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Metabolome‐Genome‐Wide Association Study (mGWAS) Reveals Novel Metabolites Associated with Future Type 2 Diabetes Risk and Susceptibility Loci in a Case‐Control Study in a Chinese Prospective Cohort

机译:代谢物 - 基因组 - 范围的协会研究(MGWAs)揭示了与未来2型糖尿病风险和易感性基因座相关的新型代谢产物在中国潜在队列中的病例对照研究中

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摘要

In a Chinese prospective cohort, 500 patients with new‐onset type 2 diabetes (T2D) within 4.61 years and 500 matched healthy participants are selected as case and control groups, and randomized into discovery and validation sets to discover the metabolite changes before T2D onset and the related diabetogenic loci. A serum metabolomics analysis reveals that 81 metabolites changed significantly before T2D onset. Based on binary logistic regression, eight metabolites are defined as a biomarker panel for T2D prediction. Pipecolinic acid, carnitine C14:0, epinephrine and phosphatidylethanolamine 34:2 are first found associated with future T2D. The addition of the biomarker panel to the clinical markers (BMI, triglycerides, and fasting glucose) significantly improves the predictive ability in the discovery and validation sets, respectively. By associating metabolomics with genomics, a significant correlation (p < 5.0 × 10−8) between eicosatetraenoic acid and the FADS1 (rs174559) gene is observed, and suggestive correlations (p < 5.0 × 10−6) between pipecolinic acid and CHRM3 (rs535514), and leucine/isoleucine and WWOX (rs72487966) are discovered. Elevated leucine/isoleucine levels increased the risk of T2D. In conclusion, multiple metabolic dysregulations are observed to occur before T2D onset, and the new biomarker panel can help to predict T2D risk.
机译:在中国前瞻性队列中,500名患有45岁的糖尿病(T2D)在4.61岁内和500名匹配的健康参与者被选为案例和对照组,并随机分为发现和验证集,以发现T2D发作前的代谢物变化。相关糖尿病基因座。血清代谢组科分析显示,在T2D发作之前,81代谢物显着变化。基于二进制逻辑回归,八个代谢物定义为T2D预测的生物标志物面板。哌啶甲酸,肉碱C14:0,肾上腺素和磷脂酰乙醇胺34:2首先与未来T2D相关联。将生物标志物面板添加到临床标记物(BMI,甘油三酯和空腹葡萄糖)中分别显着提高了发现和验证集中的预测能力。通过将代谢组织与基因组学相关联,观察到唾液酸四烯酸和FADS1(RS174559)基因之间的显着相关性(P <5.0×10-8),并在苯乙烯酸和CHRM3之间提出暗示相关性(P <5.0×10-6)(RS535514 )和亮氨酸/异亮氨酸和WWOX(RS72487966)被发现。升高的亮氨酸/异亮氨酸水平增加了T2D的风险。总之,观察到在T2D发作前发生多种代谢厌购,并且新的生物标志物面板可以有助于预测T2D风险。

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