High expression of orphan nuclear receptor NR4A1 in a subset of ovarian tumors with worse outcome

Delgado, Evan R.; Boisen, M.M.; Laskey, Robin; Chen, Rui; Song, Chi; Sallit, J. Z.; Yochum, Zachary A.; Andersen, Courtney; Sikora, Matthew J.; Wagner, Jacob P.; Safe, Stephen; Elishaev, Esther; Lee, Adrian V.; Edwards, Robert P.; Haluska, Paul; Tseng, George C.; Schurdak, Mark E.; Oesterreich, Steffi

doi:10.1016/j.ygyno.2016.02.030

Cited by 21 publications

(18 citation statements)

References 41 publications

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“…Overexpression of CYR61 has been shown to be associated with development and poor prognosis of ovarian carcinomas 46 . NT5E-expressing cancers were reported to be resistant to platinum-based therapy 47 , while NR42A has been reported to be highly expressed in ovarian cancer tumors with poor prognosis 48 . We found that these HIF1α-regulated genes play significant roles in ovarian cancer first-line chemotherapy resistance, leading to disease progression and poor clinical outcome.…”

Section: Discussionmentioning

confidence: 99%

The Prognostic 97 Chemoresponse Gene Signature in Ovarian Cancer

Matondo

Shahid

et al. 2017

Sci Rep

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Patient diagnosis and care would be significantly improved by understanding the mechanisms underlying platinum and taxane resistance in ovarian cancer. Here, we aim to establish a gene signature that can identify molecular pathways/transcription factors involved in ovarian cancer progression, poor clinical outcome, and chemotherapy resistance. To validate the robustness of the gene signature, a meta-analysis approach was applied to 1,020 patients from 7 datasets. A 97-gene signature was identified as an independent predictor of patient survival in association with other clinicopathological factors in univariate [hazard ratio (HR): 3.0, 95% Confidence Interval (CI) 1.66–5.44, p = 2.7E-4] and multivariate [HR: 2.88, 95% CI 1.57–5.2, p = 0.001] analyses. Subset analyses demonstrated that the signature could predict patients who would attain complete or partial remission or no-response to first-line chemotherapy. Pathway analyses revealed that the signature was regulated by HIF1α and TP53 and included nine HIF1α-regulated genes, which were highly expressed in non-responders and partial remission patients than in complete remission patients. We present the 97-gene signature as an accurate prognostic predictor of overall survival and chemoresponse. Our signature also provides information on potential candidate target genes for future treatment efforts in ovarian cancer.

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Section: Discussionmentioning

confidence: 99%

The Prognostic 97 Chemoresponse Gene Signature in Ovarian Cancer

Matondo

Shahid

et al. 2017

Sci Rep

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“…Notably, one report demonstrated that Nur77 is involved in the migration of transforming growth factor-β-induced breast cancer cells ( 32 ); furthermore, this process is dependent on p38α ( 33 ). Delgado et al ( 34 ) reported that the expression of Nur77 in ovaries was high relative to that in other tissues, with only skeletal muscle and tracheal tissue having higher levels of expression than the ovaries. In normal ovarian tissues, Nur77 is predominantly localized in the nucleus, whereas in ovarian cancer cell lines and tissues from patients with ovarian cancer, Nur77 is present in the cytoplasm and the nucleus.…”

Section: Structure Expression and Localization Of Nur77mentioning

confidence: 99%

“…In normal ovarian tissues, Nur77 is predominantly localized in the nucleus, whereas in ovarian cancer cell lines and tissues from patients with ovarian cancer, Nur77 is present in the cytoplasm and the nucleus. In addition, Nur77 was shown to be expressed at high levels in samples from a subset of patients with high-grade serous ovarian cancer, who had a poor progression-free survival rate ( 34 ), suggesting that Nur77 mediates the growth of cancer cells. Furthermore, Zhang et al ( 35 ) demonstrated that the expression of Nur77 was markedly reduced in the placenta of women with preeclampsia compared with placental levels during a normal pregnancy, and that Nur77 may also be involved in regulating trophoblast cell motility.…”

Section: Structure Expression and Localization Of Nur77mentioning

confidence: 99%

Characteristics of Nur77 and its ligands as potential anticancer compounds (Review)

Chen

2018

Mol Med Report

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Nuclear receptor subfamily 4 group A member 1 (NR4A1; also termed Nur77/TR3/NGFIB), a member of the nuclear receptor superfamily, is expressed as an early response gene to regulate the expression of multiple target genes. Nur77 has the typical structure of a nuclear receptor, including an N-terminal domain, a DNA binding domain, and a ligand-binding domain. The expression and localization of Nur77 are closely associated with its roles in cell proliferation and apoptosis. Nur77 was first identified as an orphan receptor, the endogenous ligand of which has not yet been identified; however, an increasing number of compounds targeting Nur77 have been reported to have beneficial effects in the treatment of cancer and other diseases. This review provides a brief overview of the identification, structure, expression and localization, transcriptional role and non-genomic function of Nur77, and summarizes the ligands that have been shown to interact with Nur77, including cytosporone B, cisplatin, TMPA, PDNPA, CCE9, THPN, Z-ligustilide, celastrol and bisindole methane compounds, which may potentially be used to treat cancer in humans.

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“…These receptors are early immediate genes induced by multiple stimuli and there is increasing evidence that NR4A receptors are potential drug targets for many diseases including cancer (4–7). Among the NR4A receptors, there has been extensive research on the expression and role of NR4A1 in cancer and one study found the loss of both NR4A1 and NR4A2 in mice results in hematological malignancies (8), suggesting tumor suppressor-like activity for NR4A1. In contrast, NR4A1 exhibits tumor promoter activity (6,7) in solid tumors.…”

Section: Introductionmentioning

confidence: 99%

PAX3-FOXO1A Expression in Rhabdomyosarcoma Is Driven by the Targetable Nuclear Receptor NR4A1

2017

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Alveolar rhabdomyosarcoma (ARMS) is a devastating pediatric disease driven by expression of the oncogenic fusion gene PAX3-FOXO1A. In this study, we report overexpression of the nuclear receptor NR4A1 is rhabdomyosarcomas which is sufficient to drive high expression of PAX3-FOXO1A there. RNAi-mediated silencing of NR4A1 decreased expression of PAX3-FOXO1A and its downstream effector genes. Similarly, cell treatment with the NR4A1 small molecule antagonists 1,1-bis(3-indolyl)-1-(p-hydroxy or p-carbomethoxyphenyl)methane (C-DIM) decreased PAX3-FOXO1A. Mechanistic investigations revealed a requirement for the NR4A1/Sp4 complex to bind GC-rich promoter regions to elevate transcription of the PAX3-FOXO1A gene. In parallel, NR4A1 also regulated expression of β1-integrin which with PAX3-FOXO1A contributed to tumor cell migration that was blocked by C-DIM/NR4A1 antagonists. Taken together, our results provide a preclinical rationale for the use of NR4A1 small molecule antagonists to treat ARMS and other rhabdomyosarcomas driven by PAX3-FOXO1A.

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High expression of orphan nuclear receptor NR4A1 in a subset of ovarian tumors with worse outcome

Cited by 21 publications

References 41 publications

The Prognostic 97 Chemoresponse Gene Signature in Ovarian Cancer

The Prognostic 97 Chemoresponse Gene Signature in Ovarian Cancer

Characteristics of Nur77 and its ligands as potential anticancer compounds (Review)

PAX3-FOXO1A Expression in Rhabdomyosarcoma Is Driven by the Targetable Nuclear Receptor NR4A1

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