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剖析非贫血个体中β-珠蛋白基因簇的两个多态性与F细胞数量变化之间的关联状况。

Dissection of the association status of two polymorphisms in the beta-globin gene cluster with variations in F-cell number in non-anemic individuals.

作者信息

Merghoub T, Perichon B, Maier-Redelsperger M, Dibenedetto S P, Samperi P, Ducrocq R, Feingold N, Elion J, Schiliro G, Labie D, Krishnamoorthy R

机构信息

INSERM U 458, Hôpital Robert Debré, Paris, France.

出版信息

Am J Hematol. 1997 Dec;56(4):239-43. doi: 10.1002/(sici)1096-8652(199712)56:4<239::aid-ajh7>3.0.co;2-y.

Abstract

Expression of fetal hemoglobin (Hb F) is under polygenic control involving determinants both linked and unlinked to the beta-globin gene cluster on chromosome 11. Variations in the DNase I-hypersensitive site 2 of the locus control region (LCR-HS2) and a C --> T change at position -158 from the Ggamma-gene (detected as an XmnI polymorphism) correlate with the high level of Hb F expression in patients with sickle-cell anemia and beta-thalassemia. Interpretation of data under these conditions of anemic stress is difficult because the preferential survival of Hb F-containing erythrocytes (F-cells) may not reflect the true status of Hb F expression. We investigated the relationship between these markers and Hb F expression in terms of F-cell levels in 48 unrelated non-anemic AS heterozygotes from Sicily. The betaS-chromosome of all these individuals was of the Benin haplotype and they differed only by their betaA chromosomes. We demonstrate that F-cell expression is more strongly associated with LCR-HS2 polymorphism than with XmnI polymorphism. The observed association between XmnI polymorphism and Hb F expression is very likely to be due to linkage disequilibrium with LCR-HS2 sequences.

摘要

胎儿血红蛋白(Hb F)的表达受多基因控制,涉及与11号染色体上β珠蛋白基因簇连锁和不连锁的决定因素。位点控制区(LCR-HS2)的DNA酶I高敏位点2的变异以及Gγ基因-158位的C→T变化(检测为XmnI多态性)与镰状细胞贫血和β地中海贫血患者的高水平Hb F表达相关。在这些贫血应激条件下对数据进行解释很困难,因为含Hb F的红细胞(F细胞)的优先存活可能无法反映Hb F表达的真实状态。我们根据来自西西里岛的48名无亲缘关系的非贫血AS杂合子的F细胞水平,研究了这些标志物与Hb F表达之间的关系。所有这些个体的βS染色体均为贝宁单倍型,它们之间的差异仅在于其βA染色体。我们证明,F细胞表达与LCR-HS2多态性的相关性比与XmnI多态性的相关性更强。观察到的XmnI多态性与Hb F表达之间的关联很可能是由于与LCR-HS2序列的连锁不平衡所致。

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