Negative-Configuration Electroretinogram in Oregon Eye Disease: Consistent Phenotype in Xp21 Deletion Syndrome

De Ann M. Pillers; William K. Seltzer; Berkley R. Powell; Peter N. Ray; François Tremblay; G. Robert Roche; Richard Alan Lewis; Edward R.B. Mccabe; Aldur W. Eriksson; Richard G. Weleber

doi:10.1001/archopht.1993.01090110124037

Negative-Configuration Electroretinogram in Oregon Eye Disease: Consistent Phenotype in Xp21 Deletion Syndrome

De Ann M. Pillers, William K. Seltzer, Berkley R. Powell, Peter N. Ray, François Tremblay, G. Robert Roche, Richard Alan Lewis, Edward R.B. Mccabe, Aldur W. Eriksson, Richard G. Weleber

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23 Citations (Scopus)

Résumé

To determine whether abnormal configurations on electroretinogram were a consistent finding in patients with Xp21 deletion and to characterize the associated ophthalmologic phenotype. Case series. University hospitals and eye institutes. Five patients with complex glycerol kinase deficiency (Duchenne-type or Becker's muscular dystrophy, glycerol kinase deficiency, and congenital adrenal hypoplasia) and demonstrated chromosomal deletions at Xp21. Control patients were matched by age. Clinical information was obtained from medical records. Complete ophthalmologic examinations were performed. Electroretinography was performed using a Ganzfeld technique and chloral hydrate sedation. We report the clinical features and abnormal configurations on electroretinograms of five patients with complex glycerol kinase deficiency, including follow-up studies on a previously described patient. The original patient had ocular hypopigmentation; four, strabismus; two, myopia; three, astigmatism; and one, symptomatic night blindness. All had negative configurations on scotopic electroretinograms showing a reduced-amplitude B wave in the dark-adapted state. Our original report suggested a diagnosis of Åland Island eye disease, which appears to be an incomplete form of congenital stationary night blindness. Linkage data place Åland Island eye disease and congenital stationary night blindness at Xp11, whereas our patients had deletions at Xp21. The phenotype reported here may represent the effects of a single gene defect or the compound effects of the Xp21 contiguous gene syndrome (complex glycerol kinase deficiency). The phenotype is referred to as Oregon eye disease.

Langue d'origine	English
Pages (de-à)	1558-1563
Nombre de pages	6
Journal	Archives of Ophthalmology
Volume	111
Numéro de publication	11
DOI	https://doi.org/10.1001/archopht.1993.01090110124037
Statut de publication	Published - nov. 1993
Publié à l'externe	Oui

Note bibliographique

Funding Information:
Accepted jor publication April 22, 1993. ThisstudywassupportedinpartbyfundsfromtheNa¬ tionalRetinitisPigmentosaFoundationFightingBlindness,Bal¬ timore, Md (DrsPiliers, Lewis, andWeleber);an unrestricted grantfromResearchtoPreventBlindness,NewYork,NY(Dr Lewis), grant ROI HD22563from the National Institute of Child Health and HumanDevelopment,Bethesda,Md(Dr McCabe);grantRR00069fromNationalInstituteofRe¬ DevelopmentandRehabilitationCenter,Portland,searchResources,Bethesda,Md(DrSeltzer);and by Ore.the Child

ASJC Scopus Subject Areas

Ophthalmology

PubMed: MeSH publication types

Case Reports
Journal Article
Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, P.H.S.

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10.1001/archopht.1993.01090110124037

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Pillers, D. A. M., Seltzer, W. K., Powell, B. R., Ray, P. N., Tremblay, F., Roche, G. R., Lewis, R. A., Mccabe, E. R. B., Eriksson, A. W., & Weleber, R. G. (1993). Negative-Configuration Electroretinogram in Oregon Eye Disease: Consistent Phenotype in Xp21 Deletion Syndrome. Archives of Ophthalmology, 111(11), 1558-1563. https://doi.org/10.1001/archopht.1993.01090110124037

@article{1eae339d767f44bdb4a9ff36d0b3a91f,

title = "Negative-Configuration Electroretinogram in Oregon Eye Disease: Consistent Phenotype in Xp21 Deletion Syndrome",

