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TMAO: how gut microbiota contributes to heart failure

机译:tmao:肠道微生物群如何导致心力衰竭

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An increasing amount of evidence reveals that the gut microbiota is involved in the pathogenesis and progression of various cardiovascular diseases. In patients with heart failure (HF), splanchnic hypoperfusion causes ischemia and intestinal edema, allowing bacterial translocation and bacterial metabolites to enter the blood circulation via an impaired intestinal barrier. This results in local and systemic inflammatory responses. Gut microbe-derived metabolites are implicated in the pathology of multiple diseases, including HF. These landmark findings suggest that gut microbiota influences the host's metabolic health, either directly or indirectly by producing several metabolites. In this review, we mainly discuss a newly identified gut microbiota-dependent metabolite, trimethylamine N-oxide (TMAO), which appears to participate in the pathologic processes of HF and can serve as an early warning marker to identify individuals who are at the risk of disease progression. We also discuss the potential of the gut-TMAO-HF axis as a new target for HF treatment and highlight the current controversies and potentially new and exciting directions for future research.
机译:越来越多的证据表明,肠道微生物群参与各种心血管疾病的发病机制和进展。在心力衰竭(HF)患者中,内脏灌注不足会导致缺血和肠水肿,使细菌移位和细菌代谢产物通过受损的肠屏障进入血液循环。这会导致局部和全身炎症反应。肠道微生物衍生的代谢物与多种疾病的病理学有关,包括心衰。这些里程碑式的发现表明,肠道微生物群通过产生几种代谢物直接或间接地影响宿主的代谢健康。在这篇综述中,我们主要讨论一种新发现的肠道微生物群依赖性代谢物三甲胺N-氧化物(TMAO),它似乎参与HF的病理过程,可以作为早期预警标志物来识别有疾病进展风险的个体。我们还讨论了肠道TMAO-HF轴作为HF治疗新靶点的潜力,并强调了当前的争议以及未来研究的潜在新的和令人兴奋的方向。

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