Pharmacometabonomic identification of a significant host-microbiome metabolic interaction affecting human drug metabolism

Clayton, T. Andrew; Baker, David; Lindon, John C.; Everett, Jeremy R.; Nicholson, Jeremy K.

doi:10.1073/pnas.0904489106

articleProceedings of the National Academy of SciencesAug 10, 2009BRONZE OA

Pharmacometabonomic identification of a significant host-microbiome metabolic interaction affecting human drug metabolism

TAT. Andrew Clayton DBDavid Baker JCJohn C. Lindon JRJeremy R. Everett JKJeremy K. Nicholson

Imperial College London · Pfizer (United States) · +1 more institution

PubMed

Indexed incrossrefpubmed

Abstract

We provide a demonstration in humans of the principle of pharmacometabonomics by showing a clear connection between an individual's metabolic phenotype, in the form of a predose urinary metabolite profile, and the metabolic fate of a standard dose of the widely used analgesic acetaminophen. Predose and postdose urinary metabolite profiles were determined by (1)H NMR spectroscopy. The predose spectra were statistically analyzed in relation to drug metabolite excretion to detect predose biomarkers of drug fate and a human-gut microbiome cometabolite predictor was identified. Thus, we found that individuals having high predose urinary levels of p-cresol sulfate had low postdose urinary ratios of acetaminophen…

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Topics & keywords

Topics

Keywords

Metabolite
Acetaminophen
Glucuronide
Drug
Pharmacology
Microbiome
Drug metabolism
Xenobiotic

UN Sustainable Development Goals

Good health and well-being

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