Evaluating the evidence for targeting FOXO3a in breast cancer: a systematic review

Taylor, S.; Lam, Matthew; Pararasa, Chathyan; Brown, James E.; Carmichael, Amtul R.; Griffiths, Helen R.

doi:10.1186/s12935-015-0156-6

Cited by 111 publications

(111 citation statements)

References 56 publications

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“…Fourth, S100A7 is responsible for cell detachment induced-anoikis resistance and tumorigenicity in human oral cancer cells. [20,38] Thus, we speculate that YAP and S100A7 might act as the compensatory function depending on cell microenvironment in well differentiated cervical and glossopharyngeal SCC. When these cells are detached or cultured in high density, the Hippo pathway is activated and nuclear YAP is attenuated, which leads to S100A7 induction in order to perform the similar effects as YAP, such as maintenance of cell survival and/or suppression of cell differentiation.…”

Section: Discussionmentioning

confidence: 94%

The Characteristic of S100A7 Induction by the Hippo-YAP Pathway in Cervical and Glossopharyngeal Squamous Cell Carcinoma

Kong

et al. 2016

PLoS ONE

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S100A7 is expressed in many squamous cell carcinomas (SCCs). Our previous study revealed that S100A7 was dramatically induced in several SCC cells and activation of the Hippo pathway significantly promoted S100A7 in epidermoid carcinoma cells. However, whether the Hippo pathway regulates S100A7 expression in SCCs remains largely unknown. Here, we uncover that S100A7 induction by the Hippo-YAP pathway displays different characteristic in cervical and glossopharyngeal SCC. In well differentiated HCC94 cervical cells and FaDu pharyngeal cells, S100A7 is easily induced by both suspension and dense culture, which is accompanied by an increase in YAP phosphorylation and a decrease in nuclear YAP. Strikingly, these correlations of S100A7 and YAP reverse after recovery of cell attachment or relief from dense culture. Further examination finds that S100A7 induction is significantly repressed by nuclear YAP, which is validated by activation or inhibition of the Hippo pathway via loss- and/or gain-of- LATS1 and MST1 function. Subsequently, we prove that TEAD1 is required for YAP transcriptional repression of S100A7. However, S100A7 is hardly induced in poorly differentiated SiHa cervical cells and NCI-H226 pulmonary cells even in suspension or activation of the Hippo pathway. More importantly, cervical and lingual SCC tissues array analyses show that S100A7 expression displays the positive correlation with pYAP-S127 and the negative correlation with nuclear YAP in the majority of well differentiated but not in poorly differentiated tissues. Collectively, our findings demonstrate that the different induction of S100A7 toward activation of the Hippo pathway mainly depends on the degree of cell differentiation in cervical and glossopharyngeal SCC.

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Section: Discussionmentioning

confidence: 94%

The Characteristic of S100A7 Induction by the Hippo-YAP Pathway in Cervical and Glossopharyngeal Squamous Cell Carcinoma

Kong

et al. 2016

PLoS ONE

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“…While PPARc is upstream of many of the effectors that are influenced by BAR, the PPARc agonist rosiglitazone did not recapitulate the effects of BAR on gene expression or prevent loss of metabolic activity. Others have shown that FOXO3a is a target for triterpenoids in cancer [15,37].…”

Section: Discussionmentioning

confidence: 99%

“…A number of existing BC drugs target PI3K/AKT [15]. Although the mechanism for the anticancer activities of BAR are not fully understood, many signaling pathways, including mitochondrial regulation via the KEAP1/Nrf2 pathway and glycolytic regulation via the PI3K/mTOR pathway, have been implicated in the anticancer effects of BAR [16].…”

Section: Introductionmentioning

confidence: 99%

Bardoxolone-methyl inhibits migration and metabolism in MCF7 cells

Refaat

Pararasa

Arif

et al. 2017

Free Radical Research

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Bardoxolone-methyl (BAR) is reported to have anti-inflammatory, anti-proliferative and anti-fibrotic effects. BAR activates Nrf2 and may ameliorate oxidative stress through induction of antioxidant genes. However, off-target effects, probably concentration and NFkB-dependent, have limited the clinical use of BAR. Nrf2 regulates expression of antioxidant and mitochondrial genes and has been proposed as a target for both obesity and breast cancer. Therefore, we explored whether BAR can alter migration and proliferation in the MCF7 cell line and whether metabolic function is affected by BAR. Incubation with BAR caused a time-dependent migratory inhibition and an associated decrease in mitochondrial respiration. Both migratory and mitochondrial inhibition by BAR were further enhanced in the presence of fatty acids. In addition to the activation of Nrf2, BAR altered the expression of target mRNA GCLC and UCP1. After 24 h, BAR inhibited both glycolytic capacity, reserve (p < 0.05) and oxidative phosphorylation (p < 0.001) with an associated increase in mitochondrial ROS and loss of intracellular glutathione in MCF7 cells; however, impairment of mitochondrial activity was prevented by N-acetyl cysteine. The fatty acid, palmitate, increased mitochondrial ROS, impaired migration and oxidative phosphorylation but palmitate toxicity towards MCF7 could not be inhibited by N-acetyl cysteine suggesting that they exert effects through different pathways. BAR-activated AKT, induced DNA damage and inhibited cell proliferation. When the proteasome was inhibited, there was loss of BAR-mediated changes in p65 phosphorylation and SOD2 expression suggesting non-canonical NFkB signaling effects. These data suggest that BAR-induced ROS are important in inhibiting MCF7 migration and metabolism by negatively affecting glycolytic capacity and mitochondrial function. ARTICLE HISTORY

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“…In TNBC, metabolic dysregulation is driven by factors such as glutathione S-transferase Pi 1 (GSTP1), forkhead box O 3a (FOXO3a), and EGFR-induced c-Myc (43–45). Specifically, c-Myc represses thioredoxin-interacting protein (TXNIP), an inhibitor of glycolytic gene expression and glucose uptake (46).…”

Section: Breast-to-brain Metastasesmentioning

confidence: 99%

Metabolic advantages and vulnerabilities in brain metastases

Ciminera

Jandial

Termini

2017

Clin Exp Metastasis

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Metabolic adaptations permit tumor cells to metastasize to and thrive in the brain. Brain metastases continue to present clinical challenges due to rising incidence and resistance to current treatments. Therefore, elucidating altered metabolic pathways in brain metastases may provide new therapeutic targets for the treatment of aggressive disease. Due to the high demand for glucose in the brain, increased glycolytic activity is favored for energy production. Primary tumors that undergo Warburg-like metabolic reprogramming become suited to growth in the brain microenvironment. Indeed, elevated metabolism is a predictor of metastasis in many cancer subtypes. Specifically, metabolic alterations are seen in primary tumors that are associated with the formation of brain metastases, namely breast cancer, lung cancer, and melanoma. Because of this selective pressure, inhibitors of key metabolic factors may reduce tumor cell viability, thus exploiting metabolic pathways for cancer therapeutics. This review summarizes the metabolic advantages and vulnerabilities of brain metastases.

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Evaluating the evidence for targeting FOXO3a in breast cancer: a systematic review

Cited by 111 publications

References 56 publications

The Characteristic of S100A7 Induction by the Hippo-YAP Pathway in Cervical and Glossopharyngeal Squamous Cell Carcinoma

The Characteristic of S100A7 Induction by the Hippo-YAP Pathway in Cervical and Glossopharyngeal Squamous Cell Carcinoma

Bardoxolone-methyl inhibits migration and metabolism in MCF7 cells

Metabolic advantages and vulnerabilities in brain metastases

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