Quantitative H2S-mediated protein sulfhydration reveals metabolic reprogramming during the integrated stress response

定量 H2S 介导的蛋白质硫化揭示了综合应激反应过程中的代谢重编程

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作者:Xing-Huang Gao, Dawid Krokowski, Bo-Jhih Guan, Ilya Bederman, Mithu Majumder, Marc Parisien, Luda Diatchenko, Omer Kabil, Belinda Willard, Ruma Banerjee, Benlian Wang, Gurkan Bebek, Charles R Evans, Paul L Fox, Stanton L Gerson, Charles L Hoppel, Ming Liu, Peter Arvan, Maria Hatzoglou

Abstract

The sulfhydration of cysteine residues in proteins is an important mechanism involved in diverse biological processes. We have developed a proteomics approach to quantitatively profile the changes of sulfhydrated cysteines in biological systems. Bioinformatics analysis revealed that sulfhydrated cysteines are part of a wide range of biological functions. In pancreatic β cells exposed to endoplasmic reticulum (ER) stress, elevated H2S promotes the sulfhydration of enzymes in energy metabolism and stimulates glycolytic flux. We propose that transcriptional and translational reprogramming by the integrated stress response (ISR) in pancreatic β cells is coupled to metabolic alternations triggered by sulfhydration of key enzymes in intermediary metabolism.

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