Activation of Transforming Growth Factor-β Signaling by SUMO-1 Modification of Tumor Suppressor Smad4/DPC4

Lin, Xia; Liang, Min; Liang, Yao-Yun; Brunicardi, F. Charles; Melchior, Frauke; Feng, Xin‐Hua

doi:10.1074/jbc.m302243200

Cited by 127 publications

(126 citation statements)

References 33 publications

Supporting

Mentioning

108

Contrasting

Order By: Relevance

“…We next used the in vitro SUMOylation assay (Desterro et al 1998) to investigate Med as a SUMOylation target. Med is SUMO modified in vitro, yet mutation of the two amino acids-K113, K159 (MedAB)-equivalent to those shown to be necessary for SUMOylation of Smad4 (Lin et al 2003a) does not abolish Med SUMOylation (Fig. 2B,D).…”

Section: Med Is Sumo Modified In Vitromentioning

confidence: 99%

“…As Smad4 has been shown to be SUMOylated (Lin et al 2003a), we tested whether Drosophila Med is also a target. First, we used the yeast two-hybrid assay to investigate a possible interaction between Lwr and Med.…”

Section: Med Is Sumo Modified In Vitromentioning

confidence: 99%

“…During C. elegans development, SUMOylation of the Polycomb group repressor protein SOP-2 is necessary for it to repress Hox genes (Zhang et al 2004), whereas modification of the Drosophila gypsy insulator may influence the establishment of chromatin domains (Capelson and Corces 2006). Smad4, the vertebrate ortholog of Med (Wisotzkey et al 1998), is SUMO modified in tissue culture cells, resulting in either activation (Lin et al 2003a) or repression (Long and Griffith 2000) of its activity depending on the reporter analyzed. Although SUMOylation activates some transcription factors, it is more commonly associated with transcriptional repression.…”

mentioning

confidence: 99%

See 2 more Smart Citations

Medea SUMOylation restricts the signaling range of the Dpp morphogen in the Drosophila embryo

Miles¹,

Jaffray²,

Campbell³

et al. 2008

Genes Dev.

View full text Add to dashboard Cite

Morphogens are secreted signaling molecules that form concentration gradients and control cell fate in developing tissues. During development, it is essential that morphogen range is strictly regulated in order for correct cell type specification to occur. One of the best characterized morphogens is Drosophila Decapentaplegic (Dpp), a BMP signaling molecule that patterns the dorsal ectoderm of the embryo by activating the Mad and Medea (Med) transcription factors. We demonstrate that there is a spatial and temporal expansion of the expression patterns of Dpp target genes in SUMO pathway mutant embryos. We identify Med as the primary SUMOylation target in the Dpp pathway, and show that failure to SUMOylate Med leads to the increased Dpp signaling range observed in the SUMO pathway mutant embryos. Med is SUMO modified in the nucleus, and we provide evidence that SUMOylation triggers Med nuclear export. Hence, Med SUMOylation provides a mechanism by which nuclei can continue to monitor the presence of extracellular Dpp signal to activate target gene expression for an appropriate duration. Overall, our results identify an unusual strategy for regulating morphogen range that, rather than impacting on the morphogen itself, targets an intracellular transducer. Med and its vertebrate ortholog Smad4 have been found to constitutively shuttle between the nucleus and cytoplasm in a signal-independent manner (Pierreux et al. 2000;Yao et al. 2008). Smad4 contains both a nuclear localization signal (NLS) and a CRM-1-dependent nuclear export signal (NES), and it has been proposed that the relative strengths of these two signals within a tissue regulate the amount of shuttling. Smad4, which shuttles into the nucleus in the absence of signal, is unable to activate transcription (Pierreux et al. 2000), possibly due to recruitment of a repressive complex harboring the SnoN oncoprotein (Stroschein et al. 1999).The small ubiquitin-like modifier protein SUMO is conjugated to its substrate through the sequential activities of E1, E2, and E3 enzymes. Ubc-9, the essential E2 enzyme, catalyzes the conjugation of SUMO to the target lysine, typically located in a ⌿KxE consensus motif (where ⌿ is a large hydrophobic residue and x is any residue) (Hay 2005). An extended SUMO motif compris-

show abstract

Section: Med Is Sumo Modified In Vitromentioning

confidence: 99%

Section: Med Is Sumo Modified In Vitromentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

Medea SUMOylation restricts the signaling range of the Dpp morphogen in the Drosophila embryo

Miles¹,

Jaffray²,

Campbell³

et al. 2008

Genes Dev.

