Frontiers in Immunology (Jan 2019)

A Novel T-Cell Engaging Bi-specific Antibody Targeting the Leukemia Antigen PR1/HLA-A2

  • Amanda C. Herrmann,
  • Jin S. Im,
  • Sumedha Pareek,
  • Wilfredo Ruiz-Vasquez,
  • Sijie Lu,
  • Anna Sergeeva,
  • Jennifer Mehrens,
  • Hong He,
  • Gheath Alatrash,
  • Pariya Sukhumalchandra,
  • Lisa St. John,
  • Karen Clise-Dwyer,
  • Dongxing Zha,
  • Jeffrey J. Molldrem

DOI
https://doi.org/10.3389/fimmu.2018.03153
Journal volume & issue
Vol. 9

Abstract

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Despite substantial advances in the treatment of acute myeloid leukemia (AML), only 30% of patients survive more than 5 years. Therefore, new therapeutics are much needed. Here, we present a novel therapeutic strategy targeting PR1, an HLA-A2 restricted myeloid leukemia antigen. Previously, we have developed and characterized a novel T-cell receptor-like monoclonal antibody (8F4) that targets PR1/HLA-A2 and eliminates AML xenografts by antibody-dependent cellular cytotoxicity (ADCC). To improve the potency of 8F4, we adopted a strategy to link T-cell cytotoxicity with a bi-specific T-cell-engaging antibody that binds PR1/HLA-A2 on leukemia and CD3 on neighboring T-cells. The 8F4 bi-specific antibody maintained high affinity and specific binding to PR1/HLA-A2 comparable to parent 8F4 antibody, shown by flow cytometry and Bio-Layer Interferometry. In addition, 8F4 bi-specific antibody activated donor T-cells in the presence of HLA-A2+ primary AML blasts and cell lines in a dose dependent manner. Importantly, activated T-cells lysed HLA-A2+ primary AML blasts and cell lines after addition of 8F4 bi-specific antibody. In conclusion, our studies demonstrate the therapeutic potential of a novel bi-specific antibody targeting the PR1/HLA-A2 leukemia-associated antigen, justifying further clinical development of this strategy.

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