Literature DB >> 12209608

Extremely potent, rapid and costimulation-independent cytotoxic T-cell response against lymphoma cells catalyzed by a single-chain bispecific antibody.

Torsten Dreier1, Grit Lorenczewski, Christian Brandl, Patrick Hoffmann, Uwe Syring, Frank Hanakam, Peter Kufer, Gert Riethmuller, Ralf Bargou, Patrick A Baeuerle.   

Abstract

A recent study reported on an anti-CD19/anti-CD3 single-chain bispecific antibody (bscCD19xCD3) exhibiting high activity against human B lymphoma cell lines (Löffler et al., Blood 2000;95:2098-103). In the present study, we have explored in detail the in vitro efficacy, T-cell donor variability, binding characteristics, specificity, kinetics and interleukin-2 (IL-2) dependence of bscCD19xCD3. We found that a majority of human donor T cells tested (n = 86) gave half-maximal B-lymphoma cell lysis (ED(50)) within a range of 10-50 pg/ml bscCD19xCD3, corresponding to sub-picomolar concentrations of the bispecific antibody. Under identical experimental conditions, the anti-CD20 monoclonal antibody rituximab had an at least 100,000-fold lower in vitro efficacy. The extreme potency of bscCD19xCD3 was in sharp contrast to the relatively low affinity of the anti-CD3 and anti-CD19 single-chain Fv portions in K(D) ranges of 10(-7) and 10(-9) M, respectively. Cell lysis by bscCD19xCD3 was predominantly mediated by the population of CD8/CD45RO-positive T cells. Both immortalized CD4- and CD8-positive human T-cell clones were highly active effector cells as well. Cell lysis by bscCD19xCD3 was rapid and specific. The respective parental monoclonal antibodies inhibited cell lysis and CD19-negative cells were not harmed by T cells in the presence of high amounts of bscCD19xCD3. The potent T-cell stimulus IL-2 could not markedly augment the activity of bscCD19xCD3-stimulated T cells. In conclusion, bscCD19xCD3 could redirect unstimulated cytotoxic T cells against CD19-positive cells in an unexpectedly potent, rapid and specific fashion. Copyright 2002 Wiley-Liss, Inc.

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Year:  2002        PMID: 12209608     DOI: 10.1002/ijc.10557

Source DB:  PubMed          Journal:  Int J Cancer        ISSN: 0020-7136            Impact factor:   7.396


  89 in total

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Journal:  Invest New Drugs       Date:  2018-12-04       Impact factor: 3.850

Review 2.  Bispecific T-cell engagers for cancer immunotherapy.

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Journal:  Immunol Cell Biol       Date:  2014-11-04       Impact factor: 5.126

3.  World Bispecific Antibody Summit, September 27-28, 2011, Boston, MA.

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Review 4.  Cancer therapy with bispecific antibodies: Clinical experience.

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5.  A tetravalent bispecific TandAb (CD19/CD3), AFM11, efficiently recruits T cells for the potent lysis of CD19(+) tumor cells.

Authors:  Uwe Reusch; Johannes Duell; Kristina Ellwanger; Carmen Herbrecht; Stefan Hj Knackmuss; Ivica Fucek; Markus Eser; Fionnuala McAleese; Vera Molkenthin; Fabrice Le Gall; Max Topp; Melvyn Little; Eugene A Zhukovsky
Journal:  MAbs       Date:  2015       Impact factor: 5.857

Review 6.  Blinatumomab for the treatment of acute lymphoblastic leukemia.

Authors:  Jason B Kaplan; Marina Grischenko; Francis J Giles
Journal:  Invest New Drugs       Date:  2015-09-17       Impact factor: 3.850

Review 7.  Recent advances and novel treatment paradigms in acute lymphocytic leukemia.

Authors:  Nikolaos Papadantonakis; Anjali S Advani
Journal:  Ther Adv Hematol       Date:  2016-06-29

8.  A novel targeted GPC3/CD3 bispecific antibody for the treatment hepatocellular carcinoma.

Authors:  Lin Yu; Xi Yang; Nan Huang; Qiao-Li Lang; Qi-Lin He; Wang Jian-Hua; Ge Liang-Peng
Journal:  Cancer Biol Ther       Date:  2020-04-02       Impact factor: 4.742

Review 9.  T cell-engaging therapies - BiTEs and beyond.

Authors:  Maria-Elisabeth Goebeler; Ralf C Bargou
Journal:  Nat Rev Clin Oncol       Date:  2020-04-02       Impact factor: 66.675

Review 10.  Recent Advances in the Management of Acute Lymphoblastic Leukaemia.

Authors:  Katharine A Hodby; David I Marks
Journal:  Curr Treat Options Oncol       Date:  2020-02-20
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