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人类X染色体α卫星多态性结构域的分子分析。

Molecular analysis of a polymorphic domain of alpha satellite from the human X chromosome.

作者信息

Durfy S J, Willard H F

出版信息

Am J Hum Genet. 1987 Sep;41(3):391-401.

Abstract

Alpha satellite DNA, a diverse family of tandemly repeated DNA sequences located at the centromeric region of each human chromosome, is organized in a highly chromosome-specific manner and is characterized by a high frequency of restriction-fragment-length polymorphism. To examine events underlying the formation and spread of these polymorphisms within a tandem array, we have cloned and sequenced a representative copy of a polymorphic array from the X chromosome and compared this polymorphic copy with the predominant higher-order repeat form of X-linked alpha satellite. Sequence data indicate that the polymorphism arose by a single base mutation that created a new restriction site (for HindIII) in the sequence of the predominant repeat unit. This variant repeat unit, marked by the new HindIII site, was subsequently amplified in copy number to create a polymorphic domain consisting of approximately 500 copies of the variant repeat unit within the X-linked array of alpha satellite. We propose that a series of intrachromosomal recombination events between misaligned tandem arrays, involving multiple rounds of either unequal crossing-over or sequence conversion, facilitated the spread and fixation of this variant HindIII repeat unit.

摘要

α卫星DNA是位于每个人类染色体着丝粒区域的一个多样化的串联重复DNA序列家族,其组织方式具有高度的染色体特异性,并且具有高频的限制性片段长度多态性。为了研究这些多态性在串联阵列中形成和传播的潜在事件,我们克隆并测序了来自X染色体的一个多态性阵列的代表性拷贝,并将这个多态性拷贝与X连锁α卫星的主要高阶重复形式进行了比较。序列数据表明,该多态性是由一个单碱基突变产生的,该突变在主要重复单元的序列中创建了一个新的限制性位点(用于HindIII)。这个以新的HindIII位点为标记的变异重复单元随后在拷贝数上被扩增,从而在α卫星的X连锁阵列中创建了一个由大约500个变异重复单元拷贝组成的多态性结构域。我们提出,在未对齐的串联阵列之间发生的一系列染色体内重组事件,涉及多轮不等交换或序列转换,促进了这个变异HindIII重复单元的传播和固定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6368/1684182/4fb20deaaf70/ajhg00132-0068-a.jpg

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