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Publication : PRC2 preserves intestinal progenitors and restricts secretory lineage commitment.

First Author  Chiacchiera F Year  2016
Journal  EMBO J Volume  35
Issue  21 Pages  2301-2314
PubMed ID  27585866 Mgi Jnum  J:237929
Mgi Id  MGI:5817528 Doi  10.15252/embj.201694550
Citation  Chiacchiera F, et al. (2016) PRC2 preserves intestinal progenitors and restricts secretory lineage commitment. EMBO J 35(21):2301-2314
abstractText  Chromatin modifications shape cell heterogeneity by activating and repressing defined sets of genes involved in cell proliferation, differentiation and development. Polycomb-repressive complexes (PRCs) act synergistically during development and differentiation by maintaining transcriptional repression of common genes. PRC2 exerts this activity by catalysing H3K27 trimethylation. Here, we show that in the intestinal epithelium PRC2 is required to sustain progenitor cell proliferation and the correct balance between secretory and absorptive lineage differentiation programs. Using genetic models, we show that PRC2 activity is largely dispensable for intestinal stem cell maintenance but is strictly required for radiation-induced regeneration by preventing Cdkn2a transcription. Combining these models with genomewide molecular analysis, we further demonstrate that preferential accumulation of secretory cells does not result from impaired proliferation of progenitor cells induced by Cdkn2a activation but rather from direct regulation of transcription factors responsible for secretory lineage commitment. Overall, our data uncover a dual role of PRC2 in intestinal homeostasis highlighting the importance of this repressive layer in controlling cell plasticity and lineage choices in adult tissues.
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