Blood Advances (Aug 2017)

Patient-derived antibody recognizes a unique CD43 epitope expressed on all AML and has antileukemia activity in mice

  • Marijn A. Gillissen,
  • Greta de Jong,
  • Martijn Kedde,
  • Etsuko Yasuda,
  • Sophie E. Levie,
  • Gemma Moiset,
  • Paul J. Hensbergen,
  • Arjen Q. Bakker,
  • Koen Wagner,
  • Jullien Villaudy,
  • Pauline M. van Helden,
  • Hergen Spits,
  • Mette D. Hazenberg

Journal volume & issue
Vol. 1, no. 19
pp. 1551 – 1564

Abstract

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Abstract: Immunotherapy has proven beneficial in many hematologic and nonhematologic malignancies, but immunotherapy for acute myeloid leukemia (AML) and myelodysplastic syndrome (MDS) is hampered by the lack of tumor-specific targets. We took advantage of the tumor-immunotherapeutic effect of allogeneic hematopoietic stem cell transplantation and searched the B-cell repertoire of a patient with a lasting and potent graft-versus-AML response for the presence of AML-specific antibodies. We identified an antibody, AT1413, that was of donor origin and that specifically recognizes a novel sialylated epitope on CD43 (CD43s). Strikingly, CD43s is expressed on all World Health Organization 2008 types of AML and MDS. AT1413 induced antibody-dependent cell-mediated cytotoxicity and complement-dependent cytotoxicity of AML cells in vitro. Of note, AT1413 was highly efficacious against AML cells in a humanized mouse model without affecting nonmalignant human myeloid cells, suggesting AT1413 has potential as a therapeutic antibody.