黄连素对缺氧复氧诱导大鼠心肌细胞内Nrf2/Keap1的影响
Effects of berberine on the expression of Nrf2/Keap1 in hypoxia reoxygenation induced myocardial cells
目的 探讨黄连素(BR)对大鼠H9c2心肌细胞缺氧/复氧(H/R)损伤后凋亡的影响及其作用机制。 方法 将培养的H9c2心肌细胞随机分为:正常对照组(NC组)、单纯药物组(BR组)、缺氧/复氧组(H/R组)、药物低剂量LBR组(1.5×10-6 mol/L)及高剂量HBR组(1.5×10-4 mol/L)。处理结束后,用MTT比色法检测H9c2心肌细胞的活力,用Hoechst33258染色检测细胞核形态的变化,用Western blot法检测Nrf2, Keap1蛋白的表达。 结果 与NC组比较,单纯BR对H9c2心肌细胞无影响。与H/R组比较,低、高剂量BR组细胞的活力明显上升(65.2±1.6%; 82.3±1.4%) (P<0.01),心肌细胞的凋亡率明显减少(P<0.05),Western blot的结果显示,BR可明显促进抗氧化相关蛋白Nrf2表达,抑制Keap1的表达。 结论 BR对H9c2心肌细胞H/R损伤后的凋亡具有显著的抑制作用,可能与其促进抗氧化核转录因子Nrf2表达有关。
Objective To examine the effect of berberine on hypoxia reoxygenation induced apoptosis in myocardial cells and to explore the potential mechanisms involved. Methods H9C2 cardiac muscle cells were divided into: normal control group (NC group), simple berberine group (BR group), hypoxia reoxygenation group (HR group) and drug treatment group (divided into LBR group: 1.5×10-6 mol/L, HBR group 1.5×10-4 mol/L). Myocardial cell vitality was detected by MTT, nucleus morphological changes were examined using Hoechst 33258 dye and Nrf2 and Keap1 protein expressions were detected by Western blot. Results Compared with that in NC group, simple berberine exerted no effect on myocardial cells in BR group. Compared with those in HR group, the cell vitality in treatment groups increased((65.2±1.6)%; (82.3±1.4)%; P<0.01),and apoptosis decreased significantly(P<0.05). Western blot results showed that berberine increased the expression of the antioxidant-related protein Nrf2, and reduced the level of Keap1. Conclusion Berberine has significant protective effect on hypoxia reoxygenation induced apoptosis in myocardial cells possibly by enhancing the release of Nrf2 and decreasing the expression of Keap1.
[1] Saks VA, Kuznetsov AV, Vendelin M, et al. Functional coupling as a basic mechanism of feedback regulation of cardiac energy metabolism[J].Mol Cell Biochem,2004, 256-257 (1-2):185-199.
[2] Wei LY, Zhang YJ, Wei BH, et al. Effect of comparability of Coptis chinensis and Scutellaria baicalensis on five sub-enzymatic activities of liver microsomes in rats[J]. Zhongguo Zhong Yao Za Zhi, 2013, 38(9):1426-1429.
[3] 于永燕,于丁.黄连素预处理对家兔心肌缺血再灌注损伤的抗氧化保护作用[J].湖南中医药大学学报, 2011, 31(10):7-11.
[4] Yu W, Sheng W, Xu R, et al. Berberine protects human renal proximal tubular cells from hypoxia/reoxygenation injury via inhibiting endoplasmic reticulum and mitochondrial stress pathways[J]. J Transl Med, 2013, 11:24.
[5] 车奕宏,王海昌. 黄连素对缺氧/复氧诱导的大鼠心肌细胞损伤的拮抗作用[J].心脏杂志, 2014,26( 3):271-273.
[6] 王松海,何虹, 李雪芬,等.红景天苷通过激活 Nrf2减轻 MPP +诱导的PC12细胞凋亡[J].神经解剖学杂志, 2013,29(6): 651-655.
[7] 车奕宏. 黄连素通过调节Bcl-2家族蛋白和Caspase通路抑制缺氧/复氧诱导的H9C2细胞凋亡[D].西安. 第四军医大学研究生院, 2014:35-36.
[8] 丁士骜, 梅举. 线粒体与心肌缺血/再灌注损伤的研究进展[J].医学综述, 2016, 22(1):37-41.
[9] 黄正新, 黄献平,袁肇凯. 养心通脉方对大鼠心肌缺血损伤模型心肌细胞线粒体功能的影响[J].湖南中医药大学学报, 2016, 36(7):25-27.
[10] Buja LM. The pathobiology of acute coronary syndromes: clinical implications and central role of the mitochondria[J]. Tex Heart Inst J, 2013, 40(3):221-228.
[11] 林春梅, 梁荫基, 张金文,等. Nrf2/ARE 通路在肝脏疾病中的研究进展[J]. 中国中西医结合消化杂志, 2015, 23(1):67-70.
[12] Tkachev VO, Menshchikova EB, Zenkov NK. Mechanism of the Nrf2/Keap1/ARE signaling system[J]. Biochemistry (Moscow), 2011, 76(4):407-422.
[13]李航, 段惠军. Nrf2/ARE信号通路及其调控的抗氧化蛋白[J].中国药理学通报, 2011, 27(3): 10-13.
[14] Vrba J, Gazák R, Kuzma M, et al. A novel semisynthetic flavonoid 7-O-galloyltaxifolin upreulates heme oxygenase-1 in RAW264.7 cells via MAPK/Nrf2 pathway[J]. J Med Chem, 2013, 56(3): 856-866.
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