首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Molecular and population genetic analysis of allelicsequence diversity at the human beta-globin locus.
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Molecular and population genetic analysis of allelicsequence diversity at the human beta-globin locus.

机译:等位基因的分子和群体遗传分析人类β-珠蛋白基因座的序列多样性。

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摘要

Allelic sequence polymorphism at the beta-globin locus was investigated in a group of 36 Melanesians. A 3-kilobase fragment containing the gene and its flanking regions was sequenced in 60 normal (beta A) and 12 thalassemic (intron 1, position 5, G-->C) chromosomes. Haplotype relationships between linked polymorphisms were derived by allele-specific PCR amplification and sequencing. Seventeen nucleotide polymorphisms and 2 length variants were identified, and these sites segregated as 17 sequence haplotypes in the normal chromosomes. This haplotype diversity is higher than that expected on the basis of the nucleotide polymorphism observed and is probably due to recombination and gene conversion. Nucleotide diversity at synonymous sites in the sample is 0.14%, suggesting an average age of sequence divergence of approximately 450,000 years, consistent with that expected for a neutrally evolving human nuclear locus.
机译:在一组36个Melanesians中研究了β-珠蛋白基因座的等位基因序列多态性。在60条正常(beta A)和12条地中海贫血(内含子1,位置5,G-> C)染色体中对包含该基因及其侧翼区域的3-kilobase片段进行了测序。连锁多态性之间的单倍型关系是通过等位基因特异性PCR扩增和测序得出的。鉴定出17个核苷酸多态性和2个长度变异,这些位点在正常染色体中被分离为17个序列单倍型。该单倍型多样性高于根据观察到的核苷酸多态性所预期的多样性,可能是由于重组和基因转化。样本中同义位点的核苷酸多样性为0.14%,表明序列差异的平均年龄约为450,000年,与预期的中性进化人类核基因座一致。

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