Vitamin D Improves the Lipotoxicity of Liver Cells by Adjusting Epigenetic Characteristics of Genes

IF 0.3 4区医学 Q4 GASTROENTEROLOGY & HEPATOLOGY

Hepatitis Monthly Pub Date : 2023-07-26 DOI:10.5812/hepatmon-133758

Suxia Hu, Reyimu Abdusemer

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引用次数: 0

Abstract

Background: With the improvement in living standards and the change in eating habits, the prevalence of nonalcoholic fatty liver disease (NAFLD) has gradually increased, and it has become one of the most common chronic liver diseases worldwide. Objectives: In this study, we used vitamin D3 to interfere with the hyperlipidemia-induced NAFLD cell model to explore the mechanism of vitamin D in improving the lipotoxicity of liver cells by regulating the epigenetic characteristics of genes and to provide new clues for the treatment of late-stage NAFLD. Methods: GSE200765, a data chip for vitamin D3 intervention in liver cell lipotoxicity, was screened from the GEO database. They were divided into the control group (untreated), model group (oleic OA/PA), and vitamin D3 intervention group (OA/PA+SV-VD3 group). Differential expression genes between the control group and model group, model group, and vitamin D3 intervention group were screened by the GEO2R tool. Differentially expressed genes construct a target PPI network map through the STRING database and analyze the KEGG pathway of differentially expressed genes in the DAVID database. The t-test or Unpaired t-test with Welch's correction was used to analyze the expression trend of pathway genes. Results: Compared with the control group, 218 genes were up-regulated, and 255 genes were down-regulated in the model group, of which 26 genes were enriched in the complex and coagulation cascades and cell cycle pathways. After oleic OA/PA was added to HepaRG cells, the complex and coordination cascades pathway was relatively weak, and the cell cycle pathway was relatively strong. Compared with the model group, 554 genes were up-regulated, and 704 genes were down-regulated in the vitamin D3 intervention group, of which 23 genes were enriched in the apoptosis pathway. The apoptosis pathway was relatively weakened after vitamin D3 intervened in oleic OA/PA-treated HepaRG cells. The trend analysis of gene expression in the pathway showed that gene expression disorder in the complex and coagulation cascades, cell cycle, and apoptosis pathways were reversed after vitamin D3 intervention. Conclusions: Through bioinformatics, key pathway genes of vitamin D intervention on hepatocyte lipotoxicity were discovered, which were related to the complex and coordination cascades, cell cycles, and apoptosis pathways. The inhibition of vitamin D on lipotoxicity of human hepatocytes and the possible reversal mechanism was found, which provided ideas for the later treatment of NAFLD and hepatocyte damage.

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维生素D通过调节基因的表观遗传特性改善肝细胞的脂肪毒性

背景:随着生活水平的提高和饮食习惯的改变，非酒精性脂肪性肝病(NAFLD)的患病率逐渐上升，已成为世界范围内最常见的慢性肝病之一。目的:本研究利用维生素D3干预高脂血症诱导的NAFLD细胞模型，探讨维生素D通过调节基因的表观遗传特征改善肝细胞脂毒性的机制，为晚期NAFLD的治疗提供新的线索。方法:从GEO数据库中筛选维生素D3干预肝细胞脂毒性的数据芯片GSE200765。将大鼠分为对照组(未经处理)、模型组(油酸OA/PA)和维生素D3干预组(OA/PA+SV-VD3组)。采用GEO2R工具筛选对照组与模型组、模型组、维生素D3干预组之间的差异表达基因。差异表达基因通过STRING数据库构建目标PPI网络图谱，并在DAVID数据库中分析差异表达基因的KEGG通路。采用t检验或Welch校正的Unpaired t检验分析通路基因的表达趋势。结果:与对照组比较，模型组有218个基因上调，255个基因下调，其中26个基因在复杂、凝血级联及细胞周期通路中富集。在HepaRG细胞中加入油酸OA/PA后，复杂和协调级联通路相对较弱，细胞周期通路相对较强。与模型组比较，维生素D3干预组554个基因上调，704个基因下调，其中23个基因在凋亡通路中富集。维生素D3干预油酸OA/ pa处理的HepaRG细胞后，凋亡途径相对减弱。通路基因表达趋势分析显示，维生素D3干预后，复合物和凝血级联、细胞周期和细胞凋亡通路的基因表达紊乱得到逆转。结论:通过生物信息学发现了维生素D干预肝细胞脂毒性的关键通路基因，这些通路与复杂协调的级联、细胞周期和凋亡通路有关。发现维生素D对人肝细胞脂毒性的抑制作用及其可能的逆转机制，为NAFLD的后期治疗及肝细胞损伤提供思路。

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来源期刊

Hepatitis Monthly 医学-胃肠肝病学

CiteScore

1.50

自引率

0.00%

发文量

审稿时长

3 months

期刊介绍： Hepatitis Monthly is a clinical journal which is informative to all practitioners like gastroenterologists, hepatologists and infectious disease specialists and internists. This authoritative clinical journal was founded by Professor Seyed-Moayed Alavian in 2002. The Journal context is devoted to the particular compilation of the latest worldwide and interdisciplinary approach and findings including original manuscripts, meta-analyses and reviews, health economic papers, debates and consensus statements of the clinical relevance of hepatological field especially liver diseases. In addition, consensus evidential reports not only highlight the new observations, original research, and results accompanied by innovative treatments and all the other relevant topics but also include highlighting disease mechanisms or important clinical observations and letters on articles published in the journal.