Literature DB >> 22745368

Trifunctional bispecific antibodies induce tumor-specific T cells and elicit a vaccination effect.

Nina Eissler1, Peter Ruf, Josef Mysliwietz, Horst Lindhofer, Ralph Mocikat.   

Abstract

A major goal of tumor immunotherapy is the induction of long-lasting systemic T-cell immunity. Bispecific antibodies (bsAbs) that lack the immunoglobulin Fc region confer T-cell-mediated killing of tumor cells but do not induce long-term memory. In contrast, trifunctional bsAbs comprise an appropriate Fc region and, therefore, not only recruit T cells but also accessory cells that bear activating Fcγ receptors (FcγR), providing additional T-cell-activating signals and securing presentation of tumor-derived antigens to T cells. In this study, we show that trifunctional bsAbs induce a polyvalent T-cell response and, therefore, a vaccination effect. Mice were treated with melanoma cells and with a trifunctional bsAb directed against the melanoma target antigen ganglioside GD2 in addition to murine CD3. The trifunctional bsAb activated dendritic cells and induced a systemic immune response that was not replicated by treatment with the F(ab')2-counterpart lacking the Fc region. Restimulation of spleen and lymph node cells in vitro yielded T-cell lines that specifically produced interferon-γ in response to tumor. In addition, trifunctional bsAb-induced T cells recognized various specific peptides derived from melanoma-associated antigens. Moreover, these polyvalent responses proved to be tumor-suppressive and could not be induced by the corresponding bsF(ab')2-fragment. Taken together, our findings provide preclinical proof of concept that trifunctional bsAbs can induce tumor-specific T cells with defined antigen specificity. ©2012 AACR.

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Year:  2012        PMID: 22745368     DOI: 10.1158/0008-5472.CAN-12-0146

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  14 in total

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3.  Retargeting T cells to GD2 pentasaccharide on human tumors using Bispecific humanized antibody.

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4.  Potential of the trifunctional bispecific antibody surek depends on dendritic cells: rationale for a new approach of tumor immunotherapy.

Authors:  Nina Eissler; Josef Mysliwietz; Nina Deppisch; Peter Ruf; Horst Lindhofer; Ralph Mocikat
Journal:  Mol Med       Date:  2013-04-30       Impact factor: 6.354

5.  Structural design of disialoganglioside GD2 and CD3-bispecific antibodies to redirect T cells for tumor therapy.

Authors:  Ming Cheng; Mahiuddin Ahmed; Hong Xu; Nai-Kong V Cheung
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7.  Novel anti-melanoma treatment: focus on immunotherapy.

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8.  GD2-directed bispecific trifunctional antibody outperforms dinutuximab beta in a murine model for aggressive metastasized neuroblastoma.

Authors:  Felix Zirngibl; Sara M Ivasko; Laura Grunewald; Anika Klaus; Silke Schwiebert; Peter Ruf; Horst Lindhofer; Kathy Astrahantseff; Lena Andersch; Johannes H Schulte; Holger N Lode; Angelika Eggert; Kathleen Anders; Patrick Hundsdoerfer; Annette Künkele
Journal:  J Immunother Cancer       Date:  2021-07       Impact factor: 13.751

9.  Ganglioside GD2-specific trifunctional surrogate antibody Surek demonstrates therapeutic activity in a mouse melanoma model.

Authors:  Peter Ruf; Beatrix Schäfer; Nina Eissler; Ralph Mocikat; Juergen Hess; Matthias Plöscher; Susanne Wosch; Ivonne Suckstorff; Christine Zehetmeier; Horst Lindhofer
Journal:  J Transl Med       Date:  2012-11-07       Impact factor: 5.531

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Journal:  J Transl Med       Date:  2013-07-02       Impact factor: 5.531

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