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黄芪甲苷通过调控宿主核糖体翻译开关抑制HBV复制的机制
DOI: 10.3969/j.issn.1001-5256.2022.07.009
利益冲突声明:本研究不存在研究者、伦理委员会成员、受试者监护人以及与公开研究成果有关的利益冲突。
作者贡献声明:常凯、王艳艳负责课题设计,资料分析,撰写论文;常凯、王艳艳、那琬琳、刘晨霞、叶雨笙、江忠勇参与实验实施与修改论文;常凯、刘媛负责拟定写作思路,指导撰写文章并最后定稿。
Mechanism of astragaloside Ⅳ inhibits hepatitis B virus replication by regulating host ribosome translation process
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摘要:
目的 分析黄芪甲苷抑制HBV复制的宿主调控机制。 方法 使用不同浓度的黄芪甲苷处理人正常肝细胞(L-02),根据黄芪甲苷浓度的不同,分为0、5、10和20 μg/mL 4组。应用CCK-8检测细胞活性,流式细胞法检测细胞凋亡,化学发光和生化方法检测AFP、ALT、AST和ALP外泌水平,评估黄芪甲苷对正常细胞的影响。用黄芪甲苷处理携带HBV的肝癌细胞Hep3B,应用qPCR方法检测HBV DNA、pgRNA、MTIF2、RPL10基因表达量,ELISA测法检测HBsAg和HBeAg,评估对HBV复制的影响。应用TCGA和GEO数据库结合R语言资料包对RPL10和MTIF2在临床样本中的预后影响进行分析验证。绘制Kaplan-Meier生存曲线,log-rank检验用于分析比较两组或多组之间的生存差异,进行了time ROC分析以比较RPL10和MTIF2基因的预测准确性和风险评分。计量资料多组间比较和同一组内不同时间段比较均采用单因素方差分析,进一步分析两两组间比较采用Bonferroni方法。 结果 20 μg/mL组处理24 h和48 h相较未处理组细胞生长活性均显著提高(P值均<0.05),20 μg/mL组处理72 h相较10 μg/mL组生长活性提高(P<0.05),5 μg/mL组处理72 h相较未处理组生长活性提高(P<0.05)。5、10和20 μg/mL 3个处理组AFP水平均较未处理组显著增高(P值均<0.05),10和20 μg/mL 2个处理组ALT水平分别均较未处理和5 μg/mL 2组显著降低(P值均<0.05),20 μg/mL组ALT水平较10 μg/mL组显著降低(P<0.05)。5、10和20 μg/mL 3个处理组AST水平较未处理组均显著增高(P值均<0.05)。5、10和20 μg/mL 3个处理组HBV DNA、pgRNA、HBsAg、HBeAg、RPL10和MTIF2水平与未处理组比较差异均有统计学意义(P值均<0.05)。生物信息学分析结果显示,HBV感染的肝癌患者中RPL10和MTIF2基因较高水平表达的患者预后较差,而在无HBV感染的肝癌患者中不存在此现象。 结论 黄芪甲苷能够抑制翻译起始蛋白MTIF2和核糖体大亚基成分RPL10,通过调控宿主核糖体翻译开关降低HBV复制。 Abstract:Objective To investigate the host regulatory mechanism of astragaloside Ⅳ in inhibiting hepatitis B virus (HBV) replication. Methods Normal human hepatocytes L-02 were treated with different concentrations of astragaloside Ⅳ, and according to the concentration of astragaloside Ⅳ, the cells were divided into 0, 5, 10, and 20 μg/mL groups. CCK-8 assay was used to measure cell viability, flow cytometry was used to measure cell apoptosis, and chemiluminescence and biochemical methods were used to measure the levels of alpha-fetoprotein (AFP), alanine aminotransferase (ALT), aspartate aminotransferase (AST), and alkaline phosphatase (ALP), so as to evaluate the influence of astragaloside Ⅳ on normal cells. Hepatoma cells Hep3B carrying HBV were treated with astragaloside Ⅳ; quantitative PCR was used to measure the mRNA expression levels of HBV DNA, pgRNA, MTIF2, and RPL10, and ELISA was used to measure the levels of HBsAg and HBeAg, so as to evaluate the effect of astragaloside Ⅳ on HBV replication. TCGA and GEO databases combined with R language package were used to analyze the prognostic effect of RPL10 and MTIF2 in clinical samples. The Kaplan-Meier method was used for survival analysis, and the log-rank test was used for comparison of survival between two or multiple groups; the time-dependent ROC curve analysis was performed to compare the predictive accuracy and risk score of RPL10 and MTIF2 genes. A one-way analysis of variance was used for comparison of continuous data between multiple groups and within each group at different time points, and the Bonferroni method was used for further comparison