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Home / Health / Brain's Immune Cells: New Alzheimer's Protectors?

Brain's Immune Cells: New Alzheimer's Protectors?

1 Dec

•

Summary

  • Brain's immune cells, microglia, may prevent Alzheimer's onset.
  • Specific microglia subtype lowers PU.1 and boosts CD28 protein.
  • Therapies could potentially enhance these protective cells.

Scientists have identified a crucial role for specific brain immune cells, microglia, in potentially preventing Alzheimer's disease. When these cells encounter amyloid-beta clumps, they can enter a protective state, distinct from their previously known inflammatory responses. This neuroprotective subtype exhibits lower levels of the PU.1 protein and increased expression of CD28, a key immune system component.

In studies using mouse models, this specialized microglia subtype effectively slowed the accumulation of amyloid-beta and tau proteins. Conversely, reducing CD28 production led to more harmful, inflammation-prone microglia and increased amyloid plaque formation. This suggests a natural defense mechanism against Alzheimer's, which current therapies might aim to enhance.

The findings offer a mechanistic explanation for why lower PU.1 levels are linked to reduced Alzheimer's risk. Researchers are hopeful that future immunotherapies could convert microglia into this beneficial state, though human studies are necessary. This work also highlights shared immune regulation logic across different cell types, paving the way for novel Alzheimer's treatments.

Disclaimer: This story has been auto-aggregated and auto-summarised by a computer program. This story has not been edited or created by the Feedzop team.
Recent studies suggest specific types of microglia in the brain may play a protective role in preventing the onset of Alzheimer's disease.
Lower levels of PU.1 and higher levels of CD28 in microglia are linked to a reduced risk and slowed progression of Alzheimer's disease.
Researchers aim to verify these findings in humans and explore therapies that could enhance the neuroprotective abilities of microglia.

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