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  4. Gut microbes with the genes determine TMAO production from L-carnitine intake and serve as a biomarker for precision nutrition.
 
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Gut microbes with the genes determine TMAO production from L-carnitine intake and serve as a biomarker for precision nutrition.

Journal
Gut microbes
Journal Volume
17
Journal Issue
1
Pages
2446374
ISSN
1949-0984
Date Issued
2025-12
Author(s)
WEI-KAI WU  
Lo, Yi-Ling
Chiu, Jian-Ying
Hsu, Chia-Lang
Lo, I-Hsuan
Panyod, Suraphan
Liao, Yu-Chieh
Chiu, Tina H T
Yang, Yu-Tang
Kuo, Han-Chun
Zou, Hsin-Bai
Chen, Yi-Hsun
Chuang, Hsiao-Li
Yen, Jeffrey J Y
JIN-TOWN WANG  
HAN-MO CHIU  
Hsu, Cheng-Chih
Kuo, Ching-Hua
LEE-YAN SHEEN  
HSIEN-LI KAO  
MING-SHIANG WU  
DOI
10.1080/19490976.2024.2446374
URI
https://pubmed.ncbi.nlm.nih.gov/39722590/
https://scholars.lib.ntu.edu.tw/handle/123456789/724655
Abstract
Gut microbial metabolism of L-carnitine, which leads to the production of detrimental trimethylamine N-oxide (TMAO), offers a plausible link between red meat consumption and cardiovascular risks. Several microbial genes, including , the operon, and the recently identified gene cluster, have been implicated in the conversion of dietary L-carnitine into TMA(O). However, the key microbial genes and associated gut microbes involved in this pathway have not been fully explored. Utilizing the oral carnitine challenge test (OCCT), which specifically measures TMAO production from L-carnitine intake and identifies TMAO producer phenotypes, we compared the abundance of microbial genes between low- and high-TMAO producers across three independent cohorts. Our findings consistently revealed that the gene cluster, rather than or the operon, was significantly enriched in high-TMAO producers. We further analyzed 292 paired multi-omic datasets from OCCT and shotgun metagenomic sequencing, which demonstrated a significant positive correlation between the abundance of fecal genes and L-carnitine-induced TMAO production, with showing the strongest correlation. Interestingly, these fecal genes were found to increase with L-carnitine supplementation and decrease with a plant-based diet. Notably, we verified a previously uncultured -containing bacterium, JAGTTR01 sp018223385, as the major contributor to TMA formation in the human gut. We isolated these -containing gut microbes and confirmed their role in TMA/TMAO production using anaerobic incubation and a gnotobiotic mouse model. Using an in-house collection of -containing isolates, we developed a qPCR-based method to quantify fecal and validated its correlation with L-carnitine-mediated TMAO production as measured by OCCT. Overall, these findings suggest that -containing gut microbes are crucial for TMAO increases following L-carnitine intake and may serve as biomarkers or targets for personalized nutrition.
Subjects
Gut microbiome
L-carnitine
Personalized nutrition
Red meat
Trimethylamine N-oxide
gbu gene cluster
SDGs

[SDGs]SDG2

[SDGs]SDG3

Publisher
Informa UK Limited
Type
journal article

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