Clinical and Molecular Hepatology

"HBV"

Review Article

SEVERE HEPATITIS B FLARE AND LIVER FAILURE – CURRENT ASSESSMENT AND MANAGEMENT: Seng Gee Lim, Maria Buti, Jordan J. Feld, James Fung, Adam J. Gehring, K. Rajender Reddy; Received February 4, 2026 Accepted March 11, 2026 Published online March 18, 2026; DOI: https://doi.org/10.3350/cmh.2026.0177 [Accepted]

Abstract
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Hepatitis B flare is a common complication of Chronic Hepatitis B (CHB) and is defined as an increase in HBV viral load associated with abnormal alanine aminotransferases (ALT), the consensus being an ALT≥5xupper limit of normal. The immunopathogenesis is related to induction of inflammatory cells and cytokines by the rise in HBV DNA. There are multiple causes of flares, and they carry the risk of progression to hepatic decompensation and acute-on-chronic liver failure (ACLF) with its associated mortality, potentially requiring liver transplantation. Initial assessment should be exclusion of other causes of liver dysfunction, determine severity, and prognosis. General prognostic models of ACLF are useful but the COSSH-ACLF II score is specific for HBV. Initiation of nucleos(t)ide analogues early is crucial and even in severe HBV flares reduces mortality by 73.6%. Once jaundice and coagulopathy occur, salvage by antivirals is challenging, and such patients should be considered for liver transplantation. However, many patients may not be suitable for transplant or may not have available donor livers as is common in Asia. Recently, there has been increasing evidence of benefit with adjunctive therapies such as corticosteroids and plasma exchange, but this needs to be balanced with the risks and should be considered as rescue therapies in severe HBV flares or ACLF. Liver transplant is the ultimate intervention when these other strategies fail to rescue patients. In summary, HBV flares are clinically serious events that can lead to hepatic decompensation and ACLF but strategies for rescue should be considered before liver transplantation.

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Reply to Correspondence

Reply to correspondence on “Factors associated with hepatitis B mother-to-child transmission in a national prevention program”: Eunho Choi, Ji Hoon Kim, Young-Sun Lee; Clin Mol Hepatol 2026;32(2):e262-e263.
Published online August 19, 2025; DOI: https://doi.org/10.3350/cmh.2025.0871

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Letter to the Editor

Letter to the editor on “Male preference for TERT alterations and HBV integration in young-age HBV-related HCC: implications for sex disparity”: Qicong Mai, Jianming Zheng, Meishi Tang, Yubin Liu; Clin Mol Hepatol 2026;32(2):e134-e135.
Published online July 28, 2025; DOI: https://doi.org/10.3350/cmh.2025.0757

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Editorial

Besifovir: a viable option for long-term disease control in chronic hepatitis B: Editorial on “Switching to besifovir in patients with chronic hepatitis B receiving tenofovir disoproxil fumarate: A randomized trial”: Wai-Kay Seto; Clin Mol Hepatol 2026;32(1):374-376.
Published online March 24, 2025; DOI: https://doi.org/10.3350/cmh.2025.0305

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Correspondence to editorial on “Switching to besifovir in patients with chronic hepatitis B receiving tenofovir disoproxil fumarate: A randomized trial”
Hyung Joon Yim, Seong Hee Kang, Young Kul Jung, Jin Mo Yang
Clinical and Molecular Hepatology.2026; 32(1): e55. CrossRef

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Original Article

Viral hepatitis

Longitudinal profile of plasma pregenomic RNA in patients with chronic hepatitis B infection on long-term nucleoside analogues and its interaction with clinical parameters: Lung-Yi Mak, Mark Anderson, Michael Stec, Matthew Shing-Hin Chung, Danny Ka-Ho Wong, Rex Wan-Hin Hui, Wai-Kay Seto, Gavin Cloherty, Man-Fung Yuen; Clin Mol Hepatol 2025;31(2):460-473.
Published online December 26, 2024; DOI: https://doi.org/10.3350/cmh.2024.0724

Backgrounds/Aims
Plasma pregenomic hepatitis B virus RNA (pgRNA) is a novel biomarker in chronic hepatitis B infection (CHB). We aimed to describe the longitudinal profile of pgRNA and factors influencing its levels in CHB patients on nucleoside analogue (NUC).
Methods
Serial plasma samples from 1,354 CHB patients started on first-line NUC were evaluated. Time of NUC initiation was taken as baseline (year 0), followed by 1-year, 3-year and 5-year of NUC therapy. pgRNA was measured by Research Use Only RealTime HBV RNA v2.0 (0.2 mL) (Abbott Diagnostics) with lower limit of detection of 0.8 log U/mL (~20 copies/mL).
Results
Among 1,354 subjects (median age at baseline 49.8 [interquartile range, IQR 40.2–57.3]) years, 65.2% male, 16.1% hepatitis B e antigen (HBeAg)-positive, 28.6% cirrhotic), baseline median HBV RNA was 3.68 (IQR 2.42–5.19) log U/mL. Upon NUC therapy, median pgRNA levels were 2.45 (IQR 1.82–3.62), 2.23 (IQR 1.67–3.05) and 2.14 (IQR 1.48–2.86) log U/mL at 1, 3 and 5 years, respectively, with the corresponding log U/mL reductions of 0.82, 1.20 and 1.54. Undetectable/ unquantifiable pgRNA was achieved in 13.5%, 15.9% and 20.1% of patients at 1, 3 and 5 years, respectively. Older age, male sex, HBeAg-negativity and high PAGE-B score were associated with lower pgRNA.
Conclusions
Plasma pgRNA declines are modest under NUC therapy, with only 16.3% achieving RNA undetectability after 5 years of first-line NUC indicating cccDNA silencing has not been achieved in the majority of patients. Clinical characteristics should be taken into consideration when interpreting the plasma pgRNA level.

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Mary A. Rodgers, Francisco Averhoff, Michael G. Berg, Mark Anderson, Carolyn Strobel, Julissa Inostroza, James Moy, Jorge Mera, Paul J. Utz, Scott C. Weaver, Charles Y. Chiu, Judith C. De Arcos, Joshua J. Anzinger, Jean H. Henrys, Juan P. Hernandez-Ortiz,
International Journal of Infectious Diseases.2026; 162: 108162. CrossRef
Targeting the innate immune system in treating hepatitis B: prospects for functional cure
Karen Cheuk-Ying Ho, Rex Wan-Hin Hui, Wai-Kay Seto, Man-Fung Yuen, Lung-Yi Mak
Clinical and Molecular Hepatology.2026; 32(1): 184. CrossRef
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Reconsidering the role of plasma pgRNA in NUC-treated CHB: Stratified biomarker interpretation and the limits of current assays: Letter to the editor on “Longitudinal profile of plasma pregenomic RNA in patients with chronic hepatitis B infection on long-
Xu Han, Jun Sun, Yinyan Li
Clinical and Molecular Hepatology.2026; 32(2): e131. CrossRef
Profiles and kinetics of PgRNA and clinical characteristics in pregnant, postpartum, and non-pregnant women with chronic HBV infection
Genju Wang, Yandan Wu, Ziyue Zhang, Qiuchen Wu, Juan Tang, Ying Ji, Yan Wang, Guanlun Zhou, Minmin Yu
Virology Journal.2025;[Epub] CrossRef

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Correspondence

Viral hepatitis

Correspondence on editorial regarding “Novel role of MHC class II transactivator in hepatitis B virus replication and viral counteraction”: Mehrangiz Dezhbord, Kyun-Hwan Kim; Clin Mol Hepatol 2024;30(4):1028-1030.
Published online July 9, 2024; DOI: https://doi.org/10.3350/cmh.2024.0515

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Reply to correspondence on “Novel role of MHC class II transactivator in hepatitis B virus replication and viral counteraction”
Cho-Rong Lee, Sung-Gyoo Park
Clinical and Molecular Hepatology.2024; 30(4): 1053. CrossRef

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Editorial

Hepatic neoplasm

Engineering HBV-specific T cells for the treatment of HBV-related HCC and HBV infection: Past, Present, and Future. Editorial on “Genetically-modified, redirected T cells target hepatitis B surface antigen-positive hepatocytes and hepatocellular carcinoma lesions in a clinical setting”: Antonio Bertoletti, Anthony T Tan; Clin Mol Hepatol 2024;30(4):728-734.
Published online June 27, 2024; DOI: https://doi.org/10.3350/cmh.2024.0469

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Rahaf Albarghash, Carina Jacobsen, Helenie Kefalakes
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Antonio Bertoletti, Anthony T Tan
Clinical and Molecular Hepatology.2025; 31(1): e113. CrossRef
Correspondence to editorial on “Genetically-modified, redirected T cells target hepatitis B surface antigen-positive hepatocytes and hepatocellular carcinoma lesions in a clinical setting”
Shunda Du, Karin Wisskirchen, Ke Zhang, Ulrike Protzer
Clinical and Molecular Hepatology.2025; 31(1): e44. CrossRef
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Qing Xiao, Yi Liu, Tingting Li, Chaoyu Wang, Sanxiu He, Liuyue Zhai, Zailin Yang, Xiaomei Zhang, Yongzhong Wu, Yao Liu
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Journal of Viral Hepatitis.2025;[Epub] CrossRef
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Lihua Qi, Bai Hu, Canhui Cao, Ting Peng, Miaochun Xu, Shiyi Liu, Yashi Xu, Xiaojie Liu, Wencheng Ding, Li Li, Shitong Lin
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Original Article

Viral hepatitis

Novel role of MHC class II transactivator in hepatitis B virus replication and viral counteraction: Mehrangiz Dezhbord, Seong Ho Kim, Soree Park, Da Rae Lee, Nayeon Kim, Juhee Won, Ah Ram Lee, Dong-Sik Kim, Kyun-Hwan Kim; Clin Mol Hepatol 2024;30(3):539-560.
Published online May 14, 2024; DOI: https://doi.org/10.3350/cmh.2024.0060

Background/Aims
The major histocompatibility class II (MHC II) transactivator, known as CIITA, is induced by Interferon gamma (IFN-γ) and plays a well-established role in regulating the expression of class II MHC molecules in antigen-presenting cells.
Methods
Primary human hepatocytes (PHH) were isolated via therapeutic hepatectomy from two donors. The hepatocellular carcinoma (HCC) cell lines HepG2 and Huh7 were used for the mechanistic study, and HBV infection was performed in HepG2-NTCP cells. HBV DNA replication intermediates and secreted antigen levels were measured using Southern blotting and ELISA, respectively.
Results
We identified a non-canonical function of CIITA in the inhibition of hepatitis B virus (HBV) replication in both HCC cells and patient-derived PHH. Notably, in vivo experiments demonstrated that HBV DNA and secreted antigen levels were significantly decreased in mice injected with the CIITA construct. Mechanistically, CIITA inhibited HBV transcription and replication by suppressing the activity of HBV-specific enhancers/promoters. Indeed, CIITA exerts antiviral activity in hepatocytes through ERK1/2-mediated down-regulation of the expression of hepatocyte nuclear factor 1α (HNF1α) and HNF4α, which are essential factors for virus replication. In addition, silencing of CIITA significantly abolished the IFN-γ-mediated anti-HBV activity, suggesting that CIITA mediates the anti-HBV activity of IFN-γ to some extent. HBV X protein (HBx) counteracts the antiviral activity of CIITA via direct binding and impairing its function.
Conclusions
Our findings reveal a novel antiviral mechanism of CIITA that involves the modulation of the ERK pathway to restrict HBV transcription. Additionally, our results suggest the possibility of a new immune avoidance mechanism involving HBx.

