Your search keyword '"hepatitis B virus replication"' showing total 27 results

1. Study on the role of histone epigenetic modification in replication of hepatitis B virus.

Author

Wei, Fenfen and Meng, Die

Subjects

*HEPATITIS B virus, *NUCLEAR factor of activated T-cells, *ANIMAL rescue, *HEPATITIS associated antigen, *WESTERN immunoblotting, *EPIGENETICS, *HISTONE deacetylase

Abstract

Hepatitis B virus (HBV) infection is a global health problem and lacks effective therapies in clinic. This study attempted to investigate the role of histone deacetylase 3 (HDAC3) in HBV replication. Cells were treated with 1.3 folds of HBV genome. The expression patterns of HDAC3, miR-29a-3p, and nuclear factor of activated T-cells 5 (NFAT5) in cells were determined by real-time quantitative polymerase chain reaction and Western blot analysis. HBV replication was assessed by measurements of HBV DNA, HBV RNA, hepatitis B surface antigen, and hepatitis B E antigen. After chromatin immunoprecipitation and RNA pull-down assays to testify gene interactions, rescue experiments and animal experiments were performed to assess the role of miR-29a-3p/NFAT5 in HBV replication and the role of HDAC3 in vivo. HDAC3 level was decreased by pHBV1.3 plasmid in a concentration-dependent manner. HDAC3 overexpression can inhibit HBV replication, which was neutralized by miR-29a-3p overexpression or NFAT5 downregulation. Mechanically, HDAC3 overexpression reduced the enrichment of histone 3 lysine 9 acetylation on the miR-29a-3p promoter to inhibit miR-29a-3p expression and then promote NFAT5 transcription. In vivo , HDAC3 restrained HBV replication through the miR-29a-3p/NFAT5 axis. Overall, HDAC3 downregulation was associated with HBV replication and HDAC3 overexpression inhibited HBV replication through H3K9ac/miR-29a-3p/NFAT5. • HDAC3 is decreased in HBV replication. • HDAC3 overexpression inhibits HBV replication. • HDAC3 inhibits miR-29a-3p by reducing H3K9ac enrichment on the promoter. • NFAT5 is a downstream target gene of miR-29a-3p. • HDAC3 attenuates HBV replication via the miR-29a-3p/NFAT5 axis. [ABSTRACT FROM AUTHOR]

Published

2023

2. Occult Hepatitis B Infection

Author

Yuen, Man-Fung, Kao, Jia-Horng, editor, and Chen, Ding-Shinn, editor

Published

2018

3. Cisplatin induces autophagy to enhance hepatitis B virus replication via activation of ROS/JNK and inhibition of the Akt/mTOR pathway.

Author

Chen, Xuemei, Hu, Yuan, Zhang, Wenlu, Chen, Ke, Hu, Jie, Li, Xiaosong, Liang, Li, Cai, Xuefei, Hu, Jieli, Wang, Kai, Huang, Ailong, and Tang, Ni

Subjects

*HEPATITIS B virus, *VIRAL replication, *CISPLATIN, *MICROTUBULE-associated proteins, *MTOR protein

Abstract

Abstract Chronic hepatitis B virus (HBV) infection remains a serious global health concern. Cisplatin is a chemotherapeutic agent commonly used to treat various cancers. However, HBV-infected patients receiving chemotherapy are at risk of HBV reactivation via unknown mechanisms, which we aimed to elucidate in this study. We found that autophagy plays a central role in cisplatin-induced HBV replication. Cisplatin treatment induced autophagy in both HBV-replicating cells and an HBV-transgenic mouse model as evident from marked upregulation of microtubule-associated protein 1 light chain 3 (LC3)-II and the accumulation of red fluorescent protein (RFP)-LC3 puncta. Cisplatin induced complete autophagic flux, which was detected via monitoring of p62 degradation and RFP-GFP-LC3 expression. Inhibition of autophagy by chloroquine, 3-methyladenine, or Atg5 knockdown significantly attenuated cisplatin-induced HBV replication. Additionally, cisplatin-induced autophagy could be significantly attenuated by using the ROS scavenger N-acetyl- l -cysteine. Mechanically, cisplatin promoted HBV replication and autophagy through ROS/JNK and AKT/mTOR signaling. Inhibition of JNK or activation of Akt/mTOR signaling reversed cisplatin-mediated autophagy and HBV replication promotion. In contrast, suppression of Akt/mTOR signaling further promoted cisplatin-induced HBV replication. Finally, pharmacotherapeutic inhibition of autophagy or ROS production impaired HBV production induced by cisplatin in vivo. Together, our results indicate that ROS/JNK and mTOR/AKT-mediated autophagy plays an important role in cisplatin-induced HBV reactivation. Graphical abstract fx1 Highlights • Cisplatin stimulates HBV replication in vitro and in vivo. • Cisplatin induces autophagy to enhance hepatitis B virus replication. • Inhibition of autophagy or ROS/JNK axis rendered cisplatin-induced HBV biosynthesis. • Cisplatin promotes HBV replication and autophagy by ROS/JNK and AKT/mTOR pathway. [ABSTRACT FROM AUTHOR]

Published

2019

4. Identification of TRIM14 as a Type I IFN-Stimulated Gene Controlling Hepatitis B Virus Replication by Targeting HBx

Author

Guangyun Tan, Fengchao Xu, Hongxiao Song, Ye Yuan, Qingfei Xiao, Feng Ma, F. Xiao-Feng Qin, and Genhong Cheng

Subjects

type I IFN, STAT1, TRIM14, hepatitis B virus X protein, hepatitis B virus replication, Immunologic diseases. Allergy, RC581-607

Abstract

Hepatitis B virus (HBV) remains a major cause of hepatic disease that threatens human health worldwide. Type I IFN (IFN-I) therapy is an important therapeutic option for HBV patients. The antiviral effect of IFN is mainly mediated via upregulation of the expressions of the downstream IFN-stimulated genes. However, the mechanisms by which IFN induces ISG production and inhibits HBV replication are yet to be clarified. TRIM14 was recently reported as a key molecule in the IFN-signaling pathway that regulates IFN production in response to viral infection. In this study, we sought to understand the mechanisms by which IFN restricts HBV replication. We confirmed that TRIM14 is an ISG in the hepatic cells, and that the pattern-recognition receptor ligands polyI:C and polydAdT induce TRIM14 dependent on IFN-I production. In addition, IFN-I-activated STAT1 (but not STAT3) directly bound to the TRIM14 promoter and mediated the induction of TRIM14. Interestingly, TRIM14 played an important role in IFN-I-mediated inhibition of HBV, and the TRIM14 SPRY domain interacted with the C-terminal of HBx, which might block the role of HBx in facilitating HBV replication by inhibiting the formation of the Smc-HBx–DDB1 complex. Thus, our study clearly demonstrates that TRIM14 is a STAT1-dependent ISG, and that the IFN-I–TRIM14–HBx axis shows an alternative way to understand the mechanism by which IFN-I inhibits virus replication.

