High-Throughput Sequencing to Identify Mutations Associated with Retinal Dystrophies

Fei Song; Marta Owczarek-Lipska; Tim Ahmels; Marius Book; Sabine Aisenbrey; Moreno Menghini; Daniel Barthelmes; Stefan Schrader; Georg Spital; John Neidhardt

doi:10.3390/genes12081269

Genes (Aug 2021)

High-Throughput Sequencing to Identify Mutations Associated with Retinal Dystrophies

Fei Song,
Marta Owczarek-Lipska,
Tim Ahmels,
Marius Book,
Sabine Aisenbrey,
Moreno Menghini,
Daniel Barthelmes,
Stefan Schrader,
Georg Spital,
John Neidhardt

Affiliations

Fei Song: Human Genetics Faculty VI-School of Medicine and Health Sciences, University of Oldenburg, Ammerländer Heerstrasse 114-118, 26129 Oldenburg, Germany
Marta Owczarek-Lipska: Human Genetics Faculty VI-School of Medicine and Health Sciences, University of Oldenburg, Ammerländer Heerstrasse 114-118, 26129 Oldenburg, Germany
Tim Ahmels: Department of Ophthalmology, Pius-Hospital, University of Oldenburg, 26121 Oldenburg, Germany
Marius Book: Eye Centre at the St. Franziskus Hospital, 48145 Münster, Germany
Sabine Aisenbrey: Department of Ophthalmology, Vivantes Health Network Ltd., Neukölln Hospital, 12351 Berlin, Germany
Moreno Menghini: Department of Ophthalmology, Ospedale Regionale di Lugano, 6900 Lugano, Switzerland
Daniel Barthelmes: Department of Ophthalmology, University Hospital Zurich, University of Zurich, 8091 Zurich, Switzerland
Stefan Schrader: Department of Ophthalmology, Pius-Hospital, University of Oldenburg, 26121 Oldenburg, Germany
Georg Spital: Eye Centre at the St. Franziskus Hospital, 48145 Münster, Germany
John Neidhardt: Human Genetics Faculty VI-School of Medicine and Health Sciences, University of Oldenburg, Ammerländer Heerstrasse 114-118, 26129 Oldenburg, Germany

DOI: https://doi.org/10.3390/genes12081269
Journal volume & issue: Vol. 12, no. 8
p. 1269

Abstract

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Retinal dystrophies (RD) are clinically and genetically heterogenous disorders showing mutations in over 270 disease-associated genes. Several millions of people worldwide are affected with different types of RD. Studying the relevance of disease-associated sequence alterations will assist in understanding disorders and may lead to the development of therapeutic approaches. Here, we established a whole exome sequencing (WES) pipeline to rapidly identify disease-associated mutations in patients. Sanger sequencing was applied to identify deep-intronic variants and to verify the co-segregation of WES results within families. We analyzed 26 unrelated patients with different syndromic and non-syndromic clinical manifestations of RD. All patients underwent ophthalmic examinations. We identified nine novel disease-associated sequence variants among 37 variants identified in total. The sequence variants located to 17 different genes. Interestingly, two cases presenting with Stargardt disease carried deep-intronic variants in ABCA4. We have classified 21 variants as pathogenic variants, 4 as benign/likely benign variants, and 12 as variants of uncertain significance. This study highlights the importance of WES-based mutation analyses in RD patients supporting clinical decisions, broadly based genetic diagnosis and support genetic counselling. It is essential for any genetic therapy to expand the mutation spectrum, understand the genes’ function, and correlate phenotypes with genotypes.

Published in Genes

ISSN: 2073-4425 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Biology (General): Genetics
Website: http://www.mdpi.com/journal/genes/

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