Tau PET positivity in individuals with and without cognitive impairment varies with age, amyloid-ß status, APOE genotype and sex

Rik Ossenkoppele; Emma M. Coomans; Liana G. Apostolova; Suzanne L. Baker; Henryk Barthel; Thomas G. Beach; Tammy L. S. Benzinger; Tobey Betthauser; Gerard N. Bischof; Michel Bottlaender; Pierick Bourgeat; Anouk den Braber; Matthias Brendel; Adam M. Brickman; David M. Cash; Maria C. Carrillo; William Coath; Bradley T. Christian; Brad C. Dickerson; Vincent Dore; Alexander Drzezga; Azadeh Feizpour; Wiesje M. van der Flier; Nicolai Franzmeier; Giovanni B. Frisoni; Valentina Garibotto; Elsmarieke van de Giessen; Juan Domingo-Gispert; Johannes Gnoerich; Yuna Gu; Yihui Guan; Bernard J. Hanseeuw; Theresa M. Harrison; Clifford R. Jack; Elena Jaeger; William J. Jagust; Willemijn J. Jansen; Renaud La Joie; Keith A. Johnson; Sterling C. Johnson; Ian A. Kennedy; Jun Pyo Kim; Koen van Laere; Julien Lagarde; Patrick Lao; Jose A. Luchsinger; Silke Kern; William C. Kreisl; Vincent Malotaux; Maura Malpetti; Mayo Clinic Study Aging; PREVENT-AD research group

doi:10.1038/s41593-025-02000-6

Tau PET positivity in individuals with and without cognitive impairment varies with age, amyloid-ß status, APOE genotype and sex

Rik Ossenkoppele^*, Emma M. Coomans, Liana G. Apostolova, Suzanne L. Baker, Henryk Barthel, Thomas G. Beach, Tammy L. S. Benzinger, Tobey Betthauser, Gerard N. Bischof, Michel Bottlaender, Pierick Bourgeat, Anouk den Braber, Matthias Brendel, Adam M. Brickman, David M. Cash, Maria C. Carrillo, William Coath, Bradley T. Christian, Brad C. Dickerson, Vincent DoreAlexander Drzezga, Azadeh Feizpour, Wiesje M. van der Flier, Nicolai Franzmeier, Giovanni B. Frisoni, Valentina Garibotto, Elsmarieke van de Giessen, Juan Domingo-Gispert, Johannes Gnoerich, Yuna Gu, Yihui Guan, Bernard J. Hanseeuw, Theresa M. Harrison, Clifford R. Jack, Elena Jaeger, William J. Jagust, Willemijn J. Jansen, Renaud La Joie, Keith A. Johnson, Sterling C. Johnson, Ian A. Kennedy, Jun Pyo Kim, Koen van Laere, Julien Lagarde, Patrick Lao, Jose A. Luchsinger, Silke Kern, William C. Kreisl, Vincent Malotaux, Maura Malpetti, Mayo Clinic Study Aging, PREVENT-AD research group

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Tau positron emission tomography (PET) imaging allows in vivo detection of tau proteinopathy in Alzheimer's disease, which is associated with neurodegeneration and cognitive decline. Understanding how demographic, clinical and genetic factors relate to tau PET positivity will facilitate its use for clinical practice and research. Here we conducted an analysis of 42 cohorts worldwide (N = 12,048), including 7,394 cognitively unimpaired (CU) participants, 2,177 participants with mild cognitive impairment (MCI) and 2,477 participants with dementia. We found that from age 60 years to 80 years, tau PET positivity in a temporal composite region increased from 1.1% to 4.4% among CU amyloid-β (Aβ)-negative participants and from 17.4% to 22.2% among CU Aβ-positive participants. Across the same age span, tau PET positivity decreased from 68.0% to 52.9% in participants with MCI and from 91.5% to 74.6% in participants with dementia. Age, Aβ status, APOE ε4 carriership and female sex were all associated with a higher prevalence of tau PET positivity across groups. APOE ε4 carriership in CU individuals lowered the age at onset of both Aβ positivity and tau positivity by decades. Finally, we replicated these associations in an independent autopsy dataset (N = 5,072 from 3 cohorts).

