Locus-specific epigenetic remodeling controls addiction- and depression-related behaviors.
Elizabeth A HellerHannah M CatesCatherine J PeñaHaosheng SunNingyi ShaoJian FengSam A GoldenJames P HermanJessica J WalshMichelle Mazei-RobisonDeveroux FergusonScott KnightMark A GerberChristian NieveraMing-Hu HanScott J RussoCarol S TammingaRachael L NeveLi ShenH Steve ZhangFeng ZhangEric J NestlerPublished in: Nature neuroscience (2014)
Chronic exposure to drugs of abuse or stress regulates transcription factors, chromatin-modifying enzymes and histone post-translational modifications in discrete brain regions. Given the promiscuity of the enzymes involved, it has not yet been possible to obtain direct causal evidence to implicate the regulation of transcription and consequent behavioral plasticity by chromatin remodeling that occurs at a single gene. We investigated the mechanism linking chromatin dynamics to neurobiological phenomena by applying engineered transcription factors to selectively modify chromatin at a specific mouse gene in vivo. We found that histone methylation or acetylation at the Fosb locus in nucleus accumbens, a brain reward region, was sufficient to control drug- and stress-evoked transcriptional and behavioral responses via interactions with the endogenous transcriptional machinery. This approach allowed us to relate the epigenetic landscape at a given gene directly to regulation of its expression and to its subsequent effects on reward behavior.
Keyphrases
- transcription factor
- genome wide
- dna methylation
- genome wide identification
- gene expression
- copy number
- dna binding
- dna damage
- white matter
- poor prognosis
- depressive symptoms
- multiple sclerosis
- emergency department
- cerebral ischemia
- atomic force microscopy
- heat stress
- single cell
- brain injury
- physical activity
- subarachnoid hemorrhage