Respiratory Fungal Communities are Associated with Systemic Inflammation and Predict Survival in Patients with Acute Respiratory Failure

Author:

Britton Noel,Yang Haopu,Fitch Adam,Li Kelvin,Seyed Khaled,Guo Rui,Qin Shulin,Zhang Yingze,Bain WilliamORCID,Shah Faraaz,Biswas Partha,Choi Wonseok,Finkelman Malcolm,Zhang Yonglong,Haggerty Catherine L.,Benos Panayiotis V.,Brooks Maria M.,McVerry Bryan J.,Methe Barbara,Kitsios Georgios D.ORCID,Morris Alison

Abstract

ABSTRACTRationaleDisruption of respiratory bacterial communities predicts poor clinical outcomes in critical illness; however, the role of respiratory fungal communities (mycobiome) is poorly understood.ObjectivesWe investigated whether mycobiota variation in the respiratory tract is associated with host-response and clinical outcomes in critically ill patients.MethodsTo characterize the upper and lower respiratory tract mycobiota, we performed rRNA gene sequencing (internal transcribed spacer) of oral swabs and endotracheal aspirates (ETA) from 316 mechanically-ventilated patients. We examined associations of mycobiome profiles (diversity and composition) with clinical variables, host-response biomarkers, and outcomes.Measurements and Main ResultsETA samples with >50% relative abundance forC. albicans(51%) were associated with elevated plasma IL-8 and pentraxin-3 (p=0.05), longer time-to-liberation from mechanical ventilation (p=0.04) and worse 30-day survival (adjusted hazards ratio (adjHR): 1.96 [1.04-3.81], p=0.05). Using unsupervised clustering, we derived two clusters in ETA samples, with Cluster 2 (39%) showing lower alpha diversity (p<0.001) and higher abundance ofC. albicans(p<0.001). Cluster 2 was significantly associated with the prognostically adverse hyperinflammatory subphenotype (odds ratio 2.07 [1.03-4.18], p=0.04) and predicted worse survival (adjHR: 1.81 [1.03-3.19], p=0.03).C. albicansabundance in oral swabs was also associated with the hyper-inflammatory subphenotype and mortality.ConclusionsVariation in respiratory mycobiota was significantly associated with systemic inflammation and clinical outcomes.C. albicansabundance emerged as a negative predictor in both the upper and lower respiratory tract. The lung mycobiome may play an important role in the biological and clinical heterogeneity among critically ill patients and represent a potential therapeutic target for lung injury in critical illness.

Publisher

Cold Spring Harbor Laboratory

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