Population-level Metagenomics Uncovers Distinct Effects of Multiple Medications on the Human Gut Microbiome

Naoyoshi Nagata; Suguru Nishijima; Tohru Miyoshi‐Akiyama; Yasushi Kojima; Moto Kimura; Ryo Aoki; Mitsuru Ohsugi; Kohjiro Ueki; Kuniko Miki; Eri Iwata; Kayoko Hayakawa; Norio Ohmagari; Shinichi Oka; Masashi Mizokami; Takao Itoi; Takashi Kawai; Naomi Uemura; Masahira Hattori

doi:10.1053/j.gastro.2022.06.070

Population-level Metagenomics Uncovers Distinct Effects of Multiple Medications on the Human Gut Microbiome

Naoyoshi Nagata(Tokyo Medical University), Suguru Nishijima(Waseda University), Tohru Miyoshi‐Akiyama(National Center for Global Health and Medicine), Yasushi Kojima(National Center for Global Health and Medicine), Moto Kimura(National Center for Global Health and Medicine), Ryo Aoki(Ezaki Glico (Japan)), Mitsuru Ohsugi(National Center for Global Health and Medicine), Kohjiro Ueki(National Center for Global Health and Medicine), Kuniko Miki(Tokyo Medical University), Eri Iwata(Tokyo Medical University), Kayoko Hayakawa(National Center for Global Health and Medicine), Norio Ohmagari(National Center for Global Health and Medicine), Shinichi Oka(National Center for Global Health and Medicine), Masashi Mizokami(National Center for Global Health and Medicine), Takao Itoi(Tokyo Medical University), Takashi Kawai(Tokyo Medical University), Naomi Uemura(National Center for Global Health and Medicine), Masahira Hattori(Waseda University)

Gastroenterology

July 2, 2022

10.1053/j.gastro.2022.06.070

Cited by 170Open Access

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Abstract

BACKGROUND & AIMS: Medication is a major determinant of human gut microbiome structure, and its overuse increases the risks of morbidity and mortality. However, effects of certain commonly prescribed drugs and multiple medications on the gut microbiome are still underinvestigated. METHODS: We performed shotgun metagenomic analysis of fecal samples from 4198 individuals in the Japanese 4D (Disease, Drug, Diet, Daily life) microbiome project. A total of 759 drugs were profiled, and other metadata, such as anthropometrics, lifestyles, diets, physical activities, and diseases, were prospectively collected. Second fecal samples were collected from 243 individuals to assess the effects of drug initiation and discontinuation on the microbiome. RESULTS: We found that numerous drugs across different treatment categories influence the microbiome; more than 70% of the drugs we profiled had not been examined before. Individuals exposed to multiple drugs, polypharmacy, showed distinct gut microbiome structures harboring significantly more abundant upper gastrointestinal species and several nosocomial pathobionts due to additive drug effects. Polypharmacy was also associated with microbial functions, including the reduction of short-chain fatty acid metabolism and increased bacterial stress responses. Even nonantibiotic drugs were significantly correlated with an increased antimicrobial resistance potential through polypharmacy. Notably, a 2-time points dataset revealed the alteration and recovery of the microbiome in response to drug initiation and cessation, corroborating the observed drug-microbe associations in the cross-sectional cohort. CONCLUSION: Our large-scale metagenomics unravels extensive and disruptive impacts of individual and multiple drug exposures on the human gut microbiome, providing a drug-microbe catalog as a basis for a deeper understanding of the role of the microbiome in drug efficacy and toxicity.

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