Disease #01189 (SCRA (atrophy, chorioretinal, Sveinsson (SCRA)), OMIM:108985)

Official abbreviation	SCRA
Name	atrophy, chorioretinal, Sveinsson (SCRA)
OMIM ID	108985
Human Phenotype Ontology Project (HPO)	HPO
Inheritance	Autosomal dominant
Individuals reported having this disease	6
Phenotype entries for this disease	6
Associated with 1 gene	TEAD1
Associated tissues	-
Disease features	-
Remarks	-
Date created	2014-09-25 23:29:40 +02:00 (CEST)
Date last edited	2020-11-26 19:25:04 +01:00 (CET)

Individuals

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ID_report: ID of the individual that can be publically shared, e.g. as listed in a publication

Reference: reference to publication describing the individual/family, possibly giving more phenotypic details than listed in this database entry, incl. link to PubMed or other source, e.g. "den Dunnen ASHG2003 P2346"

Remarks: remarks about the individual

Gender: gender individual
All options:

? = unknown
- = not applicable
F = female
M = male
rF = raised as female
rM = raised as male

Consanguinity: indicates whether the parents are related (consanguineous), not related (non-consanguineous) or whether consanguinity is not known (unknown)
All options:

no = non-consanguineous parents
yes = consanguineous parents
likely = consanguinity likely
? = unknown
- = not applicable

Country: where (country) does the individual live/recently came from. Give additional details (population, specific sub-group) and when parents come from different countries in "Population". Belgium = individual lives in/recently came from Belgium, (France) = reported by laboratory in France, individual's country of origin not sure
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Population: population the individual (or ancestors) belongs to; e.g. white, gypsy, Jewish-Ashkenazi, Africa-N, Sardinia, etc.

Age at death: age at which the individual deceased (when applicable):

35y = 35 years
>43y = still alive at 43y
04y08m = 4 years and 8 months
00y00m01d12h = 1 day and 12 hours
18y? = around 18 years
30y-40y = between 30 and 40 years
>54y = older than 54
? = unknown

VIP: individual/phenotype VIP-status was requested for matchmaking - need collaboration(s) to crack the case - please contact the submitter/curator. NOTE: to get VIP status ask the curator.

Data_av: are additional data available upon request: e.g. pedigree (yes/no/?)

Treatment: treatment of patient

Variants in genes: The individual has variants for this gene.

Panel size: Number of individuals this entry represents; e.g. 1 for an individual, 5 for a family with 5 affected members.

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6 entries on 1 page. Showing entries 1 - 6.

