Identification and characterization of a novel bipartite nuclear localization signal in the hepatitis B virus polymerase 被引量：8

Identification and characterization of a novel bipartite nuclear localization signal in the hepatitis B virus polymerase

下载PDF

导出

摘要 AIM:To characterize the nuclear import of hepatitis B virus(HBV)polymerase(P)and its relevance for the viral life cycle.METHODS:Sequence analysis was performed to predict functional motives within P.Phosphorylation of P was analyzed by in vitro phosphorylation.Phosphorylation site and nuclear localization signal(NLS)were destroyed by site directed mutagenesis.Functionality of the identified NLS was analyzed by confocal fluorescence microscopy and characterizing the karyopherin binding.Relevance of the structural motives for viral life cycle was studied by infection of primary Tupaia hepatocytes with HBV.RESULTS:We identified by sequence alignment and functional experiments a conserved bipartite NLS containing a casein kinaseⅡ(CKⅡ)phosphorylation site located within the terminal protein domain(TP)of the HBV polymerase.Inhibition of CKⅡimpairs the functionality of this NLS and thereby prevents the nuclear import of the polymerase.Binding of the import factor karyopherin-α2 to the polymerase depends on its CKⅡ-mediated phosphorylation of the bipartite NLS.In HBV-infected primary Tupaia hepatocytes CKⅡinhibition in the early phase(post entry phase)of the infection process prevents the establishment of the infection.CONCLUSION:Based on these data it is suggested that during HBV infection the final import of the genome complex into the nucleus is mediated by a novel bipartite NLS localized in the TP domain of HBV polymerase. AIM: To characterize the nuclear import of hepatitis B virus (HBV) polymerase (P) and its relevance for the viral life cycle. METHODS: Sequence analysis was performed to predict functional motives within P. Phosphorylation of P was analyzed by in vitro phosphorylation. Phosphorylation site and nuclear localization signal (NLS) were destroyed by site directed mutagenesis. Functionality of the identified NLS was analyzed by confocal fluorescence microscopy and characterizing the karyopherin binding. Relevance of the structural motives for viral life cycle was studied by infection of primary Tupaia hepatocytes with HBV. RESULTS: We identified by sequence alignment and functional experiments a conserved bipartite NLS containing a casein kinase II (CKII) phosphorylation site located within the terminal protein domain (TP) of the HBV polymerase. Inhibition of CKII impairs the functionality of this NLS and thereby prevents the nuclear import of the polymerase. Binding of the import factor karyopherin-α2 to the polymerase depends on its CKII-mediated phosphorylation of the bipartite NLS. In HBV-infected primary Tupaia hepatocytes CKII inhibition in the early phase (post entry phase) of the infection process prevents the establishment of the infection. CONCLUSION: Based on these data it is suggested that during HBV infection the final import of the genome complex into the nucleus is mediated by a novel bipartite NLS localized in the TP domain of HBV polymerase.

作者 Joachim Lupberger Stephanie Schaedler Alexander Peiran Eberhard Hildt

机构地区 Department of Medicine Ⅱ Inserm Division of Virology Division of Virology

出处《World Journal of Gastroenterology》 SCIE CAS 2013年第44期8000-8010,共11页 世界胃肠病学杂志（英文版）

基金 Supported by A Grant from DZIF to Hildt E

关键词 Hepatitis B virus Nuclear localization signal CASEIN kinase Ⅱ TRAFFICKING REPLICATION Hepatitis B virus Nuclear localization signal Casein kinase II Trafficking Replication

分类号 R512.62 [医药卫生—内科学]

