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首页> 外文期刊>Journal of neurosurgical sciences >Body Mass Index as a Determinant of Systemic Exposure to Gallotannin Metabolites during 6-Week Consumption of Mango (Mangifera indica L.) and Modulation of Intestinal Microbiota in Lean and Obese Individuals
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Body Mass Index as a Determinant of Systemic Exposure to Gallotannin Metabolites during 6-Week Consumption of Mango (Mangifera indica L.) and Modulation of Intestinal Microbiota in Lean and Obese Individuals

机译:体重指数作为芒果(Mangifera Indema L.)6周消费期间全身暴露于Gallotannin代谢物的决定因素,并在瘦弱和肥胖个体中调节肠道微生物群

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摘要

Scope This human clinical pilot trial investigated pharmacokinetics of gallotannin-metabolites and modulation of intestinal microbiota in healthy lean and obese individuals after 6 weeks of daily mango consumption. Methods and results Participants are divided into three groups: Lean Mango (LM: n = 12; BMI = 22.9 kg m(-2)), Obese Mango (OM: n = 9; BMI = 34.6 kg m(-2)), and Lean Control (LC: n = 11; BMI = 22.1 kg m(-2)). LM and OM consumed 400 g of mango per day for 6 weeks. LC consumed mango only on Days 0 and 42. After 6 weeks, LM experienced increased systemic exposure (AUC(0-8h)) to gallotannin-metabolites, 1.4-fold (p = 0.043). The greatest increase is 4-O-methyl-gallic acid, 3.3-fold (p = 0.0026). Cumulative urinary excretion of gallotannin-metabolites significantly increased in LM and OM, but not LC. For OM, qPCR data show increased levels of tannase-producing Lactococcus lactis and decreased levels of Clostridium leptum and Bacteroides thetaiotaomicron, bacteria associated with obesity. LM experienced an increased trend of fecal levels of butyric (1.3-fold; p = 0.09) and valeric acids (1.5-fold; p = 0.056). Plasma endotoxins showed a decreased trend in LM and OM. Conclusion Continuous mango intake significantly increased systemic exposure to gallotannin- metabolites and induced an increased trend for fecal short-chain fatty acids in lean but not obese individuals. This pharmacokinetic discrepancy may result in BMI-associated reduced gallotannin-derived health benefits.
机译:该人类临床试验试验研究了每次芒果消费6周后健康瘦肉和肥胖个体肠道微生物的药代动力学和肠道微生物的调节。方法和结果参与者分为三组:瘦芒果(LM:N = 12; BMI = 22.9kg M(-2)),肥胖芒果(OM:n = 9; BMI = 34.6 kg m(-2)),和瘦控制(LC:n = 11; BMI = 22.1 kg m(-2))。 LM和OM每天消耗400克芒果6周。 LC仅在第0天和42天消耗芒果。6周后,LM经历了增加的全身暴露(AUC(0-8H))到Gallot annin-代谢物,1.4倍(P = 0.043)。最大的增加是4-O-甲基小酸,3.3倍(p = 0.0026)。 LM和OM的Gallot annin-代谢物的累积尿释放显着增加,但不是LC。对于OM,QPCR数据显示出增加的鞣酸乳乳球菌水平和患有腹腔炎和菌株的蛋白酶和肥胖的细菌水平降低。 LM经历了粪便水平的趋势增加(1.3倍; P = 0.09)和valeric酸(1.5倍; P = 0.056)。血浆内毒素在LM和OM中显示出降低的趋势。结论连续芒果摄入量显着提高全身暴露于Gallot anninin-代谢物,诱导瘦症患者粪便短链脂肪酸增加趋势。这种药代动力学差异可能导致BMI相关的Gallotannin-ressived健康益处。

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