Frontiers in Oncology (Aug 2022)

Small molecule MMRi62 targets MDM4 for degradation and induces leukemic cell apoptosis regardless of p53 status

  • Rati Lama,
  • Chao Xu,
  • Samuel L. Galster,
  • Javier Querol-García,
  • Scott Portwood,
  • Cory K. Mavis,
  • Federico M. Ruiz,
  • Diana Martin,
  • Jin Wu,
  • Marianna C. Giorgi,
  • Jill Bargonetti,
  • Eunice S. Wang,
  • Francisco J. Hernandez-Ilizaliturri,
  • Gerald B. Koudelka,
  • Sherry R. Chemler,
  • Inés G. Muñoz,
  • Xinjiang Wang

DOI
https://doi.org/10.3389/fonc.2022.933446
Journal volume & issue
Vol. 12

Abstract

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MDM2 and MDM4 proteins are key negative regulators of tumor suppressor p53. MDM2 and MDM4 interact via their RING domains and form a heterodimer polyubiquitin E3 ligase essential for p53 degradation. MDM4 also forms heterodimer E3 ligases with MDM2 isoforms that lack p53-binding domains, which regulate p53 and MDM4 stability. We are working to identify small-molecule inhibitors targeting the RING domain of MDM2-MDM4 (MMRi) that can inactivate the total oncogenic activity of MDM2-MDM4 heterodimers. Here, we describe the identification and characterization of MMRi62 as an MDM4-degrader and apoptosis inducer in leukemia cells. Biochemically, in our experiments, MMRi62 bound to preformed RING domain heterodimers altered the substrate preference toward MDM4 ubiquitination and promoted MDM2-dependent MDM4 degradation in cells. This MDM4-degrader activity of MMRi62 was found to be associated with potent apoptosis induction in leukemia cells. Interestingly, MMRi62 effectively induced apoptosis in p53 mutant, multidrug-resistant leukemia cells and patient samples in addition to p53 wild-type cells. In contrast, MMRi67 as a RING heterodimer disruptor and an enzymatic inhibitor of the MDM2-MDM4 E3 complex lacked MDM4-degrader activity and failed to induce apoptosis in these cells. In summary, this study identifies MMRi62 as a novel MDM2-MDM4-targeting agent and suggests that small molecules capable of promoting MDM4 degradation may be a viable new approach to killing leukemia cells bearing non-functional p53 by apoptosis.

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