The lncRNA SLNCR Recruits the Androgen Receptor to EGR1-Bound Genes in Melanoma and Inhibits Expression of Tumor Suppressor p21

Schmidt, Karyn; Carroll, Johanna S.; Yee, Elaine; Thomas, Dylan C.; Wert-Lamas, León; Neier, Steven C.; Sheynkman, Gloria; Ritz, Justin; Novina, Carl D.

doi:10.1016/j.celrep.2019.04.101

Cited by 60 publications

(48 citation statements)

References 95 publications

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“…Wee1 phosphorylates Cdc2 and suppresses its activity, and p21 is an inhibitor of the cyclin B1/Cdc2 kinase complex. 37) Our data demonstrated increased upregulation of p21 and Wee1 and downregulation of Cdc2 and cyclin B1 at the mRNA and protein levels during G2/M phase arrest in EC-109, Kyse-150 and Kyse-520 cells (Figs. 2, 4) and increased phosphorylation of Cdc2 (Fig.…”

Section: Discussionsupporting

confidence: 55%

Cinobufagin Promotes Cell Cycle Arrest and Apoptosis to Block Human Esophageal Squamous Cell Carcinoma Cells Growth <i>via</i> the p73 Signalling Pathway

Deng¹,

Sheng²,

Liu

et al. 2019

Biological & Pharmaceutical Bulletin

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Cinobufagin isolated from traditional Chinese herbs has antitumour, anaesthetic, analgesic and antiinflammatory effects. Recently, the antitumour activity of cinobufagin has attracted increasing attention from researchers. However, the anticancer activity of this drug on esophageal cancer cells and the precise mechanism are unclear. In this study, we determined the inhibitory effect of cinobufagin on the growth of three esophageal squamous cell carcinoma cell lines and explored its underlying mechanism. EC-109, Kyse-150, and Kyse-520 cells were treated with different concentrations of cinobufagin. The results of the Cell Counting Kit-8 (CCK-8) and clone formation assays showed that cinobufagin significantly reduced cell proliferation in a dose-and time-dependent manner. Also, flow cytometry and Hoechst 33342 staining indicated that the inhibition of growth induced by cinobufagin was mediated by G2/M cell cycle arrest and apoptosis. In addition, the expression of proteins related to cell cycle arrest and apoptosis was assessed by realtime quantitative (q)RT-PCR and Western blot. The results showed that cinobufagin caused G2/M arrest via upregulation of p21 and Wee1 and downregulation of cyclin B1 and Cdc2 at the mRNA and protein levels and induced apoptosis via upregulation of cleaved caspase-3, Puma and Noxa expression and an increased Bax/Bcl-2 ratio. Other data further showed that cinobufagin increased p73 expression and decreased Mdm2 expression, whereas p53 expression was not significantly changed. Taken together, these results suggest that growth inhibition of cinobufagin in esophageal cancer cells might act through the p73 pathway and its downstream molecules.

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Section: Discussionsupporting

confidence: 55%

Cinobufagin Promotes Cell Cycle Arrest and Apoptosis to Block Human Esophageal Squamous Cell Carcinoma Cells Growth <i>via</i> the p73 Signalling Pathway

Deng¹,

Sheng²,

Liu

et al. 2019

Biological & Pharmaceutical Bulletin

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“…Long non-coding RNAs (lncRNAs) are newlydiscovered transcripts larger than 200 nucleotides [6][7][8]. Recent research has reported that lncRNAs participate in numerous biological activities, such as apoptosis, cell differentiation and metastasis, thus contributing to cancer progression [9][10][11].…”

Section: Introductionmentioning

confidence: 99%

TEAD4 modulated LncRNA MNX1-AS1 contributes to gastric cancer progression partly through suppressing BTG2 and activating BCL2

