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

Wu, Ling Juan; Chen, Liqun

doi:10.3892/mmr.2018.9515

Cited by 47 publications

(46 citation statements)

References 96 publications

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“…NR4A1 (also called Nur77, TR3, or NGFIB) is an orphan nuclear receptor that belongs to the steroid/thyroid/retinoid receptor superfamily (Hazel et al, 1988). NR4A1 contains DNA binding domain (DBD) and ligand binding domain (LBD) (Lin et al, 2004), by which NR4A1 is activated and regulates gene expression (Wu and Chen, 2018). In addition, it plays a significant role in pro-apoptotic function through mitochondrial localization and binding to Bcl-2 (Godoi et al, 2016;Lin et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

A Regulation Loop between YAP and NR4A1 Balances Cell Proliferation and Apoptosis

Yuan

et al. 2020

Cell Reports

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Section: Introductionmentioning

confidence: 99%

A Regulation Loop between YAP and NR4A1 Balances Cell Proliferation and Apoptosis

Yuan

et al. 2020

Cell Reports

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“…And we found a new target protein Nur77, who play an important role in G-apo A-induced antiangiogenesis. Nur77(NR4A1) is one of the NR4A subfamily, which consists of 3 well conserved members, Nur77, Nurr1 (NR4A2) and NOR-1 (NR4A3), respective [35]. NR4A receptors are immediate-early genes that are regulated by many physiological stimuli including growth factors, hormones, and in ammatory signals and are involved in a wide array of important biological process, including cell apoptosis, brain development, glucose metabolism, and vascular remodeling [36].…”

Section: Discussionmentioning

confidence: 99%

Glycation of Apolipoprotein A-IV Impairs Angiogenesis Through The Orphan Nuclear Receptor Nur77

Liu¹,

Dai²,

Xu³

et al. 2021

Preprint

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Background Apo A-Ⅳ played an key role in Cardiovascular diseases, but the effect and mechanism of glycated apo A-Ⅳ on angiogenesis remains unclear. Methods In this study, we demonstrated that oral administration of glycated apoA-Ⅳ impaired blood perfusion recovery in a mouse hind-limb ischemia model. A reduction in blood perfusion recovery at day 21 was observed in the ischemic tissue of apoA-Ⅳ and glycated apoA-Ⅳ-treated mice. Results In this study, we demonstrated that glycated apo A-Ⅳ impaired blood perfusion recovery in a mouse hind-limb ischemia model. And in vitro study also showed that glycated apo A-Ⅳ inhibited the migration, proliferation, and tube-formation abilities of endothelial cells. Further research revealed that glycated apo A-Ⅳ regulated angiogenesis partly by interrupting Nur77. In addition, CML levels were increased in patients with Lower limb circulation (n = 30) compared with those with no limb circulation(n = 50). Conclusions We found impaired angiogenesis induced by glycated apo A-Ⅳ might contribute to poor coronary collateral growth by inhibit the expression of Nur77.

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“…In normal conditions Nur77 is found in the nucleus but regulated by phosphorylation, which occurs by MAPK and AKT. Phosphorylation of Nur77 drives the abnormal translocation of the transcription factor to the mitochondria where it causes MOMP ensuing cytochrome c release [110]. The activity of this transcription factor in the context of viral protein cancer toxicity has been mostly studied in CAV-Apoptin.…”

Section: Mitochondrial Cell Deathmentioning

confidence: 99%

“…Interestingly, Nur77 is known to interact with Bcl-2 and turn it from anti-to pro-apoptotic which may explain the conflicting results for this protein [111]. Nur77 is also important for HGV-Apoptin as treatment triggers cytoplasmic translocation of Nur77 93 Nevertheless, although less is known about this transcription factor in other viral protein mechanisms, studies have found that Nur77 interacts with an E1A binding partner p300, and the overexpression of E1A can repress Nur77 transactivation [110,112].…”

Section: Mitochondrial Cell Deathmentioning

confidence: 99%

Cancer Treatment Goes Viral: Using Viral Proteins to Induce Tumour-Specific Cell Death

Wyatt

Müller

Tavassoli

2019

Cancers

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Cell death is a tightly regulated process which can be exploited in cancer treatment to drive the killing of the tumour. Several conventional cancer therapies including chemotherapeutic agents target pathways involved in cell death, yet they often fail due to the lack of selectivity they have for tumour cells over healthy cells. Over the past decade, research has demonstrated the existence of numerous proteins which have an intrinsic tumour-specific toxicity, several of which originate from viruses. These tumour-selective viral proteins, although from distinct backgrounds, have several similar and interesting properties. Though the mechanism(s) of action of these proteins are not fully understood, it is possible that they can manipulate several cell death modes in cancer exemplifying the intricate interplay between these pathways. This review will discuss our current knowledge on the topic and outstanding questions, as well as deliberate the potential for viral proteins to progress into the clinic as successful cancer therapeutics.

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

Cited by 47 publications

References 96 publications

A Regulation Loop between YAP and NR4A1 Balances Cell Proliferation and Apoptosis

A Regulation Loop between YAP and NR4A1 Balances Cell Proliferation and Apoptosis

Glycation of Apolipoprotein A-IV Impairs Angiogenesis Through The Orphan Nuclear Receptor Nur77

Cancer Treatment Goes Viral: Using Viral Proteins to Induce Tumour-Specific Cell Death

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