Noradrenaline release from the locus coeruleus shapes stress-induced hippocampal gene expression
- PMID: 38477670
- PMCID: PMC10937036
- DOI: 10.7554/eLife.88559
Noradrenaline release from the locus coeruleus shapes stress-induced hippocampal gene expression
Abstract
Exposure to an acute stressor triggers a complex cascade of neurochemical events in the brain. However, deciphering their individual impact on stress-induced molecular changes remains a major challenge. Here, we combine RNA sequencing with selective pharmacological, chemogenetic, and optogenetic manipulations to isolate the contribution of the locus coeruleus-noradrenaline (LC-NA) system to the acute stress response in mice. We reveal that NA release during stress exposure regulates a large and reproducible set of genes in the dorsal and ventral hippocampus via β-adrenergic receptors. For a smaller subset of these genes, we show that NA release triggered by LC stimulation is sufficient to mimic the stress-induced transcriptional response. We observe these effects in both sexes, and independent of the pattern and frequency of LC activation. Using a retrograde optogenetic approach, we demonstrate that hippocampus-projecting LC neurons directly regulate hippocampal gene expression. Overall, a highly selective set of astrocyte-enriched genes emerges as key targets of LC-NA activation, most prominently several subunits of protein phosphatase 1 (Ppp1r3c, Ppp1r3d, Ppp1r3g) and type II iodothyronine deiodinase (Dio2). These results highlight the importance of astrocytic energy metabolism and thyroid hormone signaling in LC-mediated hippocampal function and offer new molecular targets for understanding how NA impacts brain function in health and disease.
Keywords: hippocampus; locus coeruleus; mouse; neuroscience; noradrenaline; optogenetics; stress; transcriptome.
© 2023, Privitera et al.
Conflict of interest statement
MP, Lv, AF, SD, RZ, RW, SL, OS, FR, AH, YV, DV, PD, PG, JB No competing interests declared
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Update of
- doi: 10.1101/2023.02.02.526661
- doi: 10.7554/eLife.88559.1
- doi: 10.7554/eLife.88559.2
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