Disease-Causing TIMP3 Variants and Deep Phenotyping of Two Czech Families with Sorsby Fundus Dystrophy Associated with Novel p.(Tyr152Cys) Mutation-Reference-Cited by-同舟云学术

Disease-Causing TIMP3 Variants and Deep Phenotyping of Two Czech Families with Sorsby Fundus Dystrophy Associated with Novel p.(Tyr152Cys) Mutation

Published:2024-03-27 Issue:7 Volume:25 Page:3744
ISSN:1422-0067
Container-title:International Journal of Molecular Sciences
language:en
Short-container-title:IJMS

Author:

Vergaro Andrea¹²,Pankievic Monika¹,Jedlickova Jana¹,Dudakova Lubica¹^ORCID,Vajter Marie¹²^ORCID,Michaelides Michel³,Meliska Martin²,Nemec Pavel⁴,Babincova Daniela⁵^ORCID,Kousal Bohdan²^ORCID,Liskova Petra¹²^ORCID

Affiliation:

1. Department of Paediatrics and Inherited Metabolic Disorders, First Faculty of Medicine, Charles University and General University Hospital in Prague, 121 08 Prague, Czech Republic

2. Department of Ophthalmology, First Faculty of Medicine, Charles University and General University Hospital in Prague, 128 08 Prague, Czech Republic

3. UCL Institute of Ophthalmology, University College London and Moorfields Eye Hospital, London EC1V 9EL, UK

4. Department of Ophthalmology, First Faculty of Medicine and Military University Hospital Prague, 162 00 Prague, Czech Republic

5. Laboratory of Molecular Biology, AGEL, 741 01 Nový Jíčín, Czech Republic

Abstract

We aim to report the ocular phenotype and molecular genetic findings in two Czech families with Sorsby fundus dystrophy and to review all the reported TIMP3 pathogenic variants. Two probands with Sorsby fundus dystrophy and three first-degree relatives underwent ocular examination and retinal imaging, including optical coherence tomography angiography. The DNA of the first proband was screened using a targeted ocular gene panel, while, in the second proband, direct sequencing of the TIMP3 coding region was performed. Sanger sequencing was also used for segregation analysis within the families. All the previously reported TIMP3 variants were reviewed using the American College of Medical Genetics and the Association for Molecular Pathology interpretation framework. A novel heterozygous variant, c.455A>G p.(Tyr152Cys), in TIMP3 was identified in both families and potentially de novo in one. Optical coherence tomography angiography documented in one patient the development of a choroidal neovascular membrane at 54 years. Including this study, 23 heterozygous variants in TIMP3 have been reported as disease-causing. Application of gene-specific criteria denoted eleven variants as pathogenic, eleven as likely pathogenic, and one as a variant of unknown significance. Our study expands the spectrum of TIMP3 pathogenic variants and highlights the importance of optical coherence tomography angiography for early detection of choroidal neovascular membranes.

Funder

Ministry of Health, Czech Republic

Charles University

National Institute for Health Research Biomedical Research Centre at Moorfields Eye Hospital NHS Foundation Trust

UCL Institute of Ophthalmology

Welcome Trust

Publisher

MDPI AG

Link

https://www.mdpi.com/1422-0067/25/7/3744/pdf

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