生物
器官发生
胚胎
细胞生物学
计算生物学
遗传学
基因
作者
Peng Xie,Juan Shen,Yi Yang,Xinrui Wang,Wei Liu,Hailong Cao,Yanying Zheng,Chen Wu,Guangyao Mao,Linjin Chen,Jingjing He,Weiheng Zheng,Zehong Yang,Xiao Zhang,Xu Jiang,Xianfa Yang,Ke Fang,Yan Liu,Xin Xue,Xueting Chen
出处
期刊:Cell
[Elsevier]
日期:2025-06-18
卷期号:188 (17): 4754-4772.e18
被引量:5
标识
DOI:10.1016/j.cell.2025.05.035
摘要
Early organogenesis is a crucial stage in embryonic development, characterized by extensive cell fate specification to initiate organ formation but also by a high susceptibility to developmental defects. Here, we profiled 285 serial sections from six E7.5-E8.0 embryos to generate full spatiotemporal transcriptome and signal maps during early organogenesis at single-cell resolution. By developing SEU-3D, we reconstructed digital embryos, enabling investigation of regionalized gene expression in the native spatial context. We established a space-informed gene-cell co-embedding approach, systematically characterized the spatial atlas of endoderm and mesoderm derivatives, and elucidated signaling networks across germ layers and cell types. Furthermore, we characterized a primordium determination zone (PDZ) formed along the anterior embryonic-extraembryonic interface at E7.75, and it revealed that the coordinated signaling communications contribute to the formation of cardiac primordium. Collectively, the high-resolution "digital embryo" provides significant insights into early organogenesis and a unique spatial platform for studying development and diseases.
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