View full text Add to dashboard Cite

show abstract

“…In addition to being poly-ubiquitinated and degraded by proteasomes, Smad4 has also been shown to be mono-ubiquitinated and sumoylated [57,[63][64][65][66]. Monoubiquitination of Smad4 occurs on Lys-507 in the MH2 domain and leads to improved transcriptional TGFb signaling [63], but also promotes export of Smad4 to the cytoplasm [67].…”

Section: Regulation Of Co-smad Stabilitymentioning

confidence: 99%

Regulating the stability of TGFβ receptors and Smads

et al. 2008

View full text Add to dashboard Cite

Abbreviations: AIP4 (atrophin 1-interacting protein 4); BMP (bone morphogenetic protein); CHIP (carboxyl terminus of Hsc70-interacting protein); GSK3b (glycogen synthase kinase 3-b); HECT (homologous to E6-AP carboxyl terminus); MAPK (mitogen-activated protein kinase); NEDD4-2 (neural precursor cell expressed, developmentally downregulated 4-2); PIAS (protein inhibitor of activated Stat); Smurf (Smad ubiquitylation regulatory factor); STRAP (serine-threonine kinase receptorassociated protein); SUMO (small ubiquitin-like modifier); TbRI/TbRII (TGFb receptor type I and II); TGFb (transforming growth factor b); WWP1 (WW domain-containing protein 1); Ub (ubiquitin) npg Transforming growth factor β (TGFβ) controls cellular behavior in embryonic and adult tissues. TGFβ binding to serine/threonine kinase receptors on the plasma membrane activates Smad molecules and additional signaling proteins that together regulate gene expression. In this review, mechanisms and models that aim at explaining the coordination between several components of the signaling network downstream of TGFβ are presented. We discuss how the activity and duration of TGFβ receptor/Smad signaling can be regulated by post-translational modifications that affect the stability of key proteins in the pathway. We highlight links between these mechanisms and human diseases, such as tissue fibrosis and cancer. Regulating the stability of TGFβ receptors and Smads

show abstract

“…Smad4 is modified by SUMO-1 on lysines 159 and 113 in/near the MH1 domain (Figure 2), and this SUMOylation has been shown to require the PIAS (Protein Inhibitors of Activated STAT) family member PIASy [72], PIAS1 [73,74] or PIASxβ [74] as an E3 ligase. Smad4 SUMOylation has largely been shown to increase its stability in the nucleus and/or decrease its nuclear export, ultimately stimulating TGF-β signaling [72,[74][75][76]. However, SUMOylation has also been shown to decrease Smad4s transcriptional activity in some reporter assays [77], and the transcriptional co-repressor Daxx can suppress Smad4-mediated transcriptional activity by directly interacting with SUMOylated-Smad4 in a lys159 (but not lys113) SUMO dependent manner [78].…”

Section: Modifications Of Smad4 In Normal Cellsmentioning

confidence: 99%

To (TGF)β or not to (TGF)β: Fine-tuning of Smad signaling via post-translational modifications

Wrighton

Feng

2008

Cellular Signalling

Self Cite

View full text Add to dashboard Cite

show abstract

Activation of Transforming Growth Factor-β Signaling by SUMO-1 Modification of Tumor Suppressor Smad4/DPC4

Cited by 127 publications

References 33 publications

Medea SUMOylation restricts the signaling range of the Dpp morphogen in the Drosophila embryo

Medea SUMOylation restricts the signaling range of the Dpp morphogen in the Drosophila embryo

Regulating the stability of TGFβ receptors and Smads

To (TGF)β or not to (TGF)β: Fine-tuning of Smad signaling via post-translational modifications

Contact Info

Product

Resources

About