Abstract

BackgroundNeuroglial cells that provide homeostatic support and form defence of the nervous system contribute to all neurological disorders. We analyzed three major types of neuroglia, astrocytes, oligodendrocytes, and microglia in the brains of an animal model of autism spectrum disorder, in which rats were exposed prenatally to antiepileptic and mood stabilizer drug valproic acid; this model being of acknowledged clinical relevance.MethodsWe tested the autistic-like behaviors of valproic acid-prenatally exposed male rats by performing isolation-induced ultrasonic vocalizations, the three-chamber test, and the hole board test. To account for human infancy, adolescence, and adulthood, such tasks were performed at postnatal day 13, postnatal day 35, and postnatal day 90, respectively. After sacrifice, we examined gene and protein expression of specific markers of neuroglia in hippocampus, prefrontal cortex, and cerebellum, these brain regions being associated with autism spectrum disorder pathogenesis.ResultsInfant offspring of VPA-exposed dams emitted less ultrasonic vocalizations when isolated from their mothers and siblings and, in adolescence and adulthood, they showed altered sociability in the three chamber test and increased stereotypic behavior in the hole board test. Molecular analyses indicate that prenatal valproic acid exposure affects all types of neuroglia, mainly causing transcriptional modifications. The most prominent changes occur in prefrontal cortex and in the hippocampus of autistic-like animals; these changes are particularly evident during infancy and adolescence, while they appear to be mitigated in adulthood.ConclusionsNeuroglial pathological phenotype in autism spectrum disorder rat model appears to be rather mild with little signs of widespread and chronic neuroinflammation.

Highlights

  • Neuroglial cells that provide homeostatic support and form defence of the nervous system contribute to all neurological disorders

  • Astrocytes in Autism spectrum disorder (ASD) model rats To investigate the effect of prenatal valproic acid (VPA) exposure on astrocyte phenotype, we analyzed transcription and expression of the archetypal astroglial markers glial fibrillary acidic protein (GFAP) and the neurotrophin/Ca2+ binding protein S100B

  • We detected a significant increase of GFAP mRNA in the HPC of VPA-exposed rats (Fig. 2c)

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Summary

Introduction

Neuroglial cells that provide homeostatic support and form defence of the nervous system contribute to all neurological disorders. Glial cells are non-excitable (2018) 9:66 homeostatic cells of the central nervous system (CNS), sub-classified into astrocytes, oligodendrocytes and their precursors ( known as NG-2 glia) and microglia; all types of glia sustain vital brain functions [12]. Microglia detect diverse pathological extracellular signals, and respond to them to protect the brain. These cells contribute to the development of the nervous tissue, shaping neuronal ensembles and synaptic plasticity [21,22,23,24]

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