Hinge disulfides in human IgG2 CD40 antibodies modulate receptor signaling by 
regulation of conformation and flexibility

Orr, C. M.; Fisher, H.; Yu, X.; Chan, C. H.-T.; Gao, Y.; Duriez, P. J.; Booth, S. G.; Elliott, I.; Inzhelevskaya, T.; Mockridge, I.; Penfold, C. A.; Wagner, A.; Glennie, M. J.; White, A. L.; Essex, J. W.; Pearson, A. R.; Cragg, M. S.; Tews, I.

doi:10.1126/sciimmunol.abm3723

Item

ITEM ACTIONSEXPORT

Add to Basket

Local TagsRelease HistoryDetailsSummary

Released

Journal Article

Hinge disulfides in human IgG2 CD40 antibodies modulate receptor signaling by regulation of conformation and flexibility

MPS-Authors

/persons/resource/persons196435

Gao, Y.
Hamburg Centre for Ultrafast Imaging CFEL;
Institute for Nanostructure and Solid State Physics;
International Max Planck Research School for Ultrafast Imaging & Structural Dynamics (IMPRS-UFAST), Max Planck Institute for the Structure and Dynamics of Matter, Max Planck Society;

External Resource

https://doi.org/10.1126/sciimmunol.abm3723
(Publisher version)

Fulltext (restricted access)

There are currently no full texts shared for your IP range.

Fulltext (public)

There are no public fulltexts stored in PuRe

Supplementary Material (public)

suppl.zip
(Supplementary material), 8MB

Citation

Orr, C. M., Fisher, H., Yu, X., Chan, C.-H.-T., Gao, Y., Duriez, P. J., et al. (2022). Hinge disulfides in human IgG2 CD40 antibodies modulate receptor signaling by regulation of conformation and flexibility. Science Immunology, 7(73): eabm3723. doi:10.1126/sciimmunol.abm3723.

Cite as: https://hdl.handle.net/21.11116/0000-000A-B45B-5

Abstract

Antibodies protect from infection, underpin successful vaccines and elicit therapeutic responses in otherwise untreatable cancers and autoimmune conditions. The human IgG2 isotype displays a unique capacity to undergo disulfide shuffling in the hinge region, leading to modulation of its ability to drive target receptor signaling (agonism) in a variety of important immune receptors, through hitherto unexplained molecular mechanisms. To address the underlying process and reveal how hinge disulfide orientation affects agonistic activity, we generated a series of cysteine to serine exchange variants in the hinge region of the clinically relevant monoclonal antibody ChiLob7/4, directed against the key immune receptor CD40. We report how agonistic activity varies with disulfide pattern and is afforded by the presence of a disulfide crossover between F(ab) arms in the agonistic forms, independently of epitope, as observed in the determined crystallographic structures. This structural “switch” affects directly on antibody conformation and flexibility. Small-angle x-ray scattering and ensemble modeling demonstrated that the least flexible variants adopt the fewest conformations and evoke the highest levels of receptor agonism. This covalent change may be amenable for broad implementation to modulate receptor signaling in an epitope-independent manner in future therapeutics.