Targeted Therapy With the T-Cell–Engaging Antibody Blinatumomab of Chemotherapy-Refractory Minimal Residual Disease in B-Lineage Acute Lymphoblastic Leukemia Patients Results in High Response Rate and Prolonged Leukemia-Free Survival

Topp, Max S.; Kufer, Peter; Gökbuget, Nicola; Goebeler, Mariele; Klinger, Matthias; Neumann, Svenja; Horst, Heinz-A.; Raff, Thorsten; Viardot, Andreas; Schmid, Mathias; Stelljes, Matthias; Schaich, Markus; Degenhard, Evelyn; Köhne-Volland, R; Brüggemann, Monika; Ottmann, Oliver G.; Pfeifer, Heike; Burmeister, Thomas; Nagorsen, Dirk; Schmidt, Margit; Lutterbuese, Ralf; Reinhardt, Carsten; Baeuerle, Patrick A.; Kneba, Michael; Einsele, Hermann; Riethmüller, Gert; Hoelzer, Dieter; Zugmaier, Gerhard; Bargou, Ralf C.

doi:10.1200/jco.2010.32.7270

Cited by 809 publications

(696 citation statements)

References 24 publications

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“…In the population-variability study, the cytokine release (IL-2, IL-6, TNF, and IFN-g) induced by AFM11 in unfractionated PBMC is reduced relative to that induced by OKT3 across all of the cytokines, and only AFM11-induced IL-6 release approaches that of OKT3; this is consistent with the blinatumomab clinical experience. 32 In unstimulated PBMC spiked with CD19 C tumor cells at a ratio of 5:1, AFM11 induces a dose-responsive cytokine release consistent with its mode of action. Lastly, in the biodistribution study radiolabeled AFM11 exhibited excellent localization to tumor tissue with minimal distribution to normal tissue, excepting the spleen as expected.…”

Section: Discussionmentioning

confidence: 99%

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

Reusch

Duell

Ellwanger

et al. 2015

mAbs

119

109

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To harness the potent tumor-killing capacity of T cells for the treatment of CD19 C malignancies, we constructed AFM11, a humanized tetravalent bispecific CD19/CD3 tandem diabody (TandAb) consisting solely of Fv domains. The molecule exhibits good manufacturability and stability properties. AFM11 has 2 binding sites for CD3 and 2 for CD19, an antigen that is expressed from early B cell development through differentiation into plasma cells, and is an attractive alternative to CD20 as a target for the development of therapeutic antibodies to treat B cell malignancies. Comparison of the binding and cytotoxicity of AFM11 with those of a tandem scFv bispecific T cell engager (BiTE) molecule targeting the same antigens revealed that AFM11 elicited more potent in vitro B cell lysis. Though possessing high affinity to CD3, the TandAb mediates serial-killing of CD19 C cells with little dependence of potency or efficacy upon effector:target ratio, unlike the BiTE. The advantage of the TandAb over the BiTE was most pronounced at lower effector:target ratios. AFM11 mediated strictly targetdependent T cell activation evidenced by CD25 and CD69 induction, proliferation, and cytokine release, notwithstanding bivalent CD3 engagement. In a NOD/scid xenograft model, AFM11 induced dose-dependent growth inhibition of Raji tumors in vivo, and radiolabeled TandAb exhibited excellent localization to tumor but not to normal tissue. After intravenous administration in mice, half-life ranged from 18.4 to 22.9 h. In a human ex vivo B-cell chronic lymphocytic leukemia study, AFM11 exhibited substantial cytotoxic activity in an autologous setting. Thus, AFM11 may represent a promising therapeutic for treatment of CD19 C malignancies with an advantageous safety risk profile and anticipated dosing regimen.

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Section: Discussionmentioning

confidence: 99%

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

Reusch

Duell

Ellwanger

et al. 2015

mAbs

119

109

View full text Add to dashboard Cite

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“…Indeed, convincing data to extrapolate a benefit of additional pre-HCT therapy may come from a phase 2 trial with blinatumomab, a bispecific single-chain Ab targeting CD19, in patients with B-lineage ALL having chemotherapy-refractory MRD. 81 In this study, 16 out of 20 MRD þ patients became MRD À after treatment with blinatumomab, and none of the 8 patients subsequently undergoing AlloHCT experienced post-HCT relapse. Although not all patients were responsive to Ab therapy, this finding suggests that elimination of MRD with blinatumomab may improve post-HCT outcomes of patients that otherwise would have been MRD þ at transplantation, but larger studies will be required to conclusively test this possibility.…”

Section: Using Pre-hct Mrd To Tailor Therapy In Acute Leukemiamentioning

confidence: 95%

Prognostic and therapeutic implications of minimal residual disease at the time of transplantation in acute leukemia

Buckley

Appelbaum

Walter

2012

Bone Marrow Transplant

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“…T cells responding to infection expand, then contract; recovery after contraction was the basis for the selection of the dosing holiday 70. The primary endpoint, MRD‐negativity, was achieved in 16 of 20 (80%) evaluable subjects (one subject experienced a Grade 3 seizure and was not evaluable) 71. At a median follow‐up of 33 months, hematologic relapse‐free survival was 60% 72.…”

Section: Clinical Experience With Blinatumomabmentioning

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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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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Targeted Therapy With the T-Cell–Engaging Antibody Blinatumomab of Chemotherapy-Refractory Minimal Residual Disease in B-Lineage Acute Lymphoblastic Leukemia Patients Results in High Response Rate and Prolonged Leukemia-Free Survival

Abstract: Blinatumomab is an efficacious and well-tolerated treatment in patients with MRD-positive B-lineage ALL after intensive chemotherapy. T cells engaged by blinatumomab seem capable of eradicating chemotherapy-resistant tumor cells that otherwise cause clinical relapse.

Cited by 809 publications

References 24 publications

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

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

Prognostic and therapeutic implications of minimal residual disease at the time of transplantation in acute leukemia

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

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Targeted Therapy With the T-Cell–Engaging Antibody Blinatumomab of Chemotherapy-Refractory Minimal Residual Disease in B-Lineage Acute Lymphoblastic Leukemia Patients Results in High Response Rate and Prolonged Leukemia-Free Survival

Abstract: Blinatumomab is an efficacious and well-tolerated treatment in patients with MRD-positive B-lineage ALL after intensive chemotherapy. T cells engaged by blinatumomab seem capable of eradicating chemotherapy-resistant tumor cells that otherwise cause clinical relapse.

Cited by 809 publications

References 24 publications

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

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

Prognostic and therapeutic implications of minimal residual disease at the time of transplantation in acute leukemia

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

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Resources

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

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