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对北美黑人和白人家庭中与囊性纤维化基因座相关的DNA多态性单倍型的分析支持囊性纤维化基因存在多种突变。

Analysis of DNA polymorphism haplotypes linked to the cystic fibrosis locus in North American black and Caucasian families supports the existence of multiple mutations of the cystic fibrosis gene.

作者信息

Cutting G R, Antonarakis S E, Buetow K H, Kasch L M, Rosenstein B J, Kazazian H H

机构信息

Department of Pediatrics, Johns Hopkins University School of Medicine, Baltimore, MD.

出版信息

Am J Hum Genet. 1989 Mar;44(3):307-18.

Abstract

Strong linkage disequilibrium (LD) was found between DNA marker XV2c and the cystic fibrosis (CF) locus (delta = 0.46) and between DNA marker KM19 and CF (delta = 0.67) in 157 CF and 138 normal chromosomes from U.S. Caucasians. DNA haplotypes with nine polymorphic sites were created in 54 Caucasian families. There is a strong LD between the haplotypes and the presence of the mutant CF genes. This implies that the DNA polymorphisms examined are close to the CF gene and that one mutation of the CF gene predominates in the Caucasian population. Haplotype analysis can also be used to refine estimates of CF carrier risk in Caucasians. Data for XV2c and MET markers in 16 American black patients and their families revealed a different haplotype distribution and LD pattern with the CF locus. These data suggest that racial admixture alone does not explain the occurrence of CF in American blacks and that multiple alleles of the CF gene may exist in this population.

摘要

在美国白人的157条囊性纤维化(CF)染色体和138条正常染色体中,发现DNA标记XV2c与CF位点之间存在强连锁不平衡(LD,δ=0.46),以及DNA标记KM19与CF之间存在强连锁不平衡(δ=0.67)。在54个白人家庭中构建了具有9个多态性位点的DNA单倍型。单倍型与突变CF基因的存在之间存在强连锁不平衡。这意味着所检测的DNA多态性与CF基因接近,并且CF基因的一种突变在白人群体中占主导地位。单倍型分析还可用于完善对白人群体中CF携带者风险的估计。16名美国黑人患者及其家族中XV2c和MET标记的数据显示,其与CF位点的单倍型分布和连锁不平衡模式不同。这些数据表明,仅种族混合并不能解释美国黑人中CF的发生,并且该群体中可能存在CF基因的多个等位基因。

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