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Genome Resequencing Reveals Congenital Causes of Embryo and Nestling Death in Crested Ibis (Nipponia nippon)

机译:基因组重排揭示了朱I(Nipponia nippon)的胚胎和雏鸟死亡的先天原因。

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摘要

The crested ibis (Nipponia nippon) is endangered worldwide. Although a series of conservation measures have markedly increased the population size and distribution area of these birds, the high mortality of embryos and nestlings considerably decreases the survival potential of this bird species. High-throughput sequencing technology was utilized to compare whole genomes between ten samples from dead crested ibises (including six dead embryos and four dead nestlings aged 0–45 days) and 32 samples from living birds. The results indicated that the dead samples all shared the genetic background of a specific ancestral subpopulation. Furthermore, the dead individuals were less genetically diverse and suffered higher degrees of inbreeding compared with these measures in live birds. Several candidate genes (KLHL3, SETDB2, TNNT2, PKP1, AK1, and EXOSC3) associated with detrimental diseases were identified in the genomic regions that differed between the alive and dead samples, which are likely responsible for the death of embryos and nestlings. In addition, in these regions, we also found several genes involved in the protein catabolic process (UBE4A and LONP1), lipid metabolism (ACOT1), glycan biosynthesis and metabolism (HYAL1 and HYAL4), and the immune system (JAM2) that are likely to promote the normal development of embryos and nestlings. The aberrant conditions of these genes and biological processes may contribute to the death of embryos and nestlings. Our data identify congenital factors underlying the death of embryos and nestlings at the whole genome level, which may be useful toward informing more effective conservation efforts for this bird species.
机译:凤头宜必思(Nipponia nippon)在世界范围内受到威胁。尽管一系列的保护措施显着增加了这些鸟类的种群规模和分布面积,但是胚胎和雏鸟的高死亡率大大降低了该鸟类的生存潜力。利用高通量测序技术比较了十只死有冠朱鹭的样本(包括六个死胚和四个0-45日龄的死雏)和整个活禽的32个样本的完整基因组。结果表明,死样品均具有特定祖先亚群的遗传背景。此外,与活禽相比,这些死者的遗传多样性较少,近交程度更高。在活样品和死样品之间存在差异的基因组区域中,鉴定了与有害疾病相关的几个候选基因(KLHL3,SETDB2,TNNT2,PKP1,AK1和EXOSC3),这很可能是造成胚胎和雏鸟死亡的原因。此外,在这些区域中,我们还发现了可能与蛋白质分解代谢过程(UBE4A和LONP1),脂质代谢(ACOT1),聚糖生物合成和代谢(HYAL1和HYAL4)以及免疫系统(JAM2)有关的几个基因。促进胚胎和雏鸟的正常发育。这些基因和生物学过程的异常状况可能导致胚胎和雏鸟的死亡。我们的数据确定了在整个基因组水平上导致胚胎和雏鸟死亡的先天因素,这可能有助于为该鸟类提供更有效的保护方法。

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