et al. 2020

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Background: Gastric cancer (GC) is the third leading cause of cancer-related mortality globally. Long noncoding RNAs (lncRNAs) are dysregulated in obvious malignancies including GC and exploring the regulatory mechanisms underlying their expression is an attractive research area. However, these molecular mechanisms require further clarification, especially upstream mechanisms. Methods: LncRNA MNX1-AS1 expression in GC tissue samples was investigated via microarray analysis and further determined in a cohort of GC tissues via quantitative reverse transcription polymerase chain reaction (qRT-PCR) assays. Cell proliferation and flow cytometry assays were performed to confirm the roles of MNX1-AS1 in GC proliferation, cell cycle regulation, and apoptosis. The influence of MNX1-AS1 on GC cell migration and invasion was explored with Transwell assays. A xenograft tumour model was established to verify the effects of MNX1-AS1 on in vivo tumourigenesis. The TEAD4-involved upstream regulatory mechanism of MNX1-AS1 was explored through ChIP and luciferase reporter assays. The mechanistic model of MNX1-AS1 in regulating gene expression was further detected by subcellular fractionation, FISH, RIP, ChIP and luciferase reporter assays. Results: It was found that MNX1-AS1 displayed obvious upregulation in GC tissue samples and cell lines, and ectopic expression of MNX1-AS1 predicted poor clinical outcomes for patients with GC. Overexpressed MNX1-AS1 expression promoted proliferation, migration and invasion of GC cells markedly, whereas decreased MNX1-AS1 expression elicited the opposite effects. Consistent with the in vitro results, MNX1-AS1 depletion effectively inhibited the growth of xenograft tumour in vivo. Mechanistically, TEAD4 directly bound the promoter region of MNX1-AS1 and stimulated the transcription of MNX1-AS1. Furthermore, MNX1-AS1 can sponge miR-6785-5p to upregulate the expression of BCL2 in GC cells. Meanwhile, MNX1-AS1 suppressed the transcription of BTG2 by recruiting polycomb repressive complex 2 to BTG2 promoter regions. Conclusions: Our findings demonstrate that MNX1-AS1 may be able to serve as a prognostic indicator in GC patients and that TEAD4-activatd MNX1-AS1 can promote GC progression through EZH2/BTG2 and miR-6785-5p/ BCL2 axes, implicating it as a novel and potent target for the treatment of GC.

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“…The 2 0 -FANA-modified oligonucleotides are incompatible with RNase H-mediated cleavage, thereby preventing downregulation of SLNCR1 or other potential off-target RNAs ( Figure S7C; Schmidt et al, 2019). Consistent with a steric-blocking mechanism, these oligonucleotides decrease melanoma proliferation, another cancer phenotype attributed to the interaction of AR and SLNCR1, without decreasing SLNCR1 expression (Schmidt et al, 2019). Both SLNCR1-(antisense) and AR-binding (mimic) oligonucleotides sterically block the AR/SLNCR1 interaction in vitro (Figure 7B).…”

Section: Inhibiting Ar Binding Negates Slncr1-mediated Melanoma Invasionmentioning

confidence: 99%

“…In many cases, RNA-driven AR function promotes oncogenesis (Yang et al, 2013;Zhang et al, 2015). For example, our work has revealed that SLNCR1 increases AR occupancy at the promoter of the gene encoding the matrix metalloproteinase MMP9 to increase melanoma invasion, and regulates AR occupancy at the promoter of many growth-regulatory genes to increase cell proliferation (Schmidt et al, 2016(Schmidt et al, , 2019. Although AR has been implicated in multiple cancers, including prostate, bladder, kidney, lung, liver, pancreatic, thyroid, and breast cancers, the fundamental mechanisms of AR activation in many of these cancers is not well-established (Chang et al, 2014;Kanda et al, 2014;Stanley et al, 2012).…”

Section: Introductionmentioning

confidence: 95%

Targeting the Oncogenic Long Non-coding RNA SLNCR1 by Blocking Its Sequence-Specific Binding to the Androgen Receptor

et al. 2020

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The lncRNA SLNCR Recruits the Androgen Receptor to EGR1-Bound Genes in Melanoma and Inhibits Expression of Tumor Suppressor p21

Abstract: Highlights d SLNCR-AR complexes drive melanoma growth and invasion d SLNCR-AR complexes are recruited to EGR1-bound loci d SLCNR-AR-EGR1 complexes regulate transcription of proliferative genes d EGR1 normally activates p21; SLNCR-AR-EGR1 complexes repress p21

Cited by 60 publications

References 95 publications

Cinobufagin Promotes Cell Cycle Arrest and Apoptosis to Block Human Esophageal Squamous Cell Carcinoma Cells Growth <i>via</i> the p73 Signalling Pathway

Cinobufagin Promotes Cell Cycle Arrest and Apoptosis to Block Human Esophageal Squamous Cell Carcinoma Cells Growth <i>via</i> the p73 Signalling Pathway

TEAD4 modulated LncRNA MNX1-AS1 contributes to gastric cancer progression partly through suppressing BTG2 and activating BCL2

Targeting the Oncogenic Long Non-coding RNA SLNCR1 by Blocking Its Sequence-Specific Binding to the Androgen Receptor

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