Divalent nanobodies to platelet CLEC-2 can serve as agonists or antagonists

Joanne C. Clark; Eleyna M. Martin; Luis A. Morán; Ying Di; Xueqing Wang; Malou Zuidscherwoude; Helena C. Brown; Deirdre M. Kavanagh; Johan Hummert; Johannes A. Eble; Bernhard Nieswandt; David Stegner; Alice Y. Pollitt; Dirk-peter Herten; Michael G. Tomlinson; Angel García; Steve P. Watson

doi:10.1038/s42003-023-04766-6

Divalent nanobodies to platelet CLEC-2 can serve as agonists or antagonists

Joanne C. Clark^*, Eleyna M. Martin, Luis A. Morán, Ying Di, Xueqing Wang, Malou Zuidscherwoude, Helena C. Brown, Deirdre M. Kavanagh, Johan Hummert, Johannes A. Eble, Bernhard Nieswandt, David Stegner, Alice Y. Pollitt, Dirk-peter Herten, Michael G. Tomlinson, Angel García, Steve P. Watson^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

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Abstract

CLEC-2 is a target for a new class of antiplatelet agent. Clustering of CLEC-2 leads to phosphorylation of a cytosolic YxxL and binding of the tandem SH2 domains in Syk, crosslinking two receptors. We have raised 48 nanobodies to CLEC-2 and crosslinked the most potent of these to generate divalent and tetravalent nanobody ligands. Fluorescence correlation spectroscopy (FCS) was used to show that the multivalent nanobodies cluster CLEC-2 in the membrane and that clustering is reduced by inhibition of Syk. Strikingly, the tetravalent nanobody stimulated aggregation of human platelets, whereas the divalent nanobody was an antagonist. In contrast, in human CLEC-2 knock-in mouse platelets, the divalent nanobody stimulated aggregation. Mouse platelets express a higher level of CLEC-2 than human platelets. In line with this, the divalent nanobody was an agonist in high-expressing transfected DT40 cells and an antagonist in low-expressing cells. FCS, stepwise photobleaching and non-detergent membrane extraction show that CLEC-2 is a mixture of monomers and dimers, with the degree of dimerisation increasing with expression thereby favouring crosslinking of CLEC-2 dimers. These results identify ligand valency, receptor expression/dimerisation and Syk as variables that govern activation of CLEC-2 and suggest that divalent ligands should be considered as partial agonists.

Original language	English
Article number	376
Number of pages	17
Journal	Communications Biology
Volume	6
Issue number	1
Early online date	7 Apr 2023
DOIs	https://doi.org/10.1038/s42003-023-04766-6
Publication status	Published - 7 Apr 2023

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Clark, J. C., Martin, E. M., Morán, L. A., Di, Y., Wang, X., Zuidscherwoude, M., Brown, H. C., Kavanagh, D. M., Hummert, J., Eble, J. A., Nieswandt, B., Stegner, D., Pollitt, A. Y., Herten, D., Tomlinson, M. G., García, A., & Watson, S. P. (2023). Divalent nanobodies to platelet CLEC-2 can serve as agonists or antagonists. Communications Biology, 6(1), Article 376. https://doi.org/10.1038/s42003-023-04766-6

@article{d37525efeb2b4b2f8ed7bf7ba75d7a8f,

title = "Divalent nanobodies to platelet CLEC-2 can serve as agonists or antagonists",

abstract = "CLEC-2 is a target for a new class of antiplatelet agent. Clustering of CLEC-2 leads to phosphorylation of a cytosolic YxxL and binding of the tandem SH2 domains in Syk, crosslinking two receptors. We have raised 48 nanobodies to CLEC-2 and crosslinked the most potent of these to generate divalent and tetravalent nanobody ligands. Fluorescence correlation spectroscopy (FCS) was used to show that the multivalent nanobodies cluster CLEC-2 in the membrane and that clustering is reduced by inhibition of Syk. Strikingly, the tetravalent nanobody stimulated aggregation of human platelets, whereas the divalent nanobody was an antagonist. In contrast, in human CLEC-2 knock-in mouse platelets, the divalent nanobody stimulated aggregation. Mouse platelets express a higher level of CLEC-2 than human platelets. In line with this, the divalent nanobody was an agonist in high-expressing transfected DT40 cells and an antagonist in low-expressing cells. FCS, stepwise photobleaching and non-detergent membrane extraction show that CLEC-2 is a mixture of monomers and dimers, with the degree of dimerisation increasing with expression thereby favouring crosslinking of CLEC-2 dimers. These results identify ligand valency, receptor expression/dimerisation and Syk as variables that govern activation of CLEC-2 and suggest that divalent ligands should be considered as partial agonists.",

