Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model

INTRODUCTION: Despite advances in treating high-risk neuroblastoma, 50-60% of patients still suffer relapse, necessitating new treatment options. Bispecific trifunctional antibodies (trAbs) are a promising new class of immunotherapy. TrAbs are heterodimeric IgG-like molecules that bind CD3 and a tum...

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Autores principales: Ivasko, Sara Marie, Anders, Kathleen, Grunewald, Laura, Launspach, Michael, Klaus, Anika, Schwiebert, Silke, Ruf, Peter, Lindhofer, Horst, Lode, Holger N., Andersch, Lena, Schulte, Johannes H., Eggert, Angelika, Hundsdoerfer, Patrick, Künkele, Annette, Zirngibl, Felix
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9869131/
https://www.ncbi.nlm.nih.gov/pubmed/36700232
http://dx.doi.org/10.3389/fimmu.2022.1023206
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author Ivasko, Sara Marie
Anders, Kathleen
Grunewald, Laura
Launspach, Michael
Klaus, Anika
Schwiebert, Silke
Ruf, Peter
Lindhofer, Horst
Lode, Holger N.
Andersch, Lena
Schulte, Johannes H.
Eggert, Angelika
Hundsdoerfer, Patrick
Künkele, Annette
Zirngibl, Felix
author_facet Ivasko, Sara Marie
Anders, Kathleen
Grunewald, Laura
Launspach, Michael
Klaus, Anika
Schwiebert, Silke
Ruf, Peter
Lindhofer, Horst
Lode, Holger N.
Andersch, Lena
Schulte, Johannes H.
Eggert, Angelika
Hundsdoerfer, Patrick
Künkele, Annette
Zirngibl, Felix
author_sort Ivasko, Sara Marie
collection PubMed
description INTRODUCTION: Despite advances in treating high-risk neuroblastoma, 50-60% of patients still suffer relapse, necessitating new treatment options. Bispecific trifunctional antibodies (trAbs) are a promising new class of immunotherapy. TrAbs are heterodimeric IgG-like molecules that bind CD3 and a tumor-associated antigen simultaneously, whereby inducing a TCR-independent anti-cancer T cell response. Moreover, via their functional Fc region they recruit and activate cells of the innate immune system like antigen-presenting cells potentially enhancing induction of adaptive tumor-specific immune responses. METHODS: We used the SUREK trAb, which is bispecific for GD2 and murine Cd3. Tumor-blind trAb and the monoclonal ch14.18 antibody were used as controls. A co-culture model of murine dendritic cells (DCs), T cells and a neuroblastoma cell line was established to evaluate the cytotoxic effect and the T cell effector function in vitro. Expression of immune checkpoint molecules on tumor-infiltrating T cells and the induction of an anti-neuroblastoma immune response using a combination of whole cell vaccination and trAb therapy was investigated in a syngeneic immunocompetent neuroblastoma mouse model (NXS2 in A/J background). Finally, vaccinated mice were assessed for the presence of neuroblastoma-directed antibodies. We show that SUREK trAb-mediated effective killing of NXS2 cells in vitro was strictly dependent on the combined presence of DCs and T cells. RESULTS: Using a syngeneic neuroblastoma mouse model, we showed that vaccination with irradiated tumor cells combined with SUREK trAb treatment significantly prolonged survival of tumor challenged mice and partially prevent tumor outgrowth compared to tumor vaccination alone. Treatment led to upregulation of programmed cell death protein 1 (Pd-1) on tumor infiltrating T cells and combination with anti-Pd-1 checkpoint inhibition enhanced the NXS2-directed humoral immune response. CONCLUSION: Here, we provide first preclinical evidence that a tumor vaccination combined with SUREK trAb therapy induces an endogenous anti-neuroblastoma immune response reducing tumor recurrence. Furthermore, a combination with anti-Pd-1 immune checkpoint blockade might even further improve this promising immunotherapeutic concept in order to prevent relapse in high-risk neuroblastoma patients.
