Mast cells proliferate in the peri-hippocampal space during early development and modulate local and peripheral immune cells

  • Alexa C. Blanchard
  • , Anna Maximova
  • , Taylor Phillips-Jones
  • , Matthew R. Bruce
  • , Pavlos Anastasiadis
  • , Christie V. Dionisos
  • , Kaliroi Engel
  • , Erin Reinl
  • , Aidan Pham
  • , Sonia Malaiya
  • , Nevil Singh
  • , Seth Ament
  • , Margaret M. McCarthy

Research output: Contribution to journalArticlepeer-review

Abstract

Brain development is a non-linear process of regionally specific epochs occurring during windows of sensitivity to endogenous and exogenous stimuli. We have identified an epoch in the neonatal rat brain defined by a transient population of peri-hippocampal mast cells (phMCs) that are abundant from birth through 2-weeks post-natal but absent thereafter. The phMCs are maintained by proliferation and harbor a unique transcriptome compared with mast cells residing in the skin, bone marrow, or other brain regions. Pharmacological activation of this population broadly increases blood-brain barrier permeability, recruits peripheral immune cells, and stunts local microglia proliferation. Examination of the post-mortem human brain demonstrated mast cells in the peri-hippocampal region of a newborn, but not an older infant, suggesting a similar developmental period exists in humans. Mast cells specifically, and early-life inflammation generally, have been linked to heightened risk for neurodevelopmental disorders, and these results demonstrate a plausible source of that risk.

Original languageEnglish
Pages (from-to)853-870.e7
JournalDevelopmental cell
Volume60
Issue number6
DOIs
StatePublished - Mar 24 2025

Keywords

  • CCL2
  • blood-brain-barrier
  • hippocampal development
  • hippocampus
  • inflammation
  • mast cells
  • microglia
  • monocytes
  • neurodevelopment
  • proliferation

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