Your search keyword '"Lu-Lu Gong"' showing total 8 results

1. T lymphocytes from chronic HCV-infected patients are primed for activation-induced apoptosis and express unique pro-apoptotic gene signature.

Author

Bin-Bin Zhao, Su-Jun Zheng, Lu-Lu Gong, Yu Wang, Cai-Feng Chen, Wen-Jing Jin, Ding Zhang, Xiao-Hui Yuan, Jian Guo, Zhong-Ping Duan, and You-Wen He

Subjects

Medicine, Science

Abstract

Although extensive studies have demonstrated the functional impairment of antigen-specific CD4(+) and CD8(+) T-cells during chronic hepatitis C virus (HCV) infection, the functional status of global CD4(+) and CD8(+) T-cells remains unclear. In this report, we recruited 42 long-term (~20 years) treatment-naïve chronic HCV (CHC) patients and 15 healthy donors (HDs) to investigate differences in global CD4(+) and CD8(+) T-cells function. We show that CD4(+) and CD8(+) T-cells from CHC patients underwent increased apoptosis after TCR stimulation. Furthermore, IFN-γ, IL-9 and IP-10 were elevated in CHC patients' plasma and promoted activation-induced T-cells death. Global CD4(+) and CD8(+) T-cells also showed unique transcriptional profiles in the expression of apoptosis-related genes. We identified BCL2, PMAIP1, and CASP1 in CD4(+) T-cells and IER3 and BCL2A1 in CD8(+) T-cells from CHC patients as HCV-specific gene signatures. Importantly, the gene expression patterns of CD4(+) and CD8(+) T-cells from CHC patients differ from those in CD4(+) and CD8(+) T-cells from human immunodeficiency virus type 1 (HIV-1) or hepatitis B virus (HBV) infected individuals. Our results indicate that chronic HCV infection causes a systemic change in cytokine levels that primes T-cells for activation-induced apoptosis. Furthermore, HCV infection programs unique apoptosis-related gene expression profiles in CD4(+) and CD8(+) T-cells, leading to their enhanced activation-induced apoptosis. These results provide novel insights to the pathogenesis of chronic HCV infection.

Published

2013

2. A novel antibody humanization method based on epitopes scanning and molecular dynamics simulation.

Author

Ding Zhang, Cai-Feng Chen, Bin-Bin Zhao, Lu-Lu Gong, Wen-Jing Jin, Jing-Jun Liu, Jing-Fei Wang, Tian-Tian Wang, Xiao-Hui Yuan, and You-Wen He

Subjects

Medicine, Science

Abstract

1-17-2 is a rat anti-human DEC-205 monoclonal antibody that induces internalization and delivers antigen to dendritic cells (DCs). The potentially clinical application of this antibody is limited by its murine origin. Traditional humanization method such as complementarity determining regions (CDRs) graft often leads to a decreased or even lost affinity. Here we have developed a novel antibody humanization method based on computer modeling and bioinformatics analysis. First, we used homology modeling technology to build the precise model of Fab. A novel epitope scanning algorithm was designed to identify antigenic residues in the framework regions (FRs) that need to be mutated to human counterpart in the humanization process. Then virtual mutation and molecular dynamics (MD) simulation were used to assess the conformational impact imposed by all the mutations. By comparing the root-mean-square deviations (RMSDs) of CDRs, we found five key residues whose mutations would destroy the original conformation of CDRs. These residues need to be back-mutated to rescue the antibody binding affinity. Finally we constructed the antibodies in vitro and compared their binding affinity by flow cytometry and surface plasmon resonance (SPR) assay. The binding affinity of the refined humanized antibody was similar to that of the original rat antibody. Our results have established a novel method based on epitopes scanning and MD simulation for antibody humanization.

