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Autor: Rodrigue, Karen M

3 záznamů v PubMed Filtry

Článek

Depressive Symptoms and Amyloid Pathology

Wiels, Wietse A
Autor Wiels, Wietse A Faculty of Medicine and Pharmacy, Vrije Universiteit Brussel, Brussels, Belgium Department of Neurology, Onze-Lieve-Vrouw Hospital, Aalst, Belgium
Oomens, Julie E
Autor Oomens, Julie E Department of Psychiatry & Neuropsychology, Alzheimer Center Limburg, School for Mental Health and Neuroscience, Maastricht University, Maastricht, the Netherlands
Engelborghs, Sebastiaan
Autor Engelborghs, Sebastiaan Vrije Universiteit Brussel, Center for Neurosciences, Neuroprotection & Neuromodulation Research Group, Brussels, Belgium Departments of Neurology and Psychiatry and Bru-BRAIN, Universitair Ziekenhuis Brussel, Brussels, Belgium Department of Biomedical Sciences, University of Antwerp, Antwerp, Belgium
Baeken, Chris
Autor Baeken, Chris Vrije Universiteit Brussel, Center for Neurosciences, Neuroprotection & Neuromodulation Research Group, Brussels, Belgium Departments of Neurology and Psychiatry and Bru-BRAIN, Universitair Ziekenhuis Brussel, Brussels, Belgium Department of Head and Skin, Ghent Experimental Psychiatry Lab, Faculty of Medicine and Health Sciences, Ghent University, Ghent, Belgium Department of Electrical Engineering, Eindhoven University of Technology, Eindhoven, the Netherlands
von Arnim, Christine A F
Autor von Arnim, Christine A F Department of Geriatrics, University of Goettingen Medical School, Goettingen, Germany Clinic for Neurogeriatrics and Neurological Rehabilitation, University and Rehabilitation Hospital Ulm, Ulm, Germany
Boada, Mercè
Autor Boada, Mercè Ace Alzheimer Center Barcelona - Universitat Internacional de Catalunya, Barcelona, Spain Centre for Biomedical Research Network on Neurodegenerative Diseases, Network Center for Biomedical Research in Neurodegenerative Diseases, National Institute of Health Carlos III, Madrid, Spain
Didic, Mira
Autor Didic, Mira Assitance Publique des Hopitaux de Marseille, Timone, Service de Neurologie et Neuropsychologie, Hôpital Timone Adultes, Marseille, France Aix Marseille University, National Institute of Health and Medical Research, Neurosciences des Systèmes, Marseille, France
Dubois, Bruno
Autor Dubois, Bruno Department of Neurology, Institut de la Mémoire et de la Maladie d'Alzheimer, Centre de Référence Démences Rares, Hôpital de la Pitié-Salpêtrière, Assistance Publique- Hôpitaux de Paris, Paris, France
Fladby, Tormod
Autor Fladby, Tormod Department of Neurology, Akershus University Hospital, Lorenskog, Norway
van der Flier, Wiesje M
Autor van der Flier, Wiesje M Department of Neurology, Alzheimer Centre Amsterdam, Amsterdam Neuroscience, Amsterdam University Medical Centers location Vrije Universiteit Medical Center, Amsterdam, Amsterdam, the Netherlands Epidemiology and Data Science, Vrije Universiteit Amsterdam, Amsterdam University Medical Centers, location Vrije Universiteit Medical Center, Amsterdam, the Netherlands

JAMA psychiatry. 2025 Mar 01 ; 82 (3) : 296-310.

