木犀草素和漆黄素在糖尿病条件下通过调节沉默调节蛋白和叉头框蛋白O3a的表达来抑制氧化应激。

Luteolin and fisetin suppress oxidative stress by modulating sirtuins and forkhead box O3a expression under diabetic conditions.

作者信息

Kim Arang, Lee Wooje, Yun Jung-Mi

机构信息

Department of Food and Nutrition, Chonnam National University, Yongbong-ro, Buk-gu, Gwangju 61186, Korea.

National Research Center for Dementia, Chosun University, Gwangju 61452, Korea.

出版信息

Nutr Res Pract. 2017 Oct;11(5):430-434. doi: 10.4162/nrp.2017.11.5.430. Epub 2017 Sep 18.

DOI:10.4162/nrp.2017.11.5.430

PMID:28989580

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5621366/

Abstract

BACKGROUND/OBJECTIVE: Chronic hyperglycemia induces oxidative stress via accumulation of reactive oxygen species (ROS) and contributes to diabetic complications. Hyperglycemia induces mitochondrial superoxide anion production through the increased activity of nicotinamide adenine dinucleotide phosphate (NADPH) oxidase. This study aimed to determine whether fisetin and luteolin treatments suppress the oxidative stress by modulating the expression of sirtuins (SIRTs) and forkhead box O3a (FOXO3a) under hyperglycemic conditions in human monocytes.

MATERIALS/METHODS: Human monocytic cells (THP-1) were cultured under osmotic control (14.5 mmol/L mannitol), normoglycemic (NG, 5.5 mmol/L glucose), or hyperglycemic (HG, 20 mmol/L glucose) conditions, in the absence or presence of fisetin and luteolin for 48 h. To determine the effect of fisetin and luteolin treatments on high glucose-induced oxidative stress, western blotting and intracellular staining were performed.

RESULTS

Hyperglycemic conditions increased the ROS production, as compared to normoglycemic condition. However, fisetin and luteolin treatments inhibited ROS production under hyperglycemia. To obtain further insight into ROS production in hyperglycemic conditions, evaluation of p47phox expression revealed that fisetin and luteolin treatments inhibited p47phox expression under hyperglycemic conditions. Conversely, the expression levels of SIRT1, SIRT3, SIRT6, and FOXO3a were decreased under high glucose conditions compared to normal glucose conditions, but exposure to fisetin and luteolin induced the expression of SIRT1, SIRT3, SIRT6, and FOXO3a. The above findings suggest that fisetin and luteolin inhibited high glucose-induced ROS production in monocytes through the activation of SIRTs and FOXO3a.

CONCLUSIONS

The results of our study supports current researches that state fisetin and luteolin as potential agents for the development of novel strategies for diabetes.

摘要

背景/目的：慢性高血糖通过活性氧（ROS）的积累诱导氧化应激，并导致糖尿病并发症。高血糖通过烟酰胺腺嘌呤二核苷酸磷酸（NADPH）氧化酶活性增加诱导线粒体超氧阴离子产生。本研究旨在确定在高血糖条件下，杨梅素和木犀草素处理是否通过调节沉默调节蛋白（SIRTs）和叉头框O3a（FOXO3a）的表达来抑制人单核细胞中的氧化应激。

材料/方法：人单核细胞（THP-1）在渗透压对照（14.5 mmol/L甘露醇）、正常血糖（NG，5.5 mmol/L葡萄糖）或高血糖（HG，20 mmol/L葡萄糖）条件下培养，在不存在或存在杨梅素和木犀草素的情况下培养48小时。为了确定杨梅素和木犀草素处理对高糖诱导的氧化应激的影响，进行了蛋白质印迹和细胞内染色。

结果

与正常血糖条件相比，高血糖条件下ROS生成增加。然而，杨梅素和木犀草素处理可抑制高血糖条件下的ROS生成。为了进一步了解高血糖条件下的ROS生成，对p47phox表达的评估显示，杨梅素和木犀草素处理可抑制高血糖条件下的p47phox表达。相反，与正常葡萄糖条件相比，高糖条件下SIRT1、SIRT3、SIRT6和FOXO3a的表达水平降低，但暴露于杨梅素和木犀草素可诱导SIRT1、SIRT3、SIRT6和FOXO3a的表达。上述结果表明，杨梅素和木犀草素通过激活SIRTs和FOXO3a抑制高糖诱导的单核细胞ROS生成。

结论

我们的研究结果支持目前的研究，即杨梅素和木犀草素是开发糖尿病新策略的潜在药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c910/5621366/3e9907ade9c5/nrp-11-430-g001.jpg

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木犀草素和漆黄素在糖尿病条件下通过调节沉默调节蛋白和叉头框蛋白O3a的表达来抑制氧化应激。

Luteolin and fisetin suppress oxidative stress by modulating sirtuins and forkhead box O3a expression under diabetic conditions.

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