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Dominant influence of gamma-globin promoter polymorphisms on fetal haemoglobin expression in sickle cell disease.

机译:γ-球蛋白启动子多态性对镰状细胞病中胎儿血红蛋白表达的显着影响。

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摘要

Polymorphisms of multiple cis-acting elements in the beta-globin locus are associated with variable fetal haemoglobin (HbF) level in sickle cell disease. We developed a multiplex assay permitting simultaneous analysis of three polymorphic cis elements spanning 53 kb of the beta-globin locus. We identified concordance between polymorphic alleles in gamma- and beta-globin promoters however a significant number of betaS-chromosomes were identified with polymorphisms in hypersensitive site 2 (HS2) of the beta-globin locus control region juxtaposed to atypical cis alleles in the gamma-promoter. Analysis of an unusually large number of such hybrid haplotype chromosomes provided unique insight into HbF level associated with specific cis alleles. Associations between cis alleles and HbF level in patients were verified by in vitro functional analysis. Our findings indicate that compared to HS2, polymorphism in the gamma-promoter exerts a dominant influence on HbF level in sickle cell disease.
机译:β-珠蛋白基因座中多个顺式作用元件的多态性与镰状细胞病中的可变胎儿血红蛋白(HbF)水平相关。我们开发了一种多重分析方法,可以同时分析跨越53 kbβ-球蛋白基因座的三个多态性顺式元件。我们确定了γ-和β-球蛋白启动子中的多态性等位基因之间的一致性,但是,在β-球蛋白基因座控制区域的超敏位点2(HS2)中,与γ-非典型顺式等位基因并列的多态性中发现了大量的βS染色体。启动子。对大量此类杂种单倍型染色体的分析提供了与特定顺式等位基因相关的HbF水平的独特见解。通过体外功能分析验证了患者体内顺式等位基因与HbF水平之间的关联。我们的发现表明,与HS2相比,γ-启动子中的多态性对镰状细胞病中的HbF水平起主要作用。

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