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spelling pubmed-98691312023-01-24 Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model Ivasko, Sara Marie Anders, Kathleen Grunewald, Laura Launspach, Michael Klaus, Anika Schwiebert, Silke Ruf, Peter Lindhofer, Horst Lode, Holger N. Andersch, Lena Schulte, Johannes H. Eggert, Angelika Hundsdoerfer, Patrick Künkele, Annette Zirngibl, Felix Front Immunol Immunology INTRODUCTION: Despite advances in treating high-risk neuroblastoma, 50-60% of patients still suffer relapse, necessitating new treatment options. Bispecific trifunctional antibodies (trAbs) are a promising new class of immunotherapy. TrAbs are heterodimeric IgG-like molecules that bind CD3 and a tumor-associated antigen simultaneously, whereby inducing a TCR-independent anti-cancer T cell response. Moreover, via their functional Fc region they recruit and activate cells of the innate immune system like antigen-presenting cells potentially enhancing induction of adaptive tumor-specific immune responses. METHODS: We used the SUREK trAb, which is bispecific for GD2 and murine Cd3. Tumor-blind trAb and the monoclonal ch14.18 antibody were used as controls. A co-culture model of murine dendritic cells (DCs), T cells and a neuroblastoma cell line was established to evaluate the cytotoxic effect and the T cell effector function in vitro. Expression of immune checkpoint molecules on tumor-infiltrating T cells and the induction of an anti-neuroblastoma immune response using a combination of whole cell vaccination and trAb therapy was investigated in a syngeneic immunocompetent neuroblastoma mouse model (NXS2 in A/J background). Finally, vaccinated mice were assessed for the presence of neuroblastoma-directed antibodies. We show that SUREK trAb-mediated effective killing of NXS2 cells in vitro was strictly dependent on the combined presence of DCs and T cells. RESULTS: Using a syngeneic neuroblastoma mouse model, we showed that vaccination with irradiated tumor cells combined with SUREK trAb treatment significantly prolonged survival of tumor challenged mice and partially prevent tumor outgrowth compared to tumor vaccination alone. Treatment led to upregulation of programmed cell death protein 1 (Pd-1) on tumor infiltrating T cells and combination with anti-Pd-1 checkpoint inhibition enhanced the NXS2-directed humoral immune response. CONCLUSION: Here, we provide first preclinical evidence that a tumor vaccination combined with SUREK trAb therapy induces an endogenous anti-neuroblastoma immune response reducing tumor recurrence. Furthermore, a combination with anti-Pd-1 immune checkpoint blockade might even further improve this promising immunotherapeutic concept in order to prevent relapse in high-risk neuroblastoma patients. Frontiers Media S.A. 2023-01-09 /pmc/articles/PMC9869131/ /pubmed/36700232 http://dx.doi.org/10.3389/fimmu.2022.1023206 Text en Copyright © 2023 Ivasko, Anders, Grunewald, Launspach, Klaus, Schwiebert, Ruf, Lindhofer, Lode, Andersch, Schulte, Eggert, Hundsdoerfer, Künkele and Zirngibl https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Ivasko, Sara Marie
Anders, Kathleen
Grunewald, Laura
Launspach, Michael
Klaus, Anika
Schwiebert, Silke
Ruf, Peter
Lindhofer, Horst
Lode, Holger N.
Andersch, Lena
Schulte, Johannes H.
Eggert, Angelika
Hundsdoerfer, Patrick
Künkele, Annette
Zirngibl, Felix
Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model
title Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model
title_full Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model
title_fullStr Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model
title_full_unstemmed Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model
title_short Combination of GD2-directed bispecific trifunctional antibody therapy with Pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model
title_sort combination of gd2-directed bispecific trifunctional antibody therapy with pd-1 immune checkpoint blockade induces anti-neuroblastoma immunity in a syngeneic mouse model
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9869131/
https://www.ncbi.nlm.nih.gov/pubmed/36700232
http://dx.doi.org/10.3389/fimmu.2022.1023206
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