L-aspartate ameliorates diet-induced obesity by increasing adipocyte energy expenditure.

IF 5.4 2区 医学 Q1 ENDOCRINOLOGY & METABOLISM Diabetes, Obesity & Metabolism Pub Date : 2024-11-11 DOI:10.1111/dom.16053
Shi-Yao Guo, Yu-Tao Hu, Yong Rao, Zhi Jiang, Chan Li, Yu-Wei Lin, Shu-Min Xu, Dan-Dan Zhao, Li-Yuan Wei, Shi-Liang Huang, Qing-Jiang Li, Jia-Heng Tan, Shuo-Bin Chen, Zhi-Shu Huang
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Abstract

Aims: Obesity always leads to profound perturbation of metabolome. Metabolome studies enrich the knowledge on associations between endogenous metabolites and obesity, potentially providing innovative strategies for the development of novel anti-obesity pharmacotherapy. This study aims to identify an endogenous metabolite that regulates energy expenditure and to explore its application for obesity treatment.

Materials and methods: C57BL/6 mice were fed with a high-fat and high-cholesterol (HFC) diet, comprising 60% fat and 1.2% cholesterol, for 12 weeks to induce obesity. Significant metabolites were identified in the livers of both health and obese mice through comparative hepatic metabolomics analysis. Correlation between serum or adipose L-aspartate level and body weight in obese mice, as well as human body mass index (BMI), was evaluated. In addition, saline or 200 mg/kg L-aspartate was orally administrated to HFC diet mice and HFC diet-induced obese mice for 6-7 weeks. Body weight, adipose tissue weight, glucose tolerance and liver damage were assessed to evaluate the effect on obesity prevention and treatment. Comprehensive lab animal monitoring system (CLAMS) and seahorse assay were employed to investigate the regulatory effect of L-aspartate on energy metabolism in vivo and in vitro, respectively. 3T3-L1 preadipocytes and murine white adipose tissue (WAT) were utilized to examine the impact of L-aspartate on adipocyte adipogenesis and lipogenesis and cellular signalling pathway in vitro and in vivo.

Results: L-aspartate, an approved drug for liver injury and chronic fatigue, was identified as an endogenous inducer of energy expenditure. Serum or adipose L-aspartate levels were found to be negatively correlated with the severity of obesity in both humans and mice. Administration of L-aspartate to HFC diet mice led to a significant reduction in body weight, with decreases of 14.5% in HFC diet mice and 8.5% in HFC diet-induced obese mice, respectively. In addition, the treatment improved related metabolic syndrome (Figure 2 and Figure S3). These therapeutics were associated with enhancements in whole-body energy expenditure and suppression of adipocyte adipogenesis along with activation of Adenosine 5'-monophosphate-activated protein kinase (AMPK) signalling pathway.

Conclusion: L-aspartate may serve as a novel endogenous inducer of energy expenditure and suppressor of adipogenesis and lipogenesis along with activation of AMPK, thereby offering a promising therapeutic strategy for obesity prevention and treatment.

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L-天门冬氨酸可通过增加脂肪细胞的能量消耗来改善饮食引起的肥胖。
目的:肥胖总是导致代谢组的严重紊乱。代谢组研究丰富了内源性代谢物与肥胖之间关系的知识,可能为开发新型抗肥胖药物疗法提供创新策略。本研究旨在确定一种调节能量消耗的内源性代谢物,并探索其在肥胖治疗中的应用:用高脂肪、高胆固醇(HFC)饮食(含 60% 脂肪和 1.2% 胆固醇)喂养 C57BL/6 小鼠 12 周以诱发肥胖。通过肝脏代谢组学比较分析,确定了健康小鼠和肥胖小鼠肝脏中的重要代谢物。评估了血清或脂肪中 L-天门冬氨酸水平与肥胖小鼠体重以及人类体重指数(BMI)之间的相关性。此外,给氢氟碳化合物饮食小鼠和氢氟碳化合物饮食诱导的肥胖小鼠口服生理盐水或 200 毫克/千克 L-天门冬氨酸,持续 6-7 周。对体重、脂肪组织重量、糖耐量和肝损伤进行评估,以评价其对肥胖症的预防和治疗效果。采用综合实验动物监测系统(CLAMS)和海马测定法分别研究 L-天门冬氨酸在体内和体外对能量代谢的调节作用。利用3T3-L1前脂肪细胞和小鼠白色脂肪组织(WAT)研究了L-天门冬氨酸在体外和体内对脂肪细胞脂肪生成和脂肪生成以及细胞信号通路的影响:结果:L-天门冬氨酸是一种被批准用于治疗肝损伤和慢性疲劳的药物,被认为是能量消耗的内源性诱导剂。研究发现,人和小鼠血清或脂肪中的 L-天门冬氨酸水平与肥胖的严重程度呈负相关。给氢氟碳化合物饮食小鼠注射 L-天门冬氨酸可显著降低体重,氢氟碳化合物饮食小鼠和氢氟碳化合物饮食诱发的肥胖小鼠的体重分别下降了 14.5%和 8.5%。此外,治疗还改善了相关的代谢综合征(图 2 和图 S3)。这些疗法与增强全身能量消耗、抑制脂肪细胞脂肪生成以及激活腺苷-5'-单磷酸激活蛋白激酶(AMPK)信号通路有关:结论:L-天门冬氨酸可作为一种新型的内源性能量消耗诱导剂,在激活 AMPK 的同时抑制脂肪细胞的脂肪生成,从而为肥胖症的预防和治疗提供了一种前景广阔的治疗策略。
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来源期刊
Diabetes, Obesity & Metabolism
Diabetes, Obesity & Metabolism 医学-内分泌学与代谢
CiteScore
10.90
自引率
6.90%
发文量
319
审稿时长
3-8 weeks
期刊介绍: Diabetes, Obesity and Metabolism is primarily a journal of clinical and experimental pharmacology and therapeutics covering the interrelated areas of diabetes, obesity and metabolism. The journal prioritises high-quality original research that reports on the effects of new or existing therapies, including dietary, exercise and lifestyle (non-pharmacological) interventions, in any aspect of metabolic and endocrine disease, either in humans or animal and cellular systems. ‘Metabolism’ may relate to lipids, bone and drug metabolism, or broader aspects of endocrine dysfunction. Preclinical pharmacology, pharmacokinetic studies, meta-analyses and those addressing drug safety and tolerability are also highly suitable for publication in this journal. Original research may be published as a main paper or as a research letter.
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