首页> 外文期刊>Croatian medical journal >Y-chromosome short tandem repeat intermediate variant alleles DYS392.2, DYS449.2, and DYS385.2 delineate new phylogenetic substructure in human Y-chromosome haplogroup tree.
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Y-chromosome short tandem repeat intermediate variant alleles DYS392.2, DYS449.2, and DYS385.2 delineate new phylogenetic substructure in human Y-chromosome haplogroup tree.

机译:Y染色体短串联重复中间变异等位基因DYS392.2,DYS449.2和DYS385.2描绘了人Y染色体单倍群树中的新系统发育亚结构。

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AIM: To determine the human Y-chromosome haplogroup backgrounds of intermediate-sized variant alleles displayed by short tandem repeat (STR) loci DYS392, DYS449, and DYS385, and to evaluate the potential of each intermediate variant to elucidate new phylogenetic substructure within the human Y-chromosome haplogroup tree. METHODS: Molecular characterization of lineages was achieved using a combination of Y-chromosome haplogroup defining binary polymorphisms and up to 37 short tandem repeat loci. DNA sequencing and median-joining network analyses were used to evaluate Y-chromosome lineages displaying intermediate variant alleles. RESULTS: We show that DYS392.2 occurs on a single haplogroup background, specifically I1*-M253, and likely represents a new phylogenetic subdivision in this European haplogroup. Intermediate variants DYS449.2 and DYS385.2 both occur on multiple haplogroup backgrounds, and when evaluated within specific haplogroup contexts, delineate new phylogenetic substructure, with DYS449.2 being informative within haplogroup A-P97 and DYS385.2 in haplogroups D-M145, E1b1a-M2, and R1b*-M343. Sequence analysis of variant alleles observed within the various haplogroup backgrounds showed that the nature of the intermediate variant differed, confirming the mutations arose independently. CONCLUSIONS: Y-chromosome short tandem repeat intermediate variant alleles, while relatively rare, typically occur on multiple haplogroup backgrounds. This distribution indicates that such mutations arise at a rate generally intermediate to those of binary markers and STR loci. As a result, intermediate-sized Y-STR variants can reveal phylogenetic substructure within the Y-chromosome phylogeny not currently detected by either binary or Y-STR markers alone, but only when such variants are evaluated within a haplogroup context.
机译:目的:确定由短串联重复序列(STR)位点DYS392,DYS449和DYS385显示的中等大小变异等位基因的人Y染色体单倍体背景,并评估每种中间变异体阐明人体内新的系统发生亚结构的潜力Y染色体单倍群树。方法:谱系的分子表征是使用Y染色体单倍群定义二进制多态性和最多37个短串联重复基因座的组合来实现的。 DNA测序和中位连接网络分析用于评估显示中间变异等位基因的Y染色体谱系。结果:我们显示DYS392.2发生在单个单倍群背景下,特别是I1 * -M253,并且可能代表了该欧洲单倍群中的一个新的系统发育细分。中间变体DYS449.2和DYS385.2都出现在多个单倍群背景上,并且在特定单倍群背景下进行评估时,描绘出了新的系统发育亚结构,其中DYS449.2在单倍群A-P97和DYS385.2中对单倍群D-M145具有参考意义, E1b1a-M2和R1b * -M343。在各种单倍体背景下观察到的变异等位基因的序列分析表明,中间变异的性质不同,从而证实了突变是独立发生的。结论:Y染色体短串联重复序列中间变异等位基因虽然相对罕见,但通常发生在多个单倍体背景上。这种分布表明这种突变通常以比二元标记和STR基因座的突变率中等的速率出现。结果,中等大小的Y-STR变体可以揭示Y染色体系统发育内的系统发育亚结构,目前尚不能单独通过二进制或Y-STR标记检测到,但仅当在单倍群环境中评估此类变体时才可以。

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