FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2726191260> ?p ?o ?g. }

• W2726191260 abstract "Introduction - The normal process of epithelial mesenchymal transition (EMT) is subverted by carcinoma cells to facilitate metastatic spread. Cancer cells rarely undergo a full conversion to the mesenchymal phenotype, and instead adopt positions along the epithelial-mesenchymal axis, a propensity we refer to as epithelial mesenchymal plasticity (EMP). EMP is associated with increased risk of metastasis in breast cancer and consequent poor prognosis. Drivers towards the mesenchymal state in malignant cells include growth factor stimulation or exposure to hypoxic conditions. Methods - We have examined EMP in two cell line models of breast cancer: the PMC42 system (PMC42-ET and PMC42-LA sublines) and MDA-MB-468 cells. Transition to a mesenchymal phenotype was induced across all three cell lines using epidermal growth factor (EGF) stimulation, and in MDA-MB-468 cells by hypoxia. We used RNA sequencing to identify gene expression changes that occur as cells transition to a more-mesenchymal phenotype, and identified the cell signalling pathways regulated across these experimental systems. We then used inhibitors to modulate signalling through these pathways, verifying the conclusions of our transcriptomic analysis. Results - We found that EGF and hypoxia both drive MDA-MB-468 cells to phenotypically similar mesenchymal states. Comparing the transcriptional response to EGF and hypoxia, we have identified differences in the cellular signalling pathways that mediate, and are influenced by, EMT. Significant differences were observed for a number of important cellular signalling components previously implicated in EMT, such as HBEGF and VEGFA. We have shown that EGF- and hypoxia-induced transitions respond differently to treatment with chemical inhibitors (presented individually and in combinations) in these breast cancer cells. Unexpectedly, MDA-MB-468 cells grown under hypoxic growth conditions became even more mesenchymal following exposure to certain kinase inhibitors that prevent growth-factor induced EMT, including the mTOR inhibitor everolimus and the AKT1/2/3 inhibitor AZD5363. Conclusions - While resulting in a common phenotype, EGF and hypoxia induced subtly different signalling systems in breast cancer cells. Our findings have important implications for the use of kinase inhibitor-based therapeutic interventions in breast cancers, where these heterogeneous signalling landscapes will influence the therapeutic response. © 2015 Cursons et al.; licensee BioMed Central." @default.
• W2726191260 created "2017-07-14" @default.
• W2726191260 creator A5002033152 @default.
• W2726191260 creator A5004957581 @default.
• W2726191260 creator A5011259254 @default.
• W2726191260 creator A5018252802 @default.
• W2726191260 creator A5048486605 @default.
• W2726191260 creator A5049570974 @default.
• W2726191260 creator A5051916558 @default.
• W2726191260 creator A5055292298 @default.
• W2726191260 creator A5061492074 @default.
• W2726191260 creator A5075948104 @default.
• W2726191260 creator A5083478373 @default.
• W2726191260 date "2015-11-03" @default.
• W2726191260 modified "2023-09-23" @default.
• W2726191260 title "Stimulus-dependent differences in signalling regulate epithelial-mesenchymal plasticity and change the effects of drugs in breast cancer cell lines" @default.
• W2726191260 doi "https://doi.org/10.7490/f1000research.1110933.1" @default.
• W2726191260 hasPublicationYear "2015" @default.
• W2726191260 type Work @default.
• W2726191260 sameAs 2726191260 @default.
• W2726191260 citedByCount "0" @default.
• W2726191260 crossrefType "journal-article" @default.
• W2726191260 hasAuthorship W2726191260A5002033152 @default.
• W2726191260 hasAuthorship W2726191260A5004957581 @default.
• W2726191260 hasAuthorship W2726191260A5011259254 @default.
• W2726191260 hasAuthorship W2726191260A5018252802 @default.
• W2726191260 hasAuthorship W2726191260A5048486605 @default.
• W2726191260 hasAuthorship W2726191260A5049570974 @default.
