Author:
Yang Yandan,Oellerich Thomas,Chen Ping,Bolomsky Arnold,Ceribelli Michele,Häupl Björn,Wright George W.,Phelan James D.,Huang Da Wei,Lord James W.,Van Winkle Callie K.,Yu Xin,Wisnieski Jan,Wang James Q.,Tosto Frances A.,Beck Erin,Wilson Kelli,McKnight Crystal,Travers Jameson,Klumpp-Thomas Carleen,Smith Grace A.,Pittaluga Stefania,Maric Irina,Kazandjian Dickran,Thomas Craig J.,Young Ryan M.
Abstract
AbstractOncogenic mutations within the RAS pathway are common in multiple myeloma (MM), an incurable malignancy of plasma cells. However, the mechanisms of pathogenic RAS signaling in this disease remain enigmatic and difficult to inhibit therapeutically. We employed an unbiased proteogenomic approach to dissect RAS signaling in MM by combining genome-wide CRISPR-Cas9 screening with quantitative mass spectrometry focused on RAS biology. We discovered that mutant isoforms of RAS organized a signaling complex with the amino acid transporter, SLC3A2, and MTOR on endolysosomes, which directly activated mTORC1 by co-opting amino acid sensing pathways. MM tumors with high expression of mTORC1-dependent genes were more aggressive and enriched in RAS mutations, and we detected interactions between RAS and MTOR in MM patient tumors harboring mutant RAS isoforms. Inhibition of RAS-dependent mTORC1 activity synergized with MEK and ERK inhibitors to quench pathogenic RAS signaling in MM cells. This study redefines the RAS pathway in MM and provides a mechanistic and rational basis to target this novel mode of RAS signaling.
Publisher
Cold Spring Harbor Laboratory