Antimicrobial-induced oral dysbiosis exacerbates naturally occurring alveolar bone loss.
Brooks A SwansonMatthew D CarsonJessica D Hathaway-SchraderAmy J WarnerJoy E KirkpatrickAlexa CorkerAlexander V AlekseyenkoCaroline WestwaterJ Ignacio AguirreChad M NovincePublished in: FASEB journal : official publication of the Federation of American Societies for Experimental Biology (2021)
Periodontitis-mediated alveolar bone loss is caused by dysbiotic shifts in the commensal oral microbiota that upregulate proinflammatory osteoimmune responses. The study purpose was to determine whether antimicrobial-induced disruption of the commensal microbiota has deleterious effects on alveolar bone. We administered an antibiotic cocktail, minocycline, or vehicle-control to sex-matched C57BL/6T mice from age 6- to 12 weeks. Antibiotic cocktail and minocycline had catabolic effects on alveolar bone in specific-pathogen-free (SPF) mice. We then administered minocycline or vehicle-control to male mice reared under SPF and germ-free conditions, and we subjected minocycline-treated SPF mice to chlorhexidine oral antiseptic rinses. Alveolar bone loss was greater in vehicle-treated SPF versus germ-free mice, demonstrating that the commensal microbiota drives naturally occurring alveolar bone loss. Minocycline- versus vehicle-treated germ-free mice had similar alveolar bone loss outcomes, implying that antimicrobial-driven alveolar bone loss is microbiota dependent. Minocycline induced phylum-level shifts in the oral bacteriome and exacerbated naturally occurring alveolar bone loss in SPF mice. Chlorhexidine further disrupted the oral bacteriome and worsened alveolar bone loss in minocycline-treated SPF mice, validating that antimicrobial-induced oral dysbiosis has deleterious effects on alveolar bone. Minocycline enhanced osteoclast size and interface with alveolar bone in SPF mice. Neutrophils and plasmacytoid dendritic cells were upregulated in cervical lymph nodes of minocycline-treated SPF mice. Paralleling the upregulated proinflammatory innate immune cells, minocycline therapy increased TH 1 and TH 17 cells that have known pro-osteoclastic actions in the alveolar bone. This report reveals that antimicrobial perturbation of the commensal microbiota induces a proinflammatory oral dysbiotic state that exacerbates naturally occurring alveolar bone loss.
Keyphrases
- bone loss
- high fat diet induced
- dendritic cells
- immune response
- high glucose
- diabetic rats
- stem cells
- insulin resistance
- mesenchymal stem cells
- skeletal muscle
- type diabetes
- endothelial cells
- cell death
- drug induced
- metabolic syndrome
- candida albicans
- oxidative stress
- signaling pathway
- early stage
- locally advanced
- glycemic control