• W2726191260 hasAuthorship W2726191260A5051916558 @default.
• W2726191260 hasAuthorship W2726191260A5055292298 @default.
• W2726191260 hasAuthorship W2726191260A5061492074 @default.
• W2726191260 hasAuthorship W2726191260A5075948104 @default.
• W2726191260 hasAuthorship W2726191260A5083478373 @default.
• W2726191260 hasConcept C104317684 @default.
• W2726191260 hasConcept C121608353 @default.
• W2726191260 hasConcept C127716648 @default.
• W2726191260 hasConcept C150194340 @default.
• W2726191260 hasConcept C162317418 @default.
• W2726191260 hasConcept C198826908 @default.
• W2726191260 hasConcept C2776362946 @default.
• W2726191260 hasConcept C2779013556 @default.
• W2726191260 hasConcept C502942594 @default.
• W2726191260 hasConcept C54355233 @default.
• W2726191260 hasConcept C76419328 @default.
• W2726191260 hasConcept C81885089 @default.
• W2726191260 hasConcept C86803240 @default.
• W2726191260 hasConcept C95444343 @default.
• W2726191260 hasConcept C96232424 @default.
• W2726191260 hasConceptScore W2726191260C104317684 @default.
• W2726191260 hasConceptScore W2726191260C121608353 @default.
• W2726191260 hasConceptScore W2726191260C127716648 @default.
• W2726191260 hasConceptScore W2726191260C150194340 @default.
• W2726191260 hasConceptScore W2726191260C162317418 @default.
• W2726191260 hasConceptScore W2726191260C198826908 @default.
• W2726191260 hasConceptScore W2726191260C2776362946 @default.
• W2726191260 hasConceptScore W2726191260C2779013556 @default.
• W2726191260 hasConceptScore W2726191260C502942594 @default.
• W2726191260 hasConceptScore W2726191260C54355233 @default.
• W2726191260 hasConceptScore W2726191260C76419328 @default.
• W2726191260 hasConceptScore W2726191260C81885089 @default.
• W2726191260 hasConceptScore W2726191260C86803240 @default.
• W2726191260 hasConceptScore W2726191260C95444343 @default.
• W2726191260 hasConceptScore W2726191260C96232424 @default.
• W2726191260 hasLocation W27261912601 @default.
• W2726191260 hasOpenAccess W2726191260 @default.
• W2726191260 hasPrimaryLocation W27261912601 @default.
• W2726191260 hasRelatedWork W1574291767 @default.
• W2726191260 hasRelatedWork W1747528388 @default.
• W2726191260 hasRelatedWork W1853333644 @default.
• W2726191260 hasRelatedWork W1967170442 @default.
• W2726191260 hasRelatedWork W1987656608 @default.
• W2726191260 hasRelatedWork W2058443035 @default.
• W2726191260 hasRelatedWork W2064921823 @default.
• W2726191260 hasRelatedWork W2069053195 @default.
• W2726191260 hasRelatedWork W2093148809 @default.
• W2726191260 hasRelatedWork W2151756364 @default.
• W2726191260 hasRelatedWork W2326637203 @default.
• W2726191260 hasRelatedWork W2409208261 @default.
• W2726191260 hasRelatedWork W2465821720 @default.
• W2726191260 hasRelatedWork W2576512904 @default.
• W2726191260 hasRelatedWork W2826708737 @default.
• W2726191260 hasRelatedWork W2883265098 @default.
• W2726191260 hasRelatedWork W2989690384 @default.
• W2726191260 hasRelatedWork W3098004644 @default.
• W2726191260 hasRelatedWork W91582749 @default.
• W2726191260 hasRelatedWork W2181528366 @default.
• W2726191260 hasVolume "4" @default.
• W2726191260 isParatext "false" @default.
• W2726191260 isRetracted "false" @default.
• W2726191260 magId "2726191260" @default.
• W2726191260 workType "article" @default.