4.7 Article

The Repo Homeodomain Transcription Factor Suppresses Hematopoiesis in Drosophila and Preserves the Glial Fate

Journal

JOURNAL OF NEUROSCIENCE
Volume 39, Issue 2, Pages 238-255

Publisher

SOC NEUROSCIENCE
DOI: 10.1523/JNEUROSCI.1059-18.2018

Keywords

Drosophila; Gcm; glia; glide; hemocytes; repo

Categories

Funding

  1. INSERM
  2. CNRS
  3. UDS
  4. Ligue Regionale contre le Cancer
  5. Hopital de Strasbourg
  6. Association pour la Recherche sur le Cancer (ARC)
  7. Agence Nationale de la Recherche (ANR)
  8. ANR
  9. ARSEP (Fondation pour l'Aide a la Recherche sur la Sclerose en Plaques)
  10. ARC
  11. Ataxia UK [2491]
  12. NC3R [NC/L000199/1]
  13. French state fund through the ANR labex
  14. Marie Curie Grant [CIG 334077/IRTIM]

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Despite their different origins, Drosophila glia and hemocytes are related cell populations that provide an immune function. Drosophila hemocytes patrol the body cavity and act as macrophages outside the nervous system, whereas glia originate from the neuroepithelium and provide the scavenger population of the nervous system. Drosophila glia are hence the functional orthologs of vertebrate microglia, even though the latter are cells of immune origin that subsequently move into the brain during development. Interestingly, the Drosophila immune cells within (glia) and outside (hemocytes) the nervous system require the same transcription factor glial cells deficient/glial cells missing (Glide/Gcm) for their development. This raises the issue of how do glia specifically differentiate in the nervous system, and hemocytes in the procephalic mesoderm. The Repo homeodomain transcription factor and panglial direct target of Glide/Gcm is known to ensure glial terminal differentiation. Here we show that Repo also takes center stage in the process that discriminates between glia and hemocytes. First, Repo expression is repressed in the hemocyte anlagen by mesoderm-specific factors. Second, Repo ectopic activation in the procephalic mesoderm is sufficient to repress the expression of hemocyte-specific genes. Third, the lack of Repo triggers the expression of hemocyte markers in glia. Thus, a complex network of tissue-specific cues biases the potential of Glide/Gcm. These data allow us to revise the concept of fate determinants and help us to understand the bases of cell specification. Both sexes were analyzed.

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