Published

2018

5. Negative regulation of hepatitis B virus replication by forkhead box protein A in human hepatoma cells.

Author

Okumura, Nobuaki, Ikeda, Masanori, Satoh, Shinya, Dansako, Hiromichi, Sugiyama, Masaya, Mizokami, Masashi, and Kato, Nobuyuki

Subjects

*HEPATITIS B virus, *FORKHEAD transcription factors, *HEPATOCELLULAR carcinoma, *NUCLEAR receptors (Biochemistry), *DNA replication

Abstract

Hepatitis B virus (HBV) replication is controlled by liver-enriched transcriptional factors, including forkhead box protein A (FOXA) members. Here, we found that FOXA members are directly and indirectly involved in HBV replication in human hepatic cells. HBV replication was elevated in HuH-7 treated with individual FOXA members-specific siRNA. Reciprocally, the downregulation of HBV replication was observed in FOXA-induced HuH-7. However, the mechanism of downregulation is different among FOXA members at the level of HBV RNA transcription, such as precore/pg RNA and 2.1 kb RNA. In addition, FOXA1 and FOXA2 suppressed nuclear hormone receptors, such as HNF4α, that are related to HBV replication. [ABSTRACT FROM AUTHOR]

Published

2015

6. Hepatocystin/80K-H inhibits replication of hepatitis B virus through interaction with HBx protein in hepatoma cell.

Author

Shin, Gu-Choul, Ahn, Sung Hyun, Choi, Hyo-Sun, Lim, Keo-Heun, Choi, Do Young, Kim, Kwang Pyo, and Kim, Kyun-Hwan

Subjects

*HEPATITIS B virus, *HEPATOCELLULAR carcinoma, *VIRAL proteins, *LIVER cancer, *IMMUNOCYTOCHEMISTRY, *WESTERN immunoblotting, *CYSTINE, *VIRAL replication

Abstract

Abstract: Hepatitis B virus (HBV) X protein (HBx) is a key player in HBV replication as well as HBV-induced hepatocellular carcinoma (HCC). However, the pathogenesis of HBV infection and the mechanisms of host–virus interactions are still elusive. In this study, a combination of affinity purification and mass spectrometry was applied to identify the host factors interacting with HBx in hepatoma cells. Thirteen proteins were identified as HBx binding partners. Among them, we first focused on determining the functional significance of the interaction between HBx and hepatocystin. A physical interaction between HBx and hepatocystin was confirmed by co-immunoprecipitation and Western blotting. Immunocytochemistry demonstrated that HBx and hepatocystin colocalized in the hepatoma cells. Domain mapping of both proteins revealed that the HBx C-terminus (amino acids 110–154) was responsible for binding to the mannose 6-phosphate receptor homology domain (amino acids, 419–525) of hepatocystin. Using translation and proteasome inhibitors, we found that hepatocystin overexpression accelerated HBx degradation via a ubiquitin-independent proteasome pathway. We demonstrated that this effect was mediated by an interaction between both proteins using a HBx deletion mutant. Hepatocystin overexpression significantly inhibited HBV DNA replication and expression of HBs antigen concomitant with HBx degradation. Using the hepatocystin mutant constructs that bind HBx, we also confirmed that hepatocystin inhibited HBx-dependent HBV replication. In conclusion, we demonstrated for the first time that hepatocystin functions as a chaperon-like molecule by accelerating HBx degradation, and thereby inhibits HBV replication. Our results suggest that inducing hepatocystin may provide a novel therapeutic approach to control HBV infection. [Copyright &y& Elsevier]

Published

2013

7. Adiponectin, a downstream target gene of peroxisome proliferator-activated receptor γ, controls hepatitis B virus replication

Author

Yoon, Sarah, Jung, Jaesung, Kim, Taeyeung, Park, Sun, Chwae, Yong-Joon, Shin, Ho-Joon, and Kim, Kyongmin

Subjects

*HEPATITIS B virus, *VIRAL replication, *CARRIER proteins, *ROSIGLITAZONE, *LAMIVUDINE, *NUCLEAR receptors (Biochemistry), *HEPATITIS B treatment, *GENE expression

Abstract

Abstract: In this study, HepG2-hepatitis B virus (HBV)-stable cells that did not overexpress HBx and HBx-deficient mutant-transfected cells were analyzed for their expression of HBV-induced, upregulated adipogenic and lipogenic genes. The mRNAs of CCAAT enhancer binding protein α (C/EBPα), peroxisome proliferator-activated receptor γ (PPARγ), adiponectin, liver X receptor α (LXRα), sterol regulatory element binding protein 1c (SREBP1c), and fatty acid synthase (FAS) were expressed at higher levels in HepG2–HBV and lamivudine-treated stable cells and HBx-deficient mutant-transfected cells than in the HepG2 cells. Lamivudine treatment reduced the mRNA levels of PPARγ and C/EBPα. Conversely, HBV replication was upregulated by adiponectin and PPARγ agonist rosiglitazone treatments and was downregulated by adiponectin siRNAs. Collectively, our results demonstrate that HBV replication and/or protein expression, even in the absence of HBx, upregulated adipogenic or lipogenic genes, and that the control of adiponectin might prove useful as a therapeutic modality for the treatment of chronic hepatitis B. [Copyright &y& Elsevier]

Published

2011

8. Modulation of hepatitis B virus replication by expression of polymerase-surface fusion protein through splicing: Implications for viral persistence

Author

Park, Gil-Soon, Kim, Hee-Young, Shin, Hyun-Soo, Park, Sun, Shin, Ho-Joon, and Kim, Kyongmin

Subjects

*HEPATITIS B, *HEPATITIS viruses, *POLYMERASE chain reaction, *BIOLOGICAL transport

