Your search keyword '"Jin-Hai, Chang"' showing total 4 results

1. Polymorphism of OAS‐1 determines liver fibrosis progression in hepatitis C by reduced ability to inhibit viral replication

Author

Jin-Hai Chang, Takao Kawabe, Radsamee Sermsathanasawadi, Run-Xuan Shao, Ryosuke Muroyama, Narayan Dharel, Naoya Kato, Masao Omata, and Chang-Zheng Li

Subjects

Adult, Liver Cirrhosis, Male, Cirrhosis, Genotype, Hepatitis C virus, SNP, Single-nucleotide polymorphism, Biology, medicine.disease_cause, Virus Replication, Polymorphism, Single Nucleotide, Clinical Studies, medicine, 2',5'-Oligoadenylate Synthetase, Humans, JFH1, Allele, Genotyping, Aged, Aged, 80 and over, Hepatology, cirrhosis, fibrosis, Hepatitis C, Hepatitis C, Chronic, Middle Aged, medicine.disease, Virology, Viral replication, Disease Progression, Female, Interferons, replicon

Abstract

Background: Progression of disease after hepatitis C virus (HCV) infection differs among individuals, indicating a possibility of participation of host genetic factors. 2′-5′-oligoadenylate synthetase 1 (OAS-1), an important component of the innate immune system, has an antiviral function, and may therefore have a certain relationship with progression of disease. Aim: To evaluate single nucleotide polymorphisms (SNPs) of OAS-1 and its relationship with the disease status of HCV infection. Methods: Six SNPs of OAS-1 were selected and examined in 409 Japanese patients with chronic HCV infection using the TaqMan PCR genotyping method. The relationship of SNP genotypes and clinical manifestations of patients was analysed. Then, a pair of OAS-1-expression plasmids mimicking the clinical-related SNPs were created and transfected into liver cells carrying the HCV subgenomic replicon or the full-length genome, JFH1, and HCV replication after transfection was compared. Results: Patients with genotypes A/A, A/G and G/G of an SNP of OAS-1 at the exon 3 of its coding sequence were at gradient increased risks of suffering from higher serum alanine aminotransferase (P

Published

2009

2. Potential contribution of tumor suppressor p53 in the host defense against hepatitis C virus

Author

Ryosuke Muroyama, Run-Xuan Shao, Narayan Dharel, Jin-Hai Chang, Hiroyoshi Taniguchi, Mark K. Adler, Motoyuki Otsuka, Masao Omata, Takao Kawabe, Yue Wang, Amarsanaa Jazag, and Naoya Kato

Subjects

Viral protein, Hepatitis C virus, Gene Expression, Hepacivirus, Biology, medicine.disease_cause, Virus Replication, Virus, Viral Proteins, Interferon, Cell Line, Tumor, medicine, Humans, Cell Proliferation, Cell Nucleus, Hepatology, Cell Cycle, Protein kinase R, Virology, Hepatitis C, Interferon-Stimulated Gene Factor 3, gamma Subunit, NS2-3 protease, Viral replication, Host-Pathogen Interactions, STAT protein, Replicon, Interferons, Tumor Suppressor Protein p53, medicine.drug

Abstract

Infection by hepatitis C virus (HCV) usually results into chronic hepatitis that can ultimately lead to cirrhosis and hepatocellular carcinoma. Type 1 interferons (IFN-α/β) constitute the primary cellular defense against viral infection including HCV. IFN binding to their receptors activates associated Jak1 and Tyk2 kinases, which ultimately leads to phosphorylation and assembly of a signal transducer and activator of transcription protein (STAT)1-STAT2-interferon regulatory factor (IRF)9 trimetric complex called interferon-stimulated gene factor 3 that translocates into the nucleus and binds to the interferon- stimulated response elements (ISRE), leading to transcriptional induction of several antiviral genes, including double-stranded RNA-activated protein kinase (PKR), 2′,5′- oligoadenylate synthetase (OAS), and myxovirus resistance protein A (MxA). Understanding the mechanisms of how the virus evades this cellular innate defense and establishes a chronic infection is the key for the development of better therapeutics against HCV infection. Here, we demonstrate that p53 could have a crucial role in the cellular innate defense against HCV. We observed significantly higher levels of HCV RNA replication and viral protein expression in the Huh7 cells when their p53 expressions were knocked down. Moreover, IFN treatment was less effective in inhibiting the HCV RNA replication in the p53–knocked-down (p53kd) Huh7 cells. In fact, the activation of the ISRE and the induction of ISGs were significantly attenuated in the p53kd Huh7 cells and p53 was found to directly interact with IRF9. Conclusion: These observations underscore the potential contributions of the tumor suppressor p53 in cellular antiviral immunity against HCV with possible therapeutic implications. (HEPATOLOGY 2008.)