引文网络
相关文献

参考文献14

1Ya-Jun Tan.Hepatitis B virus infection and the risk of hepatocellular carcinoma[J].World Journal of Gastroenterology,2011,17(44):4853-4857. 被引量：25
2Daniela Ploen,Mohamed Lamine Hafirassou,Kiyoshi Himmelsbach,Daniel Sauter,Martin L. Biniossek,Thomas S. Weiss,Thomas F. Baumert,Catherine Schuster,Eberhard Hildt.TIP47 plays a crucial role in the life cycle of hepatitis C virus[J]. Journal of Hepatology . 2013 (6)
3Reinhild Prange.Host factors involved in hepatitis B virus maturation, assembly, and egress[J]. Medical Microbiology and Immunology . 2012 (4)
4Anika Prange,Melanie Bartsch,Julia Meiners,Margrethe Serek,Traud Winkelmann.Interspecific somatic hybrids between Cyclamen persicum and C. coum, two sexually incompatible species[J]. Plant Cell Reports . 2012 (4)
5Youn-Chul Shin,Chunkyu Ko,Wang-Shick Ryu.Hydrophobic residues of terminal protein domain of hepatitis B virus polymerase contribute to distinct steps in viral genome replication[J]. FEBS Letters . 2011 (24)
6LindaWittkop,AlexandraSchwarz,AureliaCassany,StefanieGrün‐Bernhard,MildredDelaleau,BirgitRabe,ChristianCazenave,WolframGerlich,DieterGlebe,MichaelKann.Inhibition of protein kinase C phosphorylation of hepatitis B virus capsids inhibits virion formation and causes intracellular capsid accumulation[J]. Cellular Microbiology . 2010 (7)
7Vera C. Kantelhardt,Alexandra Schwarz,Ulrike Wend,Christian G. Schüttler,Wulf R. Willems,Pascale Trimoulet,Hervé Fleury,Wolfram H. Gerlich,Michael Kann.Re-evaluation of anti-HBc non-reactive serum samples from patients with persistent hepatitis B infection by immune precipitation with labelled HBV core antigen[J]. Journal of Clinical Virology . 2009 (2)
8Michael Nassal.Hepatitis B viruses: Reverse transcription a different way[J]. Virus Research . 2008 (1)
9Joachim Lupberger,Andreas Mund,Josef Kock,Eberhard Hildt.Cultivation of HepG2.2.15 on Cytodex-3: Higher yield of hepatitis B virus and less subviral particles compared to conventional culture methods[J]. Journal of Hepatology . 2006 (4)
10E. Bleifuss?,T. Kammertoens?,A. Hutloff,D. Quarcoo,M. Dorner,P. Straub,W. Uckert,E. Hildt.The translocation motif of hepatitis B virus improves protein vaccination[J]. Cellular and Molecular Life Sciences . 2006 (5)

二级参考文献41

1Dong Q,Chan HL,Liu Z,Chan DP,Zhang B,Chen Y,Kung HF,Sung JJ,He ML. A1762T/G1764A mutations of hepatitis B virus,associated with the increased risk of hepatocellular carcinoma,reduce basal core promoter activities. Biochem Biophys Res Commun 2008; 374: 773-776.
2Kusakabe A,Tanaka Y,Inoue M,Kurbanov F,Tatematsu K, Nojiri S,Joh T,Tsugane S,Mizokami M. A population-based cohort study for the risk factors of HCC among hepatitis B virus mono-infected subjects in Japan. J Gastroenterol 2011; 46: 117-124.
3Tanaka Y,Mukaide M,Orito E,Yuen MF,Ito K,Kurbanov F,Sugauchi F,Asahina Y,Izumi N,Kato M,Lai CL,Ueda R,Mizokami M. Specific mutations in enhancer II/core promoter of hepatitis B virus subgenotypes C1/C2 increase the risk of hepatocellular carcinoma. J Hepatol 2006; 45: 646-653.
4Xu L,Qian G,Tang L,Su J,Wang JS. Genetic variations of hepatitis B virus and serum aflatoxin-lysine adduct on high risk of hepatocellular carcinoma in Southern Guangxi,China. J Hepatol 2010; 53: 671-676.
5Fan W,Shi B,Wei H,Du G,Song S. Comparison of hepatitis B X gene mutation between patients with hepatocellular carcinoma and patients with chronic hepatitis B. Virus Genes 2011; 42: 162-170.
6Chu CM,Liaw YF. Genotype C hepatitis B virus infection is associated with a higher risk of reactivation of hepatitis B and progression to cirrhosis than genotype B: a longitudinal study of hepatitis B e antigen-positive patients with normal aminotransferase levels at baseline. J Hepatol 2005; 43: 411-417.
7Fang ZL,Sabin CA,Dong BQ,Wei SC,Chen QY,Fang KX, Yang JY,Huang J,Wang XY,Harrison TJ. Hepatitis B virus pre-S deletion mutations are a risk factor for hepatocellular carcinoma: a matched nested case-control study. J Gen Virol 2008; 89: 2882-2890.
8Wang HC,Chang WT,Chang WW,Wu HC,Huang W,Lei HY,Lai MD,Fausto N,Su IJ. Hepatitis B virus pre-S2 mutant upregulates cyclin A expression and induces nodular proliferation of hepatocytes. Hepatology 2005; 41: 761-770.
9Park IY,Sohn BH,Yu E,Suh DJ,Chung YH,Lee JH,Surzycki SJ,Lee YI. Aberrant epigenetic modifications in hepatocarcinogenesis induced by hepatitis B virus X protein. Gastroenterology 2007; 132: 1476-1494.
10Su H,Zhao J,Xiong Y,Xu T,Zhou F,Yuan Y,Zhang Y,Zhuang SM. Large-scale analysis of the genetic and epigenetic alterations in hepatocellular carcinoma from Southeast China. Mutat Res 2008; 641: 27-35.

