4.3 Article

Validation of the neuropathologic criteria of the Third Consortium for Dementia with Lewy bodies for prospectively diagnosed cases

Journal

Publisher

OXFORD UNIV PRESS INC
DOI: 10.1097/NEN.0b013e31817d7a1d

Keywords

Alzheimer disease; alpha-synuclein; clinicopathologic correlation; diagnostic criteria; dementia with Lewy bodies; prospective study; REM behavior disorder

Funding

  1. NIA NIH HHS [R01 AG015866-10, P50 AG 16574, P50 AG016574-109002, R01 AG 15866, R01 AG015866, P50 AG016574] Funding Source: Medline
  2. NINDS NIH HHS [P50 NS040256, P50 NS040256-06, P50 NS040256-109004, P50 NS 40256] Funding Source: Medline

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There is limited information on the validity of the pathologic criteria of the Third Consortium on Dementia with Lewy bodies (CDLB), and none are based on prospectively diagnosed cases. In this study, the core clinical features of dementia with Lewy bodies (DLB) and the suggestive clinical feature of rapid eye movement sleep behavior disorder were assessed using a battery of standardized clinical instruments in 76 patients with the clinical diagnosis of either DLB or Alzheimer disease. At autopsy, 29 patients had high-likelihood, 17 had intermediate-likelihood, and 6 had low-likelihood DLB pathology. The frequency of core clinical features and the accuracy of the clinical diagnosis of probable DLB were significantly greater in high-likelihood than in low-likelihood cases. This is consistent with the concept that the DLB clinical syndrome is directly related to Lewy body pathology and inversely related to Alzheimer pathology. Thus, the Third Consortium on DLB neuropathologic criteria scheme performed reasonably well and are useful for estimating the likelihood of the premortern DLB syndrome based on postmortem findings. In view of differences in the frequency of clinically probable DLB in cases with Braak neurofibrillary tangle stages V (90%) and VI (20%) and diffuse cortical Lewy bodies, a possible modification of the scheme is to consider cases with neurofibrillary tangle stage VI to be low-likelihood DLB.

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