Stargardt disease

Stargardt disease
Classification and external resources
Specialty	ophthalmology
ICD-10	H35.5
OMIM	248200 600110 603786
DiseasesDB	31282

Stargardt disease, or fundus flavimaculatus, is an inherited form of juvenile macular degeneration that causes progressive vision loss usually to the point of legal blindness. Several genes are associated with the disorder. Symptoms, mainly vision loss, typically develop before age 20, and also include wavy vision, blind spots, blurriness, impaired color vision, and difficulty adapting to dim lighting.

Characteristics and symptoms

The main symptom of Stargardt disease is loss of visual acuity, which ranges from 20/50 to 20/200.^[1] Other symptoms include wavy vision, blind spots, blurriness, impaired color vision, and difficulty adapting to dim lighting.^[2]^[3] The disease causes sensitivity to glare; overcast days offer some relief. Vision is most noticeably impaired when the macula (center of retina and focus of vision) is damaged, leaving peripheral vision more intact. Generally, vision loss starts within the first 20 years of life.^[4]

Genetics

Stargardt disease is associated with several different genes:

STGD1: The most common form of Stargardt disease is the recessive form caused by mutations in the ABCA4 gene. It can also be associated with CNGB3.
STGD3: There is also a rare dominant form of Stargardt disease caused by mutations in the ELOVL4 gene.
STGD4: Associated with PROM1.

The classification "STGD2" is no longer used.

Pathophysiology

In STGD1, the genetic defect is manifest in the visual phototransduction cycle. The ATP-binding cassette transporter (ABCA4) is defective and leads to rapid formation of toxic vitamin A dimers (also known as bisretinoids), which then build up in fluorescent granules called lipofuscin in the retinal pigmented epithelium of the retina.

In STGD4, a butterfly pattern of dystrophy is caused by mutations in a gene that encodes a membrane bound protein that is involved in the elongation of very long chain fatty acids (ELOVL4).

Treatment

Currently, there is no treatment for the disease. However, ophthalmologists recommend wearing sunglasses and hats outdoors and blue-light blocking glasses when exposed to artificial light sources, such as screens and lights.Tobacco smoke and second-hand smoke should be avoided. Animal studies also show that high doses of vitamin A can be detrimental by building up more lipofuscin toxin. Dietary non-supplemental vitamin A intake may not further the disease progression. Clinical trials are being conducted with promising early results. The trials may one day lead to treatments that might halt, and possibly even reverse, the effects of Stargardt disease using stem cell therapy.^[5]

Prognosis

The long-term prognosis for patients with Stargardt disease is widely variable although the majority of people will progress to legal blindness.^[1]

Stargardt disease has no impact on general health and life expectancy is normal.^[6] Some patients are able to drive.

Epidemiology

STGD1 is the most common form of inherited juvenile macular degeneration with a prevalence of approximately 1 in 10,000 births.^[2]

Research

Treatment modalities currently under clinical investigation include cell therapy, gene therapy and oral therapies. Anecdotal evidence suggests that new technology called esight may help some individuals with Stargardt who retain some visual function, recover vision.^[7]

On November 22, 2010, it was announced that Advanced Cell Technology,^[8] now called Ocata Therapeutics, received United States Food and Drug Administration clearance to immediately initiate a Phase I/II multicenter clinical trial using retinal cells derived from human embryonic stem cells (hESCs) to treat patients with Stargardt’s Macular Dystrophy. In September 2011, ACT announced they were beginning the next stage of treatment for SMD, and Dry AMD as the first stage proved to be safe by an independent board of experts.^[9] In March 2013, after treating and collecting data on 18 patients, Advanced Cell was given approval to test its stem cell therapy on patients with 20/100 vision.^[10] In October 2014, the results of the Phase I/II clinical trial were published in the Lancet.^[11]

Gene therapy trials are also on-going. During gene therapy, a working copy of the ABCA4 gene is incorporated in a lentivirus (an inactivated virus which transports the working copy of the gene) and injected into the eye through a subretinal injection. It is hoped that such injection, if performed early enough, could prevent the progression of the disease.

Finally, oral therapies that are being investigated include ALK-001, modified vitamin A delivered orally which prevents the formation of toxic vitamin A dimers in the eye. ALK-001 has completed a phase 1 clinical trials.

ACT, Oxford Biomedica and Alkeus Pharmaceuticals have all received orphan drug designation in the United States for the treatment of Stargardt Disease.

Preclinical research include a new compound that can remove lipofuscin from retinal pigment epithelial cells.^[12] The compound drug has been granted orphan drug designation for the treatment of Stargardt disease by the European Medicines Agency.