Abstract

Abstract: In hepatitis B virus (HBV)-infected livers and -transfected hepatoma cells, spliced transcripts are not essential for HBV replication. However, their ability to modulate HBV replication has not been clearly elucidated. In the current study, we found that the polymerase-surface (PS) fusion protein, generated from a spliced HBV transcript, colocalized with the nuclear pore complex, vimentin, microtubules, and the endoplasmic reticulum (ER) in the perinuclear region of transfected cells. We found that PLC/PRF/5-hepatoma cells expressed PS transcript and PS protein. Hepatitis B surface antigen (HBs) secretion, core particle formation, and HBV DNA synthesis were inhibited by the expression of PS transcript and PS protein, and by expression of PS transcript alone, suggesting that HBV replication is modulated by splicing. Our results suggest that splicing may be one of the outcomes of the host–virus interaction. [Copyright &y& Elsevier]

Published

2008

9. Rac1 GTPase is activated by hepatitis B virus replication — involvement of HBX

Author

Tan, Tuan Lin, Fang, Ning, Neo, Tuan Ling, Singh, Pritpal, Zhang, Jianhua, Zhou, Ruijie, Koh, Cheng-Gee, Chan, Vincent, Lim, Seng Gee, and Chen, Wei Ning

Subjects

*LIVER diseases, *HEPATITIS B, *HEPATITIS viruses, *HEPATITIS B virus

Abstract

Abstract: Hepatitis B virus (HBV) is a causative agent for liver diseases including hepatocellular carcinoma. Understanding its interactions with cellular proteins is critical in the elucidation of the mechanisms of disease progression. Using a cell-based HBV replication system, we showed that HBV replication in HepG2 cells resulted in a cellular morphological changes displaying membrane rufflings and lamellipodia like structures reminiscent of cells expressing constitutively activated Rac1. We also showed that activated Rac1 resulted in increased viral replication. HBV replication specifically activated wild type Rac1, but not Cdc42. The Rac1 activation by HBV replication also resulted in the phosphorylation of ERK1/2 and AKT, the downstream targets of Rac1 signaling cascade. The smallest HBV viral protein, HBX, was able to activate the endogenous Rac1 and induce membrane ruffling when transfected into cells. Significantly, HBX was found to directly interact with a Rac1 nucleotide exchange factor (βPIX) through a SH3 binding motif. Taken together, we have shown the interaction of HBV with the Rho GTPase, affecting cell morphology through the Rac1 activation pathway. HBV may possibly make use of an activated Rac1 signaling pathway for increased replication and resultant metastatic effects. [Copyright &y& Elsevier]

Published

2008

10. Future therapy for hepatitis B.

Author

Rustgi, Vinod K. and Koff, Raymond S.

Subjects

THERAPEUTICS, HEPATITIS B virus, VIRAL replication, IMMUNOREGULATION, INTERFERONS, NUCLEOSIDES, NUCLEOTIDES

Abstract

Therapy for hepatitis B virus (HBV) infection, the most common worldwide cause of viremia and chronic liver disease, is currently limited to interferon preparations and nucleoside or nucleotide analogs. Although these treatments result in suppression of HBV replication, virologic rebounds are common when treatment is ended or when viral resistance emerges. This review considers novel approaches targeting viral or host factors involved in the HBV lifecycle, as well as immunomodulatory strategies that are likely to be used concomitantly with antiviral drugs in future research. [ABSTRACT FROM AUTHOR]

Published

2007

11. Complementation analysis of mutants defective in different steps of HBV reverse transcription.

Author

Schaller, Heinz and Radziwill, Gerald

Abstract

The HBV P gene encodes a multifuctional polyprotein which contains the major enzymatic activities required for hepadnaviral reverse transcription (protein primer, DNA polymerase, and RNase H). Mutant HBV genomes unable to synthesize fully functional P gene products were analysed for their potential to be rescued by a second mutant HBV genome that either contained a wild type P gene (intergenic complementation) or a mutation in a functionally different P gene domain (intragenic complementation). This analysis was carried out by cotransfecting two mutants at a time into HepG2 cells and assaying for the production of core particles containing DNA polymerase activity. The results obtained demonstrate the existence of intergenic, but not of intragenic complementation. This indicates that the primary P gene product is not processed before core assembly, and furthermore that there is a rather free mixing of all HBV gene products in the HBV infected cell which can lead to the efficient propagation of defective viral genomes. [ABSTRACT FROM AUTHOR]

Published

1990

12. The novel HBx mutation F30V correlates with hepatocellular carcinoma in vivo, reduces hepatitis B virus replicative efficiency and enhances anti-apoptotic activity of HBx N terminus in vitro

Author

Francesca Ceccherini-Silberstein, Rossana Scutari, Massimo Andreoni, Mario Angelico, Carmen Mirabelli, Massimo Levrero, Laura Belloni, Maria Francesca Cortese, Loredana Sarmati, Gabriele Missale, Caterina Pasquazzi, Valentina Svicher, J. Vecchiet, Simona Francioso, G.A. Palumbo, Matteo Surdo, A. Sacco, Hervé Fleury, Pascale Trimoulet, Carlo Federico Perno, L. Carioti, Mohammad Alkhatib, Alberto Spanò, Giuseppina Cappiello, and Romina Salpini

Subjects

0301 basic medicine, Microbiology (medical), Adult, Male, apoptosis, hbx, hepatitis b, hepatitis b virus replication, hepatocellular carcinoma, Hepatitis B virus, Carcinoma, Hepatocellular, Genotype, 030106 microbiology, Apoptosis, Biology, medicine.disease_cause, Virus Replication, 03 medical and health sciences, 0302 clinical medicine, Hepatitis B, Chronic, medicine, Humans, Viral Regulatory and Accessory Proteins, 030212 general & internal medicine, Aged, Mutation, Liver Neoplasms, General Medicine, cccDNA, Hep G2 Cells, Hepatitis B, Middle Aged, Settore MED/07 - Microbiologia e Microbiologia Clinica, medicine.disease, digestive system diseases, HBx, Infectious Diseases, Liver, Structural Homology, Protein, Hepatocellular carcinoma, DNA, Viral, Cancer research, Trans-Activators, Female

