Safety and Efficacy of Emixustat in Stargardt Disease
- Registration Number
- NCT03772665
- Lead Sponsor
- Kubota Vision Inc.
- Brief Summary
The purpose of this study is to determine if emixustat hydrochloride reduces the rate of progression of macular atrophy compared to placebo in subjects with Stargardt disease.
Funding Source -- FDA OOPD
- Detailed Description
Stargardt disease is a rare, inherited degenerative disease of the retina affecting approximately 1 in 8000 to 10 000 people and is the most common type of hereditary macular dystrophy. There are no approved treatments for STGD. This disease is characterized by an excessive accumulation of lipofuscin at the level of the retinal pigment epithelium (RPE). Lipofuscin is made of lipids, proteins, and toxic bis retinoids (such as N retinylidene N retinylethanolamine \[A2E\]). Accumulation of the toxic bis retinoids found in lipofuscin is thought to cause RPE cell dysfunction and eventual apoptosis, resulting in photoreceptor death and loss of vision.
Stargardt disease has several sub types, where autosomal recessive STGD (STGD1) accounts for the majority (\>95%) of all cases. STGD1 is typically diagnosed in the first 3 decades of life and is caused by mutations of the adenosine triphosphate binding cassette subfamily A member 4 (ABCA4) gene. The ABCA4 gene product transports N retinylidene phosphatidylethanolamine (a precursor of toxic bis retinoids) from the lumen side of photoreceptor disc membranes to the cytoplasmic side where the retinal is hydrolyzed from phosphatidylethanolamine. Mutations of the ABCA4 gene result in accumulation of this precursor in disc membranes that are eventually phagocytized by RPE cells, where the precursors are converted into toxic bis retinoids such as A2E. In addition to being a precursor to A2E, all trans retinal has also been implicated in the pathogenesis of STGD through its role in light-mediated toxicity.
Emixustat hydrochloride (emixustat) has been developed by Acucela Inc. for retinal diseases including Stargardt disease (STGD). Emixustat is a potent inhibitor of RPE65 isomerization activity and reduces visual chromophore (11 cis retinal) production in a dose-dependent and reversible manner. Because 11 cis-retinal and its photoproduct (all trans retinal) are substrates for biosynthesis of retinoid toxins (eg, A2E), chronic treatment with emixustat retards the rate at which these toxins accumulate.
Recruitment & Eligibility
- Status
- COMPLETED
- Sex
- All
- Target Recruitment
- 194
- A clinical diagnosis of macular atrophy secondary to Stargardt disease (STGD)
- Macular atrophy measured to fall within a defined size range
- Two mutations of the ABCA4 gene. If only one mutation, a typical STGD appearance of the retina.
- Visual acuity in the study eye of at least 20/320
- Macular atrophy secondary to a disease other than STGD
- Mutations of genes, other than ABCA4, that are associated with retinal degeneration
- Surgery in the study eye in the past 3 months
- Prior participation in a gene therapy or stem cell clinical trial for STGD
- Recent participation in a clinical trial for STGD evaluating a complement inhibitor or vitamin A derivative
- Use of certain medications in the past 4 weeks that might interfere with emixustat
- An abnormal electrocardiogram (ECG)
- Certain abnormalities on laboratory blood testing
- Female subjects who are pregnant or nursing
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Arm && Interventions
Group Intervention Description Placebo Placebo Includes identical tablets with only inactive ingredients (0 mg). Emixustat Emixustat 10 mg
- Primary Outcome Measures
Name Time Method Mean Rate of Change in Total Area of Macular Atrophy, as Measured by Fundus Autofluorescence (FAF) 24 months Mean rate of change in total area of macular atrophy, as measured by fundus autofluorescence (FAF)
- Secondary Outcome Measures
Name Time Method
Trial Locations
- Locations (29)
The Wilmer Eye Institute Johns Hopkins University
๐บ๐ธBaltimore, Maryland, United States
Emory University
๐บ๐ธAtlanta, Georgia, United States
Retina-Vitreous Associates Medical Group
๐บ๐ธBeverly Hills, California, United States
Mayo Clinic Rochester
๐บ๐ธRochester, Minnesota, United States
University of Michigan Kellogg Eye Center
๐บ๐ธAnn Arbor, Michigan, United States
Casey Eye Institute - OHSU
๐บ๐ธPortland, Oregon, United States
Retina Foundation of the Southwest
๐บ๐ธDallas, Texas, United States
Medical College of Wisconsin-Eye Institute
๐บ๐ธMilwaukee, Wisconsin, United States
Hospital Sao Paulo
๐ง๐ทSรฃo Paulo, Brazil
Service D'Ophtalmologie Chi Creteil
๐ซ๐ทCrรฉteil, รle-de-France, France
CHNO Quinze-Vingts - CIC
๐ซ๐ทParis, รle-de-France, France
Universitร Cattolica del Sacro Cuore - Fondazione Policlinico Gemelli
๐ฎ๐นRome, Lazio, Italy
UOC Oculistica Asst Fatebene Pratelli Sacco Universita delgi Studi di Milano
๐ฎ๐นMilan, Lombardy, Italy
Fundacion Jimenez Diaz University Hospital
๐ช๐ธMadrid, Spain
Radboud University Medical Center
๐ณ๐ฑNijmegen, Gelderland, Netherlands
Pretoria Eye Institute
๐ฟ๐ฆPretoria, Gauteng, South Africa
Moorfields Eye Hospital NHS Foundation Trust
๐ฌ๐งLondon, United Kingdom
Oxford Eye Hospital,Oxford University Hospitals NHS Foundation Trust
๐ฌ๐งOxford, Oxfordshire, United Kingdom
IRCCS Ospedale San Raffaele
๐ฎ๐นMilan, Lombardy, Italy
SODC di Oculistica AOU Careggi
๐ฎ๐นFlorence, Tuscany, Italy
UCSF Dept. of Ophthalmology
๐บ๐ธSan Francisco, California, United States
Duke Eye Center
๐บ๐ธDurham, North Carolina, United States
University of Utah John Moran Eye Center
๐บ๐ธSalt Lake City, Utah, United States
Santa Casa de Misericรณrdia de Belo Horizonte
๐ง๐ทBelo Horizonte, Minas Gerais, Brazil
Universitรคtsklinikum Tรผbingen, Department fรผr Augenheilkunde
๐ฉ๐ชTรผbingen, Baden-Wรผrttemberg, Germany
The Hospital for Sick Children
๐จ๐ฆToronto, Ontario, Canada
Rigshospitalet-Glostrup
๐ฉ๐ฐGlostrup, Hovedstaden, Denmark
Universitรคts-Augenklinik Bonn
๐ฉ๐ชBonn, Germany
AOU Universitร della Campania Luigi Vanvitelli
๐ฎ๐นNaples, Campania, Italy