The accumulation rate of tau aggregates is higher in females and younger amyloid-positive subjects

Smith, Ruben; Strandberg, Olof; Mattsson-Carlgren, Niklas; Leuzy, Antoine; Palmqvist, Sebastian; Pontecorvo, Michael J.; Devous, Michael D.; Ossenkoppele, Rik; Hansson, Oskar

The accumulation rate of tau aggregates is higher in females and younger amyloid-positive subjects

Mark

Smith, Ruben ^LU ; Strandberg, Olof ^LU ; Mattsson-Carlgren, Niklas ^LU

; Leuzy, Antoine ^LU ; Palmqvist, Sebastian ^LU

; Pontecorvo, Michael J. ; Devous, Michael D. ; Ossenkoppele, Rik ^LU and Hansson, Oskar ^LU

(2020) In Brain 143(12). p.3805-3815

Abstract: The development of tau-PET allows paired helical filament tau pathology to be visualized in vivo. Increased knowledge about conditions affecting the rate of tau accumulation could guide the development of therapies halting the progression of Alzheimer's disease. However, the factors modifying the rate of tau accumulation over time in Alzheimer's disease are still largely unknown. Large-scale longitudinal cohort studies, adjusting for baseline tau load, are needed to establish such risk factors. In the present longitudinal study, 419 participants from four cohorts in the USA (Avid 05e, n = 157; Expedition-3, n = 82; ADNI, n = 123) and Sweden (BioFINDER, n = 57) were scanned repeatedly with tau-PET. The study participants were cognitively... (More); The development of tau-PET allows paired helical filament tau pathology to be visualized in vivo. Increased knowledge about conditions affecting the rate of tau accumulation could guide the development of therapies halting the progression of Alzheimer's disease. However, the factors modifying the rate of tau accumulation over time in Alzheimer's disease are still largely unknown. Large-scale longitudinal cohort studies, adjusting for baseline tau load, are needed to establish such risk factors. In the present longitudinal study, 419 participants from four cohorts in the USA (Avid 05e, n = 157; Expedition-3, n = 82; ADNI, n = 123) and Sweden (BioFINDER, n = 57) were scanned repeatedly with tau-PET. The study participants were cognitively unimpaired (n = 153), or patients with mild cognitive impairment (n = 139) or Alzheimer's disease dementia (n = 127). Participants underwent two to four tau-PET (18F-flortaucipir) scans with a mean (± standard deviation) of 537 (±163) days between the first and last scan. The change in tau-PET signal was estimated in temporal meta- and neocortical regions of interest. Subject specific tau-PET slopes were predicted simultaneously by age, sex, amyloid status (determined by amyloid-β PET), APOE ϵ4 genotype, study cohort, diagnosis and baseline tau load. We found that accelerated increase in tau-PET signal was observed in amyloid-β-positive mild cognitive impairment (3.0 ± 5.3%) and Alzheimer's disease dementia (2.9 ± 5.7%), respectively, when compared to either amyloid-β-negative cognitively unimpaired (0.4 ± 2.7%), amyloid-β-negative mild cognitive impairment (-0.4 ± 2.3%) or amyloid-β-positive cognitively unimpaired (1.2 ± 2.8%). Tau-PET uptake was accelerated in females (temporal region of interest: t = 2.86, P = 0.005; neocortical region of interest: t = 2.90, P = 0.004), younger individuals (temporal region of interest: t = -2.49, P = 0.013), and individuals with higher baseline tau-PET signal (temporal region of interest: t = 3.83, P < 0.001; neocortical region of interest: t = 5.01, P < 0.001). Tau-PET slopes decreased with age in amyloid-β-positive subjects, but were stable by age in amyloid-β-negative subjects (age × amyloid-β status interaction: t = -2.39, P = 0.018). There were no effects of study cohort or APOE ϵ4 positivity. In a similar analysis on longitudinal amyloid-β-PET (in ADNI subjects only, n = 639), we found significant associations between the rate of amyloid-β accumulation and APOE ϵ4 positivity, older age and baseline amyloid-β positivity, but no effect of sex. In conclusion, in this longitudinal PET study comprising four cohorts, we found that the tau accumulation rate is greater in females and younger amyloid-β-positive individuals, while amyloid-β accumulation is greater in APOE ϵ4 carriers and older individuals. These findings are important considerations for the design of clinical trials, and might improve our understanding of factors associated with faster tau aggregation and spread.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/5572171c-ed0a-4e92-a562-77e4e8feb076

author

Smith, Ruben ^LU ; Strandberg, Olof ^LU ; Mattsson-Carlgren, Niklas ^LU

; Leuzy, Antoine ^LU ; Palmqvist, Sebastian ^LU

; Pontecorvo, Michael J. ; Devous, Michael D. ; Ossenkoppele, Rik ^LU and Hansson, Oskar ^LU

organization

publishing date

2020

type

Contribution to journal

publication status

published

subject

Neurology

keywords

Alzheimer's disease, disease progression, PET, sex differences, tau

in

Brain

volume

143

issue

12

pages

11 pages

publisher

Oxford University Press

external identifiers

scopus:85099898908
pmid:33439987

ISSN

0006-8950

DOI

10.1093/brain/awaa327

language

English

LU publication?

