Journal of neuroinflammation

Lack of VPS35 in brain immune cells reduces their ability to clear amyloid beta and increases amyloid beta-related damage

Updated

Abstract

Microglial deficiency in 5XFAD mice is associated with impaired learning and increased β-amyloid plaques.

  • Learning and memory functions are significantly decreased in microglial VPS35 deficient 5XFAD mice.
  • There is an observed increase in insoluble, fibrillar β-amyloid plaques and reactive astrocytes in these mice.
  • Microglial VPS35 is necessary for the development of disease-associated microglia ().
  • A strong association exists between microglial uptake of β-amyloid and the development of DAM.
  • Impairment of DAM development may contribute to the acceleration of cognitive decline in this model of Alzheimer’s disease.

Simplified

Key numbers

3 of 6
Increase in Aβ Plaques
Plaque-associated microglia per plaque in deficient mice
6
Cognitive Decline
Number of male mice per group in behavioral tests

Full Text

What this is

  • Microglial deficiency exacerbates Alzheimer's disease (AD) pathology in a mouse model.
  • The study investigates the role of in microglial cells and its impact on Aβ phagocytosis and cognitive function.
  • Findings indicate that loss of impairs the development of disease-associated microglia () and Aβ clearance.

Essence

  • Microglial deficiency accelerates Aβ pathology and cognitive decline in 5XFAD mice, suggesting its critical role in AD development through impaired formation and Aβ uptake.

Key takeaways

  • Microglial deficiency leads to increased levels of insoluble and fibrillar Aβ, as well as plaque formation in 5XFAD mice.
  • Learning and memory deficits are observed in deficient mice, indicating a direct link between loss and cognitive decline.
  • Impaired development and reduced Aβ phagocytosis are associated with microglial deficiency, highlighting its role in AD pathology.

Caveats

  • The study is limited to a mouse model, which may not fully replicate human AD pathology.
  • Further research is needed to elucidate the precise molecular mechanisms by which influences formation and Aβ clearance.

Definitions

  • VPS35: A protein involved in the retromer complex, crucial for sorting and recycling membrane proteins in cells.
  • DAM (disease-associated microglia): A subtype of activated microglia that responds to pathological conditions, such as Aβ accumulation in Alzheimer's disease.

Simplified

Funding

Competing interests

The authors declare that they have no competing interests.
PubMed

Funding Sources

NIA NIH HHS
PubMed
NIH HHS
PubMed

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