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非洲裔美国人中的 DARC 等位基因和 Duffy 表型。

DARC alleles and Duffy phenotypes in African Americans.

机构信息

Department of Transfusion Medicine, Clinical Center and National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

Transfusion. 2012 Jun;52(6):1260-7. doi: 10.1111/j.1537-2995.2011.03431.x. Epub 2011 Nov 14.

Abstract

BACKGROUND

The DARC (Duffy blood group, chemokine receptor) gene encodes for a transmembrane glycoprotein that functions as a chemokine transporter, is a receptor for Plasmodium vivax and P. knowlesi, and expresses the Duffy blood group antigens (Fy). The Fy(a-b-) phenotype found in people of African descent is typically associated with a -67t>c mutation in the 5'-untranslated region (UTR), which prevents red blood cells being invaded by P. vivax and P. knowlesi. The aim of this study was to establish DARC allele frequencies in an African American blood donor cohort, determine a phylogenetic tree for DARC, and compare human and Neandertal DARC genes.

STUDY DESIGN AND METHODS

The DARC nucleotide sequence of 54 African American blood donors was determined from genomic DNA. Heterozygous substitutions were resolved by sequencing of haplotype-specific amplifications. A phylogenetic tree for DARC was established using the neighbor-joining method with Pan troglodytes as root.

RESULTS

A total of 108 haplotypes of the DARC gene could be unambiguously determined from nucleotide position -300 in the 5' UTR to +300 in the 3' UTR. Eleven different alleles were found, including the clinically relevant FYA, FYB, FYB-67C, FYB298A, and FY*X alleles. All phenotype predictions based on genotypes matched the serologically determined phenotypes exactly: 52% Fy(a-b-), 28% Fy(a-b+), and 20% Fy(a+b-).

CONCLUSIONS

The nucleotide sequencing approach using one amplicon is a practical genotyping method for DARC and allows the determination of haplotypes even in heterozygous constellations. We developed a phylogenetic tree for DARC alleles and postulated a distinct FY*B allele as ancestral for the extant DARC alleles in humans.

摘要

背景

DARC(达菲血型、趋化因子受体)基因编码一种跨膜糖蛋白,作为趋化因子转运蛋白,是间日疟原虫和疟原虫的受体,并表达达菲血型抗原(Fy)。非洲裔人群中发现的 Fy(a-b-)表型通常与 5'非翻译区(UTR)中的-67t>c 突变相关,该突变可防止间日疟原虫和疟原虫入侵红细胞。本研究旨在确定非裔美国献血者队列中的 DARC 等位基因频率,构建 DARC 系统发育树,并比较人类和尼安德特人 DARC 基因。

研究设计和方法

从基因组 DNA 中确定了 54 名非裔美国献血者的 DARC 核苷酸序列。通过对单倍型特异性扩增产物的测序来解决杂合子替换。使用邻接法建立 DARC 系统发育树,以 Pan troglodytes 为根。

结果

从 5'UTR 的-300 位核苷酸到 3'UTR 的+300 位核苷酸,可以明确确定 DARC 基因的 108 个单倍型。共发现 11 种不同的等位基因,包括临床上相关的 FYA、FYB、FYB-67C、FYB298A 和 FY*X 等位基因。所有基于基因型的表型预测与血清学确定的表型完全匹配:52%为 Fy(a-b-),28%为 Fy(a-b+),20%为 Fy(a+b-)。

结论

使用一个扩增子的核苷酸测序方法是 DARC 的一种实用基因分型方法,即使在杂合子构型中也可以确定单倍型。我们为 DARC 等位基因开发了一个系统发育树,并假设 FY*B 等位基因为人类现存 DARC 等位基因的祖先。

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