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Structure-guided disulfide engineering restricts antibody conformation to elicit TNFR agonism

Structure-guided disulfide engineering restricts antibody conformation to elicit TNFR agonism
Structure-guided disulfide engineering restricts antibody conformation to elicit TNFR agonism

A promising strategy in cancer immunotherapy is activation of immune signalling pathways through antibodies that target co-stimulatory receptors. hIgG2, one of four human antibody isotypes, is known to deliver strong agonistic activity, and modification of hIgG2 hinge disulfides can influence immune-stimulating activity. This was shown for antibodies directed against the hCD40 receptor, where cysteine-to-serine exchange mutations caused changes in antibody conformational flexibility. Here we demonstrate that the principles of increasing agonism by restricting antibody conformation through disulfide modification can be translated to the co-stimulatory receptor h4-1BB, another member of the tumour necrosis factor receptor superfamily. Furthermore, we explore structure-guided design of the anti-hCD40 antibody ChiLob7/4 and show that engineering additional disulfides between opposing F(ab’) arms can elicit conformational restriction, concomitant with enhanced agonism. These results support a mode where subtle increases in rigidity can deliver significant improvements in immunostimulatory activity, thus providing a strategy for the rational design of more powerful antibody therapeutics.

2041-1723
Elliott, Isabel G.
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Fisher, Hayden
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Chan, H.T. Claude
b109c93f-7e9a-44ee-ad12-da757b1b11fc
Inzhelevskaya, Tatyana
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Mockridge, C. Ian
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Penfold, Christine A.
400d743e-a639-45ea-a027-5b778800f6d3
Duriez, Patrick J.
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Orr, Christian M.
f64259af-4120-481a-8e12-11344d005de0
Herniman, Julie
530b1a36-1386-4602-8df7-defa6eb3512b
Müller, Kri T.J.
2a2ec30f-a037-44b3-816d-c6fd1d0a0ce9
Essex, Jonathan W.
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Cragg, Mark S.
ec97f80e-f3c8-49b7-a960-20dff648b78c
Tews, Ivo
9117fc5e-d01c-4f8d-a734-5b14d3eee8dd
Elliott, Isabel G.
96cc4cfc-e3f8-4548-91b0-6eb4f04647a6
Fisher, Hayden
4ae88aa8-e168-4882-9563-3e5840b32bd6
Chan, H.T. Claude
b109c93f-7e9a-44ee-ad12-da757b1b11fc
Inzhelevskaya, Tatyana
2d84ec97-18c9-4406-a96b-206c21eae7d5
Mockridge, C. Ian
327aef17-4837-4f2a-a93b-3d17cd1a7f9f
Penfold, Christine A.
400d743e-a639-45ea-a027-5b778800f6d3
Duriez, Patrick J.
4cf499bc-007a-43b3-b180-d6e5dc3d151b
Orr, Christian M.
f64259af-4120-481a-8e12-11344d005de0
Herniman, Julie
530b1a36-1386-4602-8df7-defa6eb3512b
Müller, Kri T.J.
2a2ec30f-a037-44b3-816d-c6fd1d0a0ce9
Essex, Jonathan W.
1f409cfe-6ba4-42e2-a0ab-a931826314b5
Cragg, Mark S.
ec97f80e-f3c8-49b7-a960-20dff648b78c
Tews, Ivo
9117fc5e-d01c-4f8d-a734-5b14d3eee8dd

Elliott, Isabel G., Fisher, Hayden, Chan, H.T. Claude, Inzhelevskaya, Tatyana, Mockridge, C. Ian, Penfold, Christine A., Duriez, Patrick J., Orr, Christian M., Herniman, Julie, Müller, Kri T.J., Essex, Jonathan W., Cragg, Mark S. and Tews, Ivo (2025) Structure-guided disulfide engineering restricts antibody conformation to elicit TNFR agonism. Nature Communications, 16 (1), [3495]. (doi:10.1038/s41467-025-58773-8).

Record type: Article

Abstract

A promising strategy in cancer immunotherapy is activation of immune signalling pathways through antibodies that target co-stimulatory receptors. hIgG2, one of four human antibody isotypes, is known to deliver strong agonistic activity, and modification of hIgG2 hinge disulfides can influence immune-stimulating activity. This was shown for antibodies directed against the hCD40 receptor, where cysteine-to-serine exchange mutations caused changes in antibody conformational flexibility. Here we demonstrate that the principles of increasing agonism by restricting antibody conformation through disulfide modification can be translated to the co-stimulatory receptor h4-1BB, another member of the tumour necrosis factor receptor superfamily. Furthermore, we explore structure-guided design of the anti-hCD40 antibody ChiLob7/4 and show that engineering additional disulfides between opposing F(ab’) arms can elicit conformational restriction, concomitant with enhanced agonism. These results support a mode where subtle increases in rigidity can deliver significant improvements in immunostimulatory activity, thus providing a strategy for the rational design of more powerful antibody therapeutics.

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Accepted/In Press date: 28 March 2025
Published date: 12 April 2025
Additional Information: Publisher Copyright: © The Author(s) 2025.
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Identifiers

Local EPrints ID: 502459
URI: http://eprints.soton.ac.uk/id/eprint/502459
DOI: doi:10.1038/s41467-025-58773-8
ISSN: 2041-1723
PURE UUID: 95edc26e-e080-4019-bc8d-edde4a33cf5e
ORCID for Isabel G. Elliott: ORCID iD orcid.org/0000-0003-4535-5932
ORCID for H.T. Claude Chan: ORCID iD orcid.org/0000-0003-0530-9480
ORCID for Patrick J. Duriez: ORCID iD orcid.org/0000-0003-1814-2552
ORCID for Christian M. Orr: ORCID iD orcid.org/0000-0002-6137-8969
ORCID for Julie Herniman: ORCID iD orcid.org/0000-0003-4834-1093
ORCID for Kri T.J. Müller: ORCID iD orcid.org/0000-0001-5674-6125
ORCID for Jonathan W. Essex: ORCID iD orcid.org/0000-0003-2639-2746
ORCID for Mark S. Cragg: ORCID iD orcid.org/0000-0003-2077-089X
ORCID for Ivo Tews: ORCID iD orcid.org/0000-0002-4704-1139

Catalogue record

Date deposited: 26 Jun 2025 17:06
Last modified: 22 Aug 2025 02:33

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Contributors

Author: Isabel G. Elliott ORCID iD
Author: Hayden Fisher
Author: H.T. Claude Chan ORCID iD
Author: Tatyana Inzhelevskaya
Author: C. Ian Mockridge
Author: Christine A. Penfold
Author: Patrick J. Duriez ORCID iD
Author: Christian M. Orr ORCID iD
Author: Julie Herniman ORCID iD
Author: Kri T.J. Müller ORCID iD
Author: Jonathan W. Essex ORCID iD
Author: Mark S. Cragg ORCID iD
Author: Ivo Tews ORCID iD

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