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Publication : Histone hyperacetylation within the beta-globin locus is context-dependent and precedes high-level gene expression.

First Author  Fromm G Year  2009
Journal  Blood Volume  114
Issue  16 Pages  3479-88
PubMed ID  19690338 Mgi Jnum  J:153540
Mgi Id  MGI:4365687 Doi  10.1182/blood-2009-03-210690
Citation  Fromm G, et al. (2009) Histone hyperacetylation within the beta-globin locus is context-dependent and precedes high-level gene expression. Blood 114(16):3479-88
abstractText  Active gene promoters are associated with covalent histone modifications, such as hyperacetylation, which can modulate chromatin structure and stabilize binding of transcription factors that recognize these modifications. At the beta-globin locus and several other loci, however, histone hyperacetylation extends beyond the promoter, over tens of kilobases; we term such patterns of histone modifications 'hyperacetylated domains.' Little is known of either the mechanism by which these domains form or their function. Here, we show that domain formation within the murine beta-globin locus occurs before either high-level gene expression or erythroid commitment. Analysis of beta-globin alleles harboring deletions of promoters or the locus control region demonstrates that these sequences are not required for domain formation, suggesting the existence of additional regulatory sequences within the locus. Deletion of embryonic globin gene promoters, however, resulted in the formation of a hyperacetylated domain over these genes in definitive erythroid cells, where they are otherwise inactive. Finally, sequences within beta-globin domains exhibit hyperacetylation in a context-dependent manner, and domains are maintained when transcriptional elongation is inhibited. These data narrow the range of possible mechanisms by which hyperacetylated domains form.
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