COP1 is a tumour suppressor that causes degradation of ETS transcription factors

Vitari, Alberto C.; Leong, Kin Fon; Newton, Kim; Yee, Cindy J.; O’Rourke, Karen; Liu, Jinfeng; Phu, Lilian; Vij, Rajesh; Ferrando, Ronald E.; Couto, Suzana; Mohan, Sankar; Pandita, Ajay; Hongo, Jo-Anne; Arnott, David; Wertz, Ingrid E.; Gao, Wei‐Qiang; French, Dorothy; Dixit, Vishva M.

doi:10.1038/nature10005

Cited by 144 publications

(197 citation statements)

References 40 publications

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“…Given the principal role of Ras signaling in metastases, combined with the fact that Ras signaling is generally refractory to conventional therapy (64,65), targeting ETV4 in prostate cancer may provide an alternative means of inhibiting metastasis. This idea is supported by the potential to target the ubiquitin ligase COP1, which has been shown to regulate ETV function in prostate cancer (66). Thus, our findings support the idea of targeting ETV4 as a means of abrogating Ras signaling in advanced prostate cancer.…”

Section: Discussionsupporting

confidence: 76%

ETV4 promotes metastasis in response to activation of PI3-kinase and Ras signaling in a mouse model of advanced prostate cancer

Aytés

Mitrofanova

Kinkade³

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

121

129

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Combinatorial activation of PI3-kinase and RAS signaling occurs frequently in advanced prostate cancer and is associated with adverse patient outcome. We now report that the oncogenic Ets variant 4 (Etv4) promotes prostate cancer metastasis in response to coactivation of PI3-kinase and Ras signaling pathways in a genetically engineered mouse model of highly penetrant, metastatic prostate cancer. Using an inducible Cre driver to simultaneously inactivate Pten while activating oncogenic Kras and a fluorescent reporter allele in the prostate epithelium, we performed lineage tracing in vivo to define the temporal and spatial occurrence of prostate tumors, disseminated tumor cells, and metastases. These analyses revealed that though disseminated tumors cells arise early following the initial occurrence of prostate tumors, there is a significant temporal lag in metastasis, which is temporally coincident with the up-regulation of Etv4 expression in primary tumors. Functional studies showed that knockdown of Etv4 in a metastatic cell line derived from the mouse model abrogates the metastatic phenotype but does not affect tumor growth. Notably, expression and activation of ETV4, but not other oncogenic ETS genes, is correlated with activation of both PI3-kinase and Ras signaling in human prostate tumors and metastases. Our findings indicate that ETV4 promotes metastasis in prostate tumors that have activation of PI3-kinase and Ras signaling, and therefore, ETV4 represents a potential target of therapeutic intervention for metastatic prostate cancer. M etastasis is a highly inefficient process that involves multiple steps, including invasion of local stroma, intravasation into the bloodstream and/or lymphatic system, and extravasation into a secondary tissue, which is thought to arise as a consequence of multiple molecular/epigenetic alterations in tumor cells, as well as in the microenvironment of metastatic sites (1-4). Nonetheless, despite its inefficiency, most cancer deaths are due to metastases and our current inability to treat them once they arise. In particular, in prostate cancer, the locally invasive disease has a nearly 100% survival rate, whereas metastatic prostate cancer is very often lethal (5).Recent analyses have identified key molecular pathways that are frequently dysregulated during prostate cancer progression, as a consequence of copy number alterations, chromosomal rearrangements, and other aberrant genetic/epigenetic events (6-10). For example, loss of chromosomal region 8p21 and coincident haploinsufficiency for the NKX3.1 homeobox gene occurs frequently in precursor lesions known as prostatic intraepithelial neoplasia (PIN) and are associated with prostate cancer initiation (11,12). Another early event in prostate tumorigenesis is the formation of the TMPRSS2-ERG rearrangement, which fuses the transmembrane protease TMPRSS2 promoter with the coding region of the ETS transcription factor ERG (13, 14). The TMPRSS2-ERG fusion is highly prevalent in prostate cancer and is associated with disease out...

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Section: Discussionsupporting

confidence: 76%

ETV4 promotes metastasis in response to activation of PI3-kinase and Ras signaling in a mouse model of advanced prostate cancer

Aytés

Mitrofanova

Kinkade³

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

121

129

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“…Most interestingly, EWS-FLI1 displays a higher turnover compared with its full-length proteins EWSR1 and FLI1. In contrast, the ETS proteins ERG and ETV1, which are fused to the TMPRSS2 promoter in prostate cancer, stabilize the protein and confer a physiological advantage to cancer cells (33,34,36). The truncated protein versions display increased stability due to loss of the N-terminal E3 ligase motif.…”

Section: Ews-fli1 Degradation Is Mediated By One Lysine Residuementioning

confidence: 99%

“…If the turnover and subsequent E3 ligase binding of ETS members are conserved, EWS-FLI1 might possibly interact with E3 ligases via its EWSR1 domain, giving rise to a new regulatory mechanism. However, the basic concept that truncated oncogenic TFs are more stable than their wild type counterparts (36) might not apply for fusion proteins consisting of two unrelated protein domains. Whether this is indeed a general paradigm or rather specific for EWSR1-related fusion proteins needs to be further elucidated.…”

