Author/Authors :
Chae، نويسنده , , Young Chan and Caino، نويسنده , , M. Cecilia and Lisanti، نويسنده , , Sofia and Ghosh، نويسنده , , Jagadish C. and Dohi، نويسنده , , Takehiko and Danial، نويسنده , , Nika N. and Villanueva، نويسنده , , Jessie and Ferrero، نويسنده , , Stefano and Vaira، نويسنده , , Valentina and Santambrogio، نويسنده , , Luigi and Bosari، نويسنده , , Silvano and Languino، نويسنده , , Lucia R. and Herlyn، نويسنده , , Meenhard and Altieri، نويسنده , , Dario C.، نويسنده ,
Abstract :
Summary
successfully adapt to constantly changing intra- and extracellular environments, but the wirings of this process are still largely elusive. Here, we show that heat-shock-protein-90-directed protein folding in mitochondria, but not cytosol, maintains energy production in tumor cells. Interference with this process activates a signaling network that involves phosphorylation of nutrient-sensing AMP-activated kinase, inhibition of rapamycin-sensitive mTOR complex 1, induction of autophagy, and expression of an endoplasmic reticulum unfolded protein response. This signaling network confers a survival and proliferative advantage to genetically disparate tumors, and correlates with worse outcome in lung cancer patients. Therefore, mitochondrial heat shock protein 90s are adaptive regulators of tumor bioenergetics and tractable targets for cancer therapy.
