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Hi-C 引导组装揭示了 X 和常染色体上保守的调控拓扑结构,尽管存在广泛的基因组重排。

Hi-C guided assemblies reveal conserved regulatory topologies on X and autosomes despite extensive genome shuffling.

机构信息

Max Planck Institute of Immunobiology and Epigenetics, 79108 Freiburg im Breisgau, Germany.

Faculty of Biology, University of Freiburg, 79104 Freiburg, Germany.

出版信息

Genes Dev. 2019 Nov 1;33(21-22):1591-1612. doi: 10.1101/gad.328971.119. Epub 2019 Oct 10.

Abstract

Genome rearrangements that occur during evolution impose major challenges on regulatory mechanisms that rely on three-dimensional genome architecture. Here, we developed a scaffolding algorithm and generated chromosome-length assemblies from Hi-C data for studying genome topology in three distantly related species. We observe extensive genome shuffling between these species with one synteny breakpoint after approximately every six genes. A/B compartments, a set of large gene-dense topologically associating domains (TADs), and spatial contacts between high-affinity sites (HAS) located on the X chromosome are maintained over 40 million years, indicating architectural conservation at various hierarchies. Evolutionary conserved genes cluster in the vicinity of HAS, while HAS locations appear evolutionarily flexible, thus uncoupling functional requirement of dosage compensation from individual positions on the linear X chromosome. Therefore, 3D architecture is preserved even in scenarios of thousands of rearrangements highlighting its relevance for essential processes such as dosage compensation of the X chromosome.

摘要

在进化过程中发生的基因组重排对依赖于三维基因组结构的调控机制提出了重大挑战。在这里,我们开发了一种支架算法,并从 Hi-C 数据中生成了染色体长度的组装,以研究三个远缘物种的基因组拓扑结构。我们观察到这些物种之间广泛的基因组重排,大约每六个基因就有一个同线性断点。A/B 区室、一组大型基因密集的拓扑关联结构域 (TAD),以及位于 X 染色体上的高亲和力位点 (HAS) 之间的空间接触,在 4000 多万年的时间里得以维持,表明在不同层次上存在结构保守性。进化保守基因簇在 HAS 附近聚集,而 HAS 位置似乎在进化上具有灵活性,从而将剂量补偿的功能需求与其在线性 X 染色体上的个别位置脱钩。因此,即使在数千次重排的情况下,三维结构也得以保留,突出了其在剂量补偿等重要过程中的相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aa56/6824461/f4befce11fc6/1591f01.jpg

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