Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition

Howard, Gregory Caleb; Wang, Jing; Rose, Kristie L; Jones, Camden; Patel, Purvi; Tsui, Tina; Florian, Andrea C; Vlach, Logan; Lorey, Shelly L; Grieb, Brian C; Smith, Brianna N; Slota, Macey J; Reynolds, Elizabeth M; Goswami, Soumita; Savona, Michael R; Mason, Frank M; Lee, Taekyu; Fesik, Stephen; Liu, Qi; Tansey, William P

doi:10.7554/elife.90683

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2024

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Cited by 5 publications

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MDM4 exon skipping upon dysfunctional ribosome assembly

Jansen,

Dobbelstein

2024

Trends in Cell Biology

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MDM4 exon skipping upon dysfunctional ribosome assembly

Jansen,

Dobbelstein

2024

Trends in Cell Biology

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SURF2 is a MDM2 antagonist in triggering the nucleolar stress response

Tagnères,

Santo,

Radermecker

et al. 2024

Nat Commun

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Expanded profiling of WD repeat domain 5 inhibitors reveals actionable strategies for the treatment of hematologic malignancies

Meyer,

Smith,

Wang

et al. 2024

Proc. Natl. Acad. Sci. U.S.A.

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WD40 Repeat Domain 5 (WDR5) is a highly conserved nuclear protein that recruits MYC oncoprotein transcription factors to chromatin to stimulate ribosomal protein gene expression. WDR5 is tethered to chromatin via an arginine-binding cavity known as the “WIN” site. Multiple pharmacological inhibitors of the WDR5-interaction site of WDR5 (WINi) have been described, including those with picomolar affinity and oral bioavailability in mice. Thus far, however, WINi have only been shown to be effective against a number of rare cancer types retaining wild-type p53. To explore the full potential of WINi for cancer therapy, we systematically profiled WINi across a panel of cancer cells, alone and in combination with other agents. We report that WINi are unexpectedly active against cells derived from both solid and blood-borne cancers, including those with mutant p53. Among hematologic malignancies, we find that WINi are effective as a single agent against leukemia and diffuse large B cell lymphoma xenograft models, and can be combined with the approved drug venetoclax to suppress disseminated acute myeloid leukemia in vivo. These studies reveal actionable strategies for the application of WINi to treat blood-borne cancers and forecast expanded utility of WINi against other cancer types.

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Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition

Cited by 5 publications

References 130 publications

MDM4 exon skipping upon dysfunctional ribosome assembly

MDM4 exon skipping upon dysfunctional ribosome assembly

SURF2 is a MDM2 antagonist in triggering the nucleolar stress response

Expanded profiling of WD repeat domain 5 inhibitors reveals actionable strategies for the treatment of hematologic malignancies

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