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SMARCB1 regulates a TFCP2L1-MYC transcriptional switch promoting renal medullary carcinoma transformation and ferroptosis resistance

Author

Listed:
  • Bujamin H. Vokshi

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA)

  • Guillaume Davidson

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA)

  • Nassim Tawanaie Pour Sedehi

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA)

  • Alexandra Helleux

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA)

  • Marc Rippinger

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA)

  • Alexandre R. Haller

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA)

  • Justine Gantzer

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA
    Institut de Cancérologie Strasbourg Europe)

  • Jonathan Thouvenin

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA
    Institut de Cancérologie Strasbourg Europe)

  • Philippe Baltzinger

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA)

  • Rachida Bouarich

    (INSERM U830, Équipe Labellisée LNCC, Diversity and Plasticity of Childhood Tumors Lab, Institut Curie Research Centre)

  • Valeria Manriquez

    (INSERM U830, Équipe Labellisée LNCC, Diversity and Plasticity of Childhood Tumors Lab, Institut Curie Research Centre)

  • Sakina Zaidi

    (INSERM U830, Équipe Labellisée LNCC, Diversity and Plasticity of Childhood Tumors Lab, Institut Curie Research Centre)

  • Priya Rao

    (The University of Texas MD Anderson Cancer Center)

  • Pavlos Msaouel

    (The University of Texas MD Anderson Cancer Center)

  • Xiaoping Su

    (The University of Texas MD Anderson Cancer Center)

  • Hervé Lang

    (CHRU Strasbourg, Strasbourg University)

  • Thibault Tricard

    (CHRU Strasbourg, Strasbourg University)

  • Véronique Lindner

    (CHRU Strasbourg, Strasbourg University)

  • Didier Surdez

    (Balgrist University Hospital, University of Zurich
    INSERM, U830, Pediatric Translational Research, PSL Research University, SIREDO Oncology Center, Institut Curie)

  • Jean-Emmanuel Kurtz

    (Institut de Cancérologie Strasbourg Europe)

  • Franck Bourdeaut

    (INSERM U830, Équipe Labellisée LNCC, Diversity and Plasticity of Childhood Tumors Lab, Institut Curie Research Centre)

  • Nizar M. Tannir

    (The University of Texas MD Anderson Cancer Center)

  • Irwin Davidson

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA
    ‘Équipe Labellisée’ Ligue National contre le Cancer)

  • Gabriel G. Malouf

    (Institute of Genetics and Molecular and Cellular Biology, CNRS/INSERM/UNISTRA
    Institut de Cancérologie Strasbourg Europe
    ‘Équipe Labellisée’ Ligue National contre le Cancer)

Abstract

Renal medullary carcinoma (RMC) is an aggressive tumour driven by bi-allelic loss of SMARCB1 and tightly associated with sickle cell trait. However, the cell-of-origin and oncogenic mechanism remain poorly understood. Using single-cell sequencing of human RMC, we defined transformation of thick ascending limb (TAL) cells into an epithelial-mesenchymal gradient of RMC cells associated with loss of renal epithelial transcription factors TFCP2L1, HOXB9 and MITF and gain of MYC and NFE2L2-associated oncogenic and ferroptosis resistance programs. We describe the molecular basis for this transcriptional switch that is reversed by SMARCB1 re-expression repressing the oncogenic and ferroptosis resistance programs leading to ferroptotic cell death. Ferroptosis resistance links TAL cell survival with the high extracellular medullar iron concentrations associated with sickle cell trait, an environment propitious to the mutagenic events associated with RMC development. This unique environment may explain why RMC is the only SMARCB1-deficient tumour arising from epithelial cells, differentiating RMC from rhabdoid tumours arising from neural crest cells.

Suggested Citation

  • Bujamin H. Vokshi & Guillaume Davidson & Nassim Tawanaie Pour Sedehi & Alexandra Helleux & Marc Rippinger & Alexandre R. Haller & Justine Gantzer & Jonathan Thouvenin & Philippe Baltzinger & Rachida B, 2023. "SMARCB1 regulates a TFCP2L1-MYC transcriptional switch promoting renal medullary carcinoma transformation and ferroptosis resistance," Nature Communications, Nature, vol. 14(1), pages 1-19, December.
    • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-38472-y
    DOI: 10.1038/s41467-023-38472-y
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