Pharmacological inhibition of cystine-glutamate exchange induces endoplasmic reticulum stress and ferroptosis
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Exchange of extracellular cystine for intracellular glutamate by the antiporter system xcâ is implicated in numerous pathologies. Pharmacological agents that inhibit system xcâ activity with high potency have long been sought, but have remained elusive. In this study, we report that the small molecule erastin is a potent, selective inhibitor of system xcâ. RNA sequencing revealed that inhibition of cystineâglutamate exchange leads to activation of an ER stress response and upregulation of CHAC1, providing a pharmacodynamic marker for system xcâ inhibition. We also found that the clinically approved anti-cancer drug sorafenib, but not other kinase inhibitors, inhibits system xcâ function and can trigger ER stress and ferroptosis. In an analysis of hospital records and adverse event reports, we found that patients treated with sorafenib exhibited unique metabolic and phenotypic alterations compared to patients treated with other kinase-inhibiting drugs. Finally, using a genetic approach, ...
创建时间:
2025-06-10



