4.7 Article

Imaging correlates of pathology in corticobasal syndrome

期刊

NEUROLOGY
卷 75, 期 21, 页码 1879-1887

出版社

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1212/WNL.0b013e3181feb2e8

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资金

  1. Dana Foundation
  2. NIH [R01-DC010367, P50-AG16574, U01-AG06786, R01-AG11378, NIH C06 RR018898, R01-AG037491, P50 AG16574, UO1 AG06786, RO1 AG15866, NS32352-13, R01-AG023195, U01 AG 06786, R01 HL70825, P50-AG25711, P50-NS40256, P01-AG17216, P01-AG03949, R01-AG15866, ES010751-10]
  3. Mayo Foundation
  4. Pfizer Inc.
  5. Cephalon, Inc.
  6. Alzheimer's Association
  7. Center for Inherited Disease Research [U24 AG026395]
  8. American Parkinson's Disease Association
  9. Elan Corporation
  10. Baxter International Inc.
  11. Forest Laboratories, Inc.
  12. NIH (NIDCD) [R01-DC010367]
  13. NIH (NIA) [R01-AG037491]
  14. NIH (NINDS) [2P50 NS040256-10, P50 NS 40256-R]
  15. NIH/NIA [P50-AG16574, U01-AG06786, R01-AG11378, U01-24904]

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Background: Corticobasal syndrome (CBS) can be associated with different underlying pathologies that are difficult to predict based on clinical presentation. The aim of this study was to determine whether patterns of atrophy on imaging could be useful to help predict underlying pathology in CBS. Methods: This was a case-control study of 24 patients with CBS who had undergone MRI during life and came to autopsy. Pathologic diagnoses included frontotemporal lobar degeneration (FTLD) with TDP-43 immunoreactivity in 5 (CBS-TDP), Alzheimer disease (AD) in 6 (CBS-AD), corticobasal degeneration in 7 (CBS-CBD), and progressive supranuclear palsy in 6 (CBS-PSP). Voxel-based morphometry and atlas-based parcellation were used to assess atrophy across the CBS groups and compared to 24 age-and gender-matched controls. Results: All CBS pathologic groups showed gray matter loss in premotor cortices, supplemental motor area, and insula on imaging. However, CBS-TDP and CBS-AD showed more widespread patterns of loss, with frontotemporal loss observed in CBS-TDP and temporoparietal loss observed in CBS-AD. CBS-TDP showed significantly greater loss in prefrontal cortex than the other groups, whereas CBS-AD showed significantly greater loss in parietal lobe than the other groups. The focus of loss was similar in CBS-CBD and CBS-PSP, although more severe in CBS-CBD. Conclusions: Imaging patterns of atrophy in CBS vary according to pathologic diagnosis. Widespread atrophy points toward a pathologic diagnosis of FTLD-TDP or AD, with frontotemporal loss suggesting FTLD-TDP and temporoparietal loss suggesting AD. On the contrary, more focal atrophy predominantly involving the premotor and supplemental motor area suggests CBD or PSP pathology. Neurology (R) 2010;75:1879-1887

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