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Dynamics of genome reorganization during human cardiogenesis reveal an RBM20-dependent splicing factory

机译:人类心脏发生过程中基因组重组的动力学揭示了一个依赖RBM20的剪接工厂

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摘要

Functional changes in spatial genome organization during human development are poorly understood. Here we report a comprehensive profile of nuclear dynamics during human cardiogenesis from pluripotent stem cells by integrating Hi-C, RNA-seq and ATAC-seq. While chromatin accessibility and gene expression show complex on/off dynamics, large-scale genome architecture changes are mostly unidirectional. Many large cardiac genes transition from a repressive to an active compartment during differentiation, coincident with upregulation. We identify a network of such gene loci that increase their association inter-chromosomally, and are targets of the muscle-specific splicing factor RBM20. Genome editing studies show that TTN pre-mRNA, the main RBM20-regulated transcript in the heart, nucleates RBM20 foci that drive spatial proximity between the TTN locus and other inter-chromosomal RBM20 targets such as CACNA1C and CAMK2D. This mechanism promotes RBM20-dependent alternative splicing of the resulting transcripts, indicating the existence of a cardiac-specific trans-interacting chromatin domain (TID) functioning as a splicing factory.
机译:人们对人类发展过程中空间基因组组织的功能变化知之甚少。在这里,我们通过整合Hi-C,RNA-seq和ATAC-seq报道了多能干细胞在人类心脏发生过程中核动力学的全面概况。虽然染色质的可及性和基因表达显示出复杂的开/关动态,但大规模的基因组架构变化大多是单向的。在分化过程中,许多大的心脏基因从抑制性转变为活动区室,与上调相吻合。我们确定这种基因位点的网络,增加其染色体间的关联,并且是肌肉特异性剪接因子RBM20的目标。基因组编辑研究表明,心脏中主要RBM20调控的转录本TTN pre-mRNA能够使RBM20焦点成核,从而推动TTN基因座与其他染色体间RBM20靶标(例如CACNA1C和CAMK2D)之间的空间接近。该机制促进了所得转录本的RBM20依赖性选择性剪接,表明存在心脏特异性反式相互作用染色质域(TID)作为剪接工厂。

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