HDV RNA在細胞核與細胞質中的複製動態

劉思琳; Si-Lin Liu

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/99967

完整後設資料紀錄

DC 欄位	值	語言
dc.contributor.advisor	陳培哲	zh_TW
dc.contributor.advisor	Pei-Jer Chen	en
dc.contributor.author	劉思琳	zh_TW
dc.contributor.author	Si-Lin Liu	en
dc.date.accessioned	2025-09-22T16:10:31Z	-
dc.date.available	2025-09-23	-
dc.date.copyright	2025-09-22	-
dc.date.issued	2025	-
dc.date.submitted	2025-08-08	-
dc.identifier.citation	1.Rizzetto, M., et al., Immunofluorescence detection of new antigen-antibody system (delta/anti-delta) associated to hepatitis B virus in liver and in serum of HBsAg carriers. Gut, 1977. 18(12): p. 997-1003. 2.Sellier, P.O., et al., Hepatitis B Virus-Hepatitis D Virus mother-to-child co-transmission: A retrospective study in a developed country. Liver Int, 2018. 38(4): p. 611-618. 3.Wu, J.C., et al., Evidence of transmission of hepatitis D virus to spouses from sequence analysis of the viral genome. Hepatology, 1995. 22(6): p. 1656-60. 4.Lettau, L.A., et al., Outbreak of severe hepatitis due to delta and hepatitis B viruses in parenteral drug abusers and their contacts. N Engl J Med, 1987. 317(20): p. 1256-62. 5.Stockdale, A.J., et al., The global prevalence of hepatitis D virus infection: Systematic review and meta-analysis. Journal of Hepatology, 2020. 73(3): p. 523-532. 6.Botelho-Souza, L.F., et al., Hepatitis delta: virological and clinical aspects. Virol J, 2017. 14(1): p. 177. 7.Pan, C., et al., Diagnosis and Management of Hepatitis Delta Virus Infection. Digestive Diseases and Sciences 2023. 68: p. 3237-3248. 8.Kuhn, J.H., et al., ICTV Virus Taxonomy Profile: Kolmioviridae 2024. J Gen Virol, 2024. 105(2). 9.Wang, K.S., et al., Structure, sequence and expression of the hepatitis delta (delta) viral genome. Nature, 1986. 323(6088): p. 508-14. 10.Chen, P.J., et al., Structure and replication of the genome of the hepatitis delta virus. Proc Natl Acad Sci U S A, 1986. 83(22): p. 8774-8. 11.Sharmeen, L., et al., Antigenomic RNA of human hepatitis delta virus can undergo self-cleavage. J Virol, 1988. 62(8): p. 2674-9. 12.KUO, M.Y.-P., et al., Characterization of self-cleaving RNA sequences on the genome and antigenome of human hepatitis delta virus. Journal of virology, 1988. 62(12): p. 4439-4444. 13.Gudima, S., et al., Origin of hepatitis delta virus mRNA. J Virol, 2000. 74(16): p. 7204-10. 14.Hsieh, S.Y., et al., Hepatitis delta virus genome replication: a polyadenylated mRNA for delta antigen. J Virol, 1990. 64(7): p. 3192-8. 15.Weiner, A.J., et al., A single antigenomic open reading frame of the hepatitis delta virus encodes the epitope(s) of both hepatitis delta antigen polypeptides p24 delta and p27 delta. J Virol, 1988. 62(2): p. 594-9. 16.Chou, H.C., et al., Hepatitis delta antigen mediates the nuclear import of hepatitis delta virus RNA. J Virol, 1998. 72(5): p. 3684-90. 17.Chang, J., et al., Transcription of hepatitis delta virus RNA by RNA polymerase II. J Virol, 2008. 82(3): p. 1118-27. 18.Branch, A.D. and H.D. Robertson, A replication cycle for viroids and other small infectious RNA's. Science, 1984. 223(4635): p. 450-5. 19.Lai, M.M., The molecular biology of hepatitis delta virus. Annu Rev Biochem, 1995. 64: p. 259-86. 20.Casey, J.L., RNA editing in hepatitis delta virus. Curr Top Microbiol Immunol, 2006. 307: p. 67-89. 21.Chao, M., S.Y. Hsieh, and J. Taylor, Role of two forms of hepatitis delta virus antigen: evidence for a mechanism of self-limiting genome replication. J Virol, 1990. 64(10): p. 5066-9. 22.Chang, F.L., et al., The large form of hepatitis delta antigen is crucial for assembly of hepatitis delta virus. Proc Natl Acad Sci U S A, 1991. 88(19): p. 8490-4. 23.Ryu, W.S., M. Bayer, and J. Taylor, Assembly of hepatitis delta virus particles. J Virol, 1992. 66(4): p. 2310-5. 24.Strauss, J.H. and E.G. Strauss, Minus-Strand RNA Viruses. Viruses and Human Disease, 2008: p. 137-91. 