4.6 Article

Bile Acid Signal Molecules Associate Temporally with Respiratory Inflammation and Microbiome Signatures in Clinically Stable Cystic Fibrosis Patients

Journal

MICROORGANISMS
Volume 8, Issue 11, Pages -

Publisher

MDPI
DOI: 10.3390/microorganisms8111741

Keywords

cystic fibrosis; bile acids; lung microbiota; inflammation; gut– lung axis

Categories

Funding

  1. European Commission [EU-634486-INMARE]
  2. Irish Research Council for Science, Engineering and Technology [GOIPG/2014/647 IRCSET]
  3. Science Foundation Ireland [SSPC3-Pharm5, 15/TIDA/2977]
  4. Health Research Board/Irish Thoracic Society [MRCG-2014-6, MRCG-2018-16, HRB-ILP-POR-2019-004]
  5. Glenn Brown Memorial Grant 2017 (Institute for Respiratory Health, Perth, Australia)
  6. U.S. CF Foundation [CFF 1710]
  7. Australian NHMRC [Synergy APP1183640]
  8. Marine Institute [C2CRA 2007/082]
  9. Science Foundation Ireland (SFI) [15/TIDA/2977] Funding Source: Science Foundation Ireland (SFI)

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Cystic fibrosis (CF) is a congenital disorder resulting in a multisystemic impairment in ion homeostasis. The subsequent alteration of electrochemical gradients severely compromises the function of the airway epithelia. These functional changes are accompanied by recurrent cycles of inflammation-infection that progressively lead to pulmonary insufficiency. Recent developments have pointed to the existence of a gut-lung axis connection, which may modulate the progression of lung disease. Molecular signals governing the interplay between these two organs are therefore candidate molecules requiring further clinical evaluation as potential biomarkers. We demonstrate a temporal association between bile acid (BA) metabolites and inflammatory markers in bronchoalveolar lavage fluid (BALF) from clinically stable children with CF. By modelling the BALF-associated microbial communities, we demonstrate that profiles enriched in operational taxonomic units assigned to supraglottic taxa and opportunistic pathogens are closely associated with inflammatory biomarkers. Applying regression analyses, we also confirmed a linear link between BA concentration and pathogen abundance in BALF. Analysis of the time series data suggests that the continuous detection of BAs in BALF is linked to differential ecological succession trajectories of the lung microbiota. Our data provide further evidence supporting a role for BAs in the early pathogenesis and progression of CF lung disease.

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