Biallelic expansion of an intronic repeat in RFC1 is a common cause of late-onset ataxia

doi:10.1038/s41588-019-0372-4

. 2019 Apr;51(4):649-658.

doi: 10.1038/s41588-019-0372-4. Epub 2019 Mar 29.

Biallelic expansion of an intronic repeat in RFC1 is a common cause of late-onset ataxia

Andrea Cortese¹, Roberto Simone², Roisin Sullivan^#³, Jana Vandrovcova^#³, Huma Tariq³, Wai Yan Yau³, Jack Humphrey³, Zane Jaunmuktane², Prasanth Sivakumar³, James Polke⁴, Muhammad Ilyas⁵, Eloise Tribollet³, Pedro J Tomaselli⁶, Grazia Devigili⁷, Ilaria Callegari⁸, Maurizio Versino^{8

9}, Vincenzo Salpietro³, Stephanie Efthymiou³, Diego Kaski³, Nick W Wood³, Nadja S Andrade¹⁰, Elena Buglo¹¹, Adriana Rebelo¹¹, Alexander M Rossor³, Adolfo Bronstein², Pietro Fratta³, Wilson J Marques⁶, Stephan Züchner¹¹, Mary M Reilly^#³, Henry Houlden^{12

13}

Affiliations

¹ Department of Neuromuscular Disease, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK. andrea.cortese@ucl.ac.uk.
² Department of Clinical and Movement Neurosciences, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK.
³ Department of Neuromuscular Disease, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK.
⁴ Neurogenetics Laboratory, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK.
⁵ Department of Biological Sciences, International Islamic University, Islamabad, Pakistan.
⁶ Department of Neurology, School of Medicine at Ribeirão Preto, University of São Paulo, Ribeirão Preto, Brazil.
⁷ UO Neurologia I, Fondazione IRCCS Istituto Neurologico 'Carlo Besta', Milan, Italy.
⁸ IRCCS Mondino Foundation, Pavia, Italy.
⁹ Department of Brain and Behavioral Sciences, University of Pavia, Pavia, Italy.
¹⁰ Department of Psychiatry and Behavioural Sciences, Center for Therapeutic Innovation, University of Miami Miller School of Medicine, Miami, FL, USA.
¹¹ Dr. John T. Macdonald Foundation Department of Human Genetics and John P. Hussman Institute for Human Genomics, University of Miami Miller School of Medicine, Miami, FL, USA.
¹² Department of Neuromuscular Disease, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK. h.houlden@ucl.ac.uk.
¹³ Neurogenetics Laboratory, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK. h.houlden@ucl.ac.uk.

^# Contributed equally.

PMID: 30926972
PMCID: PMC6709527
DOI: 10.1038/s41588-019-0372-4

Biallelic expansion of an intronic repeat in RFC1 is a common cause of late-onset ataxia

Andrea Cortese et al. Nat Genet. 2019 Apr.

. 2019 Apr;51(4):649-658.

doi: 10.1038/s41588-019-0372-4. Epub 2019 Mar 29.

Authors

Affiliations

¹ Department of Neuromuscular Disease, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK. andrea.cortese@ucl.ac.uk.
² Department of Clinical and Movement Neurosciences, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK.
³ Department of Neuromuscular Disease, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK.
⁴ Neurogenetics Laboratory, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK.
⁵ Department of Biological Sciences, International Islamic University, Islamabad, Pakistan.
⁶ Department of Neurology, School of Medicine at Ribeirão Preto, University of São Paulo, Ribeirão Preto, Brazil.
⁷ UO Neurologia I, Fondazione IRCCS Istituto Neurologico 'Carlo Besta', Milan, Italy.
⁸ IRCCS Mondino Foundation, Pavia, Italy.
⁹ Department of Brain and Behavioral Sciences, University of Pavia, Pavia, Italy.
¹⁰ Department of Psychiatry and Behavioural Sciences, Center for Therapeutic Innovation, University of Miami Miller School of Medicine, Miami, FL, USA.
¹¹ Dr. John T. Macdonald Foundation Department of Human Genetics and John P. Hussman Institute for Human Genomics, University of Miami Miller School of Medicine, Miami, FL, USA.
¹² Department of Neuromuscular Disease, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK. h.houlden@ucl.ac.uk.
¹³ Neurogenetics Laboratory, UCL Queen Square Institute of Neurology and The National Hospital for Neurology and Neurosurgery, London, UK. h.houlden@ucl.ac.uk.

