AUTOSOMAL DOMINANT MÜLLER CELL SHEEN DYSTROPHY: Clinical, Histopathologic, and Genetic Assessment in an Extended Family with Long Follow-Up

José Dalma-Weiszhausz; Oscar Chacón-Camacho; Patricia Chevez-Barrios; Juan C. Zenteno; Valentina Franco-Cárdenas; Leopoldo A. García-Montaño; Jehieli Pérez-Bravo; Iván A. García-Montalvo; Juan M. Jiménez-Sierra; Alexander Dalma

doi:10.1097/IAE.0000000000003413

AUTOSOMAL DOMINANT MÜLLER CELL SHEEN DYSTROPHY: Clinical, Histopathologic, and Genetic Assessment in an Extended Family with Long Follow-Up

José Dalma-Weiszhausz, Oscar Chacón-Camacho, Patricia Chevez-Barrios, Juan C. Zenteno, Valentina Franco-Cárdenas, Leopoldo A. García-Montaño, Jehieli Pérez-Bravo, Iván A. García-Montalvo, Juan M. Jiménez-Sierra, Alexander Dalma

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Abstract

Background:Autosomal dominant Müller cell dystrophy is a rare condition we described in 1991. It is characterized by a striking sheen appearance on the retinal surface with progressive retinal changes leading to disorganization and atrophy with a decreased b-wave electroretinograms.Materials and Methods:We examined 45 members of a 4-generation family. Fifteen subjects from three generations were found with the disease, without gender predilection. Seven patients underwent ophthalmic examination including fundus examination, intravenous fluorescein angiogram, spectral-domain optical coherence tomography, and electroretinogram. Six patients have a 30-year follow-up. Histopathology examination was performed on eyes of the eldest patient. Whole exome sequencing was done in four affected subjects.Results:Findings include a decreased visual acuity, abnormal cellophane-like sheen of the vitreoretinal interface, a "plush" nerve fiber layer, and characteristic macular changes. Electroretinogram showed a selective b-wave diminution. Intravenous fluorescein angiogram presented perifoveal hyperfluorescence and capillary leakage. Spectral-domain optical coherence tomography revealed cavitations involving inner and later outer retinal layers with later disorganization. Histopathologic findings included Müller cell abnormalities with cystic disruption of inner retinal layers, pseudoexfoliation in anterior segment, and amyloidosis of extraocular vessels. Pedigree analysis suggests an autosomal dominant inheritance with late onset. DNA analysis demonstrated a previously undescribed heterozygous missense p.Glu109Val mutation in transthyretin.Conclusion:To the best of our knowledge, this is the first family reported with this disorder. Our data support the hypothesis that autosomal dominant Müller cell dystrophy is a distinct retinal dystrophy affecting Müller cells. Mutations in transthyretin gene may manifest as a predominantly retinal disorder.

Original language	English (US)
Pages (from-to)	981-991
Number of pages	11
Journal	Retina
Volume	42
Issue number	5
DOIs	https://doi.org/10.1097/IAE.0000000000003413
State	Published - May 1 2022

Keywords

Müller cell
amyloidosis
autosomal dominant
cellophane
dystrophy
internal limiting membrane
macula
reflex
retina
sheen
vitreous

ASJC Scopus subject areas

Ophthalmology

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10.1097/IAE.0000000000003413

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Dalma-Weiszhausz, J., Chacón-Camacho, O., Chevez-Barrios, P., Zenteno, J. C., Franco-Cárdenas, V., García-Montaño, L. A., Pérez-Bravo, J., García-Montalvo, I. A., Jiménez-Sierra, J. M., & Dalma, A. (2022). AUTOSOMAL DOMINANT MÜLLER CELL SHEEN DYSTROPHY: Clinical, Histopathologic, and Genetic Assessment in an Extended Family with Long Follow-Up. Retina, 42(5), 981-991. https://doi.org/10.1097/IAE.0000000000003413

