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首页> 外文期刊>PLoS Genetics >Meiosis reveals the early steps in the evolution of a neo-XY sex chromosome pair in the African pygmy mouse Mus minutoides
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Meiosis reveals the early steps in the evolution of a neo-XY sex chromosome pair in the African pygmy mouse Mus minutoides

机译:Meiosis揭示了非洲侏儒小鼠的新XY性染色体对的演变的早期步骤<斜体> MUS minutoides

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Sex chromosomes of eutherian mammals are highly different in size and gene content, and share only a small region of homology (pseudoautosomal region, PAR). They are thought to have evolved through an addition-attrition cycle involving the addition of autosomal segments to sex chromosomes and their subsequent differentiation. The events that drive this process are difficult to investigate because sex chromosomes in almost all mammals are at a very advanced stage of differentiation. Here, we have taken advantage of a recent translocation of an autosome to both sex chromosomes in the African pygmy mouse Mus minutoides , which has restored a large segment of homology (neo-PAR). By studying meiotic sex chromosome behavior and identifying fully sex-linked genetic markers in the neo-PAR, we demonstrate that this region shows unequivocal signs of early sex-differentiation. First, synapsis and resolution of DNA damage intermediates are delayed in the neo-PAR during meiosis. Second, recombination is suppressed or largely reduced in a large portion of the neo-PAR. However, the inactivation process that characterizes sex chromosomes during meiosis does not extend to this region. Finally, the sex chromosomes show a dual mechanism of association at metaphase-I that involves the formation of a chiasma in the neo-PAR and the preservation of an ancestral achiasmate mode of association in the non-homologous segments. We show that the study of meiosis is crucial to apprehend the onset of sex chromosome differentiation, as it introduces structural and functional constrains to sex chromosome evolution. Synapsis and DNA repair dynamics are the first processes affected in the incipient differentiation of X and Y chromosomes, and they may be involved in accelerating their evolution. This provides one of the very first reports of early steps in neo-sex chromosome differentiation in mammals, and for the first time a cellular framework for the addition-attrition model of sex chromosome evolution.
机译:Eutherian哺乳动物的性染色体在大小和基因含量方面具有高度不同,并且仅为一小部分同源性(伪染色体区域,PAR)。他们被认为通过添加蒸馏周期来演变,涉及向性染色体添加常染色体细分和它们随后的分化。驱动此过程的事件难以调查,因为几乎所有哺乳动物中的性染色体都是非常先进的分化阶段。在这里,我们利用了最近对非洲侏儒小鼠Mus Minutoides中的性染色体进行了最近的易于迁移,这已经恢复了大量的同源性(Neo-Par)。通过研究Meiotic性别染色体行为并在新靶中鉴定完全性别联系的遗传标记,我们证明该地区显示出早期性别分化的明确症状。首先,DNA损伤中间体的突触和分辨率被延迟在MeIosis期间的新靶。其次,在新靶的大部分中,抑制重组或大幅下降。然而,在减数分裂中表征性染色体的灭活过程并未延伸到该区域。最后,性染色体显示了在中磷脂 - I的结合的双重机制,涉及在非同源区段中的新靶中的形成和保存祖先治疗的祖先治疗模式。我们表明,减数分裂的研究至关重要,以逮捕性染色体分化的发作,因为它引入了性染色体演化的结构和功能。 Synapsis和DNA修复动态是在X和Y染色体的初期分化中影响的第一个过程,它们可能参与加速其进化。这提供了哺乳动物中新性染色体分化的早期步骤的第一报告之一,并且首次进行性染色体演化的附加磨损模型的蜂窝框架。

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