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GENOMIC IMPRINTING DISRUPTED PLACENTAL EXPRESSION AND SPECIATION

机译:基因组印迹胎盘表达异常和特异性

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摘要

The importance of regulatory incompatibilities to the early stages of speciation remains unclear. Hybrid mammals often show extreme parent-of-origin growth effects that are thought to be a consequence of disrupted genetic imprinting (parent-specific epigenetic gene silencing) during early development. Here we test the long-standing hypothesis that abnormal hybrid growth reflects disrupted gene expression due to loss of imprinting (LOI) in hybrid placentas, resulting in dosage imbalances between paternal growth factors and maternal growth repressors. We analyzed placental gene expression in reciprocal dwarf hamster hybrids that show extreme parent-of-origin growth effects relative to their parental species. In massively enlarged hybrid placentas, we observed both extensive transgressive expression of growth-related genes and bi-allelic expression of many genes that were paternally silenced in normal sized hybrids. However, the apparent widespread disruption of paternal silencing was coupled with reduced gene expression levels overall. These patterns are contrary to the predictions of the LOI model and indicate that hybrid misexpression of dosage sensitive genes is caused by other regulatory mechanisms in this system. Collectively, our results support a central role for disrupted gene expression and imprinting in the evolution of mammalian hybrid inviability, but call into question the generality of the widely invoked LOI model.
机译:监管不兼容对物种形成的早期阶段的重要性仍然不清楚。杂种哺乳动物通常表现出极高的父本起源生长效应,这被认为是早期发育过程中遗传烙印(父母特异性表观遗传基因沉默)受到破坏的结果。在这里,我们测试了一个长期存在的假说,即杂种生长异常反映了由于杂种胎盘中的印记(LOI)丢失而导致基因表达受到破坏,从而导致父本生长因子与母体生长抑制因子之间的剂量失衡。我们分析了相对矮矮的仓鼠杂种中的胎盘基因表达,这些杂种显示出相对于其亲本物种而言,极高的父本起源生长效应。在大规模扩大的杂种胎盘中,我们观察到了生长相关基因的大量过表达和许多在正常大小杂种中父本沉默的基因的双等位基因表达。但是,父亲沉默的明显广泛破坏与总体上基因表达水平的降低相结合。这些模式与LOI模型的预测相反,表明剂量敏感性基因的杂合错误表达是由该系统中的其他调控机制引起的。总的来说,我们的研究结果支持在哺乳动物杂种无性进化中破坏基因表达和印迹的重要作用,但令人质疑广泛使用的LOI模型的普遍性。

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