Lung Mycobiota α-Diversity Is Linked to Severity in Critically Ill Patients with Acute Exacerbation of Chronic Obstructive Pulmonary Disease

Raphaël Enaud; Pierre Sioniac; Sebastien Imbert; Pierre-Laurent Janvier; Adrian Camino; Hoang-Nam Bui; Odile Pillet; Arthur Orieux; Alexandre Boyer; Patrick Berger; Didier Gruson; Laurence Delhaes; Renaud Prevel

doi:10.1128/spectrum.05062-22

Lung Mycobiota α-Diversity Is Linked to Severity in Critically Ill Patients with Acute Exacerbation of Chronic Obstructive Pulmonary Disease

Microbiol Spectr. 2023 Mar 28;11(2):e0506222. doi: 10.1128/spectrum.05062-22. Online ahead of print.

Authors

Raphaël Enaud^{1

2}, Pierre Sioniac³, Sebastien Imbert^{1

4}, Pierre-Laurent Janvier³, Adrian Camino¹, Hoang-Nam Bui³, Odile Pillet³, Arthur Orieux³, Alexandre Boyer^{1

3}, Patrick Berger¹, Didier Gruson^{1

3}, Laurence Delhaes^{1

4}, Renaud Prevel^{1

3}

Affiliations

¹ Université Bordeaux, Center de Recherche Cardio-Thoracique de Bordeaux, INSERM UMR 1045, Bordeaux, France.
² Centre Hospitalier Universitaire Bordeaux, Le Centre de Ressources et de Compétences de la Mucoviscidose Pédiatrique, CIC 1401, Bordeaux, France.
³ Centre Hospitalier Universitaire Bordeaux, Medical Intensive Care Unit, Bordeaux, France.
⁴ Centre Hospitalier Universitaire Bordeaux, Mycology-Parasitology Department, CIC 1401, Bordeaux, France.

Abstract

Chronic obstructive pulmonary disease (COPD) affects more than 200 million people worldwide. The chronic course of COPD is frequently worsened by acute exacerbations (AECOPD). Mortality in patients hospitalized for severe AECOPD remains dramatically high, and the underlying mechanisms are poorly understood. Lung microbiota is associated with COPD outcomes in nonsevere AECOPD, but no study specifically investigated severe AECOPD patients. The aim of this study is thus to compare lung microbiota composition between severe AECOPD survivors and nonsurvivors. Induced sputum or endotracheal aspirate was collected at admission from every consecutive severe AECOPD patient. After DNA extraction, the V3-V4 and ITS2 regions were amplified by PCR. Deep-sequencing was performed on a MiSeq sequencer (Illumina); the data were analyzed using DADA2 pipeline. Among 47 patients admitted for severe AECOPD, 25 (53%) with samples of sufficient quality were included: 21 of 25 (84%) survivors and 4 of 25 (16%) nonsurvivors. AECOPD nonsurvivors had lower α-diversities indices than survivors for lung mycobiota but not for lung bacteriobiota. Similar results were demonstrated comparing patients receiving invasive mechanical ventilation (n = 13 [52%]) with those receiving only noninvasive ventilation (n = 12 [48%]). Previous systemic antimicrobial therapy and long-term inhaled corticosteroid therapy could alter the lung microbiota composition in severe AECOPD patients. In acidemic AECOPD, lower lung mycobiota α-diversity is linked to the severity of the exacerbation, assessed by mortality and the requirement for invasive mechanical ventilation, whereas lung bacteriobiota α-diversity is not. This study encourages a multicenter cohort study investigating the role of lung microbiota, especially fungal kingdom, in severe AECOPD. IMPORTANCE In AECOPD with acidemia, more severe patients-i.e., nonsurvivors and patients requiring invasive mechanical ventilation-have lower lung mycobiota α-diversity than survivors and patients receiving only noninvasive ventilation, respectively. This study encourages a large multicenter cohort study investigating the role of lung microbiota in severe AECOPD and urges investigation of the role of the fungal kingdom in severe AECOPD.

Keywords: chronic obstructive pulmonary disease; human microbiota; intensive care unit; microbiota; mycobiota; severe exacerbation.