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Transcriptomic classification of diffuse large B-cell lymphoma identifies a high-risk activated B-cell-like subpopulation with targetable MYC dysregulation

Author

Listed:
  • Matthew E. Stokes

    (Bristol Myers Squibb)

  • Kerstin Wenzl

    (Mayo Clinic)

  • C. Chris Huang

    (Bristol Myers Squibb)

  • María Ortiz

    (Bristol Myers Squibb)

  • Chih-Chao Hsu

    (Bristol Myers Squibb)

  • Matthew J. Maurer

    (Mayo Clinic)

  • Nicholas Stong

    (Bristol Myers Squibb)

  • Yumi Nakayama

    (Bristol Myers Squibb)

  • Lei Wu

    (Bristol Myers Squibb)

  • Hsiling Chiu

    (Bristol Myers Squibb)

  • Ann Polonskaia

    (Bristol Myers Squibb)

  • Samuel A. Danziger

    (Amazon)

  • Fadi Towfic

    (Prometheus Biosciences)

  • Joel Parker

    (Research Triangle Park)

  • Rebecca L. King

    (Mayo Clinic)

  • Brian K. Link

    (University of Iowa)

  • Susan L. Slager

    (Mayo Clinic
    Mayo Clinic)

  • Vivekananda Sarangi

    (Mayo Clinic)

  • Yan W. Asmann

    (Mayo Clinic)

  • Joseph P. Novak

    (Mayo Clinic)

  • Akshay Sudhindra

    (Bristol Myers Squibb)

  • Stephen M. Ansell

    (Mayo Clinic)

  • Thomas M. Habermann

    (Mayo Clinic)

  • Patrick R. Hagner

    (Bristol Myers Squibb)

  • Grzegorz S. Nowakowski

    (Mayo Clinic)

  • James R. Cerhan

    (Mayo Clinic)

  • Anne J. Novak

    (Mayo Clinic)

  • Anita K. Gandhi

    (Bristol Myers Squibb)

Abstract

Immunochemotherapy has been the mainstay of treatment for newly diagnosed diffuse large B-cell lymphoma (ndDLBCL) yet is inadequate for many patients. In this work, we perform unsupervised clustering on transcriptomic features from a large cohort of ndDLBCL patients and identify seven clusters, one called A7 with poor prognosis, and develop a classifier to identify these clusters in independent ndDLBCL cohorts. This high-risk cluster is enriched for activated B-cell cell-of-origin, low immune infiltration, high MYC expression, and copy number aberrations. We compare and contrast our methodology with recent DLBCL classifiers to contextualize our clusters and show improved prognostic utility. Finally, using pre-clinical models, we demonstrate a mechanistic rationale for IKZF1/3 degraders such as lenalidomide to overcome the low immune infiltration phenotype of A7 by inducing T-cell trafficking into tumors and upregulating MHC I and II on tumor cells, and demonstrate that TCF4 is an important regulator of MYC-related biology in A7.

Suggested Citation

  • Matthew E. Stokes & Kerstin Wenzl & C. Chris Huang & María Ortiz & Chih-Chao Hsu & Matthew J. Maurer & Nicholas Stong & Yumi Nakayama & Lei Wu & Hsiling Chiu & Ann Polonskaia & Samuel A. Danziger & Fa, 2024. "Transcriptomic classification of diffuse large B-cell lymphoma identifies a high-risk activated B-cell-like subpopulation with targetable MYC dysregulation," Nature Communications, Nature, vol. 15(1), pages 1-19, December.
    • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-50830-y
    DOI: 10.1038/s41467-024-50830-y
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