Early life adversity targets the transcriptional signature of hippocampal NG2+ glia and affects voltage gated sodium (Nav) channels properties

6533b7d4fe1ef96bd12633df

RESEARCH PRODUCT

Early life adversity targets the transcriptional signature of hippocampal NG2+ glia and affects voltage gated sodium (Nav) channels properties

Markus Fricke Hatice Yigit Malin Wennström Marianne B. Müller Marianne B. Müller Gregers Wegener Giulia Treccani Matthias Linke Thomas Mittmann Franziska Mey Vanessa Schleuβner Jacqueline Trotter Thomas Lingner Michael A. Van Der Kooij Michael J. Schmeisser David B. Herzog

subject

Neurophysiology and neuropsychology Candidate gene Nav-channels Physiology Na-channels Neurosciences. Biological psychiatry. Neuropsychiatry Hippocampal formation Biology Biochemistry NG2+ glia Transcriptome 03 medical and health sciences Cellular and Molecular Neuroscience 0302 clinical medicine Endocrinology Mediator Downregulation and upregulation Original Research Article RC346-429 Molecular Biology Voltage-gated ion channel Endocrine and Autonomic Systems QP351-495 Nav-channels ; Scn7a ; Transcriptome ; Early life stress ; Translational psychiatry ; NG2+ glia Early life stress 030227 psychiatry Scn7a Crosstalk (biology)nervous system Neurology. Diseases of the nervous system Transcriptome Neuroscience Translational psychiatry 030217 neurology & neurosurgery Homeostasis RC321-571

description

The precise mechanisms underlying the detrimental effects of early life adversity (ELA) on adult mental health remain still elusive. To date, most studies have exclusively targeted neuronal populations and not considered neuron-glia crosstalk as a crucially important element for the integrity of stress-related brain function. Here, we have investigated the impact of ELA, in the form of a limited bedding and nesting material (LBN) paradigm, on a glial subpopulation with unique properties in brain homeostasis, the NG2+ cells. First, we have established a link between maternal behavior, activation of the offspring's stress response and heterogeneity in the outcome to LBN manipulation. We further showed that LBN targets the hippocampal NG2+ transcriptome with glucocorticoids being an important mediator of the LBN-induced molecular changes. LBN altered the NG2+ transcriptome and these transcriptional effects were correlated with glucocorticoids levels. The functional relevance of one LBN-induced candidate gene, Scn7a, could be confirmed by an increase in the density of voltage-gated sodium (Nav) channel activated currents in hippocampal NG2+ cells. Scn7a remained upregulated until adulthood in LBN animals, which displayed impaired cognitive performance. Considering that Nav channels are important for NG2+ cell-to-neuron communication, our findings provide novel insights into the disruption of this process in LBN mice.

year	journal	country	edition	language
2021-11-01	Neurobiology of Stress

https://doi.org/10.1016/j.ynstr.2021.100338