A unique macrophage subpopulation signals directly to progenitor cells to 
promote regenerative neurogenesis in the zebrafish spinal cord

Cavone, Leonardo; McCann, Tess; Drake, Louisa K.; Aguzzi, Erika A.; Oprisoreanu, Ana-Maria; Pedersen, Elisa; Sandi, Soe; Selvarajah, Jathurshan; Tsarouchas, Themistoklis M.; Wehner, Daniel; Keatinge, Marcus; Mysiak, Karolina S.; Henderson, Beth E. P.; Dobie, Ross; Henderson, Neil C.; Becker, Thomas; Becker, Catherina G.

doi:10.1016/j.devcel.2021.04.031

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A unique macrophage subpopulation signals directly to progenitor cells to promote regenerative neurogenesis in the zebrafish spinal cord

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Wehner, Daniel
Wehner Research Group, Guck Division, Max Planck Institute for the Science of Light, Max Planck Society;
Max-Planck-Zentrum für Physik und Medizin, Max Planck Institute for the Science of Light, Max Planck Society;
University of Edinburgh;

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Cavone, L., McCann, T., Drake, L. K., Aguzzi, E. A., Oprisoreanu, A.-M., Pedersen, E., et al. (2021). A unique macrophage subpopulation signals directly to progenitor cells to promote regenerative neurogenesis in the zebrafish spinal cord. Developmental Cell, 56(11), 1617-+. doi:10.1016/j.devcel.2021.04.031.

Zitierlink: https://hdl.handle.net/21.11116/0000-0009-ACDF-B

Zusammenfassung

Central nervous system injury re-initiates neurogenesis in anamniotes (amphibians and fishes), but not in mammals. Activation of the innate immune system promotes regenerative neurogenesis, but it is fundamentally unknown whether this is indirect through the activation of known developmental signaling pathways or whether immune cells directly signal to progenitor cells using mechanisms that are unique to regeneration. Using single-cell RNA-seq of progenitor cells and macrophages, as well as cell-type-specific manipulations, we provide evidence for a direct signaling axis from specific lesion-activated macrophages to spinal progenitor cells to promote regenerative neurogenesis in zebrafish. Mechanistically, TNFa from pro-regenerative macrophages induces Tnfrsf1a-mediated AP-1 activity in progenitors to increase regeneration-promoting expression of hdac1 and neurogenesis. This establishes the principle that macrophages directly communicate to spinal progenitor cells via non-developmental signals after injury, providing potential targets for future interventions in the regeneration-deficient spinal cord of mammals.