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Fine Tuning of Globin Gene Expression by DNA Methylation
Author(s) -
Alon Goren,
Giora Simchen,
Eitan Fibach,
Piroska E. Szabó,
Keiji Tanimoto,
Lyubomira Chakalova,
Gerd P. Pfeifer,
Peter Fraser,
James Douglas Engel,
Howard Cedar
Publication year - 2006
Publication title -
plos one
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.99
H-Index - 332
ISSN - 1932-6203
DOI - 10.1371/journal.pone.0000046
Subject(s) - dna methylation , biology , epigenetics , microbiology and biotechnology , locus control region , regulation of gene expression , methylation , gene expression , histone methylation , gene , histone , epigenetics of physical exercise , promoter , transcription (linguistics) , globin , hypersensitive site , genetics , linguistics , philosophy
Expression patterns in the globin gene cluster are subject to developmental regulation in vivo. While the γ A and γ G genes are expressed in fetal liver, both are silenced in adult erythrocytes. In order to decipher the role of DNA methylation in this process, we generated a YAC transgenic mouse system that allowed us to control γ A methylation during development. DNA methylation causes a 20-fold repression of γ A both in non-erythroid and adult erythroid cells. In erythroid cells this modification works as a dominant mechanism to repress γ gene expression, probably through changes in histone acetylation that prevent the binding of erythroid transcription factors to the promoter. These studies demonstrate that DNA methylation serves as an elegant in vivo fine-tuning device for selecting appropriate genes in the globin locus. In addition, our findings provide a mechanism for understanding the high levels of γ-globin transcription seen in patients with Hereditary Persistence of Fetal Hemoglobin, and help explain why 5azaC and butyrate compounds stimulate γ-globin expression in patients with β-hemoglobinopathies.

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