CD33 target validation and sustained depletion of AML blasts in long-term cultures by the bispecific T-cell-engaging antibody AMG 330

Christina Krupka; Peter Kufer; Roman Kischel; Gerhard Zugmaier; Jan Bögeholz; Thomas Köhnke; Felix S. Lichtenegger; Stephanie Schneider; Klaus H. Metzeler; Michael Fiegl; Karsten Spiekermann; Patrick A. Baeuerle; Wolfgang Hiddemann; Gert Riethmüller; Marion Subklewe

Journal ArticleOPEN ACCESS

CD33 target validation and sustained depletion of AML blasts in long-term cultures by the bispecific T-cell-engaging antibody AMG 330

Blood (2014) 123(3) 356-365

DOI: 10.1182/blood-2013-08-523548

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Abstract

Antibody-based immunotherapy represents a promising strategy to target and eliminate chemoresistant leukemic cells. Here, we evaluated the CD33/CD3-bispecific T cell engaging (BiTE) antibody (AMG 330) for its suitability as a therapeutic agent in acute myeloid leukemia (AML). We first assessed CD33 expression levels by flow cytometry and found expression in >99% of patient samples (n = 621). CD33 was highest expressed in AMLs with NPM1 mutations (P < .001) and lower in AMLs with complex karyotypes and t(8;21) translocations (P

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Krupka, C., Kufer, P., Kischel, R., Zugmaier, G., Bögeholz, J., Köhnke, T., … Subklewe, M. (2014). CD33 target validation and sustained depletion of AML blasts in long-term cultures by the bispecific T-cell-engaging antibody AMG 330. Blood, 123(3), 356–365. https://doi.org/10.1182/blood-2013-08-523548

CD33 target validation and sustained depletion of AML blasts in long-term cultures by the bispecific T-cell-engaging antibody AMG 330

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