abstract = "To determine whether abnormal configurations on electroretinogram were a consistent finding in patients with Xp21 deletion and to characterize the associated ophthalmologic phenotype. Case series. University hospitals and eye institutes. Five patients with complex glycerol kinase deficiency (Duchenne-type or Becker's muscular dystrophy, glycerol kinase deficiency, and congenital adrenal hypoplasia) and demonstrated chromosomal deletions at Xp21. Control patients were matched by age. Clinical information was obtained from medical records. Complete ophthalmologic examinations were performed. Electroretinography was performed using a Ganzfeld technique and chloral hydrate sedation. We report the clinical features and abnormal configurations on electroretinograms of five patients with complex glycerol kinase deficiency, including follow-up studies on a previously described patient. The original patient had ocular hypopigmentation; four, strabismus; two, myopia; three, astigmatism; and one, symptomatic night blindness. All had negative configurations on scotopic electroretinograms showing a reduced-amplitude B wave in the dark-adapted state. Our original report suggested a diagnosis of {\AA}land Island eye disease, which appears to be an incomplete form of congenital stationary night blindness. Linkage data place {\AA}land Island eye disease and congenital stationary night blindness at Xp11, whereas our patients had deletions at Xp21. The phenotype reported here may represent the effects of a single gene defect or the compound effects of the Xp21 contiguous gene syndrome (complex glycerol kinase deficiency). The phenotype is referred to as Oregon eye disease.",

author = "Pillers, {De Ann M.} and Seltzer, {William K.} and Powell, {Berkley R.} and Ray, {Peter N.} and Fran{\c c}ois Tremblay and Roche, {G. Robert} and Lewis, {Richard Alan} and Mccabe, {Edward R.B.} and Eriksson, {Aldur W.} and Weleber, {Richard G.}",

note = "Funding Information: Accepted jor publication April 22, 1993. ThisstudywassupportedinpartbyfundsfromtheNa¬ tionalRetinitisPigmentosaFoundationFightingBlindness,Bal¬ timore, Md (DrsPiliers, Lewis, andWeleber);an unrestricted grantfromResearchtoPreventBlindness,NewYork,NY(Dr Lewis), grant ROI HD22563from the National Institute of Child Health and HumanDevelopment,Bethesda,Md(Dr McCabe);grantRR00069fromNationalInstituteofRe¬ DevelopmentandRehabilitationCenter,Portland,searchResources,Bethesda,Md(DrSeltzer);and by Ore.the Child",

year = "1993",

month = nov,

doi = "10.1001/archopht.1993.01090110124037",

language = "English",

volume = "111",

pages = "1558--1563",

journal = "Archives of Ophthalmology",

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T1 - Negative-Configuration Electroretinogram in Oregon Eye Disease

T2 - Consistent Phenotype in Xp21 Deletion Syndrome

AU - Pillers, De Ann M.

AU - Seltzer, William K.

AU - Powell, Berkley R.

AU - Ray, Peter N.

AU - Tremblay, François

AU - Roche, G. Robert

AU - Lewis, Richard Alan

AU - Mccabe, Edward R.B.

AU - Eriksson, Aldur W.

AU - Weleber, Richard G.

N1 - Funding Information: Accepted jor publication April 22, 1993. ThisstudywassupportedinpartbyfundsfromtheNa¬ tionalRetinitisPigmentosaFoundationFightingBlindness,Bal¬ timore, Md (DrsPiliers, Lewis, andWeleber);an unrestricted grantfromResearchtoPreventBlindness,NewYork,NY(Dr Lewis), grant ROI HD22563from the National Institute of Child Health and HumanDevelopment,Bethesda,Md(Dr McCabe);grantRR00069fromNationalInstituteofRe¬ DevelopmentandRehabilitationCenter,Portland,searchResources,Bethesda,Md(DrSeltzer);and by Ore.the Child

PY - 1993/11

Y1 - 1993/11

N2 - To determine whether abnormal configurations on electroretinogram were a consistent finding in patients with Xp21 deletion and to characterize the associated ophthalmologic phenotype. Case series. University hospitals and eye institutes. Five patients with complex glycerol kinase deficiency (Duchenne-type or Becker's muscular dystrophy, glycerol kinase deficiency, and congenital adrenal hypoplasia) and demonstrated chromosomal deletions at Xp21. Control patients were matched by age. Clinical information was obtained from medical records. Complete ophthalmologic examinations were performed. Electroretinography was performed using a Ganzfeld technique and chloral hydrate sedation. We report the clinical features and abnormal configurations on electroretinograms of five patients with complex glycerol kinase deficiency, including follow-up studies on a previously described patient. The original patient had ocular hypopigmentation; four, strabismus; two, myopia; three, astigmatism; and one, symptomatic night blindness. All had negative configurations on scotopic electroretinograms showing a reduced-amplitude B wave in the dark-adapted state. Our original report suggested a diagnosis of Åland Island eye disease, which appears to be an incomplete form of congenital stationary night blindness. Linkage data place Åland Island eye disease and congenital stationary night blindness at Xp11, whereas our patients had deletions at Xp21. The phenotype reported here may represent the effects of a single gene defect or the compound effects of the Xp21 contiguous gene syndrome (complex glycerol kinase deficiency). The phenotype is referred to as Oregon eye disease.

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Negative-Configuration Electroretinogram in Oregon Eye Disease: Consistent Phenotype in Xp21 Deletion Syndrome

Résumé

Note bibliographique

ASJC Scopus Subject Areas

PubMed: MeSH publication types

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