Fcγ receptor binding is required for maximal immunostimulation by CD70-Fc
Fcγ receptor binding is required for maximal immunostimulation by CD70-Fc
Introduction: T cell expressed CD27 provides costimulation upon binding to inducible membrane expressed trimeric CD70 and is required for protective CD8 T cell responses. CD27 agonists could therefore be used to bolster cellular vaccines and anti-tumour immune responses. To date, clinical development of CD27 agonists has focussed on anti-CD27 antibodies with little attention given to alternative approaches.
Methods: here, we describe the generation and activity of soluble variants of CD70 that form either trimeric (t) or dimer-of-trimer proteins and conduct side-by-side comparisons with an agonist anti-CD27 antibody. To generate a dimer-of-trimer protein (dt), we fused three extracellular domains of CD70 to the Fc domain of mouse IgG1 in a ‘string of beads’ configuration (dtCD70-Fc).
Results: whereas tCD70 failed to costimulate CD8 T cells, both dtCD70-Fc and an agonist anti-CD27 antibody were capable of enhancing T cell proliferation in vitro. Initial studies demonstrated that dtCD70-Fc was less efficacious than anti-CD27 in boosting a CD8 T cell vaccine response in vivo, concomitant with rapid clearance of dtCD70-Fc from the circulation. The accelerated plasma clearance of dtCD70-Fc was not due to the lack of neonatal Fc receptor binding but was dependent on the large population of oligomannose type glycosylation. Enzymatic treatment to reduce the oligomannose-type glycans in dtCD70-Fc improved its half-life and significantly enhanced its T cell stimulatory activity in vivo surpassing that of anti-CD27 antibody. We also show that whereas the ability of the anti-CD27 to boost a vaccine response was abolished in Fc gamma receptor (FcγR)-deficient mice, dtCD70-Fc remained active. By comparing the activity of dtCD70-Fc with a variant (dtCD70-Fc(D265A)) that lacks binding to FcγRs, we unexpectedly found that FcγR binding to dtCD70-Fc was required for maximal boosting of a CD8 T cell response in vivo. Interestingly, both dtCD70-Fc and dtCD70-Fc(D265A) were effective in prolonging the survival of mice harbouring BCL1 B cell lymphoma, demonstrating that a substantial part of the stimulatory activity of dtCD70-Fc in this setting is retained in the absence of FcγR interaction.
Discussion: these data reveal that TNFRSF ligands can be generated with a tunable activity profile and suggest that this class of immune agonists could have broad applications in immunotherapy.
cancer, CD27, costimulation, immunotherapy, T cells, TNFRSF, vaccine
Dadas, Osman
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Allen, Joel D.
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Buchan, Sarah L.
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Kim, Jinny H.
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Chan, H.T. Claude
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Mockridge, C. Ian
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Duriez, Patrick J.
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Rogel, Anne
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Crispin, Max
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Al-Shamkhani, Aymen
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27 October 2023
Dadas, Osman
f231026d-4201-40d3-ab10-137ff53f3830
Allen, Joel D.
c89d5569-7659-4835-b535-c9586e956b3a
Buchan, Sarah L.
9ade187d-f127-45de-ad90-9d544d64718a
Kim, Jinny H.
ea81033c-8f9b-427b-be10-7a320a3f2651
Chan, H.T. Claude
b109c93f-7e9a-44ee-ad12-da757b1b11fc
Mockridge, C. Ian
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Duriez, Patrick J.
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Rogel, Anne
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Crispin, Max
cd980957-0943-4b89-b2b2-710f01f33bc9
Al-Shamkhani, Aymen
0a40b3ce-9d71-4d41-9369-7212f0a84504
Dadas, Osman, Allen, Joel D., Buchan, Sarah L., Kim, Jinny H., Chan, H.T. Claude, Mockridge, C. Ian, Duriez, Patrick J., Rogel, Anne, Crispin, Max and Al-Shamkhani, Aymen
(2023)
Fcγ receptor binding is required for maximal immunostimulation by CD70-Fc.