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Class II transactivator restricts viral replication, extending its effect to HBV: Editorial on “Novel role of MHC class II transactivator in hepatitis B virus replication and viral counteraction”
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Editorials

Viral hepatitis

Enhancing off-nucleos(t)ide analogue outcome predictions in chronic hepatitis B with time-varying hepatitis B core-related antigen: Chen-Te Huang, Tai-Chung Tseng; Clin Mol Hepatol 2024;30(2):154-156.
Published online February 22, 2024; DOI: https://doi.org/10.3350/cmh.2024.0120

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Optimizing off-treatment outcome predictions: The potential of time-varying HBcrAg and the need for more research
Ying-Nan Tsai, Jia-Ling Wu, Yao-Chun Hsu
Clinical and Molecular Hepatology.2024; 30(2): 276. CrossRef

5,579 View
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Viral hepatitis

Cardiovascular risk of tenofovir disoproxil fumarate or tenofovir alafenamide in patients with chronic hepatitis B: More questions than an answer: Pin-Nan Cheng, Ming-Lung Yu; Clin Mol Hepatol 2024;30(2):144-146.
Published online February 19, 2024; DOI: https://doi.org/10.3350/cmh.2024.0115

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Effect of switching from prior Nucleos(t)ide Analogue(s) to Tenofovir alafenamide on lipid profile and cardiovascular risk in patients with Chronic Hepatitis B
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Letter: Cardiovascular risk of tenofovir disoproxil fumarate or tenofovir alafenamide fumarate in patients with chronic hepatitis B: More questions than an answer – author’s reply
Hyeyeon Hong, Jonggi Choi
Clinical and Molecular Hepatology.2024; 30(2): 272. CrossRef
Reply to correspondence on “Cardiovascular risk in chronic hepatitis B patients treated with tenofovir disoproxil fumarate or tenofovir alafenamide”
Pin-Nan Cheng, Ming-Lung Yu
Clinical and Molecular Hepatology.2024; 30(4): 1031. CrossRef

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Letters to the Editor

Viral hepatitis

Letter regarding “Hepatitis B core-related antigen dynamics and risk of subsequent clinical relapses after nucleos(t)ide analog cessation”: Yun-Fan Liaw; Clin Mol Hepatol 2024;30(2):269-271.
Published online January 31, 2024; DOI: https://doi.org/10.3350/cmh.2024.0064

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Harnessing hepatitis B core-related antigen measurement to optimize posttreatment monitoring
Ying-Nan Tsai, Jia-Ling Wu, Yao-Chun Hsu
Clinical and Molecular Hepatology.2024; 30(2): 293. CrossRef

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Viral hepatitis

Letter regarding “Treated chronic hepatitis B is a good prognostic factor of diffuse large B-cell lymphoma”: Chi Hsiao, Yung-Po Liaw; Clin Mol Hepatol 2024;30(1):109-110.
Published online October 11, 2023; DOI: https://doi.org/10.3350/cmh.2023.0373

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Editorial

Viral hepatitis

The latest evidence on the impact of fatty liver on liver-related outcomes and mortality in chronic hepatitis B: Xianhua Mao, Lung Yi Mak, Wai-Kay Seto; Clin Mol Hepatol 2023;29(3):690-692.
Published online May 30, 2023; DOI: https://doi.org/10.3350/cmh.2023.0173

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Cohort Profile: Taizhou Study of Liver Diseases (T-SOLID)
Zhenqiu Liu, Yanfeng Jiang, Chen Suo, Huangbo Yuan, Ziyu Yuan, Tiejun Zhang, Li Jin, Xingdong Chen
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Review

Viral hepatitis

Hepatitis B core-related antigen: A novel and promising surrogate biomarker to guide anti-hepatitis B virus therapy: Takako Inoue, Takehisa Watanabe, Yasuhito Tanaka; Clin Mol Hepatol 2023;29(4):851-868.
Published online March 9, 2023; DOI: https://doi.org/10.3350/cmh.2022.0434

Abstract
PDF

The current requirement for biomarkers to detect hepatitis B virus (HBV) infection is polarized. One is a fully-automated and highly sensitive measurement system; the other is a simple system for point-of-care testing (POCT) in resource-limited areas. Hepatitis B core-related antigen (HBcrAg) reflects intrahepatic covalently closed circular DNA and serum HBV DNA. Even in patients with undetectable serum HBV DNA or HBsAg loss, HBcrAg may remain detectable. Decreased HBcrAg levels are associated with reduction of the occurrence of hepatocellular carcinoma (HCC) in chronic hepatitis B. Recently, a fully-automated, novel high-sensitivity HBcrAg assay (iTACT-HBcrAg, cut-off value: 2.1 logIU/mL) has been developed. This attractive assay has been released in Japan very recently. iTACT-HBcrAg can be useful for monitoring HBV reactivation and prediction of HCC occurrence, as an alternative to HBV DNA. Moreover, monitoring HBcrAg may be suitable for determining the therapeutic effectiveness of approved drugs and novel drugs under development. Presently, international guidelines recommend anti-HBV prophylaxis for pregnant women with high viral loads to prevent mother-to-child transmission of HBV. However, >95% of HBV-infected individuals live in countries where HBV DNA quantification is not available. Worldwide elimination of HBV needs the scaling-up of examination and medication services in resource-limited areas. Based on this situation, a rapid and easy HBcrAg assay as a POCT is valuable. This review provides the latest information regarding the clinical use of a new surrogate marker, HBcrAg, in HBV management, based on iTACT-HBcrAg or POCT, and introduces novel agents targeting HBV RNA/protein.

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Original Articles

Viral hepatitis

Tenofovir alafenamide treatment may not worsen the lipid profile of chronic hepatitis B patients: A propensity score-matched analysis: Joonho Jeong, Jung Woo Shin, Seok Won Jung, Eun Ji Park, Neung Hwa Park; Clin Mol Hepatol 2022;28(2):254-264.
Published online December 28, 2021; DOI: https://doi.org/10.3350/cmh.2021.0314

Background/Aims
Tenofovir alafenamide (TAF) has shown less favorable effect on lipids compared to tenofovir disoproxil fumarate (TDF) in clinical trials. However, data regarding these outcomes in patients with chronic hepatitis B (CHB) are scarce. Therefore, this study aimed to evaluate the effect of TAF on the lipid in patients with CHB.
Methods
A total of 237 TAF-treated CHB patients compared with TDF, inactive CHB, and non-hepatitis B virus (HBV)-infected control groups using propensity score matching (PSM).
Results
Following PSM, each analysis was conducted on cohorts via the matching of 70:140 (TAF:TDF), 89:89 (TAF:inactive CHB), 140:560 (TAF:non-HBV infected control), and 368:1,472 (TDF:non-HBV-infected control). A significant decrease in the total cholesterol (TC) level was noted at 48 weeks in the TDF group compared to the TAF group (176.3±32.9 vs. 156.7±27.7, P<0.001) and the non-HBV-infected control group (175.0±29.5 vs. 156.2±28.3, P<0.001). However, no significant change in TC was observed in the TAF group and inactive CHB or non-HBV-infected control groups at 48 weeks. For the subgroup analyses of TAF vs. non-HBV-infected control subjects and inactive CHB patients whose detailed lipid profile information were available, no between-group differences in TC, low-density lipoprotein (LDL)-cholesterol, highdensity lipoprotein (HDL)-cholesterol, TC/HDL ratio, and LDL/HDL ratio were observed at 48 weeks.
Conclusions
TDF seems to have a lipid-lowering effect compared to the non-HBV-infected control and TAF-treated groups. However, in real practice, TAF might not worsen the lipid profiles of subjects compared to non-HBV-infected controls and patients with inactive CHB.

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Viral hepatitis

Clinical characteristics of patients with chronic hepatitis B who developed genotypic resistance to entecavir: Real-life experience: Hong Joo Kim, Yong Kyun Cho, Woo Kyu Jeon, Byung Ik Kim; Clin Mol Hepatol 2017;23(4):323-330.
Published online September 5, 2017; DOI: https://doi.org/10.3350/cmh.2017.0005

Abstract
PDF

Background/Aims
Clinical characteristics of patients with chronic hepatitis B (CHB) who developed genotypic resistance to entecavir (ETV) were compared to those without resistance.
Methods
Two hundred fifty eight CHB patients who underwent ETV treatment in our institution from July 2007 to May 2013 were included.
Results
Eight (3.1%) patients developed genotypic resistance to ETV during the follow-up period. The patterns of genotypic resistance to ETV were as follows: L180M + M204V + S202G (n=3); M204I + V173M (n=1); I169V + V173M (n=1); L180M + M204V + V173L (n=1); L180M + M204V + V173L + M250V (n=1); M204I + V214A + P237H (n=1). The cumulative occurrence rates of genotypic resistance to ETV were not significantly different between CHB patients with prior nucleos(t)tide analogues (NA) exposure (NA experienced, n=56) and NA naïve patients (n=202, P=0.823 by log rank comparison). Older age, higher baseline log₁₀hepatitis B virus-deoxynucleic acid (log₁₀HBV-DNA), higher log₁₀HBV-DNA at 3, 6, 12 and 24 months after baseline, and complete virologic response (CVR, undetectable serum HBV-DNA by polymerase chain reaction 6 months after ETV treatment) were significant contributors to the development of genotypic resistance to ETV. Multivariate analyses showed higher log₁₀HBV-DNA 6 months after baseline and absence of CVR were independent and significant contributors to the development of ETV resistance.
Conclusions
Clinical characteristics of patients who developed ETV resistance were higher log₁₀HBV-DNA 6 months after baseline and absence of CVR during the ETV treatment.

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Frontiers in Medicine.2025;[Epub] CrossRef
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Review

Viral hepatitis

New perspectives of biomarkers for the management of chronic hepatitis B: Chih-Lin Lin, Jia-Horng Kao; Clin Mol Hepatol 2016;22(4):423-431.
Published online December 25, 2016; DOI: https://doi.org/10.3350/cmh.2016.0069

Abstract
PDF

With recent advances in molecular and genomic investigations, the impact of hepatitis B viral and host factors on the progression of chronic HBV infection has been explored. For viral factors, hepatitis B viral load is a strong predictor for liver disease progression. Hepatitis B viral kinetics appear to be important for successful anti-viral therapy. Serum HBsAg level serves as a complementary marker to viral load for the prediction of HBV-related adverse outcomes in patients with low viral load. In those with low viral load, high serum HBsAg level is associated with higher risks of cirrhosis and HCC. Hepatitis B core-related antigen (HBcrAg) induces host immune responses, and the reduction of the HBcrAg level as well as the increment of total anti-HBc level are significantly associated with favorable outcomes. HBV genotypes (genotype C/D) and mutants (basal core promoter and deletion mutation in pre-S genes) are well known viral genetic markers to predict disease progression. For host factors, serum inflammatory biomarkers have been developed to evaluate the HBV-associated hepatic necroinflammation and fibrosis. Host single nucleotide polymorphism on sodium taurocholate cotransporting polypeptide (NTCP, an HBV entry receptor) may be associated with a decreased risk for cirrhosis and HCC. In conclusion, patients with chronic hepatitis B should be evaluated with relevant viral and host markers to identify those who are at a higher risk of liver disease progression and then receive timely antiviral therapy.

