4.7 Review

Iron Homeostasis Disorder and Alzheimer's Disease

Journal

Publisher

MDPI
DOI: 10.3390/ijms222212442

Keywords

Alzheimer's disease; iron homeostasis disorder; iron homeostasis regulators; beta-amyloid; tau; APP; central nervous system; oxidative stress; pathogenesis; genetic intervention

Funding

  1. Fundamental Research Funds for the Central Universities, Beijing Municipal Natural Science Foundation [7202129]
  2. Class B Breeding Program of Special Projects for Leading Science and Technology of the Chinese Academy of Sciences [XDPB16]
  3. National Natural Science Foundation of China [31571042]
  4. Key Basic Research Project of Applied Basic Research Program of Hebei Province [18966315D]
  5. One Hundred Outstanding Creative Talents Support Program of Hebei [BR2-218]

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Iron is essential for organisms, but excess can cause oxidative stress and toxicity. Alzheimer's disease (AD) is a common degenerative disease of the central nervous system, with unclear pathogenesis, potentially linked to abnormal iron accumulation in the brain. Understanding the relationship between iron metabolism and AD is crucial for new treatment strategies.
Iron is an essential trace metal for almost all organisms, including human; however, oxidative stress can easily be caused when iron is in excess, producing toxicity to the human body due to its capability to be both an electron donor and an electron acceptor. Although there is a strict regulation mechanism for iron homeostasis in the human body and brain, it is usually inevitably disturbed by genetic and environmental factors, or disordered with aging, which leads to iron metabolism diseases, including many neurodegenerative diseases such as Alzheimer's disease (AD). AD is one of the most common degenerative diseases of the central nervous system (CNS) threatening human health. However, the precise pathogenesis of AD is still unclear, which seriously restricts the design of interventions and treatment drugs based on the pathogenesis of AD. Many studies have observed abnormal iron accumulation in different regions of the AD brain, resulting in cognitive, memory, motor and other nerve damages. Understanding the metabolic balance mechanism of iron in the brain is crucial for the treatment of AD, which would provide new cures for the disease. This paper reviews the recent progress in the relationship between iron and AD from the aspects of iron absorption in intestinal cells, storage and regulation of iron in cells and organs, especially for the regulation of iron homeostasis in the human brain and prospects the future directions for AD treatments.

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