“…Relevant bacterial species in CF, such as P. aeruginosa [69] and Staphylococcus aureus [70,71], possess large, flexible gene pools, including genes encoding antibiotic resistance, pathogenicity, environmental response, and metabolic flexibility, which may explain the adaptive nature of chronic infections [72]. Although the metagenome contributes greatly to interactions with the host [25,73], very few studies on CF metagenomes have been performed, involving a limited number of both patients [29,63,74,75] and specific metabolic functions [76]. By analyzing the abundance of specific genes, such studies found a homogeneous distribution of predicted bacterial community activities (e.g., specific metabolic pathways) across patients with similar pulmonary function, as indicated by forced expiratory volume in 1 second (FEV 1 ) [73], suggesting a relationship between microbiome function and clinical status.…”