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Observational Study
. 2024 Dec;23(12):1214-1224.
doi: 10.1016/S1474-4422(24)00426-5.

Timeline to symptomatic Alzheimer's disease in people with Down syndrome as assessed by amyloid-PET and tau-PET: a longitudinal cohort study

Emily K Schworer  1 Matthew D Zammit  1 Jiebiao Wang  2 Benjamin L Handen  3 Tobey Betthauser  4 Charles M Laymon  5 Dana L Tudorascu  6 Annie D Cohen  3 Shahid H Zaman  7 Beau M Ances  8 Mark Mapstone  9 Elizabeth Head  10 Bradley T Christian  11 Sigan L Hartley  12 Alzheimer's Biomarker Consortium–Down Syndrome (ABC–DS)
Collaborators, Affiliations
Observational Study

Timeline to symptomatic Alzheimer's disease in people with Down syndrome as assessed by amyloid-PET and tau-PET: a longitudinal cohort study

Emily K Schworer et al. Lancet Neurol. 2024 Dec.

Abstract

Background: Adults with Down syndrome are at risk for Alzheimer's disease. Natural history cohort studies have characterised the progression of Alzheimer's disease biomarkers in people with Down syndrome, with a focus on amyloid β-PET and tau-PET. In this study, we aimed to leverage these well characterised imaging biomarkers in a large cohort of individuals with Down syndrome, to examine the timeline to symptomatic Alzheimer's disease based on estimated years since the detection on PET of amyloid β-positivity, referred to here as amyloid age, and in relation to tau burden as assessed by PET.

Methods: In this prospective, longitudinal, observational cohort study, data were collected at four university research sites in the UK and USA as part of the Alzheimer's Biomarker Consortium-Down Syndrome (ABC-DS) study. Eligible participants were aged 25 years or older with Down syndrome, had a mental age of at least 3 years (based on a standardised intelligence quotient test), and had trisomy 21 (full, mosaic, or translocation) confirmed through karyotyping. Participants were assessed twice between 2017 and 2022, with approximately 32 months between visits. Participants had amyloid-PET and tau-PET scans, and underwent cognitive assessment with the modified Cued Recall Test (mCRT) and the Down Syndrome Mental Status Examination (DSMSE) to assess cognitive functioning. Study partners completed the National Task Group-Early Detection Screen for Dementia (NTG-EDSD). Generalised linear models were used to assess the association between amyloid age (whereby 0 years equated to 18 centiloids) and mCRT, DSMSE, NTG-EDSD, and tau PET at baseline and the 32-month follow-up. Broken stick regression was used to identify the amyloid age that corresponded to decreases in cognitive performance and increases in tau PET after the onset of amyloid β positivity.

Findings: 167 adults with Down syndrome, of whom 92 had longitudinal data, were included in our analyses. Generalised linear regressions showed significant quadratic associations between amyloid age and cognitive performance and cubic associations between amyloid age and tau, both at baseline and at the 32-month follow-up. Using broken stick regression models, differences in mCRT total scores were detected beginning 2·7 years (95% credible interval [CrI] 0·2 to 5·4; equating to 29·8 centiloids) after the onset of amyloid β positivity in cross-sectional models. Based on cross-sectional data, increases in tau deposition started a mean of 2·7-6·1 years (equating to 29·8-47·9 centiloids) after the onset of amyloid β positivity. Mild cognitive impairment was observed at a mean amyloid age of 7·4 years (SD 6·6; equating to 56·8 centiloids) and dementia was observed at a mean amyloid age of 12·7 years (5·6; equating to 97·4 centiloids).

Interpretation: There is a short timeline to initial cognitive decline and dementia from onset of amyloid β positivity and tau deposition in people with Down syndrome. This newly established timeline based on amyloid age (or equivalent centiloid values) is important for clinical practice and informing the design of Alzheimer's disease clinical trials, and it avoids the limitations of timelines based on chronological age.

Funding: National Institute on Aging and the National Institute for Child Health and Human Development.

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Conflict of interest statement

Declaration of interests MZ received honoraria from LuMind International Down Syndrome Community and a travel award from the Trisomy21 Research Society. BH receives royalties from two co-authored books; is paid consulting fees from Patient-Centered Outcomes Research Institute grant; received honoraria from the University of North Carolina; and served on a data monitoring board for a Department of Defense funded grant. TB has received honoraria from National Institutes of Health and Intermountain Healthcare; and travel support from University College London, the Alzheimer's Association, and National Institutes of Health. DLT participated in the REMBRAND study advisory board. SZ reports grants from Cambridgeshire and Peterborough Foundation National Health Service Trust and serves on committees for the Trisomy21 Research Society. MM receives royalties from University of Rochester; and consulting fees from NovoGlia and Ireneo Health; has US patents (numbers 7 645 140, 10 578 629, #10 718 021, 10 890 589, 10 900 977, and 10 900 980); serves on the scientific advisory board for Brain Neurotherapy Bio, Davis Phinney Foundation for Parkinson's, and Alzheon; is the chair of data and safety monitoring board for the Aerobic Exercise and Cognitive Training Trial; and owns stock in Ireneo Health. EH reports grants from Brightfocus and the Alzheimer's Association. ES, JW AC, BA, CL, BC, and SH declare no competing interests.

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