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Obesity-related dysregulation of the Tryptophan-Kynurenine metabolism: Role of age and parameters of the metabolic syndrome

机译:肥胖相关的色氨酸-Kynurenine代谢失调:年龄和代谢综合征参数的作用

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Objective Obesity-related immune mediated systemic inflammation was associated with the development of the metabolic syndrome by induction of the tryptophan (TRP)-kynurenine (KYN) pathway. The study aimed to assess whether this holds true across the lifespan from juvenility to adulthood. Design and Methods Five hundred twenty-seven participants aged between 10 and 65 years were analyzed. Standard anthropometric measures, carotid ultrasound, and laboratory analysis including interleukin-6, ultra-sensitive C-reactive protein, lipids, glucose metabolism, neopterin, TRP, KYN levels, and the KYN/TRP ratio were performed. Results Overweight/obese (ow/ob) adults had significantly increased KYN serum levels and a significantly increased KYN/TRP ratio. In sharp contrast, ow/ob juvenile males aged ≤18 years showed decreased, females similar KYN and KYN/TRP ratio in comparison to their control counterparts. Also, adult ow/ob subjects with metabolic syndrome showed markedly increased KYN/TRP ratios contrary to decreased KYN/TRP ratios in ow/ob juveniles. Abdominal fat content, characterized by age normalized waist circumference, and not body mass index, had the strongest effect for an increase of the KYN/TRP ratio in adults. Conclusions TRP metabolism and obesity-related immune mediated inflammation differs markedly between juveniles and adults. While childhood obesity seems to be dominated by a Th2-driven activation, an accelerated production of Th1-type cytokines may pave the way for later atherosclerotic endpoints.
机译:目的肥胖相关的免疫介导的全身性炎症与色氨酸(TRP)-犬尿氨酸(KYN)途径的诱导与代谢综合征的发生有关。该研究旨在评估从少年到成年的整个生命周期是否成立。设计与方法分析了257位年龄在10至65岁之间的参与者。进行了标准的人体测量,颈动脉超声检查和实验室分析,包括白介素-6,超敏C反应蛋白,脂质,葡萄糖代谢,新蝶呤,TRP,KYN水平和KYN / TRP比。结果超重/肥胖(ow / ob)成年人的KYN血清水平显着升高,而KYN / TRP比率显着升高。与之形成鲜明对比的是,与对照组相比,年龄≤18岁的ow / ob少年男性下降,女性的KYN和KYN / TRP比率相似。同样,患有代谢综合征的成年ow / ob受试者显示出明显的KYN / TRP比升高,而ow / ob幼年的KYN / TRP比降低。腹部脂肪含量以年龄归一化的腰围而非体重指数为特征,对增加成年人KYN / TRP比具有最强的作用。结论成年人与成年人之间的TRP代谢和肥胖相关的免疫介导的炎症明显不同。虽然儿童肥胖似乎是由Th2驱动的激活所主导,但Th1型细胞因子的加速生产可能为以后的动脉粥样硬化终点铺平了道路。

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