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Abrupt-mediated control of ninjurins regulates Drosophila sessile haemocyte compartments. | LitMetric

AI Article Synopsis

  • Hemocytes, macrophage-like cells in Drosophila, play a crucial role in the immune response and can be found either circulating or in stationary groups known as sessile hemocyte compartments (SHCs).
  • The study identifies the transcription factor Abrupt and Ninjurin cell adhesion molecules as key regulators for the recruitment of hemocytes to SHCs, particularly during the developmental stage of pupariation.
  • Manipulations affecting Ninjurin function reveal that it is essential for hemocyte targeting to SHCs; disrupting this function leads to premature dispersal of hemocytes, highlighting the importance of Ninjurin in mediating immune responses and managing hemocyte distribution during development.

Article Abstract

Macrophage-like cells called haemocytes are key effectors of Drosophila cellular innate immune function. Larval haemocytes exist either in circulation or localize to segmentally repeated sessile haemocyte compartments (SHCs). While numerous functions have been proposed for SHCs, the mechanisms directing haemocytes to them are unclear. Here, we have exploited the developmentally regulated dispersal of SHCs that occurs at pupariation to identify the Abrupt (Ab) transcription factor (TF) and ninjurin cell-adhesion molecules as regulators of haemocyte recruitment to SHCs. We show that larval haemocytes express ninjurins, which are required for targeting haemocytes to SHCs. However, at pupariation, ecdysteroid signalling stimulates Ab expression, which collaborates with TFs, including Blimp-1 and Hr3, to repress ninjurins and disperse haemocytes. We observe that experimental manipulations that antagonize ninjurin function in larval haemocytes cause premature SHC dispersal, while stabilization of ninjurins in haemocytes blocks developmentally regulated SHC remodelling and increases sensitivity to immune challenges. Cumulatively, our data indicate that control of ninjurin activity provides a common target through which diverse developmental, environmental and immune stimuli can be integrated to control haemocyte dispersal and immune function.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11664169PMC
http://dx.doi.org/10.1242/dev.202977DOI Listing

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