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Pevonedistat (MLN4924): mechanism of cell death induction and therapeutic potential in colorectal cancer

Jennifer S. Ferris, Margarita Espona‐Fiedler, Claudia Hamilton, Caitriona Holohan, Nyree Crawford, Alex J. McIntyre, Jamie Z. Roberts, Mark Wappett, Simon S. McDade, Daniel B. Longley, Victoria Coyle

2020Cell Death Discovery42 citationsDOIOpen Access PDF

Abstract

Abstract Pevonedistat (MLN4924), a selective inhibitor of the NEDD8-activating enzyme E1 regulatory subunit (NAE1), has demonstrated significant therapeutic potential in several malignancies. Although multiple mechanisms-of-action have been identified, how MLN4924 induces cell death and its potential as a combinatorial agent with standard-of-care (SoC) chemotherapy in colorectal cancer (CRC) remains largely undefined. In an effort to understand MLN4924-induced cell death in CRC, we identified p53 as an important mediator of the apoptotic response to MLN4924. We also identified roles for the extrinsic (TRAIL-R2/caspase-8) and intrinsic (BAX/BAK) apoptotic pathways in mediating the apoptotic effects of MLN4924 in CRC cells, as well as a role for BID, which modulates a cross-talk between these pathways. Depletion of the anti-apoptotic protein FLIP, which we identify as a novel mediator of resistance to MLN4924, enhanced apoptosis in a p53-, TRAIL-R2/DR5-, and caspase-8-dependent manner. Notably, TRAIL-R2 was involved in potentiating the apoptotic response to MLN4924 in the absence of FLIP, in a ligand-independent manner. Moreoever, when paired with SoC chemotherapies, MLN4924 demonstrated synergy with the irinotecan metabolite SN38. The cell death induced by MLN4924/SN38 combination was dependent on activation of mitochondria through BAX/BAK, but in a p53-independent manner, an important observation given the high frequency of TP53 mutation(s) in advanced CRC. These results uncover mechanisms of cell death induced by MLN4924 and suggest that this second-generation proteostasis-disrupting agent may have its most widespread activity in CRC, in combination with irinotecan-containing treatment regimens.

Topics & Concepts

Mechanism (biology)Colorectal cancerProgrammed cell deathCancer researchMedicineCancerOncologyInternal medicineBiologyApoptosisBiochemistryEpistemologyPhilosophyUbiquitin and proteasome pathwaysPlant biochemistry and biosynthesisNuclear Structure and Function
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