Estrogen receptor α drives pro-resilient transcription in mouse models of depression.
Zachary S LorschYong-Hwee Eddie LohImmanuel PurushothamanDeena M WalkerEric M PariseMarine SaleryMichael E CahillGeorgia E HodesMadeline L PfauHope KronmanPeter J HamiltonOrna IsslerBenoit LabontéAnn E SymondsMatthew ZuckerTie-Yuan ZhangMichael J MeaneyScott J RussoLi ShenRosemary C BagotEric J NestlerPublished in: Nature communications (2018)
Most people exposed to stress do not develop depression. Animal models have shown that stress resilience is an active state that requires broad transcriptional adaptations, but how this homeostatic process is regulated remains poorly understood. In this study, we analyze upstream regulators of genes differentially expressed after chronic social defeat stress. We identify estrogen receptor α (ERα) as the top regulator of pro-resilient transcriptional changes in the nucleus accumbens (NAc), a key brain reward region implicated in depression. In accordance with these findings, nuclear ERα protein levels are altered by stress in male and female mice. Further, overexpression of ERα in the NAc promotes stress resilience in both sexes. Subsequent RNA-sequencing reveals that ERα overexpression in NAc reproduces the transcriptional signature of resilience in male, but not female, mice. These results indicate that NAc ERα is an important regulator of pro-resilient transcriptional changes, but with sex-specific downstream targets.
Keyphrases
- transcription factor
- estrogen receptor
- genome wide identification
- depressive symptoms
- stress induced
- social support
- gene expression
- anti inflammatory
- endoplasmic reticulum
- breast cancer cells
- healthcare
- mouse model
- sleep quality
- high fat diet induced
- multiple sclerosis
- type diabetes
- single cell
- adipose tissue
- white matter
- heat stress
- subarachnoid hemorrhage
- oxidative stress
- protein protein
- binding protein
- heat shock
- heat shock protein