Citations

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Original Article

Viral hepatitis

Is it necessary to delay antiviral therapy for 3-6 months to anticipate HBeAg seroconversion in patients with HBeAg-positive chronic hepatitis B in endemic areas of HBV genotype C?: Byung-Cheol Song, Yoo-Kyung Cho, Hyeyoung Jwa, Eun Kwang Choi, Heung Up Kim, Hyun Joo Song, Soo-Young Na, Sun-Jin Boo, Seung Uk Jeong; Clin Mol Hepatol 2014;20(4):355-360.
Published online December 24, 2014; DOI: https://doi.org/10.3350/cmh.2014.20.4.355

Abstract
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Background/Aims

Spontaneous HBeAg seroconversion occurs frequently in the immune reactive phase in HBeAg-positive chronic hepatitis B (CHB). Therefore, observation for 3-6 months before commencing antiviral therapy is recommended in patients with alanine aminotransferase (ALT) levels that exceed twice the upper limit of normal (ULN). However, HBeAg seroconversion occurs infrequently in patients infected with hepatitis B virus (HBV) genotype C. The aim of the present study was to determine whether the waiting policy is necessary in endemic areas of HBV genotype C infection.

Methods

Ninety patients with HBeAg-positive CHB were followed prospectively without administering antiviral therapy for 6 months. Antiviral therapy was initiated promptly at any time if there was any evidence of biochemical (i.e., acute exacerbation of HBV infection or aggravation of jaundice) or symptomatic deterioration. After 6 months of observation, antiviral therapy was initiated according to the patient's ALT and HBV DNA levels.

Results

Only one patient (1.1%) achieved spontaneous HBeAg seroconversion. Biochemical and symptomatic deterioration occurred before 6 months in 17 patients (18.9%) and 5 patients, respectively. High ALT and HBV DNA levels were both independent risk factors for biochemical deterioration. Of 15 patients with HBV DNA ≥5.1×10⁷ IU/mL and ALT ≥5×ULN, biochemical deterioration occurred in 7 (46.7%), including 1 patient receiving liver transplantation due to liver failure.

Conclusions

Spontaneous HBeAg seroconversion in patients with HBeAg-positive CHB is rare within 6 months. Biochemical deterioration was common and may lead to liver failure. Immediate antiviral therapy should be considered, especially in patients with high ALT and HBV DNA levels in endemic areas of genotype C infection.

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KASL clinical practice guidelines for management of chronic hepatitis B

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Review

Viral hepatitis

Risk stratification of HBV infection in Asia-Pacific region: Jia-Horng Kao; Clin Mol Hepatol 2014;20(3):223-227.
Published online September 25, 2014; DOI: https://doi.org/10.3350/cmh.2014.20.3.223

Abstract
PDF

Hepatitis B virus (HBV) infection is the major etiology of chronic liver disease worldwide and thus a global health problem, especially in Asia-Pacific region. The long-term outcomes of Asian HBV carriers vary widely; however, a significant proportion of them will finally develop end-stage liver disease. Over the past decade, several host and HBV factors predictive of clinical outcomes in Asian HBV carriers have been identified. The community-based REVEAL-HBV study illustrated the strong association between HBV-DNA level at study entry and risk of HCC over time, and male gender, older age, high serum alanine aminotransferase (ALT) level, positive HBeAg, higher HBV-DNA level, HBV genotype C infection and core promoter mutation are independently associated with a higher hepatocellular carcinoma (HCC) risk. Another hospital-based ERADICATE-B cohort further validated the HCC risk started to increase when HBV-DNA level was higher than 2,000 IU/mL. Of particular note, in patients with low viral load (HBV-DNA level <2,000 IU/mL), HBsAg level ≥1,000 IU/mL was a new independent risk factor for HCC. With the results from REVEAL-HBV study, a risk calculator for predicting HCC in adult non-cirrhotic patients has been developed and validated by independent international cohorts (REACH-B). With the combination of HBV-DNA, HBsAg, and ALT levels, ERADICATE-B study proposed an algorithm to predict disease progression and categorize risk levels of HCC as well as corresponding management in Asian HBV carriers. The introduction of transient elastography may further enhance the predictive power. In conclusion, HBsAg level can complement HBV-DNA level for the risk stratification of disease progression in Asian adult patients with chronic HBV infection.

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Original Articles

Viral hepatitis

Performance evaluation of the HepB Typer-Entecavir kit for detection of entecavir resistance mutations in chronic hepatitis B: Sang Hoon Ahn, Ji-Yong Chun, Soo-Kyung Shin, Jun Yong Park, Wangdon Yoo, Sun Pyo Hong, Soo-Ok Kim, Kwang-Hyub Han; Clin Mol Hepatol 2013;19(4):399-408.
Published online December 28, 2013; DOI: https://doi.org/10.3350/cmh.2013.19.4.399

Background/Aims

Molecular diagnostic methods have enabled the rapid diagnosis of drug-resistant mutations in hepatitis B virus (HBV) and have reduced both unnecessary therapeutic interventions and medical costs. In this study we evaluated the analytical and clinical performances of the HepB Typer-Entecavir kit (GeneMatrix, Korea) in detecting entecavir-resistance-associated mutations.

Methods

The HepB Typer-Entecavir kit was evaluated for its limit of detection, interference, cross-reactivity, and precision using HBV reference standards made by diluting high-titer viral stocks in HBV-negative human serum. The performance of the HepB Typer-Entecavir kit for detecting mutations related to entecavir resistance was compared with direct sequencing for 396 clinical samples from 108 patients.

Results

Using the reference standards, the detection limit of the HepB Typer-Entecavir kit was found to be as low as 500 copies/mL. No cross-reactivity was observed, and elevated levels of various interfering substances did not adversely affect its analytical performance. The precision test conducted by repetitive analysis of 2,400 replicates with reference standards at various concentrations showed 99.9% agreement (2398/2400). The overall concordance rate between the HepB Typer-Entecavir kit and direct sequencing assays in 396 clinical samples was 99.5%.

Conclusions

The HepB Typer-Entecavir kit showed high reliability and precision, and comparable sensitivity and specificity for detecting mutant virus populations in reference and clinical samples in comparison with direct sequencing. Therefore, this assay would be clinically useful in the diagnosis of entecavir-resistance-associated mutations in chronic hepatitis B.

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Tao Yang, Tian-Hui Zheng, Qiang Zhao, Wei Liu, Shu-Ping Li, Yan-Yan Tao, Chang-Hong Wang, Cheng-Hai Liu
Pharmaceutical Biology.2020; 58(1): 1. CrossRef

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Clinical significance of occult hepatitis B virus infection in chronic hepatitis C patients: Jae Young Jang, Soung Won Jeong, Sung Ran Cheon, Sae Hwan Lee, Sang Gyune Kim, Young Koog Cheon, Young Seok Kim, Young Deok Cho, Hong Soo Kim, So Young Jin, Yun Soo Kim, Boo Sung Kim; Korean J Hepatol 2011;17(3):206-212.
Published online September 30, 2011; DOI: https://doi.org/10.3350/kjhep.2011.17.3.206

Abstract
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Background/Aims

We investigated the frequency of occult hepatitis B virus (HBV) infection in anti-hepatitis C virus (HCV)-positive individuals and the effects of occult HBV infection on the severity of liver disease.

Methods

Seventy-one hepatitis B virus surface-antigen (HBsAg)-negative patients were divided according to their HBV serological status into groups A (anti-HBc positive, anti-HBs negative; n=18), B (anti-HBc positive, anti-HBs positive; n=34), and C (anti-HBc negative, anti-HBs positive/negative; n=19), and by anti-HCV positivity (anti-HCV positive; n=32 vs. anti-HCV negative; n=39). Liver biopsy samples were taken, and HBV DNA was quantified by real-time PCR.

Results

Intrahepatic HBV DNA was detected in 32.4% (23/71) of the entire cohort, and HBV DNA levels were invariably low in the different groups. Occult HBV infection was detected more frequently in the anti-HBc-positive patients. Intrahepatic HBV DNA was detected in 28.1% (9/32) of the anti-HCV-positive and 35.9% (14/39) of the anti-HCV-negative subjects. The HCV genotype did not affect the detection rate of intrahepatic HBV DNA. In anti-HCV-positive cases, occult HBV infection did not affect liver disease severity.

Conclusions

Low levels of intrahepatic HBV DNA were detected frequently in both HBsAg-negative and anti-HCV-positive cases. However, the frequency of occult HBV infection was not affected by the presence of hepatitis C, and occult HBV infection did not have a significant effect on the disease severity of hepatitis C.

Citations

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Clinicopathological study of occult hepatitis B virus infection in hepatitis C virus-associated hepatocellular carcinoma
Mohamed A. El-Maksoud, Maha R. Habeeb, Hayam F. Ghazy, Manal M. Nomir, Hatem Elalfy, Sally Abed, Maysaa E.S. Zaki
European Journal of Gastroenterology & Hepatology.2019; 31(6): 716. CrossRef
Occult Hepatitis B Virus infection in a cohort of patients with chronic Hepatitis C
MA Amin, MI Naga, DA Algendy, AI El Badry, MM Fawzi
Archives of Hepatitis Research.2019; 5(1): 017. CrossRef
Occult Hepatitis B Infection in Hepatitis C Patients with Hematological Disorders
Nematollah Jonaidi-Jafari, Mohammad Saeid Rezaee-Zavareh, Javad Tavallaei-Nosratabadi, Reza Ajudani, Mahdi Ramezani-Binabaj, Hamidreza Karimi-Sari, Morteza Izadi, Reza Ranjbar, Seyyed Mohammad Miri, Seyed Moayed Alavian
Jundishapur Journal of Microbiology.2016;[Epub] CrossRef
Occult hepatitis B virus infection is not associated with disease progression of chronic hepatitis C virus infection
Junhyeon Cho, Sang Soo Lee, Yun Suk Choi, Yejoo Jeon, Jung Wha Chung, Joo Yeong Baeg, Won Keun Si, Eun Sun Jang, Jin-Wook Kim, Sook-Hyang Jeong
World Journal of Gastroenterology.2016; 22(42): 9427. CrossRef
Update on occult hepatitis B virus infection
Manoochehr Makvandi
World Journal of Gastroenterology.2016; 22(39): 8720. CrossRef
Seroprevalence of occult hepatitis B among Egyptian paediatric hepatitis C cancer patients
H. E. Raouf, A. S. Yassin, S. A. Megahed, M. S. Ashour, T. M. Mansour
Journal of Viral Hepatitis.2015; 22(2): 103. CrossRef
Spontaneous HBsAg loss in Korean patients: relevance of viral genotypes, S gene mutations, and covalently closed circular DNA copy numbers
Kyun-Hwan Kim, Hye-Young Chang, Jun Yong Park, Eun-Sook Park, Yong Kwang Park, Kwang-Hyub Han, Sang Hoon Ahn
Clinical and Molecular Hepatology.2014; 20(3): 251. CrossRef
Occult Hepatitis B Virus Infection in Chronic Hepatitis C
Jae Young Jang, Eui Ju Park
The Korean Journal of Gastroenterology.2013; 62(3): 154. CrossRef
The presence of hepatitis B core antibody is associated with more advanced liver disease in alcoholic patients with cirrhosis
Mingyuan Zhang, Ruihong Wu, Jing Jiang, Gerald Y. Minuk, Junqi Niu
Alcohol.2013; 47(7): 553. CrossRef
Definition, Diagnosis, and Prevalence of Occult Hepatitis B Virus Infection
Yun Soo Kim
The Korean Journal of Gastroenterology.2013; 62(3): 143. CrossRef
Detection of occult HBV infection by nested PCR assay among chronic hepatitis C patients with and without hepatocellular carcinoma
Shereen E. Taha, Soha A. El-Hady, Tamer M. Ahmed, Iman Z. Ahmed
Egyptian Journal of Medical Human Genetics.2013; 14(4): 353. CrossRef
Clinical Characteristics of Occult HBV Infection and Impact on Treatment Response in Patients with Chronic Hepatitis C
Sung Soo Byun, Jung Woo Shin, Myung Kwan Ko, Jung Min Hong, Kyung Hoon Kim, Mu Yeol Lee, Hye-Jeong Choi, Yoong Ki Jeong, Bo Ryung Park, Neung Hwa Park
Korean Journal of Medicine.2012; 83(6): 731. CrossRef

