Small ubiquitin-like modifier conjugation regulates nuclear export of TEL, a putative tumor suppressor

Wood, Lauren D.; Irvin, Brenda J.; Nucifora, Giuseppina; Luce, K. Scott; Hiebert, Scott W.

doi:10.1073/pnas.0637114100

Cited by 113 publications

(111 citation statements)

References 63 publications

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“…The C-terminal ETV6 mutations were either inframe or resulted in truncation of the ETS domain by out-of-frame mutation. In concordance with earlier studies (Waga et al, 2003;Wood et al, 2003), the truncated ETV6 proteins were impaired in repressing transcription in a ETV6-specific luciferase assay. Moreover, coexpression of the mutants with an intact homodimerization domain (#2236, 3102, 2649 and N) completely abolished the transcription repression by wt ETV6.…”

Section: Discussionsupporting

confidence: 77%

Somatic heterozygous mutations in ETV6 (TEL) and frequent absence of ETV6 protein in acute myeloid leukemia

et al. 2005

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ETV6 (ets translocation variant gene 6) TEL (translocation ets leukemia), encoding a transcriptional repressor, is involved in various translocations associated with human malignancies. Strikingly, the nonrearranged ETV6 allele is often deleted or inactivated in cells harboring these translocations. Although ETV6 translocations are infrequent in acute myeloid leukemia (AML), mutations or deregulated expression of ETV6 may contribute to leukemogenesis. To investigate the involvement of ETV6 in AML, we analysed 300 newly diagnosed patients for mutations in the coding region of the gene. Furthermore, we studied protein expression in 77 patients using two ETV6-specific antibodies. Five somatic heterozygous mutations were detected, which affected either the homodimerization-or the DNA-binding domain of ETV6. The proteins translated from the cDNAs of these mutants were unable to repress transcription and showed dominant-negative effects. In addition, we demonstrate that one-third of AML patients have deficient ETV6 protein expression, which is not related to ETV6 mRNA expression levels. In conclusion, we demonstrate that ETV6 abnormalities are not restricted to translocations and occur more frequently in AML than previously thought. Additional comprehensive studies are required to define the clinical consequence of ETV6 loss of function in AML.

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Section: Discussionsupporting

confidence: 77%

Somatic heterozygous mutations in ETV6 (TEL) and frequent absence of ETV6 protein in acute myeloid leukemia

et al. 2005

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“…Work in Dictyostelium on the MAP kinase MEK-1 revealed that SUMOylation is required for MEK1's translocation from the nucleus to the cytosol (Galy et al, 2002). A similar mechanism was proposed recently for the transcriptional repressor TEL (Wood et al, 2003). The localization of a SUMO-ligase at the nuclear pore now strengthens the idea that SUMOylation is coupled to nuclear transport processes.…”

Section: E3-like Ligases and Isopeptidases As Regulators In The Sumo supporting

confidence: 55%

SUMO: a regulator of gene expression and genome integrity

2004

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Post-translational modification with the ubiquitin-like SUMO protein is involved in the regulation of many cellular key processes. The SUMO system modulates signal transduction pathways, including cytokine, Wnt, growth factor and steroid hormone signalling. SUMO frequently restrains the activity of downstream transcription factors in these pathways presumably by facilitating the recruitment of corepressors or mediating the assembly of repressor complexes. Additionally, evidence is accumulating that SUMO controls pathways important for the surveillance of genome integrity. SUMO regulates the PML/p53 tumour suppressor network, a key determinant in the cellular response to DNA damage. Moreover, proteins that maintain genomic stability by functioning at the interface between DNA replication, recombination and repair processes undergo SUMOylation. We will discuss some key findings that exemplify the role of SUMO in transcriptional regulation and genome surveillance.

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“…For example, SUMO has been implicated in promoting the nuclear retention of the Elk-1 transcription factor (Salinas et al 2004), adenoviral E1B-55K protein (Kindsmuller et al 2007), and CtBP1 corepressor (Lin et al 2003b). In terms of SUMO promoting nuclear export, as our data suggest for Med, examples include the TEL repressor protein (Wood et al 2003), MEK1 kinase (Sobko et al 2002), ribosome biogenesis factors (Panse et al 2006), and p53 transcription factor (Carter et al 2007).…”

Section: Sumoylation Promotes Med Nuclear Exportmentioning

confidence: 80%

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

Miles¹,

Jaffray²,

Campbell³

et al. 2008

Genes Dev.

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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-

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Small ubiquitin-like modifier conjugation regulates nuclear export of TEL, a putative tumor suppressor

Cited by 113 publications

References 63 publications

Somatic heterozygous mutations in ETV6 (TEL) and frequent absence of ETV6 protein in acute myeloid leukemia

Somatic heterozygous mutations in ETV6 (TEL) and frequent absence of ETV6 protein in acute myeloid leukemia

SUMO: a regulator of gene expression and genome integrity

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

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