A critical function for CD200 in lung immune homeostasis and the severity of influenza infection

Robert J. Snelgrove; John Goulding; Arnaud M. Didierlaurent; Daphne Lyonga; Seema Vekaria; Lorna Edwards; Emily Gwyer; Jonathon D. Sedgwick; A. Neil Barclay; Tracy Hussell

doi:10.1038/ni.1637

A critical function for CD200 in lung immune homeostasis and the severity of influenza infection

Robert J. Snelgrove, John Goulding, Arnaud M. Didierlaurent, Daphne Lyonga, Seema Vekaria, Lorna Edwards, Emily Gwyer, Jonathon D. Sedgwick, A. Neil Barclay, Tracy Hussell

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

Abstract

The lung must maintain a high threshold of immune 'ignorance' to innocuous antigens to avoid inflammatory disease that depends on the balance of positive inflammatory signals and repressor pathways. We demonstrate here that airway macrophages had higher expression of the negative regulator CD200 receptor (CD200R) than did their systemic counterparts. Lung macrophages were restrained by CD200 expressed on airway epithelium. Mice lacking CD200 had more macrophage activity and enhanced sensitivity to influenza infection, which led to delayed resolution of inflammation and, ultimately, death. The administration of agonists that bind CD200R, however, prevented inflammatory lung disease. Thus, CD200R is critical for lung macrophage immune homeostasis in the resting state and limits inflammatory amplitude and duration during pulmonary influenza infection.

Original language	English
Pages (from-to)	1074-1083
Number of pages	9
Journal	Nature Immunology
Volume	9
Issue number	9
DOIs	https://doi.org/10.1038/ni.1637
Publication status	Published - 2008

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10.1038/ni.1637

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title = "A critical function for CD200 in lung immune homeostasis and the severity of influenza infection",

abstract = "The lung must maintain a high threshold of immune 'ignorance' to innocuous antigens to avoid inflammatory disease that depends on the balance of positive inflammatory signals and repressor pathways. We demonstrate here that airway macrophages had higher expression of the negative regulator CD200 receptor (CD200R) than did their systemic counterparts. Lung macrophages were restrained by CD200 expressed on airway epithelium. Mice lacking CD200 had more macrophage activity and enhanced sensitivity to influenza infection, which led to delayed resolution of inflammation and, ultimately, death. The administration of agonists that bind CD200R, however, prevented inflammatory lung disease. Thus, CD200R is critical for lung macrophage immune homeostasis in the resting state and limits inflammatory amplitude and duration during pulmonary influenza infection.",

author = "Snelgrove, {Robert J.} and John Goulding and Didierlaurent, {Arnaud M.} and Daphne Lyonga and Seema Vekaria and Lorna Edwards and Emily Gwyer and Sedgwick, {Jonathon D.} and Barclay, {A. Neil} and Tracy Hussell",

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AU - Snelgrove, Robert J.

AU - Goulding, John

AU - Didierlaurent, Arnaud M.

AU - Lyonga, Daphne

AU - Vekaria, Seema

AU - Edwards, Lorna

AU - Gwyer, Emily

AU - Sedgwick, Jonathon D.

AU - Barclay, A. Neil

AU - Hussell, Tracy

PY - 2008

Y1 - 2008

N2 - The lung must maintain a high threshold of immune 'ignorance' to innocuous antigens to avoid inflammatory disease that depends on the balance of positive inflammatory signals and repressor pathways. We demonstrate here that airway macrophages had higher expression of the negative regulator CD200 receptor (CD200R) than did their systemic counterparts. Lung macrophages were restrained by CD200 expressed on airway epithelium. Mice lacking CD200 had more macrophage activity and enhanced sensitivity to influenza infection, which led to delayed resolution of inflammation and, ultimately, death. The administration of agonists that bind CD200R, however, prevented inflammatory lung disease. Thus, CD200R is critical for lung macrophage immune homeostasis in the resting state and limits inflammatory amplitude and duration during pulmonary influenza infection.

AB - The lung must maintain a high threshold of immune 'ignorance' to innocuous antigens to avoid inflammatory disease that depends on the balance of positive inflammatory signals and repressor pathways. We demonstrate here that airway macrophages had higher expression of the negative regulator CD200 receptor (CD200R) than did their systemic counterparts. Lung macrophages were restrained by CD200 expressed on airway epithelium. Mice lacking CD200 had more macrophage activity and enhanced sensitivity to influenza infection, which led to delayed resolution of inflammation and, ultimately, death. The administration of agonists that bind CD200R, however, prevented inflammatory lung disease. Thus, CD200R is critical for lung macrophage immune homeostasis in the resting state and limits inflammatory amplitude and duration during pulmonary influenza infection.

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SP - 1074

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JO - Nature Immunology

JF - Nature Immunology

IS - 9

ER -

A critical function for CD200 in lung immune homeostasis and the severity of influenza infection

Abstract

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