4.5 Article

Disentangling Clinical Profiles of Apathy in Behavioral Variant Frontotemporal Dementia

Journal

JOURNAL OF ALZHEIMERS DISEASE
Volume 90, Issue 2, Pages 639-654

Publisher

IOS PRESS
DOI: 10.3233/JAD-220370

Keywords

Apathy; apathy subtypes; exploratory clustering; frontotemporal dementia; grey matter atrophy; voxel-based morphometry

Categories

Funding

  1. Program Investissements d'avenir [ANR-10-IAIHU-06]
  2. Foundation Fondation pour la recherche medicale [FRM DEQ20150331725]
  3. ENEDIS company
  4. Federation pour la Recherche sur le Cerveau
  5. FondationVaincre Alzheimer
  6. France Alzheimer Foundation
  7. Philippe Chatrier Foundation
  8. Rosita Gomez association

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This study found distinct clinical subtypes of apathy in bvFTD patients, corresponding to different anatomical subtypes. These findings have important implications for clinicians in personalizing the treatment of apathy.
Background: Apathy is highly frequent in behavioral variant frontotemporal dementia (bvFTD). It is presumed to involve different pathophysiological mechanisms and neuroanatomical regions. Objective: We explored the hypothesis that subgroups showing distinct profiles of apathy and distinct patterns of atrophy within frontal lobes could be disentangled in bvFTD. Methods: Using data-driven clustering applied to 20 bvFTD patients, we isolated subgroups according to their profiles on the three subscales of the Dimensional Apathy Scale (DAS). We explored their apathy profiles and atrophy patterns. Apathy profiles were characterized through both subjective measures of apathy by questionnaires and measures including objective behavioral metrics. Atrophy patterns were obtained by voxel-based morphometry, contrasting each bvFTD subgroup with healthy controls (N = 16). Results: By clustering based on DAS dimensions, we disentangled three subgroups of bvFTD patients, with distinct apathy profiles and atrophy patterns. One subgroup, which presented the smallest pattern of atrophy (including orbitofrontal cortex) with a right asymmetry, was characterized by high self-reported emotional and initiation apathy and by a self-initiation deficit reversible by external guidance. In other subgroups showing more diffuse bilateral atrophies extending to lateral prefrontal cortex, apathy was not reversible by external guidance and more difficulty to focus on goal-management was observed, especially in the subgroup with the largest atrophy and highest levels of executive apathy. Conclusion: Distinct clinical profiles of apathy, corresponding to distinct anatomical subtypes of bvFTD, were identified. These findings have implications for clinicians in a perspective of precision medicine as they could contribute to personalize treatments of apathy.

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