Antibodies (May 2013)

Immunotherapy of B-Cell Lymphoma with an Engineered Bispecific Antibody Targeting CD19 and CD5

  • Frank Breitling,
  • Gerhard Moldenhauer,
  • Antonio Pezzutto,
  • Oliver Schmetzer,
  • Martin Lipp,
  • Saskia Meyer,
  • Regina Fertig,
  • Hossein Panjideh,
  • Dorothée Deppe,
  • Sandra Lüttgau

DOI
https://doi.org/10.3390/antib2020338
Journal volume & issue
Vol. 2, no. 2
pp. 338 – 352

Abstract

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Using genetic engineering a humanized Fab fragment with specificity for CD19 was fused to a disulfide-stabilized single-chain antibody (dsFv) recognizing CD5. This format should show reduced immunogenicity and improved tissue penetration. The specificity of bsAb FabCD19xdsFvCD5 binding to target cells was verified by flow cytometry on B and T lymphoma cell lines. Binding affinities of both arms were compared with the bivalent parental antibodies against CD19 and CD5 by binding competition assay. Redirected lysis of B lymphoma cells by preactivated PBMC from healthy donors was demonstrated in a chromium-release assay. A clear dose-response relationship could be established in the range from 1 ng/mL to 10 mg/mL bsAb. To evaluate the in vivo efficacy of bsAb FabCD19xdsFvCD5, NOD/SCID mice were intravenously injected with luciferase transfected Raji lymphoma cells together with pre-activated PBMC. Mice received five injections of therapeutic bsAb or control antibodies. While in the control groups all mice died within 40 to 50 days, 40% of bsAb treated animals survived longer than 60 days.

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