帕立骨化醇抑制氧化应激减轻小鼠肝细胞紧密连接受损

doi:10.16352/j.issn.1001-6325.2024.03.0317

基础医学与临床 ›› 2024, Vol. 44 ›› Issue (3): 317-324.doi: 10.16352/j.issn.1001-6325.2024.03.0317

帕立骨化醇抑制氧化应激减轻小鼠肝细胞紧密连接受损

张威威^1,2, 谢婧², 李丽华^1*

1.沈阳医学院病理生理教研室,辽宁沈阳 110034;
2.台州学院医学院基础教研室,浙江台州 318000

收稿日期:2023-11-20 修回日期:2023-12-28 出版日期:2024-03-05 发布日期:2024-02-22
通讯作者: ^*:347584368@qq.com
基金资助:
浙江省自然科学基金(LY23H030002)

Paricalcitol inhibition of oxidative stress alleviates the damage of hepatocyte tight junction in mice

ZHANG Weiwei^1,2, XIE Jing², LI Lihua^1*

1. Department of Pathophysiology, Shenyang Medical College, Shenyang 110034;
2. Department of Basic Education, School of Medicine, Taizhou University, Taizhou 318000, China

Received:2023-11-20 Revised:2023-12-28 Online:2024-03-05 Published:2024-02-22
Contact: ^*:347584368@qq.com

摘要/Abstract

摘要： 目的探讨帕立骨化醇(Pal)对氧化应激诱导的肝细胞紧密连接受损的影响及其机制研究。方法体内实验:采用胆总管结扎构建胆汁淤积性肝损伤模型。小鼠随机分为对照组(control)、模型组(BDL)、治疗组(BDL+Pal)。通过HE染色,探究各组小鼠肝组织病理形态变化。体外培养人肝癌细胞系HepG2,分为空白组、模型组(400 μmol/L H₂O₂)、治疗组(400 μmol/L H₂O₂+20 nmol/L Pal)。Western blot检测各组紧密连接蛋白1(ZO-1)、闭合蛋白(occludin)、磷酸化p65(p-p65)、磷酸化ERK(p-ERK)、磷酸化肌球蛋白II调节轻链(p-MLC)蛋白水平。结果与对照组相比,模型组p-p65、p-ERK、p-MLC蛋白水平显著升高(P＜0.0001或P＜0.01或P＜0.001);ZO-1、occludin蛋白表达水平显著降低(P＜0.01);HE染色显示肝细胞坏死及炎性细胞浸润增多。而治疗组相对于模型组,上述水平呈相反趋势。结论 Pal通过抑制胆汁淤积性小鼠及HepG2细胞中的氧化应激,从而减轻肝细胞紧密连接受损,其机制可能与抑制活性氧及NF-κB/p65、ERK信号通路有关。

关键词: 帕立骨化醇, 氧化应激, 胆汁淤积, 肝损伤

Abstract: Objective To explore the impact of paricalcitol (Pal) on the oxidative stress-induced tight junction damage of mouse hepatocytes and its mechanism. Methods A model of cholestatic liver injury was created by routine bile duct ligation. The mice were randomly divided into control group (control), model group (BDL) and treatment group (BDL+Pal). HE staining microscopy was used to observe the morphological changes of liver tissues. The human hepatoma cell line HepG2 was cultured and divided into blank group, model group (400 μmol/L H₂O₂) and treatment group (400 μmol/L H₂O₂+20 nmol/L Pal). Western blot was used to examine the level of tight junction protein 1 (ZO-1), occludin, phosphorylated p65 (p-p65), phosphorylated ERK (p-ERK) and phosphorylated myosin II regulated light chain (p-MLC) protein were checked in each group. Results Compared with the control group, the level of p-p65, p-ERK and p-MLC in the model group was significantly increased (P＜0.000 1 or P＜0.01 or P＜0.001). The protein expression of ZO-1 and occludin was significantly decreased (P＜0.01). HE staining microscopy showed an increased hepatocyte necrosis and inflammatory cell infiltration. In contrast, the above levels in the treatment group showed an opposite trend relative to the model group. Conclusions Pal is able to alleviate the damage of hepatocyte tight junctions by inhibiting oxidative stress in cholestatic mice and HepG2 cells. Its mechanism is potentially related to the inhibition of reactive oxygen species and NF-κB/p65 and ERK signaling pathways.

