1. Academic Validation
  2. The ARE-dependent mRNA-destabilizing activity of BRF1 is regulated by protein kinase B

The ARE-dependent mRNA-destabilizing activity of BRF1 is regulated by protein kinase B

  • EMBO J. 2004 Dec 8;23(24):4760-9. doi: 10.1038/sj.emboj.7600477.
Martin Schmidlin 1 Min Lu Sabrina A Leuenberger Georg Stoecklin Michel Mallaun Brigitte Gross Roberto Gherzi Daniel Hess Brian A Hemmings Christoph Moroni
Affiliations

Affiliation

  • 1 Institute for Medical Microbiology, University of Basel, Basel, Switzerland.
Abstract

Butyrate response factor (BRF1) belongs to the Tis11 family of CCCH zinc-finger proteins, which bind to mRNAs containing an AU-rich element (ARE) in their 3' untranslated region and promote their deadenylation and rapid degradation. Independent signal transduction pathways have been reported to stabilize ARE-containing transcripts by a process thought to involve phosphorylation of ARE-binding proteins. Here we report that protein kinase B (PKB/Akt) stabilizes ARE transcripts by phosphorylating BRF1 at serine 92 (S92). Recombinant BRF1 promoted in vitro decay of ARE-containing mRNA (ARE-mRNA), yet phosphorylation by PKB impaired this activity. S92 phosphorylation of BRF1 did not impair ARE binding, but induced complex formation with the scaffold protein 14-3-3. In vivo and in vitro data support a model where PKB causes ARE-mRNA stabilization by inactivating BRF1 through binding to 14-3-3.

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