IREI[alpha] RNase-dependent lipid homeostasis promotes survival in Myc- transformed cancers

Introduction The Myc family of proto-oncogenes (MYC, MYCN, MYCL) encodes bHLHZ (basic helix-loop-helix leucine zipper) transcription factors, which regulate thousands of genes coordinating numerous cellular processes, including proliferation, differentiation, self-renewal, [...]
Myc activation is a primary oncogenic event in many human cancers; however, these transcription factors are difficult to inhibit pharmacologically, suggesting that Myc-dependent downstream effectors may be more tractable therapeutic targets. Here, we show that Myc overexpression induces endoplasmic reticulum (ER) stress and engages the inositol-requiring enzyme 1[alpha] (IRE1[alpha])/X-box binding protein 1 (XBP1) pathway through multiple molecular mechanisms in a variety of c- Myc- and N-Myc-dependent cancers. In particular, Myc-overexpressing cells require IRE1[alpha]/XBP1 signaling for sustained growth and survival in vitro and in vivo, dependent on elevated stearoyl-CoA-desaturase 1 (SCD1) activity. Pharmacological and genetic XBP1 inhibition induces Myc-dependent apoptosis, which is alleviated by exogenous unsaturated fatty acids. Of note, SCD1 inhibition phenocopies IRE1[alpha] RNase activity suppression in vivo. Furthermore, IRE1[alpha] inhibition enhances the cytotoxic effects of standard chemotherapy drugs used to treat c-Myc-overexpressing Burkitt's lymphoma, suggesting that inhibiting the IRE1[alpha]/XBP1 pathway is a useful general strategy for treatment of Myc- driven cancers.