Clinical and genetic characteristics of sporadic adult-onset degenerative ataxia

Ilaria Giordano; Florian Harmuth; Heike Jacobi; Brigitte Paap; Stefan Vielhaber; Judith Machts; Ludger Schã¶ls; Matthis Synofzik; Marc Sturm; Chantal Tallaksen; Iselin M. Wedding; Sylvia Boesch; Andreas Eigentler; Bart Van De Warrenburg; Judith Van Gaalen; Christoph Kamm; Ales Dudesek; Jun-suk Kang; Dagmar Timmann; Gabriella Silvestri; Marcella Masciullo; Thomas Klopstock; Christiane Neuhofer; Christos Ganos; Alessandro Filla; Peter Bauer; Sophie Tezenas Du Montcel; Thomas Klockgether

doi:10.1212/WNL.0000000000004311

Clinical and genetic characteristics of sporadic adult-onset degenerative ataxia

Ilaria Giordano, Florian Harmuth, Heike Jacobi, Brigitte Paap, Stefan Vielhaber, Judith Machts, Ludger Schã¶ls, Matthis Synofzik, Marc Sturm, Chantal Tallaksen, Iselin M. Wedding, Sylvia Boesch, Andreas Eigentler, Bart Van De Warrenburg, Judith Van Gaalen, Christoph Kamm, Ales Dudesek, Jun-suk Kang, Dagmar Timmann, Gabriella SilvestriMarcella Masciullo, Thomas Klopstock, Christiane Neuhofer, Christos Ganos, Alessandro Filla, Peter Bauer, Sophie Tezenas Du Montcel, Thomas Klockgether^*

^*Autore corrispondente per questo lavoro

Risultato della ricerca: Contributo in rivista › Articolo

22 Citazioni (Scopus)

Abstract

To define the clinical phenotype and natural history of sporadic adult-onset degenerative ataxia and to identify putative disease-causing mutations. Methods: The primary measure of disease severity was the Scale for the Assessment and Rating of Ataxia (SARA). DNA samples were screened for mutations using a high-coverage ataxia-specific gene panel in combination with next-generation sequencing. Results: The analysis was performed on 249 participants. Among them, 83 met diagnostic criteria of clinically probable multiple system atrophy cerebellar type (MSA-C) at baseline and another 12 during follow-up. Positive MSA-C criteria (4.94 Â± 0.74, p < 0.0001) and disease duration (0.22 Â± 0.06 per additional year, p = 0.0007) were associated with a higher SARA score. Forty-eight participants who did not fulfill MSA-C criteria and had a disease duration of >10 years were designated sporadic adult-onset ataxia of unknown etiology/non-MSA (SAOA/non-MSA). Compared with MSA-C, SAOA/non-MSA patients had lower SARA scores (13.6 Â± 6.0 vs 16.0 Â± 5.8, p = 0.0200) and a slower annual SARA increase (1.1 Â± 2.3 vs 3.3 Â± 3.2, p = 0.0013). In 11 of 194 tested participants (6%), a definitive or probable genetic diagnosis was made. Conclusions: Our study provides quantitative data on the clinical phenotype and progression of sporadic ataxia with adult onset. Screening for causative mutations with a gene panel approach yielded a genetic diagnosis in 6% of the cohort. ClinicalTrials.gov registration: NCT02701036.

Lingua originale	Inglese
pagine (da-a)	1043-1049
Numero di pagine	7
Rivista	Neurology
Volume	89
Numero di pubblicazione	10
DOI	https://doi.org/10.1212/WNL.0000000000004311
Stato di pubblicazione	Pubblicato - 2017

All Science Journal Classification (ASJC) codes

Neurologia (clinica)

Keywords

Aged
Ataxia
DNA Mutational Analysis
Europe
Female
Follow-Up Studies
Humans
Male
Middle Aged
Mutation
Neurodegenerative Diseases
Neurology (clinical)
Severity of Illness Index

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10.1212/WNL.0000000000004311

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Giordano, I., Harmuth, F., Jacobi, H., Paap, B., Vielhaber, S., Machts, J., Schã¶ls, L., Synofzik, M., Sturm, M., Tallaksen, C., Wedding, I. M., Boesch, S., Eigentler, A., Van De Warrenburg, B., Van Gaalen, J., Kamm, C., Dudesek, A., Kang, J., Timmann, D., ... Klockgether, T. (2017). Clinical and genetic characteristics of sporadic adult-onset degenerative ataxia. Neurology, 89(10), 1043-1049. https://doi.org/10.1212/WNL.0000000000004311