共引文献24

1Lei Li,Wei Liu,Yu-Han Chen,Chun-Lei Fan,Pei-Ling Dong,Fei-Li Wei,Bing Li,De-Xi Chen,Hui-Guo Ding.Antiviral drug resistance increases hepatocellular carcinoma:A prospective decompensated cirrhosis cohort study[J].World Journal of Gastroenterology,2013,19(45):8373-8381. 被引量：20
2John Vlachogiannakos,George Papatheodoridis.Hepatocellular carcinoma in chronic hepatitis B patients under antiviral therapy[J].World Journal of Gastroenterology,2013,19(47):8822-8830. 被引量：10
3Zhong-Ming Tan,Bei-Cheng Sun.Effects of antiviral therapy on preventing liver tumorigenesis and hepatocellular carcinoma recurrence[J].World Journal of Gastroenterology,2013,19(47):8895-8901. 被引量：22
4Jia-Hong Yang,Hao Zhang,Xue-Bing Chen,Gao Chen,Xiu Wang.Relationship between hepatocellular carcinoma and hepatitis B virus genotype with spontaneous YMDD mutations[J].World Journal of Gastroenterology,2013,19(24):3861-3865. 被引量：13
5Hiroshi Matsumura,Kazushige Nirei,Hitomi Nakamura,Teruhisa Higuchi,Yasuo Arakawa,Masahiro Ogawa,Naohide Tanaka,Mitsuhiko Moriyama.Histopathology of type C liver disease for determining hepatocellular carcinoma risk factors[J].World Journal of Gastroenterology,2013,19(30):4887-4896. 被引量：3
6李健,马军.消化道肿瘤与微生物感染[J].胃肠病学和肝病学杂志,2013,22(2):109-115. 被引量：4
7许秀华,向晓星,龙爱华,刘丹,王劲松.原发性肝癌合并与不合并肝硬化患者年龄及乙型肝炎病毒血清学特点比较[J].临床肝胆病杂志,2013,29(3):214-216. 被引量：3
8陆盈.单项乙型肝炎病毒核心抗体阳性的原因及其临床意义[J].海南医学,2013,24(11):1636-1638. 被引量：6
9连芳,黄超源,邬国斌.乙型肝炎病毒PreS/S基因真核表达质粒的构建[J].中国实用医药,2013,8(17):1-2.
10魏飞力,石英,李庆,柳雅立,陈杰,陈德喜,吴昊.肝细胞癌患者肝癌组织中乙型肝炎病毒核心启动子变异分析[J].中国病毒病杂志,2013,3(4):264-267. 被引量：1

