Identification of TMAO-producer phenotype and host–diet–gut dysbiosis by carnitine challenge test in human and germ-free mice

Author:

Wu Wei-Kai,Chen Chieh-Chang,Liu Po-Yu,Panyod Suraphan,Liao Ben-Yang,Chen Pei-Chen,Kao Hsien-Li,Kuo Han-Chun,Kuo Ching-Hua,Chiu Tina H T,Chen Rou-An,Chuang Hsiao-Li,Huang Yen-Te,Zou Hsin-Bai,Hsu Cheng-Chih,Chang Ting-Yan,Lin Chin-Lon,Ho Chi-Tang,Yu Hon-Tsen,Sheen Lee-Yan,Wu Ming-Shiang

Abstract

ObjectiveThe gut microbiota-derived metabolite, trimethylamine N-oxide (TMAO) plays an important role in cardiovascular disease (CVD). The fasting plasma TMAO was shown as a prognostic indicator of CVD incident in patients and raised the interest of intervention targeting gut microbiota. Here we develop a clinically applicable method called oral carnitine challenge test (OCCT) for TMAO-related therapeutic drug efforts assessment and personalising dietary guidance.DesignA pharmacokinetic study was performed to verify the design of OCCT protocol. The OCCT was conducted in 23 vegetarians and 34 omnivores to validate gut microbiota TMAO production capacity. The OCCT survey was integrated with gut microbiome, host genotypes, dietary records and serum biochemistry. A humanised gnotobiotic mice study was performed for translational validation.ResultsThe OCCT showed better efficacy than fasting plasma TMAO to identify TMAO producer phenotype. The omnivores exhibited a 10-fold higher OR to be high TMAO producer than vegetarians. The TMAO-associated taxa found by OCCT in this study were consistent with previous animal studies. The TMAO producer phenotypes were also reproduced in humanised gnotobiotic mice model. Besides, we found the faecal CntA gene was not associated with TMAO production; therefore, other key relevant microbial genes might be involved. Finally, we demonstrated the urine TMAO exhibited a strong positive correlation with plasma TMAO (r=0.92, p<0.0001) and improved the feasibility of OCCT.ConclusionThe OCCT can be used to identify TMAO-producer phenotype of gut microbiota and may serve as a personal guidance in CVD prevention and treatment.Trial registration numberNCT02838732; Results.

Funder

Ministry of Science and Technology, Taiwan

Academia Sinica

Ministry of Education in Taiwan

Publisher

BMJ

Subject

Gastroenterology

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