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1000 Titel
  • Influence of antigen density and immunosuppressive factors on tumor-targeted costimulation with antibody-fusion proteins and bispecific antibody-mediated T cell response
1000 Autor/in
  1. Sapski, Sabrina |
  2. Beha, Nadine |
  3. Kontermann, Roland E. |
  4. Mueller, Dafne |
1000 Erscheinungsjahr 2020
1000 Publikationstyp
  1. Artikel |
1000 Online veröffentlicht
  • 2020-06-05
1000 Erschienen in
1000 Quellenangabe
  • 69(11):2291-2303
1000 Copyrightjahr
  • 2020
1000 Lizenz
1000 Verlagsversion
  • https://doi.org/10.1007/s00262-020-02624-6 |
  • https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7568714/ |
1000 Publikationsstatus
1000 Sprache der Publikation
1000 Abstract/Summary
  • Target expression heterogeneity and the presence of an immunosuppressive microenvironment can hamper severely the efficiency of immunotherapeutic approaches. We have analyzed the potential to encounter and overcome such conditions by a combinatory two-target approach involving a bispecific antibody retargeting T cells to tumor cells and tumor-directed antibody-fusion proteins with costimulatory members of the B7 and TNF superfamily. Targeting the tumor-associated antigens EpCAM and EGFR with the bispecific antibody and costimulatory fusion proteins, respectively, we analyzed the impact of target expression and the influence of the immunosuppressive factors IDO, IL-10, TGF-β, PD-1 and CTLA-4 on the targeting-mediated stimulation of T cells. Here, suboptimal activity of the bispecific antibody at diverse EpCAM expression levels could be effectively enhanced by targeting-mediated costimulation by B7.1, 4-1BBL and OX40L in a broad range of EGFR expression levels. Furthermore, the benefit of combined costimulation by B7.1/4-1BBL and 4-1BBL/OX40L was demonstrated. In addition, the expression of immunosuppressive factors was shown in all co-culture settings, where blocking of prominent factors led to synergistic effects with combined costimulation. Thus, targeting-mediated costimulation showed general promise for a broad application covering diverse target expression levels, with the option for further selective enhancement by the identification and blockade of main immunosuppressive factors of the particular tumor environment.
1000 Sacherschließung
lokal Tumor Escape/immunology [MeSH]
lokal Cell Line, Tumor [MeSH]
lokal Antibodies, Bispecific/immunology [MeSH]
lokal T-Lymphocytes/drug effects [MeSH]
lokal T-Lymphocytes/immunology [MeSH]
lokal Lymphocyte Activation/immunology [MeSH]
lokal Humans [MeSH]
lokal Tumor Microenvironment/drug effects [MeSH]
lokal Costimulation
lokal Tumor Escape/drug effects [MeSH]
lokal Immunosuppression
lokal Tumor Microenvironment/immunology [MeSH]
lokal Antibodies, Bispecific/pharmacology [MeSH]
lokal Antigens, Neoplasm/immunology [MeSH]
lokal Lymphocyte Activation/drug effects [MeSH]
lokal Original Article
lokal Antibody-fusion proteins
lokal ErbB Receptors/immunology [MeSH]
lokal Recombinant Fusion Proteins/immunology [MeSH]
lokal TNFSF ligands
lokal Cancer immunotherapy
lokal Bispecific antibody
lokal Epithelial Cell Adhesion Molecule/immunology [MeSH]
lokal Recombinant Fusion Proteins/pharmacology [MeSH]
1000 Liste der Beteiligten
  1. https://frl.publisso.de/adhoc/uri/U2Fwc2tpLCBTYWJyaW5h|https://frl.publisso.de/adhoc/uri/QmVoYSwgTmFkaW5l|https://frl.publisso.de/adhoc/uri/S29udGVybWFubiwgUm9sYW5kIEUu|https://orcid.org/0000-0002-1544-3475
1000 Hinweis
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1000 Erstellt am 2023-11-18T03:41:26.087+0100
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1000 Zuletzt bearbeitet 2023-12-01T11:06:15.676+0100
1000 Objekt bearb. Fri Dec 01 11:06:15 CET 2023
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