between two groups. Results Compared with the untreated group, the 20 μg/mL group had a significant increase in cell growth activity at 24 and 48 hours of treatment (both P < 0.05); compared with the 10 μg/mL group, the 20 μg/mL group had a significant increase in cell growth activity at 72 hours of treatment (P < 0.05); compared with the untreated group, the 5 μg/mL group had a significant increase in cell growth activity at 72 hours of treatment (P < 0.05). Compared with the untreated group, the 5, 10, and 20 μg/mL groups had a significant increase in AFP (all P < 0.05); compared with the untreated group and the 5 μg/mL group, the 10 and 20 μg/mL groups had a significant reduction in ALT (all P < 0.05), and compared with the 10 μg/mL group, the 20 μg/mL group had a significant reduction in ALT (P < 0.05). Compared with the untreated group, the 5, 10, and 20 μg/mL groups had a significant increase in AST (all P < 0.05). There were significant differences in the levels of HBV DNA, pgRNA, HBsAg, HBeAg, RPL10, and MTIF2 between the 5/10/20 μg/mL groups and the untreated group (all P < 0.05). The bioinformatics analysis showed that among the liver cancer patients with HBV infection, the patients with high mRNA expression levels of RPL10 and MTIF2 genes tended to have a poor prognosis, while this phenomenon was not observed in liver cancer patients without HBV infection. Conclusion Astragaloside Ⅳ can inhibit the translation initiation factor MTIF2 and the large ribosomal subunit RPL10 and reduce HBV replication by regulating the initiation of host ribosome translation. -
Key words:
- Astragaloside Ⅳ /
- Hepatitis B virus /
- Ribosomal Proteins
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图 1 不同浓度的黄芪甲苷对L-02外泌蛋白的影响
注:与0 μg/mL组比较,* P<0.05;与5 μg/mL组比较,# P<0.05。
Figure 1. Effect of Astragaloside Ⅳ on L-02 exocrine protein
图 2 RPL10 & MTIF2蛋白互作分析和黄芪甲苷参与HBV复制的分子机制示意图
注:a, RPL10 & MTIF2蛋白互作分析图;b, 黄芪甲苷参与HBV复制的分子机制示意图。
Figure 2. RPL10 and MTIF2 protein interaction analysis with GeneMANIA and molecular mechanism of Astragaloside Ⅳ on hepatitis B virus replication
图 3 RPL10 & MTIF2调控HBV复制相关基因的富集分析及临床生存曲线分析
注:a, 一致性聚类结果热图;b, 相关基因表达聚类热图;c, RPL10基因生存曲线分析;d, MTIF2基因生存曲线分析;e, RPL10和MTIF2基因联合生存曲线分析;f, 不同样本Risk score对应的生存时间和生存状态散点分布图。
Figure 3. RPL10 & MTIF2 regulated gene enrichment and clinical survival curve analysis in HBV replication
图 4 黄芪甲苷对HBV复制装配中相关基因及蛋白表达的影响
注:与0 μg/mL组比较,*P<0.05。
Figure 4. The effect of Astragaloside Ⅳ on the expression of related genes and proteins in HBV replication assembly
表 1 RT-PCR引物列表
Table 1. List of RT-PCR primers
基因名称 引物序列(5′-3′) Tm值(℃) MTIF2 F-MTIF2 CTATGATGCTTCACACGAGTG 53 R-MTIF2 TGCTCTTCCACAGCACAGG 53 RPL10 F-RPL10 CGGTATTGTAAGAACAAGCCGT 60 R-RPL10 GCCACAAAGCGGAAACTCAT 60 pgRNA F-pgRNA CTCAATCTCGGGAATCTCAATGT 53 R-pgRNA TGGATAAAACCTAGCAGGCATAAT 53 GAPDH F-GAPDH CAGGAGGCATTGCTGATGAT 52 R-GAPDH GAAGGCTGGGGCTCATTT 52 
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表 2 黄芪甲苷对人正常肝细胞L-02细胞生长活性的影响
Table 2. Effect of Astragaloside Ⅳ on L-02 cell growth activity
