequence year 5
Primary Radiological progression : new T2 lesions localisation of interest of T2 lesion MS onset assessed up to 2 years
Primary Radiological progression : new contrast enhancing lesions localisation of interest year 2
Primary Radiological progression : new contrast enhancing lesions Lesions number year 2
Primary Radiological progression : new contrast enhancing lesions Lesions number year 3
Primary Radiological progression : new contrast enhancing lesions localisation of interest year 3
Primary Radiological progression : new contrast enhancing lesions Lesions number year 4
Primary Radiological progression : new contrast enhancing lesions localisation of interest year 4
Primary Radiological progression : new contrast enhancing lesions Lesions number year 5
Primary Radiological progression : new contrast enhancing lesions localisation of interest year 5
Primary Radiological progression : new contrast enhancing lesions Lesions number MS onset assessed up to 2 years
Primary Radiological progression : new contrast enhancing lesions localisation of interest MS onset assessed up to 2 years
Secondary Collect biological data number of plasma samples At inclusion
Secondary Collect biological data number of plasma samples MS onset assessed up to 2 years
Secondary Collect digital markers The number of abnormalities identified by the eVOG application correlated with cerebral atrophy at inclusion
Secondary Collect digital markers Progression of the number of abnormalities identified by the eVOG application correlated with cerebral atrophy year 1
Secondary Collect digital markers Progression of the number of abnormalities identified by the eVOG application correlated with cerebral atrophy year 2
Secondary Collect digital markers Progression of the number of abnormalities identified by the eVOG application correlated with cerebral atrophy year 3
Secondary Collect digital markers Progression of the number of abnormalities identified by the eVOG application correlated with cerebral atrophy year 4
Secondary Collect digital markers Progression of the number of abnormalities identified by the eVOG application correlated with cerebral atrophy year 5
Secondary Collect digital markers Progression of the number of abnormalities identified by the eVOG application correlated with cerebral atrophy MS onset assessed up to 2 years
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