iScience (Dec 2021)

Pharmacological targeting of Sam68 functions in colorectal cancer stem cells

  • Angelique N. Masibag,
  • Christopher J. Bergin,
  • Joshua R. Haebe,
  • Aïcha Zouggar,
  • Muhammad S. Shah,
  • Tamara Sandouka,
  • Amanda Mendes da Silva,
  • François M. Desrochers,
  • Aube Fournier-Morin,
  • Yannick D. Benoit

Journal volume & issue
Vol. 24, no. 12
p. 103442

Abstract

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Summary: Cancer stem cells (CSCs) are documented to play a key role in tumorigenesis and therapy resistance. Despite significant progress in clinical oncology, CSC reservoirs remain elusive and difficult to eliminate. Reverse-turn peptidomimetics were characterized as disruptors of CBP/beta-Catenin interactions and represent a promising avenue to curb hyperactive canonical Wnt/beta-Catenin signaling in CSCs. Recent studies suggested Sam68 as a critical mediator of reverse-turn peptidomimetics response in CSC populations. Using computational and biochemical approaches we confirmed Sam68 as a primary target of reverse-turn peptidomimetics. Furthermore, we executed an in silico drug discovery pipeline to identify yet uncharacterized reverse-turn peptidomimetic structures displaying superior anti-CSC activity in transformed pluripotent and colorectal cancer cell models. Thus, we identified YB-0158 as a reverse-turn peptidomimetic small molecule with enhanced translational potential, altering key hallmarks of human colorectal CSCs in patient-derived ex vivo organoids and in vivo serial tumor transplantation.

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