Haematologica (Sep 2022)

Small-molecule SUMO inhibition for biomarker-informed B-cell lymphoma therapy

  • Uta M. Demel,
  • Matthias Wirth,
  • Schayan Yousefian,
  • Le Zhang,
  • Konstandina Isaakidis,
  • Judith Dönig,
  • Marlitt Böger,
  • Nikita Singh,
  • Hazal Köse,
  • Simon Haas,
  • Stefan Müller,
  • Markus Schick,
  • Ulrich Keller

DOI
https://doi.org/10.3324/haematol.2022.280995
Journal volume & issue
Vol. 108, no. 2

Abstract

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Aberrant activity of the SUMOylation pathway has been associated with MYC overexpression and poor prognosis in aggressive B-cell lymphoma (BCL) and other malignancies. Recently developed small-molecule inhibitors of SUMOylation (SUMOi) target the heterodimeric E1 SUMO activation complex (SAE1/UBA2). Here, we report that activated MYC signaling is an actionable molecular vulnerability in vitro and in a preclinical murine in vivo model of MYC-driven BCL. While SUMOi conferred direct effects on MYC-driven lymphoma cells, SUMO inhibition also resulted in substantial remodeling of various subsets of the innate and specific immunity in vivo. Specifically, SUMOi increased the number of memory B cells as well as cytotoxic and memory T cells, subsets that are attributed a key role within a coordinated anti-tumor immune response. In summary, our data constitute pharmacologic SUMOi as a powerful therapy in a subset of BCL causing massive remodeling of the normal B-cell and T-cell compartment.