We have generated a high-resolution Hi-C map of developing human retinal organoids to elucidate spatiotemporal dynamics of genomic architecture and its relationship with gene expression patterns. We demonstrate progressive stage-specific alterations in DNA topology and correlate these changes with transcription of cell-type-restricted gene markers during retinal differentiation. Temporal Hi-C reveals a shift toward A compartment for protein-coding genes and B compartment for non-coding RNAs, displaying high and low expression, respectively. Notably, retina-enriched genes are clustered near lost boundaries of topologically associated domains (TADs), and higher-order assemblages (i.e., TAD cliques) localize in active chromatin regions with binding sites for eye-field transcription factors. These genes gain chromatin contacts at their transcription start site as organoid differentiation proceeds. Our study provides a global view of chromatin architecture dynamics associated with diversification of cell types during retinal development and serves as a foundational resource for in-depth functional investigations of retinal developmental traits.
Stage-specific dynamic reorganization of genome topology shapes transcriptional neighborhoods in developing human retinal organoids.
发育中的人类视网膜类器官中,基因组拓扑结构的阶段特异性动态重组塑造了转录邻域
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作者:Qu Zepeng, Batz Zachary, Singh Nivedita, Marchal Claire, Swaroop Anand
| 期刊: | Cell Reports | 影响因子: | 6.900 |
| 时间: | 2023 | 起止号: | 2023 Dec 26; 42(12):113543 |
| doi: | 10.1016/j.celrep.2023.113543 | 种属: | Human |
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