Prospective natural history study of C9orf72 ALS clinical characteristics and biomarkers

Alexander J. Cammack; Nazem Atassi; Theodore Hyman; Leonard H. Van Den Berg; Matthew Harms; Robert H. Baloh; Robert H. Brown; Michael A. Van Es; Jan H. Veldink; Balint S. De Vries; Jeffrey D. Rothstein; Caroline Drain; Jennifer Jockel-Balsarotti; Amber Malcolm; Sonia Boodram; Amber Salter; Nicholas Wightman; Hong Yu; Alexander V. Sherman; Thomas J. Esparza; Diane McKenna-Yasek; Margaret A. Owegi; Catherine Douthwright; Alexander McCampbell; Toby Ferguson; Carlos Cruchaga; Merit Cudkowicz; Timothy M. Miller

doi:10.1212/WNL.0000000000008359

Prospective natural history study of C9orf72 ALS clinical characteristics and biomarkers

Alexander J. Cammack, Nazem Atassi, Theodore Hyman, Leonard H. Van Den Berg, Matthew Harms, Robert H. Baloh, Robert H. Brown, Michael A. Van Es, Jan H. Veldink, Balint S. De Vries, Jeffrey D. Rothstein, Caroline Drain, Jennifer Jockel-Balsarotti, Amber Malcolm, Sonia Boodram, Amber Salter, Nicholas Wightman, Hong Yu, Alexander V. Sherman, Thomas J. EsparzaDiane McKenna-Yasek, Margaret A. Owegi, Catherine Douthwright, Alexander McCampbell, Toby Ferguson, Carlos Cruchaga, Merit Cudkowicz, Timothy M. Miller

Research output: Contribution to journal › Article › peer-review

22 Scopus citations

Abstract

ObjectiveTo define the natural history of the C9orf72 amyotrophic lateral sclerosis (C9ALS) patient population, develop disease biomarkers, and characterize patient pathologies.MethodsWe prospectively collected clinical and demographic data from 116 symptomatic C9ALS and 12 non-amyotrophic lateral sclerosis (ALS) full expansion carriers across 7 institutions in the United States and the Netherlands. In addition, we collected blood samples for DNA repeat size assessment, CSF samples for biomarker identification, and autopsy samples for dipeptide repeat protein (DPR) size determination. Finally, we collected retrospective clinical data via chart review from 208 individuals with C9ALS and 450 individuals with singleton ALS.ResultsThe mean age at onset in the symptomatic prospective cohort was 57.9 ± 8.3 years, and median duration of survival after onset was 36.9 months. The monthly change was -1.8 ± 1.7 for ALS Functional Rating Scale-Revised and -1.4% ± 3.24% of predicted for slow vital capacity. In blood DNA, we found that G₄C₂ repeat size correlates positively with age. In CSF, we observed that concentrations of poly(GP) negatively correlate with DNA expansion size but do not correlate with measures of disease progression. Finally, we found that size of poly(GP) dipeptides in the brain can reach large sizes similar to that of their DNA repeat derivatives.ConclusionsWe present a thorough investigation of C9ALS natural history, providing the basis for C9ALS clinical trial design. We found that clinical features of this genetic subset are less variant than in singleton ALS. In addition, we identified important correlations of C9ALS patient pathologies with clinical and demographic data.

Original language	English (US)
Pages (from-to)	E1605-E1617
Journal	Neurology
Volume	93
Issue number	17
DOIs	https://doi.org/10.1212/WNL.0000000000008359
State	Published - Oct 22 2019
Externally published	Yes

ASJC Scopus subject areas

Clinical Neurology

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10.1212/WNL.0000000000008359

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Cammack, A. J., Atassi, N., Hyman, T., Van Den Berg, L. H., Harms, M., Baloh, R. H., Brown, R. H., Van Es, M. A., Veldink, J. H., De Vries, B. S., Rothstein, J. D., Drain, C., Jockel-Balsarotti, J., Malcolm, A., Boodram, S., Salter, A., Wightman, N., Yu, H., Sherman, A. V., ... Miller, T. M. (2019). Prospective natural history study of C9orf72 ALS clinical characteristics and biomarkers. Neurology, 93(17), E1605-E1617. https://doi.org/10.1212/WNL.0000000000008359

