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Inflammatory Molecular Endotypes in Bronchiectasis: A European Multicenter Cohort Study

Authors
Choi, HayoungRyu, SoorackKeir, Holly R.Giam, Yan HuiDicker, Alison J.Perea, LidiaRichardson, HollianHuang, Jeffrey T JCant, ErinBlasi, FrancescoPollock, JenniferShteinberg, MichalFinch, SimonAliberti, StefanoSibila, OriolShoemark, AmeliaChalmers, James D.
Issue Date
Dec-2023
Publisher
American Thoracic Society
Keywords
biomarkers; bronchiectasis; cluster analysis; inflammation; microbiome
Citation
American Journal of Respiratory and Critical Care Medicine, v.208, no.11, pp 1166 - 1176
Pages
11
Indexed
SCIE
SCOPUS
Journal Title
American Journal of Respiratory and Critical Care Medicine
Volume
208
Number
11
Start Page
1166
End Page
1176
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/197156
DOI
10.1164/rccm.202303-0499OC
ISSN
1073-449X
1535-4970
Abstract
Rationale: Although inflammation and infection are key disease drivers in bronchiectasis, few studies have integrated host inflammatory and microbiome data to guide precision medicine. Objectives: To identify clusters among patients with bronchiectasis on the basis of inflammatory markers and to assess the association between inflammatory endotypes, microbiome characteristics, and exacerbation risk. Methods: Patients with stable bronchiectasis were enrolled at three European centers, and cluster analysis was used to stratify the patients according to the levels of 33 sputum and serum inflammatory markers. Clusters were compared in terms of microbiome composition (16S ribosomal RNA sequencing) and exacerbation risk over a 12-month follow-up. Measurements and Main Results: A total of 199 patients were enrolled (109 [54.8%] female; median age, 69 yr). Four clusters of patients were defined according to their inflammatory profiles: cluster 1, milder neutrophilic inflammation; cluster 2, mixed-neutrophilic and type 2; cluster 3, most severe neutrophilic; and cluster 4, mixed-epithelial and type 2. Lower microbiome diversity was associated with more severe inflammatory clusters (P < 0.001), and β-diversity analysis demonstrated distinct microbiome profiles associated with each inflammatory cluster (P = 0.001). Proteobacteria and Pseudomonas at phylum and genus levels, respectively, were more enriched in clusters 2 and 3 than in clusters 1 and 4. Furthermore, patients in cluster 2 (rate ratio [RR], 1.49; 95% confidence interval [CI], 1.16-1.92) and cluster 3 (RR, 1.61; 95% CI, 1.12-2.32) were at higher risk of exacerbation over a 12-month follow-up compared with cluster 1, even after adjustment for prior exacerbation history. Conclusions: Bronchiectasis inflammatory endotypes are associated with distinct microbiome profiles and future exacerbation risk.
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