25.Wang, M., et al., Developments in Negative-Strand RNA Virus Reverse Genetics. Microorganisms, 2024. 12(3). 26.Ouizougun-Oubari, M. and R. Fearns, Structures and Mechanisms of Nonsegmented, Negative-Strand RNA Virus Polymerases. Annu Rev Virol, 2023. 10(1): p. 199-215. 27.Pacchioni, D., et al., Detection of hepatitis delta virus RNA by a nonradioactive in situ hybridization procedure. Hum Pathol, 1992. 23(5): p. 557-61. 28.Cunha, C., et al., Localization of hepatitis delta virus RNA in the nucleus of human cells. RNA, 1998. 4(6): p. 680-93. 29.Macnaughton, T.B. and M.M. Lai, Genomic but not antigenomic hepatitis delta virus RNA is preferentially exported from the nucleus immediately after synthesis and processing. J Virol, 2002. 76(8): p. 3928-35. 30.Gudima, S., et al., Assembly of Hepatitis Delta Virus: Particle Characterization, Including the Ability To Infect Primary Human Hepatocytes. JOURNAL OF VIROLOGY, 2007. 81(7): p. 3608–3617. 31.Wettengel, J.M., et al., Rapid and Robust Continuous Purification of High-Titer Hepatitis B Virus for In Vitro and In Vivo Applications. Viruses, 2021. 13(8). 32.Zahn, A. and J.-P. Allain, Hepatitis C virus and hepatitis B virus bind to heparin: purification of largely IgG-free virions from infected plasma by heparin chromatography. Journal of General Virology, 2005. 86: p. 677-685. 33.Stieger, B., et al., In situ localization of the hepatocytic Na+/Taurocholate cotransporting polypeptide in rat liver. Gastroenterology, 1994. 107(6): p. 1781-7. 34.Matsui, T., et al., Multiple factors required for accurate initiation of transcription by purified RNA polymerase II. J Biol Chem, 1980. 255(24): p. 11992-6.	-
dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/99967	-
dc.description.abstract	丁型肝炎病毒(Hepatitis delta virus, HDV)是一種需要乙型肝炎病毒(Hepatitis B virus, HBV)提供包膜蛋白的負股RNA病毒。由於HDV本身不具備病毒專屬的聚合酶，因此其基因體複製需依賴宿主細胞的RNA聚合酶。與其他負股RNA病毒相似，HDV必須先將其基因體轉錄為messenger RNA (mRNA)，才能產生病毒蛋白；但不同於典型的負股RNA病毒，HDV並不攜帶自身的RNA依賴性RNA聚合酶(RNA dependent RNA polymerase)，而是利用宿主的聚合酶進行轉錄與複製。雖然HDV一般被認為是在細胞核中進行複製，然而也有部分研究指出其複製中間產物反基因體RNA也會在細胞質中出現，然而，HDV是否能在細胞質中複製，目前尚未被充分研究。本研究旨在探討HDV是否可於細胞質中進行複製，以及其是否可能包裹宿主聚合酶以協助此一過程。透過HDV感染的Huh7-NTCP細胞進行核質分離，結果發現HDV的基因體與反基因體RNA，以及丁型肝炎抗原(HDAg)皆可在細胞質與細胞核中被偵測，顯示HDV在細胞質中可能具備複製能力。為了進一步驗證此假說，我們純化HDV病毒顆粒並進行等密度梯度離心。雖然質譜分析(LC-MS/MS)未能確認RNA polymerase II subunit RPB1與HDV病毒顆粒的結合，但Western blot與Northern blot分析顯示病毒成分與RPB1出現在相同分離層，暗示RPB1可能與HDV存在某種關聯。然而，類似的共分布現象也出現在HBV病毒顆粒與次病毒顆粒中，顯示此種關聯可能僅為非特異性結合。此外，使用抗HBsAg抗體進行的免疫沉澱實驗未能成功拉下病毒蛋白，因此無法進一步證實病毒顆粒與RPB1之間的關聯。綜上所述，HDV病毒顆粒可能與宿主聚合酶存在關聯，但其特異性及生物學意義仍需更深入探討。	zh_TW
dc.description.abstract	Hepatitis delta virus (HDV) is a negative-strand RNA virus that relies on hepatitis B virus (HBV) for envelope proteins supply. Since HDV lacks its own polymerase, it utilizes the host RNA polymerase for genome replication. Like other negative-strand RNA viruses, HDV must transcribe its genome into messenger RNA (mRNA) to produce viral proteins. However, unlike typical RNA viruses, it uses host polymerases instead of encoding its own. Although HDV is generally considered to replicate in the nucleus, some evidence suggests that its replication intermediate—antigenomic RNA—may also be present in the cytoplasm. However, this aspect of HDV replication has not been thoroughly explored. In this study, we investigated whether HDV replicates in the cytoplasm and whether it encapsulates host polymerases to support this process. Through nuclear and cytoplasmic fractionation of HDV-infected Huh7-NTCP cells, we detected both genomic and antigenomic HDV RNAs, as well as hepatitis delta antigen (HDAg), in both the cytoplasmic and nuclear compartments. These findings suggest the possibility of cytoplasmic HDV replication. To further examine this hypothesis, HDV virions were purified and subjected to isopycnic density