^# Contributed equally.

PMID: 30926972
PMCID: PMC6709527
DOI: 10.1038/s41588-019-0372-4

Erratum in

Author Correction: Biallelic expansion of an intronic repeat in RFC1 is a common cause of late-onset ataxia.
Cortese A, Simone R, Sullivan R, Vandrovcova J, Tariq H, Yau WY, Humphrey J, Jaunmuktane Z, Sivakumar P, Polke J, Ilyas M, Tribollet E, Tomaselli PJ, Devigili G, Callegari I, Versino M, Salpietro V, Efthymiou S, Kaski D, Wood NW, Andrade NS, Buglo E, Rebelo A, Rossor AM, Bronstein A, Fratta P, Marques WJ, Züchner S, Reilly MM, Houlden H. Cortese A, et al. Nat Genet. 2019 May;51(5):920. doi: 10.1038/s41588-019-0422-y. Nat Genet. 2019. PMID: 31028356 Free PMC article.

Abstract

Late-onset ataxia is common, often idiopathic, and can result from cerebellar, proprioceptive, or vestibular impairment; when in combination, it is also termed cerebellar ataxia, neuropathy, vestibular areflexia syndrome (CANVAS). We used non-parametric linkage analysis and genome sequencing to identify a biallelic intronic AAGGG repeat expansion in the replication factor C subunit 1 (RFC1) gene as the cause of familial CANVAS and a frequent cause of late-onset ataxia, particularly if sensory neuronopathy and bilateral vestibular areflexia coexist. The expansion, which occurs in the poly(A) tail of an AluSx3 element and differs in both size and nucleotide sequence from the reference (AAAAG)₁₁ allele, does not affect RFC1 expression in patient peripheral and brain tissue, suggesting no overt loss of function. These data, along with an expansion carrier frequency of 0.7% in Europeans, implies that biallelic AAGGG expansion in RFC1 is a frequent cause of late-onset ataxia.

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Figures

**Fig. 1 |. Clinical spectrum and pedigrees of late-onset ataxia.**
a, Clinical spectrum of idiopathic late-onset ataxia from isolated cerebellar, vestibular, and sensory variants to full-blown CANVAS. b, Pedigrees of CANVAS families. The squares indicate males and the circles females. The diagonal lines are used for deceased individuals. CANVAS patients are indicated with filled shapes. The black dots indicate genotyped individuals. The red dots indicate patients enrolled for WGS study.

**Fig. 2 |. Identification of CANVAS locus.**
a, Non-parametric multipoint linkage analysis identifies a unique locus associated with the disease in chromosomal region 4p14 with a maximal HLOD score of 5.8. b, Schematic representation of shared haplotypes within single families. The light blue bars indicate a genomic region shared by affected siblings in a family and for which unaffected siblings are discordant. Two red dashed lines define a 1.7-Mb region common to the different families. SNPs defining the haplotypes are represented on the top line. c, Fine mapping inside the 1.7-Mb region identifies a recessive haplotype shared by all distinct families (highlighted in green), except for individual Fam 5b-2, who probably shares only one allele (highlighted in light green). d, Schematic representation of the candidate region encompassing all 24 exons and flanking regions of *RFC1* and the last exon and flanking intron of *WDR19.*

