JCI Insight (Jul 2022)

MEF2C opposes Notch in lymphoid lineage decision and drives leukemia in the thymus

  • Kirsten Canté-Barrett,
  • Mariska T. Meijer,
  • Valentina Cordo’,
  • Rico Hagelaar,
  • Wentao Yang,
  • Jiyang Yu,
  • Willem K. Smits,
  • Marloes E. Nulle,
  • Joris P. Jansen,
  • Rob Pieters,
  • Jun J. Yang,
  • Jody J. Haigh,
  • Steven Goossens,
  • Jules P.P. Meijerink

Journal volume & issue
Vol. 7, no. 13

Abstract

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Rearrangements that drive ectopic MEF2C expression have recurrently been found in patients with human early thymocyte progenitor acute lymphoblastic leukemia (ETP-ALL). Here, we show high levels of MEF2C expression in patients with ETP-ALL. Using both in vivo and in vitro models of ETP-ALL, we demonstrate that elevated MEF2C expression blocks NOTCH-induced T cell differentiation while promoting a B-lineage program. MEF2C activates a B cell transcriptional program in addition to RUNX1, GATA3, and LMO2; upregulates the IL-7R; and boosts cell survival by upregulation of BCL2. MEF2C and the Notch pathway, therefore, demarcate opposite regulators of B- or T-lineage choices, respectively. Enforced MEF2C expression in mouse or human progenitor cells effectively blocks early T cell differentiation and promotes the development of biphenotypic lymphoid tumors that coexpress CD3 and CD19, resembling human mixed phenotype acute leukemia. Salt-inducible kinase (SIK) inhibitors impair MEF2C activity and alleviate the T cell developmental block. Importantly, this sensitizes cells to prednisolone treatment. Therefore, SIK-inhibiting compounds such as dasatinib are potentially valuable additions to standard chemotherapy for human ETP-ALL.

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