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An In Vitro Human Segmentation Clock Model Derived from Embryonic Stem Cells

Cell Rep.. 2019; 
Chu LF1, Mamott D2, Ni Z3, Bacher R4, Liu C2, Swanson S2, Kendziorski C5, Stewart R2, Thomson JA6.
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摘要

Defects in somitogenesis result in vertebral malformations at birth known as spondylocostal dysostosis (SCDO). Somites are formed with a species-specific periodicity controlled by the "segmentation clock," which comprises a group of oscillatory genes in the presomitic mesoderm. Here, we report that a segmentation clock model derived from human embryonic stem cells shows many hallmarks of the mammalian segmentation clock in vivo, including a dependence on the NOTCH and WNT signaling pathways. The gene expression oscillations are highly synchronized, displaying a periodicity specific to the human clock. Introduction of a point of mutation into HES7, a specific mutation previously associated with clinical SCDO, e... More

关键词

HES7; gene oscillation; human embryonic stem cells; segmentation clock; spondylocostal dysostosis