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The efficacy of adefovir dipivoxil monotherapy and the incidence of genotypic resistance to adefovir dipivoxil in patients with Lamivudine-resistant chronic hepatitis B infection: Jae Hyeon Moon , Mong Cho , Ki Tae Yoon , Jung Ho Bae , Jeong Heo , Gwang Ha Kim , Dae Hwan Kang , Geun Am Song; Korean J Hepatol 2008;14(4):503-512.
Published online December 31, 2008; DOI: https://doi.org/10.3350/kjhep.2008.14.4.503

Abstract
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Background/Aims
Adefovir dipivoxil (ADV) is a nucleotide analogue that inhibits wild-type hepatitis B virus (HBV) and lamivudine (LMV)-resistant HBV mutants. The aim of this study was to elucidate the efficacy of ADV monotherapy and the incidence of genotypic resistance to ADV in patients with LMV-resistant chronic HBV infection. Methods: This study involved 124 patients with chronic HBV infection who had received ADV monotherapy due to the presence of LMV-resistant HBV mutants. The efficacy of ADV was evaluated by the normalization of serum alanine aminotransferase (ALT) level and by the reduction of serum HBV DNA level (with cutoff levels of 2×10⁴ IU/mL and 2×10² IU/mL). The cumulative rate of HBeAg loss or seroconversion was assessed in HBeAg-positive patients. The development of mutations in the reverse trancriptase region of HBV DNA polymerase was evaluated by direct sequencing analysis during ADV monotherapy. Results: The mean serum HBV DNA level was 5.94 log10IU/mL. At 12 and 24 months after ADV monotherapy, the cumulative rates of serum ALT normalization were 69.4% and 75.5%, respectively, and those of serum HBV DNA reduction were 79.8% and 89.2% for a cutoff level of 2×10⁴ IU/mL, and 44.2% and 59.0% for a cutoff of 2×10² IU/mL. The mean serum HBV DNA levels at 12 and 24 months were significantly lower than baseline, at 3.24 and 3.04 log10IU/mL, respectively (P<0.001). At 12 months after ADV treatment, the cumulative rates of HBeAg loss and seroconversion were 15.8% and 10.5%, respectively, and the rtN236T and rtA181T/V mutants in HBV DNA polymerase were identified in 25% and 64% of patients, respectively. Conclusions: Although ADV monotherapy is effective, it leads to a high rate of mutations of HBV DNA reverse transcriptase gene in patients with chronic HBV infections who have LMV-resistant HBV mutants. (Korean J Hepatol 2008;14:503-512)

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Analysis of Reverse Transcriptase Gene Mutations in the Hepatitis B Virus at a University Hospital in Korea
A-Jin Lee, Chang Hyeong Lee, Chang-Ho Jeon
Annals of Laboratory Medicine.2014; 34(3): 230. CrossRef
A Low Viral Load Predicts a Higher Initial Virologic Response to Adefovir in Patients with Lamivudine-Resistant Chronic Hepatitis B
Su Rin Shin, Kwang Cheol Koh, Geum-Youn Gwak, Moon Seok Choi, Joon Hyoek Lee, Seung Woon Paik, Byung Chul Yoo
Gut and Liver.2010; 4(4): 530. CrossRef

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The significance of anti-HBc and occult hepatitis B virus infection in the occurrence of hepatocellular carcinoma in patients with HBsAg and anti-HCV negative alcoholic cirrhosis: Min Ju Kim , Oh Sang Kwon , Nak So Chung , Seo Young Lee , Hyuk Sang Jung , Dong Kyun Park , Yang Suh Ku , Yu Kyung Kim , Yun Soo Kim , Ju Hyun Kim; Korean J Hepatol 2008;14(1):67-76.
Published online March 20, 2008; DOI: https://doi.org/10.3350/kjhep.2008.14.1.67

Abstract
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Background/Aims
Alcohol and the hepatitis B virus (HBV) exert synergistic effects in hepatocelluar carcinogenesis. We aimed to elucidate the clinical significance of the antibody to hepatitis B core antigen (anti-HBc) and occult HBV infection on the development of hepatocellular carcinoma (HCC) in patients with alcoholic liver cirrhosis (LC). Methods: Patients with alcoholic LC alone (n=193) or combined with HCC (n=36), who did not have HBsAg or antibody to hepatitis C virus were enrolled. Clinical data and laboratory data including anti-HBc were investigated at enrollment. The polymerase chain reaction was applied to HBV DNA using sera of patients with HCC or LC after age and sex matching. Results: Patients with HCC were older (60±11 years vs. 53±10 years, mean±SD, P<0.001), more likely to be male (100% vs. 89%, P=0.03), and had a higher positive rate of anti-HBc (91.2% vs. 77.3%, P=0.067), and a higher alcohol intake (739±448 kg vs. 603±409 kg, P=0.076) than those with LC. Age was the only significant risk factor for HCC revealed by multiple logistic regression analysis (odds ratio, 1.056; P=0.003). The positive rate of anti-HBc and alcohol intake did not differ in age- and sex-matched subjects between the LC (n=32) and HCC (n=31) groups. However, the detection rate of serum HBV DNA was higher in the HCC group (48.4%) than in the LC group (0%, P<0.001). Conclusions: Anti-HBc positivity is not a risk factor for HCC. However, occult HBV infection may be a risk factor for HCC in patients with alcoholic LC. (Korean J Hepatol 2008;14:67-76)

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Camilla Rodrigues de Almeida Ribeiro, Nathalia Alves Araújo de Almeida, Katrini Guidolini Martinelli, Marcia Amendola Pires, Carlos Eduardo Brandao Mello, José J. Barros, Vanessa Salete de Paula
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Sang Soo Lee, Sook‐Hyang Jeong, Eun Sun Jang, Young Seok Kim, Youn Jae Lee, Eun Uk Jung, In Hee Kim, Si Hyun Bae, Han Chu Lee, Mee‐Kyung Kee, Chun Kang
Journal of Gastroenterology and Hepatology.2015; 30(8): 1281. CrossRef
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International Reviews of Immunology.2008; 27(6): 427. CrossRef

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Change of HBV DNA Level as a Predictor of HBeAg Loss after Lamivudine Treatment: Jae Kwon Jung, M.D., Chang Hyeong Lee, M.D., Eun Young Kim, M.D., Jin Tae Jung, M.D., Joon Hyuck Choi, M.D., Ji Min Han, M.D., Myoung In Jin, M.D., Ju Yeon Cho, M.D., Byung Seok Kim, M.D., Im Hee Shin, Ph.D.1; Korean J Hepatol 2007;13(4):513-520.
Published online December 20, 2007; DOI: https://doi.org/10.3350/kjhep.2007.13.4.513

Abstract
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Backgroud/Aims: Lamivudine is an effective, safe therapeutic agent for the treatment of chronic hepatitis B. The aim of this study was to investigate whether early suppression of the viral load predicts HBeAg loss within 1 year during lamivudine therapy. Methods: This prospective study encompassed 74 patients (mean age: 37.1 years, male/female: 51/23) who were positive HBeAg, their AST or ALT levels were ≥2 times the upper limit of normal and their HBV DNA was ≥105 copies/mL. The patients received lamivudine 100 mg for 12 months with monitoring their HBV DNA, AST, ALT, HBeAg and anti-HBe, and all these tests were performed at pretreatment and 1, 3, 6, 9 and 12 months after treatment. The serum HBV DNA was measured by HBV branched DNA assay. Results: HBeAg loss was observed in 12 patients (16.2%), and 9 patients achieved anti-HBe seroconversion during up to 1 year of lamivudine therapy. The mean time to HBeAg loss was 5.6 months (range: 1-12 months). The posttreatment HBV DNA (<2,000 copies/mL) after 3 month (P=0.008) and 6 month (P=0.012)) were significant predictors of HBeAg loss after 1 year of lamivudine treatment on univariate analysis. Pretreatment HBV DNA, AST/ALT, gender, age and liver cirrhosis had no impact on HBeAg loss. The six-month posttreatment HBV DNA level <2,000 copies/mL was a significant predictor of HBeAg loss on multivariate analysis (P=0.008, odds ratio=0.108). Conclusion: We suggest that an HBV DNA level <2,000 copies/mL at 6 month after lamivudine therapy is the most important predictor of HBeAg loss during up to 1 year of lamivudine therapy. (Korean J Hepatol 2007;13:513-520)

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Abstract: Oral

Nucleotide Sequencing of HBV S Gene in Patients with Chronic Liver Disease and Isolated IgG Antibody to HBcAg: 윤정환, 이효석, 김정룡; Korean J Hepatol 1995;1(1):103-103.

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Abstract: Poster

B형 만성 간질환 환자들의 간조직내 HBV precore 돌연변이종에 관한 관찰: 정정명, 정해철, 설상영, 최하진, 박영홍; Korean J Hepatol 1995;1(1):120-120.

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Original Articles

Study of Long Term Follow - up of Interferon Therapy in Chronic Viral Hepatitis - in 222 cases during 127 weeks -: Jin Il Kim , Jong Soon Na , Choon Sang Bang , Soo Heon Park , Joon Yeol Han , Jeong Min Suh , Jae Kwang Kim , Young Seok Lee , Kyu Won Chung , Hee Sik Sun; Korean J Hepatol 1997;3(3):241-251.

