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果蝇 Y 染色体到常染色体基因复制的分子进化。

Molecular evolution of a Y chromosome to autosome gene duplication in Drosophila.

机构信息

Department of Genetics, University of Georgia, GA, USA.

出版信息

Mol Biol Evol. 2011 Mar;28(3):1293-306. doi: 10.1093/molbev/msq334. Epub 2010 Dec 16.

Abstract

In contrast to the rest of the genome, the Y chromosome is restricted to males and lacks recombination. As a result, Y chromosomes are unable to respond efficiently to selection, and newly formed Y chromosomes degenerate until few genes remain. The rapid loss of genes from newly formed Y chromosomes has been well studied, but gene loss from highly degenerate Y chromosomes has only recently received attention. Here, we identify and characterize a Y to autosome duplication of the male fertility gene kl-5 that occurred during the evolution of the testacea group species of Drosophila. The duplication was likely DNA based, as other Y-linked genes remain on the Y chromosome, the locations of introns are conserved, and expression analyses suggest that regulatory elements remain linked. Genetic mapping reveals that the autosomal copy of kl-5 resides on the dot chromosome, a tiny autosome with strongly suppressed recombination. Molecular evolutionary analyses show that autosomal copies of kl-5 have reduced polymorphism and little recombination. Importantly, the rate of protein evolution of kl-5 has increased significantly in lineages where it is on the dot versus Y linked. Further analyses suggest this pattern is a consequence of relaxed purifying selection, rather than adaptive evolution. Thus, although the initial fixation of the kl-5 duplication may have been advantageous, slightly deleterious mutations have accumulated in the dot-linked copies of kl-5 faster than in the Y-linked copies. Because the dot chromosome contains seven times more genes than the Y and is exposed to selection in both males and females, these results suggest that the dot suffers the deleterious effects of genetic linkage to more selective targets compared with the Y chromosome. Thus, a highly degenerate Y chromosome may not be the worst environment in the genome, as is generally thought, but may in fact be protected from the accumulation of deleterious mutations relative to other nonrecombining regions that contain more genes.

摘要

与基因组的其他部分相比,Y 染色体仅限于男性,并且缺乏重组。因此,Y 染色体无法有效地响应选择,新形成的 Y 染色体退化,直到只剩下少数基因。新形成的 Y 染色体的基因快速丢失已经得到了很好的研究,但高度退化的 Y 染色体的基因丢失最近才受到关注。在这里,我们鉴定并表征了一个在果蝇的 testacea 组物种的演化过程中发生的雄性生育基因 kl-5 的 Y 到常染色体的复制。该复制很可能是基于 DNA 的,因为其他 Y 连锁基因仍然存在于 Y 染色体上,内含子的位置是保守的,并且表达分析表明调节元件仍然是连锁的。遗传图谱显示,kl-5 的常染色体副本位于点染色体上,点染色体是一个具有强烈抑制重组的微小常染色体。分子进化分析表明,kl-5 的常染色体副本的多态性降低,重组很少。重要的是,kl-5 的蛋白质进化率在其位于点染色体而非 Y 染色体的谱系中显著增加。进一步的分析表明,这种模式是由于纯化选择放松而不是适应性进化的结果。因此,尽管 kl-5 重复的最初固定可能是有利的,但在点染色体连接的 kl-5 副本中积累的稍微有害的突变比在 Y 染色体连接的 kl-5 副本中更快。由于点染色体包含的基因是 Y 染色体的七倍,并且在雄性和雌性中都受到选择,因此这些结果表明,与 Y 染色体相比,点染色体受到遗传连锁到更多选择性靶标的有害影响。因此,高度退化的 Y 染色体可能不是基因组中最糟糕的环境,这与普遍的看法相反,但实际上可能受到保护,免受有害突变的积累,而其他非重组区域包含更多的基因。

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