Abnormal rod dark adaptation in autosomal dominant retinitis pigmentosa with proline-23-histidine rhodopsin mutation

C. M. Kemp; S. G. Jacobson; A. J. Roman; C. H. Sung; J. Nathans

doi:10.1016/S0002-9394(14)71529-6

Abnormal rod dark adaptation in autosomal dominant retinitis pigmentosa with proline-23-histidine rhodopsin mutation

C. M. Kemp, S. G. Jacobson, A. J. Roman, C. H. Sung, J. Nathans

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Abstract

We studied rod and cone function in 13 patients from four families with autosomal dominant retinitis pigmentosa and the proline-23-histidine rhodopsin mutation. In patients with early stages of this disease, rod sensitivity was mildly abnormal throughout the retina and cone sensitivity was normal. In more severely affected patients, sensitivity loss varied with retinal region, some regions showing mild rod loss only and other regions having pronounced rod and cone dysfunction. Rhodopsin levels were decreased below normal by amounts that indicated the rod sensitivity loss was determined by the reduced ability to absorb light. The most characteristic abnormality of this genotype was a slowed rod branch of dark adaptation, which was present regardless of the extent or severity of disease. The time required for recovery of rod sensitivity was more than twice the normal time. These findings with dark-adapted perimetry, fundus reflectometry, and dark adaptometry showed intrafamilial and interfamilial consistency.

Original language	English (US)
Pages (from-to)	165-174
Number of pages	10
Journal	American journal of ophthalmology
Volume	113
Issue number	2
DOIs	https://doi.org/10.1016/S0002-9394(14)71529-6
State	Published - 1992
Externally published	Yes

ASJC Scopus subject areas

Ophthalmology

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@article{65c6063232494040b2b2541e420a75bd,

title = "Abnormal rod dark adaptation in autosomal dominant retinitis pigmentosa with proline-23-histidine rhodopsin mutation",

abstract = "We studied rod and cone function in 13 patients from four families with autosomal dominant retinitis pigmentosa and the proline-23-histidine rhodopsin mutation. In patients with early stages of this disease, rod sensitivity was mildly abnormal throughout the retina and cone sensitivity was normal. In more severely affected patients, sensitivity loss varied with retinal region, some regions showing mild rod loss only and other regions having pronounced rod and cone dysfunction. Rhodopsin levels were decreased below normal by amounts that indicated the rod sensitivity loss was determined by the reduced ability to absorb light. The most characteristic abnormality of this genotype was a slowed rod branch of dark adaptation, which was present regardless of the extent or severity of disease. The time required for recovery of rod sensitivity was more than twice the normal time. These findings with dark-adapted perimetry, fundus reflectometry, and dark adaptometry showed intrafamilial and interfamilial consistency.",

author = "Kemp, {C. M.} and Jacobson, {S. G.} and Roman, {A. J.} and Sung, {C. H.} and J. Nathans",

note = "Funding Information: From the Department of Ophthalmology, University of Miami School of Medicine, Bascom Palmer Eye Institute, Miami, Florida (Drs. Kemp and Jacobson and Mr. Roman); and Department of Molecular Biology and Genetics and Department of Neuroscience, Howard Hughes Medical Institute, Johns Hopkins University School ofMedicine, Baltimore, Maryland (Drs. Sung and Nathans). This study wassupported in part by Public Health Service research grant EY05627; the National Retinitis Pigmentosa Foundation, Inc., Baltimore, Maryland; The Chatlos Foundation, Inc., Longwood, Florida; and the Howard Hughes Medical Institute, Bethesda, Maryland. Dr. Jacobson is a Research to Prevent Blindness Dolly Green Scholar.",

year = "1992",

doi = "10.1016/S0002-9394(14)71529-6",

language = "English (US)",

volume = "113",

pages = "165--174",

journal = "American journal of ophthalmology",

issn = "0002-9394",

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T1 - Abnormal rod dark adaptation in autosomal dominant retinitis pigmentosa with proline-23-histidine rhodopsin mutation

AU - Kemp, C. M.

AU - Jacobson, S. G.

AU - Roman, A. J.

AU - Sung, C. H.

AU - Nathans, J.

N1 - Funding Information: From the Department of Ophthalmology, University of Miami School of Medicine, Bascom Palmer Eye Institute, Miami, Florida (Drs. Kemp and Jacobson and Mr. Roman); and Department of Molecular Biology and Genetics and Department of Neuroscience, Howard Hughes Medical Institute, Johns Hopkins University School ofMedicine, Baltimore, Maryland (Drs. Sung and Nathans). This study wassupported in part by Public Health Service research grant EY05627; the National Retinitis Pigmentosa Foundation, Inc., Baltimore, Maryland; The Chatlos Foundation, Inc., Longwood, Florida; and the Howard Hughes Medical Institute, Bethesda, Maryland. Dr. Jacobson is a Research to Prevent Blindness Dolly Green Scholar.

PY - 1992

Y1 - 1992

N2 - We studied rod and cone function in 13 patients from four families with autosomal dominant retinitis pigmentosa and the proline-23-histidine rhodopsin mutation. In patients with early stages of this disease, rod sensitivity was mildly abnormal throughout the retina and cone sensitivity was normal. In more severely affected patients, sensitivity loss varied with retinal region, some regions showing mild rod loss only and other regions having pronounced rod and cone dysfunction. Rhodopsin levels were decreased below normal by amounts that indicated the rod sensitivity loss was determined by the reduced ability to absorb light. The most characteristic abnormality of this genotype was a slowed rod branch of dark adaptation, which was present regardless of the extent or severity of disease. The time required for recovery of rod sensitivity was more than twice the normal time. These findings with dark-adapted perimetry, fundus reflectometry, and dark adaptometry showed intrafamilial and interfamilial consistency.

AB - We studied rod and cone function in 13 patients from four families with autosomal dominant retinitis pigmentosa and the proline-23-histidine rhodopsin mutation. In patients with early stages of this disease, rod sensitivity was mildly abnormal throughout the retina and cone sensitivity was normal. In more severely affected patients, sensitivity loss varied with retinal region, some regions showing mild rod loss only and other regions having pronounced rod and cone dysfunction. Rhodopsin levels were decreased below normal by amounts that indicated the rod sensitivity loss was determined by the reduced ability to absorb light. The most characteristic abnormality of this genotype was a slowed rod branch of dark adaptation, which was present regardless of the extent or severity of disease. The time required for recovery of rod sensitivity was more than twice the normal time. These findings with dark-adapted perimetry, fundus reflectometry, and dark adaptometry showed intrafamilial and interfamilial consistency.

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Abnormal rod dark adaptation in autosomal dominant retinitis pigmentosa with proline-23-histidine rhodopsin mutation

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