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EYS mutations and implementation of minigene assay for variant classification in EYS-associated retinitis pigmentosa in northern Sweden
Umeå University, Faculty of Medicine, Department of Medical Biosciences, Medical and Clinical Genetics.
Umeå University, Faculty of Medicine, Department of Medical Biosciences, Medical and Clinical Genetics.
Umeå University, Faculty of Medicine, Department of Medical Biosciences, Medical and Clinical Genetics.
Umeå University, Faculty of Medicine, Department of Medical Biosciences, Medical and Clinical Genetics.ORCID iD: 0000-0003-4146-7531
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2021 (English)In: Scientific Reports, E-ISSN 2045-2322, Vol. 11, no 1, article id 7696Article in journal (Refereed) Published
Abstract [en]

Retinitis pigmentosa (RP) is a clinically and genetically heterogeneous group of inherited retinal degenerations. The ortholog of Drosophila eyes shut/spacemaker, EYS on chromosome 6q12 is a major genetic cause of recessive RP worldwide, with prevalence of 5 to 30%. In this study, by using targeted NGS, MLPA and Sanger sequencing we uncovered the EYS gene as one of the most common genetic cause of autosomal recessive RP in northern Sweden accounting for at least 16%. The most frequent pathogenic variant was c.8648_8655del that in some patients was identified in cis with c.1155T>A, indicating Finnish ancestry. We also showed that two novel EYS variants, c.2992_2992+6delinsTG and c.3877+1G>A caused exon skipping in human embryonic kidney cells, HEK293T and in retinal pigment epithelium cells, ARPE-19 demonstrating that in vitro minigene assay is a straightforward tool for the analysis of intronic variants. We conclude, that whenever it is possible, functional testing is of great value for classification of intronic EYS variants and the following molecular testing of family members, their genetic counselling, and inclusion of RP patients to future treatment studies.
Place, publisher, year, edition, pages
Nature Publishing Group, 2021. Vol. 11, no 1, article id 7696
National Category
Medical Genetics and Genomics Ophthalmology
Identifiers
URN: urn:nbn:se:umu:diva-182475DOI: 10.1038/s41598-021-87224-9ISI: 000639562100016Scopus ID: 2-s2.0-85104048909OAI: oai:DiVA.org:umu-182475DiVA, id: diva2:1548163
Available from: 2021-04-29 Created: 2021-04-29 Last updated: 2025-02-10Bibliographically approved
In thesis
1. Genetics, epigenetics and functional mechanisms in inherited corneal and retinal dystrophies
Open this publication in new window or tab >>Genetics, epigenetics and functional mechanisms in inherited corneal and retinal dystrophies
2022 (English)Doctoral thesis, comprehensive summary (Other academic)
Alternative title[sv]
Genetik, epigenetik och funktionella mekanismer i ärftliga corneala och retinala dystrofier
Abstract [en]

Inherited eye disorders (IED) are groups of genetically and clinically heterogenous conditions affecting different tissues in the eye. IED are most often progressive with reduced vision or legal blindness as outcome. This thesis is focused on investigating the underlying mechanisms in Fuchs’ endothelial corneal dystrophy (FECD) and two retinal dystrophies, Stargardt disease (STGD1) and autosomal recessive Retinitis pigmentosa (arRP, RP25).

In FECD, we studied the association between FECD and the (CTG)n repeat expansion at the CTG18.1 locus in the TCF4 gene, in patients from northern Sweden. By using STR-PCR and TP-PCR, we found that 90% of FECD patients carry an expanded CTG18.1 allele, establishing the highest prevalence among FECD patients world-wide. With droplet digital PCR, we showed that transcripts spanning over the CTG18.1 have lower fractions in human corneal endothelium (CE) compared to skin, brain, muscle, and white blood cells. With Illumina Methylation arrays (850K), we detected a decreased global methylation in the CE at advanced age, that could possibly contribute to the late onset of FECD. We also found distinct differences in methylation between FECD patients and controls, that led us to two coagulation factors, found to be over-expressed in the CE from FECD patients.

For the two retinal dystrophies, STGD1 and RP25, we investigated the functional effect of four genetic variants residing adjacent to or in splice consensus sequence of the ABCA4 gene (STDG1) and the EYS gene (RP25). With an in vitro mini-gene splicing assay we showed that all four genetic variants caused exon skipping in Retinal Pigment Epithelial cell line (ARPE-19) and Human Embryonic kidney cell line (HEK293T). Our results functionally proved these variants to be pathogenic and causative of STGD1 and RP25.

In RP25, we also investigated the prevalence of pathogenic EYS variants in a cohort of patients from northern Sweden. DNA from 81 patients with a clinical diagnosis of RP were interrogated with a "cascade-targeted mutation analysis" approach, where NGS, MLPA and Sanger sequencing was used to find common EYS variants in this acknowledged genetically homogenous population. EYS mutations were present in at least 16% of all arRP patients and the most recurrent mutation in the study was an 8-bp deletion, previously found in the Finnish population.

In conclusion, this thesis provides knowledge on disease causative mechanisms in IED and contributes with valuable information for future genetic counselling and genetic testing for affected families.
Place, publisher, year, edition, pages
Umeå: Umeå University, 2022. p. 77
Series
Umeå University medical dissertations, ISSN 0346-6612 ; 2187
Keywords
Genetics, Epigenetics, Splicing, Methylation, Ophtalmology, FECD, Stargardt, Retinitis pigmentosa, ABCA4, EYS, TCF4, F5, THBD, Coagulation factor V, Thrombomodulin
National Category
Medical Genetics and Genomics Ophthalmology
Research subject
Medical Genetics
Identifiers
urn:nbn:se:umu:diva-200205 (URN)978-91-7855-810-0 (ISBN)978-91-7855-811-7 (ISBN)
Public defence
2022-11-18, Sal 933, 9 tr., byggnad 3A, Norrlands universitetssjukhus, Umeå, 13:00 (English)
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I tryckt spikblad kan stå Filosofie doktorsexamen. I digital version står korrekt: Medicine doktorsexamen. 

Available from: 2022-10-28 Created: 2022-10-12 Last updated: 2025-02-10Bibliographically approved

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Jonsson, FridaÖsterman, LennartHolmberg, MonicaBurstedt, MarieGolovleva, Irina

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