Dual role of the Smad4/DPC4 tumor suppressor in TGFβ-inducible transcriptional complexes

  1. Fang Liu,
  2. Celio Pouponnot, and
  3. Joan Massagué1
  1. Cell Biology Program and Howard Hughes Medical Institute, Memorial Sloan-Kettering Cancer Center, New York, New York 10021 USA

Abstract

Upon ligand binding, the receptors of the TGFβ family phosphorylate Smad proteins, which then move into the nucleus where they activate transcription. To carry out this function, the receptor-activated Smads 1 and 2 require association with the product of deleted in pancreatic carcinoma, locus 4 (DPC4), Smad4. We investigated the step at which Smad4 is required for transcriptional activation. Smad4 is not required for nuclear translocation of Smads 1 or 2, or for association of Smad2 with a DNA binding partner, the winged helix protein FAST-1. Receptor-activated Smad2 takes Smad4 into the nucleus where they form a complex with FAST-1 that requires these three components to activate transcription. Smad4 contributes two functions: Through its amino-terminal domain, Smad4 promotes binding of the Smad2/Smad4/FAST-1 complex to DNA; through its carboxy-terminal domain, Smad4 provides an activation function required for Smad1 or Smad2 to stimulate transcription. The dual function of Smad4 in transcriptional activation underscores its central role in TGFβ signaling.

Keywords

Footnotes

  • 1 Corresponding author.

  • E-MAIL j-massague{at}ski.mskcc.org; FAX (212) 717-3298.

    • Received August 29, 1997.
    • Accepted October 3, 1997.
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