Polycomb repressive complex 2 (PRC2) silences genes responsible for neurodegeneration.
Melanie von SchimmelmannPhilip A FeinbergJosefa M SullivanStacy M KuAna BadimonMary Kaye DuffZichen WangAlexander LachmannScott DewellAvi Ma'ayanMing-Hu HanAlexander TarakhovskyAnne SchaeferPublished in: Nature neuroscience (2016)
Normal brain function depends on the interaction between highly specialized neurons that operate within anatomically and functionally distinct brain regions. Neuronal specification is driven by transcriptional programs that are established during early neuronal development and remain in place in the adult brain. The fidelity of neuronal specification depends on the robustness of the transcriptional program that supports the neuron type-specific gene expression patterns. Here we show that polycomb repressive complex 2 (PRC2), which supports neuron specification during differentiation, contributes to the suppression of a transcriptional program that is detrimental to adult neuron function and survival. We show that PRC2 deficiency in striatal neurons leads to the de-repression of selected, predominantly bivalent PRC2 target genes that are dominated by self-regulating transcription factors normally suppressed in these neurons. The transcriptional changes in PRC2-deficient neurons lead to progressive and fatal neurodegeneration in mice. Our results point to a key role of PRC2 in protecting neurons against degeneration.
Keyphrases
- gene expression
- transcription factor
- spinal cord
- cerebral ischemia
- resting state
- white matter
- functional connectivity
- genome wide
- dna methylation
- quality improvement
- cell fate
- multiple sclerosis
- heat shock
- subarachnoid hemorrhage
- spinal cord injury
- palliative care
- dna binding
- brain injury
- parkinson disease
- young adults
- wild type
- free survival