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and models define a molecular signature reference for human embryonic notochordal cells. | LitMetric

Understanding the emergence of human notochordal cells (NC) is essential for the development of regenerative approaches. We present a comprehensive investigation into the specification and generation of NC using a straightforward pluripotent stem cell (PSC)-based system benchmarked with human fetal notochord. By integrating and transcriptomic data at single-cell resolution, we establish an extended molecular signature and overcome the limitations associated with studying human notochordal lineage at early developmental stages. We show that TGF-β inhibition enhances the yield and homogeneity of notochordal lineage commitment . Furthermore, this study characterizes regulators of cell-fate decision and matrisome enriched in the notochordal niche. Importantly, we identify specific cell-surface markers opening avenues for differentiation refinement, NC purification, and functional studies. Altogether, this study provides a human notochord transcriptomic reference that will serve as a resource for notochord identification in human systems, diseased-tissues modeling, and facilitating future biomedical research.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10865399PMC
http://dx.doi.org/10.1016/j.isci.2024.109018DOI Listing

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