Abstract

We aimed to investigate HBx genetic elements correlated with hepatitis B virus (HBV) -related hepatocellular carcinoma (HCC) and their impact on (a) HBV replicative efficiency, (b) HBx binding to circular covalently closed DNA (cccDNA), (c) apoptosis and cell-cycle progression, and (d) HBx structural stability.This study included 123 individuals chronically infected with HBV: 27 with HCC (77.9% (21/27) genotype D; 22.1% (6/27) genotype A) and 96 without HCC (75% (72/96) genotype D; 25.0% (24/96) genotype A). HepG2 cells were transfected by wild-type or mutated linear HBV genome to assess pre-genomic RNA (pgRNA) and core-associated HBV-DNA levels, HBx-binding onto cccDNA by chromatin immunoprecipitation-based quantitative assay, and rate of apoptosis and cell-cycle progression by cytofluorimetry.F30V was the only HBx mutation correlated with HCC (18.5% (5/27) in HCC patients versus 1.0% (1/96) in non-HCC patients, p 0.002); a result confirmed by multivariate analysis. In vitro, F30V determined a 40% and 60% reduction in pgRNA and core-associated HBV-DNA compared with wild-type (p0.05), in parallel with a significant decrease of HBx binding to cccDNA and decreased HBx stability. F30V also decreased the percentage of apoptotic cells compared with wild-type (14.8 ± 6.8% versus 19.1 ± 10.1%, p0.01, without affecting cell-cycle progression) and increased the probability of HBx-Ser-31 being phosphorylated by PI3K-Akt kinase (known to promote anti-apoptotic activity).F30V was closely correlated with HBV-induced HCC in vivo, reduced HBV replicative efficiency by affecting HBx-binding to cccDNA and increased anti-apoptotic HBx activity in vitro. This suggests that F30V (although hampering HBV's replicative capacity) may promote hepatocyte survival, so potentially allowing persistent production of viral progeny and initiating HBV-driven hepatocarcinogenesis. Investigation of viral genetic markers associated with HCC is crucial to identify those patients at higher risk of HCC, who hence deserve intensive liver monitoring and/or early anti-HBV therapy.

Published

2018

13. Negative regulation of hepatitis B virus replication by forkhead box protein A in human hepatoma cells

Author

Masashi Mizokami, Masaya Sugiyama, Hiromichi Dansako, Masanori Ikeda, Nobuyuki Kato, Nobuaki Okumura, and Shinya Satoh

Subjects

DNA Replication, Hepatocyte Nuclear Factor 3-alpha, Hepatitis B virus, Carcinoma, Hepatocellular, animal structures, Biophysics, Biology, Virus Replication, medicine.disease_cause, Biochemistry, Hepatitis B virus PRE beta, HNF3, Structural Biology, Transcription (biology), Cell Line, Tumor, Genetics, medicine, Humans, Molecular Biology, Liver Neoplasms, fungi, DNA replication, virus diseases, Cell Biology, Virology, Molecular biology, digestive system diseases, Neoplasm Proteins, Hepatocyte Nuclear Factor 4, Viral replication, FOXA3, DNA, Viral, embryonic structures, Hepatocyte Nuclear Factor 3-beta, Hepatitis B virus replication, FOXA2, FOXA1

Abstract

Hepatitis B virus (HBV) replication is controlled by liver-enriched transcriptional factors, including forkhead box protein A (FOXA) members. Here, we found that FOXA members are directly and indirectly involved in HBV replication in human hepatic cells. HBV replication was elevated in HuH-7 treated with individual FOXA members-specific siRNA. Reciprocally, the downregulation of HBV replication was observed in FOXA-induced HuH-7. However, the mechanism of downregulation is different among FOXA members at the level of HBV RNA transcription, such as precore/pg RNA and 2.1kb RNA. In addition, FOXA1 and FOXA2 suppressed nuclear hormone receptors, such as HNF4α, that are related to HBV replication.

Published

2015

14. miR-29a promotes hepatitis B virus replication and expression by targeting SMARCE1 in hepatoma carcinoma

Author

Ya Zhuo, Yan-Cai Zhou, Yan-Ping Wang, Xin-Wei Wang, Xin-Hong Wang, Hong-Jie Wu, and Chang-Yun Si

Subjects

0301 basic medicine, Hepatitis b e antigen, DNA Replication, Gene Expression Regulation, Viral, Hepatitis B virus, Carcinoma, Hepatocellular, Cell Survival, Chromosomal Proteins, Non-Histone, Blotting, Western, Enzyme-Linked Immunosorbent Assay, Biology, medicine.disease_cause, Hepatitis b surface antigen, Real-Time Polymerase Chain Reaction, Virus Replication, 03 medical and health sciences, Replication (statistics), medicine, Carcinoma, Humans, Hepatitis B e Antigens, Hepatitis B e antigen, Hepatitis B Surface Antigens, miR-29a, Liver Neoplasms, Gastroenterology, General Medicine, Hep G2 Cells, Basic Study, medicine.disease, Hepatitis B, Virology, SMARCE1, digestive system diseases, Up-Regulation, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, MicroRNAs, 030104 developmental biology, Hepatitis B surface antigen, DNA, Viral, Hepatitis B virus replication

Abstract

AIM To investigate the functional role and underlying molecular mechanism of miR-29a in hepatitis B virus (HBV) expression and replication. METHODS The levels of miR-29a and SMARCE1 in HBV-infected HepG2.2.15 cells were measured by quantitative real-time PCR and western blot analysis. HBV DNA replication was measured by quantitative PCR and Southern blot analysis. The relative levels of hepatitis B surface antigen and hepatitis B e antigen were detected by enzyme-linked immunosorbent assay. The Cell Counting Kit-8 (CCK-8) was used to detect the viability of HepG2.2.15 cells. The relationship between miR-29a and SMARCE1 were identified by target prediction and luciferase reporter analysis. RESULTS miR-29a promoted HBV replication and expression, while SMARCE1 repressed HBV replication and expression. Cell viability detection indicated that miR-29a transfection had no adverse effect on the host cells. Moreover, SMARCE1 was identified and validated to be a functional target of miR-29a. Furthermore, restored expression of SMARCE1 could relieve the increased HBV replication and expression caused by miR-29a overexpression. CONCLUSION miR-29a promotes HBV replication and expression through regulating SMARCE1. As a potential regulator of HBV replication and expression, miR-29a could be a promising therapeutic target for patients with HBV infection.