Dalma-Weiszhausz, J, Chacón-Camacho, O, Chevez-Barrios, P, Zenteno, JC, Franco-Cárdenas, V, García-Montaño, LA, Pérez-Bravo, J, García-Montalvo, IA, Jiménez-Sierra, JM & Dalma, A 2022, 'AUTOSOMAL DOMINANT MÜLLER CELL SHEEN DYSTROPHY: Clinical, Histopathologic, and Genetic Assessment in an Extended Family with Long Follow-Up', Retina, vol. 42, no. 5, pp. 981-991. https://doi.org/10.1097/IAE.0000000000003413

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title = "AUTOSOMAL DOMINANT M{\"U}LLER CELL SHEEN DYSTROPHY: Clinical, Histopathologic, and Genetic Assessment in an Extended Family with Long Follow-Up",

abstract = "Background:Autosomal dominant M{\"u}ller cell dystrophy is a rare condition we described in 1991. It is characterized by a striking sheen appearance on the retinal surface with progressive retinal changes leading to disorganization and atrophy with a decreased b-wave electroretinograms.Materials and Methods:We examined 45 members of a 4-generation family. Fifteen subjects from three generations were found with the disease, without gender predilection. Seven patients underwent ophthalmic examination including fundus examination, intravenous fluorescein angiogram, spectral-domain optical coherence tomography, and electroretinogram. Six patients have a 30-year follow-up. Histopathology examination was performed on eyes of the eldest patient. Whole exome sequencing was done in four affected subjects.Results:Findings include a decreased visual acuity, abnormal cellophane-like sheen of the vitreoretinal interface, a {"}plush{"} nerve fiber layer, and characteristic macular changes. Electroretinogram showed a selective b-wave diminution. Intravenous fluorescein angiogram presented perifoveal hyperfluorescence and capillary leakage. Spectral-domain optical coherence tomography revealed cavitations involving inner and later outer retinal layers with later disorganization. Histopathologic findings included M{\"u}ller cell abnormalities with cystic disruption of inner retinal layers, pseudoexfoliation in anterior segment, and amyloidosis of extraocular vessels. Pedigree analysis suggests an autosomal dominant inheritance with late onset. DNA analysis demonstrated a previously undescribed heterozygous missense p.Glu109Val mutation in transthyretin.Conclusion:To the best of our knowledge, this is the first family reported with this disorder. Our data support the hypothesis that autosomal dominant M{\"u}ller cell dystrophy is a distinct retinal dystrophy affecting M{\"u}ller cells. Mutations in transthyretin gene may manifest as a predominantly retinal disorder.",

keywords = "M{\"u}ller cell, amyloidosis, autosomal dominant, cellophane, dystrophy, internal limiting membrane, macula, reflex, retina, sheen, vitreous",

author = "Jos{\'e} Dalma-Weiszhausz and Oscar Chac{\'o}n-Camacho and Patricia Chevez-Barrios and Zenteno, {Juan C.} and Valentina Franco-C{\'a}rdenas and Garc{\'i}a-Monta{\~n}o, {Leopoldo A.} and Jehieli P{\'e}rez-Bravo and Garc{\'i}a-Montalvo, {Iv{\'a}n A.} and Jim{\'e}nez-Sierra, {Juan M.} and Alexander Dalma",

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doi = "10.1097/IAE.0000000000003413",

language = "English (US)",

volume = "42",

pages = "981--991",

journal = "Retina",

issn = "0275-004X",

publisher = "Lippincott Williams and Wilkins",

number = "5",

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T1 - AUTOSOMAL DOMINANT MÜLLER CELL SHEEN DYSTROPHY

T2 - Clinical, Histopathologic, and Genetic Assessment in an Extended Family with Long Follow-Up

AU - Dalma-Weiszhausz, José

AU - Chacón-Camacho, Oscar

AU - Chevez-Barrios, Patricia

AU - Zenteno, Juan C.

AU - Franco-Cárdenas, Valentina

AU - García-Montaño, Leopoldo A.

AU - Pérez-Bravo, Jehieli

AU - García-Montalvo, Iván A.

