Sporadic late onset cerebellar ataxia is a well-described clinical presentation with a broad differential diagnosis that adult neurologists should be familiar with. However, despite extensive clinical investigations, an acquired cause is identified in only a minority of cases. Thereafter, an underlying genetic basis is often considered, even in those without a family history. Here we apply whole exome sequencing to a cohort of 12 patients with late onset cerebellar ataxia. We show that 33% of 'idiopathic' cases harbor compound heterozygous mutations in known ataxia genes, including genes not included on multi-gene panels, or primarily associated with an ataxic presentation

Chinnery, PF

Douroudis, K

Duff, J

Griffin, H

Horvath, R

Hussain, R

Keogh, MJ

Pyle, A

Santibanez-Koref, M

Smertenko, T

Steele, H

Journal of Neurology

English

PubMed

M. J. Keogh

H. Steele

K. Douroudis

A. Pyle

J. Duff

R. Hussain

T. Smertenko

H. Griffin

M. Santibanez-Koref

R. Horvath

P. F. Chinnery

Crossref

ORIGINAL COMMUNICATIONFrequency of rare recessive mutations in unexplained late onsetcerebellar ataxiaM. J. Keogh1,2 • H. Steele1,2 • K. Douroudis1 • A. Pyle1 • J. Duff1 • R. Hussain1 •T. Smertenko1 • H. Griffin1 • M. Santibanez-Koref1 • R. Horvath1,2 •P. F. Chinnery1,2Received: 24 February 2015 / Accepted: 29 April 2015 / Published online: 16 May 2015 The Author(s) 2015. This article is published with open access at Springerlink.comAbstract Sporadic late onset cerebellar ataxia is a well-described clinical presentation with a broad differentialdiagnosis that adult neurologists should be familiar with.However, despite extensive clinical investigations, an ac-quired cause is identified in only a minority of cases.Thereafter, an underlying genetic basis is often considered,even in those without a family history. Here we apply wholeexome sequencing to a cohort of 12 patients with late onsetcerebellar ataxia. We show that 33 % of ‘idiopathic’ casesharbor compound heterozygous mutations in known ataxiagenes, including genes not included on multi-gene panels,or primarily associated with an ataxic presentation.Keywords Ataxia  Whole exome sequencing  Nextgeneration sequencing  DiagnosisIntroductionAdult onset cerebellar ataxia poses a considerable diag-nostic challenge. Initial investigations focus on detectingdegenerative, toxic, structural and inflammatory etiologieswhich together underlie around a third of cases [1].Thereafter, molecular investigations for a monogenic basisof disease are often undertaken despite 80 % of patientshaving no relevant family history [2].Current molecular investigations for sporadic cases echothat of familial forms, beginning with testing for trinu-cleotide repeat disorders, such as the spinocerebellarataxias (SCA1, 2, 3, 6, 7 and 17), dentatorubral palli-doluysian atrophy (DRPLA) and Friedreich’s ataxia (FDR)in most centres [1]. However, this approach fails to identifya molecular diagnosis in 87–98 % of late onset sporadiccases [1, 3], and subsequent investigations are undertakenon a gene-by-gene basis, often at considerable time andexpense.The difficulty in establishing monogenic forms of dis-ease using this approach is increasingly challenging giventhat at least 60 causative ataxia genes are reported [4].Recent studies have therefore utilized next generation se-quencing focusing on infantile or juvenile onset cases [5],or adult onset ataxia with a demonstrable family history[4]. Only two studies have described sub-sets of patientswith sporadic onset adult disease, despite it being a majorform of ataxia, and suggested that a molecular diagnosiscan be reached in *10 % of cases [4, 6]. Given this, weapplied whole exome sequencing to a cohort of individualswith sporadic late onset ataxia.MethodsUnrelated individuals with sporadic ataxia beginning at30 years of age or over were identified from routine re-ferrals to our regional neurogenetic service, in Newcastleupon Tyne, England.M. J. Keogh and H. Steele contributed equally to this work andR. Horvath and P. F. Chinnery contributed equally to this work.Electronic supplementary material The online version of thisarticle (doi:10.1007/s00415-015-7772-x) contains supplementarymaterial, which is available to authorized users.