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Social defeat stress affects resident's clock gene and bdnf expression in the brain

Publikace na Přírodovědecká fakulta |
2021

Tento text není v aktuálním jazyce dostupný. Zobrazuje se verze "en".Abstrakt

Social defeat stress affects behavior and changes the expression of the genes underlying neuronal plasticity in the brain. The circadian clock regulates most neuronal processes in the brain, which results in daily variations of complex behavior, and any disturbance in circadian clock oscillations increases the risk of mood and cognitive disbalance.

In this study, we assessed the effect of acute and repeated social defeat stress onPer2andNr1d1expression in prefrontal cortexes, hippocampi, pineal glands, olfactory bulbs, cerebella, and pituitary glands. We also evaluated the effect of our experimental setting on levels ofBdnfand plasma corticosterone, two markers widely used to asses the impact of stress on mammalian physiology.

Our data show that single and repeated social defeat stress upregulates the expression of both clock genes andBdnfin all brain structures, and corticosterone in the blood. While the general pattern ofBdnfupregulation suggests higher sensitivity in the intruder group, the clock genes are induced more significantly in residents, especially by repeated stress sessions.

Our work thus suggests that the model of stress-induced anxiety and depression should consider a group of residents because, for some parameters, they may respond more distinctively than intruders.LAY SUMMARY The resident/intruder experimental paradigm affects the expression of clock genesPer2,Nr1d1andBdnfin the brain structures and plasma corticosterone level. The induction of clock genes is evident in both experimental groups; however, it is more marked in residents.

Together with the significant increase inBdnflevels in the majority of brain structures and plasma corticosterone in residents, our data suggest that in the model of social defeat stress, the utility of an experimental group of residents could be contributive.