Molecular Therapy: Oncology (Sep 2024)

Co-stimulation of CD28/CD40 signaling molecule potentiates CAR-T cell efficacy and stemness

  • Wannakorn Khopanlert,
  • Pongsakorn Choochuen,
  • Kajornkiat Maneechai,
  • Nawaphat Jangphattananont,
  • Socheatraksmey Ung,
  • Shingo Okuno,
  • Peter Steinberger,
  • Judith Leitner,
  • Surasak Sangkhathat,
  • Pongtep Viboonjuntra,
  • Seitaro Terakura,
  • Jakrawadee Julamanee

Journal volume & issue
Vol. 32, no. 3
p. 200837

Abstract

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CD19 chimeric antigen receptor T (CD19CAR-T) cells have achieved promising outcomes in relapsed/refractory B cell malignancies. However, recurrences occur due to the loss of CAR-T cell persistence. We developed dual T/B cell co-stimulatory molecules (CD28 and CD40) in CAR-T cells to enhance intense tumoricidal activity and persistence. CD19.28.40z CAR-T cells promoted pNF-κB and pRelB downstream signaling while diminishing NFAT signaling upon antigen exposure. CD19.28.40z CAR-T cells demonstrated greater proliferation, which translated into effective anti-tumor cytotoxicity in long-term co-culture assay. Repetitive weekly antigen stimulation unveiled continuous CAR-T cell expansion while preserving central memory T cell subset and lower expression of exhaustion phenotypes. The intrinsic genes underlying CD19.28.40z CAR-T cell responses were compared with conventional CARs and demonstrated the up-regulated genes associated with T cell proliferation and memory as well as down-regulated genes related to apoptosis, exhaustion, and glycolysis pathway. Enrichment of genes toward T cell stemness, particularly SELL, IL-7r, TCF7, and KLF2, was observed. Effective and continuing anti-tumor cytotoxicity in vivo was exhibited in both B cell lymphoblastic leukemia and B cell non-Hodgkin lymphoma xenograft models while demonstrating persistent T cell memory signatures. The functional enhancement of CD37.28.40z CAR-T cell activities against CD37+ tumor cells was further validated. The modification of dual T/B cell signaling molecules remarkably maximized the efficacy of CAR-T cell therapy.

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