Cammack, AJ, Atassi, N, Hyman, T, Van Den Berg, LH, Harms, M, Baloh, RH, Brown, RH, Van Es, MA, Veldink, JH, De Vries, BS, Rothstein, JD, Drain, C, Jockel-Balsarotti, J, Malcolm, A, Boodram, S, Salter, A, Wightman, N, Yu, H, Sherman, AV, Esparza, TJ, McKenna-Yasek, D, Owegi, MA, Douthwright, C, McCampbell, A, Ferguson, T, Cruchaga, C, Cudkowicz, M & Miller, TM 2019, 'Prospective natural history study of C9orf72 ALS clinical characteristics and biomarkers', Neurology, vol. 93, no. 17, pp. E1605-E1617. https://doi.org/10.1212/WNL.0000000000008359

@article{00372a0f22e1430683ee8daaf08265cd,

title = "Prospective natural history study of C9orf72 ALS clinical characteristics and biomarkers",

abstract = "ObjectiveTo define the natural history of the C9orf72 amyotrophic lateral sclerosis (C9ALS) patient population, develop disease biomarkers, and characterize patient pathologies.MethodsWe prospectively collected clinical and demographic data from 116 symptomatic C9ALS and 12 non-amyotrophic lateral sclerosis (ALS) full expansion carriers across 7 institutions in the United States and the Netherlands. In addition, we collected blood samples for DNA repeat size assessment, CSF samples for biomarker identification, and autopsy samples for dipeptide repeat protein (DPR) size determination. Finally, we collected retrospective clinical data via chart review from 208 individuals with C9ALS and 450 individuals with singleton ALS.ResultsThe mean age at onset in the symptomatic prospective cohort was 57.9 ± 8.3 years, and median duration of survival after onset was 36.9 months. The monthly change was -1.8 ± 1.7 for ALS Functional Rating Scale-Revised and -1.4% ± 3.24% of predicted for slow vital capacity. In blood DNA, we found that G4C2 repeat size correlates positively with age. In CSF, we observed that concentrations of poly(GP) negatively correlate with DNA expansion size but do not correlate with measures of disease progression. Finally, we found that size of poly(GP) dipeptides in the brain can reach large sizes similar to that of their DNA repeat derivatives.ConclusionsWe present a thorough investigation of C9ALS natural history, providing the basis for C9ALS clinical trial design. We found that clinical features of this genetic subset are less variant than in singleton ALS. In addition, we identified important correlations of C9ALS patient pathologies with clinical and demographic data.",

author = "Cammack, {Alexander J.} and Nazem Atassi and Theodore Hyman and {Van Den Berg}, {Leonard H.} and Matthew Harms and Baloh, {Robert H.} and Brown, {Robert H.} and {Van Es}, {Michael A.} and Veldink, {Jan H.} and {De Vries}, {Balint S.} and Rothstein, {Jeffrey D.} and Caroline Drain and Jennifer Jockel-Balsarotti and Amber Malcolm and Sonia Boodram and Amber Salter and Nicholas Wightman and Hong Yu and Sherman, {Alexander V.} and Esparza, {Thomas J.} and Diane McKenna-Yasek and Owegi, {Margaret A.} and Catherine Douthwright and Alexander McCampbell and Toby Ferguson and Carlos Cruchaga and Merit Cudkowicz and Miller, {Timothy M.}",