同被引文献13

1Teresa Antonia Santantonio,Massimo Fasano.Chronic hepatitis B: Advances in treatment[J].World Journal of Hepatology,2014,6(5):284-292. 被引量：12
2Francisco Rodriguez-Frias,Maria Buti,David Tabernero,Maria Homs.Quasispecies structure,cornerstone of hepatitis B virus infection: Mass sequencing approach[J].World Journal of Gastroenterology,2013,19(41):6995-7023. 被引量：11
3王红,黄岚,宋耀明,耿昭华,于学军,晋军,覃军,赵刚,高云华,刘政,杨丽,夏红梅.采用定性定量经冠脉超声心肌声学造影对非闭塞性病变心肌灌注水平的探讨[J].第三军医大学学报,2005,27(21):2180-2183. 被引量：1
4胡晓丽,赵宏伟,吴晓岩,牛俊奇.乙型肝炎病毒感染的流行现状[J].临床肝胆病杂志,2012,28(6):413-416. 被引量：69
5邓鹏,龚小卫,姜勇.在活细胞上研究核定位信号介导核移位的方法[J].南方医科大学学报,2012,32(8):1148-1150. 被引量：1
6陈金玲,邓倾,郭瑞强,周青,曹省,胡波,宋宏宁.NF-κB核定位基序促进SDF-1α质粒转染的入核效率[J].武汉大学学报（医学版）,2013,34(6):858-861. 被引量：2
7中华医学会传染病与,寄生虫病学分会,肝病学分会.病毒性肝炎防治方案[J].中华肝脏病杂志,2000,8(6):324-329. 被引量：14005
8丁尚伟,张艳容,吴文谦,任萍萍,黄晓宇,张培歌,武彧,于艾嘉,谢明星,吕清.不同转染方式介导基因转染效果的评价[J].中华超声影像学杂志,2014,23(4):349-352. 被引量：4
9Cheng Sun,Haoyu Sun,Cai Zhang,Zhigang Tian.NK cell receptor imbalance and NK cell dysfunction in HBV nfection and hepatocellular carcinoma[J].Cellular & Molecular Immunology,2015,12(3):292-302. 被引量：56
10Scott Bowden,Stephen Locarnini,Ting-Tsung Chang,You-Chen Chao,Kwang-Hyub Han,Robert G Gish,Robert A de Man,Miao Yu,Cyril Llamoso,Hong Tang.Covalently closed-circular hepatitis B virus DNA reduction with entecavir or lamivudine[J].World Journal of Gastroenterology,2015,21(15):4644-4651. 被引量：13

引证文献8

1王立志,肖作汉,汪燕,王运东,孙文锦.慢性乙型肝炎患者外周血单个核细胞Toll样受体9及其下游信号分子的表达水平及临床意义[J].中国实用医刊,2015,42(1):4-6. 被引量：2
2李强,卓其斌,黄玉仙,陈良.靶向HBV共价闭合环状DNA的治疗策略[J].临床肝胆病杂志,2015,31(9):1520-1523. 被引量：1
3杨松,段雪飞,范小玲,成军.针对共价闭合环状DNA的抗HBV治疗进展[J].中国肝脏病杂志（电子版）,2015,7(4):19-21. 被引量：1
4曹省,周青,陈金玲,邓倾,胡波,郭瑞强.利用核定位信号提高非病毒基因载体转化效率的研究进展[J].武汉大学学报（医学版）,2016,37(5):855-860.
5曹省,周青,王益佳,姜楠,胡波,郭瑞强.超声靶向微泡破坏联合经典核定位信号肽促进基因转染的实验研究[J].中华超声影像学杂志,2016,25(9):808-813. 被引量：1
6李强,卓其斌,黄玉仙,陈良.抗乙型肝炎病毒新靶点及相关药物研究进展[J].中华临床感染病杂志,2016,9(4):379-384. 被引量：2
7崔晶晶,周青,曹省,邓倾,胡波,王益佳.超声靶向破坏微泡联合核定位信号肽增强基因转染治疗犬心肌梗死的实验研究[J].中华超声影像学杂志,2017,26(2):159-164. 被引量：2
8魏粉菊,马悦,俞霁,贾海永,刘新泳,展鹏.基于新靶标的HBV抑制剂研究进展(2):RNase H及其他靶标[J].药学学报,2020,55(4):566-574. 被引量：8