Published

2013

3. Structure-based high-throughput epitope analysis of hexon proteins in B and C species human adenoviruses (HAdVs).

Author

Xiao-Hui Yuan, Ying-Chen Wang, Wen-Jing Jin, Bin-Bin Zhao, Cai-Feng Chen, Jian Yang, Jing-Fei Wang, Ying-Ying Guo, Jing-Jun Liu, Ding Zhang, Lu-Lu Gong, and You-Wen He

Subjects

Medicine, Science

Abstract

Human adenoviruses (HAdVs) are the etiologic agent of many human infectious diseases. The existence of at least 54 different serotypes of HAdVs has resulted in difficulties in clinical diagnosis. Acute respiratory tract disease (ARD) caused by some serotypes from B and C species is particularly serious. Hexon, the main coat protein of HAdV, contains the major serotype-specific B cell epitopes; however, few studies have addressed epitope mapping in most HAdV serotypes. In this study, we utilized a novel and rapid method for the modeling of homologous proteins based on the phylogenetic tree of protein families and built three-dimensional (3D) models of hexon proteins in B and C species HAdVs. Based on refined hexon structures, we used reverse evolutionary trace (RET) bioinformatics analysis combined with a specially designed hexon epitope screening algorithm to achieve high-throughput epitope mapping of all 13 hexon proteins in B and C species HAdVs. This study has demonstrated that all of the epitopes from the 13 hexon proteins are located in the proteins' tower regions; however, the exact number, location, and size of the epitopes differ among the HAdV serotypes.

Published

2012

4. Downregulation of the AU-rich RNA-binding protein ZFP36 in chronic HBV patients: implications for anti-inflammatory therapy.

Author

Wen-Jing Jin, Cai-Feng Chen, Hui-Yu Liao, Lu-Lu Gong, Xiao-Hui Yuan, Bin-Bin Zhao, Ding Zhang, Xia Feng, Jing-Jun Liu, Yu Wang, Guo-Feng Chen, Hui-Ping Yan, and You-Wen He

Subjects

Medicine, Science

Abstract

Inflammation caused by chronic hepatitis B virus (HBV) infection is associated with the development of cirrhosis and hepatocellular carcinoma; however, the mechanisms by which HBV infection induces inflammation and inflammatory cytokine production remain largely unknown. We analyzed the gene expression patterns of lymphocytes from chronic HBV-infected patients and found that the expression of ZFP36, an AU-rich element (ARE)-binding protein, was dramatically reduced in CD4(+) and CD8(+) T lymphocytes from chronic HBV patients. ZFP36 expression was also reduced in CD14(+) monocytes and in total PBMCs from chronic HBV patients. To investigate the functional consequences of reduced ZFP36 expression, we knocked down ZFP36 in PBMCs from healthy donors using siRNA. siRNA-mediated silencing of ZFP36 resulted in dramatically increased expression of multiple inflammatory cytokines, most of which were also increased in the plasma of chronic HBV patients. Furthermore, we found that IL-8 and RANTES induced ZFP36 downregulation, and this effect was mediated through protein kinase C. Importantly, we found that HBsAg stimulated PBMCs to express IL-8 and RANTES, resulting in decreased ZFP36 expression. Our results suggest that an inflammatory feedback loop involving HBsAg, ZFP36, and inflammatory cytokines may play a critical role in the pathogenesis of chronic HBV and further indicate that ZFP36 may be an important target for anti-inflammatory therapy during chronic HBV infection.

Published

2012

5. T lymphocytes from chronic HCV-infected patients are primed for activation-induced apoptosis and express unique pro-apoptotic gene signature

Author

Sujun Zheng, Yu Wang, Xiaohui Yuan, Cai-Feng Chen, Ding Zhang, You-Wen He, Zhongping Duan, Lu-Lu Gong, Bin-Bin Zhao, Jian Guo, and Wen-Jing Jin

Subjects

Adult, Male, IER3, Hepatitis C virus, T-Lymphocytes, lcsh:Medicine, Apoptosis, Biology, medicine.disease_cause, Lymphocyte Activation, Virus, Pathogenesis, medicine, Cytotoxic T cell, Humans, lcsh:Science, Aged, Hepatitis B virus, Multidisciplinary, lcsh:R, Hepatitis C, Chronic, Middle Aged, Virology, Gene Expression Regulation, Immunology, Cytokines, lcsh:Q, Female, CD8, Research Article

