| Literature DB >> 27380762 |
Ursula Jördis Eva Seidel1, Patrick Schlegel1, Ludger Grosse-Hovest2,3, Martin Hofmann2,3, Steffen Aulwurm2,3, Elwira Pyz3, Friedhelm R Schuster4, Roland Meisel4, Martin Ebinger1, Tobias Feuchtinger5, Heiko-Manuel Teltschik1, Kai-Erik Witte1, Carl-Philipp Schwarze1, Hans-Georg Rammensee3,6, Rupert Handgretinger1,6, Gundram Jung3,6, Peter Lang1,6.
Abstract
Prognosis of primary refractory and relapsed pediatric B-lineage acute lymphoblastic leukemia (ALL) is very poor. Relapse rates significantly correlate with persistent minimal residual disease (MRD). In MRD, favorable effector-target ratios prevail and thus this situation might be optimally suited for immunotherapy with antibodies recruiting immunological effector cells. We here report on the generation, preclinical characterization and first clinical application in B-lineage ALL of an Fc-optimized CD19 antibody. This third-generation antibody (4G7SDIE) mediated enhanced antibody-dependent cellular cytotoxicity (ADCC) against leukemic blasts with effector cells from healthy volunteers and B-lineage ALL patients. The antibody was produced in a university-owned production unit and was applied on a compassionate use basis to 14 pediatric patients with refractory and relapsed B-lineage ALL at the stage of MRD. In 10/14 patients, MRD was reduced by ≥ 1 log or below the patient-individual detection limit, and 5/14 patients have achieved ongoing complete molecular remission with a median leukemia-free survival of 428 days. Two additional patients died in complete molecular remission due to complications not related to antibody therapy. Besides profound in vivo B-cell depletion, side effects were negligible. A clinical phase 1/2 study to further assess the therapeutic activity of 4G7SDIE is in preparation.Entities:
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Year: 2016 PMID: 27380762 PMCID: PMC5113107 DOI: 10.1038/mt.2016.141
Source DB: PubMed Journal: Mol Ther ISSN: 1525-0016 Impact factor: 11.454