Section: Ews-fli1 Degradation Is Mediated By One Lysine Residuementioning

confidence: 99%

“…Considering their high conservation, proteasomal degradation is likely to be the main mechanism of turnover for most ETS family members. Most interestingly, truncated ERG and ETV1 lack the N-terminal E3 binding domain, which results in a delayed turnover of aberrant ETS proteins (34,36). Here, we focus specifically on the turnover of the fusion protein EWS-FLI1, which only harbors the ETS and the C-terminal domain from FLI1.…”

mentioning

confidence: 99%

“…Several ETS proteins can be polyubiquitinated by different E3 ligases and subsequently degraded by the proteasome (33)(34)(35)(36). Considering their high conservation, proteasomal degradation is likely to be the main mechanism of turnover for most ETS family members.…”

mentioning

confidence: 99%

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Proteasomal Degradation of the EWS-FLI1 Fusion Protein Is Regulated by a Single Lysine Residue

Gierisch

Pfistner

Lopez-Garcia

et al. 2016

Journal of Biological Chemistry

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Edited by George DeMartinoEHere, we identify the EWS-FLI1 protein as a substrate of the ubiquitin-proteasome system with a characteristic polyubiquitination pattern. Using a global protein stability approach, we determined the half-life of EWS-FLI1 to lie between 2 and 4 h, whereas full-length EWSR1 and FLI1 were more stable. By mass spectrometry, we identified two ubiquitin acceptor lysine residues of which only mutation of Lys-380 in the ETS domain of the FLI1 part abolished EWS-FLI1 ubiquitination and stabilized the protein posttranslationally. Expression of this highly stable mutant protein in Ewing cells while simultaneously depleting the endogenous wild type protein differentially modulates two subgroups of target genes to be either EWS-FLI1 protein-dependent or turnover-dependent. The majority of target genes are in an unaltered state and cannot be further activated. Our study provides novel insights into EWS-FLI1 turnover, a critical pathway in Ewing sarcoma pathogenesis, and lays new ground to develop novel therapeutic strategies in Ewing sarcoma. E-26 transformation-specific (ETS)2 family members are strong activators or repressors of transcription with a highly conserved ETS domain (1-3). ETS transcription factors (TFs) bind most commonly in complexes to a GGA core region to mediate gene expression (4, 5). Their main biological functions include regulation of differentiation, lineage determination of the hematopoietic system, and control of angiogenesis (6, 7). Most of the ETS family members have oncogenic potential because truncated or overexpressed ETS proteins have been linked to several cancer entities (8 -11). ERG and ETV1 are frequently fused to the TMPRSS2 promoter in prostate cancer, whereas ETV1 and ETV6 are implicated in leukemia (12, 13). Like other aberrant fusion proteins, they act as drivers of uncontrolled cell growth and survival (14, 15). However, most TFs do not harbor an enzymatic pocket and are therefore difficult to target directly. Novel strategies that uncover vulnerable sites in TFs are urgently needed to develop novel targeted therapies (16).Ewing sarcoma is a rare pediatric bone and soft tissue tumor with an aggressive behavior and prevalence to metastasize (17,18). Its main genetic abnormalities are EWS-ETS rearrangements, among them most commonly the EWS gene on chromosome 22 fused to FLI1 on chromosome 11, which results in expression of the chimeric transcription factor . Continuous expression of the fusion protein is crucial for tumor formation, progression, and maintenance (22, 23), and its down-regulation inhibits proliferation and reduces tumor cell growth (24 -26). EWS-FLI1 is thought to function mainly as a modulator to activate and repress a wide range of target genes but also as a regulator of splicing processes or as a component of large interaction networks (27-31). However, inhibition of a single downstream target gene has not been proven effective yet for Ewing sarcoma therapy.The turnover of most intracellular proteins is mediated via the ubiquitin-proteasome ...

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EGF Relays Signals to COP1 and Facilitates FOXO4 Degradation to Promote Tumorigenesis

Choi

Zou

et al. 2020

Advanced Science

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Forkhead-Box Class O 4 (FOXO4) is involved in critical biological functions, but its response to EGF-PKB/Akt signal regulation is not well characterized. Here, it is reported that FOXO4 levels are downregulated in response to EGF treatment, with concurrent elevation of COP9 Signalosome subunit 6 (CSN6) and E3 ubiquitin ligase constitutive photomorphogenic 1 (COP1) levels. Mechanistic studies show that CSN6 binds and regulates FOXO4 stability through enhancing the E3 ligase activity of COP1, and that COP1 directly interacts with FOXO4 through a VP motif on FOXO4 and accelerates the ubiquitin-mediated degradation of FOXO4. Metabolomic studies demonstrate that CSN6 expression leads to serine and glycine production. It is shown that FOXO4 directly binds and suppresses the promoters of serine-glycine-one-carbon (SGOC) pathway genes, thereby diminishing SGOC metabolism. Evidence shows that CSN6 can regulate FOXO4-mediated SGOC gene expression. Thus, these data suggest a link of CSN6-FOXO4 axis and ser/gly metabolism. Further, it is shown that CSN6-COP1-FOXO4 axis is deregulated in cancer and that the protein expression levels of CSN6 and FOXO4 can serve as prognostic markers for cancers. The results illustrate a pathway regulation of FOXO4-mediated serine/glycine metabolism through the function of CSN6-COP1 axis. Insights into this pathway may be strategically designed for therapeutic intervention in cancers.

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COP1 is a tumour suppressor that causes degradation of ETS transcription factors

Cited by 144 publications

References 40 publications

ETV4 promotes metastasis in response to activation of PI3-kinase and Ras signaling in a mouse model of advanced prostate cancer

ETV4 promotes metastasis in response to activation of PI3-kinase and Ras signaling in a mouse model of advanced prostate cancer

Proteasomal Degradation of the EWS-FLI1 Fusion Protein Is Regulated by a Single Lysine Residue

EGF Relays Signals to COP1 and Facilitates FOXO4 Degradation to Promote Tumorigenesis

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