JAMA Psychiatry
ISSN 2168-6238 | 2168-622X
Zdroj

IMPORTANCE: Depressive symptoms are associated with cognitive decline in older individuals. Uncertainty about underlying mechanisms hampers diagnostic and therapeutic efforts. This large-scale study aimed to elucidate the association between depressive symptoms and amyloid pathology. OBJECTIVE: To examine the association between depressive symptoms and amyloid pathology and its dependency on age, sex, education, and APOE genotype in older individuals without dementia. DESIGN, SETTING, AND PARTICIPANTS: Cross-sectional analyses were performed using data from the Amyloid Biomarker Study data pooling initiative. Data from 49 research, population-based, and memory clinic studies were pooled and harmonized. The Amyloid Biomarker Study has been collecting data since 2012 and data collection is ongoing. At the time of analysis, 95 centers were included in the Amyloid Biomarker Study. The study included 9746 individuals with normal cognition (NC) and 3023 participants with mild cognitive impairment (MCI) aged between 34 and 100 years for whom data on amyloid biomarkers, presence of depressive symptoms, and age were available. Data were analyzed from December 2022 to February 2024. MAIN OUTCOMES AND MEASURES: Amyloid-β1-42 levels in cerebrospinal fluid or amyloid positron emission tomography scans were used to determine presence or absence of amyloid pathology. Presence of depressive symptoms was determined on the basis of validated depression rating scale scores, evidence of a current clinical diagnosis of depression, or self-reported depressive symptoms. RESULTS: In individuals with NC (mean [SD] age, 68.6 [8.9] years; 5664 [58.2%] female; 3002 [34.0%] APOE ε4 carriers; 937 [9.6%] had depressive symptoms; 2648 [27.2%] had amyloid pathology), the presence of depressive symptoms was not associated with amyloid pathology (odds ratio [OR], 1.13; 95% CI, 0.90-1.40; P = .29). In individuals with MCI (mean [SD] age, 70.2 [8.7] years; 1481 [49.0%] female; 1046 [44.8%] APOE ε4 carriers; 824 [27.3%] had depressive symptoms; 1668 [55.8%] had amyloid pathology), the presence of depressive symptoms was associated with a lower likelihood of amyloid pathology (OR, 0.73; 95% CI 0.61-0.89; P = .001). When considering subgroup effects, in individuals with NC, the presence of depressive symptoms was associated with a higher frequency of amyloid pathology in APOE ε4 noncarriers (mean difference, 5.0%; 95% CI 1.0-9.0; P = .02) but not in APOE ε4 carriers. This was not the case in individuals with MCI. CONCLUSIONS AND RELEVANCE: Depressive symptoms were not consistently associated with a higher frequency of amyloid pathology in participants with NC and were associated with a lower likelihood of amyloid pathology in participants with MCI. These findings were not influenced by age, sex, or education level. Mechanisms other than amyloid accumulation may commonly underlie depressive symptoms in late life.

MeSH
amyloidní beta-protein * mozkomíšní mok metabolismus MeSH
apolipoprotein E4 genetika MeSH
biologické markery mozkomíšní mok MeSH
deprese * MeSH
dospělí MeSH
kognitivní dysfunkce * MeSH
lidé středního věku MeSH
lidé MeSH
peptidové fragmenty mozkomíšní mok MeSH
pozitronová emisní tomografie * MeSH
průřezové studie MeSH
senioři nad 80 let MeSH
senioři MeSH
věkové faktory MeSH
Check Tag
dospělí MeSH
lidé středního věku MeSH
lidé MeSH
mužské pohlaví MeSH
senioři nad 80 let MeSH
senioři MeSH
ženské pohlaví MeSH
Publikační typ
časopisecké články MeSH
Názvy látek
amyloid beta-protein (1-42) MeSH Prohlížeč
amyloidní beta-protein * MeSH
apolipoprotein E4 MeSH
biologické markery MeSH
peptidové fragmenty MeSH

Článek

Cerebral Microbleeds and Amyloid Pathology Estimates From the Amyloid Biomarker Study

