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October 26, 2004; 63 (8) Articles

Clinical and neuropathologic variation in neuronal intermediate filament inclusion disease

N. J. Cairns, M. Grossman, S. E. Arnold, D. J. Burn, E. Jaros, R. H. Perry, C. Duyckaerts, B. Stankoff, B. Pillon, K. Skullerud, F. F. Cruz-Sanchez, E. H. Bigio, I. R.A. Mackenzie, M. Gearing, J. L. Juncos, J. D. Glass, H. Yokoo, Y. Nakazato, S. Mosaheb, J. R. Thorpe, K. Uryu, V. M.-Y. Lee, J .Q. Trojanowski
First published October 25, 2004, DOI: https://doi.org/10.1212/01.WNL.0000139809.16817.DD
N. J. Cairns
PhD
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M. Grossman
MD
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S. E. Arnold
MD
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D. J. Burn
MD
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E. Jaros
PhD
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R. H. Perry
MD
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C. Duyckaerts
MD
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B. Stankoff
MD
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B. Pillon
PhD
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K. Skullerud
MD
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F. F. Cruz-Sanchez
MD
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E. H. Bigio
MD
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I. R.A. Mackenzie
MD
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M. Gearing
PhD
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J. L. Juncos
MD
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J. D. Glass
MD
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H. Yokoo
MD
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Y. Nakazato
MD
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S. Mosaheb
BSc
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J. R. Thorpe
DPhil
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K. Uryu
PhD
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V. M.-Y. Lee
PhD
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J .Q. Trojanowski
MD PhD
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Full PDF
Citation
Clinical and neuropathologic variation in neuronal intermediate filament inclusion disease
N. J. Cairns, M. Grossman, S. E. Arnold, D. J. Burn, E. Jaros, R. H. Perry, C. Duyckaerts, B. Stankoff, B. Pillon, K. Skullerud, F. F. Cruz-Sanchez, E. H. Bigio, I. R.A. Mackenzie, M. Gearing, J. L. Juncos, J. D. Glass, H. Yokoo, Y. Nakazato, S. Mosaheb, J. R. Thorpe, K. Uryu, V. M.-Y. Lee, J .Q. Trojanowski
Neurology Oct 2004, 63 (8) 1376-1384; DOI: 10.1212/01.WNL.0000139809.16817.DD

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Abstract

Background: Recently described neuronal intermediate filament inclusion disease (NIFID) shows considerable clinical heterogeneity.

Objective: To assess the spectrum of the clinical and neuropathological features in 10 NIFID cases.

Methods: Retrospective chart and comprehensive neuropathological review of these NIFID cases was conducted.

Results: The mean age at onset was 40.8 (range 23 to 56) years, mean disease duration was 4.5 (range 2.7 to 13) years, and mean age at death was 45.3 (range 28 to 61) years. The most common presenting symptoms were behavioral and personality changes in 7 of 10 cases and, less often, memory loss, cognitive impairment, language deficits, and motor weakness. Extrapyramidal features were present in 8 of 10 patients. Language impairment, perseveration, executive dysfunction, hyperreflexia, and primitive reflexes were frequent signs, whereas a minority had buccofacial apraxia, supranuclear ophthalmoplegia, upper motor neuron disease (MND), and limb dystonia. Frontotemporal and caudate atrophy were common. Histologic changes were extensive in many cortical areas, deep gray matter, cerebellum, and spinal cord. The hallmark lesions of NIFID were unique neuronal IF inclusions detected most robustly by antibodies to neurofilament triplet proteins and α-internexin.

Conclusion: NIFID is a neuropathologically distinct, clinically heterogeneous variant of frontotemporal dementia (FTD) that may include parkinsonism or MND. Neuronal IF inclusions are the neuropathological signatures of NIFID that distinguish it from all other FTD variants including FTD with MND and FTD tauopathies.

  • Received March 8, 2004.
  • Accepted May 11, 2004.
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