Abstract
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Background/Aims
To evaluate the therapeutic efficacy of interferon in chrcnic viral hepatitis, interferon was administered to 222 patients with biopsy proven chronic viral hepatitis. Methods: 32 patients were excluded and the 190 patients was included, 149 men and 41 women. Average age was 34.4+-8.93 (14-67) years. 161 cases had HBsAg and HBeAg, and 29 cases had anti-HCV Ab. Three millicn units of interferon beta were given to 37 patients with chronic B hepatitis, daily for one month Six million units of interferon alpha were given to 124 patients with chronic B hepatitis and 29 patients with chr onic C hepatitis, three times a week for six months. Results: 1) Out of 124 patients with clronic hepatitis B treated with a-interferon, HBeAg negativity for more tban six months was observed in 25 patients (20.2%), and defined as responder group. The 23 patients (18.5%) were defined as probable responder, because of persistent seroregativity of HBeAg for the last 6 months, despite of fluctuation of sercangativity during the follow-up. The 29 patients (23.4%) were defined as probable non-responder because of recurrence of HBeAg, which once was cleared but reappeared during last 6 months. But there was no seroconversion in 47 cases (37.9%). The overall response rate was 38.7%. 2) Out of 37 patients with chronic hepatitis B treated with B-interferon, 7 patients (18.9%) were responder, 6 patients (16.2%) probable responder, 12 patients (32.4%) probable non-responder, 12 patients (32.4%) non-responder. The overall response rate was 35.1%. 3) Out of 29 patients with chronic hepatitis C treated with a-interferon, normalization of alanine aminotransferase (ALT) level for mcrre than six months was observed in 9 patients (31.0%), and defined as responder group. The 3 patients (10.3%) were defined as probable responder, because ALT levels fluctuated but wes normalized during the last 6 months. The 5 patients (17.2%) were defined as pobable ncn-mponder, because of persistent fluctuation of ALT levels during the last 6manths, which once were normalized but reelevated. In 12 patients (41.4%), there had never been a normalization of ALT level. The overall resporate was 41.1%. 4) The period of HBeAg seropositivity was 1.33 times longer than the period of seronegativity. The faster the seroconvmion, the more the tendency to be a respander for the patients with chronic hepatitis B. Conclusion: Interferon therapy may be effective in some cleonic viral hepatitis. (Korean J Hepatol 1997;6:241 251)

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Distinct Expressions of TGF - α among Chronic Hepatitis , Liver Cirrhosis , and Hepatocellular Carcinoma: Byeong Moo Yoo , Sung Soo Park , Dong Hoo Lee , Jung Dal Lee; Korean J Hepatol 1997;3(4):316-328.

Abstract
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Background
/Aim: Transforming growth factor-a(TGF-a) is a polypeptide cytokine related to cell proliferation and transformation. TGF- a binds to EGF receptor and stimulating DNA synthesis in liver cell. The hepatitis B virus (HBV) by itself is also believed to play a role in the hepatic carcinogenesis. Recently, it was reported that TGF- a and HBV were synergistic in action with rapid appearance of hepatocelluar carcinoma in bitransgenic mice. Although TGF- a is thought to play an important role in hepatocarcinogenesis, its expression during the natural history of HBV hepatitis was poorly understood. This investigation was performed to elucidate the dynamic changes and distinct immunohistochemical staining patterns in the course of chronic HBV hepatitis with specific reference to hepatocelluar carcinoma and to explain the role of TGF- a in the pathogenesis of hepatocelluar carcinoma. Materials/Methods: Employing TGF- a monoclonal antibody, signal detection was carried out by peroxidase-conjugated streptavidin in deparaffinized liver tissue sections taken from HBsAg positive patients. All of the liver tissue sections were proven HBV DNA positive by in situ hybridization. Immunohistochemical staining was performed in the tissue sections obtained from four normal controls, six from patients with chronic persistent hepatitis, five with chronic active hepatitis, eight with liver cirrhosis and eleven with hepatocellular carcinoma. Results: The patterns of TGF- a immunoreactivity were cytoplasmic-grain types in normal controls and chronic persistent hepatitis, honeycomb types in chronic active hepatitis, occasional cytoplasmic-flooding types in liver cirrhosis, and cytoplasmic-grape types in hepatocellular carcinoma. A Shapiro-Wilk W test for frequency table analysis for the expression of TGF- a in these different disease groups was statistically significant. Conclusion: These data suggest that step-wise distinct expression of TGF-a enhancement in HBV associated chranic liver diseases which eventually resulted in the development of hepatocellular carcinoma were conceivably due to dysregulation of liver cell cycles by both HBV and TGF- a during the persistent repetition of cell cycles. (Korean J Hepatol 1997;7:316 328)

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The Effect of Long-term Lamivudine Therapy for Chronic Liver Disease due to Hepatitis B Virus: Kwang Hyub Han, M.D., Jin Suk Kim, M.D., Hyo Young Chung1, Sang Hoon Ahn, M.D., Yong Han Paik, M.D., Kwan Sik Lee, M.D., Chae Yoon Chon, M.D. and Young Myoung Moon, M.D.; Korean J Hepatol 1999;5(2):97-104.

Abstract
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Background/Aims
: We studied to evaluate the virological and biochemical responses to lamivudine and to detect YMDD mutants in patients who received long-term lamivudine therapy. Methods : We conducted a one-year trial of lamivudine in 45 Korean patients with chronic liver disease due to hepatitis B virus. The patients were treated with a single oral average dose of 100 mg of lamivudine every day for 12 months. Results : The suppression of serum HBV DNA was sustained in 77.8% of the patients and the normalization of serum ALT in 80%. The proportions of patients with HBeAg seroconversion were 25%. YMDD mutants were detected in 4 of 8 patients who showed sustained HBV DNA and serum ALT response (n=31) and in 3 of 8 patients who showed HBV DNA or serum ALT breakthrough (n=9). The response to lamivudine therapy in HBeAg-negative patients was excellent. Conclusion : Lamivudine therapy resulted in a significant virological and biochemical improvements and were well tolerated. But, YMDD mutants were detected during lamivudine therapy. (Korean J Hepatol 1999;5:97－104)

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Persistent Negative Anti-HBc in Chronic Hepatitis B Virus Carrier -Clinical Review, HBcAg and Nucleotide Sequence of It`s Epitope in HLA A2 Heterozygotes-: Jae Heung Kim,Haak Cheoul Kim; Korean J Hepatol 1999;5(2):105-115.

Abstract
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Background/Aims
: HBcAg is the most immunogenic HBV component and anti-HBc usually persists irrespective of ongoing liver disease or clearance of the virus in human. Therefore anti-HBc is considered as the most sensitive and occasionally the only marker of the HBV infection. Nevertheless, there are a few HBsAg carrier with persistent negative anti-HBc. The epitope which responds to HBcAg is recently defined in HLA A2 from acute viral hepatitis patient due to HBV. So we studied the clinical and laboratory features and nucleotide sequence of HBcAg corresponding to HLA A2 in the HBsAg carrier with persistent negative anti-HBc. Methods : The subject of these study consists of eight HBsAg chronic carriers with persistent negative anti-HBc. We followed up the clinical features and serological markers of HBV infection and determined the amount of humoral immunoglobulin, HBV DNA and HBcAg when we performed the HLA class I typing and sequencing analysis of core of HBV. Control cases were selected from 3 HLA A2 heterozygote cases with chronic HBsAg carriers with anti-HBc. Results : All subjects had the HBsAg persistently and good health conditions with normal ranges of aminotransferase and humoral immunoglobulin. One of them was converted to anti-HBc-positive during follow-up period. The level of HBV DNA in serum was higher than 1.2 pg/mL in 7 of 8 chronic HBV carriers. There was a trend of differences between chronic anti-HBc negative carriers and converted one case to anti-HBc positive in the serum of HBcAg and HBV DNA(p=0.06). But strong positive correlation was observed between the amount of HBcAg and HBV DNA in sera. The core portion of HBV was amplified in 4 of 6 HLA A2 heterozygotes by single PCR. When sequenced the PCR products of the above 4 chronic anti-HBc negative HBV carriers and 3 control cases directly, there were no significant difference in the nucleotide and amino acid sequence at the HBcAg epitope which corresopond to class 1 HLA A2. Conclusions : Our results show that persistent anti-HBc negative chronic HBV carriers may be caused by large amounts of HBV DNA and HBcAg in their sera and not by variants of HBV. These suggested that active viral replication was going on, but are undetectable by the available commercial tests due to binding with excessive amount of HBcAg in the HBV carriers with persistent negative anti-HBc. (Korean J Hepatol 1999;5:105－115)

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Emergence of YMDD Motif Mutant Hepatitis B Virus during Short-term Lamivudine Therapy: Yong Han Paik,Kwang Hyub Han,Hyo Young Chung,Chae Yoon Chun,Young Myoung Moon; Korean J Hepatol 1999;5(3):173-183.

Abstract
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Background/Aims
The emergence of lamivudine-resistant mutant hepatitis B virus (HBV), with aminoacid substitution in the YMDD motif of DNA polymerase, has been reported in the long-term lamivudine use group. However there is no report about the emergence of mutant viruses during the short-term lamivudine therapy. The objective of this study was to investigate the emergence of YMDD mutant HBV during short-term lamivudine therapy. Methods: We evaluated twenty-eight chronic hepatitis B patients who were HBeAg and HBV DNA positive and treated with lamivudine 100mg p.o. daily for 12 weeks. First, we investigated the emergence of YMDD mutants by nested polymerase chain reaction (PCR) method developed by Chayama et al in 19 patients who lost HBV DNA during lamivudine therapy but showed HBV DNA re-emergence 2 weeks after the end of therapy. Second, DNA subcloning and sequencing of HBV DNA polymerase including YMDD motif was undertaken in one patient's serial blood samples at 0, 8, 12 weeks to confirm the results of nested PCR. Results: YMDD motif mutation was detected in 17(90%) out of 19 patients at the end of therapy and the type of mutations were YIDD only. At the end of therapy, mutant was predominant in 5 patients, both mutant and wild type were similar in proportion in 3 patients, and wild type was predominant in 9 patients. When we carried out nested PCR serially with samples of 0, 2, 4, 8, 12, 14 weeks after initiation of therapy in 5 patients who were mutant predominant at 12 weeks, YIDD mutant began to be detected from 2 weeks in 4 patients and from 4 weeks in one patient. However, rapid turnover from mutant to wild type happened after the end of therapy, so only wild type was detected in 3 patients and wild type became predominant in 2 patients at 2 weeks after the end of therapy. All the sequencing results of serial blood samples in one patient were consistent with nested PCR data. Conclusions: The presence of YMDD motif HBV polymerase mutant may be possible before administration of lamivudine in Korean chronic hepatitis B patients. Nested PCR assay would be an useful method to detect YMDD mutant. (Korean J Hepatol 1999;5:173－183)

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Identification of eplication-Competent Dimeric Human Hepatitis B Viral Using PCR Screening Technique: Seok Hyun Nam, Ph.D.1, Sung Won Cho, M.D.2; Korean J Hepatol 1999;5(3):184-189.

