Treg-depleted mice were more likely to hide in darkness, moved less, and gave up on self-preservation actions more easilysuggesting that Treg-depleted mice were more anxious and depressed than control mice.
These neurobehavioral changes in Treg-depleted mice were reversed after restoration of Foxp3-expressing cells, and Treg-restored mice were more similar to controls than Treg-depleted mice were. Additionally, mice bred to model Alzheimer’s disease showed cognitive impairments when their Tregs were depleted.
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The authors posit that Treg depletion causes proliferation of peripheral immune cells, some of which can cross the blood-brain barrier into the brain and cause inflammatory responses in the hippocampal formation.
This transient activation of innate immunity in the brain can cause anxiety, depression or Alzheimer’s disease-type cognitive deterioration, according to the authors.
Source: Eurekalert