Abstract
Background: Adults with Down syndrome (DS) have an elevated risk and early age of onset for Alzheimer's disease (AD). To support upcoming clinical AD trials, there is a critical need to establish cognitive outcome measures that can be used to capture intervention effects. One measure that has successfully been used to detect AD-related cognitive decline in the DS population is a measure of episodic memory, the modified Cued Recall Test (mCRT). Demonstrated utility of the mCRT warrants further investigation into comparisons between the A and B versions, free versus cued recall and changes in performance over time to better understand sensitivity for tracking memory decline over time based on age and AD clinical status. Method: Participants were 272 adults with DS aged 25–81 (mean age = 43.12 years, SD = 9.79). Study procedures were completed at three cycles of data collection: baseline, 16-month follow-up and 32-month follow-up. Participants were enrolled in the Alzheimer Biomarker Consortium–Down Syndrome longitudinal study and completed the mCRT as part of a multiday evaluation. Comparisons were made between the A and B versions of the mCRT in recall and intrusion scores. Participants' ratio of free relative to cued recall was also examined at baseline and longitudinally. Participant performance was compared by age group, clinical AD status (cognitively stable [CS], mild cognitive impairment [MCI] or AD dementia) and premorbid level of intellectual disability (ID). Results: Version differences were identified, with the most salient differences in the moderate and severe/profound ID groups. The mCRT free recall declined with age in CS participants. Free and cued recall scores were lower in those with MCI and AD dementia, with the exception of the mild ID MCI group, whose cued recall scores were not significantly different from the CS group. Decline across 32 months (mCRT total score decline of 1.29 points/year) was observed for CS participants beginning at ≥ 50 years old, with more pronounced declines in adults with DS with an MCI or AD dementia diagnosis (3.36 and 4.20 points/year, respectively). Conclusion: Characterising test version differences and participant free versus cued recall performance on the mCRT is important for understanding performance under testing conditions and to maximise the sensitivity of clinical interventions to capture meaningful effects. Our findings suggest that clinical AD trials for DS should be cautious about using both versions of the mCRT. Examining the profile of free relative to cued recall may enhance sensitivity for detecting treatment benefits for adults with DS across the range of premorbid ID levels.
| Original language | English |
|---|---|
| Journal | Journal of Intellectual Disability Research |
| DOIs | |
| State | Accepted/In press - 2025 |
Bibliographical note
Publisher Copyright:© 2025 MENCAP and John Wiley & Sons Ltd.
Funding
The Alzheimer Biomarkers Consortium–Down Syndrome (ABC‐DS) is funded by the National Institute on Aging (K99AG084738) and the National Institute for Child Health and Human Development (U01 AG051406, U01 AG051412 and U19 AG068054). The work contained in this publication was also supported through the following National Institutes of Health Programs: The Alzheimer's Disease Research Centers Program (P50 AG008702, P30 AG062421, P50 AG16537, P50 AG005133, P50 AG005681, P30 AG062715 and P30 AG066519), the Eunice Kennedy Shriver Intellectual and Developmental Disabilities Research Centers Program (U54 HD090256, U54 HD087011 and P50 HD105353), the National Center for Advancing Translational Sciences (UL1 TR001873, UL1 TR002373, UL1 TR001414, UL1 TR001857 and UL1 TR002345), the National Centralized Repository for Alzheimer Disease and Related Dementias (U24 AG21886) and DS‐Connect (The Down Syndrome Registry) supported by the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) (T32HD007489). All research at the Department of Psychiatry in the University of Cambridge was supported by the NIHR Cambridge Biomedical Research Centre (NIHR203312) and the NIHR Applied Research Collaboration East of England. Funding:
| Funders | Funder number |
|---|---|
| National Institute on Handicapped Research | |
| Down Syndrome Registry | |
| Eunice Kennedy Shriver National Institute of Child Health and Human Development | T32HD007489 |
| Eunice Kennedy Shriver National Institute of Child Health and Human Development | |
| NIHR Cambridge Biomedical Research Centre | NIHR203312 |
| NIHR Cambridge Biomedical Research Centre | |
| National Center for Advancing Translational Sciences (NCATS) | UL1 TR002373, UL1 TR001873, UL1 TR002345, UL1 TR001414, UL1 TR001857 |
| National Center for Advancing Translational Sciences (NCATS) | |
| NIH National Institute of Child Health and Human Development National Center for Medical Rehabilitation Research | U01 AG051412, U01 AG051406, U19 AG068054 |
| NIH National Institute of Child Health and Human Development National Center for Medical Rehabilitation Research | |
| National Institutes of Health (NIH) | P50 AG008702, P30 AG062421, P50 AG16537, P50 AG005681, P50 AG005133, P30 AG062715, P30 AG066519 |
| National Institutes of Health (NIH) | |
| Eunice Kennedy Shriver Intellectual and Developmental Disabilities Research Centers Program | U54 HD090256, U54 HD087011, P50 HD105353 |
| National Centralized Repository for Alzheimer Disease and Related Dementias | U24 AG21886 |
| National Institute on Aging | K99AG084738 |
| National Institute on Aging |
Keywords
- Alzheimer's disease
- ageing
- cognitive decline
- list learning
- memory
- outcome measures
ASJC Scopus subject areas
- Rehabilitation
- Arts and Humanities (miscellaneous)
- Neurology
- Clinical Neurology
- Psychiatry and Mental health