note = "Funding Information: A. Cammack reports no disclosures relevant to the manuscript. N. Atassi has consulted for MT Pharma, Neuropore, Chronos, Boston Pharmaceuticals, Denali, GSK, and Anelixis. T. Hyman reports no disclosures relevant to the manuscript. L. van den Berg has received personal fees from Shire, Biogen, Cytokinetics, and Treeway, outside the submitted work. M. Harms has grant funding from Biogen. R. Baloh has consulted for Kite Pharmaceuticals, Maze Therapeutics, and Acurastem. R. Brown, M. van Es, J. Veldink, and B. de Vries report no disclosures relevant to the manuscript. J. Rothstein is a consultant for Glaxo Smith Kline and Expansion Therapeutics. C. Drain, J. Jockel-Balsarotti, A. Malcolm, and S. Boodram report no disclosures relevant to the manuscript. A. Salter has received consulting fees for statistical reviews in Circulation: Cardiovascular Imaging. N. Wightman, H. Yu, A. Sherman, T. Esparza, D. McKenna-Yasek, M. Owegi, and C. Douthwright report no disclosures relevant to the manuscript. A. McCampbell is an employee of Biogen. T. Ferguson is an employee of Biogen. C. Cruchaga receives research support from Biogen, EISAI, Alector, and Parabon and is a member of the advisory board of ADx Healthcare, Halia Therapeutics, and Vivid Genomics. M. Cudkowicz is a consultant for Bio-haven, Takeda, Avexis, and Biogen and was chair of DSMB for Lilly. T. Miller has served on medical advisory boards for Biogen and Ionis Pharmaceuticals and is a consultant for Cytokinetics. T.M. Miller and Washington University have a licensing agreement with Ionis Pharmaceuticals and with C2N. Go to Neurology.org/N for full disclosures. Publisher Copyright: {\textcopyright} 2019 American Academy of Neurology.",

year = "2019",

month = oct,

day = "22",

doi = "10.1212/WNL.0000000000008359",

language = "English (US)",

volume = "93",

pages = "E1605--E1617",

journal = "Neurology",

issn = "0028-3878",

publisher = "Lippincott Williams and Wilkins",

number = "17",

}

TY - JOUR

T1 - Prospective natural history study of C9orf72 ALS clinical characteristics and biomarkers

AU - Cammack, Alexander J.

AU - Atassi, Nazem

AU - Hyman, Theodore

AU - Van Den Berg, Leonard H.

AU - Harms, Matthew

AU - Baloh, Robert H.

AU - Brown, Robert H.

AU - Van Es, Michael A.

AU - Veldink, Jan H.

AU - De Vries, Balint S.

AU - Rothstein, Jeffrey D.

AU - Drain, Caroline

AU - Jockel-Balsarotti, Jennifer

AU - Malcolm, Amber

AU - Boodram, Sonia

AU - Salter, Amber

AU - Wightman, Nicholas

AU - Yu, Hong

AU - Sherman, Alexander V.

AU - Esparza, Thomas J.

AU - McKenna-Yasek, Diane

AU - Owegi, Margaret A.

AU - Douthwright, Catherine

AU - McCampbell, Alexander

AU - Ferguson, Toby

AU - Cruchaga, Carlos

AU - Cudkowicz, Merit

AU - Miller, Timothy M.

N1 - Funding Information: A. Cammack reports no disclosures relevant to the manuscript. N. Atassi has consulted for MT Pharma, Neuropore, Chronos, Boston Pharmaceuticals, Denali, GSK, and Anelixis. T. Hyman reports no disclosures relevant to the manuscript. L. van den Berg has received personal fees from Shire, Biogen, Cytokinetics, and Treeway, outside the submitted work. M. Harms has grant funding from Biogen. R. Baloh has consulted for Kite Pharmaceuticals, Maze Therapeutics, and Acurastem. R. Brown, M. van Es, J. Veldink, and B. de Vries report no disclosures relevant to the manuscript. J. Rothstein is a consultant for Glaxo Smith Kline and Expansion Therapeutics. C. Drain, J. Jockel-Balsarotti, A. Malcolm, and S. Boodram report no disclosures relevant to the manuscript. A. Salter has received consulting fees for statistical reviews in Circulation: Cardiovascular Imaging. N. Wightman, H. Yu, A. Sherman, T. Esparza, D. McKenna-Yasek, M. Owegi, and C. Douthwright report no disclosures relevant to the manuscript. A. McCampbell is an employee of Biogen. T. Ferguson is an employee of Biogen. C. Cruchaga receives research support from Biogen, EISAI, Alector, and Parabon and is a member of the advisory board of ADx Healthcare, Halia Therapeutics, and Vivid Genomics. M. Cudkowicz is a consultant for Bio-haven, Takeda, Avexis, and Biogen and was chair of DSMB for Lilly. T. Miller has served on medical advisory boards for Biogen and Ionis Pharmaceuticals and is a consultant for Cytokinetics. T.M. Miller and Washington University have a licensing agreement with Ionis Pharmaceuticals and with C2N. Go to Neurology.org/N for full disclosures. Publisher Copyright: © 2019 American Academy of Neurology.

