Commensal antimicrobial resistance mediates microbiome resilience to antibiotic disruption.
Shakti K BhattaraiMuxue DuAbigail L ZeamerBenedikt M MortzfeldTasia D KelloggFirat KayaAnna BenjaminJames M BeanMatthew D ZimmermanGertrude MardiStalz Charles VilbrunKathleen Frances WalshDaniel W FitzgeraldMichael S GlickmanVanni BucciPublished in: Science translational medicine (2024)
Despite their therapeutic benefits, antibiotics exert collateral damage on the microbiome and promote antimicrobial resistance. However, the mechanisms governing microbiome recovery from antibiotics are poorly understood. Treatment of Mycobacterium tuberculosis , the world's most common infection, represents the longest antimicrobial exposure in humans. Here, we investigate gut microbiome dynamics over 20 months of multidrug-resistant tuberculosis (TB) and 6 months of drug-sensitive TB treatment in humans. We find that gut microbiome dynamics and TB clearance are shared predictive cofactors of the resolution of TB-driven inflammation. The initial severe taxonomic and functional microbiome disruption, pathobiont domination, and enhancement of antibiotic resistance that initially accompanied long-term antibiotics were countered by later recovery of commensals. This resilience was driven by the competing evolution of antimicrobial resistance mutations in pathobionts and commensals, with commensal strains with resistance mutations reestablishing dominance. Fecal-microbiota transplantation of the antibiotic-resistant commensal microbiome in mice recapitulated resistance to further antibiotic disruption. These findings demonstrate that antimicrobial resistance mutations in commensals can have paradoxically beneficial effects by promoting microbiome resilience to antimicrobials and identify microbiome dynamics as a predictor of disease resolution in antibiotic therapy of a chronic infection.
Keyphrases
- antimicrobial resistance
- mycobacterium tuberculosis
- multidrug resistant
- climate change
- oxidative stress
- pulmonary tuberculosis
- social support
- stem cells
- type diabetes
- staphylococcus aureus
- drug induced
- metabolic syndrome
- emergency department
- mesenchymal stem cells
- depressive symptoms
- adipose tissue
- insulin resistance
- hiv aids
- hepatitis c virus
- cell therapy