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人类小卫星MS205(D16S309)的突变率异质性与等位基因多样性的产生

Mutation rate heterogeneity and the generation of allele diversity at the human minisatellite MS205 (D16S309).

作者信息

May C A, Jeffreys A J, Armour J A

机构信息

Department of Genetics, University of Leicester, UK.

出版信息

Hum Mol Genet. 1996 Nov;5(11):1823-33. doi: 10.1093/hmg/5.11.1823.

Abstract

Many tandemly repeated minisatellite loci display extreme levels of length variation as a consequence of high rates of spontaneous germline mutation altering repeat copy number. Direct screening for new allele lengths by small-pool PCR has shown that instability at the human minisatellite locus MS205 (D16S309) is largely germline specific and usually results in the gain or loss of just a few repeat units. Structural analysis of the order of variant repeats has shown that these events occur preferentially at one end of the tandem array and can result in complex rearrangements including the inter-allelic transfer of repeat units. In contrast, putative mutants recovered from somatic DNA occur at a substantially lower rate and are simple and non-polar in nature. Germline mutation rates vary considerably between alleles, consistent with regulation occurring in cis. Although examination of DNA sequence polymorphisms immediately flanking the minisatellite reveals no definitive associations with germline mutation rate variation, differences in rate may be paralleled by changes in mutation spectrum. These findings help to explain the diversity of MS205 allele structures in modern humans and suggest a common mutation pathway with some other minisatellites.

摘要

由于自发种系突变率高,改变重复拷贝数,许多串联重复的微卫星位点表现出极高的长度变异水平。通过小池PCR直接筛选新的等位基因长度表明,人类微卫星位点MS205(D16S309)的不稳定性在很大程度上是种系特异性的,通常只导致少数几个重复单元的增减。对变异重复序列顺序的结构分析表明,这些事件优先发生在串联阵列的一端,并可导致复杂的重排,包括重复单元的等位基因间转移。相比之下,从体细胞DNA中回收的推定突变体发生率要低得多,而且本质上是简单的、非极性的。种系突变率在不同等位基因之间差异很大,这与顺式调控一致。虽然对微卫星紧邻的DNA序列多态性的检查没有发现与种系突变率变异有明确的关联,但突变率的差异可能与突变谱的变化平行。这些发现有助于解释现代人类中MS205等位基因结构的多样性,并提示与其他一些微卫星有共同的突变途径。

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