二级引证文献17

1张欣.慢性乙型肝炎患者血浆D-二聚体与肝功能指标TP、Alb、Glo水平的相关性分析[J].中国当代医药,2016,23(12):131-133.
2孙杨,骆洁丽,陈建设,黄品同.低频聚焦超声联合微泡治疗兔VX2原位肝癌移植瘤的疗效评价[J].中华超声影像学杂志,2017,26(6):535-540. 被引量：1
3刘星晨,谷守芹,董金皋.CRISPR/Cas9介导的基因组定点编辑技术在丝状真菌中的研究进展[J].微生物学报,2017,57(11):1634-1642. 被引量：1
4谭洋,谢晓燕,王伟,郭焕玲,黄通毅,郑巧,徐明,吕明德.载索拉非尼-阿霉素智能控释纳米液滴制备及其超声响应性的实验研究[J].中华超声影像学杂志,2017,26(10):906-910.
5章晓莉,贾红宇,蔡欢,杨益大.提高慢性乙型肝炎功能性治愈率的新方法和新策略[J].中华临床感染病杂志,2018,11(4):254-260. 被引量：1
6刘娜,葛军,沈思岚,许燕妮,张小勇,刘红艳.干扰素α调控乙型肝炎病毒特异性T细胞免疫应答抑制慢性感染小鼠模型体内病毒基因表达[J].中国感染与化疗杂志,2018,18(2):177-183. 被引量：11
7盛常睿,陈赛君,严利明,胡晶晶,洪芳芳,贲志飞.注射用六氟化硫微泡造影剂剂量与机械指数对孕鼠胎盘超声造影成像的影响[J].中华妇幼临床医学杂志（电子版）,2020,16(3):329-334. 被引量：1
8相佳瑶,许敏,冯阳.抗HBV天然化合物作用机制的研究进展[J].中国药理学通报,2021,37(10):1346-1351. 被引量：3
9张莹,侯凌欣,鞠翰,刘新泳,展鹏.以聚合酶为靶标的抗病毒药物研究进展[J].中国药物化学杂志,2021,31(9):657-679. 被引量：3
10张续杰,徐淑静,孙林,刘新泳,展鹏.以衣壳蛋白为靶标的抗病毒药物研究进展[J].中国药物化学杂志,2021,31(9):705-720. 被引量：1

1王维力.Hashimotos—Riedel氏甲状腺炎并甲状腺癌甲状腺功能亢进1例报告[J].汕头大学医学院学报,1992(1):132-132.
2YANG Zhen,TIAN Lei,PENG Lin,QIU Fazu(Department of Surgery, Tongji Hospital, Tongji Medical University Wuhan 430030).Immunohistochemical　Analysis　of　Growth　Factor　Expression　and　Localization　in　Gastric　Coronary　Vein　of　Cirrhotic　Patients[J].Journal of Huazhong University of Science and Technology(Medical Sciences),1996,16(4):229-233. 被引量：9
3张道华,牛文堂,王克志.动脉导管未闭并发重度肺动脉高压的介入治疗[J].中国心血管病研究,2005,3(1):36-37. 被引量：7
4王健,冉丕鑫.肺动脉高压血管收缩与重塑的研究[J].中华结核和呼吸杂志,2007,30(9):645-648. 被引量：11
5王丽松,李娜.慢性肾衰竭、充血性心力衰竭与贫血三者之间的关系[J].心血管康复医学杂志,2007,16(3):285-287. 被引量：3
6张洋.Disruption of low-density lipoprotein receptor pathway induced by inflammation contributes to podocyte injury in diabetic nephropathy[J].China Medical Abstracts(Internal Medicine),2014,31(2):114-114.
7Yansheng,ZhengZhaoshuang.Analysis on the Epidemic Characterization and Trend of AIDS in Fujian Province[J].Biomedical and Environmental Sciences,1999,12(2):156-157.
8华亮,李婉玲,蔡燕娜,邝璐,韩宁,朱冰.广州地区疑诊地中海贫血患儿α-地中海贫血基因突变型研究[J].中国小儿血液与肿瘤杂志,2010,15(5):212-214. 被引量：6
9郑德武.三普心脑欣治疗冠心病169例临床研究[J].美国中华健康卫生杂志,2004,7(4):16-19.
10WANG Fu-xiang,ZHOU Hui,LING Hong,ZHOU Hai-zhou,LIU Wei-hua,SHAO Yi-ming,ZHOU Jin.Subtype and sequence analysis of HIV-1 strains in Heilongjiang Province[J].Chinese Medical Journal,2007(22):2006-2010. 被引量：3

World Journal of Gastroenterology

2013年第44期

浏览历史

内容加载中请稍等...