4.6 Article

Changes in Microbiome Dominance Are Associated With Declining Lung Function and Fluctuating Inflammation in People With Cystic Fibrosis

Journal

FRONTIERS IN MICROBIOLOGY
Volume 13, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fmicb.2022.885822

Keywords

microbiome; cystic fibrosis; 16S rRNA gene; inflammation; longitudinal study

Categories

Funding

  1. German Ministry for Education and Research [82DZL00401, 82DZL004A1, 82DZL009B1, 82DZL004B1]
  2. European Commission (Seventh Framework Program) [603038]
  3. German Cystic Fibrosis Association Mukoviszidose e. V. [1605, 1805]
  4. Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) [SFB-TR84 B08]
  5. Einstein Foundation Berlin [EP-2017-393]
  6. Charite-Universitatsmedizin Berlin
  7. Berlin Institute of Health
  8. HRCMM (Heidelberg Research Center for Molecular Medicine) Career Development Fellowship

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This study investigated the relationship between microbiome fluctuation and inflammatory parameters in patients with cystic fibrosis. The results showed that the diversity of the microbiome varied greatly over a one-year period, while the inflammatory markers evolved slower, with significant changes observed only in patients followed for three or more years. The degree of microbiome fluctuation and the dominance of specific pathogens were associated with changes in inflammatory markers, especially IL-1 beta and IL-8.
Airway inflammation and microbiome dysbiosis are hallmarks of cystic fibrosis (CF) lung disease. However, longitudinal studies are needed to decipher which factors contribute to the long-term evolution of these key features of CF. We therefore evaluated the relationship between fluctuation in microbiome and inflammatory parameters in a longitudinal study including a short- (1-year) and a long-term (3+ years) period. We collected 118 sputum samples from 26 CF adult patients and analyzed them by 16S rRNA gene sequencing. We measured the levels of inflammatory cytokines, neutrophil elastase, and anti-proteinases; lung function (FEV1% predicted); and BMI. The longitudinal evolution was analyzed based on (i) the rates of changes; (ii) the intra-patient stability of the variables; and (iii) the dependency of the rates of changes on the baseline values. We observed that the diversity of the microbiome was highly variable over a 1-year period, while the inflammatory markers showed a slower evolution, with significant changes only observed in the 3+ year cohort. Further, the degree of fluctuation of the biomass and the dominance of the microbiome were associated with changes in inflammatory markers, especially IL-1 beta and IL-8. This longitudinal study demonstrates for the first time that the long-term establishment and periodical variation of the abundance of a dominant pathogen is associated with a more severe increase in inflammation. This result indicates that a single time point or 1-year study might fail to reveal the correlation between microbial evolution and clinical degradation in cystic fibrosis.

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