Transcriptomics

Dataset Information

0

Epithelial mesenchymal transition using doxycycline-inducible Snail, Zeb1, TGFbeta or Vector in H358 NSCLC cell line

ABSTRACT: Epithelial – mesenchymal transition (EMT) is an important contributor to the invasion and metastasis of epithelial-derived cancers. While considerable effort has focused in the regulators involved in the transition process, we have focused on consequences of EMT to prosurvival signaling. Changes in distinct metastable and ‘epigentically-fixed’ EMT states were measured by correlation of protein, phosphoprotein, phosphopeptide and RNA transcript abundance. The assembly of 1167 modulated components into functional systems or machines simplified biological understanding and increased prediction confidence highlighting four functional groups: cell adhesion and migration, metabolism, transcription nodes and proliferation/survival networks. A coordinate metabolic reduction in a cluster of 17 free-radical stress pathway components was observed and correlated with reduced glycolytic and increased oxidative phosphorylation enzyme capacity, consistent with reduced cell cycling and reduced need for macromolecular biosynthesis in the mesenchymal state. An attenuation of EGFR autophosphorylation and a switch from autocrine to paracrine-competent EGFR signaling was implicated in the enablement of tumor cell chemotaxis. A similar attenuation of IGF1R, MET and RON signaling with EMT was observed. In contrast, EMT increased prosurvival autocrine IL11/IL6-JAK2-STAT signaling, autocrine fibronectin-integrin activation, autocrine Axl/Tyro3/PDGFR/FGFR RTK signaling and autocrine TGF-R signaling. A relatively uniform loss of polarity and cell-cell junction linkages to actin cytoskeleton and intermediate filaments was measured at a systems level. A more heterogeneous gain of ECM remodeling and associated with invasion and migration was observed. Correlation to stem cell, EMT, invasion and metastasis datasets revealed the greatest similarity with normal and cancerous breast stem cell populations, CD49fhi/EpCAM-/lo and CD44hi/CD24lo respectively. Thomson, S., Petti, F., Sujka-Kwok, I., Mercado, P., Bean, J., Monaghan, M., Seymour, S.L., Argast, G., Epstein, D. and Haley, J.D. (2011). ‘A systems view of epithelial - mesenchymal transition signaling states’ Clin. Exp. Metastasis 28, 137-55.

ORGANISM(S): Homo sapiens

PROVIDER: GSE125113 | GEO | 2019/01/16

REPOSITORIES: GEO

Json Xml

Similar Datasets

Transcriptomics Genome-wide identification of transcripts associated with lncRNA-ATB by RIP-seq
2014-02-08 | E-GEOD-54799 | biostudies-arrayexpress
Models Regan2022 - Mechanosensitive EMT model with autocrine TGFbeta signaling
2023-12-13 | MODEL2208050002 | BioModels
Models Selvaggio2020 - Microenvironment control of hybrid Epithelial-Mesenchymal phenotypes
2020-06-30 | MODEL2004040001 | BioModels
Other Genome-wide identification of transcripts associated with lncRNA-ATB by RIP-seq
2014-02-08 | GSE54799 | GEO
Transcriptomics Cellular and extracellular vesicle RNA sequence for E-cadherin-RFP EMT reporter system expressing mouse breast cancer cell line Py2T during EMT/MET
2020-12-31 | E-MTAB-9750 | biostudies-arrayexpress
Transcriptomics Gene expression changes in a breast cancer stem cell model.
2014-06-22 | E-GEOD-53266 | biostudies-arrayexpress
Proteomics CD44 regulates epigenetic plasticity by mediating iron endocytosis - part 1
2019-10-01 | PXD011447 | Pride
Metabolomics EMT alterations in the solute carrier landscape uncover SLC22A10/A15 imposed vulnerabilities in pancreatic cancer
2021-10-15 | MTBLS1925 | MetaboLights
Transcriptomics Epithelial-to-Mesenchymal Transition of Murine PTEN-/- Liver Tumor Cells Promotes Tumor Growth and Invasion
2010-05-28 | E-GEOD-18255 | biostudies-arrayexpress
Proteomics CD44 regulates epigenetic plasticity by mediating iron endocytosis - part 2
2010-10-09 | PXD012862 | Pride