RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics

Cerebellar ataxia, neuropathy and vestibular areflexia syndrome is a progressive, generally late-onset, neurological disorder associated with biallelic pentanucleotide expansions in Intron 2 of the RFC1 gene. The locus exhibits substantial genetic variability, with multiple pathogenic and benign pen...

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Autores principales: Scriba, Carolin K, Stevanovski, Igor, Chintalaphani, Sanjog R, Gamaarachchi, Hasindu, Ghaoui, Roula, Ghia, Darshan, Henderson, Robert D, Jordan, Nerissa, Winkel, Antony, Lamont, Phillipa J, Rodrigues, Miriam J, Roxburgh, Richard H, Weisburd, Ben, Laing, Nigel G, Deveson, Ira W, Davis, Mark R, Ravenscroft, Gianina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2023
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10445415/
https://www.ncbi.nlm.nih.gov/pubmed/37621409
http://dx.doi.org/10.1093/braincomms/fcad208
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author Scriba, Carolin K
Stevanovski, Igor
Chintalaphani, Sanjog R
Gamaarachchi, Hasindu
Ghaoui, Roula
Ghia, Darshan
Henderson, Robert D
Jordan, Nerissa
Winkel, Antony
Lamont, Phillipa J
Rodrigues, Miriam J
Roxburgh, Richard H
Weisburd, Ben
Laing, Nigel G
Deveson, Ira W
Davis, Mark R
Ravenscroft, Gianina
author_facet Scriba, Carolin K
Stevanovski, Igor
Chintalaphani, Sanjog R
Gamaarachchi, Hasindu
Ghaoui, Roula
Ghia, Darshan
Henderson, Robert D
Jordan, Nerissa
Winkel, Antony
Lamont, Phillipa J
Rodrigues, Miriam J
Roxburgh, Richard H
Weisburd, Ben
Laing, Nigel G
Deveson, Ira W
Davis, Mark R
Ravenscroft, Gianina
author_sort Scriba, Carolin K
collection PubMed
description Cerebellar ataxia, neuropathy and vestibular areflexia syndrome is a progressive, generally late-onset, neurological disorder associated with biallelic pentanucleotide expansions in Intron 2 of the RFC1 gene. The locus exhibits substantial genetic variability, with multiple pathogenic and benign pentanucleotide repeat alleles previously identified. To determine the contribution of pathogenic RFC1 expansions to neurological disease within an Australasian cohort and further investigate the heterogeneity exhibited at the locus, a combination of flanking and repeat-primed PCR was used to screen a cohort of 242 Australasian patients with neurological disease. Patients whose data indicated large gaps within expanded alleles following repeat-primed PCR, underwent targeted long-read sequencing to identify novel repeat motifs at the locus. To increase diagnostic yield, additional probes at the RFC1 repeat region were incorporated into the PathWest diagnostic laboratory targeted neurological disease gene panel to enable first-pass screening of the locus for all samples tested on the panel. Within the Australasian cohort, we detected known pathogenic biallelic expansions in 15.3% (n = 37) of patients. Thirty indicated biallelic AAGGG expansions, two had biallelic ‘Māori alleles’ [(AAAGG)(exp)(AAGGG)(exp)], two samples were compound heterozygous for the Māori allele and an AAGGG expansion, two samples had biallelic ACAGG expansions and one sample was compound heterozygous for the ACAGG and AAGGG expansions. Forty-five samples tested indicated the presence of biallelic expansions not known to be pathogenic. A large proportion (84%) showed complex interrupted patterns following repeat-primed PCR, suggesting that these expansions are likely to be comprised of more than one repeat motif, including previously unknown repeats. Using targeted long-read sequencing, we identified three novel repeat motifs in expanded alleles. Here, we also show that short-read sequencing can be used to reliably screen for the presence or absence of biallelic RFC1 expansions in all samples tested using the PathWest targeted neurological disease gene panel. Our results show that RFC1 pathogenic expansions make a substantial contribution to neurological disease in the Australasian population and further extend the heterogeneity of the locus. To accommodate the increased complexity, we outline a multi-step workflow utilizing both targeted short- and long-read sequencing to achieve a definitive genotype and provide accurate diagnoses for patients.
