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Antigen discrimination by T cells relies on size-constrained microvillar contact.

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Peer-reviewed

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Abstract

T cells use finger-like protrusions called 'microvilli' to interrogate their targets, but why they do so is unknown. To form contacts, T cells must overcome the highly charged, barrier-like layer of large molecules forming a target cell's glycocalyx. Here, T cells are observed to use microvilli to breach a model glycocalyx barrier, forming numerous small (<0.5 μm diameter) contacts each of which is stabilized by the small adhesive protein CD2 expressed by the T cell, and excludes large proteins including CD45, allowing sensitive, antigen dependent TCR signaling. In the absence of the glycocalyx or when microvillar contact-size is increased by enhancing CD2 expression, strong signaling occurs that is no longer antigen dependent. Our observations suggest that, modulated by the opposing effects of the target cell glycocalyx and small adhesive proteins, the use of microvilli equips T cells with the ability to effect discriminatory receptor signaling.

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Acknowledgements: The authors thank Professors P. A. van der Merwe, P. Jönsson, M. L. Dustin, and Dr. Y. Lui for helpful discussion and comments on the manuscript, Professor O. Dushek and Dr. J. Pettman for providing sequences, prior to publication, of weakly-agonistic peptides, A. Mørch for providing the pHR-Lck-HaloTag plasmid, M. Vuong for pMHC refolding, the staff of the WIMM FACS Facility for cell sorting, and Dr. C. Lagerholm for help with the microscopy. We also thank the staff of the Wolfson Imaging Centre, University of Oxford, for providing access to their imaging facility. This work was funded by the Wellcome Trust (Grant 207547/Z/17/Z awarded to S.J.D.) and by a Royal Society Research Professorship (RP150066 awarded to D.K.).

Journal Title

Nat Commun

Conference Name

Journal ISSN

2041-1723
2041-1723

Volume Title

Publisher

Springer Science and Business Media LLC

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Except where otherwised noted, this item's license is described as http://creativecommons.org/licenses/by/4.0/
Sponsorship
Wellcome Trust (via University of Oxford) (207547/Z/17/Z)