CRB1 related retinal degeneration with novel mutation

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Abstract

Purpose

To describe novel and previously unreported genetic mutations in the CRB1 gene in a patient with retinal dystrophy. To increase the genotype-phenotype understanding of CRB1-related retinal degenerative diseases and describe patients’ response to therapy.

Observations

Patient was evaluated for progressive loss of central and peripheral vision. Fundus photography, fundus autofluorescence (FAF), fluorescein angiography (FA), and ocular-coherence tomography (OCT) were used in the evaluation. Genetic screening was performed to explore underlying mutations. Genetics revealed a previously reported, pathogenic variant in the CRB1 gene (c.2842+5G > A), and a novel mutation (c.4014T > A) whose clinical significance is uncertain due to the absence of conclusive evidence. This case is phenotypically unique in that CME was refractory to therapy, while CME in CRB1 related maculopathy typically responds well to treatment.

Conclusions and importance

This study adds a breadth of phenotypic understanding to genetic analysis in CRB1 related retinal degenerative conditions. The newly described CRB1 variant mutation c.4014T > A may portend a poor prognosis for CME responsiveness to therapy. Genetic testing in an otherwise unexplained CME event may be useful to identify underlying CRB1 variants and reveal genotype-phenotype correlations, which may alter the treatment plan and prognosis.

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Most cited references 2

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CRB1 mutation spectrum in inherited retinal dystrophies.

Frederieke van der Deen, John R. Heckenlively, Ronald Roepman … (2004)

Mutations in the Crumbs homologue 1 (CRB1) gene have been reported in patients with a variety of autosomal recessive retinal dystrophies, including retinitis pigmentosa (RP) with preserved paraarteriolar retinal pigment epithelium (PPRPE), RP with Coats-like exudative vasculopathy, early onset RP without PPRPE, and Leber congenital amaurosis (LCA). We extended our investigations of CRB1 in these retinal dystrophies, and identified nine novel CRB1 sequence variants. In addition, we screened patients with "classic" RP and classic Coats disease (without RP), but no pathologic sequence variants were found in the CRB1 gene. In total, 71 different sequence variants have been identified on 184 CRB1 alleles of patients with retinal dystrophies, including amino acid substitutions, frameshift, nonsense, and splice site mutations, in-frame deletions, and large insertions. Recent studies in two animal models, mouse and Drosophila, and in vivo high-resolution microscopy in patients with LCA, have shed light on the role of CRB1 in the pathogenesis of retinal dystrophies and its function in the photoreceptors. In this article, we provide an overview of the currently known CRB1 sequence variants, predict their effect, and propose a genotype-phenotype correlation model for CRB1 mutations. Copyright 2004 Wiley-Liss, Inc.

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CRB1 mutations may result in retinitis pigmentosa without para-arteriolar RPE preservation.

Eli Moore, Valerie Stone, Firhan Malik … (2001)

To report a new phenotype in retinitis pigmentosa (RP) patients with CRB1 mutations at the RP12 locus. Thirty-seven patients from two Pakistani families with severe retinitis pigmentosa. Samples were screened with single-strand conformation polymorphism analysis followed by DNA sequencing of the coding sequence of the CRB1 gene. Two novel CRB1 mutations were discovered. No patients had evidence of preservation of the para-arteriolar retinal pigment epithelium (PPRPE) that has been previously reported in all cases of RP associated with CRB1 mutations. Patients with severe autosomal recessive (or simplex) RP who lack the finding of PPRPE should not be excluded from molecular analysis of CRB1 purely because they lack the clinical feature of PPRPE. This report illustrates that RP at the RP12 locus is not clinically uniform. The absence of PPRPE cannot be used to exclude CRB1 as a potential molecular explanation for RP.

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Author and article information

Contributors

Sandeep Randhawa

Journal

Journal ID (nlm-ta): Am J Ophthalmol Case Rep

Journal ID (iso-abbrev): Am J Ophthalmol Case Rep

Title: American Journal of Ophthalmology Case Reports

Publisher: Elsevier

ISSN (Electronic): 2451-9936

Publication date PMC-release: 09 April 2020

Publication date Collection: June 2020

Publication date (Electronic): 09 April 2020

Volume: 18

Electronic Location Identifier: 100699

Affiliations

[a ]William Beaumont Hospital, 3555 W. 13 Mile Road, Suite LL-20, Royal Oak, MI, 48073, USA

[b ]Oakland University, William Beaumont School of Medicine, 586 Pioneer Dr, Rochester, MI, 48309, USA

[c ]Legacy Health, Legacy Emanuel Medical Center, 300 N. Graham St., Suite 300 Medical Office Building 3, Portland, OR, 97227, USA

Author notes

[∗ ]Corresponding author. William Beaumont Hospital, Neuroscience Center, 3555 W. 13 Mile Road, Suite LL-20, Royal Oak, MI, 48073, USA. srandhawa@ 123456arcpc.net

Article

Publisher ID: S2451-9936(19)30023-4 Publisher ID: 100699

DOI: 10.1016/j.ajoc.2020.100699

PMC ID: 7160514

PubMed ID: 32322752

SO-VID: 982fc97a-69b7-4dc6-bdd7-f35cded72a3d

License:

This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).

History

Date received : 18 January 2019

Date revision received : 2 April 2020

Date accepted : 3 April 2020

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