Abstract
Epithelial-to-mesenchymal transition (EMT) relates to many molecular and cellular alterations that occur when epithelial cells undergo a switch in differentiation generating mesenchymal-like cells with newly acquired migratory and invasive properties. In cancer cells, EMT leads to drug resistance and metastasis. Moreover, differences in genetic backgrounds, even between patients with the same type of cancer, also determine resistance to some treatments. Metabolic rewiring is essential to induce EMT, hence it is important to identify key metabolic elements for this process, which can be later used to treat cancer cells with different genetic backgrounds. Here we used a mathematical modeling approach to determine which are the metabolic reactions altered after induction of EMT, based on metabolomic and transcriptional data of three non-small cell lung cancer (NSCLC) cell lines. The model suggested that the most affected pathways were the Krebs cycle, amino acid metabolism, and glutathione metabolism. However, glutathione metabolism had many alterations either on the metabolic reactions or at the transcriptional level in the three cell lines. We identified Glutamate-cysteine ligase (GCL), a key enzyme of glutathione synthesis, as an important common feature that is dysregulated after EMT. Analyzing survival data of men with lung cancer, we observed that patients with mutations in GCL catalytic subunit (GCLC) or Glutathione peroxidase 1 (GPX1) genes survived less time than people without mutations on these genes. Besides, patients with low expression of ANPEP, GPX3 and GLS genes also survived less time than those with high expression. Hence, we propose that glutathione metabolism and glutathione itself could be good targets to delay or potentially prevent EMT induction in NSCLC cell lines.
Highlights
Epithelial-mesenchymal transition (EMT) is a natural cellular phenomenon that converts epithelial cells to mesenchymal-like, giving them motile, and invasive properties [1]
These results suggested that glutathione metabolism plays an important role during Epithelial-to-mesenchymal transition (EMT), we looked for survival data of lung cancer patients to observe the significance of these genes
Despite EMT being experimentally triggered with TGF-β in all the cell lines, we found a lot of differences in metabolic concentration profiles
Summary
Epithelial-mesenchymal transition (EMT) is a natural cellular phenomenon that converts epithelial cells to mesenchymal-like, giving them motile, and invasive properties [1]. This process induces changes at different cellular levels, such as morphology (loss of apical-basal polarity), surface markers (cadherins), cytoskeleton (production of vimentin), transcriptional factors (Twist, Snail), miRNAs (miR-200), and metabolic pathways, among others [2, 3]. EMT is a general phenomenon among many cancers, the cellular context and genetic background determine how this process is carried out [4]. Only specific enzymes and metabolites have been recognized as necessary for EMT induction [3, 5, 6], and most of them in specific genetic backgrounds and conditions
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