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黄嘌呤氧化酶抑制剂托匹司他对糖尿病肥胖小鼠体重的影响。

Influence of xanthine oxidoreductase inhibitor, topiroxostat, on body weight of diabetic obese mice.

机构信息

Pharmacological Study Group Pharmaceutical Research Laboratories, Sanwa Kagaku Kenkyusho, Mie, Japan.

Medical Affairs Department, Sanwa Kagaku Kenkyusho, Aichi, Japan.

出版信息

Nutr Diabetes. 2021 Apr 13;11(1):12. doi: 10.1038/s41387-021-00155-2.

Abstract

Plasma xanthine oxidoreductase (XOR) activity is high in metabolic disorders such as diabetic mellitus, obesity, or overweight. Thus, this study investigated whether the XOR inhibitor, topiroxostat, affected body weight. Male db/db mice were fed standard diets with or without topiroxostat for 4 weeks. Body weight and food intake were constantly monitored, along with monitoring plasma biochemical markers, including insulin and XOR activity. Additionally, hepatic hypoxanthine and XOR activity were also documented. Single regression analysis was performed to determine the mechanism. Topiroxostat treatment suppressed weight gain relative to the vehicle without any impact on food intake. However, the weight of fat pads and hepatic and muscle triglyceride content did not change. Topiroxostat decreased the plasma uric acid and increased hepatic hypoxanthine in response to the inhibition of XOR activity. Plasma ketone body and free fatty acid were also increased. Moreover, fat weight was weakly associated with plasma XOR activity in the diabetic state and was negatively associated with ketone body by topiroxostat. These results suggested that topiroxostat amplified the burning of lipids and the salvage pathway, resulting in predisposing the body toward catabolism. The inhibition of plasma XOR activity may contribute to weight loss.

摘要

血浆黄嘌呤氧化还原酶 (XOR) 活性在代谢紊乱如糖尿病、肥胖或超重中较高。因此,本研究调查了 XOR 抑制剂托匹司他是否影响体重。雄性 db/db 小鼠喂食标准饮食,或添加或不添加托匹司他共 4 周。持续监测体重和食物摄入量,同时监测包括胰岛素和 XOR 活性在内的血浆生化标志物。此外,还记录了肝次黄嘌呤和 XOR 活性。进行了单回归分析以确定机制。托匹司他治疗相对于载体抑制了体重增加,而对食物摄入没有影响。然而,脂肪垫、肝和肌肉甘油三酯含量没有变化。托匹司他降低了血浆尿酸并增加了肝次黄嘌呤,这是对 XOR 活性抑制的反应。血浆酮体和游离脂肪酸也增加了。此外,在糖尿病状态下,脂肪重量与血浆 XOR 活性呈弱相关,而托匹司他使酮体与脂肪重量呈负相关。这些结果表明,托匹司他增强了脂肪的燃烧和补救途径,导致身体倾向于分解代谢。血浆 XOR 活性的抑制可能有助于减轻体重。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1995/8044114/4f7069fa5d8e/41387_2021_155_Fig1_HTML.jpg

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