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人类17号染色体α卫星中缺失多态性的分子分析:同源不等交换及随后固定的证据

Molecular analysis of a deletion polymorphism in alpha satellite of human chromosome 17: evidence for homologous unequal crossing-over and subsequent fixation.

作者信息

Waye J S, Willard H F

出版信息

Nucleic Acids Res. 1986 Sep 11;14(17):6915-27. doi: 10.1093/nar/14.17.6915.

DOI:10.1093/nar/14.17.6915
PMID:3763396
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC311708/
Abstract

The human alpha satellite DNA family is organized into chromosome-specific subsets characterized by distinct higher-order repeats based on a approximately 171 basepair monomer unit. On human chromosome 17, the predominant form of alpha satellite is a 16-monomer (16-mer) higher-order repeat present in 500-1000 copies per chromosome 17. In addition, less abundant 15-monomer and 14-monomer repeats are also found constitutively on chromosome 17. Polymorphisms in the form of different higher-order repeat lengths have been described for this subset, the most prominent polymorphism being a 13-monomer (13-mer) higher-order repeat present on approximately 35% of all chromosomes 17. To investigate the nature of this polymorphism, we have cloned, sequenced and compared the relevant regions of the 13-mer to the previously characterized 16-mer repeat. The results show that the repeats are virtually identical, with the principal difference being the exclusion of three monomers from the 13-mer repeat. We propose that the 13-mer is the product of an isolated homologous recombination event between two monomers of the 16-mer repeat. Sequence comparisons reveal the approximate site of recombination and flanking regions of homology. This recombination site corresponds to a position within the alphoid monomer which has been previously implicated in an independent homologous recombination event, suggesting that there may exist a preferred register for recombination in alphoid DNA. We suggest that these events are representative of an ongoing process capable of reorganizing the satellite subset of a given chromosome, thereby contributing to the establishment of chromosome-specific alpha satellite subsets.

摘要

人类α卫星DNA家族被组织成特定于染色体的亚群,其特征是基于大约171个碱基对的单体单元具有独特的高阶重复序列。在人类17号染色体上,α卫星的主要形式是一种16聚体(16-mer)高阶重复序列,每条17号染色体上存在500 - 1000个拷贝。此外,在17号染色体上还组成性地发现了丰度较低的15聚体和14聚体重复序列。已经描述了该亚群中不同高阶重复长度形式的多态性,最显著的多态性是大约35%的所有17号染色体上存在的13聚体(13-mer)高阶重复序列。为了研究这种多态性的本质,我们克隆、测序并比较了13聚体的相关区域与先前表征的16聚体重复序列。结果表明,这些重复序列实际上是相同的,主要差异在于13聚体重复序列中排除了三个单体。我们提出13聚体是16聚体重复序列的两个单体之间孤立的同源重组事件的产物。序列比较揭示了重组的大致位点和同源侧翼区域。这个重组位点对应于α卫星单体中的一个位置,该位置先前已涉及一个独立的同源重组事件,这表明在α卫星DNA中可能存在一个优先的重组登记位点。我们认为这些事件代表了一个正在进行的过程,该过程能够重组给定染色体的卫星亚群,从而有助于建立特定于染色体的α卫星亚群。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9c2/311708/ba0b1a3480e0/nar00286-0149-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9c2/311708/b0bdc8fa3a2a/nar00286-0145-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9c2/311708/ba0b1a3480e0/nar00286-0149-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9c2/311708/b0bdc8fa3a2a/nar00286-0145-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9c2/311708/ba0b1a3480e0/nar00286-0149-a.jpg

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