Journal Article DZNE-2026-00437

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Pathways to resilience: relationships between cognitive reserve, psychological debt, and Alzheimer's disease biomarkers.

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2026
BioMed Central London

Alzheimer's research & therapy 18(1), 93 () [10.1186/s13195-026-02054-z]

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Abstract: Potentially modifiable lifestyle and psychological factors may influence Alzheimer’s disease (AD)-related brain pathology and cognitive function, thereby influencing cognitive resilience in late life.This cross-sectional study investigated associations and pathways between lifestyle and psychological factors related to cognitive reserve and psychological debt, AD-related biomarkers, and cognitive function, as well as potential differences in these associations between AD risk groups.In total, 298 non-demented older adults (mean age = 69.5 years, 44% women) of the DELCODE study were included. Structural equation modeling was used to assess the associations between the constructs of cognitive reserve (education, occupational complexity, leisure activity participation) and psychological debt (depression and anxiety symptoms, neuroticism, sleep quality), manifest AD-related biomarkers (cerebrospinal fluid [CSF] amyloid-beta [Aβ] 42, splenial white matter hyperintensities [WMH], hippocampal volume), and latent cognitive function of increased AD risk (Preclinical Alzheimer’s Cognitive Composite [PACC]). In the structural equation model, biomarkers were transformed such that higher values indicated greater AD-related brain pathology and age was included as a covariate. Multigroup analyses assessed moderations by established AD risk modifiers, namely sex and apolipoprotein ε4 (APOE ε4) genotype.In the total sample, higher cognitive reserve was associated with better cognitive function (p = .005), independent of AD-related biomarkers. Higher cognitive reserve was associated with lower psychological debt (p = .035); however, neither construct showed a significant association with the AD-related biomarkers (p ≥ .177). AD-related biomarkers of CSF Aβ42 (p = .021), splenial WMH (p = .044), and hippocampal neurodegeneration (p = .007) were each independently associated with lower cognitive function. Most associations were comparable between AD risk groups stratified by sex and APOE ε4 genotype. The relationships between cognitive reserve and psychological debt, and between CSF Aβ42 and splenial WMH were stronger in APOE ε4 non-carriers than in carriers (all p ≤ .020).Cognitive reserve emerges as a key resilience pathway, supporting late-life cognition independently of AD-related pathology, with largely consistent effects across AD risk groups. The role of psychological debt warrants longitudinal investigation, particularly in vulnerable older populations.German Clinical Trials Register: DRKS00007966, Registered: 4 May 2015.The online version contains supplementary material available at 10.1186/s13195-026-02054-z.

Keyword(s): APOE ε4 genotype ; Alzheimer’s disease (AD) ; Biomarkers ; Healthy aging ; Prevention ; Sex differences ; Structural equation modeling

Classification:

Contributing Institute(s):
  1. Brain Resilience (AG Wirth)
  2. Patient Studies (Bonn) (Patient Studies (Bonn))
  3. Clinical Neurophysiology and Memory (AG Düzel)
  4. Clinical Research (Munich) (Clinical Research (Munich))
  5. Clinical Dementia Research (Rostock /Greifswald) (AG Teipel)
  6. Neuropsychology (AG Wagner)
  7. Clinical Research Platform (CRP) (AG Spottke)
  8. Epigenetics and Systems Medicine in Neurodegenerative Diseases (AG Fischer)
  9. Core ICRU (ICRU)
  10. Translational Neuropsychiatry (AG Priller)
  11. Molecular Neurobiology (AG Simons)
  12. Neuroinflammation, Biomarker (AG Heneka)
  13. Interdisciplinary Dementia Research (AG Endres)
  14. Parkinson Genetics (AG Gasser)
  15. Vascular Cognitive Impairment & Post-Stroke Dementia (AG Dichgans)
  16. Biomarker-Assisted Early Detection of Dementias (AG Peters)
  17. Translational Dementia Research (Bonn) (AG Schneider)
  18. Molecular biomarkers for predictive diagnostics of neurodegenerative diseases (AG Wiltfang)
  19. Clinical Alzheimer’s Disease Research (AG Jessen)
Research Program(s):
  1. 353 - Clinical and Health Care Research (POF4-353) (POF4-353)
  2. 352 - Disease Mechanisms (POF4-352) (POF4-352)
  3. 351 - Brain Function (POF4-351) (POF4-351)
Experiment(s):
  1. Longitudinal Cognitive Impairment and Dementia Study

Appears in the scientific report 2026
Database coverage:
Medline ; Creative Commons Attribution CC BY 4.0 ; DOAJ ; OpenAccess ; Article Processing Charges ; Clarivate Analytics Master Journal List ; Current Contents - Clinical Medicine ; DOAJ Seal ; Ebsco Academic Search ; Essential Science Indicators ; Fees ; IF >= 5 ; JCR ; PubMed Central ; SCOPUS ; Science Citation Index Expanded ; Web of Science Core Collection
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The record appears in these collections:
Institute Collections > M DZNE > M DZNE-Clinical Research (Munich)
Institute Collections > BN DZNE > BN DZNE-Patient Studies (Bonn)
Document types > Articles > Journal Article
Institute Collections > GÖ DZNE > GÖ DZNE-AG Wiltfang
Institute Collections > BN DZNE > BN DZNE-AG Schneider
Institute Collections > GÖ DZNE > GÖ DZNE-AG Fischer
Institute Collections > ROS DZNE > ROS DZNE-AG Teipel
Institute Collections > TÜ DZNE > TÜ DZNE-AG Gasser
Institute Collections > BN DZNE > BN DZNE-AG Spottke
Institute Collections > BN DZNE > BN DZNE-AG Jessen
Institute Collections > MD DZNE > MD DZNE-AG Düzel
Institute Collections > BN DZNE > BN DZNE-AG Wagner
Institute Collections > BN DZNE > BN DZNE-AG Heneka
Institute Collections > M DZNE > M DZNE-AG Dichgans
Institute Collections > DD DZNE > DD DZNE-AG Wirth
Institute Collections > B DZNE > B DZNE-AG Priller
Institute Collections > M DZNE > M DZNE-AG Simons
Institute Collections > B DZNE > B DZNE-AG Peters
Institute Collections > B DZNE > B DZNE-AG Endres
Institute Collections > TÜ DZNE > TÜ DZNE-ICRU
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 Record created 2026-04-27, last modified 2026-05-04