Gene interactions and pathways from curated databases and text-mining
Nat Cell Biol 2008, PMID: 18758450

The type I TGF-beta receptor engages TRAF6 to activate TAK1 in a receptor kinase-independent manner.

Sorrentino, Alessandro; Thakur, Noopur; Grimsby, Susanne; Marcusson, Anders; von Bulow, Verena; Schuster, Norbert; Zhang, Shouting; Heldin, Carl-Henrik; Landström, Maréne

Transforming growth factor-beta (TGF-beta) is a multifunctional cytokine that regulates embryonic development and tissue homeostasis; however, aberrations of its activity occur in cancer. TGF-beta signals through its Type II and Type I receptors (TbetaRII and TbetaRI) causing phosphorylation of Smad proteins. TGF-beta-associated kinase 1 (TAK1), a member of the mitogen-activated protein kinase kinase kinase (MAPKKK) family, was originally identified as an effector of TGF-beta-induced p38 activation. However, the molecular mechanisms for its activation are unknown. Here we report that the ubiquitin ligase (E3) TRAF6 interacts with a consensus motif present in TbetaRI. The TbetaRI-TRAF6 interaction is required for TGF-beta-induced autoubiquitylation of TRAF6 and subsequent activation of the TAK1-p38/JNK pathway, which leads to apoptosis. TbetaRI kinase activity is required for activation of the canonical Smad pathway, whereas E3 activity of TRAF6 regulates the activation of TAK1 in a receptor kinase-independent manner. Intriguingly, TGF-beta-induced TRAF6-mediated Lys 63-linked polyubiquitylation of TAK1 Lys 34 correlates with TAK1 activation. Our data show that TGF-beta specifically activates TAK1 through interaction of TbetaRI with TRAF6, whereas activation of Smad2 is not dependent on TRAF6.

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Text Mining Data

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Manually curated Databases

  • IRef Biogrid Interaction: TGFBR1 — MAPK14 (physical association, affinity chromatography technology)
  • IRef Biogrid Interaction: TRAF6 — TGFBR1 (physical association, affinity chromatography technology)
  • IRef Biogrid Interaction: BMPR1B — TRAF6 (physical association, affinity chromatography technology)
  • IRef Biogrid Interaction: TRAF6 — MAP3K7 (physical association, affinity chromatography technology)
  • IRef Biogrid Interaction: MAP3K7 — TGFBR1 (physical association, affinity chromatography technology)
  • IRef Hprd Interaction: TGFBR1 — TRAF6 (in vivo)
  • IRef Hprd Interaction: BMPR1B — TRAF6 (in vivo)
  • IRef Hprd Interaction: TRAF6 — MAP3K7 (in vivo)
  • IRef Hprd Interaction: TRAF6 — MAP3K7 (in vitro)
  • IRef Hprd Interaction: MAP3K7 — MAP3K7 (two hybrid)
  • IRef Hprd Interaction: MAP3K7 — MAP3K7 (in vivo)
  • IRef Hprd Interaction: MAP3K7 — MAP3K7 (in vitro)
  • IRef Hprd Interaction: TGFBR1 — MAP3K7 (in vivo)
In total, 6 gene pairs are associated to this article in curated databases