PY - 2019/10/22

Y1 - 2019/10/22

N2 - ObjectiveTo define the natural history of the C9orf72 amyotrophic lateral sclerosis (C9ALS) patient population, develop disease biomarkers, and characterize patient pathologies.MethodsWe prospectively collected clinical and demographic data from 116 symptomatic C9ALS and 12 non-amyotrophic lateral sclerosis (ALS) full expansion carriers across 7 institutions in the United States and the Netherlands. In addition, we collected blood samples for DNA repeat size assessment, CSF samples for biomarker identification, and autopsy samples for dipeptide repeat protein (DPR) size determination. Finally, we collected retrospective clinical data via chart review from 208 individuals with C9ALS and 450 individuals with singleton ALS.ResultsThe mean age at onset in the symptomatic prospective cohort was 57.9 ± 8.3 years, and median duration of survival after onset was 36.9 months. The monthly change was -1.8 ± 1.7 for ALS Functional Rating Scale-Revised and -1.4% ± 3.24% of predicted for slow vital capacity. In blood DNA, we found that G4C2 repeat size correlates positively with age. In CSF, we observed that concentrations of poly(GP) negatively correlate with DNA expansion size but do not correlate with measures of disease progression. Finally, we found that size of poly(GP) dipeptides in the brain can reach large sizes similar to that of their DNA repeat derivatives.ConclusionsWe present a thorough investigation of C9ALS natural history, providing the basis for C9ALS clinical trial design. We found that clinical features of this genetic subset are less variant than in singleton ALS. In addition, we identified important correlations of C9ALS patient pathologies with clinical and demographic data.

AB - ObjectiveTo define the natural history of the C9orf72 amyotrophic lateral sclerosis (C9ALS) patient population, develop disease biomarkers, and characterize patient pathologies.MethodsWe prospectively collected clinical and demographic data from 116 symptomatic C9ALS and 12 non-amyotrophic lateral sclerosis (ALS) full expansion carriers across 7 institutions in the United States and the Netherlands. In addition, we collected blood samples for DNA repeat size assessment, CSF samples for biomarker identification, and autopsy samples for dipeptide repeat protein (DPR) size determination. Finally, we collected retrospective clinical data via chart review from 208 individuals with C9ALS and 450 individuals with singleton ALS.ResultsThe mean age at onset in the symptomatic prospective cohort was 57.9 ± 8.3 years, and median duration of survival after onset was 36.9 months. The monthly change was -1.8 ± 1.7 for ALS Functional Rating Scale-Revised and -1.4% ± 3.24% of predicted for slow vital capacity. In blood DNA, we found that G4C2 repeat size correlates positively with age. In CSF, we observed that concentrations of poly(GP) negatively correlate with DNA expansion size but do not correlate with measures of disease progression. Finally, we found that size of poly(GP) dipeptides in the brain can reach large sizes similar to that of their DNA repeat derivatives.ConclusionsWe present a thorough investigation of C9ALS natural history, providing the basis for C9ALS clinical trial design. We found that clinical features of this genetic subset are less variant than in singleton ALS. In addition, we identified important correlations of C9ALS patient pathologies with clinical and demographic data.

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DO - 10.1212/WNL.0000000000008359

M3 - Article

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SP - E1605-E1617

JO - Neurology

JF - Neurology

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ER -

Prospective natural history study of C9orf72 ALS clinical characteristics and biomarkers

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