NRH, a potent NAD+ booster, improves glucose homeostasis and lipid metabolism in diet-induced obese mice though an active adenosine kinase pathway.

bioRxiv - Pharmacology and Toxicology Pub Date : 2024-08-30 DOI:10.1101/2024.08.29.610289
Xinliu Zeng, Yongjie Wang, Karina Gisselle Farias, Andrew Rappa, Christine Darko, Anthony A Sauve, Yue Yang
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Abstract

NAD+ deficiency underlies obesity-induced metabolic disturbances. Here we evaluated the treatment effect of a new and potent NAD+ enhancer, dihydronicotinamide riboside (NRH), in diet-induced obese mice with hyperglycemia and hyperlipidemia. Administering NRH for 7 weeks improved glucose homeostasis by enhancing pancreatic beta-cell functional mass, increasing muscle insulin sensitivity, and reducing hepatic gluconeogenesis. NRH treatment also mobilized fat deposition, reduced circulating lipid, and improved white adipose function. Significant elevation in multi-tissue NAD+ levels and sirtuin (SIRT) activities, especially SIRT3, mediated these metabolic improvements. Inhibiting adenosine kinase (ADK), a newly recognized enzyme in the NRH-induced NAD+ synthesis pathway, blocked NRH effect in improving glucose and lipid metabolism. ADK inhibition also reduced tissue NAD+ elevation and the subsequent activation of SIRT3, suggesting an active ADK pathway is necessary for NRH-induced metabolic benefits. These observations, for the first time, establish NRH as a promising intervention for correcting obesity-induced metabolic syndrome.
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NRH 是一种有效的 NAD+ 促进剂,它通过活跃的腺苷激酶途径改善饮食诱导肥胖小鼠的葡萄糖稳态和脂质代谢。
NAD+ 缺乏是肥胖诱发代谢紊乱的基础。在这里,我们评估了一种新型强效 NAD+ 增强剂--二氢烟酰胺核糖甙(NRH)--对饮食诱导的高血糖和高脂血症肥胖小鼠的治疗效果。连续 7 周服用 NRH 可增强胰岛β细胞功能、提高肌肉对胰岛素的敏感性并减少肝脏葡萄糖生成,从而改善葡萄糖稳态。NRH 治疗还能动员脂肪沉积、降低循环血脂并改善白色脂肪功能。多组织 NAD+ 水平和 sirtuin(SIRT)活性(尤其是 SIRT3)的显著提高促成了这些代谢改善。腺苷激酶(ADK)是新发现的 NRH 诱导 NAD+ 合成途径中的一种酶,它的抑制阻断了 NRH 在改善葡萄糖和脂质代谢方面的作用。抑制 ADK 还降低了组织 NAD+ 的升高和随后 SIRT3 的激活,这表明活跃的 ADK 途径是 NRH 诱导代谢益处的必要条件。这些观察结果首次证明,NRH 是纠正肥胖引起的代谢综合征的一种很有前景的干预措施。
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bioRxiv - Pharmacology and Toxicology
bioRxiv - Pharmacology and Toxicology
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