Single-cell transcriptomics identifies conserved regulators of neuroglandular lineages.

Cell Rep

Department of Neurosciences and Developmental Biology, Faculty of Life Sciences, University of Vienna, 1030 Vienna, Austria; Max-Perutz Labs, Dr.-Bohr-Gasse 9, 1030 Vienna, Austria; Research Platform "SinCeReSt: Single Cell Regulation of Stem Cells, " University of Vienna, 1030 Vienna, Austria. Electronic address:

Published: September 2022

Communication in bilaterian nervous systems is mediated by electrical and secreted signals; however, the evolutionary origin and relation of neurons to other secretory cell types has not been elucidated. Here, we use developmental single-cell RNA sequencing in the cnidarian Nematostella vectensis, representing an early evolutionary lineage with a simple nervous system. Validated by transgenics, we demonstrate that neurons, stinging cells, and gland cells arise from a common multipotent progenitor population. We identify the conserved transcription factor gene SoxC as a key upstream regulator of all neuroglandular lineages and demonstrate that SoxC knockdown eliminates both neuronal and secretory cell types. While in vertebrates and many other bilaterians neurogenesis is largely restricted to early developmental stages, we show that in the sea anemone, differentiation of neuroglandular cells is maintained throughout all life stages, and follows the same molecular trajectories from embryo to adulthood, ensuring lifelong homeostasis of neuroglandular cell lineages.

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Source
http://dx.doi.org/10.1016/j.celrep.2022.111370DOI Listing

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