Crosstalk between C/EBPβ phosphorylation, arginine methylation, and SWI/SNF/Mediator implies an indexing transcription factor code

E Kowenz‐Leutz, O Pless, G Dittmar, M Knoblich… - The EMBO …, 2010 - embopress.org
E Kowenz‐Leutz, O Pless, G Dittmar, M Knoblich, A Leutz
The EMBO journal, 2010embopress.org
Cellular signalling cascades regulate the activity of transcription factors that convert
extracellular information into gene regulation. C/EBPβ is a ras/MAPkinase signal‐sensitive
transcription factor that regulates genes involved in metabolism, proliferation, differentiation,
immunity, senescence, and tumourigenesis. The protein arginine methyltransferase 4
PRMT4/CARM1 interacts with C/EBPβ and dimethylates a conserved arginine residue (R3)
in the C/EBPβ N‐terminal transactivation domain, as identified by mass spectrometry of cell …
Cellular signalling cascades regulate the activity of transcription factors that convert extracellular information into gene regulation. C/EBPβ is a ras/MAPkinase signal‐sensitive transcription factor that regulates genes involved in metabolism, proliferation, differentiation, immunity, senescence, and tumourigenesis. The protein arginine methyltransferase 4 PRMT4/CARM1 interacts with C/EBPβ and dimethylates a conserved arginine residue (R3) in the C/EBPβ N‐terminal transactivation domain, as identified by mass spectrometry of cell‐derived C/EBPβ. Phosphorylation of the C/EBPβ regulatory domain by ras/MAPkinase signalling abrogates the interaction between C/EBPβ and PRMT4/CARM1. Differential proteomic screening, protein interaction studies, and mutational analysis revealed that methylation of R3 constraines interaction with SWI/SNF and Mediator complexes. Mutation of the R3 methylation site alters endogenous myeloid gene expression and adipogenic differentiation. Thus, phosphorylation of the transcription factor C/EBPβ couples ras signalling to arginine methylation and regulates the interaction of C/EBPβ with epigenetic gene regulatory protein complexes during cell differentiation.
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