AI Article Synopsis

  • Autoregulation is a feedback mechanism in gene expression, and in Drosophila, the Rel gene "dorsal" can both activate and repress its own expression using this mechanism.
  • In response to immune challenges, Dorsal dynamically switches between two separate binding sites—kappaB(I) for activation and kappaB(P) for repression—that control its gene expression.
  • The study also reveals that the transcription factor AP1 is crucial for the repression phase, with its depletion leading to continuous expression of Dorsal, suggesting a complex regulatory system during the immune response.

Article Abstract

Autoregulation is one of the mechanisms of imparting feedback control on gene expression. Positive autoregulatory feedback results in induction of a gene, and negative feedback leads to its suppression. Here, we report an interesting mechanism of autoregulation operating on Drosophila Rel gene dorsal that can activate as well as repress its expression. Using biochemical and genetic approaches, we show that upon immune challenge Dorsal regulates its activation as well as repression by dynamically binding to two different kappaB motifs, kappaB(I) (intronic kappaB) and kappaB(P) (promoter kappaB), present in the dorsal gene. Although the kappaB(I) motif functions as an enhancer, the kappaB(P) motif acts as a transcriptional repressor. Interestingly, Dorsal binding to these two motifs is dynamic; immediately upon immune challenge, Dorsal binds to the kappaB(I) leading to auto-activation, whereas at the terminal phase of the immune response, it is removed from the kappaB(I) and repositioned at the kappaB(P), resulting in its repression. Furthermore, we show that repression of Dorsal as well as its binding to the kappaB(P) depends on the transcription factor AP1. Depletion of AP1 by RNA interference resulted in constitutive expression of Dorsal. In conclusion, this study suggests that during acute phase response dorsal is regulated by following two subcircuits: (i) Dl-kappaB(I) for activation and (ii) Dl-AP1-kappaB(P) for repression. These two subcircuits are temporally delineated and bring about overall regulation of dorsal during immune response. These results suggest the presence of a previously unknown mechanism of Dorsal autoregulation in immune-challenged Drosophila.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2911332PMC
http://dx.doi.org/10.1074/jbc.M109.097196DOI Listing

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