Clinical and Biomarker Changes in Dominantly Inherited Alzheimer's Disease

Randall J. Bateman(Washington University in St. Louis), Chengjie Xiong(Washington University in St. Louis), Tammie L.S. Benzinger(Washington University in St. Louis), Anne M. Fagan(Washington University in St. Louis), Alison Goate(Washington University in St. Louis), Nick C. Fox(University of Pittsburgh), Daniel S. Marcus(Washington University in St. Louis), Nigel J. Cairns(Washington University in St. Louis), Xianyun Xie(Washington University in St. Louis), Tyler Blazey(Washington University in St. Louis), David M. Holtzman(Washington University in St. Louis), Anna Santacruz(Washington University in St. Louis), Virginia Buckles(Washington University in St. Louis), Angela Oliver(Washington University in St. Louis), Krista L. Moulder(Washington University in St. Louis), Paul Aisen(University of Pittsburgh), Bernardino Ghetti(Indiana University – Purdue University Indianapolis), William E. Klunk(University of Pittsburgh), Eric McDade(University of Pittsburgh), Ralph N. Martins(Edith Cowan University), Colin L. Masters(Mental Health Research Institute), Richard Mayeux(Columbia University), John M. Ringman(University of California, Los Angeles), Martin N. Rossor(University College London), Peter R. Schofield(UNSW Sydney), Reisa A. Sperling(Massachusetts General Hospital), Stephen Salloway(Butler Hospital), John C. Morris(Washington University in St. Louis)
New England Journal of Medicine
July 11, 2012
10.1056/nejmoa1202753
Cited by 3,797Open Access
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Abstract

BACKGROUND: The order and magnitude of pathologic processes in Alzheimer's disease are not well understood, partly because the disease develops over many years. Autosomal dominant Alzheimer's disease has a predictable age at onset and provides an opportunity to determine the sequence and magnitude of pathologic changes that culminate in symptomatic disease. METHODS: In this prospective, longitudinal study, we analyzed data from 128 participants who underwent baseline clinical and cognitive assessments, brain imaging, and cerebrospinal fluid (CSF) and blood tests. We used the participant's age at baseline assessment and the parent's age at the onset of symptoms of Alzheimer's disease to calculate the estimated years from expected symptom onset (age of the participant minus parent's age at symptom onset). We conducted cross-sectional analyses of baseline data in relation to estimated years from expected symptom onset in order to determine the relative order and magnitude of pathophysiological changes. RESULTS: Concentrations of amyloid-beta (Aβ)(42) in the CSF appeared to decline 25 years before expected symptom onset. Aβ deposition, as measured by positron-emission tomography with the use of Pittsburgh compound B, was detected 15 years before expected symptom onset. Increased concentrations of tau protein in the CSF and an increase in brain atrophy were detected 15 years before expected symptom onset. Cerebral hypometabolism and impaired episodic memory were observed 10 years before expected symptom onset. Global cognitive impairment, as measured by the Mini-Mental State Examination and the Clinical Dementia Rating scale, was detected 5 years before expected symptom onset, and patients met diagnostic criteria for dementia at an average of 3 years after expected symptom onset. CONCLUSIONS: We found that autosomal dominant Alzheimer's disease was associated with a series of pathophysiological changes over decades in CSF biochemical markers of Alzheimer's disease, brain amyloid deposition, and brain metabolism as well as progressive cognitive impairment. Our results require confirmation with the use of longitudinal data and may not apply to patients with sporadic Alzheimer's disease. (Funded by the National Institute on Aging and others; DIAN ClinicalTrials.gov number, NCT00869817.).

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