The Amyloid-Beta Clearance: From Molecular Targets to Glial and Neural Cells.
Wenjun CaiTong WuNing ChenPublished in: Biomolecules (2023)
The deposition of amyloid-beta (Aβ) plaques in the brain is one of the primary pathological characteristics of Alzheimer's disease (AD). It can take place 20-30 years before the onset of clinical symptoms. The imbalance between the production and the clearance of Aβ is one of the major causes of AD. Enhancing Aβ clearance at an early stage is an attractive preventive and therapeutic strategy of AD. Direct inhibition of Aβ production and aggregation using small molecules, peptides, and monoclonal antibody drugs has not yielded satisfactory efficacy in clinical trials for decades. Novel approaches are required to understand and combat Aβ deposition. Neurological dysfunction is a complex process that integrates the functions of different types of cells in the brain. The role of non-neurons in AD has not been fully elucidated. An in-depth understanding of the interactions between neurons and non-neurons can contribute to the elucidation of Aβ formation and the identification of effective drug targets. AD patient-derived pluripotent stem cells (PSCs) contain complete disease background information and have the potential to differentiate into various types of neurons and non-neurons in vitro, which may bring new insight into the treatment of AD. Here, we systematically review the latest studies on Aβ clearance and clarify the roles of cell interactions among microglia, astroglia and neurons in response to Aβ plaques, which will be beneficial to explore methods for reconstructing AD disease models using inducible PSCs (iPSCs) through cell differentiation techniques and validating the applications of models in understanding the formation of Aβ plaques. This review may provide the most promising directions of finding the clues for preventing and delaying the development of AD.
Keyphrases
- spinal cord
- early stage
- clinical trial
- induced apoptosis
- monoclonal antibody
- squamous cell carcinoma
- stem cells
- white matter
- multiple sclerosis
- oxidative stress
- inflammatory response
- healthcare
- mesenchymal stem cells
- bone marrow
- study protocol
- cerebral ischemia
- lymph node
- cell therapy
- open label
- drug induced
- risk assessment
- electronic health record
- combination therapy
- sentinel lymph node