yes

id

5572171c-ed0a-4e92-a562-77e4e8feb076

date added to LUP

2021-02-10 10:23:11

date last changed

2024-05-30 05:59:35

@article{5572171c-ed0a-4e92-a562-77e4e8feb076,
  abstract     = {{<p>The development of tau-PET allows paired helical filament tau pathology to be visualized in vivo. Increased knowledge about conditions affecting the rate of tau accumulation could guide the development of therapies halting the progression of Alzheimer's disease. However, the factors modifying the rate of tau accumulation over time in Alzheimer's disease are still largely unknown. Large-scale longitudinal cohort studies, adjusting for baseline tau load, are needed to establish such risk factors. In the present longitudinal study, 419 participants from four cohorts in the USA (Avid 05e, n = 157; Expedition-3, n = 82; ADNI, n = 123) and Sweden (BioFINDER, n = 57) were scanned repeatedly with tau-PET. The study participants were cognitively unimpaired (n = 153), or patients with mild cognitive impairment (n = 139) or Alzheimer's disease dementia (n = 127). Participants underwent two to four tau-PET (18F-flortaucipir) scans with a mean (± standard deviation) of 537 (±163) days between the first and last scan. The change in tau-PET signal was estimated in temporal meta- and neocortical regions of interest. Subject specific tau-PET slopes were predicted simultaneously by age, sex, amyloid status (determined by amyloid-β PET), APOE ϵ4 genotype, study cohort, diagnosis and baseline tau load. We found that accelerated increase in tau-PET signal was observed in amyloid-β-positive mild cognitive impairment (3.0 ± 5.3%) and Alzheimer's disease dementia (2.9 ± 5.7%), respectively, when compared to either amyloid-β-negative cognitively unimpaired (0.4 ± 2.7%), amyloid-β-negative mild cognitive impairment (-0.4 ± 2.3%) or amyloid-β-positive cognitively unimpaired (1.2 ± 2.8%). Tau-PET uptake was accelerated in females (temporal region of interest: t = 2.86, P = 0.005; neocortical region of interest: t = 2.90, P = 0.004), younger individuals (temporal region of interest: t = -2.49, P = 0.013), and individuals with higher baseline tau-PET signal (temporal region of interest: t = 3.83, P &lt; 0.001; neocortical region of interest: t = 5.01, P &lt; 0.001). Tau-PET slopes decreased with age in amyloid-β-positive subjects, but were stable by age in amyloid-β-negative subjects (age × amyloid-β status interaction: t = -2.39, P = 0.018). There were no effects of study cohort or APOE ϵ4 positivity. In a similar analysis on longitudinal amyloid-β-PET (in ADNI subjects only, n = 639), we found significant associations between the rate of amyloid-β accumulation and APOE ϵ4 positivity, older age and baseline amyloid-β positivity, but no effect of sex. In conclusion, in this longitudinal PET study comprising four cohorts, we found that the tau accumulation rate is greater in females and younger amyloid-β-positive individuals, while amyloid-β accumulation is greater in APOE ϵ4 carriers and older individuals. These findings are important considerations for the design of clinical trials, and might improve our understanding of factors associated with faster tau aggregation and spread. </p>}},
  author       = {{Smith, Ruben and Strandberg, Olof and Mattsson-Carlgren, Niklas and Leuzy, Antoine and Palmqvist, Sebastian and Pontecorvo, Michael J. and Devous, Michael D. and Ossenkoppele, Rik and Hansson, Oskar}},
  issn         = {{0006-8950}},
  keywords     = {{Alzheimer's disease; disease progression; PET; sex differences; tau}},
  language     = {{eng}},
  number       = {{12}},
  pages        = {{3805--3815}},
  publisher    = {{Oxford University Press}},
  series       = {{Brain}},
  title        = {{The accumulation rate of tau aggregates is higher in females and younger amyloid-positive subjects}},
  url          = {{http://dx.doi.org/10.1093/brain/awaa327}},
  doi          = {{10.1093/brain/awaa327}},
  volume       = {{143}},
  year         = {{2020}},
}

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The accumulation rate of tau aggregates is higher in females and younger amyloid-positive subjects