CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism

Background: A strategy to broaden the applicability of checkpoint inhibitors is the combined use with antibodies targeting the immune stimulatory receptors CD40 and 41BB. However, the use of anti-CD40 and anti-41BB antibodies as agonists is problematic in two ways. First, anti-CD40 and anti-41BB ant...

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Autores principales: Medler, Juliane, Kucka, Kirstin, Melo, Vinicio, Zhang, Tengyu, von Rotenhan, Stefan, Ulrich, Jakob, Bremer, Edwin, Hudecek, Michael, Beilhack, Andreas, Wajant, Harald
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2022
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Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8825603/
https://www.ncbi.nlm.nih.gov/pubmed/35198053
http://dx.doi.org/10.7150/thno.66119
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author Medler, Juliane
Kucka, Kirstin
Melo, Vinicio
Zhang, Tengyu
von Rotenhan, Stefan
Ulrich, Jakob
Bremer, Edwin
Hudecek, Michael
Beilhack, Andreas
Wajant, Harald
author_facet Medler, Juliane
Kucka, Kirstin
Melo, Vinicio
Zhang, Tengyu
von Rotenhan, Stefan
Ulrich, Jakob
Bremer, Edwin
Hudecek, Michael
Beilhack, Andreas
Wajant, Harald
author_sort Medler, Juliane
collection PubMed
description Background: A strategy to broaden the applicability of checkpoint inhibitors is the combined use with antibodies targeting the immune stimulatory receptors CD40 and 41BB. However, the use of anti-CD40 and anti-41BB antibodies as agonists is problematic in two ways. First, anti-CD40 and anti-41BB antibodies need plasma membrane-associated presentation by FcγR binding to exert robust agonism but this obviously limits their immune stimulatory efficacy by triggering ADCC, CDC or anti-inflammatory FcγRIIb activities. Second, off tumor activation of CD40 and 41BB may cause dose limiting systemic inflammation. Methods: To overcome the FcγR-dependency of anti-41BB and anti-CD40 antibodies, we genetically fused such antibodies with a PDL1-specific blocking scFv as anchoring domain to enable FcγR-independent plasma membrane-associated presentation of anti-CD40- and anti-41BB antibodies. By help of GpL-tagged variants of the resulting bispecific antibodies, binding to their molecular targets was evaluated by help of cellular binding studies. Membrane PDL1-restricted engagement of CD40 and 41BB but also inhibition of PDL1-induced PD1 activation were evaluated in coculture assays with PDL1-expressing tumor cell lines and 41BB, CD40 and PD1 responsible cell lines or T-cells. Results: The binding properties of the bispecific antibody fusion proteins remained largely unchanged compared to their parental molecules. Upon anchoring to membrane PDL1, the bispecific antibody fusion proteins activated CD40/41BB signaling as efficient as the parental anti-CD40/anti-41BB antibodies when bound to FcγRs or cells expressing membrane-bound CD40L/41BBL. PD1 inhibition remained intact and the anti-41BB fusion protein thus showed PDL1-restricted costimulation of T-cells activated in vitro with anti-CD3 or a BiTe. Conclusions: Targeting of anti-CD40 and anti-41BB fusion proteins to membrane PDL1 with a blocking PDL1 scFv links PD1-PDL1 checkpoint blockade intrinsically with engagement of CD40 or 41BB.
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spelling pubmed-88256032022-02-22 CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism Medler, Juliane Kucka, Kirstin Melo, Vinicio Zhang, Tengyu von Rotenhan, Stefan Ulrich, Jakob Bremer, Edwin Hudecek, Michael Beilhack, Andreas Wajant, Harald Theranostics Research Paper Background: A strategy to broaden the applicability of checkpoint inhibitors is the combined use with antibodies targeting the immune stimulatory receptors CD40 and 41BB. However, the use of anti-CD40 and anti-41BB antibodies as agonists is problematic in two ways. First, anti-CD40 and anti-41BB antibodies need plasma membrane-associated presentation by FcγR binding to exert robust agonism but this obviously limits their immune stimulatory efficacy by triggering ADCC, CDC or anti-inflammatory FcγRIIb activities. Second, off tumor activation of CD40 and 41BB may cause dose limiting systemic inflammation. Methods: To overcome the FcγR-dependency of anti-41BB and anti-CD40 antibodies, we genetically fused such antibodies with a PDL1-specific blocking scFv as anchoring domain to enable FcγR-independent plasma membrane-associated presentation of anti-CD40- and anti-41BB antibodies. By help of GpL-tagged variants of the resulting bispecific antibodies, binding to their molecular targets was evaluated by help of cellular binding studies. Membrane PDL1-restricted engagement of CD40 and 41BB but also inhibition of PDL1-induced PD1 activation were evaluated in coculture assays with PDL1-expressing tumor cell lines and 41BB, CD40 and PD1 responsible cell lines or T-cells. Results: The binding properties of the bispecific antibody fusion proteins remained largely unchanged compared to their parental molecules. Upon anchoring to membrane PDL1, the bispecific antibody fusion proteins activated CD40/41BB signaling as efficient as the parental anti-CD40/anti-41BB antibodies when bound to FcγRs or cells expressing membrane-bound CD40L/41BBL. PD1 inhibition remained intact and the anti-41BB fusion protein thus showed PDL1-restricted costimulation of T-cells activated in vitro with anti-CD3 or a BiTe. Conclusions: Targeting of anti-CD40 and anti-41BB fusion proteins to membrane PDL1 with a blocking PDL1 scFv links PD1-PDL1 checkpoint blockade intrinsically with engagement of CD40 or 41BB. Ivyspring International Publisher 2022-01-01 /pmc/articles/PMC8825603/ /pubmed/35198053 http://dx.doi.org/10.7150/thno.66119 Text en © The author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Medler, Juliane
Kucka, Kirstin
Melo, Vinicio
Zhang, Tengyu
von Rotenhan, Stefan
Ulrich, Jakob
Bremer, Edwin
Hudecek, Michael
Beilhack, Andreas
Wajant, Harald
CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism
title CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism
title_full CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism
title_fullStr CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism
title_full_unstemmed CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism
title_short CD40- and 41BB-specific antibody fusion proteins with PDL1 blockade-restricted agonism
title_sort cd40- and 41bb-specific antibody fusion proteins with pdl1 blockade-restricted agonism
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8825603/
https://www.ncbi.nlm.nih.gov/pubmed/35198053
http://dx.doi.org/10.7150/thno.66119
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