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Keywords {🔍}

cell, death, doi, figure, ferroptosis, necrosis, mefs, amino, transferrin, google, scholar, pubmed, starvation, activity, serum, serumdependent, treated, pmc, glutaminolysis, acid, cells, fbs, article, hrs, cellular, cystine, free, measured, lgln, glutamine, subsequently, protein, induce, inhibitor, induced, injury, glutathione, killing, gls, apoptosis, process, viability, difbs, acids, essential, rip, compound, levels, nature, required,

Topics {✒️}

l-g-glutamyl-p-nitroanilide amino acid/serum-free medium iron-free bovine apo-transferrin ischemia/reperfusion-induced organ damage pan-caspase inhibitor zvad-fmk amino acid/serum-double starvation trigger serum-dependent necrosis amino acid-free medium maldi-tof-ms/ms amino acid-free conditions inhibited serum-dependent necrosis bax/bak-double knockout seemingly counter-intuitive observations confocal time-lapse imaging pmc beta search recombinant human holo-transferrin inhibit serum-dependent necrosis inhibit serum-induced necrosis block serum-dependent necrosis gamma-glutamylcysteine synthetase deficiency rip3-dependent necrosis pathway gamma-glutamyl cysteine synthetase full experimental procedures genotype-selective antitumor agents serum-induced cell death stable free radical ischemia-reperfusion heart injury reverse phase-c18 hplc reversed phase xdb-c18 ngamma-aryl glutamine analogues tumor necrosis factor-α downstream necrotic response blocked erastin-induced ferroptosis supplementary materials included aldose reductase pathway rat kidney-type glutaminase gamma-glutamylcysteine synthetase gene cell type-dependent manner reduce ischemia-reperfusion injuries rip3-indepednent cell death death-inducing activity ranged ras-erk signaling mechanisms controlling iron-loading growth/survival factors function glutamine dose-dependent manner inhibit erastin-induced ferroptosis unpaired student t-test mitochondrial oxidative phosphorylation nutrient/growth factor deprivation cystine/glutamate antiporter slc7a11

Questions {❓}

• Does serum-dependent necrosis require deprivation of all amino acids or certain specific amino acid(s)?
• How do transferrin, cellular glutaminolysis, glutathione synthesis, and cellular ROS generation process communicate with each other to lead to cell death?
• In light of our finding that ferroptosis requires glutaminolysis, a metabolic pathway highly active in cancer tissues and essential for cancer growth, can ferroptosis be preferentially triggered in cancer cells as a therapeutic option?
• Under what biological conditions can ferroptosis, a necrotic process induced experimentally by cystine starvation or blockage of cystine uptake, occur?

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