Zinc supplementation attenuates ethanol- and acetaldehyde-induced liver stellate cell activation by inhibiting reactive oxygen species (ROS) production and by influencing intracellular signaling.

Szuster Ciesielska A; Plewka K; Daniluk J

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Zinc supplementation attenuates ethanol- and acetaldehyde-induced liver stellate cell activation by inhibiting reactive oxygen species (ROS) production and by influencing intracellular signaling.

机译：补锌通过抑制活性氧（ROS）的产生并影响细胞内信号传导，从而减弱了乙醇和乙醛诱导的肝星状细胞的活化。

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BACKGROUND/AIMS: Zinc has been reported to prevent and reverse liver fibrosis in vivo; however, the mechanisms of its action are poorly understood. We therefore aimed to determine the antifibrotic potential of zinc. METHODS: Assessed was the influence of preincubation of rat HSCs with 30 microM ZnCl2 on ethanol- (in the presence of 4-methyl pyrazole (4-MP)) or acetaldehyde-induced toxicity, apoptosis, migration, expression of smooth muscle alpha-actin (alpha-SMA) and procollagen I, release of reactive oxygen species (ROS), tumor necrosis factor-alpha (TNF-alpha), tumor growth factor-beta1 (TGF-beta1), metalloproteinase-2 (MMP-2) and tissue inhibitors of metalloproteinases (TIMPs) production. Intracellular signals such as nuclear factor-kappaB (NFkappaB), C-Jun N-terminal kinase (JNK) and p38 mitogen-activated protein kinase (p38 MAPK) induced by ethanol and its metabolite were also assessed. RESULTS: 30 microM zinc protected HSCs against ethanol and acetaldehyde toxicity and inhibited their apoptosis. Zinc inhibited the production of ROS by HSCs treated with ethanol and acetaldehyde and inhibited their migration. Zinc also inhibited ethanol- and acetaldehyde-induced TGF-beta1 and TNF-alpha production. Zinc down-regulated ethanol- and acetaldehyde-induced production of TIMP-1 and TIMP-2 and decreased the activity of MMP-2. In ethanol- and acetaldehyde-induced HSCs, zinc inhibited the activation of the p38 MAPK as well as the JNK transduction pathways and phosphorylation of IkappaB and Smad 3. CONCLUSION: The results indicated that zinc supplementation inhibited ethanol- and acetaldehyde-induced activation of HSCs on different levels, acting as an antioxidant and inhibitor of MAPK, TGF-beta and NFkappaB/IkappaB transduction signaling. The remarkable inhibition of several markers of HCS activation makes zinc a promising agent for antifibrotic combination therapies.

机译：背景/目的：锌在体内可预防和逆转肝纤维化。但是，其作用机理了解甚少。因此，我们旨在确定锌的抗纤维化潜力。方法：评估大鼠HSC与30 microM ZnCl2的预孵育对乙醇（在4-甲基吡唑（4-MP）存在下）或乙醛诱导的毒性，细胞凋亡，迁移，平滑肌α-肌动蛋白表达的影响（alpha-SMA）和胶原蛋白I，活性氧（ROS），肿瘤坏死因子-α（TNF-alpha），肿瘤生长因子-beta1（TGF-beta1），金属蛋白酶2（MMP-2）和组织的释放金属蛋白酶（TIMPs）生产的抑制剂。还评估了乙醇及其代谢产物诱导的细胞内信号，例如核因子-κB（NFkappaB），C-Jun N端激酶（JNK）和p38丝裂原活化蛋白激酶（p38 MAPK）。结果：30 microM锌保护HSCs免受乙醇和乙醛毒性，并抑制其凋亡。锌抑制了用乙醇和乙醛处理的HSC产生ROS，并抑制了它们的迁移。锌还抑制乙醇和乙醛诱导的TGF-β1和TNF-α的产生。锌下调乙醇和乙醛诱导的TIMP-1和TIMP-2的产生，并降低MMP-2的活性。在乙醇和乙醛诱导的HSC中，锌抑制了p38 MAPK的活化以及JNK转导途径和IkappaB和Smad 3的磷酸化。结论：结果表明，补锌可以抑制乙醇和乙醛诱导的HSC的活化。在不同水平上起着抗氧化剂和MAPK，TGF-β和NFkappaB / IkappaB转导信号的抑制剂的作用。锌对HCS活化的几种标记物的显着抑制作用使锌成为抗纤维化联合疗法的有前途的药物。

