Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals

Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals

Abstract Objective To study risk factors for decreasing aβ1–42 concentrations in cerebrospinal fluid (CSF) in cognitively unimpaired individuals with initially normal amyloid and tau markers, and to investigate whether such aβ1–42 decreases are associated with subsequent decline in cognition and oth...

Full description

Bibliographic Details
Main Authors: Betty M. Tijms, Lisa Vermunt, Marissa D. Zwan, Argonde C. vanHarten, Wiesje M. van derFlier, Charlotte E. Teunissen, Philip Scheltens, Pieter Jelle Visser, for ADNI
Format: Article
Language:English
Published: Wiley 2018-09-01
Series:Annals of Clinical and Translational Neurology
Online Access:https://doi.org/10.1002/acn3.615
id doaj-2c12719fd4114c828ca97ec927d1a64f
record_format Article
spelling doaj-2c12719fd4114c828ca97ec927d1a64f2021-05-02T02:49:22ZengWileyAnnals of Clinical and Translational Neurology2328-95032018-09-01591037104710.1002/acn3.615Pre‐amyloid stage of Alzheimer's disease in cognitively normal individualsBetty M. Tijms0Lisa Vermunt1Marissa D. Zwan2Argonde C. vanHarten3Wiesje M. van derFlier4Charlotte E. Teunissen5Philip Scheltens6Pieter Jelle Visser7for ADNIAlzheimer Center Department of Neurology VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsAlzheimer Center Department of Neurology VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsAlzheimer Center Department of Neurology VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsAlzheimer Center Department of Neurology VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsAlzheimer Center Department of Neurology VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsDepartment of Epidemiology and Biostatistics VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsAlzheimer Center Department of Neurology VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsAlzheimer Center Department of Neurology VU University Medical Center Amsterdam Neuroscience Amsterdam The NetherlandsAbstract Objective To study risk factors for decreasing aβ1–42 concentrations in cerebrospinal fluid (CSF) in cognitively unimpaired individuals with initially normal amyloid and tau markers, and to investigate whether such aβ1–42 decreases are associated with subsequent decline in cognition and other biomarkers of Alzheimer's disease. Methods Cognitively normal subjects (n = 83, 75 ± 5 years, 35(42%) female) with normal CSF aβ1–42 and tau and repeated CSF sampling were selected from ADNI. Subject level slopes of aβ1–42 decreases were estimated with mixed models. We tested associations of baseline APP processing markers (BACE1 activity, aβ1–40, aβ1–38 and sAPPβ) and decreasing aβ1–42 levels by including an interaction term between time and APP marker. Associations between decreasing aβ1–42 levels and clinical decline (i.e., progression to mild cognitive impairment or dementia, MMSE, memory functioning) and biological decline (tau, hippocampal volume, glucose processing and amyloid PET) over a time period of 8–10 years were assessed. Results Aβ1–42 levels decreased annually with −4.6 ± 1 pg/mL. Higher baseline BACE1 activity (β(se) = −0.06(0.03), P < 0.05), aβ1–40 (β(se)= −0.11(.03), P < 0.001), and aβ1–38 levels (β(se) = −0.11(0.03), P < 0.001) predicted faster decreasing aβ1–42. The fastest tertile of decreasing aβ1–42 rates was associated with subsequent pathophysiological processes: 11(14%) subjects developed abnormal amyloid levels after 3 ± 1.7 years, showed increased risk for clinical progression (Hazard Ratio[95CI] = 4.8[1.1–21.0]), decreases in MMSE, glucose metabolism and hippocampal volume, and increased CSF tau and amyloid aggregation on PET (all P < 0.05). Interpretation Higher APP processing and fast decreasing aβ1–42 could be among the earliest, pre‐amyloid, pathological changes in Alzheimer's disease.https://doi.org/10.1002/acn3.615
collection DOAJ
language English
format Article
sources DOAJ
author Betty M. Tijms
Lisa Vermunt
Marissa D. Zwan
Argonde C. vanHarten
Wiesje M. van derFlier
Charlotte E. Teunissen
Philip Scheltens
Pieter Jelle Visser
for ADNI
spellingShingle Betty M. Tijms
Lisa Vermunt
Marissa D. Zwan
Argonde C. vanHarten
Wiesje M. van derFlier
Charlotte E. Teunissen
Philip Scheltens
Pieter Jelle Visser
for ADNI
Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals
Annals of Clinical and Translational Neurology
author_facet Betty M. Tijms
Lisa Vermunt
Marissa D. Zwan
Argonde C. vanHarten
Wiesje M. van derFlier
Charlotte E. Teunissen
Philip Scheltens
Pieter Jelle Visser
for ADNI
author_sort Betty M. Tijms
title Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals
title_short Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals
title_full Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals
title_fullStr Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals
title_full_unstemmed Pre‐amyloid stage of Alzheimer's disease in cognitively normal individuals
title_sort pre‐amyloid stage of alzheimer's disease in cognitively normal individuals
publisher Wiley
series Annals of Clinical and Translational Neurology
issn 2328-9503
publishDate 2018-09-01
description Abstract Objective To study risk factors for decreasing aβ1–42 concentrations in cerebrospinal fluid (CSF) in cognitively unimpaired individuals with initially normal amyloid and tau markers, and to investigate whether such aβ1–42 decreases are associated with subsequent decline in cognition and other biomarkers of Alzheimer's disease. Methods Cognitively normal subjects (n = 83, 75 ± 5 years, 35(42%) female) with normal CSF aβ1–42 and tau and repeated CSF sampling were selected from ADNI. Subject level slopes of aβ1–42 decreases were estimated with mixed models. We tested associations of baseline APP processing markers (BACE1 activity, aβ1–40, aβ1–38 and sAPPβ) and decreasing aβ1–42 levels by including an interaction term between time and APP marker. Associations between decreasing aβ1–42 levels and clinical decline (i.e., progression to mild cognitive impairment or dementia, MMSE, memory functioning) and biological decline (tau, hippocampal volume, glucose processing and amyloid PET) over a time period of 8–10 years were assessed. Results Aβ1–42 levels decreased annually with −4.6 ± 1 pg/mL. Higher baseline BACE1 activity (β(se) = −0.06(0.03), P < 0.05), aβ1–40 (β(se)= −0.11(.03), P < 0.001), and aβ1–38 levels (β(se) = −0.11(0.03), P < 0.001) predicted faster decreasing aβ1–42. The fastest tertile of decreasing aβ1–42 rates was associated with subsequent pathophysiological processes: 11(14%) subjects developed abnormal amyloid levels after 3 ± 1.7 years, showed increased risk for clinical progression (Hazard Ratio[95CI] = 4.8[1.1–21.0]), decreases in MMSE, glucose metabolism and hippocampal volume, and increased CSF tau and amyloid aggregation on PET (all P < 0.05). Interpretation Higher APP processing and fast decreasing aβ1–42 could be among the earliest, pre‐amyloid, pathological changes in Alzheimer's disease.
url https://doi.org/10.1002/acn3.615
work_keys_str_mv AT bettymtijms preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT lisavermunt preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT marissadzwan preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT argondecvanharten preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT wiesjemvanderflier preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT charlotteeteunissen preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT philipscheltens preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT pieterjellevisser preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
AT foradni preamyloidstageofalzheimersdiseaseincognitivelynormalindividuals
_version_ 1721495926192734208

Similar Items