组别 细胞活性(%) 24 h 48 h 72 h 0 μg/mL组 95.11±0.88 91.69±0.52 90.85±1.41 5 μg/mL组 94.40±6.05 92.35±3.81 91.13±3.371) 10 μg/mL组 94.31±7.44 94.47±4.60 91.64±1.84 20 μg/mL组 100.23±1.401) 97.35±0.671) 99.56±0.442) F值 0.682 1.433 8.301 P值 0.617 0.362 0.030 注:与0 μg/mL组比较,1)P<0.05;与10 μg/mL组,2)P<0.05。
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表 3 黄芪甲苷对L-02细胞凋亡的影响
Table 3. Effect of Astragaloside Ⅳ on L-02 cell apoptosis
组别 死亡率(%) 凋亡率(%) 死亡+凋亡率(%) 0 μg/mL组 2.74±0.45 2.72±0.27 5.46±0.72 5 μg/mL组 3.07±0.68 3.27±0.43 6.34±0.92 10 μg/mL组 3.16±0.56 3.10±0.34 6.26±0.47 20 μg/mL组 3.35±0.69 2.96±0.76 6.31±0.96 F值 0.533 0.689 0.853 P值 0.672 0.584 0.503
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表 4 不同浓度的黄芪甲苷处理对L-02外泌蛋白的影响
Table 4. Effect of different concentrations of Astragaloside Ⅳ treatment on L-02 cell exoprotein
组别 AFP(ng/mL) ALT(U/L) AST(U/L) ALP(U/L) 0 μg/mL组 13.25±0.20 6.46±0.67 5.68±0.21 40.68±0.61 5 μg/mL组 14.75±0.201) 6.27±0.16 7.63±0.221) 38.68±0.921) 10 μg/mL组 14.48±0.131) 3.09±0.081)2) 6.57±0.461) 40.37±0.37 20 μg/mL组 14.42±0.481) 1.80±0.131)2)3) 7.61±0.171) 43.77±0.341) F值 16.180 129.523 31.670 36.847 P值 0.001 0.001 0.001 0.001 注:与0 μg/mL组比较,1)P<0.05;与5 μg/mL组,2)P<0.05;与10 μg/mL组,3)P<0.05。
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表 5 黄芪甲苷对HBV复制装配中相关基因及蛋白表达的影响
Table 5. The effect of Astragaloside Ⅳ on the expression of related genes and proteins in HBV replication assembly
组别 HBV DNA(IU/mL) pgRNA HBsAg HBeAg RPL10 MTIF2 0 μg/mL组 43 300.00±23 356.25 1.07±0.09 0.70±0.03 0.62±0.06 1.30±0.51 1.02±0.05 5 μg/mL组 7 420.00±955.981) 0.46±0.191) 0.58±0.041) 0.41±0.041) 0.79±0.041) 0.51±0.181) 10 μg/mL组 6 730.00±141.071) 0.63±0.131) 0.32±0.041) 0.46±0.011) 0.32±0.041) 0.63±0.081) 20 μg/mL组 4900.00±400.371) 0.74±0.031) 0.56±0.051) 0.34±0.021) 0.56±0.051) 0.56±0.221) F值 7.532 12.159 33.026 17.251 4.633 4.712 P值 0.010 0.002 0.003 0.009 0.037 0.035 注:与0 μg/mL组比较,1)P<0.05。
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[1] PAN J, ZHANG M, YAO TT, et al. Efficiency and influencing factors of interferon therapy for 1-6 years old children with chronic hepatitis B[J]. Int J Virol, 2020, 27(3): 214-218. DOI: 10.3760/cma.j.issn.1673-4092.2020.03.009.潘静, 张敏, 姚甜甜, 等. 干扰素治疗1~6岁慢性乙型肝炎的疗效及影响因素[J]. 国际病毒学杂志, 2020, 27(3): 214-218. DOI: 10.3760/cma.j.issn.1673-4092.2020.03.009. [2] REVILL PA, PENICAUD C, BRECHOT C, et al. Meeting the challenge of eliminating chronic hepatitis B infection[J]. Genes (Basel), 2019, 10(4): 260. DOI: 10.3390/genes10040260. [3] ZHENG X, LIU J, WU J, et al. Advances and challenges in immune control and functional cure of chronic hepatitis B[J]. J Clin Hepatol, 2020, 36(5): 961-964. DOI: 10.3969/j.issn.1001-5256.2020.05.001郑昕, 刘嘉, 吴珺, 等. 免疫控制与慢性乙型肝炎功能性治愈的进展与挑战[J]. 