A monoclonal antibody to Siglec-8 suppresses non-allergic airway inflammation and inhibits IgE-independent mast cell activation

Julia Schanin; Simon Gebremeskel; Wouter Korver; Rustom Falahati; Melina Butuci; Tatt Jhong Haw; Prema M. Nair; Gang Liu; Nicole G. Hansbro; Philip M. Hansbro; Erik Evensen; Emily C. Brock; Alan Xu; Alan Wong; John Leung; Christopher Bebbington; Nenad Tomasevic; Bradford A. Youngblood

doi:10.1038/s41385-020-00336-9

A monoclonal antibody to Siglec-8 suppresses non-allergic airway inflammation and inhibits IgE-independent mast cell activation

Julia Schanin, Simon Gebremeskel, Wouter Korver, Rustom Falahati, Melina Butuci, Tatt Jhong Haw, Prema M. Nair, Gang Liu, Nicole G. Hansbro, Philip M. Hansbro, Erik Evensen, Emily C. Brock, Alan Xu, Alan Wong, John Leung, Christopher Bebbington, Nenad Tomasevic, Bradford A. Youngblood

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65 Citas (Scopus)

Resumen

In addition to their well characterized role in mediating IgE-dependent allergic diseases, aberrant accumulation and activation of mast cells (MCs) is associated with many non-allergic inflammatory diseases, whereby their activation is likely triggered by non-IgE stimuli (e.g., IL-33). Siglec-8 is an inhibitory receptor expressed on MCs and eosinophils that has been shown to inhibit IgE-mediated MC responses and reduce allergic inflammation upon ligation with a monoclonal antibody (mAb). Herein, we evaluated the effects of an anti-Siglec-8 mAb (anti-S8) in non-allergic disease models of experimental cigarette-smoke-induced chronic obstructive pulmonary disease and bleomycin-induced lung injury in Siglec-8 transgenic mice. Therapeutic treatment with anti-S8 inhibited MC activation and reduced recruitment of immune cells, airway inflammation, and lung fibrosis. Similarly, using a model of MC-dependent, IL-33-induced inflammation, anti-S8 treatment suppressed neutrophil influx, and cytokine production through MC inhibition. Transcriptomic profiling of MCs further demonstrated anti-S8-mediated downregulation of MC signaling pathways induced by IL-33, including TNF signaling via NF-κB. Collectively, these findings demonstrate that ligating Siglec-8 with an antibody reduces non-allergic inflammation and inhibits IgE-independent MC activation, supporting the evaluation of an anti-Siglec-8 mAb as a therapeutic approach in both allergic and non-allergic inflammatory diseases in which MCs play a role.

Idioma original	English
Páginas (desde-hasta)	366-376
Número de páginas	11
Publicación	Mucosal Immunology
Volumen	14
N.º	2
DOI	https://doi.org/10.1038/s41385-020-00336-9
Estado	Published - mar. 2021
Publicado de forma externa	Sí

Nota bibliográfica

Funding Information:
We thank Drs. Bruce S. Bochner and Robert P. Schleimer for their critical review and feedback on the manuscript and Ingrid Koo, Ph.D. for writing support. Research was funded by Allakos, Inc. PMH is funded by a Fellowship and grants from the National Health and Medical Research Council (NHMRC) of Australia (1079187, 1175134, and 1023131) and the Australian Research Council (150102153). P.M.H. and N.G.H. are supported by the University of Technology Sydney. Research was funded by Allakos, Inc. PMH is funded by a Fellowship and grants from the National Health and Medical Research Council (NHMRC) of Australia (1079187, 1175134, and 1023131) and the Australian Research Council (150102153). P.M.H. and N.G.H. are supported by the University of Technology Sydney.

Publisher Copyright:
© 2020, The Author(s).

ASJC Scopus Subject Areas

Immunology and Allergy
Immunology

PubMed: MeSH publication types

Journal Article
Research Support, Non-U.S. Gov't

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10.1038/s41385-020-00336-9

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Schanin, J., Gebremeskel, S., Korver, W., Falahati, R., Butuci, M., Haw, T. J., Nair, P. M., Liu, G., Hansbro, N. G., Hansbro, P. M., Evensen, E., Brock, E. C., Xu, A., Wong, A., Leung, J., Bebbington, C., Tomasevic, N., & Youngblood, B. A. (2021). A monoclonal antibody to Siglec-8 suppresses non-allergic airway inflammation and inhibits IgE-independent mast cell activation. Mucosal Immunology, 14(2), 366-376. https://doi.org/10.1038/s41385-020-00336-9

Schanin, J, Gebremeskel, S, Korver, W, Falahati, R, Butuci, M, Haw, TJ, Nair, PM, Liu, G, Hansbro, NG, Hansbro, PM, Evensen, E, Brock, EC, Xu, A, Wong, A, Leung, J, Bebbington, C, Tomasevic, N & Youngblood, BA 2021, 'A monoclonal antibody to Siglec-8 suppresses non-allergic airway inflammation and inhibits IgE-independent mast cell activation', Mucosal Immunology, vol. 14, n.º 2, pp. 366-376. https://doi.org/10.1038/s41385-020-00336-9