**Fig. 3 |. Recessive expansion of a mutated AAGGG repeated unit in intron 2 of *RFC1* causes CANVAS and late-onset ataxia in familial and sporadic cases.**
a, A reduced read depth of WGS is observed in CANVAS patients (n = 6) in a region corresponding to a short tandem AAAAG repeat in intron 2 of *RFC1.* b, Visualization on IGV of reads aligned to the short repeat and flanking region shows in patients (*n =* 6) the presence of a mutated AAGGG repeat unit (representative image). Reads from both sides are interrupted and are unable to cover the entire length of the microsatellite region. Note that, per IGV default setting, AAGGG repeated units that do not map to the (AAAAG)₁₁ reference sequence are soft-clipped and do not contribute to the coverage of the STR in a, which is virtually absent. However, ≥20 reads containing the AAGGG repeated unit could be observed in each patient if soft-clipped reads were shown. c, RP-PCR targeting the mutated AAGGG repeated unit. Fluorescein amidite-labeled PCR products were separated on an ABI 3730 DNA Analyzer. Electropherograms were visualized on GeneMapper at 2,000 relative fluorescence units. The representative plots from a patient carrying the AAGGG repeat expansion and one non-carrier are shown. RP-PCR experiments were repeated independently twice with similar results. d, Sanger sequencing of long-range PCR reactions confirms the AAAAG to AAGGG nucleotide change of the repeated unit in patients.

**Fig. 4 |. Polymorphic configurations of the repeat expansion locus and allelic distribution in healthy controls.**
a, Schematic representation of the repeat expansion locus in intron 2 of *RFC1* and its main allelic variants. b, Estimated allelic frequencies in 608 chromosomes from 304 healthy controls. c, Average size and s.d. of (AAAAG)_exp (n = 24) and (AAAGG)_exp (n = 30) expansions in healthy controls and (AAGGG)_exp (n = 72) in controls and CANVAS patients.

**Fig. 5 |. Pathology of cerebellar degeneration in a patient with CANVAS carrying the recessive AAGGG repeat expansion.**
**a-j**, Hematoxylin and eosin (H&E)-stained sections (**a-e**) and sections immunostained for p62 (**f-j**). In a control brain (a), age-matched for the patient with CANVAS syndrome, there is well preserved density of Purkinje cells (yellow arrowhead); the granule cell layer is densely populated with small neurocytes (green asterisk). b, In CANVAS syndrome, there is severe, widespread depletion of Purkinje cells with associated prominent Bergmann gliosis (blue arrowhead), while cell density in the granule cell layer is well preserved. c, In a patient with genetically confirmed FRDA, there is patchy depletion of Purkinje cells associated with Bergmann gliosis and unremarkable appearance of the granule cell layer. d, In a patient with genetically confirmed SCA17, there is widespread Purkinje cell loss with only occasional Purkinje cells remaining; also, in this patient, the granule cell layer is densely populated with small neurocytes. e, In a patient with FTD due to *C9orf72* expansion, Purkinje cell loss is patchy and the granule cell layer is unremarkable. **f-h**, Immunostaining for p62 shows no pathological cytoplasmic or intranuclear inclusions in the cerebellar cortex in the control patient (f), the patient with CANVAS syndrome (g), and also in the patient with FRDA (h). i, In the SCA17 patient, there are scattered discrete intranuclear p62 immunoreactive inclusions in the small neurons within the granule cell layer (high-power view of a representative intranuclear inclusion is demonstrated in the inset within i). j, In the patient with the *C9orf72* expansion, there are frequent characteristic perinuclear p62 positive inclusions in the granule cell layer (high-power view of a representative inclusion is shown in the inset within j). Scale bar, 100 μm in **a-e**, 30 μm in **f-j**, and 5μm in the insets in **f-j**. Staining was carried out once on patient samples with appropriate controls according to standard practice and histopathology procedures in an ISO 15189-accredited laboratory.

