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Structural Determinant of β-Amyloid Formation: From Transmembrane Protein Dimerization to β-Amyloid Aggregates

BIOMEDICINES (2022)

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Journal

BIOMEDICINES
Volume 10, Issue 11, Pages -

Publisher

MDPI
DOI: 10.3390/biomedicines10112753

Keywords

Alzheimer's disease; Amyloid Precursor Protein; amyloid beta; APP-C99; dimerization; orientations; aggregation; oligomerization

Categories

Biochemistry & Molecular Biology Medicine, Research & Experimental Pharmacology & Pharmacy

Funding

  1. Universite catholique de Louvain
  2. FRS-FNRS [ASP/A 876]
  3. Alzheimer Research Foundation (SAO-FRA/Stop Alzheimer Research Foundation)
  4. Ludwig Institute for Cancer Research
  5. Fondation contre le cancer
  6. Salus Sanguinis and Fondation Les avions de Sebastien
  7. Projets Action de recherche concertee (ARC) [16/21-073]
  8. FNRS [T.0043.21, F 44/8/5-MCF/UIG-10955]
  9. FWO postdoctoral fellowship [12B7423N]
  10. Consortium Interaction of KU Leuven [C14/21/095]
  11. SAO-FRA/Stop Alzheimer Research Foundation
  12. Fondation Louvain and Queen Elisabeth Medical Research Foundation
  13. FNRS grant [PDRT.0177.18]
  14. UCLouvain Action de Reechrche Concertee [ARC 21/26-114]

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Most neurodegenerative diseases are characterized by protein folding disorders, such as Alzheimer's disease. These diseases lead to the appearance of protein aggregates in vulnerable regions of the nervous system, which progressively spread through the neuronal network. Alzheimer's disease is characterized by neurofibrillary tangles composed of tau proteins and senile plaques composed of amyloid peptides. Understanding the structural determinants of the precursor protein APP and the formation of different A beta aggregates is crucial in deciphering the pathological conformational changes and mechanisms underlying amyloid fibril formation.
Most neurodegenerative diseases have the characteristics of protein folding disorders, i.e., they cause lesions to appear in vulnerable regions of the nervous system, corresponding to protein aggregates that progressively spread through the neuronal network as the symptoms progress. Alzheimer's disease is one of these diseases. It is characterized by two types of lesions: neurofibrillary tangles (NFTs) composed of tau proteins and senile plaques, formed essentially of amyloid peptides (A beta). A combination of factors ranging from genetic mutations to age-related changes in the cellular context converge in this disease to accelerate A beta deposition. Over the last two decades, numerous studies have attempted to elucidate how structural determinants of its precursor (APP) modify A beta production, and to understand the processes leading to the formation of different A beta aggregates, e.g., fibrils and oligomers. The synthesis proposed in this review indicates that the same motifs can control APP function and A beta production essentially by regulating membrane protein dimerization, and subsequently A beta aggregation processes. The distinct properties of these motifs and the cellular context regulate the APP conformation to trigger the transition to the amyloid pathology. This concept is critical to better decipher the patterns switching APP protein conformation from physiological to pathological and improve our understanding of the mechanisms underpinning the formation of amyloid fibrils that devastate neuronal functions.

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