Integrated 16S rDNA sequencing and metabolomics to explore the intestinal changes in children and rats with dental fluorosis.

Ecotoxicol Environ Saf

Department of Environment Health, School of Public Health of Zhengzhou University, Zhengzhou, Henan, PR China; Yellow River Institute for Ecological Protection & Regional Coordinated Development, Zhengzhou University, Zhengzhou, Henan, PR China. Electronic address:

Published: February 2023

AI Article Synopsis

  • This study investigates dental fluorosis (DF) caused by excess fluoride and its link to changes in the intestinal microbiome.
  • A pilot study with 23 children in China found significant differences in gut microbiome composition between those with DF and a control group, particularly notable in specific bacterial groups.
  • Experiments in rats confirmed that fluoride affects gut microbiota and associated metabolites, suggesting that DF's pathogenesis is related to shifts in intestinal microorganisms involved in metabolic pathways.

Article Abstract

Dental fluorosis (DF) is a widely prevalent disease caused by excessive fluoride with limited awareness of its underlying pathogenesis. Here, a pilot population study was conducted to explore the pathogenesis of DF from the perspective of intestinal microbiome changes, and verified it in animal experiments combining intestinal microbiome and metabolomics. A total of 23 children were recruited in 2017 in China and divided into DF (n = 9) and control (n = 14) groups (DFG and CG, respectively). The SD rat model was established by drinking water containing sodium fluoride (NaF). Gut microbiome profiles of children and rats were analyzed by16S rDNA V3-V4 sequencing, and the intestinal metabolomics analysis of rats was performed by LC-MS methods. The 16 S rDNA sequencing revealed that the gut microbiome composition was significantly perturbed in children in DFG compared to that in CG. Acidobacteria and Thermi were specifically observed in DFG and CG, respectively. Besides, 15 fecal microbiotas were significantly altered at the genus level in DFG. Furthermore, only the expression of annotated genes for pentose and glucuronate interconversion pathway was significant lower in DFG than that in CG (P = 0.04). Notably, in NaF-treated rats, we also observed the changes of some key components of pentose and glucuronate interconversion pathway at the level of microorganisms and metabolites. Our findings suggested that the occurrence of DF is closely related to the alteration of intestinal microorganisms and metabolites annotated in the pentose and glucuronate interconversion pathway.

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http://dx.doi.org/10.1016/j.ecoenv.2023.114518DOI Listing

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