Original language	English
Pages (from-to)	1610-1621
Number of pages	12
Journal	Nature Neuroscience
Volume	28
Issue number	8
Early online date	1 Jul 2025
DOIs	https://doi.org/10.1038/s41593-025-02000-6
Publication status	Published - 1 Aug 2025

Keywords

ALZHEIMERS ASSOCIATION WORKGROUPS
POSITRON-EMISSION-TOMOGRAPHY
NATIONAL INSTITUTE
DIAGNOSTIC GUIDELINES
NEUROPATHOLOGIC ASSESSMENT
DISEASE
BRAIN
RECOMMENDATIONS
DEMENTIA
PREVALENCE

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Ossenkoppele, R., Coomans, E. M., Apostolova, L. G., Baker, S. L., Barthel, H., Beach, T. G., Benzinger, T. L. S., Betthauser, T., Bischof, G. N., Bottlaender, M., Bourgeat, P., den Braber, A., Brendel, M., Brickman, A. M., Cash, D. M., Carrillo, M. C., Coath, W., Christian, B. T., Dickerson, B. C., ... PREVENT-AD research group (2025). Tau PET positivity in individuals with and without cognitive impairment varies with age, amyloid-ß status, APOE genotype and sex. Nature Neuroscience, 28(8), 1610-1621. https://doi.org/10.1038/s41593-025-02000-6

@article{63f6fcaf5aa945e984f1471e815d74a1,

title = "Tau PET positivity in individuals with and without cognitive impairment varies with age, amyloid-{\ss} status, APOE genotype and sex",

abstract = "Tau positron emission tomography (PET) imaging allows in vivo detection of tau proteinopathy in Alzheimer's disease, which is associated with neurodegeneration and cognitive decline. Understanding how demographic, clinical and genetic factors relate to tau PET positivity will facilitate its use for clinical practice and research. Here we conducted an analysis of 42 cohorts worldwide (N = 12,048), including 7,394 cognitively unimpaired (CU) participants, 2,177 participants with mild cognitive impairment (MCI) and 2,477 participants with dementia. We found that from age 60 years to 80 years, tau PET positivity in a temporal composite region increased from 1.1\% to 4.4\% among CU amyloid-β (Aβ)-negative participants and from 17.4\% to 22.2\% among CU Aβ-positive participants. Across the same age span, tau PET positivity decreased from 68.0\% to 52.9\% in participants with MCI and from 91.5\% to 74.6\% in participants with dementia. Age, Aβ status, APOE ε4 carriership and female sex were all associated with a higher prevalence of tau PET positivity across groups. APOE ε4 carriership in CU individuals lowered the age at onset of both Aβ positivity and tau positivity by decades. Finally, we replicated these associations in an independent autopsy dataset (N = 5,072 from 3 cohorts).",

keywords = "ALZHEIMERS ASSOCIATION WORKGROUPS, POSITRON-EMISSION-TOMOGRAPHY, NATIONAL INSTITUTE, DIAGNOSTIC GUIDELINES, NEUROPATHOLOGIC ASSESSMENT, DISEASE, BRAIN, RECOMMENDATIONS, DEMENTIA, PREVALENCE",

