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Fc-γ receptor-mediated crosslinking co-defines the immunostimulatory activity of anti-human CD96 antibodies

Fc-γ receptor-mediated crosslinking co-defines the immunostimulatory activity of anti-human CD96 antibodies
Fc-γ receptor-mediated crosslinking co-defines the immunostimulatory activity of anti-human CD96 antibodies
New strategies that augment T-cell responses are required to broaden the therapeutic arsenal against cancer. CD96, TIGIT and CD226 are receptors that bind to a communal ligand, CD155, and transduce either inhibitory or activating signals. Whereas the function of TIGIT and CD226 is established, the role of CD96 remains ambiguous. Using a panel of engineered antibodies, we discovered that the T-cell stimulatory activity of anti-CD96 antibodies requires antibody crosslinking and is potentiated by Fc-gamma receptors. Thus, soluble 'Fc silent' anti-CD96 antibodies failed to stimulate human T cells, whereas the same antibodies were stimulatory after coating onto plastic surfaces. Remarkably, the activity of soluble anti-CD96 antibodies was reinstated by engineering the Fc domain to a human IgG1 isotype and was dependent on antibody trans-crosslinking by Fc-γRI. In contrast, neither human IgG2 nor variants with increased Fc-γ receptor IIB binding possessed stimulatory activity. Anti-CD96 antibodies acted directly on T cells and augmented gene expression networks associated with T-cell activation, leading to proliferation, cytokine secretion and resistance to regulatory T-cell suppression. Furthermore, CD96 expression correlated with survival in HPV+ head and neck squamous cell carcinoma and its crosslinking activated tumor-infiltrating T cells, thus highlighting the potential of anti-CD96 antibodies in cancer immunotherapy.
2379-3708
Rogel, Anne
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Ibrahim, Fathima M
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Thirdborough, Stephen
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Renart-Depontieu, Florence
d215b05e-d068-4af1-ae6a-8cf47c83d37c
Birts, Charles
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Buchan, Sarah
87e38403-54ed-4d88-802c-9a1107b7d304
Preville, Xavier
c329385f-698f-4022-86c1-431b864787bb
King, Emma
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Al-Shamkhani, Aymen
0a40b3ce-9d71-4d41-9369-7212f0a84504
Rogel, Anne
5a895ba8-c877-484f-a9c1-34a2b1af6414
Ibrahim, Fathima M
b1436b35-1117-4a45-ab18-6235af2a3f6c
Thirdborough, Stephen
161784fb-c8e3-4beb-86b1-cd8bc8ddf8de
Renart-Depontieu, Florence
d215b05e-d068-4af1-ae6a-8cf47c83d37c
Birts, Charles
8689ddad-ba47-4ca6-82c5-001315dbd250
Buchan, Sarah
87e38403-54ed-4d88-802c-9a1107b7d304
Preville, Xavier
c329385f-698f-4022-86c1-431b864787bb
King, Emma
d85e0e8f-7295-4912-9052-646a790d99db
Al-Shamkhani, Aymen
0a40b3ce-9d71-4d41-9369-7212f0a84504

Rogel, Anne, Ibrahim, Fathima M, Thirdborough, Stephen, Renart-Depontieu, Florence, Birts, Charles, Buchan, Sarah, Preville, Xavier, King, Emma and Al-Shamkhani, Aymen (2022) Fc-γ receptor-mediated crosslinking co-defines the immunostimulatory activity of anti-human CD96 antibodies. JCI Insight, 7 (19), [e158444]. (doi:10.1172/jci.insight.158444).

Record type: Article

Abstract

New strategies that augment T-cell responses are required to broaden the therapeutic arsenal against cancer. CD96, TIGIT and CD226 are receptors that bind to a communal ligand, CD155, and transduce either inhibitory or activating signals. Whereas the function of TIGIT and CD226 is established, the role of CD96 remains ambiguous. Using a panel of engineered antibodies, we discovered that the T-cell stimulatory activity of anti-CD96 antibodies requires antibody crosslinking and is potentiated by Fc-gamma receptors. Thus, soluble 'Fc silent' anti-CD96 antibodies failed to stimulate human T cells, whereas the same antibodies were stimulatory after coating onto plastic surfaces. Remarkably, the activity of soluble anti-CD96 antibodies was reinstated by engineering the Fc domain to a human IgG1 isotype and was dependent on antibody trans-crosslinking by Fc-γRI. In contrast, neither human IgG2 nor variants with increased Fc-γ receptor IIB binding possessed stimulatory activity. Anti-CD96 antibodies acted directly on T cells and augmented gene expression networks associated with T-cell activation, leading to proliferation, cytokine secretion and resistance to regulatory T-cell suppression. Furthermore, CD96 expression correlated with survival in HPV+ head and neck squamous cell carcinoma and its crosslinking activated tumor-infiltrating T cells, thus highlighting the potential of anti-CD96 antibodies in cancer immunotherapy.

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158444.1-20220822102742-covered-e0fd13ba177f913fd3156f593ead4cfd - Accepted Manuscript
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e-pub ahead of print date: 23 August 2022
Published date: 10 October 2022
Additional Information: Funding Information: former employees of BliNK Biomedical and Talix Therapeutics, respectively. AR, CNB, and FMI have received support from BliNK Biomedical and Talix Therapeutics. AAS has received grant funding from BliNK Biomedical and Talix Therapeutics. AR, FRD, XP, and AAS are coinventors on patent WO 2019/030377 Al from Talix Therapeutics. Funding Information: The authors thank François Romagné (MImAbs) and Christine Penfold (University of Southampton) for antibody production. This work was supported by grants from Talix Therapeutics and Cancer Research UK (A30681, A25778). Publisher Copyright: Copyright: © 2022, Rogel et al. This is an open access article published under the terms of the Creative Commons Attribution 4.0 International License.

Identifiers

Local EPrints ID: 469753
URI: http://eprints.soton.ac.uk/id/eprint/469753
ISSN: 2379-3708
PURE UUID: 46be4a0b-6864-4317-820f-f67a60bd9fcd
ORCID for Charles Birts: ORCID iD orcid.org/0000-0002-0368-8766
ORCID for Aymen Al-Shamkhani: ORCID iD orcid.org/0000-0003-0727-4189

Catalogue record

Date deposited: 23 Sep 2022 17:19
Last modified: 17 Mar 2024 02:56

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Contributors

Author: Anne Rogel
Author: Fathima M Ibrahim
Author: Florence Renart-Depontieu
Author: Charles Birts ORCID iD
Author: Sarah Buchan
Author: Xavier Preville
Author: Emma King

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