4.5 Article

The Behavioral and Psychological Symptoms of Dementia in Down Syndrome Scale (BPSD-DS II): Optimization and Further Validation

Journal

JOURNAL OF ALZHEIMERS DISEASE
Volume 81, Issue 4, Pages 1505-1527

Publisher

IOS PRESS
DOI: 10.3233/JAD-201427

Keywords

Alzheimer's disease; behavior; behavioral and psychological symptoms of dementia; dementia; Down syndrome; intellectual disabilities; neuropsychiatric symptoms; trisomy 21

Categories

Funding

  1. J. Th. Guepin Stichting Onderzoek Down Syndroom
  2. Research School Behavioral and Cognitive Neurosciences (RUG/UMCG)
  3. Gratama Stichting/Stichting Groninger Universiteitsfonds [2015-04]
  4. Research Foundation Flanders [G053218N]
  5. Fondo de Investigaciones Sanitario, Instituto de SaludCarlos III [PI14/01126, PI17/01019]
  6. CIBERNED program - Europeo de Desarrollo Regional, Union Europea, Una manera de hacer Europa
  7. National Institutes of Health (NIA) [1R01AG056850-01A1, R21AG056974, R01AG061566]
  8. Fundacio La Marato de TV3 [20141210]
  9. Fundacio Catalana Sindrome de Down
  10. Fundacio Victor Grifols i Lucas
  11. Generalitat de Catalunya [SLT006/17/00119]

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The study aimed to optimize and further study the discriminative ability and reliability of the BPSD assessment scale BPSD-DS II for individuals with Down syndrome (DS). Results showed significant changes in frequency and severity of anxious, sleep-related, irritable, apathetic, depressive, and eating/drinking behaviors among DS, DS+Q, and DS+AD groups. These changes may serve as early signals of Alzheimer's disease dementia in DS.
Background: People with Down syndrome (DS) are at high risk to develop Alzheimer's disease dementia (AD). Behavioral and psychological symptoms of dementia (BPSD) are common and may also serve as early signals for dementia. However, comprehensive evaluation scales for BPSD, adapted to DS, are lacking. Therefore, we previously developed the BPSD-DS scale to identify behavioral changes between the last six months and pre-existing life-long characteristic behavior. Objective: To optimize and further study the scale (discriminative ability and reliability) in a large representative DS study population. Methods: Optimization was based on item irrelevance and clinical experiences obtained in the initial study. Using the shortened and refined BPSD-DS II, informant interviews were conducted to evaluate 524 individuals with DS grouped according to dementia status: no dementia (DS, N=292), questionable dementia (DS + Q, N=119), and clinically diagnosed dementia (DS + AD, N=113). Results: Comparing item change scores between groups revealed prominent changes in frequency and severity for anxious, sleep-related, irritable, restless/stereotypic, apathetic, depressive, and eating/drinking behavior. For most items, the proportion of individuals displaying an increased frequency was highest in DS + AD, intermediate in DS + Q, and lowest in DS. For various items within sections about anxious, sleep-related, irritable, apathetic, and depressive behaviors, the proportion of individuals showing an increased frequency was already substantial in DS + Q, suggesting that these changes may serve as early signals of AD in DS. Reliability data were promising. Conclusion: The optimized scale yields largely similar results as obtained with the initial version. Systematically evaluating BPSD in DS may increase understanding of changes among caregivers and (timely) adaptation of care/treatment.

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