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Association Between Frailty and Gut Microbiota Metabolite TMAO in Older People With Cardiovascular Disease

机译:在患有心血管疾病的老年人的脆弱和肠道微生物地区代谢物TMAO之间的关联

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摘要

The potential for the gut microbiota to affect health has particular relevance for older adults. Recent evidence suggests that microbiota-derived metabolites may modulate aging-related changes in immunity, sarcopenia, and cognitive function, all of which are elements of frailty. Trimethylamine N-oxide (TMAO) produced by the metaorganismal metabolism of choline, has been implicated in disease pathogenesis. However, relatively little geroscience research has been carried out on TMAO,and even less on other gut microbiota metabolites. The purpose of this study was to explore the relationship between frailty and circulating TMAO concentration. Data and fasting blood samples came from a prospective comprehensive geriatric assessment cohort of older adults (age≥65, n=451) with cardiovascular diseases. The frailty index based on the accumulated deficits model (48 variables) was used for evaluating the status of frailty. TMAO levels differed between groups with a significant increase for people with frailty (p<0.001). Compared with the lowest quartile of TMAO levels, patients in the highest quartile had increased 3.07-fold risk of frailty (OR=3.07, 95%CI, 1.69-2.97). After adjusting for age, gender, BMI, history of diseases, hsCRP, LDLc, TMAO levels remained associated with frailty (OR=2.11, 95%CI, 1.01-4.38). Similarly, a cubic spline curve showed a dose-dependent relationship between the odds ratio for the risk of frailty and circulating TMAO in a linear trend (p = 0.006). This study suggests that circulating TMAO are independently associated with frailty in older adult with cardiovascular diseases. Efforts to further characterize the relationship between gut microbiota metabolite and frailty should be further pursued.
机译:肠道微生物会影响健康的可能性对老年人特别相关。最近的证据表明,微生物群衍生的代谢物可以调节免疫,肌肉衰老和认知功能的衰老变化,所有这些都是脆弱的元素。通过胆碱的核肉代谢产生的三甲胺N-氧化物(TMAO)涉及疾病发病机制。然而,在TMAO上进行了相对较少的Geroscience研究,甚至更少对其他肠道微生物群代谢物。本研究的目的是探讨脆弱和循环TMAO浓度之间的关系。数据和禁食血液样本来自一名前瞻性综合性老年人评估队列(年龄≥65,n = 451),患有心血管疾病。基于累积赤字模型(48个变量)的体外索引用于评估脆弱状态。 TMAO水平在群体之间不同的群体对含有脆弱的人显着增加(P <0.001)。与TMAO水平最低的四分位数相比,最高四分位数的患者增加了3.07倍的风险(或= 3.07,95%CI,1.69-2.97)。调整年龄,性别,BMI,疾病史,HSCRP,LDLC,TMAO水平仍然与Freaty(或= 2.11,95%CI,1.01-4.38)相关。类似地,立方样条曲线显示在线性趋势中脆弱和循环TMAO风险的差距比之间的剂量依赖关系(P = 0.006)。本研究表明,循环TMAO与患有心血管疾病的老年人的脆弱性独立相关。进一步表征肠道微生物群代谢物和脆弱之间关系的努力应得到进一步追求。

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