History

The disease was discovered in 1909 by Karl Stargardt, a Berlin ophthalmologist.^[13]^[14]

In 1997, it was discovered that mutations in the ABCA4 gene cause Stargardt disease. The mutations cause the production of a dysfunctional protein that cannot perform energy transport to and from photoreceptor cells in the retina. The photoreceptor cells then degenerate, causing vision loss.^[2]

References

1 2 Yanoff, Myron; Duker, Jay S. (2008). Ophthalmology (3rd ed.). Edinburgh: Mosby. pp. 560–562. ISBN 978-0323057516.
1 2 3 Stargardt Disease
↑ "Stargardt's". Lowvision.org. 1997-03-03. Retrieved 2012-12-05.
↑ "Stargardt's Disease (Fundus Flavimaculatus)". allaboutvision.com. allaboutvision.com. Retrieved 2015-08-30.
↑
↑ Stargardt Disease from The University of Arizona College of Medicine, Department of Ophthalmology and Vision Science. Retrieved Jan 2012
↑
↑ "Advanced Cell Technology Receives FDA Clearance For the First Clinical Trial Using Embryonic Stem Cells to Treat Macular Degeneration". Advanced Cell Technology.
↑ "ACT Receives Approval from Data and Safety Monitoring Board (DSMB) to Treat Next Patients in Stem Cell Clinical Trials". Advanced Cell Technology. Retrieved 2012-12-05.
↑ "Advanced Cell Technology Receives Approval from Data Safety Monitoring Board (DSMB) to Initiate Treatment of Third Patient Cohort in All Three Clinical Trials". Advanced Cell Technology. 2013-03-14. Retrieved 2013-03-17.
↑ http://download.thelancet.com/flatcontentassets/pdfs/S0140673614613763.pdf
↑ Julien S, Schraermeyer U (Oct 2012). "Lipofuscin can be removed from the retinal pigment epithelium of monkeys". Neurobiol Aging 33 (10): 2390–7. doi:10.1016/j.neurobiolaging.2011.12.009.
↑ synd/2306 at Who Named It?
↑ K. B. Stargardt. Über familiäre, progressive Degeneration in der Makulagegend des Auges. Albrecht von Graefes Archiv für Ophthalmologie, 1909, 71: 534-550.

External links

Stargardt's Disease - from the American Macular Degeneration Foundation
Stargardt's Disease - from TheRetinaSource
Stem Cell Research NPR Special Report - from NPR

Adnexa

Eyelid

Inflammation	Stye Chalazion Blepharitis

Entropion Ectropion Lagophthalmos Blepharochalasis Ptosis Blepharophimosis Xanthelasma

Eyelash	Trichiasis Madarosis

Sclera	Scleritis Episcleritis

Cornea	Keratitis herpetic acanthamoebic fungal Corneal ulcer Photokeratitis Thygeson's superficial punctate keratopathy Corneal dystrophy Fuchs' Meesmann Corneal ectasia Keratoconus Pellucid marginal degeneration (PMD) Keratoglobus Terrien's marginal degeneration Keratoconjunctivitis sicca Corneal neovascularization Kayser–Fleischer ring Haab's striae Arcus senilis Band keratopathy

Vascular tunic

Iris Ciliary body	Uveitis Intermediate uveitis Hyphema Rubeosis iridis Persistent pupillary membrane Iridodialysis Synechia

Choroid	Choroideremia Choroiditis Chorioretinitis

Lens

Retina

Other

Pathways

Optic nerve
Optic disc

Optic neuritis optic papillitis Papilledema Foster Kennedy syndrome Optic atrophy Optic disc drusen

Optic neuropathy	Ischemic anterior (AION) posterior (PION) Kjer's Leber's hereditary Toxic and nutritional

Strabismus
Extraocular muscles
Binocular vision
Accommodation

Paralytic strabismus

Ophthalmoparesis Chronic progressive external ophthalmoplegia Kearns–Sayre syndrome

palsies	Oculomotor (III) Fourth-nerve (IV) Sixth-nerve (VI)

Other strabismus

Other binocular

Refraction

Vision disorders
Blindness

Amblyopia Leber's congenital amaurosis Diplopia Scotoma Color blindness Achromatopsia Dichromacy Monochromacy Nyctalopia Oguchi disease Blindness / Vision loss / Visual impairment

Anopsia	Hemianopsia binasal bitemporal homonymous Quadrantanopia

subjective	Asthenopia Hemeralopia Photophobia Scintillating scotoma

Pupil

Other

Infections

Trachoma Onchocerciasis

Genetic disorder, membrane: ABC-transporter disorders

ABCA	ABCA1 (Tangier disease) ABCA3 (Surfactant metabolism dysfunction 3) ABCA4 (Stargardt disease 1, Retinitis pigmentosa 19) ABCA12 (Harlequin-type ichthyosis, Lamellar ichthyosis 2)

ABCB	ABCB4 (Progressive familial intrahepatic cholestasis 3) ABCB7 (ASAT) ABCB11 (Progressive familial intrahepatic cholestasis 2)

ABCC	ABCC2 (Dubin–Johnson syndrome) ABCC6 (Pseudoxanthoma elasticum) ABCC7 (Cystic fibrosis) ABCC8 (HHF1, TNDM2) ABCC9 (Dilated cardiomyopathy 1O)

ABCD	ABCD1 (Adrenoleukodystrophy, Adrenomyeloneuropathy)

ABCG	ABCG5 (Sitosterolemia) ABCG8 (Gallbladder disease 4, Sitosterolemia)

see also ABC transporters

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