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首页> 外文期刊>Metabolism: Clinical and Experimental >Differences in the redox status of human visceral and subcutaneous adipose tissues - Relationships to obesity and metabolic risk
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Differences in the redox status of human visceral and subcutaneous adipose tissues - Relationships to obesity and metabolic risk

机译:人体内脏和皮下脂肪组织氧化还原状态的差异-与肥胖和代谢风险的关系

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摘要

Objective Metabolic homeostasis depends on adipocyte metabolic responses/processes, most of which are redox-regulated. Besides, visceral and subcutaneous adipose tissues (VAT and SAT, respectively) differ metabolically and in their contribution to metabolic complications, but their redox characteristics in humans are still unknown. To understand the molecular mechanisms of metabolic syndrome development, we analysed the redox characteristics of VAT and SAT in groups with various body weights and metabolic risks. Material and Methods Fifty premenopausal women were classified according to body mass index into normal-weight and obese groups, and these groups were further sub-classified into metabolically healthy and metabolically obese ("at risk") based on the homeostasis model assessment of insulin resistance (HOMA-IR) index and the triglyceride, total-, LDL- and HDL-cholesterol levels. Antioxidant components, NADPH oxidase protein and 4-hydroxynonenal (4-HNE) levels were analysed in VAT and SAT. Results Compared with the SAT, the VAT showed a higher basal level of glutathione (GSH) and GSH-dependent enzyme activities. Compared with the metabolically healthy normal-weight controls, the obese groups of women showed lower GSH levels in both depots. However, in these groups, additional prooxidative changes (increased NADPH oxidase and 4-HNE and decreased levels of SOD and/or CAT) were observed only in VAT. Conclusions Because of the critical role of thiol-redox homeostasis in lipogenesis, interdepot-differences in the GSH-dependent antioxidant part may be connected to the higher metabolic activity found in VAT. Analogously, the lower GSH levels that occur during obesity and the corresponding additional redox imbalance may be signs of VAT metabolic dysfunction that underlie the subsequent metabolic impairment.
机译:目的代谢稳态取决于脂肪细胞的代谢反应/过程,其中大多数受氧化还原调节。此外,内脏和皮下脂肪组织(分别为VAT和SAT)在代谢上和它们对代谢并发症的贡献上也不同,但是它们在人体中的氧化还原特性仍然未知。为了了解代谢综合征发展的分子机制,我们分析了体重和代谢风险各异的人群中VAT和SAT的氧化还原特性。材料和方法根据体重指数将50名绝经前妇女分为正常体重和肥胖组,根据胰岛素抵抗的稳态模型评估,将这些组进一步分为代谢健康和代谢肥胖(“处于危险中”)。 (HOMA-IR)指数和甘油三酸酯,总,LDL和HDL胆固醇水平。在VAT和SAT中分析了抗氧化剂成分,NADPH氧化酶蛋白和4-羟基壬烯(4-HNE)水平。结果与SAT相比,增值税显示出较高的谷胱甘肽(GSH)基础水平和GSH依赖性酶活性。与代谢健康的正常体重对照组相比,肥胖妇女在这两个仓库中均显示出较低的谷胱甘肽水平。但是,在这些组中,仅在增值税中观察到了其他的促氧化变化(NADPH氧化酶和4-HNE升高,SOD和/或CAT含量降低)。结论由于硫醇-氧化还原稳态在脂肪形成中的关键作用,依赖于GSH的抗氧化剂部分的库间差异可能与增值税中较高的代谢活性有关。类似地,在肥胖期间发生的较低的GSH水平和相应的额外氧化还原失衡可能是导致随后的代谢损害的VAT代谢功能障碍的迹象。

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