Published

2017

15. Serum microRNA-30c levels are correlated with disease progression in Xinjiang Uygur patients with chronic hepatitis B

Author

Jie Ma, Jinqian Zhang, Lizhu Guo, Junfa Li, and Huanmin Wang

Subjects

Male, 0301 basic medicine, Physiology, medicine.disease_cause, Chronic hepatitis B, Biochemistry, Medicine, General Pharmacology, Toxicology and Pharmaceutics, lcsh:QH301-705.5, Cell proliferation, Regulation of gene expression, lcsh:R5-920, General Neuroscience, Liver Neoplasms, General Medicine, Middle Aged, Cell cycle, Hepatitis B, HBx, Female, Hepatitis B virus replication, lcsh:Medicine (General), Adult, Gene Expression Regulation, Viral, China, Hepatitis B virus, Carcinoma, Hepatocellular, Immunology, Biophysics, Down-Regulation, Ocean Engineering, Virus, 03 medical and health sciences, Hepatitis B, Chronic, microRNA, Humans, Maze Learning, Disease progression, business.industry, Cell growth, Biomedical Sciences, Cell Biology, microRNA-30c, medicine.disease, digestive system diseases, MicroRNAs, 030104 developmental biology, lcsh:Biology (General), Cancer research, business

Abstract

We aimed to investigate the potential role and mechanism of microRNA-30c (miR-30c) in the pathological development of chronic hepatitis B (CHB). The serum levels of miR-30c in hepatitis B virus (HBV) carrier Xinjiang Uygur patients with inactive, low-replicative, high-replicative and HBe antigen-positive CHB were investigated. HepG2 cells were co-transfected with pHBV1.3 and miR-30c mimic or inhibitor or scramble RNA. The effects of miR-30c dysregulation on HBV replication and gene expression, cell proliferation and cell cycle were then investigated. miR-30c was down-regulated in Xinjiang Uygur patients with CHB compared to healthy controls and its expression level discriminated HBV carrier patients with inactive, low-replicative, high-replicative and HBe antigen-positive risk for disease progression. Overexpression of miR-30c significantly inhibited HBV replication and the expressions of HBV pgRNA, capsid-associated virus DNA and Hbx in hepatoma cells. Moreover, overexpression of miR-30c significantly inhibited cell proliferation and delayed G1/S phase transition in hepatoma cells. Opposite effects were obtained after suppression of miR-30c. Our results indicate that miR-30c was down-regulated in Xinjiang Uygur patients with CHB, and miR-30c levels could serve as a marker for risk stratification of HBV infection. Down-regulation of miR-30c may result in the progression of CHB via promoting HBV replication and cell proliferation.

Published

2017

16. Hepatocystin/80K-H inhibits replication of hepatitis B virus through interaction with HBx protein in hepatoma cell

Author

Kwang Pyo Kim, Gu Choul Shin, Kyun-Hwan Kim, Sung Hyun Ahn, Keo-Heun Lim, Hyo-Sun Choi, and Do Young Choi

Subjects

Hepatitis B virus, Carcinoma, Hepatocellular, viruses, Molecular Sequence Data, Mutant, Mannose, Biology, Virus Replication, medicine.disease_cause, Mass Spectrometry, chemistry.chemical_compound, Cell Line, Tumor, medicine, Humans, Immunoprecipitation, Viral Regulatory and Accessory Proteins, Amino Acid Sequence, Receptor, Molecular Biology, chemistry.chemical_classification, Molecular chaperon, Protein interaction, Calcium-Binding Proteins, Liver Neoplasms, Intracellular Signaling Peptides and Proteins, Molecular biology, digestive system diseases, Amino acid, Blot, HBx, Hepatocystin/80K-H, Proteasome, chemistry, Trans-Activators, Molecular Medicine, Hepatitis B virus replication, Glucosidases, Protein Binding

Abstract

Hepatitis B virus (HBV) X protein (HBx) is a key player in HBV replication as well as HBV-induced hepatocellular carcinoma (HCC). However, the pathogenesis of HBV infection and the mechanisms of host–virus interactions are still elusive. In this study, a combination of affinity purification and mass spectrometry was applied to identify the host factors interacting with HBx in hepatoma cells. Thirteen proteins were identified as HBx binding partners. Among them, we first focused on determining the functional significance of the interaction between HBx and hepatocystin. A physical interaction between HBx and hepatocystin was confirmed by co-immunoprecipitation and Western blotting. Immunocytochemistry demonstrated that HBx and hepatocystin colocalized in the hepatoma cells. Domain mapping of both proteins revealed that the HBx C-terminus (amino acids 110–154) was responsible for binding to the mannose 6-phosphate receptor homology domain (amino acids, 419–525) of hepatocystin. Using translation and proteasome inhibitors, we found that hepatocystin overexpression accelerated HBx degradation via a ubiquitin-independent proteasome pathway. We demonstrated that this effect was mediated by an interaction between both proteins using a HBx deletion mutant. Hepatocystin overexpression significantly inhibited HBV DNA replication and expression of HBs antigen concomitant with HBx degradation. Using the hepatocystin mutant constructs that bind HBx, we also confirmed that hepatocystin inhibited HBx-dependent HBV replication. In conclusion, we demonstrated for the first time that hepatocystin functions as a chaperon-like molecule by accelerating HBx degradation, and thereby inhibits HBV replication. Our results suggest that inducing hepatocystin may provide a novel therapeutic approach to control HBV infection.

Published

2013

17. The novel HBx mutation F30V correlates with hepatocellular carcinoma in vivo, reduces hepatitis B virus replicative efficiency and enhances anti-apoptotic activity of HBx N terminus in vitro.

Author

Salpini, R., Surdo, M., Cortese, M.F., Palumbo, G.A., Carioti, L., Cappiello, G., Spanò, A., Trimoulet, P., Fleury, H., Vecchiet, J., Pasquazzi, C., Mirabelli, C., Scutari, R., Sacco, A., Alkhatib, M., Missale, G., Francioso, S., Sarmati, L., Andreoni, M., and Angelico, M.

Subjects

*HEPATITIS B virus, *HEPATOCELLULAR carcinoma, *BIOMARKERS, *GENETIC markers

Abstract

We aimed to investigate HBx genetic elements correlated with hepatitis B virus (HBV) -related hepatocellular carcinoma (HCC) and their impact on (a) HBV replicative efficiency, (b) HBx binding to circular covalently closed DNA (cccDNA), (c) apoptosis and cell-cycle progression, and (d) HBx structural stability. This study included 123 individuals chronically infected with HBV: 27 with HCC (77.9% (21/27) genotype D; 22.1% (6/27) genotype A) and 96 without HCC (75% (72/96) genotype D; 25.0% (24/96) genotype A). HepG2 cells were transfected by wild-type or mutated linear HBV genome to assess pre-genomic RNA (pgRNA) and core-associated HBV-DNA levels, HBx-binding onto cccDNA by chromatin immunoprecipitation-based quantitative assay, and rate of apoptosis and cell-cycle progression by cytofluorimetry. F30V was the only HBx mutation correlated with HCC (18.5% (5/27) in HCC patients versus 1.0% (1/96) in non-HCC patients, p 0.002); a result confirmed by multivariate analysis. In vitro , F30V determined a 40% and 60% reduction in pgRNA and core-associated HBV-DNA compared with wild-type (p <0.05), in parallel with a significant decrease of HBx binding to cccDNA and decreased HBx stability. F30V also decreased the percentage of apoptotic cells compared with wild-type (14.8 ± 6.8% versus 19.1 ± 10.1%, p <0.01, without affecting cell-cycle progression) and increased the probability of HBx-Ser-31 being phosphorylated by PI3K-Akt kinase (known to promote anti-apoptotic activity). F30V was closely correlated with HBV-induced HCC in vivo , reduced HBV replicative efficiency by affecting HBx-binding to cccDNA and increased anti-apoptotic HBx activity in vitro. This suggests that F30V (although hampering HBV's replicative capacity) may promote hepatocyte survival, so potentially allowing persistent production of viral progeny and initiating HBV-driven hepatocarcinogenesis. Investigation of viral genetic markers associated with HCC is crucial to identify those patients at higher risk of HCC, who hence deserve intensive liver monitoring and/or early anti-HBV therapy. [ABSTRACT FROM AUTHOR]