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spelling pubmed-104454152023-08-24 RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics Scriba, Carolin K Stevanovski, Igor Chintalaphani, Sanjog R Gamaarachchi, Hasindu Ghaoui, Roula Ghia, Darshan Henderson, Robert D Jordan, Nerissa Winkel, Antony Lamont, Phillipa J Rodrigues, Miriam J Roxburgh, Richard H Weisburd, Ben Laing, Nigel G Deveson, Ira W Davis, Mark R Ravenscroft, Gianina Brain Commun Original Article Cerebellar ataxia, neuropathy and vestibular areflexia syndrome is a progressive, generally late-onset, neurological disorder associated with biallelic pentanucleotide expansions in Intron 2 of the RFC1 gene. The locus exhibits substantial genetic variability, with multiple pathogenic and benign pentanucleotide repeat alleles previously identified. To determine the contribution of pathogenic RFC1 expansions to neurological disease within an Australasian cohort and further investigate the heterogeneity exhibited at the locus, a combination of flanking and repeat-primed PCR was used to screen a cohort of 242 Australasian patients with neurological disease. Patients whose data indicated large gaps within expanded alleles following repeat-primed PCR, underwent targeted long-read sequencing to identify novel repeat motifs at the locus. To increase diagnostic yield, additional probes at the RFC1 repeat region were incorporated into the PathWest diagnostic laboratory targeted neurological disease gene panel to enable first-pass screening of the locus for all samples tested on the panel. Within the Australasian cohort, we detected known pathogenic biallelic expansions in 15.3% (n = 37) of patients. Thirty indicated biallelic AAGGG expansions, two had biallelic ‘Māori alleles’ [(AAAGG)(exp)(AAGGG)(exp)], two samples were compound heterozygous for the Māori allele and an AAGGG expansion, two samples had biallelic ACAGG expansions and one sample was compound heterozygous for the ACAGG and AAGGG expansions. Forty-five samples tested indicated the presence of biallelic expansions not known to be pathogenic. A large proportion (84%) showed complex interrupted patterns following repeat-primed PCR, suggesting that these expansions are likely to be comprised of more than one repeat motif, including previously unknown repeats. Using targeted long-read sequencing, we identified three novel repeat motifs in expanded alleles. Here, we also show that short-read sequencing can be used to reliably screen for the presence or absence of biallelic RFC1 expansions in all samples tested using the PathWest targeted neurological disease gene panel. Our results show that RFC1 pathogenic expansions make a substantial contribution to neurological disease in the Australasian population and further extend the heterogeneity of the locus. To accommodate the increased complexity, we outline a multi-step workflow utilizing both targeted short- and long-read sequencing to achieve a definitive genotype and provide accurate diagnoses for patients. Oxford University Press 2023-07-25 /pmc/articles/PMC10445415/ /pubmed/37621409 http://dx.doi.org/10.1093/braincomms/fcad208 Text en © The Author(s) 2023. Published by Oxford University Press on behalf of the Guarantors of Brain. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Scriba, Carolin K
Stevanovski, Igor
Chintalaphani, Sanjog R
Gamaarachchi, Hasindu
Ghaoui, Roula
Ghia, Darshan
Henderson, Robert D
Jordan, Nerissa
Winkel, Antony
Lamont, Phillipa J
Rodrigues, Miriam J
Roxburgh, Richard H
Weisburd, Ben
Laing, Nigel G
Deveson, Ira W
Davis, Mark R
Ravenscroft, Gianina
RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics
title RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics
title_full RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics
title_fullStr RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics
title_full_unstemmed RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics
title_short RFC1 in an Australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics
title_sort rfc1 in an australasian neurological disease cohort: extending the genetic heterogeneity and implications for diagnostics
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10445415/
https://www.ncbi.nlm.nih.gov/pubmed/37621409
http://dx.doi.org/10.1093/braincomms/fcad208
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