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血清代谢组学分析显示,轻度高胆红素血症 Gilbert 综合征个体的脂质分解代谢增加。

Serum metabolomics analysis reveals increased lipid catabolism in mildly hyperbilirubinemic Gilbert's syndrome individuals.

机构信息

Faculty of Lifesciences, Department of Nutritional Sciences, University of Vienna, Vienna, Austria.

Faculty of Lifesciences, Department of Nutritional Sciences, University of Vienna, Vienna, Austria.

出版信息

Metabolism. 2021 Dec;125:154913. doi: 10.1016/j.metabol.2021.154913. Epub 2021 Oct 20.

Abstract

BACKGROUND

The protective role of mildly elevated bilirubin against CVD and diabetes mellitus type 2 (DMT2) is associated with a favorable lipid phenotype. As the mechanistic understanding of this protection in humans remains elusive, we aimed to assess the metabolomics profile of mildly hyperbilirubinemic (Gilbert's syndrome; GS) individuals especially targeting lipid catabolism.

METHODS AND RESULTS

Using NMR serum metabolomics of 56 GS individuals and 56 age and gender-matched healthy controls, GS individuals demonstrated significantly greater concentrations of acetylcarnitine (+20%, p < 0.001) and the ketone bodies, 3-hydroxybutyric acid (+132%, p < 0.001), acetoacetic acid (+95%, p < 0.001) and acetone (+46%, p < 0.001). Metabolites associated with an increased mitochondrial lipid metabolism such as citrate (+15%, p < 0.001), anaplerotic amino acid intermediates and creatinine were significantly greater and creatine significantly reduced in GS individuals. Stimulators of lipid catabolism including AMPK (+59%, p < 0.001), pPPARα (+24%, p < 0.001) and T3 (+9%, p = 0.009) supported the metabolomics data while concomitantly blood glucose and insulin (-33%, p = 0.002) levels were significantly reduced. We further showed that the increased lipid catabolism partially mediates the favorable lipid phenotype (lower triglycerides) of GS individuals. Increased trimethylamine (+35%, p < 0.001) indicated changes in trimethylamine metabolism, an emerging predictor of metabolic health.

CONCLUSION

We showed an enhanced lipid catabolism in mildly hyperbilirubinemic individuals, novel evidence as to why these individuals are leaner and protected against chronic metabolic diseases emphasizing bilirubin to be a promising future target in obese and dyslipidemia patients.

摘要

背景

胆红素轻度升高对心血管疾病和 2 型糖尿病(DMT2)的保护作用与有利的脂质表型有关。由于人类对这种保护作用的机制理解仍不清楚,我们旨在评估轻度高胆红素血症(吉尔伯特综合征;GS)个体的代谢组学特征,特别是针对脂质分解代谢。

方法和结果

使用 56 名 GS 个体和 56 名年龄和性别匹配的健康对照者的 NMR 血清代谢组学,GS 个体的乙酰肉碱浓度显著升高(+20%,p<0.001),酮体 3-羟丁酸(+132%,p<0.001)、乙酰乙酸(+95%,p<0.001)和丙酮(+46%,p<0.001)。与增加线粒体脂质代谢相关的代谢物,如柠檬酸(+15%,p<0.001)、生酮氨基酸中间产物和肌酐,在 GS 个体中显著增加,而肌酸显著减少。脂质分解代谢的刺激物,包括 AMPK(+59%,p<0.001)、pPPARα(+24%,p<0.001)和 T3(+9%,p=0.009),支持代谢组学数据,同时血糖和胰岛素水平显著降低(-33%,p=0.002)。我们进一步表明,脂质分解代谢的增加部分介导了 GS 个体有利的脂质表型(更低的甘油三酯)。三甲胺的增加(+35%,p<0.001)表明三甲胺代谢发生了变化,这是代谢健康的一个新的预测指标。

结论

我们显示出轻度高胆红素血症个体的脂质分解代谢增强,这为为什么这些个体更瘦、免受慢性代谢性疾病的保护提供了新的证据,强调胆红素是肥胖和血脂异常患者有前途的未来治疗靶点。

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