Use of preclinical Alzheimer's disease trajectories for clinical trial design
Langhough, R. E.; Norton, D. L.; Cody, K. A.; Du, L.; Jonaitis, E. M.; Wilson, R.; Rea Reyes, R. E.; Hermann, B. P.; Zetterberg, H.; Johnson, S. C.
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INTRODUCTIONThis study uses longitudinal amyloid biomarker and cognitive data to generate sample size estimates for two-armed, pre-clinical amyloid clearance clinical trials. METHODSPET PiB DVR ranges defined three amyloid groups (positive, "A+"; sub threshold/low positive, "subA+"; and negative, "A-") in cognitively unimpaired Wisconsin Registry for Alzheimers Prevention participants. Amyloid group trajectories estimated from mixed effects models informed per-treatment-arm sample size estimates to detect plausible treatment effects over 3-year (biomarker) or 6-year (cognition) study windows (80% power). RESULTSTo detect [≥]60% slowing in PiB accumulation, [≤]40 may be needed per arm for both SubA+ and A+; to detect the same effect sizes in plasma p-tau217 trajectories, [~]50-1700 are needed, depending on assay and amyloid subgroup. Among cognitive outcomes, Digit Symbol Substitution and a 5-test Preclinical Alzheimers Cognitive Composite consistently required fewest (<2000) per arm. DISCUSSIONEarly intervention study planning will benefit from selection of outcomes that are most sensitive to AD biomarker-related preclinical change.
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