CHRONIC OPTIC NEUROPATHY IN MULTIPLE SCLEROSIS
Status
Conditions
Treatments
Details and patient eligibility
About
Patients with multiple sclerosis (MS) may show chronic signs of optic neuropathy (CON) that may follow acute optic neuritis (secondary form of CON, S-CON) or occur independently of any acute demyelinating lesion of the optic nerve (primary form of CON, P-CON). In both S-CON and P-CON, a long term progressive ganglion cell axonal loss occurs. This axonal damage could be secondary to retrograde atrophy of axons within plaques of demyelination or a primary progressive degeneration of ganglion cells, but the underlying physiopathology has not been fully questioned in the different profile types of CON.
In this project, investigators aim at understanding the pathophysiology of S-CON and P-CON, i.e. secondary to demyelination or primary degeneration, in patients complaining of persistent visual complaints. In a first cross sectional study, 30 MS patients with mild to moderate P-CPON or S-CON and 30 age-matched control subjects will perform an extensive neuro-ophthalmological assessment including clinical examination, visual evoked potentials (pattern and low contrast), electroretinogram (pattern and multifocal ERG), OCT (peripapillary and macular volume scan segmentation protocols) and MRI of the optic nerve. In these patients with mild to moderate CON, investigators aim at differentiating patients showing predominant demyelination from those showing pure or predominant axonal degeneration. Visual function assessment and degree of axonal degeneration will be compared and correlated in the two types of underlying pathophysiology and in the group of control subject. In a following longitudinal study, the patients will be re-assessed a year later in order to evaluate the progression of CON in both profile types. Our hypothesis would be that visual function and progression is worse in the degeneration group as compared to the demyelination group. This study should help to find reliable measures of the pathophysiology of CON and correlate it with the long-term visual prognostic of the disease.
Enrollment
Sex
Ages
Volunteers
Inclusion criteria
-
Inclusion criteria for patients
- All patients may have a clinically definite, laboratory-supported diagnosis of multiple sclerosis according to the Mac Donald criteria (2010).
- All patients may present a chronic visual complaint.
- All patients may present mild to moderate chronic optic neuropathy (cf infra)
- All patients may not have recent acute optic neuritis (<2 years)
- All patients will be informed about the design and purpose of the study, and all will give their informed, written consent to the protocol, which may have been approved by the local ethics committee.
- Age: > 18
- Able to understand the instructions
- Having a health coverage
- Able to sit down for 1 hour Diagnosis of mild to moderate chronic optic neuropathy
For the diagnosis of optic neuropathy, patients will have to meet 3 of the 6 next criteria:
-
Far Visual Acuity (ETDRS charts, 100% contrast) < 85 letters
-
Far Visual Acuity (ETDRS charts, 2.5% contrast) < 60 letters
-
Mean visual field defect on static perimetry> 2dB
-
Mean pRNFL in OCT < 80 µ.
-
Color vision score > 35
-
Disc pallor Diagnosis of mild to moderate optic neuropathy
-
Far Visual Acuity (ETDRS charts, 100% contrast) >70 letters Diagnosis of chronic optic neuropathy
-
Stable or worsening of visual acuity, visual field and/or RNFL in OCT, at 6 month of interval
- Inclusion criteria for controls
-
Age > 18 years
-
Visual acuity score (ETDRS) > 85
-
Able to understand the instructions
-
Having a health coverage
-
Informed and consenting to give his written consent
-
Exclusion criteria
-
Non inclusion criteria for patients.
-
Ophthalmological
- Other ophthalmological disorder that could impair corrected visual acuity (Maculopathy, Retinopathy…)
- Ocular instability in primary position of gaze
-
Neurological
- Ongoing seizure
- Severe handicap that does not allow sitting down position for 1 hour
-
General
- Unstable medical state
- Severe renal insufficiency
- Allergy to gadolinium
- Claustrophobia
- Implanted electrical stimulator (pace maker)
- Metallic prosthesis or orthesis, cochlear implants
- Intraocular foreign material
-
Pregnancy (on questioning)
-
Tutelage or any legal protection measure
-
-
Non inclusion criteria for controls
- Any ophthalmological disorder that could impair corrected visual acuity
- Any neurological disorder
- MRI contraindication
- Allergy to gadolinium
- Severe renal insufficiency
- Claustrophobia
- Implanted electrical stimulator (pace maker)
- Metallic prosthesis or orthesis, cochlear implants
- Intraocular foreign material
- Pregnancy (on questioning)
- Tutelage or any legal protection measure
Trial design
Primary purpose
Allocation
Interventional model
Masking
39 participants in 2 patient groups
Trial contacts and locations
Loading...
Data sourced from clinicaltrials.gov
Clinical trials
Research sites
Resources
Legal