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达菲趋化因子受体基因FY*B等位基因编码序列中的一种新突变与红细胞表型改变有关。

A novel mutation in the coding sequence of the FY*B allele of the Duffy chemokine receptor gene is associated with an altered erythrocyte phenotype.

作者信息

Parasol N, Reid M, Rios M, Castilho L, Harari I, Kosower N S

机构信息

Department of Human Genetics, Sackler School of Medicine, Tel-Aviv University, Tel Aviv, Israel.

出版信息

Blood. 1998 Oct 1;92(7):2237-43.

PMID:9746760
Abstract

The Duffy blood group system is of clinical and biological significance. Antibodies to Duffy antigens are responsible for some cases of transfusion incompatibility and newborn hemolytic disease. The Duffy protein is a receptor for the Plasmodium vivax erythrocyte-binding protein and is also a receptor for various chemokines (thus renamed Duffy Antigen Receptor for Chemokines [DARC]). The two Duffy polymorphic antigens, Fya and Fyb (coded by the FYA and FYB alleles), are present on erythrocyte membranes. The Fy(a-b-) phenotype is the predominant one in populations of black people and also occurs in other populations, including some non-Ashkenazi Jewish groups. The Fy(a-b-) phenotype has been associated with a mutation in the FYB promoter at the GATA box that abolishes the expression of erythrocyte Duffy protein. We describe here a novel mutation, present in the FYB coding sequence (271C --> T), that is associated with some Fy(b-) phenotypes among non-Ashkenazi Jews and among Brazilian blacks. The mutation is present in Fy(b-) individuals, who have wild-type FY*B GATA and carry the previously described 304G --> A substitution. The 271C --> T and 304G --> A can be identified by restriction enzyme-generated restriction fragment length polymorphisms. The 271C --> T substitution represents a considerable change in chemical nature (Arg91 --> Cys), one which may affect the antigenic determinants of DARC, and thus be of clinical significance. The mutation may have implications for some physiological roles of DARC and be of interest in malaria research and in studies of population genetics.

摘要

达菲血型系统具有临床和生物学意义。针对达菲抗原的抗体是导致某些输血不相容和新生儿溶血病病例的原因。达菲蛋白是间日疟原虫红细胞结合蛋白的受体,也是多种趋化因子的受体(因此重新命名为趋化因子达菲抗原受体 [DARC])。两种达菲多态性抗原,Fya 和 Fyb(由 FYA 和 FYB 等位基因编码)存在于红细胞膜上。Fy(a-b-) 表型在黑人人群中占主导地位,在其他人群中也有出现,包括一些非阿什肯纳兹犹太人群体。Fy(a-b-) 表型与 FYB 启动子在 GATA 框处的突变有关,该突变消除了红细胞达菲蛋白的表达。我们在此描述一种存在于 FYB 编码序列中的新突变(271C→T),它与非阿什肯纳兹犹太人和巴西黑人中的一些 Fy(b-) 表型相关。该突变存在于 Fy(b-) 个体中,这些个体具有野生型 FY*B GATA 并携带先前描述的 304G→A 替换。271C→T 和 304G→A 可以通过限制性内切酶产生的限制性片段长度多态性来鉴定。271C→T 替换代表化学性质的显著变化(Arg91→Cys),这可能会影响 DARC 的抗原决定簇,因此具有临床意义。该突变可能对 DARC 的某些生理作用有影响,在疟疾研究和群体遗传学研究中具有重要意义。

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A novel mutation in the coding sequence of the FY*B allele of the Duffy chemokine receptor gene is associated with an altered erythrocyte phenotype.达菲趋化因子受体基因FY*B等位基因编码序列中的一种新突变与红细胞表型改变有关。
Blood. 1998 Oct 1;92(7):2237-43.
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