The Oncoprotein SS18-SSX1 Promotes p53 Ubiquitination and Degradation by Enhancing HDM2 Stability

D’Arcy, Pádraig; Maruwge, Wessen; Ryan, Bríd Ann; Brodin, Bertha

doi:10.1158/1541-7786.mcr-07-0176

Cited by 26 publications

(17 citation statements)

References 53 publications

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“…Characteristics of the subjects were similar to those reported by Oda et al 8 In this study, the tumor was found at the extremity, head Some cases expressing p53. This result was similar to that reported by Oda et al 8 and Schneider-Stock et al 11 In synovial sarcoma, p53 should decreases as reported by D'Arcy et al 4 , though the soft tissue tumors may have increased expression of p53 and this is associated with poor prognosis. 12 Several processes can increase p53 expression such as telomere shortening, DNA damage, oxidative stress, oncogenic stress and Ras activation.…”

Section: Discussionsupporting

confidence: 91%

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p53 expression in synovial sarcoma and its association with prognostic factors

Ilmiawan¹,

Wuyung²,

Siregar³

2012

Med J Indones

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Abstrak AbstractBackground: Synovial sarcoma is an aggressive tumor and has two common histological subtype, biphasic and monophasic. It has SYT-SSX gene fusion that decreases expression of p53 tumor suppressor. The prognosis is associated with mitosis and tumor diameter. Therefore this study conducted to know the pattern of p53 expresion and its association with mitosis, histological subtype, and other prognosis factors.

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Section: Discussionsupporting

confidence: 91%

“…Moreover, SYT-SSX1 shows pro-survival activity and increases cell growth. 4 p53 plays important role to maintain genome integrity. Upon DNA damage, the p53 will be activated.…”

mentioning

confidence: 99%

p53 expression in synovial sarcoma and its association with prognostic factors

Ilmiawan¹,

Wuyung²,

Siregar³

2012

Med J Indones

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“…Previous studies by Peng et al [29] demonstrated a reduction in antiapoptotic gene B-cell lymphoma-2 (bcl-2) and a parallel increase in proapoptotic caspase-3 after knockdown of SS18-SSX by siRNA. In addition, D'Arcy et al demonstrated expression of SS18-SSX1 in U2OS osteosarcoma cells inhibited apoptosis induced by cytotoxic agents such as doxorubicin [10]. We have validated that in our cell models SS18-SSX1 reduction is also linked to apoptosis activation.…”

Section: Discussionsupporting

confidence: 82%

Loss of SS18-SSX1 Inhibits Viability and Induces Apoptosis in Synovial Sarcoma

Soni¹,

Schlottman²,

Erkizan³

et al. 2014

Clinical Orthopaedics &Amp; Related Research

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Background Most synovial sarcomas contain a chromosomal translocation t(X;18), which results in the formation of an oncoprotein SS18-SSX critical to the viability of synovial sarcoma. Questions/purposes We (1) established and characterized three novel synovial sarcoma cell lines and asked (2) whether inhibition of SS18-SSX1 decreases cell viability in these cell lines; and (3) whether reduction in viability after SS18-SSX1 knockdown is caused by apoptosis. After identifying a specific posttranscriptional splice variant in our cell lines, we asked (4) whether this provides a survival benefit in synovial sarcoma. Methods Cells lines were characterized. SS18-SSX1 knockdown was achieved using a shRNA system. Cell viability was assessed by WST-1 analysis and apoptosis examined by caspase-3 activity. Results We confirmed the SS18-SSX1 translocation in all cell lines and identified a consistent splicing variant. We achieved successful knockdown of SS18-SSX1 and with this saw a significant reduction in cell viability. Decreased viability was a result of increased apoptosis. Reintroduction of the exon 8 sequence into cells reduced cell viability in all cell lines. Conclusions We confirmed the presence of the SS18-SSX1 translocation in our cell lines and its importance in the survival of synovial sarcoma. We have also demonstrated that reduction in cell viability is related to an increase in apoptosis. In addition, we have identified a potential mediator of SS18-SSX function in exon 8. Clinical Relevance SS18-SSX represents a tumor-specific target in synovial sarcoma. Exploitation of SS18-SSX and its protein partners will allow us to develop potent tumor-specific therapeutic agents.

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“…First, MDM2 stabilizes its own protein levels through posttranslational modifications, such as sumoylation and phosphorylation. Sumoylation protects MDM2 from proteasomal degradation by competing with ubiquitin at its major conjugation site, Lys 464 (4), while the phosphorylation of MDM2 prevents it from self-ubiquitination, thereby stabilizing MDM2 (9,11). Second, the deubiquitination enzymes HAUSP and USP2a have been shown to directly bind and remove ubiquitin molecules from MDM2, resulting in its stabilization (2,26,41).…”

Section: Discussionmentioning

confidence: 99%