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氯贝丁酯影响肝线粒体功能而致肝损伤的观察 被引量:1

Clofibrate induced hepatotoxicity by mitochondrial damage
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摘要 目的研究氯贝丁酯对离体小鼠肝线粒体和体外培养的AML-12肝细胞损伤的作用机制。方法用荧光染料JC-1对线粒体膜电位进行标记,检测膜电位变化。通过DCFDA的标记,检测对线粒体膜自由基的影响。加入环孢素(CsA)和抗氧化剂维生素C、甲磺酸去铁胺、过氧化氢酶等,观察对细胞的保护作用。结果当氯贝丁酯浓度大于0.3 mmol/L时,能迅速降低肝细胞中的线粒体以及小鼠肝脏离体线粒体的膜电位。CsA通过拮抗线粒体膜通透性,抑制膜电位下降,从而抑制细胞死亡。用氯贝丁酯处理过的肝细胞及线粒体内自由基显著增加。抗氧化剂维生素C、甲磺酸去铁胺、过氧化氢酶等能够保护细胞,抑制安妥明引起的损伤和死亡。结论安妥明通过影响线粒体功能,从而诱发过多的自由基产生,最终导致细胞死亡。 Objective To explore the effect of clofibrate on freshly isolated mouse liver mitochondria and a cultured hepatocyte cell line, AML-12. Methods Mitochondrial membrane potential was determined by using the fluorescent dye, JC-1. Levels of reactive oxygen species were measured with the fluorescent probes DCFDA. CsA and antioxidants such as Vitamin C, deferoxamine and catalase were used to protecl cells. Results Application of clofibrate at concentrations greater than 0.3 mmol/L rapidly collapsed the Δψm both in liver cells and in isolated mitochondria. The loss of Δψm occurred prior to cell death, as revealed by the protective effect of cyclosporin A (CsA) on the decrease inΔψm. Treatment of hepatocytes with clofibrate caused a significant increase in intracellular and mitochondrial ROS. Antioxidants such as Vitamin C, deferoxamine, and catalase were able to protect cells against lofibrate-induced loss of viability. Conclusion Clofibrate may impair mitochondrial function, stimulates formation of ROS, and eventually contributes to cell death.
作者 李荻 孙丽红 孙婕 阎莉 瞿斌
机构地区 青岛科技大学化学与分子工程学院 青岛科技大学校医院
出处 《山东大学学报(医学版)》 CAS 北大核心 2008年第12期1192-1196,共5页 Journal of Shandong University:Health Sciences
基金 教育部留学回国人员科研启动基金第24批次资助项目
关键词 氯贝丁酯 线粒体膜电位 细胞凋亡 自由基 Clofibrate Mitochondrial membrane potential Apoptosis Free radicals
分类号 R971.2 [医药卫生—药品] R971 [医药卫生—药品]
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  • 1Lgor P P, Volodymyr P T, Tryndyak, et al. Epigenetic effects of continuous exposure to peroxisome proliferator WY-14,643 in mouse liver are dependent upon peroxisome proliferator activated receptor a[J]. Mutat Res, 2007, 625(1/2):62-71.
  • 2Tomita Y, Yuasa C, Ni R, et al. Long-term maintenance of functional rat hepatocytes in primary culture by additions of pyruvate and various hormones [ J]. Biochim Biophys Acta, 1995, 1243(3):329-335.
  • 3Kidwai N, Gong Y, Sun X P, et al. Expression of androgen receptor and prostate-specific antigen in male breast carcinoma [J]. Breast Cancer Res, 2004, 6(1):R18-R23.
  • 4Yatrik M S, Keiichirou M, Yang Q, et al. Peroxisome proliferator-activated receptor a regulates a microRNA-mediated signaling cascade responsible for hepatocellular proliferation[ J]. Mol Cell Biol, 2007, 27(12):4238-4247.
  • 5Handler J A, Seed C B, Bradford, B U, et al. Induction of per-Oxisomes by treatment with perfluoroocatanoate does not increase rates of H2 02 production in intacr liver [ J ]. Toxicol Lett, 1997(4), 60:61-68.
  • 6Luis J G, Anna C G, Liza A P. Puf3p, a Pumilio family RNA binding protein, localizes to mitochondria and regulates mitochondrial biogenesis and motility in budding yeast [ J ]. J Cell Biol, 2007, 15,176(2) : 197-207.
  • 7Janardan K R, Am J P. Peroxisome proliferators and peroxisome proliferator-activated receptor a [ J]. Biotic Xenobiotic Sensing, 2004, 164(6) :2305-2321.
  • 8Reine N, Caroline M, Philippe L, et al. Mitochondrial and metabolic effects of nucleoside reverse transcriptase inhibitors (NRTIs) in mice receiving one of five single-and three dual- NRTI treatments[J]. Antimicrob Agents Chemother, 2003, 47 ( 11 ) : 3384-3392.
  • 9Zhou S, Wallace K B. The effect of peroxisome proliferators on mitochondrial bioenergetics[ J ]. Toxicol Sci, 1999, 48 (5) : 82- 89.
  • 10Tian H, Ip L, Luo H, et al. A high throughput drug screen based on fluorescence resonance energy transfer (FRET) for anticancer activity of compounds from herbal medicine[J]. Br J Phannacol, 2007, 150(3) :321-334.

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山东大学学报(医学版)
2008年 第12期

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