Papachatzopoulou Adamantia, Kaimakis Polynikis, Pourfarzad Farzin, Menounos Panagiotis G, Evangelakou Panagiota, Kollia Panagoula, Grosveld Frank G, Patrinos George P
Department of General Biology, School of Medicine, University of Patras, Patras, Greece.
Am J Hematol. 2007 Nov;82(11):1005-9. doi: 10.1002/ajh.20979.
We report a novel set of genetic markers in the DNaseI hypersensitive sites comprising the human beta-globin locus chromatin hub (CH), namely HS-111 and 3'HS1. The HS-111 (-21 G>A) and 3'HS1 (+179 C>T) transitions form CH haplotypes, which occur at different frequencies in beta-thalassemia intermedia and major patients and normal (nonthalassemic) individuals. We also show that the 3'HS1 (+179 C>T) variation results in a GATA-1 binding site and correlates with increased fetal hemoglobin production in beta-thalassemia intermedia patients. In contrast, the HS-111 (+126 G>A) transition, found in three normal chromosomes, is simply a rare polymorphism. We conclude that the CH haplotypes are useful genetic determinants for beta-thalassemia major and intermedia patients, while the 3'HS1 (+179 C>T) mutation may have functional consequences in gamma-globin genes expression.
我们报告了一组新的位于包含人类β-珠蛋白基因座染色质枢纽(CH)的DNaseI超敏位点中的遗传标记,即HS-111和3'HS1。HS-111(-21 G>A)和3'HS1(+179 C>T)转换形成CH单倍型,其在中间型和重型β地中海贫血患者以及正常(非地中海贫血)个体中以不同频率出现。我们还表明,3'HS1(+179 C>T)变异导致一个GATA-1结合位点,并与中间型β地中海贫血患者胎儿血红蛋白产量增加相关。相比之下,在三条正常染色体中发现的HS-111(+126 G>A)转换仅仅是一种罕见的多态性。我们得出结论,CH单倍型是重型和中间型β地中海贫血患者有用的遗传决定因素,而3'HS1(+179 C>T)突变可能对γ-珠蛋白基因表达具有功能影响。