**Fig. 6 |. *RFC1* expression is not affected by the AAGGG repeat expansion.**
a, Plots showing the expression levels of *RFC1* and *FXN* in controls (n = 3), patients with FRDA (n = 2), and one CANVAS patient in postmortem cerebellum and frontal cortex. b, Mapping on *RFC1* transcript 1 of the primers used for assessment by qRT-PCR of *RFC1* mRNA (cF1-cR1 and cF2-cR2) and pre-mRNA (cF1/iR1) expression. The blue arrows indicate the primers mapping to the exonic and intronic regions of the canonical *RFC1* transcript. Primers spanning across exonic junctions are connected by dotted lines. A red triangle indicates the site of the AAGGG repeat expansion. c, Expression levels of the canonical coding *RFC1* mRNA as measured by qRT-PCR using two separate sets of primers, cF1-cR1 and cF2-cR2, in control (n = 3) and CANVAS (n = 2) lymphoblasts, control (n = 5) and CANVAS (n = 5) fibroblasts, control (n = 3), FRDA (n = 3), and CANVAS (n = 1) cerebellum and frontal cortex, and control (n = 5) and CANVAS muscles (n = 7). d, *RFC1*-encoded protein levels as measured by western blotting using the polyclonal antibody GTX129291 and normalized to β-actin in control (n = 5) and CANVAS (n = 5) fibroblasts, control (n = 3) and CANVAS (n = 4) lymphoblasts, and control (n = 3), FRDA (n = 3), and CANVAS (n = 1) postmortem cerebellum and frontal cortex. The bar graphs show the mean±s.d. and data distribution (black dots). A two-tailed t-test was performed to compare *RFC1* transcript and encoded protein expression in patients versus healthy or disease controls. All experiments were repeated independently twice with similar results.

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Comment in

CANVAS: A very late onset cerebellar ataxia, due to biallelic expansions in the RFC1 gene.
Tranchant C, Anheim M. Tranchant C, et al. Rev Neurol (Paris). 2019 Oct;175(9):493-494. doi: 10.1016/j.neurol.2019.05.002. Epub 2019 Sep 13. Rev Neurol (Paris). 2019. PMID: 31526553 No abstract available.

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References

1. Harding AE “Idiopathic” late onset cerebellar ataxia. A clinical and genetic study of 36 cases. J. Neurol. Sci. 51, 259–271 (1981). - PubMed
1. Muzaimi MB et al. Population based study of late onset cerebellar ataxia in south east Wales. J. Neurol. Neurosurg. Psychiatry 75, 1129–1134 (2004). - PMC - PubMed
1. Sghirlanzoni A, Pareyson D & Lauria G Sensory neuron diseases. Lancet Neurol. 4, 349–361 (2005). - PubMed
1. Strupp M, Feil K, Dieterich M & Brandt T Bilateral vestibulopathy. Handb. Clin. Neurol. 137, 235–240 (2016). - PubMed
1. Abele M et al. The aetiology of sporadic adult-onset ataxia. Brain 125(Pt. 5), 961–968 (2002). - PubMed

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[1] Harding AE “Idiopathic” late onset cerebellar ataxia. A clinical and genetic study of 36 cases. J. Neurol. Sci. 51, 259–271 (1981). - PubMed

[2] Harding AE “Idiopathic” late onset cerebellar ataxia. A clinical and genetic study of 36 cases. J. Neurol. Sci. 51, 259–271 (1981). - PubMed

[3] Muzaimi MB et al. Population based study of late onset cerebellar ataxia in south east Wales. J. Neurol. Neurosurg. Psychiatry 75, 1129–1134 (2004). - PMC - PubMed

[4] Muzaimi MB et al. Population based study of late onset cerebellar ataxia in south east Wales. J. Neurol. Neurosurg. Psychiatry 75, 1129–1134 (2004). - PMC - PubMed

[5] Sghirlanzoni A, Pareyson D & Lauria G Sensory neuron diseases. Lancet Neurol. 4, 349–361 (2005). - PubMed

[6] Sghirlanzoni A, Pareyson D & Lauria G Sensory neuron diseases. Lancet Neurol. 4, 349–361 (2005). - PubMed

[7] Strupp M, Feil K, Dieterich M & Brandt T Bilateral vestibulopathy. Handb. Clin. Neurol. 137, 235–240 (2016). - PubMed

[8] Strupp M, Feil K, Dieterich M & Brandt T Bilateral vestibulopathy. Handb. Clin. Neurol. 137, 235–240 (2016). - PubMed

[9] Abele M et al. The aetiology of sporadic adult-onset ataxia. Brain 125(Pt. 5), 961–968 (2002). - PubMed

[10] Abele M et al. The aetiology of sporadic adult-onset ataxia. Brain 125(Pt. 5), 961–968 (2002). - PubMed

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Biallelic expansion of an intronic repeat in RFC1 is a common cause of late-onset ataxia

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Biallelic expansion of an intronic repeat in RFC1 is a common cause of late-onset ataxia

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