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Molecular mechanisms of chromosomal rearrangement during primate evolution.

机译:灵长类动物进化过程中染色体重排的分子机制。

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Breakpoint analysis of the large chromosomal rearrangements which have occurred during primate evolution promises to yield new insights into the underlying mechanisms of mutagenesis. Comparison of these evolutionary breakpoints with those that are disease-associated in humans, and which occur during either meiotic or mitotic cell division, should help to identify basic mechanistic similarities as well as differences. It has recently become clear that segmental duplications (SDs) have had a very significant impact on genome plasticity during primate evolution. In comparisons of the human and chimpanzee genomes, SDs have been found in flanking regions of 70-80% of inversions and approximately 40% of deletions/duplications. A strong spatial association between primate-specific breakpoints and SDs has also become evident from comparisons of human with other mammalian genomes. The lineage-specific hyperexpansion of certain SDs observed in the genomes of human, chimpanzee, gorilla and gibbon is indicative ofthe intrinsic instability of some SDs in primates. However, since many primate-specific breakpoints map to regions lacking SDs, but containing interspersed high-copy repetitive sequence elements such as SINEs, LINEs, LTRs, alpha-satellites and (AT)( n ) repeats, we may infer that a range of different molecular mechanisms have probably been involved in promoting chromosomal breakage during the evolution of primate genomes.
机译:灵长类动物进化过程中发生的大型染色体重排的断点分析有望对诱变的潜在机制产生新的见解。将这些进化断点与人类疾病相关的断点进行比较,这些断点发生在减数分裂或有丝分裂细胞分裂过程中,应该有助于确定基本的机制相似性和差异性。最近已经清楚的是,分段复制(SD)在灵长类动物进化过程中对基因组可塑性产生了非常重要的影响。在人类和黑猩猩基因组的比较中,在70%至80%倒置和大约40%缺失/重复的侧翼区域发现了SD。通过人类与其他哺乳动物基因组的比较,灵长类动物特异性断点和SD之间的强烈空间关联也变得显而易见。在人类,黑猩猩,大猩猩和长臂猿的基因组中观察到的某些SD的谱系特异性过度扩增表明灵长类动物中某些SD固有的不稳定性。但是,由于许多特定于灵长类的断点映射到缺少SD的区域,但包含散布的高复制重复序列元素,例如SINE,LINE,LTR,α卫星和(AT)(n)重复序列,我们可以推断出在灵长类动物基因组进化过程中,促进染色体断裂的分子机制可能不同。

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