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December 14, 2010; 75 (24) Articles

Does TDP-43 type confer a distinct pattern of atrophy in frontotemporal lobar degeneration?

J.L. Whitwell, C.R. Jack, J.E. Parisi, M.L. Senjem, D.S. Knopman, B.F. Boeve, R. Rademakers, M. Baker, R.C. Petersen, D.W. Dickson, K.A. Josephs
First published December 13, 2010, DOI: https://doi.org/10.1212/WNL.0b013e31820203c2
J.L. Whitwell
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C.R. Jack Jr.
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J.E. Parisi
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M.L. Senjem
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D.S. Knopman
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B.F. Boeve
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R. Rademakers
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M. Baker
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R.C. Petersen
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D.W. Dickson
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K.A. Josephs
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Citation
Does TDP-43 type confer a distinct pattern of atrophy in frontotemporal lobar degeneration?
J.L. Whitwell, C.R. Jack, J.E. Parisi, M.L. Senjem, D.S. Knopman, B.F. Boeve, R. Rademakers, M. Baker, R.C. Petersen, D.W. Dickson, K.A. Josephs
Neurology Dec 2010, 75 (24) 2212-2220; DOI: 10.1212/WNL.0b013e31820203c2

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Abstract

Objective: To determine whether TDP-43 type is associated with distinct patterns of brain atrophy on MRI in subjects with pathologically confirmed frontotemporal lobar degeneration (FTLD).

Methods: In this case-control study, we identified all subjects with a pathologic diagnosis of FTLD with TDP-43 immunoreactive inclusions (FTLD-TDP) and at least one volumetric head MRI scan (n = 42). In each case we applied published criteria for subclassification of FTLD-TDP into FTLD-TDP types 1–3. Voxel-based morphometry was used to compare subjects with each of the different FTLD-TDP types to age- and gender-matched normal controls (n = 30). We also assessed different pathologic and genetic variants within, and across, the different types.

Results: Twenty-two subjects were classified as FTLD-TDP type 1, 9 as type 2, and 11 as type 3. We identified different patterns of atrophy across the types with type 1 showing frontotemporal and parietal atrophy, type 2 predominantly anterior temporal lobe atrophy, and type 3 predominantly posterior frontal atrophy. Within the FTLD-TDP type 1 group, those with a progranulin mutation had significantly more lateral temporal lobe atrophy than those without. All type 2 subjects were diagnosed with semantic dementia. Subjects with a pathologic diagnosis of FTLD with motor neuron degeneration had a similar pattern of atrophy, regardless of whether they were type 1 or type 3.

Conclusions: Although there are different patterns of atrophy across the different FTLD-TDP types, it appears that genetic and pathologic factors may also affect the patterns of atrophy.

Footnotes

  • Study funding: Supported by The Dana Foundation, NIH grants R01-AG037491, R01-DC010367, P50-AG16574, U01-AG06786, R01-AG11378, and R01 NS065782, as well as the Robert H. and Clarice Smith and Abigail Van Buren Alzheimer's Disease Research Program of the Mayo Foundation, the Alexander Family Alzheimer's Disease Research Professorship of the Mayo Foundation, and the NIH Construction Grant (NIH C06 RR018898).

  • AD
    Alzheimer disease
    ADRC
    Alzheimer's Disease Research Center
    bvFTD
    behavioral variant frontotemporal dementia
    CBS
    corticobasal syndrome
    CDR-SB
    Clinical Dementia Rating scale sum of boxes
    FTLD
    frontotemporal lobar degeneration
    FTLD-MND
    frontotemporal lobar degeneration with motor neuron degeneration
    FTLD-TDP
    frontotemporal lobar degeneration with TDP-43 immunoreactive inclusions
    MMSE
    Mini-Mental State Examination
    NCI
    neuronal cytoplasmic inclusion
    PNFA
    progressive nonfluent aphasia
    SMD
    semantic dementia
    STMS
    Short Test of Mental Status
    VBM
    voxel-based morphometry.

  • Supplemental data at www.neurology.org

  • Received June 1, 2010.
  • Accepted August 24, 2010.
  • Copyright © 2010 by AAN Enterprises, Inc.
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