author = "Clark, {Joanne C.} and Martin, {Eleyna M.} and Mor{\'a}n, {Luis A.} and Ying Di and Xueqing Wang and Malou Zuidscherwoude and Brown, {Helena C.} and Kavanagh, {Deirdre M.} and Johan Hummert and Eble, {Johannes A.} and Bernhard Nieswandt and David Stegner and Pollitt, {Alice Y.} and Dirk-peter Herten and Tomlinson, {Michael G.} and Angel Garc{\'i}a and Watson, {Steve P.}",

year = "2023",

month = apr,

day = "7",

doi = "10.1038/s42003-023-04766-6",

language = "English",

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journal = "Communications Biology",

issn = "2399-3642",

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Clark, JC , Martin, EM, Morán, LA, Di, Y, Wang, X, Zuidscherwoude, M, Brown, HC, Kavanagh, DM, Hummert, J, Eble, JA, Nieswandt, B, Stegner, D, Pollitt, AY, Herten, D , Tomlinson, MG, García, A & Watson, SP 2023, 'Divalent nanobodies to platelet CLEC-2 can serve as agonists or antagonists', Communications Biology, vol. 6, no. 1, 376. https://doi.org/10.1038/s42003-023-04766-6

TY - JOUR

T1 - Divalent nanobodies to platelet CLEC-2 can serve as agonists or antagonists

AU - Clark, Joanne C.

AU - Martin, Eleyna M.

AU - Morán, Luis A.

AU - Di, Ying

AU - Wang, Xueqing

AU - Zuidscherwoude, Malou

AU - Brown, Helena C.

AU - Kavanagh, Deirdre M.

AU - Hummert, Johan

AU - Eble, Johannes A.

AU - Nieswandt, Bernhard

AU - Stegner, David

AU - Pollitt, Alice Y.

AU - Herten, Dirk-peter

AU - Tomlinson, Michael G.

AU - García, Angel

AU - Watson, Steve P.

PY - 2023/4/7

Y1 - 2023/4/7

N2 - CLEC-2 is a target for a new class of antiplatelet agent. Clustering of CLEC-2 leads to phosphorylation of a cytosolic YxxL and binding of the tandem SH2 domains in Syk, crosslinking two receptors. We have raised 48 nanobodies to CLEC-2 and crosslinked the most potent of these to generate divalent and tetravalent nanobody ligands. Fluorescence correlation spectroscopy (FCS) was used to show that the multivalent nanobodies cluster CLEC-2 in the membrane and that clustering is reduced by inhibition of Syk. Strikingly, the tetravalent nanobody stimulated aggregation of human platelets, whereas the divalent nanobody was an antagonist. In contrast, in human CLEC-2 knock-in mouse platelets, the divalent nanobody stimulated aggregation. Mouse platelets express a higher level of CLEC-2 than human platelets. In line with this, the divalent nanobody was an agonist in high-expressing transfected DT40 cells and an antagonist in low-expressing cells. FCS, stepwise photobleaching and non-detergent membrane extraction show that CLEC-2 is a mixture of monomers and dimers, with the degree of dimerisation increasing with expression thereby favouring crosslinking of CLEC-2 dimers. These results identify ligand valency, receptor expression/dimerisation and Syk as variables that govern activation of CLEC-2 and suggest that divalent ligands should be considered as partial agonists.

AB - CLEC-2 is a target for a new class of antiplatelet agent. Clustering of CLEC-2 leads to phosphorylation of a cytosolic YxxL and binding of the tandem SH2 domains in Syk, crosslinking two receptors. We have raised 48 nanobodies to CLEC-2 and crosslinked the most potent of these to generate divalent and tetravalent nanobody ligands. Fluorescence correlation spectroscopy (FCS) was used to show that the multivalent nanobodies cluster CLEC-2 in the membrane and that clustering is reduced by inhibition of Syk. Strikingly, the tetravalent nanobody stimulated aggregation of human platelets, whereas the divalent nanobody was an antagonist. In contrast, in human CLEC-2 knock-in mouse platelets, the divalent nanobody stimulated aggregation. Mouse platelets express a higher level of CLEC-2 than human platelets. In line with this, the divalent nanobody was an agonist in high-expressing transfected DT40 cells and an antagonist in low-expressing cells. FCS, stepwise photobleaching and non-detergent membrane extraction show that CLEC-2 is a mixture of monomers and dimers, with the degree of dimerisation increasing with expression thereby favouring crosslinking of CLEC-2 dimers. These results identify ligand valency, receptor expression/dimerisation and Syk as variables that govern activation of CLEC-2 and suggest that divalent ligands should be considered as partial agonists.

U2 - 10.1038/s42003-023-04766-6

DO - 10.1038/s42003-023-04766-6

M3 - Article

SN - 2399-3642

VL - 6

JO - Communications Biology

JF - Communications Biology

IS - 1

M1 - 376

ER -

Divalent nanobodies to platelet CLEC-2 can serve as agonists or antagonists

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