Fetal Hemoglobin Altering Effects of KLF1, BCL11A rs11886868 and XmnI-HBG2 on Transfusion Dependent Beta Thalassemia Patients: Preeliminary Study

Y. Arıkan, B. Yolcular, Erdal Lu, I. Keser
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Abstract

Aim: High fetal hemoglobin value is one of the quantitative trait in beta thalassemia and may effect transfusion dependency status of beta thalassemic cases. There are population-based differences about known genetic modifiers of different fetal hemoglobin values. We aimed to find if high fetal hemoglobin value are caused by XmnI-HBG2 polymorphism, rs11886868 of BCL11A or KLF1 whole gene mutations. Material and Methods: Genotyping procedure of thirty well re-defined and characterized transfusion dependent beta thalassemia patients was conducted via either sanger sequencing or and PCR-RFLP. Statistic analysis of groups and multiple logistic regression analysis of related genotypes were performed. Results: We found strong correlations between transfusion dependency and fetal hemoglobin levels (P<0.05). IVS.I.110 (G>A) homozygous mutation was found to be predominant in HBB gene. Lower fetal hemoglobin levels were seen in IVS.I.110 (G>A) homozygous group (P<0.05). Total count of variations among the three modifier genes BCL11A polymorphism was leading first. We did not observe any statistically significant relationship in patients with beta thalassemia major patients who have high fetal hemoglobin values between three modifiers group (P>0.05). Conclusion: This is the first research report from Turkey in terms of 3 different modifiers were analysed and evaluated. Since some cases have more than one variations in these three modifiers, involving higher sample size may overcome this challenge. Other genomic alterations rather than XmnI-HBG2, variations of BCL11A rs11886868 and mutation profile of KLF1 gene, which could decrease or abolish the effect of gamma globin repressors, may have more direct role with high fetal hemoglobin levels in patients with transfusion dependent beta thalassemia in Turkey.
KLF1、BCL11A rs11886868和XmnI-HBG2对输血依赖性β -地中海贫血患者胎儿血红蛋白改变的初步研究
目的:高胎儿血红蛋白值是β -地中海贫血的数量性状之一,可能影响β -地中海贫血患者的输血依赖状况。不同胎儿血红蛋白值的已知基因修饰因子存在人群差异。我们的目的是发现高胎儿血红蛋白值是由XmnI-HBG2多态性、BCL11A rs11886868或KLF1全基因突变引起的。材料和方法:通过sanger测序或PCR-RFLP对30例重新定义和特征明确的输血依赖性地中海贫血患者进行基因分型。进行组间统计分析及相关基因型的多元logistic回归分析。结果:我们发现输血依赖与胎儿血红蛋白水平(PA)有很强的相关性,纯合突变在HBB基因中占优势。ivsi 110中胎儿血红蛋白水平较低纯合子组(G>A) (P0.05)。结论:这是土耳其首次对3种不同的调节剂进行分析和评价的研究报告。由于某些情况下这三种修饰剂有不止一种变化,涉及更高的样本量可能会克服这一挑战。与XmnI-HBG2、BCL11A rs11886868变异和KLF1基因突变谱相比,其他能够降低或消除γ -珠蛋白抑制因子作用的基因组改变可能在土耳其输血依赖性地中海贫血患者胎儿血红蛋白高水平中发挥更直接的作用。
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