& P. F. Chinneryp.f.chinnery@ncl.ac.uk; patrick.chinnery@ncl.ac.uk1 Institute of Genetic Medicine, Newcastle University,Newcastle upon Tyne NE1 3BZ, UK2 Department of Neurology, Royal Victoria Infirmary,Newcastle upon Tyne NE1 4LP, UK123J Neurol (2015) 262:1822–1827DOI 10.1007/s00415-015-7772-xAcquired causes of ataxia were excluded and all par-ticipants had negative genetic testing for SCA 1, 2, 3, 6, 7,17, DRPLA and Friedreich’s Ataxia (FA). In addition, alladult males had negative FMR1 testing.Blood genomic DNA was fragmented, exome enrichedand sequenced (Nextera Rapid Exome Capture 37 Mb andHiSeq 2000, 100 bp paired-end reads). In-house bioinfor-matic analysis included alignment to UCSC hg19, usingBWA as aligner and GATK to detect SNV and INDELSacross all samples using standard filtering parameters ac-cording to GATK Best Practise Recommendations [7] (seesupplementary methods). Further analysis was performedon variants with a minor allele frequency\0.005 in severalreference databases and 302 unrelated in-house controls(see supplementary methods). Rare heterozygous, ho-mozygous and compound heterozygous variants were de-fined, and protein altering and/or putative ‘disease causing’mutations as predicted by at least three out of four softwareprogrammes were included. Pathogenicity was defined inaccordance with American College of Medical Geneticguidelines (see supplementary methods). Genes known orsuggested to cause ataxia as a primary or secondary phe-notype in humans from two suggested clinical panels [4, 8]together with additional genes in which ataxia may resultas part of the phenotype (list-supplementary methods) wereassessed for variants according to the above criteria, andconfirmed by Sanger sequencing (supplementary methods).Variants were defined using a priori criteria: (1) con-firmed pathogenic: dominant disorders—variant previouslyshown to cause ataxia in humans; recessive disorders—either 2 variants previously shown to cause ataxia in hu-mans; or 1 pathogenic variant with a second variant pre-dicted to affect protein function by at least 3 of 4 predictionalgorithms (SIFT, Polyphen2, Mutation Taster, LRT), orthrough frameshift or truncation. (2) Probable pathogenic:dominant and recessive disorders—variants in known ge-nes causing ataxia in humans and predicted to affect pro-tein function by at least three of four prediction algorithms;(3) uncertain significance: dominant and recessive disor-ders—variants predicted to affect protein function withweak evidence that gene alteration causes ataxia inhumans.The study was granted ethical approval from a ResearchEthics Committee based in the North of England.ResultsPopulationTwelve Caucasian individuals of British origin (5 male)with no known consanguinity were included (Table 1).Mean age at disease onset was 46.7 years (SD 11; range30–70 years). Mean disease duration was 16.6 years (SD6.9; range 6–30 years). For one patient, the disease dura-tion fell within the range expected for multi-system atrophy[9]. This patient had a normal DaTscan and autonomicfunction tests. Three individuals had CSF examination withnegative oligoclonal bands. Five had nerve conductionstudies; two of which were abnormal. Detailed clinicalfeatures and the results of clinical investigations are shownin Table 1.DiagnosisWe identified previously described pathogenic mutations infour of the 12 (33 %) patients in our cohort. All werepresent on confirmatory Sanger sequencing. No probablepathogenic variants were identified and variants of uncer-tain significance were found in an additional two cases(17 %). Findings are summarised in Table 2.DiscussionWe identified confirmed or probable pathogenic variantscausing sporadic late onset ataxia in four patients (33 %) inour cohort. These findings are comparable to childhood/adolescent ataxia using targeted sequencing panels (40 %)[4] and whole exome sequencing (27 %) [5]. They are alsosignificantly higher than previous data for adult onset casesusing either panels or whole exome (both *10 %) [4, 6].We detected pathogenic variants in SPG7, SYNE1 andANO10 (previously