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《Biochemical Pharmacology 》 |2009年第3期| 共14页
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Szuster Ciesielska A; Plewka K; Daniluk J;
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1. Zinc supplementation attenuates ethanol- and acetaldehyde-induced liver stellate cell activation by inhibiting reactive oxygen species (ROS) production and by influencing intracellular signaling. [J] . Szuster Ciesielska A, Plewka K, Daniluk J Biochemical Pharmacology . 2009 ,第3期

机译：补锌通过抑制活性氧（ROS）的产生并影响细胞内信号传导，从而减弱了乙醇和乙醛诱导的肝星状细胞的活化。
2. Betulin and betulinic acid attenuate ethanol-induced liver stellate cell activation by inhibiting reactive oxygen species (ROS), cytokine (TNF-alpha, TGF-beta) production and by influencing intracellular signaling. [J] . Szuster Ciesielska A, Plewka K, Daniluk J, Toxicology: An International Journal Concerned with the Effects of Chemicals on Living Systems . 2011 ,第3期

机译：桦木蛋白和桦木酸通过抑制活性氧（ROS），细胞因子（TNF-α，TGF-β）的产生并影响细胞内信号传导来减弱乙醇诱导的肝星状细胞的活化。
3. Lycopene inhibits reactive oxygen species production in SK-Hep-1 cells and attenuates acetaminophen-induced liver injury in C57BL/6 mice [J] . Balthar Bandeira Ana Carla, da Silva Talita Prato, de Araujo Glaucy Rodrigues, Chemico-biological interactions . 2017 ,第期

机译：番茄红素抑制SK-HEP-1细胞中的反应性氧物种，并衰减C57BL / 6小鼠中的乙酰氨基酚诱导的肝损伤
4. Role of Reactive Oxygen Species in Zinc Deficiency-Induced Hepatic Stellate Cell Activation [C] . A. Kojima-Yuasa, K. Umeda, T. Ohkita, International Society for Free Radical Research . 2006

机译：活性氧物种在缺锌肝星状细胞活化中的作用
5. Mitochondria Are Required for T Cell Activation through Reactive Oxygen Species Signaling. [D] . Sena, Laura A. 2013

机译：通过活性氧信号激活T细胞需要线粒体。
6. MARVELD1 attenuates arsenic trioxide-induced apoptosis in liver cancer cells by inhibiting reactive oxygen species production [O] . Wenping Ma, Haiyang Shen, Qian Li, 2019

机译：MARVELD1通过抑制活性氧的产生来减轻三氧化二砷诱导的肝癌细胞凋亡
7. Zinc supplementation attenuates ethanol- and acetaldehyde-induced liver stellate cell activation by inhibiting reactive oxygen species (ROS) production and by influencing intracellular signaling [O] . Szuster-Ciesielska, Agnieszka, Plewka, Krzysztof, Daniluk, Jadwiga, 2009

机译：补锌通过抑制活性氧（ROS）的产生并影响细胞内信号传导，从而减弱了乙醇和乙醛诱导的肝星状细胞的活化。
8. Hypoxia Inducible Factor 1 (HIF-1) Activation in U87 Glioma Cells Involves a Decrease in Reactive Oxygen Species Production and Protein Kinase C Activity [R] . Forbes, R. A. 1998

机译：U87神经胶质瘤细胞中的缺氧诱导因子1（HIF-1）活化涉及活性氧生成和蛋白激酶C活性的降低

Zinc supplementation attenuates ethanol- and acetaldehyde-induced liver stellate cell activation by inhibiting reactive oxygen species (ROS) production and by influencing intracellular signaling.

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