@article{98849efa8e1742738dd42e79d93491a3,

title = "Clinical and genetic characteristics of sporadic adult-onset degenerative ataxia",

abstract = "To define the clinical phenotype and natural history of sporadic adult-onset degenerative ataxia and to identify putative disease-causing mutations. Methods: The primary measure of disease severity was the Scale for the Assessment and Rating of Ataxia (SARA). DNA samples were screened for mutations using a high-coverage ataxia-specific gene panel in combination with next-generation sequencing. Results: The analysis was performed on 249 participants. Among them, 83 met diagnostic criteria of clinically probable multiple system atrophy cerebellar type (MSA-C) at baseline and another 12 during follow-up. Positive MSA-C criteria (4.94 {\^A}± 0.74, p < 0.0001) and disease duration (0.22 {\^A}± 0.06 per additional year, p = 0.0007) were associated with a higher SARA score. Forty-eight participants who did not fulfill MSA-C criteria and had a disease duration of >10 years were designated sporadic adult-onset ataxia of unknown etiology/non-MSA (SAOA/non-MSA). Compared with MSA-C, SAOA/non-MSA patients had lower SARA scores (13.6 {\^A}± 6.0 vs 16.0 {\^A}± 5.8, p = 0.0200) and a slower annual SARA increase (1.1 {\^A}± 2.3 vs 3.3 {\^A}± 3.2, p = 0.0013). In 11 of 194 tested participants (6\%), a definitive or probable genetic diagnosis was made. Conclusions: Our study provides quantitative data on the clinical phenotype and progression of sporadic ataxia with adult onset. Screening for causative mutations with a gene panel approach yielded a genetic diagnosis in 6\% of the cohort. ClinicalTrials.gov registration: NCT02701036.",

keywords = "Aged, Ataxia, DNA Mutational Analysis, Europe, Female, Follow-Up Studies, Humans, Male, Middle Aged, Mutation, Neurodegenerative Diseases, Neurology (clinical), Severity of Illness Index, Aged, Ataxia, DNA Mutational Analysis, Europe, Female, Follow-Up Studies, Humans, Male, Middle Aged, Mutation, Neurodegenerative Diseases, Neurology (clinical), Severity of Illness Index",

author = "Ilaria Giordano and Florian Harmuth and Heike Jacobi and Brigitte Paap and Stefan Vielhaber and Judith Machts and Ludger Sch{\~a}¶ls and Matthis Synofzik and Marc Sturm and Chantal Tallaksen and Wedding, \{Iselin M.\} and Sylvia Boesch and Andreas Eigentler and \{Van De Warrenburg\}, Bart and \{Van Gaalen\}, Judith and Christoph Kamm and Ales Dudesek and Jun-suk Kang and Dagmar Timmann and Gabriella Silvestri and Marcella Masciullo and Thomas Klopstock and Christiane Neuhofer and Christos Ganos and Alessandro Filla and Peter Bauer and \{Tezenas Du Montcel\}, Sophie and Thomas Klockgether",

year = "2017",

doi = "10.1212/WNL.0000000000004311",

language = "English",

volume = "89",

pages = "1043--1049",

journal = "Neurology",

issn = "0028-3878",

publisher = "Lippincott Williams and Wilkins",

number = "10",

}

Giordano, I, Harmuth, F, Jacobi, H, Paap, B, Vielhaber, S, Machts, J, Schã¶ls, L, Synofzik, M, Sturm, M, Tallaksen, C, Wedding, IM, Boesch, S, Eigentler, A, Van De Warrenburg, B, Van Gaalen, J, Kamm, C, Dudesek, A, Kang, J, Timmann, D, Silvestri, G, Masciullo, M, Klopstock, T, Neuhofer, C, Ganos, C, Filla, A, Bauer, P, Tezenas Du Montcel, S & Klockgether, T 2017, 'Clinical and genetic characteristics of sporadic adult-onset degenerative ataxia', Neurology, vol. 89, n. 10, pagg. 1043-1049. https://doi.org/10.1212/WNL.0000000000004311

TY - JOUR

T1 - Clinical and genetic characteristics of sporadic adult-onset degenerative ataxia

AU - Giordano, Ilaria

AU - Harmuth, Florian

AU - Jacobi, Heike

AU - Paap, Brigitte

AU - Vielhaber, Stefan

AU - Machts, Judith

AU - Schã¶ls, Ludger

AU - Synofzik, Matthis

AU - Sturm, Marc

AU - Tallaksen, Chantal

AU - Wedding, Iselin M.