author = "Rik Ossenkoppele and Coomans, \{Emma M.\} and Apostolova, \{Liana G.\} and Baker, \{Suzanne L.\} and Henryk Barthel and Beach, \{Thomas G.\} and Benzinger, \{Tammy L. S.\} and Tobey Betthauser and Bischof, \{Gerard N.\} and Michel Bottlaender and Pierick Bourgeat and \{den Braber\}, Anouk and Matthias Brendel and Brickman, \{Adam M.\} and Cash, \{David M.\} and Carrillo, \{Maria C.\} and William Coath and Christian, \{Bradley T.\} and Dickerson, \{Brad C.\} and Vincent Dore and Alexander Drzezga and Azadeh Feizpour and \{van der Flier\}, \{Wiesje M.\} and Nicolai Franzmeier and Frisoni, \{Giovanni B.\} and Valentina Garibotto and \{van de Giessen\}, Elsmarieke and Juan Domingo-Gispert and Johannes Gnoerich and Yuna Gu and Yihui Guan and Hanseeuw, \{Bernard J.\} and Harrison, \{Theresa M.\} and Jack, \{Clifford R.\} and Elena Jaeger and Jagust, \{William J.\} and Jansen, \{Willemijn J.\} and \{La Joie\}, Renaud and Johnson, \{Keith A.\} and Johnson, \{Sterling C.\} and Kennedy, \{Ian A.\} and Kim, \{Jun Pyo\} and \{van Laere\}, Koen and Julien Lagarde and Patrick Lao and Luchsinger, \{Jose A.\} and Silke Kern and Kreisl, \{William C.\} and Vincent Malotaux and Maura Malpetti and \{Mayo Clinic Study Aging\} and \{PREVENT-AD research group\}",

year = "2025",

month = aug,

day = "1",

doi = "10.1038/s41593-025-02000-6",

language = "English",

volume = "28",

pages = "1610--1621",

journal = "Nature Neuroscience",

issn = "1097-6256",

publisher = "Nature Research",

number = "8",

}

Ossenkoppele, R, Coomans, EM, Apostolova, LG, Baker, SL, Barthel, H, Beach, TG, Benzinger, TLS, Betthauser, T, Bischof, GN, Bottlaender, M, Bourgeat, P, den Braber, A, Brendel, M, Brickman, AM, Cash, DM, Carrillo, MC, Coath, W, Christian, BT, Dickerson, BC, Dore, V, Drzezga, A, Feizpour, A, van der Flier, WM, Franzmeier, N, Frisoni, GB, Garibotto, V, van de Giessen, E, Domingo-Gispert, J, Gnoerich, J, Gu, Y, Guan, Y, Hanseeuw, BJ, Harrison, TM, Jack, CR, Jaeger, E, Jagust, WJ, Jansen, WJ, La Joie, R, Johnson, KA, Johnson, SC, Kennedy, IA, Kim, JP, van Laere, K, Lagarde, J, Lao, P, Luchsinger, JA, Kern, S, Kreisl, WC, Malotaux, V, Malpetti, M, Mayo Clinic Study Aging & PREVENT-AD research group 2025, 'Tau PET positivity in individuals with and without cognitive impairment varies with age, amyloid-ß status, APOE genotype and sex', Nature Neuroscience, vol. 28, no. 8, pp. 1610-1621. https://doi.org/10.1038/s41593-025-02000-6

TY - JOUR

T1 - Tau PET positivity in individuals with and without cognitive impairment varies with age, amyloid-ß status, APOE genotype and sex

AU - Ossenkoppele, Rik

AU - Coomans, Emma M.

AU - Apostolova, Liana G.

AU - Baker, Suzanne L.

AU - Barthel, Henryk

AU - Beach, Thomas G.

AU - Benzinger, Tammy L. S.

AU - Betthauser, Tobey

AU - Bischof, Gerard N.

AU - Bottlaender, Michel

AU - Bourgeat, Pierick

AU - den Braber, Anouk

AU - Brendel, Matthias

AU - Brickman, Adam M.

AU - Cash, David M.

AU - Carrillo, Maria C.

AU - Coath, William

AU - Christian, Bradley T.

AU - Dickerson, Brad C.

AU - Dore, Vincent

AU - Drzezga, Alexander

AU - Feizpour, Azadeh

AU - van der Flier, Wiesje M.

AU - Franzmeier, Nicolai

AU - Frisoni, Giovanni B.

AU - Garibotto, Valentina

AU - van de Giessen, Elsmarieke

AU - Domingo-Gispert, Juan

AU - Gnoerich, Johannes

AU - Gu, Yuna

AU - Guan, Yihui

AU - Hanseeuw, Bernard J.

