Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults

OBJECTIVES: Imidazole propionate (ImP), a microbiota metabolite from histidine, has been linked to cardiometabolic conditions in humans. The current study aimed to elucidate inter-relationships between histidine intake, gut microbial composition and functional potentials, circulating ImP levels, and...

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Autores principales: Zhu, Lu, Li, Jun, Li, Yanping, Ivey, Kerry, Lee, Kyu Ha, Eliassen, Heather, Qi, Qibin, Chan, Andrew, Huttenhower, Curtis, Rimm, Eric, Hu, Frank, Sun, Qi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Nutritional Microbiology/Microbiome
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9194292/
http://dx.doi.org/10.1093/cdn/nzac069.046
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author Zhu, Lu
Li, Jun
Li, Yanping
Ivey, Kerry
Lee, Kyu Ha
Eliassen, Heather
Qi, Qibin
Chan, Andrew
Huttenhower, Curtis
Rimm, Eric
Hu, Frank
Sun, Qi
author_facet Zhu, Lu
Li, Jun
Li, Yanping
Ivey, Kerry
Lee, Kyu Ha
Eliassen, Heather
Qi, Qibin
Chan, Andrew
Huttenhower, Curtis
Rimm, Eric
Hu, Frank
Sun, Qi
author_sort Zhu, Lu
collection PubMed
description OBJECTIVES: Imidazole propionate (ImP), a microbiota metabolite from histidine, has been linked to cardiometabolic conditions in humans. The current study aimed to elucidate inter-relationships between histidine intake, gut microbial composition and functional potentials, circulating ImP levels, and the risk of coronary heart disease (CHD) in U.S. adults. METHODS: A total of 896 fecal samples and 462 blood samples were collected from 298 healthy men in the Men's Lifestyle Validation Study. Multivariate Association with Linear Models 2 was used to analyze the associations between microbial features and plasma ImP levels. Associations between plasma ImP and CHD risk was examined using Cox proportional hazards regression models among 7,793 participants pooled from the Health Professionals Follow-up Study, Nurses’ Health Study (NHS), and NHSII with existing ImP measurements. RESULTS: The overall microbial composition was associated with plasma ImP levels (PERMANOVA p = 0.001). Multivariable taxa-wide association analysis identified 14 bacterial species, such as Ruminococcus Obeum, Clostridium clostridioforme, C. nexile, C. symbiosum and Gordonibacter pamelaeae, that were significantly (FDR P < 0.05) associated with plasma ImP levels. A non-parametric score was derived to summarize the abundance of the 14 species. Higher intake of red meat and histidine was significantly associated with higher ImP levels among participants with a higher ImP-Species Score (for red meat, P-inter = 0.04; for histidine, P-inter = 0.01), but not among others (P > 0.05). In the pooled cohort, compared with participants in the lowest ImP tertile, the relative risk (95% CI) of CHD was 2.06 (1.96, 2.43) among those in the highest ImP tertile (P- trend = 0.0001). Histidine consumption was not associated with CHD risk in the same study population. CONCLUSIONS: We identified multiple microbiota species that were associated with plasma ImP concentrations and collectively predicted stronger associations of histidine or red meat intake with ImP concentrations. Plasma ImP concentrations were significantly associated with an increased risk of developing CHD. These data emphasize the role of human gut microbiota in modulating the production of ImP through histidine intake. FUNDING SOURCES: The National Institutes of Health Boston Nutrition Obesity Research Centre.
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spelling pubmed-91942922022-06-14 Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults Zhu, Lu Li, Jun Li, Yanping Ivey, Kerry Lee, Kyu Ha Eliassen, Heather Qi, Qibin Chan, Andrew Huttenhower, Curtis Rimm, Eric Hu, Frank Sun, Qi Curr Dev Nutr Nutritional Microbiology/Microbiome OBJECTIVES: Imidazole propionate (ImP), a microbiota metabolite from histidine, has been linked to cardiometabolic conditions in humans. The current study aimed to elucidate inter-relationships between histidine intake, gut microbial composition and functional potentials, circulating ImP levels, and the risk of coronary heart disease (CHD) in U.S. adults. METHODS: A total of 896 fecal samples and 462 blood samples were collected from 298 healthy men in the Men's Lifestyle Validation Study. Multivariate Association with Linear Models 2 was used to analyze the associations between microbial features and plasma ImP levels. Associations between plasma ImP and CHD risk was examined using Cox proportional hazards regression models among 7,793 participants pooled from the Health Professionals Follow-up Study, Nurses’ Health Study (NHS), and NHSII with existing ImP measurements. RESULTS: The overall microbial composition was associated with plasma ImP levels (PERMANOVA p = 0.001). Multivariable taxa-wide association analysis identified 14 bacterial species, such as Ruminococcus Obeum, Clostridium clostridioforme, C. nexile, C. symbiosum and Gordonibacter pamelaeae, that were significantly (FDR P < 0.05) associated with plasma ImP levels. A non-parametric score was derived to summarize the abundance of the 14 species. Higher intake of red meat and histidine was significantly associated with higher ImP levels among participants with a higher ImP-Species Score (for red meat, P-inter = 0.04; for histidine, P-inter = 0.01), but not among others (P > 0.05). In the pooled cohort, compared with participants in the lowest ImP tertile, the relative risk (95% CI) of CHD was 2.06 (1.96, 2.43) among those in the highest ImP tertile (P- trend = 0.0001). Histidine consumption was not associated with CHD risk in the same study population. CONCLUSIONS: We identified multiple microbiota species that were associated with plasma ImP concentrations and collectively predicted stronger associations of histidine or red meat intake with ImP concentrations. Plasma ImP concentrations were significantly associated with an increased risk of developing CHD. These data emphasize the role of human gut microbiota in modulating the production of ImP through histidine intake. FUNDING SOURCES: The National Institutes of Health Boston Nutrition Obesity Research Centre. Oxford University Press 2022-06-14 /pmc/articles/PMC9194292/ http://dx.doi.org/10.1093/cdn/nzac069.046 Text en © The Author 2022. Published by Oxford University Press on behalf of The International Society for Human and Animal Mycology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Nutritional Microbiology/Microbiome
Zhu, Lu
Li, Jun
Li, Yanping
Ivey, Kerry
Lee, Kyu Ha
Eliassen, Heather
Qi, Qibin
Chan, Andrew
Huttenhower, Curtis
Rimm, Eric
Hu, Frank
Sun, Qi
Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults
title Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults
title_full Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults
title_fullStr Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults
title_full_unstemmed Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults
title_short Histidine Intake, Human Gut Microbiome, Plasma Levels of Imidazole Propionate, and Coronary Heart Disease Risk in US Adults
title_sort histidine intake, human gut microbiome, plasma levels of imidazole propionate, and coronary heart disease risk in us adults
topic Nutritional Microbiology/Microbiome
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9194292/
http://dx.doi.org/10.1093/cdn/nzac069.046
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