AU - Jiménez-Sierra, Juan M.

AU - Dalma, Alexander

PY - 2022/5/1

Y1 - 2022/5/1

N2 - Background:Autosomal dominant Müller cell dystrophy is a rare condition we described in 1991. It is characterized by a striking sheen appearance on the retinal surface with progressive retinal changes leading to disorganization and atrophy with a decreased b-wave electroretinograms.Materials and Methods:We examined 45 members of a 4-generation family. Fifteen subjects from three generations were found with the disease, without gender predilection. Seven patients underwent ophthalmic examination including fundus examination, intravenous fluorescein angiogram, spectral-domain optical coherence tomography, and electroretinogram. Six patients have a 30-year follow-up. Histopathology examination was performed on eyes of the eldest patient. Whole exome sequencing was done in four affected subjects.Results:Findings include a decreased visual acuity, abnormal cellophane-like sheen of the vitreoretinal interface, a "plush" nerve fiber layer, and characteristic macular changes. Electroretinogram showed a selective b-wave diminution. Intravenous fluorescein angiogram presented perifoveal hyperfluorescence and capillary leakage. Spectral-domain optical coherence tomography revealed cavitations involving inner and later outer retinal layers with later disorganization. Histopathologic findings included Müller cell abnormalities with cystic disruption of inner retinal layers, pseudoexfoliation in anterior segment, and amyloidosis of extraocular vessels. Pedigree analysis suggests an autosomal dominant inheritance with late onset. DNA analysis demonstrated a previously undescribed heterozygous missense p.Glu109Val mutation in transthyretin.Conclusion:To the best of our knowledge, this is the first family reported with this disorder. Our data support the hypothesis that autosomal dominant Müller cell dystrophy is a distinct retinal dystrophy affecting Müller cells. Mutations in transthyretin gene may manifest as a predominantly retinal disorder.

AB - Background:Autosomal dominant Müller cell dystrophy is a rare condition we described in 1991. It is characterized by a striking sheen appearance on the retinal surface with progressive retinal changes leading to disorganization and atrophy with a decreased b-wave electroretinograms.Materials and Methods:We examined 45 members of a 4-generation family. Fifteen subjects from three generations were found with the disease, without gender predilection. Seven patients underwent ophthalmic examination including fundus examination, intravenous fluorescein angiogram, spectral-domain optical coherence tomography, and electroretinogram. Six patients have a 30-year follow-up. Histopathology examination was performed on eyes of the eldest patient. Whole exome sequencing was done in four affected subjects.Results:Findings include a decreased visual acuity, abnormal cellophane-like sheen of the vitreoretinal interface, a "plush" nerve fiber layer, and characteristic macular changes. Electroretinogram showed a selective b-wave diminution. Intravenous fluorescein angiogram presented perifoveal hyperfluorescence and capillary leakage. Spectral-domain optical coherence tomography revealed cavitations involving inner and later outer retinal layers with later disorganization. Histopathologic findings included Müller cell abnormalities with cystic disruption of inner retinal layers, pseudoexfoliation in anterior segment, and amyloidosis of extraocular vessels. Pedigree analysis suggests an autosomal dominant inheritance with late onset. DNA analysis demonstrated a previously undescribed heterozygous missense p.Glu109Val mutation in transthyretin.Conclusion:To the best of our knowledge, this is the first family reported with this disorder. Our data support the hypothesis that autosomal dominant Müller cell dystrophy is a distinct retinal dystrophy affecting Müller cells. Mutations in transthyretin gene may manifest as a predominantly retinal disorder.

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KW - autosomal dominant

KW - cellophane

KW - dystrophy

KW - internal limiting membrane

KW - macula

KW - reflex

KW - retina

KW - sheen

KW - vitreous

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AUTOSOMAL DOMINANT MÜLLER CELL SHEEN DYSTROPHY: Clinical, Histopathologic, and Genetic Assessment in an Extended Family with Long Follow-Up

Abstract

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