par Rovira I Berger, Mireia 
;Ferrero, Giuliano ;Miserocchi, Magali ;Montanari, Alice ;Lattuca, Ruben ;Wittamer, Valérie
Référence eLife, 13
Publication Publié, 2025-12-01
;Ferrero, Giuliano ;Miserocchi, Magali ;Montanari, Alice ;Lattuca, Ruben ;Wittamer, Valérie Référence eLife, 13
Publication Publié, 2025-12-01
Article révisé par les pairs
| Résumé : | Recent studies have highlighted the heterogeneity of the immune cell compartment within the steady-state murine and human CNS. However, it is not known whether this diversity is conserved among non-mammalian vertebrates, especially in the zebrafish, a model system with increasing translational value. Here, we reveal the complexity of the immune landscape of the adult zebrafish brain. Using single-cell transcriptomics, we characterized these different immune cell subpopulations, including cell types that have not been or have only been partially characterized in zebrafish so far. By histology, we found that, despite microglia being the main immune cell type in the parenchyma, the zebrafish brain is also populated by a distinct myeloid population that shares a gene signature with mammalian dendritic cells (DC). Notably, zebrafish DC-like cells rely on batf3, a gene essential for the development of conventional DC1 in the mouse. Using specific fluorescent reporter lines that allowed us to reliably discriminate DC-like cells from microglia, we quantified brain myeloid cell defects in commonly used irf8-/-, csf1ra-/-, and csf1rb-/- mutant fish, revealing previously unappreciated distinct microglia and DC-like phenotypes. Overall, our results suggest a conserved heterogeneity of brain immune cells across vertebrate evolution and also highlights zebrafish-specific brain immunity characteristics. |
