posted on 2019-05-01, 15:12authored byChristopher Brightling, Neil Greening
Chronic obstructive pulmonary disease (COPD) is a significant cause of
morbidity and mortality worldwide and its prevalence is increasing.
Airway inflammation is a consistent feature of COPD and is implicated in
the pathogenesis and progression of COPD, but anti-inflammatory
therapy is not first line treatment. This inflammation has many guises
and phenotyping this heterogeneity has revealed different patterns.
Neutrophil-associated COPD with activation of the inflammasome, T1 and
T17 immunity is the most common phenotype with eosinophil-associated
T2-mediated immunity in a minority and autoimmunity observed in more
severe disease. Biomarkers have enabled targeted anti-inflammatory
strategies and revealed that corticosteroids are most effective in those
with evidence of eosinophilic inflammation. Whereas in contrast to
severe asthma response to anti-IL5 biologics in COPD has been
disappointing with smaller benefits for the same intensity of eosinophilic
inflammation questioning its role in COPD. Biological therapies beyond
T2-mediated inflammation have not demonstrated benefit and in some
cases increased risk of infection suggesting that neutrophilic
inflammation and inflammasome activation might be largely driven by
bacterial colonisation and dysbiosis. Herein we shall describe current and
future biomarker approaches to assess inflammation in COPD and how
this might reveal tractable approaches to precision medicine and unmask
important host-environment interactions leading to airway inflammation.
Funding
Dr Neil J Greening- Dr Greening is funded by a NIHR post-doctoral fellowship (PDF-2017-
19 10-052)
History
Citation
European Respiratory Journal, 2019
Author affiliation
/Organisation/COLLEGE OF LIFE SCIENCES/School of Medicine/Department of Infection, Immunity and Inflammation
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