AU - Harrison, Theresa M.

AU - Jack, Clifford R.

AU - Jaeger, Elena

AU - Jagust, William J.

AU - Jansen, Willemijn J.

AU - La Joie, Renaud

AU - Johnson, Keith A.

AU - Johnson, Sterling C.

AU - Kennedy, Ian A.

AU - Kim, Jun Pyo

AU - van Laere, Koen

AU - Lagarde, Julien

AU - Lao, Patrick

AU - Luchsinger, Jose A.

AU - Kern, Silke

AU - Kreisl, William C.

AU - Malotaux, Vincent

AU - Malpetti, Maura

AU - Mayo Clinic Study Aging

AU - PREVENT-AD research group

PY - 2025/8/1

Y1 - 2025/8/1

N2 - Tau positron emission tomography (PET) imaging allows in vivo detection of tau proteinopathy in Alzheimer's disease, which is associated with neurodegeneration and cognitive decline. Understanding how demographic, clinical and genetic factors relate to tau PET positivity will facilitate its use for clinical practice and research. Here we conducted an analysis of 42 cohorts worldwide (N = 12,048), including 7,394 cognitively unimpaired (CU) participants, 2,177 participants with mild cognitive impairment (MCI) and 2,477 participants with dementia. We found that from age 60 years to 80 years, tau PET positivity in a temporal composite region increased from 1.1% to 4.4% among CU amyloid-β (Aβ)-negative participants and from 17.4% to 22.2% among CU Aβ-positive participants. Across the same age span, tau PET positivity decreased from 68.0% to 52.9% in participants with MCI and from 91.5% to 74.6% in participants with dementia. Age, Aβ status, APOE ε4 carriership and female sex were all associated with a higher prevalence of tau PET positivity across groups. APOE ε4 carriership in CU individuals lowered the age at onset of both Aβ positivity and tau positivity by decades. Finally, we replicated these associations in an independent autopsy dataset (N = 5,072 from 3 cohorts).

AB - Tau positron emission tomography (PET) imaging allows in vivo detection of tau proteinopathy in Alzheimer's disease, which is associated with neurodegeneration and cognitive decline. Understanding how demographic, clinical and genetic factors relate to tau PET positivity will facilitate its use for clinical practice and research. Here we conducted an analysis of 42 cohorts worldwide (N = 12,048), including 7,394 cognitively unimpaired (CU) participants, 2,177 participants with mild cognitive impairment (MCI) and 2,477 participants with dementia. We found that from age 60 years to 80 years, tau PET positivity in a temporal composite region increased from 1.1% to 4.4% among CU amyloid-β (Aβ)-negative participants and from 17.4% to 22.2% among CU Aβ-positive participants. Across the same age span, tau PET positivity decreased from 68.0% to 52.9% in participants with MCI and from 91.5% to 74.6% in participants with dementia. Age, Aβ status, APOE ε4 carriership and female sex were all associated with a higher prevalence of tau PET positivity across groups. APOE ε4 carriership in CU individuals lowered the age at onset of both Aβ positivity and tau positivity by decades. Finally, we replicated these associations in an independent autopsy dataset (N = 5,072 from 3 cohorts).

KW - ALZHEIMERS ASSOCIATION WORKGROUPS

KW - POSITRON-EMISSION-TOMOGRAPHY

KW - NATIONAL INSTITUTE

KW - DIAGNOSTIC GUIDELINES

KW - NEUROPATHOLOGIC ASSESSMENT

KW - DISEASE

KW - BRAIN

KW - RECOMMENDATIONS

KW - DEMENTIA

KW - PREVALENCE

U2 - 10.1038/s41593-025-02000-6

DO - 10.1038/s41593-025-02000-6

M3 - Article

SN - 1097-6256

VL - 28

SP - 1610

EP - 1621

JO - Nature Neuroscience

JF - Nature Neuroscience

IS - 8

ER -

Tau PET positivity in individuals with and without cognitive impairment varies with age, amyloid-ß status, APOE genotype and sex

Abstract

Keywords

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