Abstract
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Background/Aims
Transfection of the hepatitis B virus (HBV) genome requires the cloning of tandem HBV sequences inserted into a plasmid vector, which is usually screened for by the restriction enzyme digestion of plasmid minipreparation from at least a dozen of bacterial colonies. The aim of this study was to develop a simple alternative screening method for bacterial colonies harbouring tandem HBV sequences by a PCR. Methods: A set of polymerase chain reaction (PCR) primer was designed to detect the bacterial colonies harbouring "head to tail" dimeric HBV DNA. PCR which amplifies the head to tail junction site of two tandem HBV molecules was performed. Results: PCR products with appropriate size (1.2kb) were obtained. The accurate detection by PCR screening technique was confirmed by enzyme digestion. Conclusions: These results suggest that PCR screening technique is a simple and rapid method for the identification of bacterial colonies containing tandem HBV sequences. (Korean J Hepatol 1999;5:184－189)

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A Prospective Study of Therapeutic Effect of 6 Months Trial with Lamivudine in Patients with Chronic Viral Hepatitis B: Chang Woo Gham,Soong Hwan Lee,Seung Woo Nam,Seung Woo Nam,Byung Joo Roh,Dong Hoo Lee; Korean J Hepatol 1999;5(4):282-290.

Abstract
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Background/Aims
The purpose of this study was to evaluate the effectiveness of lamivudine treatment in patients with chronic liver disease caused by chronic infection of hepatitis B virus (HBV). Methods: Thirty-five patients with chronic infection of HBV were included in this study who were diagnosed at Hanyang University Hospital from January 1998 to January 1999. They received 150mg of lamivudine per oral once daily for 6 months with follow-up of liver function test, serum HBV DNA and serologic markers for hepatitis B virus every two months. Lamivudine was well tolerated. Eight patients underwent liver biopsies before entering the study and follow-up biopsies were done at 5 patients. Results: Out of all 35 patients, chronic hepatitis patients histologically confirmed were 8, chronic hepatitis patients clinically diagnosed were 25 and liver cirrhosis patients clinically diagnosed were 2. The mean age was 35.7 years. Male-female ratio was 2.2:1. There was no hepatitis B surface antigen (HBsAg) negative seroconversion. The HBeAg loss rate was 26.9%(7/26) and HBeAg seroconversion rate was 10.7%(3/28) at the end of follow-up. Ten patients were anti-HBe positive prior to treatment, 3 of them became anti-HBe negative at the end of follow-up. Five patients underwent follow-up liver biopsies, in which histologic improvements were shown in 4 cases. Serum replicative HBV DNA by bDNA assay was decreased in all patients and HBV DNA was undetectable in 52.9%(9/17) at the end of treatment. Out of the 15 patients with abnormal alanine aminotransferase (ALT) levels at baseline, ALT level in 7 patients(46.7%) was normalized at treatment completion. Pretherapy ALT level was the only predictive factor for loss of HBeAg by stepwise logistic regression analysis(odds ratio : 1.0208) (95% Confidence Interval : 1.0023 ∼ 1.0396) (p value=0.0271). Conclusions: Lamivudine induced sustained suppression of HBV replication during treatment in all patients. In treating patients with lamivudine, who had chronic liver disease due to chronic infection of HBV, the improvement of liver function test and suppression of viral replication appeared early and was sustained during the 6months treatment. This, in turn, may induce histological improvement as well. Pretherapy ALT level was the only predictive determinant for HBeAg loss during lamivudine therapy, and that should be kept in mind in selecting patients for treatment. (Korean J Hepatol 1999;5:282－290)

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Sequence Analysis of `a` Determinant in Two Patients with De Novo HBV Infection after Renal Transplantation: Byung Hyun Choe, M.D., Kwang Hyub Han, M.D., Hyo Young Chung1 Yong Han Paik, M.D., Jung Il Chung, M.D., Yoo Sun Kim, M.D.2 Chae Yoon Chon, M.D. and Young Myoung Moon, M.D.; Korean J Hepatol 1999;5(4):291-298.

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Background/Aims
HBV infection can be seen after organ transplantation. The presence of anti-HBs in serum means protection from HBV infection. If amino acids were mutated in 'a' determinant which was a common antigenic epitope of HBsAg, escape from humoral immunity can occur. Recently, in chronic HBV infected patients who received liver transplantation but reinfected by HBV, many authors reported mutations in 'a' determinant sequence. However, in renal transplantation, there were few reports about HBV infection and 'a' determinant mutation after transplantation. Therefore, we studied the incidence of HBV reinfection after renal transplantation and also tried to analyze 'a' determinant sequence in those patients. Methods: We reviewed HBsAg-negative patients who received renal transplantation in our hospital, but turned HBsAg positive after transplantation. We selected two patients who were anti-HBs positive before transplantation but turned HBsAg positive after transplantation, and analyzed 'a' determinant of amino acid sequence of these patients. Results: Among 1682 patients who were HBsAg negative before transplantation, 21 patients were turned HBsAg positive after transplantation. Among them, 6 patients were anti-HBs positive before transplantation. Sequence analysis of the 'a' determinant amino acid in two patients whose HBsAg turned positive after transplantation revealed no evidence of mutation in comparison with previously reported subtype 'a' determinant sequences. Conclusion: In renal transplantation, HBV could be reinfected in patients who had been anti-HBs positive before transplantation even without mutation in 'a' determinant region. (Korean J Hepatol 1999;5:291－298)

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Improved Child-Pugh Score after Lamivudine Treatment in Patients with Decompensated Cirrhosis Due to Hepatits B Virus Infection: Moon Suk Choi,Seung Woon Baek,Sang Jong Park,Joon Hyuk Lee,Gwang Chul Ko,Poong Ryul Lee,Jae Joon Kim,Jong Chul Lee,Gyu Wan Choi; Korean J Hepatol 2000;6(4):481-487.

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Background/Aims
Lamivudine is an oral nucleoside analogue with potent antiviral activity against HBV inducing normalization of ALT and improvement of necro-inflammation and fibrosis in chronic hepatitis B. But its role in decompensated cirrhosis has not been established. The Child-Pugh score is a reliable and convenient prognostic indicator reflecting liver synthetic function. We evaluated the incidence of any improvement in Child-Pugh score after lamivudine treatment in patients with decompensated cirrhosis. Methods: Twenty-six patients with HBV associated active decompensated cirrhosis showing detectable serum HBV received lamivudine (100 or 150 mg/day) for 6-45 months (median 16). The Child-Pugh score at 6th month of lamivudine treatment was compared with base line score. Results: The Child-Pugh score improved ( 2-point reduction) in 17 (65.4%) patients, was constant in 8 (30.8%), and aggravated ( 2-point increase) in one (3.8%) of 26 patients. HBV DNA was initially cleared in 24 cases (92.3%) but breakthrough developed in 7 (29.2%). HBeAg was lost in 5 (25%) of 20 cases. Initial improvement was maintained in 14 (82.4%) of 17 cases but aggravated with breakthrough in 3 (17.6%). Two of 5 patients waiting for liver transplantation showed marked improvement and were removed from the list. Conclusion: Lamivudine can be an effective treatment for patients with decompensated cirrhosis due to HBV infection, improving the Child-Pugh score in many cases. However, deterioration of liver function associated with DNA breakthrough was an important problem in patients showing initial improvement.

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Editorial

Which Method Is Appropriate in Defining the Responsiveness to Lamivudine?: Han Chu Lee,Dong Jin Suh; Korean J Hepatol 2001;7(1):1-5.

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ALT, alanine aminotransferase; anti-HBe, antibody to hepatitis B virus e antigen; cccDNA, covalently closed circular DNA; HBcAg, hepatitis B virus core antigen; HBeAg, hepatitis B virus e antigen; HBsAg, hepatitis B virus surface antigen; HBV, hepatitis B virus; HBx, hepatitis B virus x protein; LHBs, large hepatitis B virus surface antigen; MHBs, middle-sized hepatitis B virus surface antigen; PCR, polymerase chain reaction; SHBs, small hepatitis B virus surface antigen.

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Original Articles

A Study on The Chang of HBsAg Anti - HBs Positivities for A Recent 15 Year Period in Korea: Soo Jung Lee, M.D., Ho Young Na, M.D., Min Ho Park, M.D., Geun Soo Park, M.D., Sung Kyu Choi, M.D., Kang Jin Lee, M.D.*, Jai Dong Moon, M.D.*, and Sei Jong Kim, M.D.; Korean J Hepatol 2001;7(3):299-307.

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Background/Aims
The HBsAg positivity in the normal Korean population has been reported as 2-10%. It has been decreasing since hepatitis B vaccine was introduced to routine vaccination regimens in 1992. Reports on the changes of anti-HBs over the years are hard to find since the discrepancies in sensitivities of test methods used by different researchers did not allow equivalent comparisons. The purpose of this study was to evaluate the changes of HBsAg and anti-HBs posivities for a recent 15 year period.Methods:From 1998 to 2000, 4771 subjects in Chonnam province were included in this study. Serum HBsAg and anti-HBs were detected by reversed passive hemagglutination(RPHA) and passive hemagglutination(PHA) respectively. The changes in the HBsAg and anti-HBs positivity by the same test methods for the period were analyzed by comparing our results with those of 12 other previous reports.Results:The positivities of HBsAg and anti-HBs were 5.3% and 47.5%. The positivity of HBsAg was significantly higher in males, while that of anti-HBs was significantly lower in males(p<0.01). There was a significant difference of HBsAg and anti-HBs positivities among age groups which were arbitrarily divided by decade(p<0.01). But there was no correlation between age and the positivities. In the HBsAg positive group and the anti-HBs negative group, abnormality in ALT level(ALT>40) was significantly higher statistically(p<0.01). The positivity of HBsAg decreased with years(r=-0.845, p<0.01), while that of anti-HBs increased with years(r=0.616, p<0.05).Conclusion:The positivity of HBsAg has significantly decreased and that of anti-HBs has increased with years for the period under study.(Korean J Hepatol 2001;7:299-307)

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Distribution of HBV Genotypes in Patients With Chronic HBV Infection in Korea: Soong Hwan Lee, M.D., Sung Hee Han, M.D., Seung Chul Cho, M.D., Byung Joo Roh, M.D., Joo Hyun Sohn, M.D., Duck An Kim, M.D. *, Dong Hoo Lee, M.D., and Choon Suhk Kee, M.D.; Korean J Hepatol 2001;7(4):373-380.

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Background
/ Aims : Choronic HBV infection is associated with a wide spectrum of clinical manifestations, including asymptomatic carrier state, choronic hepatitis, liver cirrhosis, and hepatocellular carcinoma. Genotypically, HBV genomes have been calssified into seven groups, designated A to G. Several studies have suggested recently that HBV genotypic difference influence the severity of liver disease and clinical outcomes. The distribution of HBV genotypes in Korea and its clinical relevance are poorly understood. We investigated the prevalence of HBV genotypes in Korea and the association between the distinct genotypes and the severity of liver disease. Methods : A total of 214 HBV-DNA positive serum samples, were used for the genotyping. All patients were HBV-bDNA positive chronic HBsAg carries. 199 patients were histologically verified with liver cirrhosis(6), chronic hepatitis(192) and fatty liver(1). The other patients were clinically diagnosed with liver cirrhosis(13) or hepatocelluar carcinoma(2). HBV genotype was determined by PCR using type-specific primers. Results : Genotyping was possible in all patients. Out of 214 patients, 213(99.5%) were HBV genotype C. Only one(0.5%) was genotype A, The patient with genotype A had minimal hepatitis as diagnosed by liver biopsy. Conclusions : These results indicate that almost all chronic HBV infections are genotype C in Korea. HBV grnoytpic difference therefore dose not influence the clinical outcome of HBV infection in Korea. Because genotype C may be associated with more severe liver disease, the predominance of genotype C in Korea may result in more severe outcomes than in other countries where other genotypes are predominant. (Korean J Hepatol 2001;7 :373 - 380)

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The Hepatitis B Carrier Rate in Siblings of Patients with HBV - associated Chronic Liver Disease: Hwi Kong, M.D., Ji Hoon Kim, M.D., Nam Young Cho, M.D., Yoon Hong Kim, M.D., Kil Man Jung, M.D., Jong Eun Yeon, M.D., Jae Seon Kim, M.D., Young Tae Bak, M.D., Kyung Hwan Cho, M.D.*, Yong Kyu Park, M.D.† , Kwan Soo Byun, M.D., and Chang Hong Lee, M.D.; Korean J Hepatol 2001;7(4):387-391.