published by Balreira et al. [10]). Fogelet al. [6] also identified pathogenic variants in these genes(SPG7 (n = 2), SYNE1 (n = 3) and ANO10 (n = 1). Theclinical features of these patients appear relatively ho-mogenous between their and our study, with pure cere-bellar ataxia beginning above the age of 40 for ANO10 andSYNE1 cases, and a more heterogeneous age of onset(\20–50) with additional neurological features includingspasticity and a polyneuropathy in SPG7 cases [6].Therefore, pathogenic mutations in these genes appear tobe an important and frequently identified cause of lateonset sporadic ataxia.We used whole exome sequencing (WES) rather thantargeted next generation ‘panels’, and it remains a con-tentious issue as to which is more appropriate in the inves-tigation of neurogenetic disorders. WES enables greatergenome coverage, and hence detection of pathogenic muta-tions in genes not considered as having ataxia as a primaryphenotype. Our results highlight this as SPG7 was not cov-ered by one ataxia panel [4], SYNE1 by another [8], andANO10 was not included in either panel. WES however, mayresult in detection of unexpected findings such as pathogenicmutations predisposing to cancer or neurodegenerativeJ Neurol (2015) 262:1822–1827 1823123Table1Clinicalfeaturesofthe12patientsinthecohortPatientno.,sexAge(years)Ageonset(years)Diseaseduration(years)PresentingsymptomGaitataxiaLimbataxiaOcularsignsAdditionalneurologicalfeaturesOtherfeaturesMRILPNCS/EMGOtherinvestigationsMusclebiopsyOthernegativemolecularinvestigations1,F634023Slowlyprogressivemidlineandappendicularataxicsyndrome?????EarlyCPEODysmetricpursuitBrokensaccadesDysphagia,spasticbladderLowerlimbspasticityNoneCANormal-OCBBilateralCTS(CTSstudyonly)NormalIHCNo mtDNAdeletionsFMR12,F473017Slowlyprogressivespasticataxicsyndrome??(Fr)?CPEOTemporalopticdiscpallorJerkypursuitHypometricsaccadesSpasticlowerlimbsBriskreflexesNoneMildCANormal-OCBNDMildfibresizevariationLowQ10Nil3,F574512Ataxiadevelopedaged45?????SlowsaccadesEpilepsyaged7NoneCAandparieto-occipitalatrophyNDNormalNDFMR14,F634023Slowlyprogressivemidlinecerebellarataxia???GENTLEwithongoinginfrequentfocalseizures,notreatmentCataracts(age62)CANDNDNDPOLGMT-ATP6&85,F553520Slowlyprogressivespasticataxicsyndrome???(WhC)??JerkypursuitGENHypometricsaccadesNeurogenicbladderSpasticataxicgaitBriskreflexesPositiveBabinskiNoneCANDNDNDSPG76,F76706Progressivemidlineandappendicularataxia?????GENUpanddownbeatnystagmusOrthostatictremorBriskreflexesNoneMildCANDND-DaTNormalIHCNo mtDNAdeletionsMT-ATP6&87,M716011Slowlyprogressivemidlineataxia?-JerkyocularpursuitGENNoneNoneCANDNormalNDSPG7MT-ATP6&88,M58508Midlineataxia???RAPDOAJerkypursuitGENCongenitalhearinglossEarlydysphagiaAreflexiaNoneCANDSANNormalIHCNo mtDNAdeletionsNormalQ10POLGWFS1OPA1MT-ATP6&81824 J Neurol (2015) 262:1822–1827123Table1continuedPatientno.,sexAge(years)Ageonset(years)Diseaseduration(years)PresentingsymptomGaitataxiaLimbataxiaOcularsignsAdditionalneurologicalfeaturesOtherfeaturesMRILPNCS/EMGOtherinvestigationsMusclebiopsyOthernegativemolecularinvestigations9,M704030Puremidlineataxia?(stick)-NoneNoneNoneCANDNDNormalIHCNormalRCESCA12mt.DNALR-PCR10,M594415Puremidlineataxia????NoneProminentdysarthria,chokingBriskreflexesNoneCANDNDNormalQ10SPG7SCA8SCA1211,F654712Puremidlineataxia???(WhC)?OscillopsiaJerkypursuitsHorizontalnystagmusHypometricsaccadesDorsalrootganglionopathyNeurogenicbladderDistalwastingandweaknessAreflexiaCataract,diabetesandshortstatureMildCA;highsignalC3,4posteriorcolumns;thincord-OCBDRGNDPOLGSPG7POLG2PEO1ANT1mt.DNALR-PCR12,M836023MidlineataxiaEarlyalcoholsensitivity?? (stick)?JerkypursuitCoarsephasicnystagmusNormalsaccadesNoneNoneMildCANDNDPatientdeclinedNilPresenceorabsenceofsymptomsareindicatedby?or-symbol,respectivelyAFTsautonomicfunctiontests,CACerebellaratrophy,CPEOchronicprogressiveexternalophthalmoplegia,CTScarpaltunnelsyndrome,CVDcerebrovasculardisease,DRGdorsalrootganglionopathy,FrFrame,GENgazeevokednystagmus,IHCimmunohistochemistry,NDnotdone,OAopticatrophy,OCBoligoclonalbands,PVperiventricular,RAPDrelativeafferentpupillarydefect,RCErespiratorychainenzyme,SVDsmallvesseldisease,TLEtemporallobeepilepsy,WhCwheelchair,WMwhitematterJ Neurol (2015) 262:1822–1827 1825123disease, which must be considered and included in appro-priate consent procedures. It must also be noted that neitherWES nor targeted panels are appropriate to screen for ge-nomic rearrangements or trinucleotide repeat sequences.Determining pathogenicity can be challenging forheterozygous variants without a family history of diseaseand additional living family relatives for segregation ana-lysis. In our cohort, we found heterozygous variants inSLC33A1 and PLEKHG4 in single cases (Table 2).Heterozygous mutations in SLC33A1 have been associatedwith spastic paraplegia (SPG42) with ataxia in a singlefamily, and likewise, missense mutations in PLEKHG4 havebeen implicated in dominant late onset forms of spinocere-bellar ataxia in Japanese individuals. Despite the rarity andputative pathogenicity of the variants in our patients, thelack of data to test segregation makes attributing patho-genicity difficult. As NGS begins to develop larger variantdatasets in rare diseases it is vital to share such data throughcollaborative projects which may aid pathogenicity confir-mation through the identification of the same or relatedvariants in unrelated families with a similar phenotype.In conclusion, we have demonstrated that application ofWES to a cohort of unrelated individuals following ex-clusion of common trinucleotide repeat disorders estab-lishes a molecular cause of disease in a third of cases.These findings have significant implications for clinicalpractise.Acknowledgments MJK is a Wellcome Trust Clinical ResearchTraining Fellow. PFC is an Honorary Consultant Neurologist atNewcastle upon Tyne Foundation Hospitals NHS Trust, is a Well-come Trust Senior Fellow in Clinical Science (101876/Z/13/Z), and aUK NIHR Senior Investigator. PFC receives additional support fromthe Wellcome Trust Centre for Mitochondrial Research (096919Z/11/Z), the Medical Research Council (UK) Centre for TranslationalMuscle Disease research (G0601943), and EU FP7 TIRCON, and theNational Institute for Health Research (NIHR) Newcastle BiomedicalResearch Centre based at Newcastle upon Tyne Hospitals NHSFoundation Trust and Newcastle University. The views expressed arethose of the author(s) and not necessarily those of the NHS, the NIHRor the Department of Health. RH was supported by the Medical Re-search Council (UK) (G1000848) and the European Research Council(309548).Conflicts of interest The authors report no conflicts of interest.Open Access This article is distributed under the terms of theCreative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricteduse, distribution, and reproduction in any medium, provided you giveappropriate credit to the original author(s) and the source, provide alink to the Creative Commons license, and indicate if changes weremade.References1. Abele M, Burk K, Schols L, Schwartz S, Besenthal I, Dichgans J,Zuhlke C, Riess O, Klockgether T (2002) The aetiology of spo-radic adult-onset ataxia. Brain J Neurol 125:961–968Table 2 Genetic variants of interest identified in the 12 patientsPathogenic variantsPt Gene Model Exome seqidentifiedvariant (1)rs# MAF variant (1) Exome seqidentifiedvariant (2)rs# MAF variant (2)VariantpathogenicitypredictionESP6500 1000 g ESP6500 1000 g1 SPG7 AR c.1529C[Tp. Ala510Valrs61755320 0.003463 0.0014 c. 1053dupCp. Gly352fsNA 0 0 (1) D:D:D:D(2) NA2 SPG7 AR c.1529C[Tp. Ala510Valrs61755320 0.003463 0.0014 c.233T[Ap. Leu78*rs121918358 0.000077 0 (1) D:D:D:D(2) Pathogenic3 ANO10 AR c.1843G[Ap. Asp615Asnrs138000380 0.000231 0.0005 c. 132_133insTp. Asp45fsNA 0 0 (1) D:D:D:P(2) NA4 SYNE1 AR c.9148C[Gp. Leu3050Valrs117360770 0.002307 0.0018 c.1762delCp. Leu588fsNA 0.003435 0 (1) D:D:D:D(2) NAVariants of uncertain significance5 SLC33A1 AD c.433G[Ap. 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Frequency of rare recessive mutations in unexplained late onset cerebellar ataxia

Apollo (Cambridge)

Frequency of rare recessive mutations in unexplained late onset cerebellar ataxia.

http://dx.doi.org/10.1007/s00415-015-7772-x

Frequency of rare recessive mutations in unexplained late onset cerebellar ataxia.

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