临床肝胆病杂志, 2020, 36(5): 961-964. DOI: 10.3969/j.issn.1001-5256.2020.05.001. [4] van de LAAR TJ, van GAEVER VA, SWIETEN PV, et al. Phylogenetic analysis reveals three distinct epidemiological profiles in Dutch and Flemish blood donors with hepatitis B virus infection[J]. Virology, 2018, 515: 243-249. DOI: 10.1016/j.virol.2017.12.011. [5] ZHOU R, CHEN H, CHEN J, et al. Extract from Astragalus membranaceus inhibit breast cancer cells proliferation via PI3K/AKT/mTOR signaling pathway[J]. BMC Complement Altern Med, 2018, 18(1): 83. DOI: 10.1186/s12906-018-2148-2. [6] CHE D, ADAMS S, WEI C, et al. Effects of Astragalus membranaceus fiber on growth performance, nutrient digestibility, microbial composition, VFA production, gut pH, and immunity of weaned pigs[J]. Microbiologyopen, 2019, 8(5): e00712. DOI: 10.1002/mbo3.712. [7] LUO Y, WAN Q, XU M, et al. Nutritional preconditioning induced by astragaloside Ⅳ on isolated hearts and cardiomyocytes against myocardial ischemia injury via improving Bcl-2-mediated mitochondrial function[J]. Chem Biol Interact, 2019, 309: 108723. DOI: 10.1016/j.cbi.2019.06.036. [8] LU M, TANG F, ZHANG J, et al. Astragaloside Ⅳ attenuates injury caused by myocardial ischemia/reperfusion in rats via regulation of toll-like receptor 4/nuclear factor-κ B signaling pathway[J]. Phytother Res, 2015, 29(4): 599-606. DOI: 10.1002/ptr.5297. [9] WU S, LI XF, WANG QT, et al. Effects of fermented milkvetch root on proliferation and expression of aging-related proteins in human embryonic lung diploid fibroblast cell[J]. J Changchun Univ Chin Med, 2020, 36(4): 676-679. DOI: 10.13463/j.cnki.cczyy.2020.04.019.吴爽, 李学锋, 王秋彤, 等. 发酵黄芪对人胚肺二倍体成纤维细胞增殖及衰老相关蛋白表达的影响[J]. 长春中医药大学学报, 2020, 36(4): 676-679. DOI: 10.13463/j.cnki.cczyy.2020.04.019. [10] CHEN CC, CHANG LC, YAO CH, et al. Increased calcitonin gene-related peptide and macrophages are involved in astragalus membranaceus-mediated peripheral nerve regeneration in rats[J]. Am J Chin Med, 2018, 46(1): 69-86. DOI: 10.1142/S0192415X18500040. [11] WU XM, YUAN WS. In vitro study of the anti - HBV activity of astragalus[J]. Guangdong Med J, 2008, 29(1): 37-38. DOI: 10.13820/j.cnki.gdyx.2008.01.003.吴晓蔓, 袁文声. 黄芪抗乙型肝炎病毒的体外实验研究[J]. 广东医学, 2008, 29(1): 37-38. DOI: 10.13820/j.cnki.gdyx.2008.01.003. [12] YAN JY. Effect and mechanism of huangqi injection combined with entecavir against hepatitis B virus infection[D]. Guangzhou: Guangzhou University of Chinese Medicine, 2015.严景妍. 黄芪注射液联合恩替卡韦抗乙型肝炎病毒感染机理研究[D]. 广州: 广州中医药大学, 2015. [13] ZHANG J, CHEN JZ, ZHANG JP, et al. Inhibitory effect of astragaloside Ⅳ on human hepatitis B virus replication in vitro[J]. J Fourth MilMed Univ, 2007, 28(24): 2291-2293. DOI: 1000-2790(2007)24-2291-03.张娟, 陈建宗, 张金平, 等. 黄芪甲甙体外抗乙型肝炎病毒的作用[J]. 第四军医大学学报, 2007, 28(24): 2291-2293. DOI: 1000-2790(2007)24-2291-03. [14] XU D, WANG Y, WU J, et al. MTIF2 impairs 5 fluorouracil-mediated immunogenic cell death in hepatocellular carcinoma in vivo: Molecular mechanisms and therapeutic significance[J]. Pharmacol Res, 2021, 163: 105265. DOI: 10.1016/j.phrs.2020.105265. [15] OVERMAN RG JR, ENDERLE PJ, FARROW JM 3rd, et al. The human mitochondrial translation initiation factor 2 gene (MTIF2): transcriptional analysis and identification of a pseudogene[J]. Biochim Biophys Acta, 2003, 1628(3): 195-205. DOI: 10.1016/s0167-4781(03)00144-1. [16] LEE DE, PERRY RA JR, BROWN JL, et al. Mitochondrial