gradient centrifugation. Although LC MS/MS failed to confirm the association between RNA polymerase II subunit RPB1 and virions, Western blot and Northern blot analyses revealed that viral components co-fractionated with RNA polymerase II subunit RPB1. This raised the hypothesis that HDV virions may encapsulate host polymerase. However, similar co-localization patterns were also observed in HBV virions and subviral particles, suggesting the possibility of non-specific association. Moreover, immunoprecipitation assays using an anti-HBsAg antibody failed to pull down viral proteins, leaving the association between virions and RNA polymerase II-RPB1 unconfirmed. Together, these results provide biochemical evidence suggesting a potential association between HDV virions and host polymerase, though further studies are needed to determine the specificity and functional relevance of this interaction.	en
dc.description.provenance	Submitted by admin ntu (admin@lib.ntu.edu.tw) on 2025-09-22T16:10:31Z No. of bitstreams: 0	en
dc.description.provenance	Made available in DSpace on 2025-09-22T16:10:31Z (GMT). No. of bitstreams: 0	en
dc.description.tableofcontents	致謝 i 摘要 ii Abstract iii Chapter I: Introduction 1 1.1 Introduction of hepatitis delta virus (HDV) 1 1.1.1 Epidemiology 1 1.1.2 Virology 2 1.1.3 Life cycle 3 1.2 Negative-strand RNA virus 4 1.3 HDV replication site 5 1.4 Hypothesis 6 1.5 Aims 6 Chapter II: Material and methods 7 2.1 Cell culture 7 2.2 Virus preparation and quantification 7 2.2.1 Viral production 7 2.2.2 Sucrose cushion 8 2.2.3 Heparin Affinity Chromatography-Based Purification of HDV Virions 8 2.2.4 Isopycnic ultracentrifugation (OptiprepTM / Iodixanol) 9 2.3 HDV infection 10 2.4 Nuclear and cytoplasmic fractionation 11 2.5 Immunoprecipitation of HDV virions 11 2.6 Liquid Chromatography - Tandem Mass Spectrometry (LC-MS/MS) 12 2.7 Molecular Analysis 14 2.7.1 Protein Quantification 14 2.7.2 Western blot analysis 14 2.7.3 RNA collection 15 2.7.4 Probe preparation 16 2.7.5 Standard RNA preparation 17 2.7.6 Northern blot analysis 17 Chapter III: Results 19 3.1 Production of HDV particles via DNA transfection in Huh7 cells 19 3.2 Dynamics of HDAg and HDV RNA expression in Huh7-NTCP cells during early infection 20 3.3 Some RNA polymerase subunits were detected while there was no viral proteins 21 3.4 Density gradient analysis of HDV virions suggests association with RNA Polymerase II-RPB1 21 3.5 Density gradient analysis of HBV virions and subviral particles suggests association with RNA Polymerase II-RPB1 22 3.6 The association between RNA polymerase II subunit RPB1 and viral particles could not be determined based on the immunoprecipitation results. 23 Chapter IV: Conclusion and Discussion 25 Chapter V: Figures 28 References 41	-
dc.language.iso	en	-
dc.subject	丁型肝炎病毒	zh_TW
dc.subject	負鏈RNA病毒	zh_TW
dc.subject	細胞質複製	zh_TW
dc.subject	病毒純化	zh_TW
dc.subject	viral purification	en
dc.subject	Hepatitis delta virus	en
dc.subject	negative-strand RNA virus	en
dc.subject	cytoplasmic replication	en
dc.title	HDV RNA在細胞核與細胞質中的複製動態	zh_TW
dc.title	Nuclear and cytoplasmic dynamics of HDV RNA replication	en
dc.type	Thesis	-
dc.date.schoolyear	113-2	-
dc.description.degree	碩士	-
dc.contributor.oralexamcommittee	趙玫;陳宏達	zh_TW
dc.contributor.oralexamcommittee	Mei Chao;Hung-Ta Chen	en
dc.subject.keyword	丁型肝炎病毒,負鏈RNA病毒,細胞質複製,病毒純化,	zh_TW
dc.subject.keyword	Hepatitis delta virus,negative-strand RNA virus,cytoplasmic replication,viral purification,	en
dc.relation.page	43	-
dc.identifier.doi	10.6342/NTU202504339	-
dc.rights.note	同意授權(限校園內公開)	-
dc.date.accepted	2025-08-11	-
dc.contributor.author-college	醫學院	-
dc.contributor.author-dept	微生物學研究所	-
dc.date.embargo-lift	2027-08-08	-
顯示於系所單位：	微生物學科所

文件中的檔案：

檔案	大小	格式
ntu-113-2.pdf 未授權公開取用	1.16 MB	Adobe PDF	檢視/開啟

顯示文件簡單紀錄

系統中的文件，除了特別指名其著作權條款之外，均受到著作權保護，並且保留所有的權利。