Published

2019

18. Adiponectin, a downstream target gene of peroxisome proliferator-activated receptor γ, controls hepatitis B virus replication

Author

Kyongmin Kim, Sarah Yoon, Ho-Joon Shin, Yong-Joon Chwae, Sun Park, Taeyeung Kim, and Jaesung Jung

Subjects

Hepatitis B virus, PPARγ, viruses, Peroxisome proliferator-activated receptor, medicine.disease_cause, Virus Replication, Antiviral Agents, Cell Line, Virology, medicine, Gene silencing, Humans, Gene Silencing, Liver X receptor, chemistry.chemical_classification, Adiponectin, Ccaat-enhancer-binding proteins, biology, Gene Expression Profiling, Molecular biology, digestive system diseases, PPAR gamma, Fatty acid synthase, HBx, chemistry, Lamivudine, Host-Pathogen Interactions, biology.protein, Hepatocytes, Hepatitis B virus replication

Abstract

In this study, HepG2-hepatitis B virus (HBV)-stable cells that did not overexpress HBx and HBx-deficient mutant-transfected cells were analyzed for their expression of HBV-induced, upregulated adipogenic and lipogenic genes. The mRNAs of CCAAT enhancer binding protein α (C/EBPα), peroxisome proliferator-activated receptor γ (PPARγ), adiponectin, liver X receptor α (LXRα), sterol regulatory element binding protein 1c (SREBP1c), and fatty acid synthase (FAS) were expressed at higher levels in HepG2–HBV and lamivudine-treated stable cells and HBx-deficient mutant-transfected cells than in the HepG2 cells. Lamivudine treatment reduced the mRNA levels of PPARγ and C/EBPα. Conversely, HBV replication was upregulated by adiponectin and PPARγ agonist rosiglitazone treatments and was downregulated by adiponectin siRNAs. Collectively, our results demonstrate that HBV replication and/or protein expression, even in the absence of HBx, upregulated adipogenic or lipogenic genes, and that the control of adiponectin might prove useful as a therapeutic modality for the treatment of chronic hepatitis B.

Published

2010

19. Rac1 GTPase is activated by hepatitis B virus replication--involvement of HBX

Author

Ning Fang, Seng Gee Lim, Vincent Chan, Cheng-Gee Koh, Jianhua Zhang, Wei Ning Chen, Ruijie Zhou, Tuan Ling Neo, Tuan Lin Tan, and Pritpal Singh

Subjects

rac1 GTP-Binding Protein, Hepatitis B virus, Carcinoma, Hepatocellular, Membrane ruffling, Viral protein, RAC1, Cell Cycle Proteins, CDC42, Biology, Cell morphology, medicine.disease_cause, Transfection, Virus Replication, Models, Biological, src Homology Domains, HBX, medicine, βPIX, Guanine Nucleotide Exchange Factors, Humans, Viral Regulatory and Accessory Proteins, Neoplasm Metastasis, cdc42 GTP-Binding Protein, Molecular Biology, Cell Shape, Rac1 activation, Cells, Cultured, Liver Neoplasms, Cell Biology, Molecular biology, digestive system diseases, Enzyme Activation, HBx, Viral replication, Disease Progression, Trans-Activators, Hepatitis B virus replication, Rho Guanine Nucleotide Exchange Factors, Protein Binding

Abstract

Hepatitis B virus (HBV) is a causative agent for liver diseases including hepatocellular carcinoma. Understanding its interactions with cellular proteins is critical in the elucidation of the mechanisms of disease progression. Using a cell-based HBV replication system, we showed that HBV replication in HepG2 cells resulted in a cellular morphological changes displaying membrane rufflings and lamellipodia like structures reminiscent of cells expressing constitutively activated Rac1. We also showed that activated Rac1 resulted in increased viral replication. HBV replication specifically activated wild type Rac1, but not Cdc42. The Rac1 activation by HBV replication also resulted in the phosphorylation of ERK1/2 and AKT, the downstream targets of Rac1 signaling cascade. The smallest HBV viral protein, HBX, was able to activate the endogenous Rac1 and induce membrane ruffling when transfected into cells. Significantly, HBX was found to directly interact with a Rac1 nucleotide exchange factor (βPIX) through a SH3 binding motif. Taken together, we have shown the interaction of HBV with the Rho GTPase, affecting cell morphology through the Rac1 activation pathway. HBV may possibly make use of an activated Rac1 signaling pathway for increased replication and resultant metastatic effects.

Published

2007

20. Identification of TRIM14 as a Type I IFN-Stimulated Gene Controlling Hepatitis B Virus Replication by Targeting HBx.

Author

Tan G, Xu F, Song H, Yuan Y, Xiao Q, Ma F, Qin FX, and Cheng G

Subjects

Antiviral Agents therapeutic use, Clustered Regularly Interspaced Short Palindromic Repeats, HEK293 Cells, Hep G2 Cells, Hepatitis B genetics, Hepatitis B therapy, Humans, Interferon Type I therapeutic use, Intracellular Signaling Peptides and Proteins, Promoter Regions, Genetic, Protein Binding, Receptors, Pattern Recognition metabolism, STAT1 Transcription Factor genetics, STAT1 Transcription Factor metabolism, Signal Transduction, Transcriptional Activation, Tripartite Motif Proteins, Viral Regulatory and Accessory Proteins, Virus Replication drug effects, Carrier Proteins metabolism, Hepatitis B immunology, Hepatitis B virus physiology, Immunotherapy methods, Interferon Type I metabolism, Trans-Activators metabolism