JAMA network open. 2025 Jan 02 ; 8 (1) : e2455571. [epub] 20250102

JAMA Netw Open
ISSN 2574-3805
Zdroj

IMPORTANCE: Baseline cerebral microbleeds (CMBs) and APOE ε4 allele copy number are important risk factors for amyloid-related imaging abnormalities in patients with Alzheimer disease (AD) receiving therapies to lower amyloid-β plaque levels. OBJECTIVE: To provide prevalence estimates of any, no more than 4, or fewer than 2 CMBs in association with amyloid status, APOE ε4 copy number, and age. DESIGN, SETTING, AND PARTICIPANTS: This cross-sectional study used data included in the Amyloid Biomarker Study data pooling initiative (January 1, 2012, to the present [data collection is ongoing]). Data from 15 research and memory clinic studies were pooled and harmonized. Participants included individuals for whom data on age, cognitive status, amyloid status, and presence of CMBs were available. Data were analyzed from October 22, 2023, to April 26, 2024. MAIN OUTCOMES AND MEASURES: The main outcomes were age, cognitive status, amyloid status and presence, location, and number of CMBs. Presence of amyloid pathology was determined based on 42 amino acid-long form of amyloid-β peptide (Aβ42) levels in cerebrospinal fluid or on amyloid-positron emission tomography. Presence and, in a subset, location (lobar vs deep) and number of CMBs were determined on magnetic resonance imaging (locally with visual rating). RESULTS: Among 4080 participants included in the analysis, the mean (SD) age was 66.5 (8.9) years, and 2241 (54.9%) were female. A total of 2973 participants had no cognitive impairment (cognitive unimpairment [CU]), and 1107 had mild cognitive impairment (MCI) or AD dementia (ADD). One thousand five hundred and thirteen participants (37.1%) had amyloid pathology, 1368 of 3599 (38.0%) with data available were APOE ε4 carriers, and 648 (15.9%) had CMBs. In the CU group, amyloid pathology and APOE ε4 copy number were not associated with presence of any, no more than 4, or fewer than 2 CMBs but were associated with increased odds of lobar CMBs (odds ratio [OR] for amyloid, 1.42 [95% CI, 1.20-1.69], P < .001; OR for 2 vs 0 alleles, 1.81 [95% CI, 1.19-2.74], P = .006; OR for 1 vs 0 alleles, 1.10 [95% CI, 0.83-1.46], P = .49; and OR for 2 vs 1 allele, 1.64 [95% CI, 0.90-2.97], P = .11; overall P = .02). In the MCI-ADD group, amyloid pathology was associated with presence of any CMBs (OR, 1.51 [95% CI, 1.17-1.96], P = .002), no more than 4 CMBs (OR, 1.44 [95% CI, 1.18-1.82], P = .002), and fewer than 2 CMBs (OR 1.34 [95% CI, 1.03-1.74], P = .03) but not lobar CMBs. APOE ε4 copy number was associated with presence of any (OR for 2 vs 0 alleles, 1.72 [95% CI, 0.88-3.35], P = .11; OR for 1 vs 0 alleles, 0.78 [95% CI, 0.59-1.04], P = .09; and OR for 2 vs 1 allele, 2.20 [95% CI, 1.32-3.67], P = .002; overall P < .001) and no more than 4 CMBs (OR for 2 vs 0 alleles, 1.31 [95% CI, 0.64-2.68], P = .45; OR for 1 vs 0 alleles, 0.75 [95% CI, 0.54-1.04], P = .08; and OR for 2 vs 1 allele, 1.76 [95% CI, 0.97-3.19], P = .06; overall P = .03) but not with fewer than 2 or lobar CMBs. Prevalence estimates of CMBs ranged from 6% at 50 years of age in a non-APOE ε4 allele carrier with no amyloid pathology and no cognitive impairment to 52% at 90 years of age in an APOE ε4 homozygote carrier with amyloid pathology and cognitive impairment. CONCLUSIONS AND RELEVANCE: In this cross-sectional study of 4080 participants, prevalence estimates of CMBs were associated with amyloid status, APOE ε4 copy number, and age. CMB prevalence estimates may help inform safety evaluations for antiamyloid clinical trials.

MeSH
Alzheimerova nemoc * epidemiologie genetika MeSH
amyloidní beta-protein * metabolismus mozkomíšní mok MeSH
amyloidní plaky patologie MeSH
apolipoprotein E4 genetika MeSH
biologické markery * mozkomíšní mok MeSH
cerebrální krvácení * epidemiologie MeSH
lidé středního věku MeSH
lidé MeSH
magnetická rezonanční tomografie metody MeSH
pozitronová emisní tomografie MeSH
průřezové studie MeSH
senioři nad 80 let MeSH
senioři MeSH
Check Tag
lidé středního věku MeSH
lidé MeSH
mužské pohlaví MeSH
senioři nad 80 let MeSH
senioři MeSH
ženské pohlaví MeSH
Publikační typ
časopisecké články MeSH
Názvy látek
amyloidní beta-protein * MeSH
apolipoprotein E4 MeSH
biologické markery * MeSH

Článek

Prevalence Estimates of Amyloid Abnormality Across the Alzheimer Disease Clinical Spectrum

JAMA neurology. 2022 Mar 01 ; 79 (3) : 228-243.

