自噬
饥饿
硫代谢
酿酒酵母
硫黄
细胞生物学
激活剂(遗传学)
饥饿反应
程序性细胞死亡
蛋氨酸
抄写(语言学)
新陈代谢
化学
生物化学
生物
基因
细胞凋亡
氨基酸
哲学
有机化学
内分泌学
语言学
作者
Magali Prigent,Hélène Jean-Jacques,Delphine Naquin,Stéphane Chédin,Marie‐Hélène Cuif,Renaud Legouis,Laurent Kuras
标识
DOI:10.1038/s41467-024-51309-6
摘要
Abstract Autophagy is a key lysosomal degradative mechanism allowing a prosurvival response to stresses, especially nutrient starvation. Here we investigate the mechanism of autophagy induction in response to sulfur starvation in Saccharomyces cerevisiae . We found that sulfur deprivation leads to rapid and widespread transcriptional induction of autophagy-related ( ATG ) genes in ways not seen under nitrogen starvation. This distinctive response depends mainly on the transcription activator of sulfur metabolism Met4. Consistently, Met4 is essential for autophagy under sulfur starvation. Depletion of either cysteine, methionine or SAM induces autophagy flux. However, only SAM depletion can trigger strong transcriptional induction of ATG genes and a fully functional autophagic response. Furthermore, combined inactivation of Met4 and Atg1 causes a dramatic decrease in cell survival under sulfur starvation, highlighting the interplay between sulfur metabolism and autophagy to maintain cell viability. Thus, we describe a pathway of sulfur starvation-induced autophagy depending on Met4 and involving SAM as signaling sulfur metabolite.
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