Abstract

Hepatitis B virus (HBV) remains a major cause of hepatic disease that threatens human health worldwide. Type I IFN (IFN-I) therapy is an important therapeutic option for HBV patients. The antiviral effect of IFN is mainly mediated via upregulation of the expressions of the downstream IFN-stimulated genes. However, the mechanisms by which IFN induces ISG production and inhibits HBV replication are yet to be clarified. TRIM14 was recently reported as a key molecule in the IFN-signaling pathway that regulates IFN production in response to viral infection. In this study, we sought to understand the mechanisms by which IFN restricts HBV replication. We confirmed that TRIM14 is an ISG in the hepatic cells, and that the pattern-recognition receptor ligands polyI:C and polydAdT induce TRIM14 dependent on IFN-I production. In addition, IFN-I-activated STAT1 (but not STAT3) directly bound to the TRIM14 promoter and mediated the induction of TRIM14. Interestingly, TRIM14 played an important role in IFN-I-mediated inhibition of HBV, and the TRIM14 SPRY domain interacted with the C-terminal of HBx, which might block the role of HBx in facilitating HBV replication by inhibiting the formation of the Smc-HBx-DDB1 complex. Thus, our study clearly demonstrates that TRIM14 is a STAT1-dependent ISG, and that the IFN-I-TRIM14-HBx axis shows an alternative way to understand the mechanism by which IFN-I inhibits virus replication.

Published

2018

21. Intrahepatic hepatitis B virus replication and liver histology in subjects with occult hepatitis B infection.

Author

Wong, D.K.-H., Fung, J., Lee, C.-K., Seto, W.-K., Leung, J., Huang, F.-Y., Lin, C.-K., Lai, C.-L., and Yuen, M.-F.

Subjects

*HEPATITIS B virus, *CHRONIC hepatitis B, *HISTOLOGY, *FIBROSIS, *LIVER diseases

Abstract

We studied the intrahepatic hepatitis B virus (HBV) replicative status in 40 people with occult hepatitis B infection (OBI) and 40 patients with chronic hepatitis B (CHB). Intrahepatic HBV DNA, covalently closed circular DNA (cccDNA), and pre-genomic RNA (pgRNA) were quantified. Patients with OBI had median necroinflammation and fibrosis scores of 1 and 0, respectively. Intrahepatic total HBV DNA, cccDNA and pgRNA were detectable in 30 (77%), one (3%) and five (13%) of the participants with OBI, respectively. People with OBI had lower median intrahepatic total HBV DNA than the patients with CHB (p < 0.0001). They had nearly normal liver histology and low intrahepatic HBV replication. [ABSTRACT FROM AUTHOR]

Published

2016

22. Serum microRNA-30c levels are correlated with disease progression in Xinjiang Uygur patients with chronic hepatitis B

Author

J. Zhang, J. Ma, H. Wang, L. Guo, and J. Li

Subjects

Chronic hepatitis B, Disease progression, microRNA-30c, Hepatitis B virus replication, Cell proliferation, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

We aimed to investigate the potential role and mechanism of microRNA-30c (miR-30c) in the pathological development of chronic hepatitis B (CHB). The serum levels of miR-30c in hepatitis B virus (HBV) carrier Xinjiang Uygur patients with inactive, low-replicative, high-replicative and HBe antigen-positive CHB were investigated. HepG2 cells were co-transfected with pHBV1.3 and miR-30c mimic or inhibitor or scramble RNA. The effects of miR-30c dysregulation on HBV replication and gene expression, cell proliferation and cell cycle were then investigated. miR-30c was down-regulated in Xinjiang Uygur patients with CHB compared to healthy controls and its expression level discriminated HBV carrier patients with inactive, low-replicative, high-replicative and HBe antigen-positive risk for disease progression. Overexpression of miR-30c significantly inhibited HBV replication and the expressions of HBV pgRNA, capsid-associated virus DNA and Hbx in hepatoma cells. Moreover, overexpression of miR-30c significantly inhibited cell proliferation and delayed G1/S phase transition in hepatoma cells. Opposite effects were obtained after suppression of miR-30c. Our results indicate that miR-30c was down-regulated in Xinjiang Uygur patients with CHB, and miR-30c levels could serve as a marker for risk stratification of HBV infection. Down-regulation of miR-30c may result in the progression of CHB via promoting HBV replication and cell proliferation.

23. miR-29a promotes hepatitis B virus replication and expression by targeting SMARCE1 in hepatoma carcinoma.

Author

Wu HJ, Zhuo Y, Zhou YC, Wang XW, Wang YP, Si CY, and Wang XH

Subjects

Blotting, Western, Carcinoma, Hepatocellular virology, Cell Survival, Chromosomal Proteins, Non-Histone metabolism, DNA Replication, DNA, Viral isolation & purification, DNA, Viral metabolism, DNA-Binding Proteins metabolism, Enzyme-Linked Immunosorbent Assay, Hep G2 Cells, Hepatitis B Surface Antigens isolation & purification, Hepatitis B Surface Antigens metabolism, Hepatitis B e Antigens isolation & purification, Hepatitis B e Antigens metabolism, Humans, Liver Neoplasms virology, Real-Time Polymerase Chain Reaction, Up-Regulation, Carcinoma, Hepatocellular genetics, Chromosomal Proteins, Non-Histone genetics, DNA-Binding Proteins genetics, Gene Expression Regulation, Neoplastic, Gene Expression Regulation, Viral, Hepatitis B genetics, Hepatitis B virus genetics, Liver Neoplasms genetics, MicroRNAs metabolism, Virus Replication genetics

Abstract

Aim: To investigate the functional role and underlying molecular mechanism of miR-29a in hepatitis B virus (HBV) expression and replication., Methods: The levels of miR-29a and SMARCE1 in HBV-infected HepG2.2.15 cells were measured by quantitative real-time PCR and western blot analysis. HBV DNA replication was measured by quantitative PCR and Southern blot analysis. The relative levels of hepatitis B surface antigen and hepatitis B e antigen were detected by enzyme-linked immunosorbent assay. The Cell Counting Kit-8 (CCK-8) was used to detect the viability of HepG2.2.15 cells. The relationship between miR-29a and SMARCE1 were identified by target prediction and luciferase reporter analysis., Results: miR-29a promoted HBV replication and expression, while SMARCE1 repressed HBV replication and expression. Cell viability detection indicated that miR-29a transfection had no adverse effect on the host cells. Moreover, SMARCE1 was identified and validated to be a functional target of miR-29a. Furthermore, restored expression of SMARCE1 could relieve the increased HBV replication and expression caused by miR-29a overexpression., Conclusion: miR-29a promotes HBV replication and expression through regulating SMARCE1. As a potential regulator of HBV replication and expression, miR-29a could be a promising therapeutic target for patients with HBV infection., Competing Interests: Conflict-of-interest statement: The authors declare that there is no conflict of interest related to this study.

