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Publication : MEIS homeodomain proteins facilitate PARP1/ARTD1-mediated eviction of histone H1.

First Author  Hau AC Year  2017
Journal  J Cell Biol Volume  216
Issue  9 Pages  2715-2729
PubMed ID  28739678 Mgi Jnum  J:246265
Mgi Id  MGI:5925156 Doi  10.1083/jcb.201701154
Citation  Hau AC, et al. (2017) MEIS homeodomain proteins facilitate PARP1/ARTD1-mediated eviction of histone H1. J Cell Biol 216(9):2715-2729
abstractText  Pre-B-cell leukemia homeobox (PBX) and myeloid ecotropic viral integration site (MEIS) proteins control cell fate decisions in many physiological and pathophysiological contexts, but how these proteins function mechanistically remains poorly defined. Focusing on the first hours of neuronal differentiation of adult subventricular zone-derived stem/progenitor cells, we describe a sequence of events by which PBX-MEIS facilitates chromatin accessibility of transcriptionally inactive genes: In undifferentiated cells, PBX1 is bound to the H1-compacted promoter/proximal enhancer of the neuron-specific gene doublecortin (Dcx) Once differentiation is induced, MEIS associates with chromatin-bound PBX1, recruits PARP1/ARTD1, and initiates PARP1-mediated eviction of H1 from the chromatin fiber. These results for the first time link MEIS proteins to PARP-regulated chromatin dynamics and provide a mechanistic basis to explain the profound cellular changes elicited by these proteins.
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