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人类小卫星序列生殖系突变中的复杂基因转换事件。

Complex gene conversion events in germline mutation at human minisatellites.

作者信息

Jeffreys A J, Tamaki K, MacLeod A, Monckton D G, Neil D L, Armour J A

机构信息

Department of Genetics, University of Leicester, UK.

出版信息

Nat Genet. 1994 Feb;6(2):136-45. doi: 10.1038/ng0294-136.

Abstract

Mutation at the human minisatellites MS32, MS205 and MS31A has been investigated by characterizing mutant alleles in pedigrees and in the case of MS32 by direct analysis of mutant molecules in single sperm. Most mutations at all three loci are polar, involving the preferential gain of a few repeat units at one end of the tandem repeat array. Incoming repeats can be derived from the same allele or the homologous chromosome, through they are frequently rearranged during mutation. Lack of exchange of flanking markers suggests the involvement of complex conversion-like events in the generation of mutant alleles. At MS32, high frequency mutation processes in sperm appear to be largely germline specific and to occur at a constant rate irrespective of allele size. Together with mutational polarity, this implies that germline instability is controlled by elements outside the tandem repeat array.

摘要

通过对家系中的突变等位基因进行特征分析,以及对MS32通过直接分析单个精子中的突变分子,研究了人类小卫星MS32、MS205和MS31A的突变情况。在所有这三个位点上的大多数突变都是极性的,涉及串联重复序列阵列一端少数重复单元的优先增加。导入的重复序列可以来自相同的等位基因或同源染色体,尽管它们在突变过程中经常发生重排。侧翼标记缺乏交换表明在突变等位基因的产生过程中涉及复杂的类转换事件。在MS32,精子中的高频突变过程似乎在很大程度上是种系特异性的,并且无论等位基因大小如何都以恒定速率发生。与突变极性一起,这意味着种系不稳定性受串联重复序列阵列之外的元件控制。

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