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Clinical Trial Details — Status: Active, not recruiting

Administrative data

NCT number NCT04820244
Other study ID # NL67258.091.18
Secondary ID
Status Active, not recruiting
Phase
First received
Last updated
Start date February 11, 2019
Est. completion date March 2, 2024

Study information

Verified date April 2022
Source Radboud University Medical Center
Contact n/a
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

Mutations in USH2A give rise to two phenotypes: Usher syndrome type 2a (USH2A) and nonsyndromic RP (USH2A associated nsRP). Usher syndrome is the most common form of congenital deafblindness. Patients with Usher syndrome are hearing impaired or profoundly deaf from birth and this can be rehabilitated with hearing aids or a cochlear implant. Furthermore, these patients develop retinitis pigmentosa (RP), a slowly progressive type of retinal degeneration that usually starts in the first or second decade of life. In both USH2A and nsRP patients the disease leads to severe visual impairment and eventually blindness around the 50th-70th year of life. There are no treatment options for the retinal degeneration. We do not know if they also suffer from balance complaints. Currently, genetic therapy for Usher syndrome type 2 and USH2A associated nsRP is in development. But to measure the effect of a (genetic) therapy, it is crucial to know the detailed natural course of the visual and hearing deterioration over time. Several genetic therapy studies for other disorders are currently delayed, because the natural history of the disease has not been studied in detail previously. The main objective is to map the natural course of the visual and hearing deterioration in Usher Syndrome 2 and USH2A associated nsRP for upcoming genetic therapy studies. Secondary objectives are: 1) To determine the necessary type of (combined) examinations, the sample size and length of studies (in years) essential to evaluate future genetic therapy in Usher syndrome. 2) To improve counselling of patients with Usher syndrome type 2 and USH2A associated nsRP with detailed information on the prognosis. 3) To identify additional etiological factors that explain variability in hearing impairment by adding questionnaires and psychophysical audiometric tests; and to assess the vestibular phenotype in Usher syndrome type 2 and USH2A associated nsRP patients. This is a longitudinal, prospective natural history study. The study population consists of healthy human volunteers, 16 - 55 yr old with a confirmed genetic diagnosis of Usher Syndrome type 2 or and USH2A associated nsRP. The main study endpoint is the natural course of the visual and hearing deterioration in Usher Syndrome type 2 and USH2A associated nsRP, over a time span of 4 years. There are no risks associated with participation.


Recruitment information / eligibility

Status Active, not recruiting
Enrollment 36
Est. completion date March 2, 2024
Est. primary completion date March 2, 2024
Accepts healthy volunteers No
Gender All
Age group 16 Years to 55 Years
Eligibility Inclusion Criteria: - Clinically diagnosed with rod-cone degeneration and at least two; pathogenic or likely pathogenic mutations in one of the Usher type 2 genes; - Willing and able to complete the informed consent process; - Ability to return for all study visits over 48 months; - Age = 16 years. Both eyes must meet all of the following: - Clinical diagnosis of a rod-cone degeneration; - Clear ocular media and adequate pupil dilation to permit good quality photographic imaging; - Ability to perform kinetic and static perimetry reliably; - Baseline visual acuity ETDRS letter score of 54 or more [approximate Snellen equivalent 20/80 or better]; - Stable fixation; - Clinically determined [on Octopus 900 Pro] kinetic visual field III4e area 7,5°, or more in the study eye. Exclusion Criteria: - Mutations in genes that cause autosomal dominant RP, X-linked RP, or presence of biallelic mutations in autosomal recessive RP/retinal dystrophy genes other than Usher genes; - Expected to enter experimental treatment trial at any time during this study History of more than 1 year of cumulative treatment, at any time, with an agent associated with pigmentary retinopathy (including hydroxychloroquine, chloroquine, thioridazine, and deferoxamine). If either eye has any of the following, the patient is not eligible: - Current vitreous hemorrhage; - Current or any history of rhegmatogenous retinal detachment; - Current or any history of (e.g., prior to cataract or refractive surgery) spherical equivalent of the refractive error worse than -8 Diopters of myopia; - History of intraocular surgery (e.g., cataract surgery, vitrectomy, penetrating keratoplasty, or LASIK) within the last 3 months; - Current or any history of confirmed diagnosis of glaucoma (e.g., based on glaucoma visual field, nerve changes, or glaucoma filtering surgery); - Current or any history of retinal vascular occlusion or proliferative diabetic retinopathy; - Expected to have cataract removal surgery during the study; - History or current evidence of ocular disease that, in the opinion of the investigator, may confound assessment of visual function; - History of treatment for retinitis pigmentosa that could affect the progression of retinal degeneration (including participation in a clinical trial within the last year or a retained drug delivery device). If either ear has any of the following, the patient is not eligible: - The audiometric PTA(1-2-4kHz) for the best hearing ear should not exceed 75dB HL; - Patients with bilateral cochlear implants cannot participate in the study; - A planned, second, cochlear implantation during the study.

