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Epigenetic conflict on a degenerating Y chromosome increases mutational burden in Drosophila males

机译:在退化Y染色体上的表观遗传冲突增加了果蝇男性的突变负担

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Large portions of eukaryotic genomes consist of transposable elements (TEs), and the establishment of transcription-repressing heterochromatin during early development safeguards genome integrity in Drosophila. Repeat-rich Y chromosomes can act as reservoirs for TEs (‘toxic’ Y effect), and incomplete epigenomic defenses during early development can lead to deleterious TE mobilization. Here, we contrast the dynamics of early TE activation in two Drosophila species with vastly different Y chromosomes of different ages. Zygotic TE expression is elevated in male embryos relative to females in both species, mostly due to expression of Y-linked TEs. Interestingly, male-biased TE expression diminishes across development in D. pseudoobscura, but remains elevated in D. miranda, the species with the younger and larger Y chromosome. The repeat-rich Y of D. miranda still contains many actively transcribed genes, which compromise the formation of silencing heterochromatin. Elevated TE expression results in more de novo insertions of repeats in males compared to females. This lends support to the idea that the ‘toxic’ Y chromosome can create a mutational burden in males when genome-wide defense mechanisms are compromised, and suggests a previously unappreciated epigenetic conflict on evolving Y chromosomes between transcription of essential genes and silencing of selfish DNA. Selfish DNA such as transposable elements cause intragenomic conflict. This study finds that on an evolutionarily young, gene-rich Drosophila Y chromosome, transposable elements evade heterochromatic suppression, leading to elevated transposition rates in males.
机译:大量的真核基因组包括可转换元素(TES),以及在早期发展期间的转录抑制异料素的建立保障在果蝇中的基因组完整性。重复的Y染色体可以充当TES的储层('毒性'Y效应),早期发展期间的异心性防御都可能导致有害的TE动员。在这里,我们将早期TE激活的动态与不同年龄不同的y染色体造影。在两种物种中相对于雌性的雄性胚胎中抬高了ZygoticTe表达,主要是由于Y键的表达。有趣的是,男性偏见的TE表达在D.伪佛教的发展中减少,但在米兰达的D. Miranda,患者和较大的Y染色体的物种仍然升高。 D. Miranda的重复富y仍然包含许多积极转录的基因,这损害了沉默的异铬胺的形成。与女性相比,高升高的TE表达导致更新的雌性重复的插入。这对“有毒”y染色体可以在损害基因组的防御机制时造成“毒性”y染色体可以在雄性中造成突变负担,并提出了以前未被未被覆富的表观遗传冲突,以便在基本基因转录与自私DNA的沉默之间的发展y染色体。自私DNA,如转置元素导致肿瘤内的冲突。本研究发现,在进化的幼小基因富含果蝇Y染色体上,转换元素逃避异形抑制,导致雄性的升高率升高。

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