AU - Boesch, Sylvia

AU - Eigentler, Andreas

AU - Van De Warrenburg, Bart

AU - Van Gaalen, Judith

AU - Kamm, Christoph

AU - Dudesek, Ales

AU - Kang, Jun-suk

AU - Timmann, Dagmar

AU - Silvestri, Gabriella

AU - Masciullo, Marcella

AU - Klopstock, Thomas

AU - Neuhofer, Christiane

AU - Ganos, Christos

AU - Filla, Alessandro

AU - Bauer, Peter

AU - Tezenas Du Montcel, Sophie

AU - Klockgether, Thomas

PY - 2017

Y1 - 2017

N2 - To define the clinical phenotype and natural history of sporadic adult-onset degenerative ataxia and to identify putative disease-causing mutations. Methods: The primary measure of disease severity was the Scale for the Assessment and Rating of Ataxia (SARA). DNA samples were screened for mutations using a high-coverage ataxia-specific gene panel in combination with next-generation sequencing. Results: The analysis was performed on 249 participants. Among them, 83 met diagnostic criteria of clinically probable multiple system atrophy cerebellar type (MSA-C) at baseline and another 12 during follow-up. Positive MSA-C criteria (4.94 Â± 0.74, p < 0.0001) and disease duration (0.22 Â± 0.06 per additional year, p = 0.0007) were associated with a higher SARA score. Forty-eight participants who did not fulfill MSA-C criteria and had a disease duration of >10 years were designated sporadic adult-onset ataxia of unknown etiology/non-MSA (SAOA/non-MSA). Compared with MSA-C, SAOA/non-MSA patients had lower SARA scores (13.6 Â± 6.0 vs 16.0 Â± 5.8, p = 0.0200) and a slower annual SARA increase (1.1 Â± 2.3 vs 3.3 Â± 3.2, p = 0.0013). In 11 of 194 tested participants (6%), a definitive or probable genetic diagnosis was made. Conclusions: Our study provides quantitative data on the clinical phenotype and progression of sporadic ataxia with adult onset. Screening for causative mutations with a gene panel approach yielded a genetic diagnosis in 6% of the cohort. ClinicalTrials.gov registration: NCT02701036.

AB - To define the clinical phenotype and natural history of sporadic adult-onset degenerative ataxia and to identify putative disease-causing mutations. Methods: The primary measure of disease severity was the Scale for the Assessment and Rating of Ataxia (SARA). DNA samples were screened for mutations using a high-coverage ataxia-specific gene panel in combination with next-generation sequencing. Results: The analysis was performed on 249 participants. Among them, 83 met diagnostic criteria of clinically probable multiple system atrophy cerebellar type (MSA-C) at baseline and another 12 during follow-up. Positive MSA-C criteria (4.94 Â± 0.74, p < 0.0001) and disease duration (0.22 Â± 0.06 per additional year, p = 0.0007) were associated with a higher SARA score. Forty-eight participants who did not fulfill MSA-C criteria and had a disease duration of >10 years were designated sporadic adult-onset ataxia of unknown etiology/non-MSA (SAOA/non-MSA). Compared with MSA-C, SAOA/non-MSA patients had lower SARA scores (13.6 Â± 6.0 vs 16.0 Â± 5.8, p = 0.0200) and a slower annual SARA increase (1.1 Â± 2.3 vs 3.3 Â± 3.2, p = 0.0013). In 11 of 194 tested participants (6%), a definitive or probable genetic diagnosis was made. Conclusions: Our study provides quantitative data on the clinical phenotype and progression of sporadic ataxia with adult onset. Screening for causative mutations with a gene panel approach yielded a genetic diagnosis in 6% of the cohort. ClinicalTrials.gov registration: NCT02701036.

KW - Aged

KW - Ataxia

KW - DNA Mutational Analysis

KW - Europe

KW - Female

KW - Follow-Up Studies

KW - Humans

KW - Male

KW - Middle Aged

KW - Mutation

KW - Neurodegenerative Diseases

KW - Neurology (clinical)

KW - Severity of Illness Index

KW - Aged

KW - Ataxia

KW - DNA Mutational Analysis

KW - Europe

KW - Female

KW - Follow-Up Studies

KW - Humans

KW - Male

KW - Middle Aged

KW - Mutation

KW - Neurodegenerative Diseases

KW - Neurology (clinical)

KW - Severity of Illness Index

UR - https://publicatt.unicatt.it/handle/10807/108011

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UR - https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85028827774&origin=inward

U2 - 10.1212/WNL.0000000000004311

DO - 10.1212/WNL.0000000000004311

M3 - Article

SN - 0028-3878

VL - 89

SP - 1043

EP - 1049

JO - Neurology

JF - Neurology

IS - 10

ER -

Clinical and genetic characteristics of sporadic adult-onset degenerative ataxia

Abstract

All Science Journal Classification (ASJC) codes

Keywords

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