mRNA translation initiation contributes to oxidative metabolism in the myocardia of aged, obese mice[J]. Exp Gerontol, 2019, 121: 62-70. DOI: 10.1016/j.exger.2019.03.009. [17] ZHONG Y, LIU DL, AHMED M, et al. Transcription and regulation of hepatitis B virus genes in host sperm cells[J]. Asian J Androl, 2018, 20(3): 284-289. DOI: 10.4103/aja.aja_46_17. [18] HEDGES J, WEST M, JOHNSON AW. Release of the export adapter, Nmd3p, from the 60S ribosomal subunit requires Rpl10p and the cytoplasmic GTPase Lsg1p[J]. EMBO J, 2005, 24(3): 567-579. DOI: 10.1038/sj.emboj.7600547. [19] YE YS, CHANG K, ZHU ZY, et al. Gemcitabine promotes hepatitis B virus pgRNA transcription and viral replication in HepG2.2.15 cells and related molecular mechanisms[J]. J Chongqing Med Univ, 2019, 44(12): 1564-1570. DOI: 10.13406/j.cnki.cyxb.002221.叶雨笙, 常凯, 朱紫衣, 等. 吉西他滨促进HepG2.2.15细胞系中乙肝病毒pgRNA转录和病毒复制及相关分子机制研究[J]. 重庆医科大学学报, 2019, 44(12): 1564-1570. DOI: 10.13406/j.cnki.cyxb.002221. [20] GU XL. MicroRNA-124 prevents H2O2-induced apoptosis and oxidative stress in human lens epithelial cells via inhibition of the NF-κ B signaling pathway[J]. Pharmacology, 2018, 102(3-4): 213-222. DOI: 10.1159/000491433. [21] VLASBLOM J, ZUBERI K, RODRIGUEZ H, et al. Novel function discovery with GeneMANIA: a new integrated resource for gene function prediction in Escherichia coli[J]. Bioinformatics, 2015, 31(3): 306-310. DOI: 10.1093/bioinformatics/btu671. [22] MOHD-ISMAIL NK, LIM Z, GUNARATNE J, et al. Mapping the interactions of HBV cccDNA with host factors[J]. Int J Mol Sci, 2019, 20(17): 4276. DOI: 10.3390/ijms20174276. [23] FRITZLAR S, AKTEPE TE, CHAO YW, et al. Mouse norovirus infection arrests host cell translation uncoupled from the stress granule-PKR-eIF2αaxis[J]. mBio, 2019, 10(3): e00960-19. DOI: 10.1128/mBio.00960-19. [24] TEO C, O'HARE P. A bimodal switch in global protein translation coupled to eIF4H relocalisation during advancing cell-cell transmission of herpes simplex virus[J]. PLoS Pathog, 2018, 14(7): e1007196. DOI: 10.1371/journal.ppat.1007196. [25] HU YM, LIU LH, LIU BC, et al. Radioprotective effects of astragaloside Ⅳ on the liver cell[J]. J Radiat Res Radiat Process, 2015, 33(6): 19-24. DOI: 10.11889/j.1000-3436.2015.rrj.33.060202.胡雅梦, 刘琅嬛, 刘宝婵, 等. 黄芪甲苷对肝细胞的辐射防护作用[J]. 辐射研究与辐射工艺学报, 2015, 33(6): 19-24. DOI: 10.11889/j.1000-3436.2015.rrj.33.060202. [26] LIU L, LI SJ, ZHOU Y. Protective effect of astragaloside Ⅳ against acute liver failure in experimental mice[J]. Chin J Hepatol, 2016, 24(10): 772-777. DOI: 10.3760/cma.j.issn.1007-3418.2016.10.011.刘丽, 李双杰, 周宇. 黄芪甲苷对实验性急性肝衰竭小鼠的保护作用[J]. 中华肝脏病杂志, 2016, 24(10): 772-777. DOI: 10.3760/cma.j.issn.1007-3418.2016.10.011. [27] RINGELHAN M, MCKEATING JA, PROTZER U. Viral hepatitis and liver cancer[J]. Philos Trans R Soc Lond B Biol Sci, 2017, 372(1732): 20160274. DOI: 10.1098/rstb.2016.0274. [28] LUBYOVÁ B, WEBER J. Posttranslational modifications of HBV core protein[J]. Acta Virol, 2020, 64(2): 177-186. DOI: 10.4149/av_2020_207. -
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