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Neonatal immune challenge poses a sex-specific risk for epigenetic microglial reprogramming and behavioral impairment

Marius Schwabenland, Omar Mossad, Annika Sievert, Adam G. Peres, Elena Ringel, Sebastian Baasch, Julia Kolter, Giulia Cascone, Nikolaos Dokalis, Andreas Vlachos, Zsolt Ruzsics, Philipp Henneke, Marco Prinz, Thomas Blank

2023Nature Communications22 citationsDOIOpen Access PDF

Abstract

While the precise processes underlying a sex bias in the development of central nervous system (CNS) disorders are unknown, there is growing evidence that an early life immune activation can contribute to the disease pathogenesis. When we mimicked an early systemic viral infection or applied murine cytomegalovirus (MCMV) systemically in neonatal female and male mice, only male adolescent mice presented behavioral deficits, including reduced social behavior and cognition. This was paralleled by an increased amount of infiltrating T cells in the brain parenchyma, enhanced interferon-γ (IFNγ) signaling, and epigenetic reprogramming of microglial cells. These microglial cells showed increased phagocytic activity, which resulted in abnormal loss of excitatory synapses within the hippocampal brain region. None of these alterations were seen in female adolescent mice. Our findings underscore the early postnatal period's susceptibility to cause sex-dependent long-term CNS deficiencies following infections.

Topics & Concepts

Hippocampal formationMicrogliaReprogrammingEpigeneticsImmune systemImmunologyBiologyCentral nervous systemNeurosciencePathogenesisInflammationGeneticsCellGeneNeuroinflammation and Neurodegeneration MechanismsTryptophan and brain disordersImmune Response and Inflammation
Neonatal immune challenge poses a sex-specific risk for epigenetic microglial reprogramming and behavioral impairment | Litcius