| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2041874 | Cell Reports | 2014 | 12 Pages |
•TORC2/Ypk1 and sphingolipids regulate vacuolar acidification preventing ROS•Sphingolipid depletion results in ROS and activates TORC2/Ypk1 signaling•Impaired Ypk1 activity also results in ROS via aberrant mitochondrial respiration•Regulation of ROS is essential for TORC2/Ypk1-mediated cell growth and survival
SummaryReactive oxygen species (ROS) are produced during normal metabolism and can function as signaling molecules. However, ROS at elevated levels can damage cells. Here, we identify the conserved target of rapamycin complex 2 (TORC2)/Ypk1 signaling module as an important regulator of ROS in the model eukaryotic organism, S. cerevisiae. We show that TORC2/Ypk1 suppresses ROS produced both by mitochondria as well as by nonmitochondrial sources, including changes in acidification of the vacuole. Furthermore, we link vacuole-related ROS to sphingolipids, essential components of cellular membranes, whose synthesis is also controlled by TORC2/Ypk1 signaling. In total, our data reveal that TORC2/Ypk1 act within a homeostatic feedback loop to maintain sphingolipid levels and that ROS are a critical regulatory signal within this system. Thus, ROS sensing and signaling by TORC2/Ypk1 play a central physiological role in sphingolipid biosynthesis and in the maintenance of cell growth and viability.
Graphical AbstractFigure optionsDownload full-size imageDownload as PowerPoint slide
