PLoS Genetics (Jan 2012)

A shared role for RBF1 and dCAP-D3 in the regulation of transcription with consequences for innate immunity.

  • Michelle S Longworth,
  • James A Walker,
  • Endre Anderssen,
  • Nam-Sung Moon,
  • Andrew Gladden,
  • Margarete M S Heck,
  • Sridhar Ramaswamy,
  • Nicholas J Dyson

DOI
https://doi.org/10.1371/journal.pgen.1002618
Journal volume & issue
Vol. 8, no. 4
p. e1002618

Abstract

Read online

Previously, we discovered a conserved interaction between RB proteins and the Condensin II protein CAP-D3 that is important for ensuring uniform chromatin condensation during mitotic prophase. The Drosophila melanogaster homologs RBF1 and dCAP-D3 co-localize on non-dividing polytene chromatin, suggesting the existence of a shared, non-mitotic role for these two proteins. Here, we show that the absence of RBF1 and dCAP-D3 alters the expression of many of the same genes in larvae and adult flies. Strikingly, most of the genes affected by the loss of RBF1 and dCAP-D3 are not classic cell cycle genes but are developmentally regulated genes with tissue-specific functions and these genes tend to be located in gene clusters. Our data reveal that RBF1 and dCAP-D3 are needed in fat body cells to activate transcription of clusters of antimicrobial peptide (AMP) genes. AMPs are important for innate immunity, and loss of either dCAP-D3 or RBF1 regulation results in a decrease in the ability to clear bacteria. Interestingly, in the adult fat body, RBF1 and dCAP-D3 bind to regions flanking an AMP gene cluster both prior to and following bacterial infection. These results describe a novel, non-mitotic role for the RBF1 and dCAP-D3 proteins in activation of the Drosophila immune system and suggest dCAP-D3 has an important role at specific subsets of RBF1-dependent genes.