橙皮甙、香草酸和山奈酸通过抑制胰腺离体线粒体的线粒体肿胀和维持线粒体功能,减轻阿托伐他汀诱导的线粒体功能障碍。

IF 3.5 4区 医学 Q2 CHEMISTRY, MEDICINAL
Ahmad Salimi, Saleh Khezri, Zoleikhah Vahabzadeh, Paria Rajabi, Rojin Samimi, Vahed Adhami
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引用次数: 0

摘要

据报道,阿托伐他汀等亲脂性他汀类药物更容易渗入β细胞并到达线粒体,导致线粒体功能障碍、氧化应激、胰岛素释放减少。许多研究表明,天然产物可以保护不同组织中由药物诱导的线粒体功能障碍。我们的目的是探索橙皮甙、香草酸和山奈酸作为天然化合物对阿托伐他汀诱导的胰腺线粒体功能障碍的线粒体保护作用。从大鼠胰腺中分离出线粒体,在不同浓度的橙皮甙、香草酸和山奈酸(1、10 和 100 µM)分别存在的情况下,直接用毒性浓度阿托伐他汀(500 µM)处理线粒体。测量了线粒体毒性参数,如活性氧(ROS)形成、琥珀酸脱氢酶(SDH)活性、线粒体肿胀、谷胱甘肽(GSH)消耗、线粒体膜电位(MMP)崩溃和丙二醛(MDA)产生。我们的研究结果表明,阿托伐他汀在浓度为 500 μM 或更高时可直接诱导胰腺线粒体中毒。除 MDA 外,阿托伐他汀还会导致 SDH 活性明显降低、线粒体肿胀、ROS 形成、GSH 消耗以及 MMP 崩溃。而我们的数据显示,低浓度的三种保护性化合物都能改善阿托伐他汀诱导的线粒体功能障碍,提高 SDH 活性,改善线粒体肿胀、MMP 崩溃和线粒体 GSH,减少 ROS 的形成。由此我们可以得出结论,橙皮甙、香草酸和西那品酸能直接逆转阿托伐他汀对大鼠胰腺离体线粒体的毒性,这可能有利于防止糖尿病诱导的胰腺β细胞线粒体功能障碍。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Hesperidin, vanillic acid, and sinapic acid attenuate atorvastatin-induced mitochondrial dysfunction via inhibition of mitochondrial swelling and maintenance of mitochondrial function in pancreas isolated mitochondria

It has been reported that lipophilic statins such as atorvastatin can more readily penetrate into β-cells and reach the mitochondria, resulting in mitochondrial dysfunction, oxidative stress, decrease in insulin release. Many studies have shown that natural products can protect mitochondrial dysfunction induced by drug in different tissue. We aimed to explore mitochondrial protection potency of hesperidin, vanillic acid, and sinapic acid as natural compounds against mitochondrial dysfunction induced by atorvastatin in pancreas isolated mitochondria. Mitochondria were isolated form rat pancreas and directly treated with toxic concentration of atorvastatin (500 µM) in presence of various concentrations hesperidin, vanillic acid, and sinapic acid (1, 10, and 100 µM) separately. Mitochondrial toxicity parameters such as the reactive oxygen species (ROS) formation, succinate dehydrogenases (SDH) activity, mitochondrial swelling, depletion of glutathione (GSH), mitochondrial membrane potential (MMP) collapse, and malondialdehyde (MDA) production were measured. Our findings demonstrated that atorvastatin directly induced mitochondrial toxicity at concentration of 500 μM and higher in pancreatic mitochondria. Except MDA, atorvastatin caused significantly reduction in SDH activity, mitochondrial swelling, ROS formation, depletion of GSH, and collapse of MMP. While, our data showed that all three protective compounds at low concentrations ameliorated atorvastatin-induced mitochondrial dysfunction with the increase of SDH activity, improvement of mitochondrial swelling, MMP collapse and mitochondrial GSH, and reduction of ROS formation. We can conclude that hesperidin, vanillic acid, and sinapic acid can directly reverse the toxic of atorvastatin in rat pancreas isolated mitochondria, which may be beneficial for protection against diabetogenic-induced mitochondrial dysfunction in pancreatic β-cells.

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来源期刊
CiteScore
6.40
自引率
2.60%
发文量
104
审稿时长
6-12 weeks
期刊介绍: Drug Development Research focuses on research topics related to the discovery and development of new therapeutic entities. The journal publishes original research articles on medicinal chemistry, pharmacology, biotechnology and biopharmaceuticals, toxicology, and drug delivery, formulation, and pharmacokinetics. The journal welcomes manuscripts on new compounds and technologies in all areas focused on human therapeutics, as well as global management, health care policy, and regulatory issues involving the drug discovery and development process. In addition to full-length articles, Drug Development Research publishes Brief Reports on important and timely new research findings, as well as in-depth review articles. The journal also features periodic special thematic issues devoted to specific compound classes, new technologies, and broad aspects of drug discovery and development.
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