Published

2017

24. Expression of microRNA let-7a positively correlates with hepatitis B virus replication in hepatocellular carcinoma tissues.

Author

Qiu D, Chen J, Liu J, Luo Z, Jiang W, Huang J, Qiu Z, Yue W, and Wu L

Subjects

Adult, DNA, Viral analysis, Female, Hep G2 Cells, Hepatitis B Antibodies blood, Hepatitis B Surface Antigens blood, Hepatitis B e Antigens blood, Humans, Immunoenzyme Techniques, Male, MicroRNAs analysis, Middle Aged, Real-Time Polymerase Chain Reaction, Carcinoma, Hepatocellular pathology, Carcinoma, Hepatocellular virology, Hepatitis B virus growth & development, MicroRNAs biosynthesis, Virus Replication

Abstract

Let-7a miRNA is downregulated in various cancers. However, in hepatocellular carcinoma (HCC) patients infected with hepatitis B virus (HBV), the relationship between let-7a and HBV replication has not been fully elucidated. Liver specimens were collected from 23 HCC patients with chronically active HBV. The serum levels of the HBV antigens hepatitis B surface antigen (HBsAg) and hepatitis B virus e antigen (HBeAg), and the HBV antibodies, anti-HBs, anti-HBe and anti-hepatitis B core antigen (anti-HBc) were measured using the microparticle enzyme immunoassay. Let-7a levels and HBV DNA copy numbers were measured by quantitative real-time PCR (qRT-PCR) and analyzed statistically. A let-7a specific antisense oligonucleotide was introduced to the HBV-producing cell line HepG2.2.15 and a change in HBV DNA copy numbers was assessed by qRT-PCR. HCC patients with highly active HBV replication (>10 6 DNA copies/mL) showed higher levels of serum HBsAg and anti-HBc than patients with less active HBV replication (<10 3 DNA copies/mL). The level of let-7a was lower in malignant tissues than in adjacent normal tissues. However, patients with highly active HBV replication demonstrated a significantly higher level of let-7a in hepatocarcinoma tissue than patients with less active HBV replication ( P < 0.05). A higher level of let-7a was observed in the HBV-producing cell line HepG2.2.15 than in HepG2 cells ( P < 0.05), and let-7a down-regulation by antisense oligonucleotides led to a reduction in HBV DNA copy numbers ( P < 0.05), indicating a correlation between the let-7a level and HBV replication. Down-regulation of let-7a reduces HBV replication and could prevent the development of HCC, suggesting it could be an effective therapeutic treatment for HBV infection. Impact statement Although interferon and nucleic acid analogues effectively suppress HBV replication in HBV patients, there is no treatment which eradicates the virus. Moreover, the therapeutic effect can be reduced by virus mutations or drug resistance. Let-7a is a miRNA initially found in the nematode as a master regulator of developmental processes, but also exists in humans. It has been reported that the transcription of let-7a was much lower in HCC than in normal liver tissues and specific miRNA could directly promote virus replication. Therefore we hypothesized that transcription of let-7a promotes HBV replication, which might compromise the therapeutic effects of antivirus treatments. In our present study, we demonstrated a correlation between let-7a transcription and HBV replication in surgical specimens obtained from patients with HCC, as well as in HCC cell lines. Our finding might be the base for a new approach to improve HBV infection treatments in the future.

Published

2017

25. Hepatitis B virus and microRNAs: Complex interactions affecting hepatitis B virus replication and hepatitis B virus-associated diseases.

Author

Lamontagne J, Steel LF, and Bouchard MJ

Subjects

Animals, Carcinoma, Hepatocellular metabolism, Carcinoma, Hepatocellular pathology, Carcinoma, Hepatocellular therapy, Cell Transformation, Viral, Gene Expression Regulation, Neoplastic, Genetic Therapy, Hepatitis B virus growth & development, Hepatitis B virus metabolism, Hepatitis B, Chronic complications, Hepatitis B, Chronic therapy, Host-Pathogen Interactions, Humans, Liver Neoplasms metabolism, Liver Neoplasms pathology, Liver Neoplasms therapy, MicroRNAs metabolism, Carcinoma, Hepatocellular genetics, Carcinoma, Hepatocellular virology, Hepatitis B virus genetics, Hepatitis B, Chronic virology, Liver Neoplasms genetics, Liver Neoplasms virology, MicroRNAs genetics, Virus Replication

Abstract

Chronic infection with the hepatitis B virus (HBV) is the leading risk factor for the development of hepatocellular carcinoma (HCC). With nearly 750000 deaths yearly, hepatocellular carcinoma is the second highest cause of cancer-related death in the world. Unfortunately, the molecular mechanisms that contribute to the development of HBV-associated HCC remain incompletely understood. Recently, microRNAs (miRNAs), a family of small non-coding RNAs that play a role primarily in post-transcriptional gene regulation, have been recognized as important regulators of cellular homeostasis, and altered regulation of miRNA expression has been suggested to play a significant role in virus-associated diseases and the development of many cancers. With this in mind, many groups have begun to investigate the relationship between miRNAs and HBV replication and HBV-associated disease. Multiple findings suggest that some miRNAs, such as miR-122, and miR-125 and miR-199 family members, are playing a role in HBV replication and HBV-associated disease, including the development of HBV-associated HCC. In this review, we discuss the current state of our understanding of the relationship between HBV and miRNAs, including how HBV affects cellular miRNAs, how these miRNAs impact HBV replication, and the relationship between HBV-mediated miRNA regulation and HCC development. We also address the impact of challenges in studying HBV, such as the lack of an effective model system for infectivity and a reliance on transformed cell lines, on our understanding of the relationship between HBV and miRNAs, and propose potential applications of miRNA-related techniques that could enhance our understanding of the role miRNAs play in HBV replication and HBV-associated disease, ultimately leading to new therapeutic options and improved patient outcomes.

Published

2015

26. Mutations in the Pre-Core Region of Hepatitis B Virus Serve to Enhance the Stability of the Secondary Structure of the Pre-Genome Encapsidation Signal

Author

Akarca, Ulus and Greene, Sheila

Published

1994

27. Hepatitis B Virus (HBV) Particles are Produced in a Cell Culture System by Transient Expression of Transfected HBV DNA

Author

Yaginuma, Katsuyuki, Shirakata, Yumiko, Kobayashi, Midori, and Koike, Katsuro

Published

1987