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Duplication, coclustering, and selection of human Alu retrotransposons

机译:人类Alu逆转座子的复制,共聚和选择

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Alu and L1 are families of non-LTR retrotransposons representing ≈30% of the human genome. Genomlc distributions of young Alu and L1 elements are quite similar, but over time, Alu densities in GC-rich DNA increase in comparison with L1 densities. Here we analyze two processes that may contribute to this phenomenon. First, DNA duplications in the human genome occur more frequently in Alu- and GC-rich than in AT-rich chromosomal regions. Second, most Alu elements tend to be coclustered with each other, but recently retroposed elements are likely to be inserted outside the existing clusters. These "stand-alone" elements appear to be rapidly eliminated from the genome. We also report that over time, the densities of recently retroposed Alu families on chromosome Y decline rapidly, whereas Alu densities on chromosome X increase relative to autosomal densities. We propose that these changes in the chromosomal proportions of Alu densities and the elimination of stand-alone Alus represent the same process of paternal Alu selection. We also propose that long-term Alu accumulation in GC-rich DNA is associated with DNA duplication initiated by elevated recombinogenic activities in Alu clusters.
机译:Alu和L1是非LTR逆转座子家族,占人类基因组的约30%。年轻的Alu和L1元素的基因组分布非常相似,但是随着时间的推移,富含GC的DNA中的Alu密度与L1密度相比会增加。在这里,我们分析可能导致这种现象的两个过程。首先,人类基因组中的DNA复制在富含Alu和GC的情况下比在富含AT的染色体区域中更常见。其次,大多数Alu元素倾向于相互聚集在一起,但是最近重新布置的元素很可能会插入现有簇的外部。这些“独立”元素似乎已从基因组中迅速消除。我们还报告说,随着时间的流逝,最近重新安置的Y染色体上的Alu家族的密度迅速下降,而X染色体上的Alu密度相对于常染色体密度而言却增加了。我们提出,Alu密度的染色体比例的这些变化和独立Alus的消除代表了父本Alu选择的相同过程。我们还提出,富含GC的DNA中长期的Alu积累与Alu簇中重组活动增强引起的DNA复制有关。

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