JAMA Neurol
ISSN 2168-6157 | 2168-6149
Zdroj

IMPORTANCE: One characteristic histopathological event in Alzheimer disease (AD) is cerebral amyloid aggregation, which can be detected by biomarkers in cerebrospinal fluid (CSF) and on positron emission tomography (PET) scans. Prevalence estimates of amyloid pathology are important for health care planning and clinical trial design. OBJECTIVE: To estimate the prevalence of amyloid abnormality in persons with normal cognition, subjective cognitive decline, mild cognitive impairment, or clinical AD dementia and to examine the potential implications of cutoff methods, biomarker modality (CSF or PET), age, sex, APOE genotype, educational level, geographical region, and dementia severity for these estimates. DESIGN, SETTING, AND PARTICIPANTS: This cross-sectional, individual-participant pooled study included participants from 85 Amyloid Biomarker Study cohorts. Data collection was performed from January 1, 2013, to December 31, 2020. Participants had normal cognition, subjective cognitive decline, mild cognitive impairment, or clinical AD dementia. Normal cognition and subjective cognitive decline were defined by normal scores on cognitive tests, with the presence of cognitive complaints defining subjective cognitive decline. Mild cognitive impairment and clinical AD dementia were diagnosed according to published criteria. EXPOSURES: Alzheimer disease biomarkers detected on PET or in CSF. MAIN OUTCOMES AND MEASURES: Amyloid measurements were dichotomized as normal or abnormal using cohort-provided cutoffs for CSF or PET or by visual reading for PET. Adjusted data-driven cutoffs for abnormal amyloid were calculated using gaussian mixture modeling. Prevalence of amyloid abnormality was estimated according to age, sex, cognitive status, biomarker modality, APOE carrier status, educational level, geographical location, and dementia severity using generalized estimating equations. RESULTS: Among the 19 097 participants (mean [SD] age, 69.1 [9.8] years; 10 148 women [53.1%]) included, 10 139 (53.1%) underwent an amyloid PET scan and 8958 (46.9%) had an amyloid CSF measurement. Using cohort-provided cutoffs, amyloid abnormality prevalences were similar to 2015 estimates for individuals without dementia and were similar across PET- and CSF-based estimates (24%; 95% CI, 21%-28%) in participants with normal cognition, 27% (95% CI, 21%-33%) in participants with subjective cognitive decline, and 51% (95% CI, 46%-56%) in participants with mild cognitive impairment, whereas for clinical AD dementia the estimates were higher for PET than CSF (87% vs 79%; mean difference, 8%; 95% CI, 0%-16%; P = .04). Gaussian mixture modeling-based cutoffs for amyloid measures on PET scans were similar to cohort-provided cutoffs and were not adjusted. Adjusted CSF cutoffs resulted in a 10% higher amyloid abnormality prevalence than PET-based estimates in persons with normal cognition (mean difference, 9%; 95% CI, 3%-15%; P = .004), subjective cognitive decline (9%; 95% CI, 3%-15%; P = .005), and mild cognitive impairment (10%; 95% CI, 3%-17%; P = .004), whereas the estimates were comparable in persons with clinical AD dementia (mean difference, 4%; 95% CI, -2% to 9%; P = .18). CONCLUSIONS AND RELEVANCE: This study found that CSF-based estimates using adjusted data-driven cutoffs were up to 10% higher than PET-based estimates in people without dementia, whereas the results were similar among people with dementia. This finding suggests that preclinical and prodromal AD may be more prevalent than previously estimated, which has important implications for clinical trial recruitment strategies and health care planning policies.

MeSH
Alzheimerova nemoc * mozkomíšní mok diagnostické zobrazování epidemiologie MeSH
amyloidní beta-protein mozkomíšní mok MeSH
amyloidogenní proteiny MeSH
amyloidóza * MeSH
apolipoproteiny E genetika MeSH
biologické markery mozkomíšní mok MeSH
kognitivní dysfunkce * diagnostické zobrazování epidemiologie MeSH
lidé středního věku MeSH
lidé MeSH
peptidové fragmenty mozkomíšní mok MeSH
pozitronová emisní tomografie MeSH
prevalence MeSH
proteiny tau mozkomíšní mok MeSH
průřezové studie MeSH
senioři MeSH
Check Tag
lidé středního věku MeSH
lidé MeSH
mužské pohlaví MeSH
senioři MeSH
ženské pohlaví MeSH
Publikační typ
časopisecké články MeSH
Názvy látek
amyloidní beta-protein MeSH
amyloidogenní proteiny MeSH
apolipoproteiny E MeSH
biologické markery MeSH
peptidové fragmenty MeSH
proteiny tau MeSH

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