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Scientists discover how chronic stress causes brain damage

MedicalXpress Breaking News-and-Events Aug 14, 2019

DGIST announced on July 2 that professor Seong-Woon Yu's team, in the Department of Brain and Cognitive Sciences, discovered that chronic stress causes autophagic death of adult hippocampal neural stem cells (NSCs). These findings are expected to open up new strategies for combatting stress-associated neural diseases.

Chronic stress is infamous for its association with various mental diseases such as depression and schizophrenia that have become very serious social problems. Stress can even raise the risk of neurodegenerative diseases, such as Alzheimer disease. However, the exact mechanisms underlying damage of brain functions have not been well known. While previous animal studies found that new neurons are generated less often in stressed mice, apoptosis, a well-known cell suicide pathway, was not found in NSCs, leading to a conclusion that cell death is not related to loss of NSCs during stress. Thus, the cause of decline in adult neurogenesis, which is the generation of new neural cells in the adult brain, especially in the hippocampus, has remained unclear.

Yu's team discovered for the first time that chronic stress causes autophagic death of adult hippocampal NSCs. Autophagy (self-eating in Greek) is a cellular process to protect cells from unfavorable conditions through digestion and recycling of inner cell materials, whereby cells can remove toxic or old intracellular components and get nutrients and metabolites for survival. However, autophagy can turn into a self-destruction process under certain conditions, leading to autophagic cell death. Autophagic cell death is a form of cell death distinguished from apoptosis by the causative role of autophagy for cell demise. Using NSCs derived from rodents and genetically modified mice, the research team discovered that the death of hippocampal NSCs is prevented and normal brain functions are maintained without stress symptoms when Atg7, one of the major autophagic genes, is deleted.

The research team also further examined the mechanism controlling the autophagy induction of NSCs in more depth, proving that the SGK3 (serum/glucocorticoid regulated kinase) gene is the trigger for autophagy initiation. Therefore, when the SGK3 gene is removed, hippocampal NSCs do not undergo cell death and are spared from stress.

Yu said, "It is clear from our study that cognitive defects and mood disorders brought about by stress are through autophagic death of adult hippocampal NSCs. With continuous research, we'll be able to take a step further toward the development of effective treatment of psychological disorders such as depression and anxiety. Furthermore, stress-related neurodegenerative diseases including dementia could [...] also benefit[...] from our study. We hope to be able to develop much faster and more effective mental disease treatments through joint research with the Chinese National Compound Library to develop [an] SGK3 inhibitor together."

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