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title = "A monoclonal antibody to Siglec-8 suppresses non-allergic airway inflammation and inhibits IgE-independent mast cell activation",

abstract = "In addition to their well characterized role in mediating IgE-dependent allergic diseases, aberrant accumulation and activation of mast cells (MCs) is associated with many non-allergic inflammatory diseases, whereby their activation is likely triggered by non-IgE stimuli (e.g., IL-33). Siglec-8 is an inhibitory receptor expressed on MCs and eosinophils that has been shown to inhibit IgE-mediated MC responses and reduce allergic inflammation upon ligation with a monoclonal antibody (mAb). Herein, we evaluated the effects of an anti-Siglec-8 mAb (anti-S8) in non-allergic disease models of experimental cigarette-smoke-induced chronic obstructive pulmonary disease and bleomycin-induced lung injury in Siglec-8 transgenic mice. Therapeutic treatment with anti-S8 inhibited MC activation and reduced recruitment of immune cells, airway inflammation, and lung fibrosis. Similarly, using a model of MC-dependent, IL-33-induced inflammation, anti-S8 treatment suppressed neutrophil influx, and cytokine production through MC inhibition. Transcriptomic profiling of MCs further demonstrated anti-S8-mediated downregulation of MC signaling pathways induced by IL-33, including TNF signaling via NF-κB. Collectively, these findings demonstrate that ligating Siglec-8 with an antibody reduces non-allergic inflammation and inhibits IgE-independent MC activation, supporting the evaluation of an anti-Siglec-8 mAb as a therapeutic approach in both allergic and non-allergic inflammatory diseases in which MCs play a role.",

author = "Julia Schanin and Simon Gebremeskel and Wouter Korver and Rustom Falahati and Melina Butuci and Haw, {Tatt Jhong} and Nair, {Prema M.} and Gang Liu and Hansbro, {Nicole G.} and Hansbro, {Philip M.} and Erik Evensen and Brock, {Emily C.} and Alan Xu and Alan Wong and John Leung and Christopher Bebbington and Nenad Tomasevic and Youngblood, {Bradford A.}",

note = "Funding Information: We thank Drs. Bruce S. Bochner and Robert P. Schleimer for their critical review and feedback on the manuscript and Ingrid Koo, Ph.D. for writing support. Research was funded by Allakos, Inc. PMH is funded by a Fellowship and grants from the National Health and Medical Research Council (NHMRC) of Australia (1079187, 1175134, and 1023131) and the Australian Research Council (150102153). P.M.H. and N.G.H. are supported by the University of Technology Sydney. Research was funded by Allakos, Inc. PMH is funded by a Fellowship and grants from the National Health and Medical Research Council (NHMRC) of Australia (1079187, 1175134, and 1023131) and the Australian Research Council (150102153). P.M.H. and N.G.H. are supported by the University of Technology Sydney. Publisher Copyright: {\textcopyright} 2020, The Author(s).",

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AU - Schanin, Julia

AU - Gebremeskel, Simon

AU - Korver, Wouter

AU - Falahati, Rustom

AU - Butuci, Melina

AU - Haw, Tatt Jhong

AU - Nair, Prema M.

AU - Liu, Gang

AU - Hansbro, Nicole G.

AU - Hansbro, Philip M.

AU - Evensen, Erik

AU - Brock, Emily C.

AU - Xu, Alan

AU - Wong, Alan

AU - Leung, John

AU - Bebbington, Christopher

AU - Tomasevic, Nenad

AU - Youngblood, Bradford A.

N1 - Funding Information: We thank Drs. Bruce S. Bochner and Robert P. Schleimer for their critical review and feedback on the manuscript and Ingrid Koo, Ph.D. for writing support. Research was funded by Allakos, Inc. PMH is funded by a Fellowship and grants from the National Health and Medical Research Council (NHMRC) of Australia (1079187, 1175134, and 1023131) and the Australian Research Council (150102153). P.M.H. and N.G.H. are supported by the University of Technology Sydney. Research was funded by Allakos, Inc. PMH is funded by a Fellowship and grants from the National Health and Medical Research Council (NHMRC) of Australia (1079187, 1175134, and 1023131) and the Australian Research Council (150102153). P.M.H. and N.G.H. are supported by the University of Technology Sydney. Publisher Copyright: © 2020, The Author(s).

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N2 - In addition to their well characterized role in mediating IgE-dependent allergic diseases, aberrant accumulation and activation of mast cells (MCs) is associated with many non-allergic inflammatory diseases, whereby their activation is likely triggered by non-IgE stimuli (e.g., IL-33). Siglec-8 is an inhibitory receptor expressed on MCs and eosinophils that has been shown to inhibit IgE-mediated MC responses and reduce allergic inflammation upon ligation with a monoclonal antibody (mAb). Herein, we evaluated the effects of an anti-Siglec-8 mAb (anti-S8) in non-allergic disease models of experimental cigarette-smoke-induced chronic obstructive pulmonary disease and bleomycin-induced lung injury in Siglec-8 transgenic mice. Therapeutic treatment with anti-S8 inhibited MC activation and reduced recruitment of immune cells, airway inflammation, and lung fibrosis. Similarly, using a model of MC-dependent, IL-33-induced inflammation, anti-S8 treatment suppressed neutrophil influx, and cytokine production through MC inhibition. Transcriptomic profiling of MCs further demonstrated anti-S8-mediated downregulation of MC signaling pathways induced by IL-33, including TNF signaling via NF-κB. Collectively, these findings demonstrate that ligating Siglec-8 with an antibody reduces non-allergic inflammation and inhibits IgE-independent MC activation, supporting the evaluation of an anti-Siglec-8 mAb as a therapeutic approach in both allergic and non-allergic inflammatory diseases in which MCs play a role.

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A monoclonal antibody to Siglec-8 suppresses non-allergic airway inflammation and inhibits IgE-independent mast cell activation

Resumen

Nota bibliográfica

ASJC Scopus Subject Areas

PubMed: MeSH publication types

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