Key words: paricalcitol, oxidative stress, cholestasis, liver injury

中图分类号:

R575
R332

张威威, 谢婧, 李丽华. 帕立骨化醇抑制氧化应激减轻小鼠肝细胞紧密连接受损[J]. 基础医学与临床, 2024, 44(3): 317-324.

ZHANG Weiwei, XIE Jing, LI Lihua. Paricalcitol inhibition of oxidative stress alleviates the damage of hepatocyte tight junction in mice[J]. Basic & Clinical Medicine, 2024, 44(3): 317-324.

参考文献 15

[1]	Cichoz·-Lach H, Michalak A.Oxidative stress as a crucial factor in liver diseases[J].World J Gastroenterol, 2014, 20: 8082-8091.
[2]	Copple BL, Jaeschke H, Klaassen CD.Oxidative stress and the pathogenesis of cholestasis[J].Semin Liver Dis, 2010, 30: 195-204.
[3]	Li L, Yang F, Jia R, et al. Velvet antler polypeptide prevents the disruption of hepatic tight junctions via inhibiting oxidative stress in cholestatic mice and liver cell lines[J].Food Funct, 2020, 11: 9752-9763.
[4]	Zeisel MB, Dhawan P, Baumert TF.Tight junction proteins in gastrointestinal and liver disease[J].Gut, 2019, 68: 547-561.
[5]	Rao R. Oxidative stress-induced disruption of epithelial and endothelial tight junctions[J].Front Biosci, 2008, 13: 7210-7226.
[6]	Xu J, Kausalya PJ, Van Hul N, et al. Protective functions of ZO-2/Tjp2 expressed in hepatocytes and cholangiocytes against liver injury and cholestasis[J].Gastroenterology, 2021, 160: 2103-2118.
[7]	Firrincieli D, Zúñiga S, Rey C, et al. Vitamin D nuclear receptor deficiency promotes cholestatic liver injury by disruption of biliary epithelial cell junctions in mice[J].Hepatology, 2013, 58: 1401-1412.
[8]	Zheng Z, Xie J, Ma L, et al. Vitamin D receptor activation targets ROS-mediated crosstalk between auto-phagy and apoptosis in hepatocytes in cholestasic mice[J].Cell Mol Gastroenterol Hepatol, 2023, 15: 887-901.
[9]	Rao RK, Basuroy S, Rao VU, et al. Tyrosine phosphorylation and dissociation of occludin-ZO-1 and E-cadherin-beta-catenin complexes from the cytoskeleton by oxidative stress[J].Biochem J, 2002, 368: 471-481.
[10]	Boyer JL, Soroka CJ. Bile formation and secretion: an update[J].J Hepatol, 2021, 75: 190-201.
[11]	Martínez-Arias L, Panizo S, Alonso-Montes C, et al. Effects of calcitriol and paricalcitol on renal fibrosis in CKD[J].Nephrol Dial Transplant, 2021, 36: 793-803.
[12]	Jia R, Yang F, Yan P, et al. Paricalcitol inhibits oxidative stress-induced cell senescence of the bile duct epithelium dependent on modulating Sirt1 pathway in cholestatic mice[J].Free Radic Biol Med, 2021, 169: 158-168.
[13]	Yu M Wang Q, Ma Y, et al. Aryl hydrocarbon receptor activation modulates intestinal epithelial barrier function by maintaining tight junction integrity[J].Int J Biol Sci, 2018, 14: 69-77.
[14]	Zhou HY, Zhu H, Yao XM, et al. Metformin regulates tight junction of intestinal epithelial cells via MLCK-MLC signaling pathway.[J].Eur Rev Med Pharmacol Sci, 2017, 21: 5239-5246.
[15]	Izadparast F, Riahi-Zajani B, Yarmohammadi F, et al. Protective effect of berberine against LPS-induced injury in the intestine: a review[J].Cell Cycle, 2022, 21: 2365-2378.