Published

2008

3. Hepatitis B virus precore protein augments genetic immunizations of the truncated hepatitis C virus core in BALB/c mice

Author

Xinwen Zhang, Li Weidong, Wenjie Tan, Jin-Hai Chang, Ming-bo Sun, Masao Omata, Shude Jiang, Guo-yang Liao, Jun-ying Chen, Tao Bian, Huijuan Yang, Shengli Bi, and Yue Wang

Subjects

Viral Hepatitis Vaccines, Hepatitis B virus, Hepatitis C virus, Recombinant Fusion Proteins, Gene Expression, chemical and pharmacologic phenomena, Enzyme-Linked Immunosorbent Assay, Hepacivirus, medicine.disease_cause, Virus, BALB/c, Mice, Immune system, Orthohepadnavirus, Antigen, medicine, Animals, Cell Proliferation, Immunity, Cellular, Mice, Inbred BALB C, Hepatology, biology, Viral Core Proteins, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Virology, Hepatitis C, Hepadnaviridae, Antibody Formation, bacteria, Female, Immunization, Plasmids, T-Lymphocytes, Cytotoxic

Abstract

DNA immunization has been used to induce either humoral or cellular immune responses against many antigens, including hepatitis C virus (HCV). In addition, DNA immunizations can be enhanced or modulated at the nucleotide level. Genetic immunizations were examined in BALB/c mice through the use of plasmids and chimeric DNA constructs encoding HCV core proteins and hepatitis B virus (HBV) precore (preC) regions. Plasmids encoding the truncated HCV core induced potent humoral and cellular responses to HCV; pcDNA3.0A-C154 produced a stronger antibody response than pcDNA3.0A-C191 (P < 0.01) and pcDNA3.0A-C69 (P < 0.05). HBV preC enhanced the humoral and cellular immune responses of BALB/c mice to HCV; however, pcDNA3.0A-C69preC resulted in a weak cytotoxic T lymphocyte (CTL) response. In addition, the humoral and cellular immune responses to HCV of groups immunized with pcDNA3.0A-C154preC and pcDNA3.0A-C191preC plasmids were higher than those of groups immunized with pcDNA3.0A-C154 and pcDNA3.0A-C191. In vivo CTL responses verified that mice immunized with preC core fused DNAs showed significantly high specific lysis compared with mice immunized with HCV cores only (P < 0.01). In our study, pcDNA3.0A-C154preC led to the highest immune response among all DNA constructs. Conclusion: DNA that encodes truncated HCV core proteins may lead to increased immune responses in vivo, and these responses may be enhanced by HBV preC. (HEPATOLOGY 2007.)

Published

2007

4. Polymorphism of OAS-1 determines liver fibrosis progression in hepatitis C by reduced ability to inhibit viral replication.

Author

Chang-Zheng Li, Kato, Naoya, Jin-Hai Chang, Muroyama, Ryosuke, Run-Xuan Shao, Dharel, Narayan, Sermsathanasawadi, Radsamee, Kawabe, Takao, and Omata, Masao

Subjects

GENETIC polymorphisms, FIBROSIS, LIVER diseases, HEPATITIS C, VIRAL replication

Abstract

Background: Progression of disease after hepatitis C virus (HCV) infection differs among individuals, indicating a possibility of participation of host genetic factors. 2′-5′-oligoadenylate synthetase 1 (OAS-1), an important component of the innate immune system, has an antiviral function, and may therefore have a certain relationship with progression of disease. Aim: To evaluate single nucleotide polymorphisms (SNPs) of OAS-1 and its relationship with the disease status of HCV infection. Methods: Six SNPs of OAS-1 were selected and examined in 409 Japanese patients with chronic HCV infection using the TaqMan PCR genotyping method. The relationship of SNP genotypes and clinical manifestations of patients was analysed. Then, a pair of OAS-1-expression plasmids mimicking the clinical-related SNPs were created and transfected into liver cells carrying the HCV subgenomic replicon or the full-length genome, JFH1, and HCV replication after transfection was compared. Results: Patients with genotypes A/A, A/G and G/G of an SNP of OAS-1 at the exon 3 of its coding sequence were at gradient increased risks of suffering from higher serum alanine aminotransferase ( P<0.001) and aspartate aminotransferase ( P=0.001), higher degree of liver fibrosis ( P=0.010) and higher presence of liver cirrhosis ( P=0.001). By multivariate logistic regression analysis, genotype G/G was an independent factor associated with cirrhosis ( P=0.013, odds ratio 3.11, 95% confidence interval 1.27–7.63). In liver cells, OAS-1 with the G allele showed lower ability to inhibit virus replication than OAS-1 with the A allele ( P=0.004). Conclusions: The SNP of OAS-1 at the exon 3 of its coding sequence was associated with progression of disease in Japanese patients with HCV infection. [ABSTRACT FROM AUTHOR]

Published

2009