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May 31, 2022; 98 (22) Research Article

Characterizing Amyloid-Positive Individuals With Normal Tau PET Levels After 5 Years

An ADNI Study

Keith A. Josephs, Stephen D. Weigand, Jennifer L. Whitwell
First published March 21, 2022, DOI: https://doi.org/10.1212/WNL.0000000000200287
Keith A. Josephs
From the Departments of Neurology (K.A.J.), Health Sciences Research (Division of Biomedical Informatics and Statistics) (S.D.W.), and Radiology (J.W.), Mayo Clinic, Rochester, MN.
MD, MST, MSc
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Stephen D. Weigand
From the Departments of Neurology (K.A.J.), Health Sciences Research (Division of Biomedical Informatics and Statistics) (S.D.W.), and Radiology (J.W.), Mayo Clinic, Rochester, MN.
MS
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Jennifer L. Whitwell
From the Departments of Neurology (K.A.J.), Health Sciences Research (Division of Biomedical Informatics and Statistics) (S.D.W.), and Radiology (J.W.), Mayo Clinic, Rochester, MN.
PhD
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Characterizing Amyloid-Positive Individuals With Normal Tau PET Levels After 5 Years
An ADNI Study
Keith A. Josephs, Stephen D. Weigand, Jennifer L. Whitwell
Neurology May 2022, 98 (22) e2282-e2292; DOI: 10.1212/WNL.0000000000200287

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Abstract

Background and Objective Individuals with biomarker evidence of β-amyloid (Aβ) deposition are increasingly being enrolled in clinical treatment trials but there is a need to identify markers to predict which of these individuals will also develop tau deposition. We aimed to determine whether Aβ-positive individuals can remain tau-negative for at least 5 years and identify characteristics that could distinguish between these individuals and those who develop high tau within this period.

Methods Tau PET positivity was defined using a Gaussian mixture model with log-transformed standard uptake value ratio values from 7 temporal and medial parietal regions using all participants in the Alzheimer's Disease Neuroimaging Initiative (ADNI) with flortaucipir PET. Tau PET scans were classified as normal if the posterior probability of elevated tau was less than 1%. Aβ PET positivity was defined based on ADNI cutpoints. We identified all Aβ-positive individuals from ADNI who had normal tau PET more than 5 years after their first abnormal Aβ PET (amyloid with low tau [ALT] group) and all Aβ-positive individuals with abnormal tau PET within 5 years (biomarker AD). In a case–control design, logistic regression was used to model the odds of biomarker AD vs ALT accounting for sex, age, APOE ε4 carriership, Aβ Centiloid, and hippocampal volume.

Results We identified 45 individuals meeting criteria for ALT and 157 meeting criteria for biomarker AD. The ALT group had a lower proportion of APOE ε4 carriers, lower Aβ Centiloid, larger hippocampal volumes, and more preserved cognition, and were less likely to develop dementia, than the biomarker AD group. APOE ε4, higher Aβ Centiloid, and hippocampal atrophy were independently associated with increased odds of abnormal tau within 5 years. A Centiloid value of 50 effectively discriminated biomarker AD and ALT with 80% sensitivity and specificity. The majority of the ALT participants did not develop dementia throughout the 5-year interval.

Discussion Aβ-positive individuals can remain tau-negative for at least 5 years. Baseline characteristics can help identify these ALT individuals who are less likely to develop dementia. Conservative Aβ cutpoints should be utilized for clinical trials to better capture individuals with high risk of developing biomarker AD.

Glossary

Aβ=
β-amyloid;
AD=
Alzheimer disease;
ADAS-Cog=
Alzheimer's Disease Assessment Scale–cognitive subscale;
ADNI=
Alzheimer's Disease Neuroimaging Initiative;
ALT=
amyloid+ with low tau;
AUC=
area under the receiver operating characteristic curve;
BIC=
Bayesian information criterion;
IQR=
interquartile range;
MCI=
mild cognitive impairment;
MMSE=
Mini-Mental State Examination;
OR=
odds ratio;
ROI=
region of interest;
SUVR=
standardized uptake value ratio

Footnotes

  • Go to Neurology.org/N for full disclosures. Funding information and disclosures deemed relevant by the authors, if any, are provided at the end of the article.

  • Received May 5, 2021.
  • Accepted in final form February 10, 2022.
  • © 2022 American Academy of Neurology
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