Frontiers in Immunology, 14, [1252274].
(doi:10.3389/fimmu.2023.1252274).
Abstract
Introduction: T cell expressed CD27 provides costimulation upon binding to inducible membrane expressed trimeric CD70 and is required for protective CD8 T cell responses. CD27 agonists could therefore be used to bolster cellular vaccines and anti-tumour immune responses. To date, clinical development of CD27 agonists has focussed on anti-CD27 antibodies with little attention given to alternative approaches.
Methods: here, we describe the generation and activity of soluble variants of CD70 that form either trimeric (t) or dimer-of-trimer proteins and conduct side-by-side comparisons with an agonist anti-CD27 antibody. To generate a dimer-of-trimer protein (dt), we fused three extracellular domains of CD70 to the Fc domain of mouse IgG1 in a ‘string of beads’ configuration (dtCD70-Fc).
Results: whereas tCD70 failed to costimulate CD8 T cells, both dtCD70-Fc and an agonist anti-CD27 antibody were capable of enhancing T cell proliferation in vitro. Initial studies demonstrated that dtCD70-Fc was less efficacious than anti-CD27 in boosting a CD8 T cell vaccine response in vivo, concomitant with rapid clearance of dtCD70-Fc from the circulation. The accelerated plasma clearance of dtCD70-Fc was not due to the lack of neonatal Fc receptor binding but was dependent on the large population of oligomannose type glycosylation. Enzymatic treatment to reduce the oligomannose-type glycans in dtCD70-Fc improved its half-life and significantly enhanced its T cell stimulatory activity in vivo surpassing that of anti-CD27 antibody. We also show that whereas the ability of the anti-CD27 to boost a vaccine response was abolished in Fc gamma receptor (FcγR)-deficient mice, dtCD70-Fc remained active. By comparing the activity of dtCD70-Fc with a variant (dtCD70-Fc(D265A)) that lacks binding to FcγRs, we unexpectedly found that FcγR binding to dtCD70-Fc was required for maximal boosting of a CD8 T cell response in vivo. Interestingly, both dtCD70-Fc and dtCD70-Fc(D265A) were effective in prolonging the survival of mice harbouring BCL1 B cell lymphoma, demonstrating that a substantial part of the stimulatory activity of dtCD70-Fc in this setting is retained in the absence of FcγR interaction.
Discussion: these data reveal that TNFRSF ligands can be generated with a tunable activity profile and suggest that this class of immune agonists could have broad applications in immunotherapy.
Text
Dadas et al Frontiers in Immunology accepted 16_10_23
- Accepted Manuscript
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fimmu-14-1252274
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More information
Accepted/In Press date: 16 October 2023
e-pub ahead of print date: 27 October 2023
Published date: 27 October 2023
Additional Information:
Funding Information:
The author(s) declare financial support was received for the research, authorship, and/or publication of this article. This work was funded by a Cancer Research UK grant (C1431/A21621). MC gratefully acknowledges support by Against Breast Cancer. Acknowledgments
Publisher Copyright:
Copyright © 2023 Dadas, Allen, Buchan, Kim, Chan, Mockridge, Duriez, Rogel, Crispin and Al-Shamkhani.
Keywords:
cancer, CD27, costimulation, immunotherapy, T cells, TNFRSF, vaccine
Identifiers
Local EPrints ID: 483277
URI: http://eprints.soton.ac.uk/id/eprint/483277
ISSN: 1664-3224
PURE UUID: 18866da4-71a7-4469-aaf2-77bce964c843
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Date deposited: 27 Oct 2023 16:32
Last modified: 18 Mar 2024 04:03
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Contributors
Author:
Osman Dadas
Author:
Sarah L. Buchan
Author:
Jinny H. Kim
Author:
H.T. Claude Chan
Author:
C. Ian Mockridge
Author:
Patrick J. Duriez
Author:
Anne Rogel
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