帕立骨化醇抑制氧化应激减轻小鼠肝细胞紧密连接受损

Paricalcitol inhibition of oxidative stress alleviates the damage of hepatocyte tight junction in mice

PDF

可视化

摘要/Abstract

引用本文

使用本文

参考文献 15

相关文章 15

编辑推荐

Metrics

本文评价

[1]	杨瀚毅, 宁佳怡, 汪小兰, 张益萌, 谢婷珂, 陈奕玄, 韩静. 褪黑素抑制H₂O₂诱导的人脐静脉内皮细胞氧化应激及凋亡标志蛋白质的表达[J]. 基础医学与临床, 2024, 44(5): 645-650.
[2]	王瑞, 李蕊, 李运龙, 张玉萍, 于康, 刘燕萍. 锶与妊娠及妊娠期疾病的研究进展[J]. 基础医学与临床, 2024, 44(4): 428-433.
[3]	张秀丽, 胡孝刚, 莫俊, 陈铃. 冠心宁片减轻大鼠颈动脉粥样硬化斑块损伤[J]. 基础医学与临床, 2024, 44(2): 192-198.
[4]	牟杨, 杨志文. 右美托咪定通过激活AMPK减轻TNF-α诱导人成神经细胞瘤细胞系SH-SY5Y损伤[J]. 基础医学与临床, 2024, 44(2): 147-153.
[5]	田宗源, 李展, 刘瑞霞. TERT调控线粒体氧化应激在疾病中的作用[J]. 基础医学与临床, 2024, 44(10): 1436-1441.
[6]	胡宁, 黄涵年, 夏道宗. 两种不同种属小鼠急性免疫性肝损伤模型的比较[J]. 基础医学与临床, 2023, 43(9): 1364-1368.
[7]	陈新军, 王卿语, 陈乐, 古春昱, 武卓. 紫檀茋减轻百草枯诱导的模型大鼠肺纤维化[J]. 基础医学与临床, 2023, 43(9): 1383-1389.
[8]	王琼, 董倩兰, 朱燕亭, 金刚, 张琳萍. 桔梗皂苷D减轻大鼠肾缺血/再灌注损伤[J]. 基础医学与临床, 2023, 43(8): 1222-1228.
[9]	杨为祝, 刘忠, 张峰林, 黄延林, 孙瑾, 田新华. NOX4介导的氧化应激参与垂体腺瘤出血性卒中的发生[J]. 基础医学与临床, 2023, 43(7): 1040-1044.
[10]	汪博, 张明焕. CIRC_0044235靶向miR-574-5p减轻IL-1β诱导的人软骨细胞损伤[J]. 基础医学与临床, 2023, 43(3): 419-426.
[11]	张梦瑶, 牛姝, 蔡静, 张立香, 赵志刚. 丹参酮ⅡA减轻高糖诱导的小鼠足细胞系PMC-5凋亡和氧化应激反应[J]. 基础医学与临床, 2023, 43(2): 277-282.
[12]	何綦琪, 吴晃, 李昱卓, 包军胜. 线粒体功能障碍在肾结石成石中作用的研究进展[J]. 基础医学与临床, 2023, 43(2): 306-310.
[13]	袁培根, 陈顺利, 单鸳露, 薛彬彬, 叶玉柱, 林丽娜. 艾司氯胺酮减轻大鼠骨骼肌缺血再灌注损伤[J]. 基础医学与临床, 2023, 43(12): 1822-1826.
[14]	顾炜, 祝剑平, 吴品雯. 丙泊酚减轻低氧诱导的大鼠肾上腺嗜铬细胞瘤细胞系PC12炎性反应和细胞凋亡[J]. 基础医学与临床, 2023, 43(1): 137-143.
[15]	郭丽苹, 苏娟, 田新雁, 陆丽, 胡亚荣, 秦燕. 骨桥蛋白在大鼠肝缺血/再灌注损伤中的作用[J]. 基础医学与临床, 2023, 43(1): 83-86.