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赤藓糖醇是戊糖磷酸途径的代谢产物,与年轻人的肥胖增加有关。

Erythritol is a pentose-phosphate pathway metabolite and associated with adiposity gain in young adults.

机构信息

Division of Nutritional Sciences, Cornell University, Ithaca, NY 14853.

Luxembourg Centre for Systems Biomedicine, University of Luxembourg, L-4367 Belvaux, Luxembourg.

出版信息

Proc Natl Acad Sci U S A. 2017 May 23;114(21):E4233-E4240. doi: 10.1073/pnas.1620079114. Epub 2017 May 8.

Abstract

Metabolomic markers associated with incident central adiposity gain were investigated in young adults. In a 9-mo prospective study of university freshmen ( = 264). Blood samples and anthropometry measurements were collected in the first 3 d on campus and at the end of the year. Plasma from individuals was pooled by phenotype [incident central adiposity, stable adiposity, baseline hemoglobin A1c (HbA1c) > 5.05%, HbA1c < 4.92%] and assayed using GC-MS, chromatograms were analyzed using MetaboliteDetector software, and normalized metabolite levels were compared using Welch's test. Assays were repeated using freshly prepared pools, and statistically significant metabolites were quantified in a targeted GC-MS approach. Isotope tracer studies were performed to determine if the potential marker was an endogenous human metabolite in men and in whole blood. Participants with incident central adiposity gain had statistically significantly higher blood erythritol [ < 0.001, false discovery rate (FDR) = 0.0435], and the targeted assay revealed 15-fold [95% confidence interval (CI): 13.27, 16.25] higher blood erythritol compared with participants with stable adiposity. Participants with baseline HbA1c > 5.05% had 21-fold (95% CI: 19.84, 21.41) higher blood erythritol compared with participants with lower HbA1c ( < 0.001, FDR = 0.00016). Erythritol was shown to be synthesized endogenously from glucose via the pentose-phosphate pathway (PPP) in stable isotope-assisted ex vivo blood incubation experiments and through in vivo conversion of erythritol to erythronate in stable isotope-assisted dried blood spot experiments. Therefore, endogenous production of erythritol from glucose may contribute to the association between erythritol and obesity observed in young adults.

摘要

本研究旨在探讨年轻成年人中与中心性肥胖增长相关的代谢标志物。在一项针对大学新生的为期 9 个月的前瞻性研究中(n = 264),在校园内的前 3 天和年底采集了血液样本和人体测量学测量值。根据表型(新发中心性肥胖、稳定肥胖、基线糖化血红蛋白(HbA1c)>5.05%、HbA1c<4.92%)对个体的血浆进行了汇集,并使用 GC-MS 进行了检测,使用 MetaboliteDetector 软件对色谱图进行了分析,使用 Welch's 检验比较了归一化代谢物水平。使用新制备的汇集物重复了检测,并且使用靶向 GC-MS 方法对统计学上显著的代谢物进行了定量。进行了同位素示踪研究以确定潜在的标志物是否为男性和全血中的内源性人类代谢物。与稳定肥胖的参与者相比,新发中心性肥胖的参与者血液赤藓糖醇水平显著升高(<0.001,错误发现率(FDR)= 0.0435),并且靶向检测显示血液赤藓糖醇水平高 15 倍(95%置信区间(CI):13.27,16.25)。与 HbA1c 较低的参与者相比(<0.001,FDR = 0.00016),基线 HbA1c>5.05%的参与者血液赤藓糖醇水平高 21 倍(95%CI:19.84,21.41)。在稳定同位素辅助的体外血液孵育实验中,通过戊糖磷酸途径(PPP)从葡萄糖内源性合成赤藓糖醇,以及在稳定同位素辅助的干血斑实验中,通过体内将赤藓糖醇转化为赤藓酮酸盐,证明了赤藓糖醇的这一作用。因此,葡萄糖内源性产生的赤藓糖醇可能导致在年轻成年人中观察到的赤藓糖醇与肥胖之间的关联。

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