4.7 Article

Transient deSUMOylation of IRF2BP proteins controls early transcription in EGFR signaling

Journal

EMBO REPORTS
Volume 22, Issue 3, Pages -

Publisher

WILEY
DOI: 10.15252/embr.201949651

Keywords

ATF3; DUSP1; EGFR; IRF2BP1; SUMO

Funding

  1. Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) [278001972 - TRR 186]
  2. DGF
  3. Peter and Traudl Engelhorn Foundation
  4. ProjektDEAL

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This study highlights the role of SUMO as a molecular switch in EGFR signaling, demonstrating the importance of transient deSUMOylation of IRF2BP proteins for the appropriate expression of immediate early genes. Comparative SUMO proteome analyses reveal novel regulators in signal transduction and transcription, such as IRF2BP1, IRF2BP2, and IRF2BPL.
Molecular switches are essential modules in signaling networks and transcriptional reprogramming. Here, we describe a role for small ubiquitin-related modifier SUMO as a molecular switch in epidermal growth factor receptor (EGFR) signaling. Using quantitative mass spectrometry, we compare the endogenous SUMO proteomes of HeLa cells before and after EGF stimulation. Thereby, we identify a small group of transcriptional coregulators including IRF2BP1, IRF2BP2, and IRF2BPL as novel players in EGFR signaling. Comparison of cells expressing wild type or SUMOylation-deficient IRF2BP1 indicates that transient deSUMOylation of IRF2BP proteins is important for appropriate expression of immediate early genes including dual specificity phosphatase 1 (DUSP1, MKP-1) and the transcription factor ATF3. We find that IRF2BP1 is a repressor, whose transient deSUMOylation on the DUSP1 promoter allows-and whose timely reSUMOylation restricts-DUSP1 transcription. Our work thus provides a paradigm how comparative SUMO proteome analyses serve to reveal novel regulators in signal transduction and transcription.

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