Study Design


Intervention

Other:
No intervention
No intervention

Locations

Country Name City State
Netherlands Radboud universitair medisch centrum Nijmegen Gelderland

Sponsors (2)

Lead Sponsor Collaborator
Radboud University Medical Center Stichting Ushersyndroom

Country where clinical trial is conducted

Netherlands, 

Outcome

Type Measure Description Time frame Safety issue
Primary Change in perceived visual functioning Measured by the Visual Functioning Questionnaire-48 (VFQ-48): score of difficulty of performing 48 activities (items). The score is determined using two formulas: 'average item score = total item scores / (48 - U)' in which activities for which a person has non-visual reasons not to do it or in which they are not interested are scored with 'U', and '0.9*LN((2.34-average item score) / (average item score+2.22))+0.05'. The higher the score, the lower the perceived visual functioning. Baseline, 2 years and study completion at 4 years
Primary Change in perceived handicap due to hearing impairment Measured by the Speech, Spatial and Qualities of Hearing Scale (SSQ): range 0-500, the higher the score, the fewer the perceived handicap due to hearing impairment. Baseline, 2 years and study completion at 4 years
Primary Change in perceived handicap due to dizziness Measured by the Dizziness Handicap Inventory (DHI): range 0-100, the higher the score, the greater the perceived handicap due to dizziness.1. Pure tone audiometry and speech audiometry Baseline, 2 years and study completion at 4 years
Primary Change in lifestyle adjustment due to Usher syndrome. Measured by the Usher lifestyle survey: qualitative questionnaire, no quantitative measures Baseline, 2 years and study completion at 4 years
Primary Change in perceived health Measured by the 12-item Short-Form Health Survey (SF-12): 12 items with ranges 3-6, transformation of scores: ((patient score - lowest possible score)/range of scores)) * 100, the higher the score, the greater the perceived health. Baseline, 2 years and study completion at 4 years
Primary Change in the indication of depressive symptoms Measured by the Patient Health Questionnaire Mood Scale (PHQ-9): range 0-27, the higher the score, the greater the indication of depressive symptoms. Baseline, 2 years and study completion at 4 years
Primary Change in overall condition of the eye Measured by full ophthalmic exam. Baseline and every year until study completion at 4 years
Primary Change in visual acuity Measured by best-corrected visual acuity. Baseline and every year until study completion at 4 years
Primary Change in visual fields area Measured by dynamic perimetry with topographical analysis. Baseline and study completion at 4 years
Primary Change in visual fields sensitivity Measured by static perimetry with topographical analysis. Baseline and every year until study completion at 4 years
Primary Change in mean retinal sensitivity Measured by fundus-guided microperimetry. Baseline and every year until study completion at 4 years
Primary Change in ellipsoid zone (EZ) area Measured by optical coherence tomography (SD-OCT). Baseline and every year until study completion at 4 years
Primary Change in retinal autofluorescence and Robson ring size Measured by fundus autofluorescence imaging. Baseline and every year until study completion at 4 years
Primary Change in condition of the retina, macula, optic nerve and ocular vascularization Measured by assessing stereo color fundus photography. Baseline and every year until study completion at 4 years
Primary Change in rod- and cone-mediated retinal function Measured by full-field stimulus testing (FST). Baseline and every year until study completion at 4 years
Primary Change in retinal function Measured by full field electroretinogram amplitudes and timing in response to rod- and cone-specific stimuli. Baseline and study completion at 4 years
Primary Change in hearing thresholds Measured by pure tone audiometry (PTA) and speech audiometry. Baseline and study completion at 4 years
Primary Change in auditory speech recognition abilities in noise Measured by the digits in noise test (DIN). Baseline and study completion at 4 years
Primary Change in integrity of the outer hair cells Measured by otoacoustic emissions (OAEs). Baseline and study completion at 4 years
Primary Change in integrity of the inner hair cells, the synapse and the first stage on the auditory nerve Measured by electrocochleography (ECochG). Baseline and study completion at 4 years
Primary Vestibular function Measured by rotational chair test and calorisation. 3 years
Primary Function of individual vestibular semicircular canals Measured by video head impulse test (HIT) test. 3 years
Primary Function of saccule and utricule of the vestibular organ Measured by vestibular evoked myogenic potential (VEMP) test. 3 years
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