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首页> 外文期刊>Haematologica >Estimation of the difference in HbF expression due to loss of the 5' δ-globin BCL11A binding region
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Estimation of the difference in HbF expression due to loss of the 5' δ-globin BCL11A binding region

机译:估计由于5'δ-珠蛋白BCL11A结合区缺失导致的HbF表达差异

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BCL11A was the focus of recent studies on its inhibiting effect when bound onto the β-globin cluster in the mechanism of hemoglobin switching and HbF downregulation. We examined a cohort of 10 patients displaying different HbF levels and short deletions within the γβ-δ intergenic region to find a possible correlation with the BCL11A binding site located 5' to the δ-globin gene. Precise characterization of deletions was achieved using a custom DNA-array chip and breakpoint sequencing. The α-globin cluster and major SNP associated with HbF expression were genotyped. Our results show that the loss of the BCL11A binding domain located 5' to the δ-globin gene is correlated with a strong HbF difference (mean+2.7 g/dL, ratio 2.81). This result provides evidence for the use of BCL11A level down-regulation or this domain blockage for new therapies in sickle cell disease and β-thalassemia major patients.
机译:BCL11A在结合到血红蛋白转换和HbF下调的机制中与β珠蛋白簇结合时的抑制作用成为近期研究的重点。我们检查了10名患者的队列,这些患者在γβ-δ基因间区域内表现出不同的HbF水平和短缺失,以发现其与位于δ-珠蛋白基因5'处的BCL11A结合位点可能相关。使用定制的DNA阵列芯片和断点测序可实现对缺失的精确表征。对与HbF表达相关的α珠蛋白簇和主要SNP进行基因分型。我们的结果表明,位于δ-珠蛋白基因5'处的BCL11A结合域的丢失与HbF的强烈差异相关(平均值+2.7 g / dL,比率2.81)。这一结果为镰状细胞病和重型β地中海贫血患者的新疗法提供了使用BCL11A水平下调或这种结构域阻断的证据。

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