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GAA重复序列的起源与不稳定性:来自Alu元件的见解

Origin and instability of GAA repeats: insights from Alu elements.

作者信息

Chauhan Chitra, Dash Debasis, Grover Deepak, Rajamani Jaya, Mukerji Mitali

机构信息

Functional Genomics Unit, Centre for Biochemical Technology (CSIR), Delhi University Campus, Mall Road, Delhi-110007, India.

出版信息

J Biomol Struct Dyn. 2002 Oct;20(2):253-63. doi: 10.1080/07391102.2002.10506841.

Abstract

Expansion of GAA repeats in the intron of the frataxin gene is involved in the autosomal recessive Friedreich's ataxia (FRDA). The GAA repeats arise from a stretch of adenine residues of an Alu element. These repeats have a size ranging from 7- 38 in the normal population, and expand to thousands in the affected individuals. The mechanism of origin of GAA repeats, their polymorphism and stability are not well understood. In this study, we have carried out an extensive analysis of GAA repeats at several loci in the humans. This analysis indicates the association of a majority of GAA repeats with the 3' end of an "A" stretch present in the Alu repeats. Further, the prevalence of GAA repeats correlates with the evolutionary age of Alu subfamilies as well as with their relative frequency in the genome. Our study on GAA repeat polymorphism at some loci in the normal population reveals that the length of the GAA repeats is determined by the relative length of the flanking A stretch. Based on these observations, a possible mechanism for origin of GAA repeats and modulatory effects of flanking sequences on repeat instability mediated by DNA triplex is proposed.

摘要

弗里德赖希共济失调(FRDA)是一种常染色体隐性疾病,其发病与位于frataxin基因内含子中的GAA重复序列的扩增有关。GAA重复序列源自Alu元件的一段腺嘌呤残基。在正常人群中,这些重复序列的长度为7至38个,而在患病个体中则会扩增至数千个。目前,GAA重复序列的起源机制、多态性及稳定性仍未完全明确。在本研究中,我们对人类多个位点的GAA重复序列进行了深入分析。分析结果表明,大部分GAA重复序列与Alu重复序列中“A”链的3'端相关。此外,GAA重复序列的出现频率与Alu亚家族的进化年龄及其在基因组中的相对频率相关。我们对正常人群中某些位点的GAA重复序列多态性研究发现,GAA重复序列的长度由侧翼A链的相对长度决定。基于这些观察结果,我们提出了一种GAA重复序列的可能起源机制,以及侧翼序列对由DNA三链体介导的重复序列不稳定性的调节作用。

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