Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus

PURPOSE: We aim to report noncoding pathogenic variants in patients with FRMD7-related infantile nystagmus (FIN). METHODS: Genome sequencing (n = 2 families) and reanalysis of targeted panel next generation sequencing (n = 2 families) was performed in genetically unsolved cases of suspected FIN. Pre...

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Autores principales: Lee, Junwon, Jeong, Han, Won, Dongju, Shin, Saeam, Lee, Seung-Tae, Choi, Jong Rak, Byeon, Suk Ho, Kuht, Helen J., Thomas, Mervyn G., Han, Jinu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Association for Research in Vision and Ophthalmology 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9251792/
https://www.ncbi.nlm.nih.gov/pubmed/35762937
http://dx.doi.org/10.1167/tvst.11.6.25
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author Lee, Junwon
Jeong, Han
Won, Dongju
Shin, Saeam
Lee, Seung-Tae
Choi, Jong Rak
Byeon, Suk Ho
Kuht, Helen J.
Thomas, Mervyn G.
Han, Jinu
author_facet Lee, Junwon
Jeong, Han
Won, Dongju
Shin, Saeam
Lee, Seung-Tae
Choi, Jong Rak
Byeon, Suk Ho
Kuht, Helen J.
Thomas, Mervyn G.
Han, Jinu
author_sort Lee, Junwon
collection PubMed
description PURPOSE: We aim to report noncoding pathogenic variants in patients with FRMD7-related infantile nystagmus (FIN). METHODS: Genome sequencing (n = 2 families) and reanalysis of targeted panel next generation sequencing (n = 2 families) was performed in genetically unsolved cases of suspected FIN. Previous sequence analysis showed no pathogenic coding variants in genes associated with infantile nystagmus. SpliceAI, SpliceRover, and Alamut consensus programs were used to annotate noncoding variants. Minigene splicing assay was performed to confirm aberrant splicing. In silico analysis of exonic splicing enhancer and silencer was also performed. RESULTS: FRMD7 intronic variants were identified based on genome sequencing and targeted next-generation sequencing analysis. These included c.285-12A>G (pedigree 1), c.284+63T>A (pedigrees 2 and 3), and c. 383-1368A>G (pedigree 4). All variants were absent in gnomAD, and the both c.285-12A>G and c.284+63T>A variants were predicted to enhance new splicing acceptor gains with SpliceAI, SpliceRover, and Alamut consensus approaches. However, the c.383-1368 A>G variant only had a significant impact score on the SpliceRover program. The c.383-1368A>G variant was predicted to promote pseudoexon inclusion by binding of exonic splicing enhancer. Aberrant exonizations were validated through minigene constructs, and all variants were segregated in the families. CONCLUSIONS: Deep learning–based annotation of noncoding variants facilitates the discovery of hidden genetic variations in patients with FIN. This study provides evidence of effectiveness of combined deep learning–based splicing tools to identify hidden pathogenic variants in previously unsolved patients with infantile nystagmus. TRANSLATIONAL RELEVANCE: These results demonstrate robust analysis using two deep learning splicing predictions and in vitro functional study can lead to finding hidden genetic variations in unsolved patients.
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spelling pubmed-92517922022-07-05 Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus Lee, Junwon Jeong, Han Won, Dongju Shin, Saeam Lee, Seung-Tae Choi, Jong Rak Byeon, Suk Ho Kuht, Helen J. Thomas, Mervyn G. Han, Jinu Transl Vis Sci Technol Article PURPOSE: We aim to report noncoding pathogenic variants in patients with FRMD7-related infantile nystagmus (FIN). METHODS: Genome sequencing (n = 2 families) and reanalysis of targeted panel next generation sequencing (n = 2 families) was performed in genetically unsolved cases of suspected FIN. Previous sequence analysis showed no pathogenic coding variants in genes associated with infantile nystagmus. SpliceAI, SpliceRover, and Alamut consensus programs were used to annotate noncoding variants. Minigene splicing assay was performed to confirm aberrant splicing. In silico analysis of exonic splicing enhancer and silencer was also performed. RESULTS: FRMD7 intronic variants were identified based on genome sequencing and targeted next-generation sequencing analysis. These included c.285-12A>G (pedigree 1), c.284+63T>A (pedigrees 2 and 3), and c. 383-1368A>G (pedigree 4). All variants were absent in gnomAD, and the both c.285-12A>G and c.284+63T>A variants were predicted to enhance new splicing acceptor gains with SpliceAI, SpliceRover, and Alamut consensus approaches. However, the c.383-1368 A>G variant only had a significant impact score on the SpliceRover program. The c.383-1368A>G variant was predicted to promote pseudoexon inclusion by binding of exonic splicing enhancer. Aberrant exonizations were validated through minigene constructs, and all variants were segregated in the families. CONCLUSIONS: Deep learning–based annotation of noncoding variants facilitates the discovery of hidden genetic variations in patients with FIN. This study provides evidence of effectiveness of combined deep learning–based splicing tools to identify hidden pathogenic variants in previously unsolved patients with infantile nystagmus. TRANSLATIONAL RELEVANCE: These results demonstrate robust analysis using two deep learning splicing predictions and in vitro functional study can lead to finding hidden genetic variations in unsolved patients. The Association for Research in Vision and Ophthalmology 2022-06-28 /pmc/articles/PMC9251792/ /pubmed/35762937 http://dx.doi.org/10.1167/tvst.11.6.25 Text en Copyright 2022 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License.
spellingShingle Article
Lee, Junwon
Jeong, Han
Won, Dongju
Shin, Saeam
Lee, Seung-Tae
Choi, Jong Rak
Byeon, Suk Ho
Kuht, Helen J.
Thomas, Mervyn G.
Han, Jinu
Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus
title Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus
title_full Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus
title_fullStr Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus
title_full_unstemmed Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus
title_short Noncanonical Splice Site and Deep Intronic FRMD7 Variants Activate Cryptic Exons in X-linked Infantile Nystagmus
title_sort noncanonical splice site and deep intronic frmd7 variants activate cryptic exons in x-linked infantile nystagmus
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9251792/
https://www.ncbi.nlm.nih.gov/pubmed/35762937
http://dx.doi.org/10.1167/tvst.11.6.25
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