T Cell Costimulus-Independent and Very Efficacious Inhibition of Tumor Growth in Mice Bearing Subcutaneous or Leukemic Human B Cell Lymphoma Xenografts by a CD19-/CD3- Bispecific Single-Chain Antibody Construct

Dreier, Torsten; Baeuerle, Patrick A.; Fichtner, Iduna; Grün, M.; Schlereth, Bernd; Lorenczewski, Grit; Kufer, Peter; Lutterbüse, Ralf; Riethmüller, Gert; Gjörstrup, P.; Bargou, Ralf C.

doi:10.4049/jimmunol.170.8.4397

Cited by 178 publications

(109 citation statements)

References 36 publications

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“…In preclinical species, these relatively small (blinatumomab is 55 kDa) fusion proteins have a terminal phase half‐life of only a few hours 32, 33. Full‐length monoclonal antibodies typically have a 21‐day half‐life, owing to neonatal Fc receptor (FcR n )‐mediated recycling.…”

Section: Mechanism Of Action and Key Characteristics Of Bite® Antibodmentioning

confidence: 99%

“…Because blinatumomab is not crossreactive with murine CD3, human T cells were administered as effector cells for redirected target cell lysis, but costimulatory agents were not required 32. Several other BiTE® antibody constructs are in various stages of clinical development, including AMG 211/MEDI‐565, AMG 212, AMG 420, and AMG 330.…”

Section: Mechanism Of Action and Key Characteristics Of Bite® Antibodmentioning

confidence: 99%

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Translation and Clinical Development of Bispecific T‐cell Engaging Antibodies for Cancer Treatment

Yuraszeck

Kasichayanula

Benjamin

2017

Clin Pharma and Therapeutics

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Bispecific T‐cell Engagers (BiTE®) antibody constructs enable a polyclonal T‐cell response to cell‐surface tumor‐associated antigens, bypassing the narrow specificities of T‐cell receptors and the need for antigen presentation through the major histocompatibility complex pathways. Blinatumomab, a CD19xCD3 BiTE® antibody construct, received accelerated approval for the treatment of relapsed/refractory Philadelphia chromosome negative acute lymphoblastic leukemia. Herein we review the pharmacology, safety, and efficacy observed in studies of blinatumomab and other BiTE® antibody constructs. Quantitative systems pharmacology is envisioned as a means to optimize dosing decisions for trials in which BiTE® antibody constructs are administered as monotherapy or in combination with other immunotherapies.

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Section: Mechanism Of Action and Key Characteristics Of Bite® Antibodmentioning

confidence: 99%

Section: Mechanism Of Action and Key Characteristics Of Bite® Antibodmentioning

confidence: 99%

Translation and Clinical Development of Bispecific T‐cell Engaging Antibodies for Cancer Treatment

Yuraszeck

Kasichayanula

Benjamin

2017

Clin Pharma and Therapeutics

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“…The main antigens that have been used as targets for bispecific antibodies are overexpressed by tumor cells, including EGFR (Witlox et al, 2002;Reusch et al, 2006), HER2 (Zhu et al, 1996;Maletz et al, 2001a), CD19 (Haagen et al, 1994;Csoka et al, 1996;Chen et al, 1998a, b;Kipriyanov et al, 1998;Loffler et al, 2000b;Manzke et al, 2001a, b;Dreier et al, 2003c), CD20 (Brandl et al, 1999;Xiong et al, 2002;Yu et al, 2005), EpCAM (Maletz et al, 2001b;Wimberger et al, 2003), MUC-1 (Katayose et al, 1996) and CEA (FitzGerald et al, 1997;Holliger et al, 1999;Korn et al, 2004).…”

Section: Bispecific Antibodiesmentioning

confidence: 99%

“…The BiTEs molecules, which contain anti-CD3 antibody, have the unique ability to achieve target cell lysis at low T-cell numbers (Hoffmann et al, 2005a) without the need for T-cell costimulation (Dreier et al, 2002a(Dreier et al, , 2003b. Monovalent binding to the CD3 complex is not sufficient to lead a full T-cell activation.…”

Section: Bispecific Antibodiesmentioning

confidence: 99%

“…To date, a great variety of target cells have been tested for lysis mediated by BiTEs, and no fully resistant tumor cell line expressing the target antigen has been identified (Wolf et al, 2005). MT103, a CD19-specific BiTE, showed a high ex vivo response against blood samples from B-cell lymphoma patients (Loffler et al, 2003), and was efficacious in a severe combined immunodeficiency (SCID) mouse model (Dreier et al, 2003a). It has been shown in chimpanzees that MT103 causes cumulative loss of peripheral B lymphocytes (Schlereth et al, 2006).…”

Section: Bispecific Antibodiesmentioning

confidence: 99%

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Novel antibodies as anticancer agents

2007

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In recent years antibodies, whether generated by traditional hybridoma technology or by recombinant DNA strategies, have evolved from Paul Ehrlich's 'magic bullets' to a modern age 'guided missile'. In the recent years of immunologic research, we are witnessing development in the fields of antigen screening and protein engineering in order to create specific anticancer remedies. The developments in the field of recombinant DNA, protein engineering and cancer biology have let us gain insight into many cancer-related mechanisms. Moreover, novel techniques have facilitated tools allowing unique distinction between malignantly transformed cells, and regular ones. This understanding has paved the way for the rational design of a new age of pharmaceuticals: monoclonal antibodies and their fragments. Antibodies can select antigens on both a specific and a high-affinity account, and further implementation of these qualities is used to target cancer cells by specifically identifying exogenous antigens of cancer cell populations. The structure of the antibody provides plasticity resonating from its functional sites. This review will screen some of the many novel antibodies and antibody-based approaches that are being currently developed for clinical applications as the new generation of anticancer agents.

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Bispecific Antibodies

and¹,

Kontermann²

2007

Handbook of Therapeutic Antibodies

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T Cell Costimulus-Independent and Very Efficacious Inhibition of Tumor Growth in Mice Bearing Subcutaneous or Leukemic Human B Cell Lymphoma Xenografts by a CD19-/CD3- Bispecific Single-Chain Antibody Construct

Cited by 178 publications

References 36 publications

Translation and Clinical Development of Bispecific T‐cell Engaging Antibodies for Cancer Treatment

Translation and Clinical Development of Bispecific T‐cell Engaging Antibodies for Cancer Treatment

Novel antibodies as anticancer agents

Bispecific Antibodies

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