Multiple Sclerosis Clinical Trial
— ONDDSOfficial title:
Optic Neuritis Differential Diagnosis Study (ONDDS)
NCT number | NCT03370965 |
Other study ID # | 17/B/01 |
Secondary ID | |
Status | Recruiting |
Phase | N/A |
First received | |
Last updated | |
Start date | June 7, 2019 |
Est. completion date | June 2025 |
Background: Optic neuritis is a frequent cause of vision loss encountered by ophthalmologists in the Caribbean. The diagnosis is made on clinical grounds. Optic neuritis can occur either in an isolated manner or, most often, as the first symptom of multiple sclerosis (MS) or neuromyelitisoptica (NMO). These 2 demyelinating disorders differ by many means, including treatment and prognosis. MS can cause severe long-term disability while NMO is a short-term sight- and life-threatening condition causing potential relapses, which may require plasma exchanges. Furthermore, disease-modifying therapies used in NMO are different from those used in MS, which can worsen the natural history of NMO. Early differential diagnosis of these diseases is thus crucial for preventing severe visual loss and disability.
Status | Recruiting |
Enrollment | 150 |
Est. completion date | June 2025 |
Est. primary completion date | June 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: 1. Patient aged 18 years or older at time of inclusion. 2. Table of unilateral or bilateral optic neuritis defined as follows (clinical diagnosis): 1. Visual sharpness (acuity and / or visual field) experienced acutely or subacutely (<1 month) unilateral or bilateral, not corrected by optical correction. 2. Absence of ophthalmologic lesion which may explain the visual loss. 3. Examination of the normal fundus or showing a pallor or papular edema. 4. Presence of relative pupillary deficit relative if unilateral attack. 3. Patient (s) affiliated to a social security scheme (beneficiary or beneficiary). 4. Patient who has given free and written consent. Exclusion Criteria: 1. Patients known to have an inflammatory disease of the central nervous system (MS, NMO, EMAD). 2. Known history of inflammatory pathology (lupus or sarcoidosis) or infectious pathology (syphilis, HIV) that may give rise to optical neuropathy. 3. Table suggestive of Leber's hereditary optic neuropathy (genetically confirmed). 4. Treatment in progress known to give optical neuropathies. 5. Consumption of toxic known to give optical neuropathies. 6. Drinking more than 3 alcohol drinks per day for men and 2 alcohol drinks per day for women over a period of more than 15 years. 7. Arguments for non-arteritic ischemic optic neuropathy defined by all of the following criteria: 1. Absence of pain in eye movements. 2. Altitudinal deficit of the visual field. 3. Choroidal ischemia with fluorescein angiography. 4. Presence of cardiovascular risk factors. 5. Absence of neurological signs related to inflammatory disease of the central nervous system. 8. Arguments for arterial ischemic optic neuropathy defined by all of the following criteria: 1. Absence of pain in eye movements. 2. Altitudinal deficit of the visual field. 3. Choroidal ischemia with fluorescein angiography. 4. Presence of symptoms suggestive of Horton's disease. 5. Absence of neurological signs related to inflammatory disease of the central nervous system. 9. Pregnant and lactating patients. |
Country | Name | City | State |
---|---|---|---|
France | CHU of Martinique | Fort-de-France |
Lead Sponsor | Collaborator |
---|---|
University Hospital Center of Martinique | Hospital Center of Cayenne (French Guyana), University Hospital Center of Guadeloupe |
France,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Final diagnosis using MS (McDonald, 2010) - Spatial dissemination | One T2 lesion ore more in at least two of the four central nervous system territories considered to be characteristic of MS:
juxtacortical, periventricular, sub-tentorial, medullary (in case of medullary syndrome or brain stem, symptomatic lesions are excluded from the diagnostic criteria and do not participate in the lesion count). |
12 months | |
Primary | Final diagnosis using MS (McDonald, 2010) - Time dissemination | A new lesion in T2 and / or a lesion taking gadolinium on a follow-up MRI regardless of the time of initial MRI.
The simultaneous presence of asymptomatic lesions raised and not elevated by gadolinium at any time. |
12 months | |
Primary | NMO diagnosis criteria (Wingerchuk, 2015) - Diagnosis of NMO-SD with positive anti-AQP4 Antibody | At least one main clinical criterion (1)
Exclusion of other diagnoses |
12 months | |
Primary | NMO diagnosis criteria (Wingerchuk, 2015) - Diagnosis of NMO-SD with anti-AQP4 negative antibody | At least 2 main clinical criteria occurring in the context of one or more clinical outbreaks and meeting the following criteria
At least 1 of the 2 main clinical criteria should be optic neuritis, extensive longitudinal myelitis or area postrema syndrome. Dissemination in space (at least 2 main criteria) Respect of MRI imaging criteria (2) Anti-AQP4 negative antibodies Exclusion of differential diagnoses |
12 months |
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