| Literature DB >> 29296711 |
Laura J Norton1, Alister P W Funnell1, Jon Burdach1, Beeke Wienert1, Ryo Kurita2, Yukio Nakamura2,3, Sjaak Philipsen4, Richard C M Pearson1, Kate G R Quinlan1, Merlin Crossley1.
Abstract
Genes encoding the human β-like hemoglobin proteins undergo a developmental switch from fetal γ-globin to adult β-globin expression around the time of birth. β-hemoglobinopathies, such as sickle-cell disease and β-thalassemia, result from mutations affecting the adult β-globin gene. The only treatment options currently available carry significant adverse effects. Analyses of heritable variations in fetal hemoglobin (HbF) levels have provided evidence that reactivation of the silenced fetal γ-globin genes in adult erythroid cells is a promising therapy. The γ-globin repressor BCL11A has become the major focus, with several studies investigating its regulation and function as a first step to inhibiting its expression or activity. However, a second repression mechanism was recently shown to be mediated by the transcription factor ZBTB7A/LRF, suggesting that understanding the regulation of ZBTB7A may also be useful. Here we show that Krüppel-like factor 1 (KLF1) directly drives expression of ZBTB7A in erythroid cells by binding to its proximal promoter. We have also uncovered an erythroid-specific regulation mechanism, leading to the upregulation of a novel ZBTB7A transcript in the erythroid compartment. The demonstration that ZBTB7A, like BCL11A, is a KLF1 target gene also fits with the observation that reduced KLF1 expression or activity is associated with HbF derepression.Entities:
Year: 2017 PMID: 29296711 PMCID: PMC5727813 DOI: 10.1182/bloodadvances.2016002303
Source DB: PubMed Journal: Blood Adv ISSN: 2473-9529