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Individual ID	ID_report	Reference	Remarks	Gender	Consanguinity	Country	Population	Age at death	VIP	Data_av	Treatment	Disease	Phenotype details	Genes screened	Variants in genes	Variants	Panel size	Owner
00372393	family	PubMed: Fossdale 2004	81 patients from 10 related families	F;M	-	Iceland	-	-	-	-	-	SCRA	see paper; ..., symmetrical lesions radiating from the optic disc involving retina and choroid	TEAD1	TEAD1	1	81	Johan den Dunnen
00417484	?	PubMed: Jonasson 2007	-	F	-	-	Icelandic	82y	-	-	-	SCRA	congenital anterior polar cataracts and Sveinsson chorioretinal atrophy from childhood lost central vision in both eyes within 1 year because of the extension of Sveinsson chorioretinal atrophy into the macula; intravenous fluorescein angiography: the most severely affected areas apparently lacked retinal pigment epithelium (RPE) and a choroidal vasculature, in less severely affected areas, the RPE and choriocapillaris absent but some choroidal blood vessels still present; at some sites in the transitional zone between affected and apparently healthy tissue, some fluorescein leakage apparent from the margins of a still-functioning choriocapillaris; retinal blood vessels unaffected. Eyes enucleated within 4 hours of death at the age of 82 years, right eye fixed in formalin for light microscopy; light microscopy: the macroscopic changes reflected atrophy of the sensory retina and choroid and a loss of RPE; none of the examined retinal tissue had a multilayered ganglion cell layer; macular region and fovea could not be identified, abnormalities most conspicuous in the areas of total RPE atrophy and somewhat less marked in the zones between the atrophic and normal sensory retina; at the margin of some affected areas, only RPE and the photoreceptor outer segment junctions affected; portions of the posterior retina extremely well preserved, in sharp contrast to the degenerated sensory retina; at the margin between apparently normal and atrophic retina, a portion of the retina contained small eosinophilic globular material apparently derived from photoreceptors, adjacent to a multilayered RPE that seemed to contain multinucleated cells and may reflect a tangential section through the retina; severely degenerated sensory retina rested on a thin Bruch’s membrane that devoid of a normally attached RPE; in the more severely affected areas, the sensory retina, RPE, and choriocapillaris absent, exposing an extremely thin atrophic choroid with very few melanocytes and a naked sclera; Bruch’s membrane in the vicinity of theic nerve head: several focal thickenings and excrescences; discrete atrophic areas of the posterior sensory retina characterized by degenerate retinal cells adherent to the underlying choroid, in contrast to normal eyes, in which the sensory retina is separated from the RPE by a potential space that typically becomes accentuated because of the artifactual separation of these structures in eyes studied after death; the peripheral sensory retina not adherent to the attenuated RPE. Histopathologic observations: some transitions between affected and unaffected areas, both the RPE and the outer segments of the photoreceptors ended abruptly, but the nuclei of the photoreceptors retained a normal appearance slightly further into the more severely affected area; other areas in the posterior pole affected similarly, except that the RPE immediately terminated, whereas the outer segments of the photoreceptors persisted further toward the peripheral retina; advanced changes included a disappearance of the RPE, photoreceptors, and choriocapillaris, and when Bruch’s membrane could be identified, it thin and the adjacent choriocapillaris atrophic; most advanced areas: all layers between the bipolar neurons and the sclera absent; peripheral retina contained areas without photoreceptors, underlying individual cells of the RPE sparse and attenuated, much thinner than normal but still formed a continuous layer beneath the photoreceptors in the peripheral retina; optic nerve: normal in cross sections, diameter half to two thirds of normal and the subarachnoid space wider than normal, but well myelinated, indicating hypoplasia rather than atrophy of the optic ; lens cataractous, but the remainder of the eye essentially unremarkable and within the normal limits expected for the patient’s age; inflammatory cells: not detected in any of the tissue sect	TEAD1	TEAD1	1	1	LOVD
00417489	Case 2	PubMed: Tosi 2009	proband's mother, the only family member to be screened for mutation - segregation unknown; Case 1 (daughter) and Case 3 (mother) not genetically tested	F	-	-	-	-	-	-	-	SCRA	uncorrected visual acuity right, left eye: 20/25+2, 20/20; anterior segmen: unremarkable without anterior polar cataracts; funduscopy: characteristic chorioretinal atrophy lesions radiating from the optic discs; peripapillary choroidal-retinal atrophy was symmetric in both eyes; no signs of macular edema; scanning laser ophthalmoscopy: autofluorescent pattern was consistent with retinal pigment epithelium and choroidal atrophy along the peripapillary region in both eye; autofluorescent hyperdensity along the edge of the chorioretinal degeneration secondary to the retinal pigment epithelium atrophy; optical coherence tomography examination showed only a remaining thin layer of Bruch��s membrane after retinal pigment epithelium loss, larger choroidal vessels visible through this area devoid of retinal pigment epithelium cells; electroreti	TEAD1	TEAD1	1	1	LOVD
00417490	1	PubMed: Grubisa 2021	Serbian family, father; more detailed clinical findings in Milenkovic et al.,2005	M	-	Bosnia and Herzegovina	Serbian	-	-	-	-	SCRA	-	TEAD1	TEAD1	1	1	LOVD
00417491	2	PubMed: Grubisa 2021	Serbian family, daughter; more detailed clinical findings in Milenkovic et al.,2006	F	-	Bosnia and Herzegovina	Serbian	-	-	-	-	SCRA	-	TEAD1	TEAD1	1	1	LOVD
00417492	3	PubMed: Grubisa 2021	Serbian family, son; more detailed clinical findings in Milenkovic et al.,2007	M	-	Bosnia and Herzegovina	Serbian	-	-	-	-	SCRA	-	TEAD1	TEAD1	1	1	LOVD

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Global Variome shared LOVD