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Background
/ Aims : This study aimed to estimate the seroepidemiology of hepatitis B virus(HBV) infection with emphasis on the transmission of HBV infection between mother`s and their children. Methods : For 452 patients with HBV associated chronic liver disease, and 1,098 of their offspring, who visited Korea University Kuro Hospital from February, 2000 to February,2001, HBsAg was tested by radioimmunoassay. Results : Among siblings whose mothers were HBsAg - positive, the overall prevalence rate of HBV infection was 44.9%(140/312) and decreased with decreasing age(54.7% in ≥ 20 years old age group, 33.3% in 10-19 years old age group, 7.6% in < 10 years old age group). The estimated proportion of perinatal infection out of modes of HBV transmissions in the general population was 38% in < 10 years and 63.4% in 10-19 years. Conclusion : The present hepatitis B vaccination strategies-especially against perinatal infection of Korea have performed to their utmost. More effective methods for prevention of HBV transmission are now needed. (Korean J Hepatol 2001;7 :387- 391)

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The Correlation Between The Histologic Activity and Fibrosis and The Distribution of Intrahepatic HBsAg and HBcAg in Patients With Chronic Hepatitis B: Kwang Bum Cho, M.D., Jung Ho Sohn, M.D., Kyung Sik Park, M.D., Du Young Kwon, M.D., Jae Seok Hwang, M.D., Jung Wook Hur, M.D., Sung Hoon Ahn, M.D., Soong Kuk Park, M.D., and Sang Pyo Kim, M.D.*; Korean J Hepatol 2001;7(4):401-412.

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Background
/ Aims : The purpose of this study was to assess the correlation between histologic activity and fibrosis and the distribution of intrahepatic hepatitis B core antigen(HBcAg) and surface antigen(HBcAg ) inpatients with chronic hepatitis B . Methods : 141 patients(M:F=141:27) with biopsy-proven chronic hepatitis B ,abnormal liver function, and a positive HBV viral marker(serum HBeAg , serum HBV DNA) were enrolled. Results : HBcAg was expressed in 96 of 141 patoents(68.1%), n HBcAg in 23(16.3%), c HBcAg in 58(41.25), and n-c HBcAg in 15(10.6%). In the cases of HBsAg, 114 of 141 patients(80.9%) were expressed as c HBsAg, 2(1.4%) as m HBsAg, and 16(11,3%) as m-c HBsAg. The presence of intrahepatic HBcAg and HBsAg according to gudat`s calssification was not correlated with activity and fibrosis. But the groups with nuckear expression of HBcAg revealed less inflammatory activity (grade, p=0.003), and less fibrotic stage(p=0.002) than with cytoplasmic or no expression of HBcAg. HBsAg was not. Conclusion : These observations suggest that inflammatory activity and fibrosis of chronic hepatitis B are related to the presence of HBcAg in hepatocytes and the expression of HBcAg. This is a very important finding in hepatocytolysis. (Korean J Hepatol 2001;7 :401- 412)

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Prevalence of HBV Genotypes in Korean Patients with Chronic Hepatitis B: Il Hyun Cho,Jung Youp Song,Deog Ki Kim,Hong Seok Lim,Seung Soo Sheen,Won Seok Kim,Kee Myeong Lee,Ki Baik Hahm,Jin Hong Kim,Sung Won Cho; Korean J Hepatol 2001;7(4):381-386.

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Background
/ Aims : Hepatitis B virus(HBV) genotype have distinct geographic distributions. The possibility of pathogenic difference among HBV genotypes has been suggested. We investigated the prevalence of HBV genotypes in Korea and the association between distinct genotypes and clinical outcomes. Methods : Using a PCR-RFLP and sequencing, HBV genotypes were determined in 136 patients with chronic type B hepatitis. Results : The genotype C was detected in 131 patients(96.3%), and other 5 patients(3.7%) had genotype B. There were no significant differences in sex, age, disease duration, ALT level, HBeAg/anti-HBe status, or HBeAg loss between genotype B and C patients. Conclusion : These results suggest that almost all patients with chronic hepatitis B are infected with genotype C. Genotypes do not influence the outcome of chronic hepatitis B patients in Korea. (Korean J Hepatol 200 1;7 :38 1- 386 )

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HBV DNA Levels, Aminotransferase and Histological Activity in Young Male Patients with HBeAg Positive Chronic Hepatitis B: Seung Chul Cho,Soong Hwan Lee,Joon Jae Shinn,Sung Hee Han,Byung Joo Roh,Joo Hyun Sohn,Dong Hoo Lee,Choon Suhk Kee; Korean J Hepatol 2002;8(1):44-51.

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Background
/Aim: A significant correlation between HBV DNA and liver damage was found in precore mutant strains but there was no significant association between viral replication and liver damage in HBeAg positive patients. Laboratory tests are often requested to predict hepatitis activity (grade) and fibrosis (stage) in HBeAg positive chronic hepatitis B. We assessed ALT, AST, and HBV-branched DNA to find which is the best for predicting hepatitis activity and fibrosis. Methods: Routine biochemical liver function tests and HBV DNA in sera were assessed in 119 young patients positive with HBsAg and HBeAg. The mean age of patients was 21±2 years. All patients were male. By logistic regression analysis the relationships between laboratory data, hepatitis activity, fibrosis, or risk of chronic active hepatitis were analyzed. Results: There was a significant correlation between aminotransferase (AST, ALT) and hepatitis activity/ fibrosis. A significant inverse relationship between the HBV bDNA and hepatitis activity was demonstrated (Pearson's correlation coefficient: lobular activity,-0.305; porto-periportal activity, -0.410). But HBV bDNA was not correlated with severity of fibrosis. AST and HBV bDNA was the important test for predicting the more severe hepatitis activity (lobular activity and porto-periportal activity: score≥3, respectively) Conclusion: The higher AST, but the lower HBV bDNA, in sera shows the more severe hepatitis activity. AST and HBV bDNA could be helpful for assessing the hepatitis activity in young male patients with HBeAg positive chronic hepatitis B if proper reference values are used.(Korean J Hepatol 2002;8:44-51)

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Direct Analysis of HBV - Specific CD8+ Lymphocyte By Tetrameric HLA-A2/core 18-27 Complex in Chronic Hepatitis B: Chun Kyon Lee, M.D., Jeong Hun Suh, M.D., Young Suk Cho, M.D., Kwang-Hyub Han, M.D.*, Jae Bock Chung, M.D.*, Chae Yoon Chon, M.D.*, Young Myoung Moon, M.D.*; Korean J Hepatol 2002;8(2):139-148.

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Backgrounds/Aims
Hepatitis B virus(HBV) specific cytotoxic T lymphocyte (CTL) response is believed to play a major role in virus control and liver damage in chronic hepatitis B(CHB). We performed this study to evaluate whether HBV specific CTL could be visualized directly by tetrameric HLA-A2/core 18-27 complex(Tc18-27) in the peripheral blood and liver of patients with CHB. On the basis of our results we clarified patients intrahepatic compartmentalization and correlation with HBV specific CTL and viral replication or liver damage. Methods: We stained peripheral blood mononuclear cells of 33 HLA-A2 + and 8 HLA-A2 patients with CHB with cychrome conjugated anti-CD8 mAb and phycoerythrin conjugated T c18-27. Among these we analysed intrahepatic lymphocyte of 11 HLA-A2 + patients. We compared the frequency of T c18-27 specific CD8+ cells with serum HBV-DNA levels or alanine aminotransferase(ALT) levels. Results: The frequency of circulating T c18-27 specific CD8+ cell was higher(9-101 cells per 50,000 CD8+ cells) than background level in 14 among 33 patients. The frequency of intrahepatic T c18-27 specific CD8+ cells was 12-2100 cells per 50,000 CD8+ cells in 8 out of 11 patients whose liver was obtained This was 17.4-150 times higher than circulating T c18-27 specific CD8+ cells. The frequency of circulating T c18-27 specific CD8+ cells was increased in 10 out of 18 patients with serum HBV DNA level <0.5 pg/mL and ALT < 40 IU/L. It was increased in just 4 out of 15 patients with HBV DNA level > 800 pg/mL and ALT >70 IU/L. The frequency of intrahepatic T c18-27 CTL tended to be lower in high levels of serum HBV DNA and was not correlated with liver inflammation. Conclusion: This study provess that if HBV-specific CTLs are barely detectable in the peripheral blood of CHB, much more HBV-specific CTLs are in the liver and most HBV-specific CTLs are infiltrated in the liver. Also, in the presence of an effective HBV specific CD8 response the inhibition of viral replication can be independent of liver damage.(Korean J Hepatol 002;8:139-148)

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The Clinical Significance of Quantitation of HBV DNA in Serum : Comparison of the Branched-DNA Assay with the Second-Generation Digene Hybrid Capture Assay and Long-term Observation: Eun Jung Jun, M.D., Joon-Yeol Han, M.D., Hwang Choi, M.D., U Im Chang, M.D., Tae Kyu Lee, M.D., Young Hwan Kim, M.D., Jin Il Kim, M.D., Soo Heon Park, M.D., Jae Kwang Kim, M.D., Kyu Won Chung, M.D. and Hee Sik Sun, M.D.; Korean J Hepatol 2002;8(2):157-166.

