2012
DOI: 10.1002/cncr.27785
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UBE4B levels are correlated with clinical outcomes in neuroblastoma patients and with altered neuroblastoma cell proliferation and sensitivity to epidermal growth factor receptor inhibitors

Abstract: Background The UBE4B gene, located on chromosome 1p36, encodes a ubiquitin ligase that interacts with Hrs, a protein involved in EGFR trafficking, suggesting a link between EGFR trafficking and neuroblastoma pathogenesis. We have analyzed the roles of UBE4B in the outcomes of neuroblastoma patients and in neuroblastoma tumor cell proliferation, EGFR trafficking, and response to EGFR inhibition. Methods We examined the association of UBE4B expression with neuroblastoma patient survival using available microar… Show more

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Cited by 35 publications
(43 citation statements)
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“…This sustained signaling is not necessarily an effect of the undegraded EGFR residing on the plasma membrane because the contribution of actively signaling and endosomally localized EGFRs is sufficient to activate initiate signal transduction cascades that mediate cell survival (44). These data suggest that UBE4B can regulate global cellular events, like proliferation and signaling, and identify UBE4B as a potential therapeutic target for cancer therapies because its mutation or deletion from cells may underlie enhanced signaling that may be pathogenic (43,45).…”
Section: Volume 289 • Number 5 • January 31 2014mentioning
confidence: 90%
See 1 more Smart Citation
“…This sustained signaling is not necessarily an effect of the undegraded EGFR residing on the plasma membrane because the contribution of actively signaling and endosomally localized EGFRs is sufficient to activate initiate signal transduction cascades that mediate cell survival (44). These data suggest that UBE4B can regulate global cellular events, like proliferation and signaling, and identify UBE4B as a potential therapeutic target for cancer therapies because its mutation or deletion from cells may underlie enhanced signaling that may be pathogenic (43,45).…”
Section: Volume 289 • Number 5 • January 31 2014mentioning
confidence: 90%
“…5C. When incubation with UBE4B was followed by incubation with USP8, ubiquitinated EGFR was not detected (lane 5 physiological relevance of the correlation of UBE4B levels with EGFR degradation may be related to differences in cellular UBE4B levels (and, therefore, EGFR levels and downstream signaling) that could underlie disease states such as cancer (43). In this regard, UBE4B-depleted cells displayed prolonged ERK1/2 activation compared with control cells following EGFR stimulation.…”
Section: Volume 289 • Number 5 • January 31 2014mentioning
confidence: 97%
“…This strategy identified 28 overlapping targets, of which four overlapping candidate gene targets (DICER1, UBE4B, SGPP1, and PTPN21) were further analyzed based upon their potential involvement in radiation resistance or oncogenic processes (11,(25)(26)(27)(28). Using qRT-PCR, we verified that their expression were significantly decreased in PC3-miR-95 cells relative to PC3-control cells (Fig.…”
Section: Mir-95 Promotes Radiation Resistance Through Downregulation mentioning
confidence: 93%
“…1,2 Classification as high-risk or non-high-risk neuroblastoma depends on the stage defined by the International Neuroblastoma Staging System (INSS) 3,4 or less common the International Neuroblastoma Pathology Classification (INPC) proposed by Shimada et al 5,6 Over the past decades a multitude of prognosis and risk factors such as genetic mutations (e.g., deletion of chromosome 1p36, [7][8][9] altered expression of ALK, 10 PHOX2B) epigenetics, 9,11 ploidy 12 and age 13 have been identified. In the mid-1980s, the clinical and prognostic role of the proto-oncogene MYCN encoding for the protein N-Myc (v-myc myelocytomatosis viral related oncogene, neuroblastoma derived (avian)) was first described.…”
Section: Introductionmentioning
confidence: 99%