Abstract

Although extensive studies have demonstrated the functional impairment of antigen-specific CD4(+) and CD8(+) T-cells during chronic hepatitis C virus (HCV) infection, the functional status of global CD4(+) and CD8(+) T-cells remains unclear. In this report, we recruited 42 long-term (~20 years) treatment-naïve chronic HCV (CHC) patients and 15 healthy donors (HDs) to investigate differences in global CD4(+) and CD8(+) T-cells function. We show that CD4(+) and CD8(+) T-cells from CHC patients underwent increased apoptosis after TCR stimulation. Furthermore, IFN-γ, IL-9 and IP-10 were elevated in CHC patients' plasma and promoted activation-induced T-cells death. Global CD4(+) and CD8(+) T-cells also showed unique transcriptional profiles in the expression of apoptosis-related genes. We identified BCL2, PMAIP1, and CASP1 in CD4(+) T-cells and IER3 and BCL2A1 in CD8(+) T-cells from CHC patients as HCV-specific gene signatures. Importantly, the gene expression patterns of CD4(+) and CD8(+) T-cells from CHC patients differ from those in CD4(+) and CD8(+) T-cells from human immunodeficiency virus type 1 (HIV-1) or hepatitis B virus (HBV) infected individuals. Our results indicate that chronic HCV infection causes a systemic change in cytokine levels that primes T-cells for activation-induced apoptosis. Furthermore, HCV infection programs unique apoptosis-related gene expression profiles in CD4(+) and CD8(+) T-cells, leading to their enhanced activation-induced apoptosis. These results provide novel insights to the pathogenesis of chronic HCV infection.

Published

2013

6. Structure-Based High-Throughput Epitope Analysis of Hexon Proteins in B and C Species Human Adenoviruses (HAdVs)

Author

Xiaohui Yuan, Wen-Jing Jin, Ying-Chen Wang, Jian Yang, Cai-Feng Chen, You-Wen He, Ying-Ying Guo, Lu-Lu Gong, Jing-Jun Liu, Ding Zhang, Jingfei Wang, and Bin-Bin Zhao

Subjects

Human Adenoviruses, Serotype, Models, Molecular, Anatomy and Physiology, Protein family, viruses, Biophysics, lcsh:Medicine, Biology, Biochemistry, Epitope, Phylogenetics, Immune Physiology, Macromolecular Structure Analysis, Cluster Analysis, lcsh:Science, Phylogeny, Multidisciplinary, Phylogenetic tree, Physics, Adenoviruses, Human, lcsh:R, virus diseases, Proteins, Computational Biology, Protein superfamily, Virology, eye diseases, Epitope mapping, Computer Science, Medicine, Epitopes, B-Lymphocyte, lcsh:Q, Capsid Proteins, Algorithms, Epitope Mapping, Research Article, Computer Modeling

Abstract

Human adenoviruses (HAdVs) are the etiologic agent of many human infectious diseases. The existence of at least 54 different serotypes of HAdVs has resulted in difficulties in clinical diagnosis. Acute respiratory tract disease (ARD) caused by some serotypes from B and C species is particularly serious. Hexon, the main coat protein of HAdV, contains the major serotype-specific B cell epitopes; however, few studies have addressed epitope mapping in most HAdV serotypes. In this study, we utilized a novel and rapid method for the modeling of homologous proteins based on the phylogenetic tree of protein families and built three-dimensional (3D) models of hexon proteins in B and C species HAdVs. Based on refined hexon structures, we used reverse evolutionary trace (RET) bioinformatics analysis combined with a specially designed hexon epitope screening algorithm to achieve high-throughput epitope mapping of all 13 hexon proteins in B and C species HAdVs. This study has demonstrated that all of the epitopes from the 13 hexon proteins are located in the proteins' tower regions; however, the exact number, location, and size of the epitopes differ among the HAdV serotypes.

Published

2012

7. A Novel Antibody Humanization Method Based on Epitopes Scanning and Molecular Dynamics Simulation

Author

You-Wen He, Tian-Tian Wang, Wen-Jing Jin, Jing-Jun Liu, Jingfei Wang, Lu-Lu Gong, Bin-Bin Zhao, Cai-Feng Chen, Xiaohui Yuan, and Ding Zhang

Subjects

medicine.drug_class, Molecular Sequence Data, lcsh:Medicine, Sequence alignment, Complementarity determining region, Computational biology, Molecular Dynamics Simulation, Monoclonal antibody, Humanized antibody, Epitope, Epitopes, Antigen, medicine, Humans, Amino Acid Sequence, Homology modeling, lcsh:Science, DNA Primers, Multidisciplinary, Base Sequence, Sequence Homology, Amino Acid, biology, lcsh:R, Surface Plasmon Resonance, Complementarity Determining Regions, Molecular biology, Mutation, biology.protein, lcsh:Q, Antibody, Research Article

