氧化三甲胺
代谢物
丁酸盐
心肌梗塞
医学
内科学
丙酸盐
前瞻性队列研究
心脏病学
胃肠病学
内分泌学
生物化学
三甲胺
化学
发酵
作者
José Avendaño‐Ortiz,Álvaro Lorente-Ros,Andrea Briones-Figueroa,Patricia Morán‐Álvarez,Antía García Fernández,Sandra Garrote-Corral,I. Amil-Casas,Ángela Carrasco-Sayalero,Amalia Tejeda Velarde,A. Camino-López,Manuel Jiménez-Mena,Rosa del Campo,Lourdes Villalobos-Sánchez,María Jesús García-Villanueva
出处
期刊:Heliyon
[Elsevier]
日期:2023-10-01
卷期号:9 (10): e20854-e20854
被引量:5
标识
DOI:10.1016/j.heliyon.2023.e20854
摘要
Acute myocardial infarction (AMI) is associated with systemic inflammatory processes and metabolic alterations. Microbial-derived metabolites, such as short-chain fatty acids and trimethylamine N-oxide (TMAO), have emerged in recent years as key players in the modulation of inflammation, with potential implications for cardiovascular diseases. We performed a prospective observational study that monitored the serological concentration of bacterial metabolites in 45 young patients (<55 years) without cardiovascular risk factors but with AMI, at hospital admission and at 3 months of follow-up, and compared them with a control group. TMAO and acetate levels were significantly higher in AMI, whereas butyrate and propionate were significantly lower. The acetate/propionate ratio showed the most discrimination between AMI and controls by receiver operating characteristic analysis (area under the curve 0.769, P < 0.0001). A multivariate logistic regression model revealed that this ratio was independently associated with AMI. Short-chain fatty acid concentrations, but not TMAO, exhibited significant correlations with inflammatory and coagulation parameters. Three months after the acute AMI event, all metabolite levels returned to those observed in healthy controls except butyrate. In conclusion, our study reveals disturbances of the serological concentration of microbiota-derived metabolites in AMI that are also related to inflammatory and coagulation parameters. These findings highlight an interesting field of study in the potential role of microbial metabolites from gut in cardiovascular disease.
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