Clinical & Translational Immunology (Jan 2024)

Targeting CD38 with monoclonal antibodies disrupts key survival pathways in paediatric Burkitt's lymphoma malignant B cells

  • Kathrin Kläsener,
  • Nadja Herrmann,
  • Liliana Håversen,
  • Timothy Sundell,
  • Martina Sundqvist,
  • Christina Lundqvist,
  • Paul T Manna,
  • Charlotte A Jonsson,
  • Marcella Visentini,
  • Diana Ljung Sass,
  • Sarah McGrath,
  • Kristoffer Grimstad,
  • Alaitz Aranburu,
  • Karin Mellgren,
  • Linda Fogelstrand,
  • Huamei Forsman,
  • Olov Ekwall,
  • Jan Borén,
  • Inger Gjertsson,
  • Michael Reth,
  • Inga‐Lill Mårtensson,
  • Alessandro Camponeschi

DOI
https://doi.org/10.1002/cti2.70011
Journal volume & issue
Vol. 13, no. 10
pp. n/a – n/a

Abstract

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Abstract Objectives Paediatric Burkitt's lymphoma (pBL) is the most common childhood non‐Hodgkin B‐cell lymphoma. Despite the encouraging survival rates for most children, treating cases with relapse/resistance to current therapies remains challenging. CD38 is a transmembrane protein highly expressed in pBL. This study investigates the effectiveness of CD38‐targeting monoclonal antibodies (mAbs), daratumumab and isatuximab, in impairing crucial cellular processes and survival pathways in pBL malignant cells. Methods In silico analyses of patient samples, combined with in vitro experiments using the Ramos cell line, were conducted to assess the impact of daratumumab and isatuximab on cellular proliferation, apoptosis and the phosphoinositide 3‐kinase (PI3K) pathway. Results Isatuximab was found to be more effective than daratumumab in disrupting B‐cell receptor signalling, reducing cellular proliferation and inducing apoptosis. Additionally, isatuximab caused a significant impairment of the PI3K pathway and induced metabolic reprogramming in pBL cells. The study also revealed a correlation between CD38 and MYC expression levels in pBL patient samples, suggesting CD38 involvement in key oncogenic processes. Conclusion The study emphasises the therapeutic potential of CD38‐targeting mAbs, particularly isatuximab, in pBL.

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