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Literature DB >> 22921829

Structural basis for the versatile interactions of Smad7 with regulator WW domains in TGF-β Pathways.

Eric Aragón¹, Nina Goerner, Qiaoran Xi, Tiago Gomes, Sheng Gao, Joan Massagué, Maria J Macias.

Abstract

Transforming growth factor (TGF)-β and BMP signaling is mediated by Smads 1-5 (R-Smads and Co-Smads) and inhibited by Smad7, a major hub of regulation of TGF-β and BMP receptors by negative feedback and antagonistic signals. The transcription coactivator YAP and the E3 ubiquitin ligases Smurf1/2 and Nedd4L target R-Smads for activation or degradation, respectively. Pairs of WW domain in these regulators bind PY motifs and adjacent CDK/MAPK and GSK3 phosphorylation sites in R-Smads in a selective and regulated manner. In contrast, here we show that Smad7 binds YAP, Smurf1, Smurf2, and Nedd4L constitutively, the binding involving a PY motif in Smad7 and no phosphorylation. We also provide a structural basis for how regulators that use WW domain pairs for selective interactions with R-Smads, resort to one single versatile WW domain for binding Smad7 to centralize regulation in the TGF-β and BMP pathways.

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Year: 2012 PMID： 22921829 PMCID： PMC3472128 DOI： 10.1016/j.str.2012.07.014

Source DB: PubMed Journal: Structure ISSN： 0969-2126 Impact factor: 5.006

42 in total

Structural basis for the versatile interactions of Smad7 with regulator WW domains in TGF-β Pathways.

1. Smurf1 interacts with transforming growth factor-beta type I receptor through Smad7 and induces receptor degradation.

Review 2. Mechanisms of TGF-beta signaling from cell membrane to the nucleus.

3. Integrating patterning signals: Wnt/GSK3 regulates the duration of the BMP/Smad1 signal.

4. The program XEASY for computer-supported NMR spectral analysis of biological macromolecules.

5. An expanded WW domain recognition motif revealed by the interaction between Smad7 and the E3 ubiquitin ligase Smurf2.

6. Overexpression of Smad7 results in severe pathological alterations in multiple epithelial tissues.

7. NMRPipe: a multidimensional spectral processing system based on UNIX pipes.

8. Smad6 inhibits BMP/Smad1 signaling by specifically competing with the Smad4 tumor suppressor.

9. Inhibition of transforming growth factor-beta/SMAD signalling by the interferon-gamma/STAT pathway.

10. Balancing BMP signaling through integrated inputs into the Smad1 linker.

1. Evidence for small-molecule-mediated loop stabilization in the structure of the isolated Pin1 WW domain.

Review 2. Structural determinants of Smad function in TGF-β signaling.

3. Association of colorectal cancer susceptibility variants with esophageal cancer in a Chinese population.

Review 4. Regulating the Regulators: Recent Revelations in the Control of E3 Ubiquitin Ligases.

5. Allosteric auto-inhibition and activation of the Nedd4 family E3 ligase Itch.

Review 6. Structural insights into the catalysis and regulation of E3 ubiquitin ligases.

7. The Smad7-Skp2 complex orchestrates Myc stability, impacting on the cytostatic effect of TGF-β.

8. Characterizing WW domain interactions of tumor suppressor WWOX reveals its association with multiprotein networks.

Review 9. WWOX at the crossroads of cancer, metabolic syndrome related traits and CNS pathologies.

10. RNA recognition and self-association of CPEB4 is mediated by its tandem RRM domains.