Abstract

1-17-2 is a rat anti-human DEC-205 monoclonal antibody that induces internalization and delivers antigen to dendritic cells (DCs). The potentially clinical application of this antibody is limited by its murine origin. Traditional humanization method such as complementarity determining regions (CDRs) graft often leads to a decreased or even lost affinity. Here we have developed a novel antibody humanization method based on computer modeling and bioinformatics analysis. First, we used homology modeling technology to build the precise model of Fab. A novel epitope scanning algorithm was designed to identify antigenic residues in the framework regions (FRs) that need to be mutated to human counterpart in the humanization process. Then virtual mutation and molecular dynamics (MD) simulation were used to assess the conformational impact imposed by all the mutations. By comparing the root-mean-square deviations (RMSDs) of CDRs, we found five key residues whose mutations would destroy the original conformation of CDRs. These residues need to be back-mutated to rescue the antibody binding affinity. Finally we constructed the antibodies in vitro and compared their binding affinity by flow cytometry and surface plasmon resonance (SPR) assay. The binding affinity of the refined humanized antibody was similar to that of the original rat antibody. Our results have established a novel method based on epitopes scanning and MD simulation for antibody humanization.

Published

2013

8. Downregulation of the AU-Rich RNA-Binding Protein ZFP36 in Chronic HBV Patients: Implications for Anti-Inflammatory Therapy

Author

Ding Zhang, You-Wen He, Wen-Jing Jin, Yu Wang, Jing-Jun Liu, Guo-Feng Chen, Hui-Yu Liao, Lu-Lu Gong, Bin-Bin Zhao, Hui-ping Yan, Xia Feng, Xiaohui Yuan, and Cai-Feng Chen

Subjects

CD4-Positive T-Lymphocytes, Male, Viral Diseases, HBsAg, medicine.medical_treatment, lcsh:Medicine, CD8-Positive T-Lymphocytes, medicine.disease_cause, Hepatitis, Pathogenesis, Molecular Cell Biology, RNA, Small Interfering, lcsh:Science, Chemokine CCL5, Multidisciplinary, virus diseases, Middle Aged, Hepatitis B, Infectious Diseases, Cytokine, Gene Knockdown Techniques, Cytokines, Medicine, Female, medicine.symptom, Research Article, Adult, China, CD14, Immunology, Inflammation, Biology, Real-Time Polymerase Chain Reaction, Proinflammatory cytokine, Molecular Genetics, Tristetraprolin, Genetics, medicine, Humans, DNA Primers, Hepatitis B virus, Hepatitis B Surface Antigens, Interleukin-8, lcsh:R, Immunity, medicine.disease, digestive system diseases, Gene Expression Regulation, Leukocytes, Mononuclear, Clinical Immunology, lcsh:Q

Abstract

Inflammation caused by chronic hepatitis B virus (HBV) infection is associated with the development of cirrhosis and hepatocellular carcinoma; however, the mechanisms by which HBV infection induces inflammation and inflammatory cytokine production remain largely unknown. We analyzed the gene expression patterns of lymphocytes from chronic HBV-infected patients and found that the expression of ZFP36, an AU-rich element (ARE)-binding protein, was dramatically reduced in CD4(+) and CD8(+) T lymphocytes from chronic HBV patients. ZFP36 expression was also reduced in CD14(+) monocytes and in total PBMCs from chronic HBV patients. To investigate the functional consequences of reduced ZFP36 expression, we knocked down ZFP36 in PBMCs from healthy donors using siRNA. siRNA-mediated silencing of ZFP36 resulted in dramatically increased expression of multiple inflammatory cytokines, most of which were also increased in the plasma of chronic HBV patients. Furthermore, we found that IL-8 and RANTES induced ZFP36 downregulation, and this effect was mediated through protein kinase C. Importantly, we found that HBsAg stimulated PBMCs to express IL-8 and RANTES, resulting in decreased ZFP36 expression. Our results suggest that an inflammatory feedback loop involving HBsAg, ZFP36, and inflammatory cytokines may play a critical role in the pathogenesis of chronic HBV and further indicate that ZFP36 may be an important target for anti-inflammatory therapy during chronic HBV infection.

Published

2012