坦桑尼亚和英国镰状细胞贫血症患者胎儿血红蛋白的遗传学。
Genetics of fetal hemoglobin in Tanzanian and British patients with sickle cell anemia.
机构信息
Muhimbili University of Health and Allied Sciences, Dar-es-Salaam, Tanzania.
出版信息
Blood. 2011 Jan 27;117(4):1390-2. doi: 10.1182/blood-2010-08-302703. Epub 2010 Nov 10.
Abstract
Fetal hemoglobin (HbF, α(2)γ(2)) is a major contributor to the remarkable phenotypic heterogeneity of sickle cell anemia (SCA). Genetic variation at 3 principal loci (HBB cluster on chromosome 11p, HBS1L-MYB region on chromosome 6q, and BCL11A on chromosome 2p) have been shown to influence HbF levels and disease severity in β-thalassemia and SCA. Previous studies in SCA, however, have been restricted to populations from the African diaspora, which include multiple genealogies. We have investigated the influence of these 3 loci on HbF levels in sickle cell patients from Tanzania and in a small group of African British sickle patients. All 3 loci have a significant impact on the trait in both patient groups. The results suggest the presence of HBS1L-MYB variants affecting HbF in patients who are not tracked well by European-derived markers, such as rs9399137. Additional loci may be identified through independent genome-wide association studies in African populations.
摘要
胎儿血红蛋白 (HbF, α(2)γ(2)) 是导致镰状细胞贫血 (SCA) 表型异质性显著的主要因素。在 3 个主要位点(11p 染色体上的 HBB 簇、6q 染色体上的 HBS1L-MYB 区域和 2p 染色体上的 BCL11A)的遗传变异已被证明会影响β-地中海贫血和 SCA 中的 HbF 水平和疾病严重程度。然而,以前在 SCA 中的研究仅限于来自非洲侨民的人群,其中包括多个谱系。我们研究了这 3 个位点对来自坦桑尼亚的镰状细胞患者和一小群非洲英国镰状细胞患者的 HbF 水平的影响。在这两个患者群体中,所有 3 个位点对该特征都有显著影响。结果表明,在不能很好地用欧洲衍生标记(如 rs9399137)追踪的患者中,存在影响 HbF 的 HBS1L-MYB 变体。通过在非洲人群中进行独立的全基因组关联研究,可能会发现其他位点。
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