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Backgrounds/Aims
Serum levels of hepatitis B virus (HBV) DNA are direct measures of viral replication in epatocytes. We compared branched- DNA assay (QuantiplexT M, bDNA) and Hybridization Capture II (HCII), and evaluated the clinical significance of HBV DNA quantitation in the natural course of HBV infection. Methods: We analyzed results of bDNA in 324 serum samples from 83 untreated male patients with chronic hepatitis B. Mean follow up period was 11.8 years. HCII was also performed in 157 arbitrarily selected samples. Results: HBV DNA levels measured with two assays were very similar (r²=0.893, p< 0.0001). HBV DNA detection rate of HCII was 6.4% higher than that of bDNA in HBeAg positive samples. HBV DNA detection rate was higher in cases with higher ALT . Among 73 patients with initial diagnosis of chronic hepatitis, 38 patients (52.1%) experienced progression to cirrhosis, and hepatocellular carcinoma (HCC) was developed in 9(12.3%). HCC was developed in 5 (50.0%) of 10 patients with initial diagnosis of cirrhosis. While HBeAg positive rates during chronic hepatitis, cirrhosis and HCC were 57.8%, 55.0% and 14.3%, respectively ( p=0.006), HBV DNA detection rates were 70.6%, 64.0% and 42.9%, respectively ( p=0.08). Especially in HCC, the discrepancy between HBeAg positive rate and HBV DNA detection rate may suggest the appearance of variants which cannot produce HBeAg. Conclusion: Both HCII and bDNA were similar HBV DNA quantitation assays for clinical use. HBV DNA level correlated with the severity of liver disease. Screening tests for HCC should be recommended in patients whose HBeAg is negative and have detectable HBV DNA. (Korean J Hepatol 2002;8:157-166)

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Chemokine Receptor Expression of Hepatitis B Virus-Specific CD8⁺ Lymphocyte in Chronic B Viral Infection: Chun Kyon Lee, M.D.1, Jeong Hun Suh, M.D.1, Young Suk Cho, M.D.1, Kwang-Hyub Han, M.D.2, Jae Bock Chung, M.D.1,2, Chae Yoon Chon, M.D.2 and Young Myoung Moon, M.D.2; Korean J Hepatol 2002;8(4):363-370.

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Background/Aims
The protective role of HBV-specific CD8⁺ cells is dependent on their ability to efficiently migrate to the infected liver, where they may exert an effector function. The migratory behavior of CD8⁺ cells is influenced by their expression of different chemokine receptors. This study was intended to analyse the pattern of chemokine receptor expression of HBV specific CD 8+ cells in chronic B viral infection. Methods: We analysed the CCR5 and CCR3 profile of HBV-specific CD8⁺ cells isolated from the blood and liver of patients with different patterns of HBV infection. Purified T cells were stained directly ex vivo, or after antigen-specific stimulation, using HBV peptide-specific HLA tetramers and monoclonal antibodies to CD8, CCR5 and CCR3, with analysis by flow cytometry. Results: In patients with chronic hepatitis B characterised by low levels of virus (serum HBV DNA <0.5pg/mL) and minimal liver inflammation, analysis of circulating and intrahepatic CD8⁺ cells demonstrated that liver infiltrating Tc18-27-specific cells were preferentially CCR5+ (up to 80% of HBV-specific CD8⁺ cells), in contrast to cells of the same specificity within the circulating compartment (up to 35% of HBV-specific CD8⁺ cells). Furthermore, CCR3 was expressed by about 10% of Tc18-27+ cells infiltrating the liver, but was absent from circulating cells. Following HBV-specific stimulation in vitro the CCR5 expression of circulating Tc18-27-specific cells was up-regulated, to levels found in liver infiltrating cells, whereas CCR3 expression was unchanged. Conclusions: The chemokine receptor profile of HBV-specific CD8⁺ cells is influenced by the anatomical site of these cells, and the clinical pattern of disease. The ability of circulating HBV-specific CD8⁺ cells of patients with low replicating virus to upregulate CCR5 suggests that these cells may respond to increases in virus replication by efficiently migrating into the infected liver. (Korean J Hepatol 2002;8:363-370)

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Clinical and Virologic Characteristics of Lamivudine Resistance in HBV-associated Chronic Liver Disease: Sun Suk Kim, M.D., Moon Gi Chung, M.D., Ki Tak Ju, M.D., Dong Kyun Park, M.D. Oh Sang Kwon, M.D.,Yang Suh Koo, M.D., Yu Kyung Kim, M.D., Duck Ju Choi, M.D. Yu Jin Hwang, Ph.D.* and Ju Hyun Kim, M.D.; Korean J Hepatol 2002;8(4):405-417.

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Background/Aims
Lamivudine therapy in chronic hepatitis B has been shown to be effective in inhibiting HBV replication. However, lamivudine resistance has been developed with prolonged use. We studied to etermine the prevalence, predictive factors, and clinical outcomes of lamivudine resistance. Mutations in YMDD motif of HBV polymerase, which have been associated with lamivudine resistance, were also assessed. Methods: 170 patients with HBV-associated chronic liver disease who have received lamivudine for at least one year, were studied. The clinical, biochemical, and virologic characteristics were analyzed and compared according to presence (resistance group) or absence (non-resistance group) of DNA breakthrough. Their clinical outcomes were regularly followed. Stored sera before treatment and after DNA breakthrough were examined for detection of HBV polymerase mutation by direct sequencing and/or RFLP. Results: Cumulative rates of lamivudine resistance after one and two years of treatment were 11% and 34%, respectively. In the resistance group, as compared to the non-resistance group, age, the presence of HBeAg before treatment, and disappearance of HBeAg during treatment, were significantly different. The predictive factors associated with lamivudine resistance were not found. ALT and HBV-DNA level after lamivudine resistance was variable, but jaundice or hepatic failure was absent. Mutation in YMDD motif was detected in 73% and other variable mutations were detected before treatment and after DNA breakthrough. Conclusions: Lamivudine resistance increases the longer the duration of treatment and clinical outcomes are variable. The mutation in YMDD motif was found in about 2/3 of cases. Other causes for lamivudine resistance may be considered. (Korean J Hepatol 2002;8:405-417)

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Serum ALT and HBV DNA Levels in Patients with HBeAg-Negative Chronic Hepatitis B: Kyung Hwan Kim, M.D., Il Hwan Na, M.D., Jae Moon Cha, M.D., Yong Ki Cho, M.D., Se Young Park, M.D., Hyoung Pil Kim, M.D., Chul Soo Song, M.D., Jeong Heo, M.D.1 and Mong Cho, M.D.1; Korean J Hepatol 2003;9(4):284-292.

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Background/Aims
HBeAg-negative chronic hepatitis B (CHB) has a poor long-term prognosis. Since no precise clinically relevant HBV thresholds are known in HBeAg-negative CHB, the decision to treat is difficult. The aim of this study was to evaluate the levels of serum HBV DNA and transaminase and to investigate the correlation of these values in patients with HBeAg-negative CHB. Methods: The study analyzed the sera from 82 patients with HBeAg-negative CHB, 61 men and 21 women. The mean age was 45 years. The patients were divided into two groups according to serum ALT levels: the patients with lower ALT level (n=52, UNL<ALT<2×UNL) and higher level (n=30, ALT≥ 2×UNL). The level of serum HBV DNA was determined by the Cobas Amplicor HBV Monitor™ (Roche). Results: The median serum HBV DNA level was 2.7×10⁵ copies/mL in patients with HBeAg-negative CHB. The median serum HBV DNA level of patients with a higher ALT level (1.0×10⁶ copies/mL) was significantly higher than that of patients with a lower ALT level (5.6×10⁴ copies/mL)(p<0.001). The serum ALT level was correlated with serum HBV DNA levels in patients with HBeAg-negative CHB (r=0.416, p<0.001). The serum level of HBV DNA in patients with cirrhosis (median 2.0×10⁵ copies/mL) did not differ from patients without cirrhosis (median 4.7×10⁵ copies/mL). Conclusions: The level of serum HBV DNA was higher in patients with higher serum ALT level than it was in patients with lower serum ALT, and it was closely correlated with serum ALT levels in HBeAg-negative CHB.(Korean J Hepatol 2003;9:284-292)

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Reappraisal of HBV Genotypes and Clinical Significance in Koreans Using MALDI-TOF Mass Spectrometry: Jung Min Lee , Sang Hoon Ahn , Hye Young Chang , Ji Eun Shin , Do Young Kim , Myoung Ki Sim , Sun Pyo Hong , Hyun Jae Chung , Soo Ok Kim , Kwang Hyub Han , Chae Yoon Cho; Korean J Hepatol 2004;10(4):260-270.

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Background/Aims
Recent studies have shown that the genotype of hepatitis B virus (HBV) may correlate with the disease natural history and treatment outcome. However, several of these studies used low sensitivity assays in a small number of patients, and

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Review

Treatment of Chronic Hepatitis B ; Monitoring Patients with Chronic HBV Infection During Antiviral Therapy: Yun Soo Kim; Korean J Hepatol 2005;11(1):9-12.

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Original Article

HBV-specific CD8⁺ T cells for Sustained HBeAg Seroconversion after Lamivudine Therapy: Chun Kyon Lee, M.D., Kwang-Hyub Han, M.D.1,2, Jeong Hun Suh, M.D., Young Suk Cho, M.D., Sun Young Won, M.D., Chae Yoon Chon, M.D.1, Young Myoung Moon, M.D.1 and In Suh Park, M.D.; Korean J Hepatol 2005;11(1):34-42.

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Background/Aims
Viral suppression of the hepatitis B virus (HBV) can be induced by lamivudine, but the relapse seen in many patients after cessation of lamivudine therapy is troublesome. We thought that the host immune response is important to prevent viral relapse. We compared the frequency of HBV-specific CD8⁺ T cells in the peripheral blood and their expansion capacity after exposure to viral antigen between the patients showing sustained HBeAg seroconversion after use of lamivudine and those patients without sustained response. Methods: We analyzed HBV-specific CD8⁺ T cells that were isolated from the blood of 14 patients with HLA-A2 who showed lamivudine induced HBeAg seroconversion (HBV DNA < 0.5 pg/mL, and the cells were negative for HBeAg) at the end of lamivudine therapy. The purified T cells were directly stained ex vivo, after they had been stimulate with synthetic peptide, using the HBV core 18-27-specific HLA tetramer (Tc _18-27) and monoclonal antibody to CD8. The HBV viral load was quantified by the Amplicor HBV Monitor assay. Results: In patients with a sustained HBeAg response (the sustained group) for a duration of 15.5 months of follow-up, the median number of Tc _18-27 cells out of the 5×10⁴ CD8⁺ T cells was 49.5 (15-135). On the contrary, in patients who experienced relapse (the relapsed group) during a median of 7.5 months of follow-up, the median number of Tc _18-27 cells out of the 5×10⁴ CD8⁺ T cells was 13.5 (0-95). Especially, among patients with a viral load of HBV DNA < 1×10³ copies at the end of treatment, the median number of Tc _18-27 cells out of 5×10⁴ CD8⁺ T cells was 87 (45-135) in sustained group compared to 12 (6-50) in the relapsed group. All patients in the sustained group demonstrated a vigorous expansion of the core 18-27-specific CD8⁺ T cells after stimulation with viral peptide, in contrast to only 3 out of 8 patients in the relapsed group. Conclusions: This study demonstrates that the frequency and functional responsiveness of the circulating HBV-specific CD8⁺ T cells may be important for obtaining a sustained HBeAg response to lamivudine. (Korean J Hepatol 2005;11:34-42)

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Article category

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"HBV"

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Reply to Correspondence

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Viral hepatitis

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Viral hepatitis

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Hepatic neoplasm

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Viral hepatitis

Editorials

Viral hepatitis

Viral hepatitis

Letters to the Editor

Viral hepatitis

Viral hepatitis

Editorial

Viral hepatitis

Review

Viral hepatitis

Original Articles

Viral hepatitis

Viral hepatitis

Review

Viral hepatitis

Original Article

Viral hepatitis

Review

Viral hepatitis

Original Articles

Viral hepatitis

Abstract: Oral

Abstract: Poster

Original Articles

Editorial

Original Articles

Review

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