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Association between self-reported multimorbidity and longitudinal brain Aβ deposition in Alzheimer’s disease

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  • Xian-Le Bu

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Third Military Medical University
    State Key Laboratory of Trauma and Chemical Poisoning (Third Military Medical University))

  • Wei Zhu

    (Third Military Medical University)

  • Qing-Hua Wang

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Zhuo-Ting Liu

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Yun-Yu Bao

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Yu-Di Bai

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Jiang-Hui Li

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Zhi-Hao Liu

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Jia-Ling Zhao

    (University of Electronic Science and Technology of China)

  • Yang Xiang

    (University of Electronic Science and Technology of China)

  • Wang-Sheng Jin

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Jun Wang

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Ministry of Education of China)

  • Xia Lei

    (Third Military Medical University)

  • Yan-Jiang Wang

    (Third Military Medical University
    Chongqing Key Laboratory of Ageing and Brain Diseases
    Third Military Medical University
    State Key Laboratory of Trauma and Chemical Poisoning (Third Military Medical University))

Abstract

Multimorbidity is common in older adults. However, whether multimorbidity accelerates brain beta-amyloid (Aβ) deposition, the molecular driver of Alzheimer’s disease (AD), in humans remains largely unknown. In this study, we selected 435 brain Aβ-positive participants with available longitudinal Aβ-PET data (mean duration 3.9 years) from the Alzheimer’s Disease Neuroimaging Initiative (ADNI) cohort. Twenty-two self-reported chronic disorders were considered as a measure of the severity of multimorbidity. After adjustment for age, sex, education level, APOE-ε4 status and baseline cognitive state, individuals with a high or medium multimorbidity burden had faster rates of brain Aβ accumulation than individuals with a low multimorbidity burden. Moreover, both the central nervous system and peripheral system multimorbidity burdens were associated with longitudinal brain Aβ deposition. These results indicate that peripheral organ and tissue dysfunctions may contribute to AD pathogenesis, which may help researchers better understand AD pathogenesis and tailor interventions for AD from a systemic view.

Suggested Citation

  • Xian-Le Bu & Wei Zhu & Qing-Hua Wang & Zhuo-Ting Liu & Yun-Yu Bao & Yu-Di Bai & Jiang-Hui Li & Zhi-Hao Liu & Jia-Ling Zhao & Yang Xiang & Wang-Sheng Jin & Jun Wang & Xia Lei & Yan-Jiang Wang, 2025. "Association between self-reported multimorbidity and longitudinal brain Aβ deposition in Alzheimer’s disease," Nature Communications, Nature, vol. 16(1), pages 1-12, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-60748-8
    DOI: 10.1038/s41467-025-60748-8
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