Indicators of amyloid burden in a population-based study of cognitively normal elderly

Document Type

Article

Abstract

Objectives: Secondary prevention trials in subjects with preclinical Alzheimer disease may require documentation of brain amyloidosis. The identification of inexpensive and noninvasive screening variables that can identify individuals who have significant amyloid accumulation would reduce screening costs. Methods: A total of 483 cognitively normal (CN) individuals, aged 70-92 years, from the population-based Mayo Clinic Study of Aging, underwent Pittsburgh compound B (PiB)-PET imaging. Logistic regression determined whether age, sex, APOE genotype, family history, or cognitive performance was associated with odds of a PiB retention ratio <1.4 and <1.5. Area under the receiver operating characteristic curve (AUROC) evaluated the discrimination between PiBpositive and -negative subjects. For each characteristic, we determined the number needed to screen in each age group (70-79 and 80-89) to identify 100 participants with PiB <1.4 or <1.5. Results: A total of 211 (44%) individuals had PiB <1.4 and 151 (31%) <1.5. In univariate and multivariate models, discrimination was modest (AUROC ̃0.6-0.7). Multivariately, age and APOE best predicted odds of PiB <1.4 and <1.5. Subjective memory complaints were similar to cognitive test performance in predicting PiB <1.5. Indicators of PiB positivity varied with age. Screening APOE ε4 carriers alone reduced the number needed to screen to enroll 100 subjects with PIB <1.5 by 48% in persons aged 70-79 and 33% in those aged 80-89. Conclusions: Age and APOE genotype are useful predictors of the likelihood of significant amyloid accumulation, but discrimination is modest. Nonetheless, these results suggest that inexpensive and noninvasive measures could significantly reduce the number of CN individuals needed to screen to enroll a given number of amyloid-positive subjects. © 2012 by AAN Enterprises, Inc.

Publication Date

10-9-2012

Publication Title

Neurology

ISSN

00283878

Volume

79

Issue

15

First Page

1570

Last Page

1577

PubMed ID

22972644

Digital Object Identifier (DOI)

10.1212/WNL.0b013e31826e2696

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