Your search keyword '"Xie, Youhua"' showing total 42 results

1. Hepatitis B virus core protein as a Rab-GAP suppressor driving liver disease progression.

Author

Su, Yu, Bu, Fan, Zhu, Yuanfei, Yang, Le, Wu, Qiong, Zheng, Yuan, Zhao, Jianjin, Yu, Lin, Jiang, Nan, Wang, Yongxiang, Wu, Jian, Xie, Youhua, Zhang, Xinxin, Gao, Yueqiu, Lan, Ke, and Deng, Qiang

Subjects

*CHRONIC hepatitis B, *MITOCHONDRIAL dynamics, *HEPATITIS B virus, *GTPASE-activating protein, *TRANSGENIC mice

Abstract

[Display omitted] Chronic hepatitis B virus (HBV) infection can lead to advanced liver pathology. Here, we establish a transgenic murine model expressing a basic core promoter (BCP)-mutated HBV genome. Unlike previous studies on the wild-type virus, the BCP-mutated HBV transgenic mice manifest chronic liver injury that culminates in cirrhosis and tumor development with age. Notably, agonistic anti-Fas treatment induces fulminant hepatitis in these mice even at a negligible dose. As the BCP mutant exhibits a striking increase in HBV core protein (HBc) expression, we posit that HBc is actively involved in hepatocellular injury. Accordingly, HBc interferes with Fis1-stimulated mitochondrial recruitment of Tre-2/Bub2/Cdc16 domain family member 15 (TBC1D15). HBc may also inhibit multiple Rab GTPase-activating proteins, including Rab7-specific TBC1D15 and TBC1D5, by binding to their conserved catalytic domain. In cells under mitochondrial stress, HBc thus perturbs mitochondrial dynamics and prevents the recycling of damaged mitochondria. Moreover, sustained HBc expression causes lysosomal consumption via Rab7 hyperactivation, which further hampers late-stage autophagy and substantially increases apoptotic cell death. Finally, we show that adenovirally expressed HBc in a mouse model is directly cytopathic and causes profound liver injury, independent of antigen-specific immune clearance. These findings reveal an unexpected cytopathic role of HBc, making it a pivotal target for HBV-associated liver disease treatment. The BCP-mutated HBV transgenic mice also provide a valuable model for understanding chronic hepatitis B progression and for the assessment of therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

2. Development of a Cell Culture Model for Inducible SARS-CoV-2 Replication.

Author

Wang, Xiaoyan, Zhu, Yuanfei, Wu, Qiong, Jiang, Nan, Xie, Youhua, and Deng, Qiang

Subjects

*SARS-CoV-2, *CELL culture, *DNA microarrays, *BACTERIAL artificial chromosomes, *RECOMBINANT DNA

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) induces direct cytopathic effects, complicating the establishment of low-cytotoxicity cell culture models for studying its replication. We initially developed a DNA vector-based replicon system utilizing the CMV promoter to generate a recombinant viral genome bearing reporter genes. However, this system frequently resulted in drug resistance and cytotoxicity, impeding model establishment. Herein, we present a novel cell culture model with SARS-CoV-2 replication induced by Cre/LoxP-mediated DNA recombination. An engineered SARS-CoV-2 transcription unit was subcloned into a bacterial artificial chromosome (BAC) vector. To enhance biosafety, the viral spike protein gene was deleted, and the nucleocapsid gene was replaced with a reporter gene. An exogenous sequence was inserted within NSP1 as a modulatory cassette that is removable after Cre/LoxP-mediated DNA recombination and subsequent RNA splicing. Using the PiggyBac transposon strategy, the transcription unit was integrated into host cell chromatin, yielding a stable cell line capable of inducing recombinant SARS-CoV-2 RNA replication. The model exhibited sensitivity to the potential antivirals forsythoside A and verteporfin. An innovative inducible SARS-CoV-2 replicon cell model was introduced to further explore the replication and pathogenesis of the virus and facilitate screening and assessment of anti-SARS-CoV-2 therapeutics. [ABSTRACT FROM AUTHOR]

Published

2024

3. A spike-targeting bispecific T cell engager strategy provides dual layer protection against SARS-CoV-2 infection in vivo.

Author

Li, Fanlin, Xu, Wei, Zhang, Xiaoqing, Wang, Wanting, Su, Shan, Han, Ping, Wang, Haiyong, Xu, Yanqin, Li, Min, Fan, Lilv, Zhang, Huihui, Dai, Qiang, Lin, Hao, Qi, Xinyue, Liang, Jie, Wang, Xin, Jiang, Shibo, Xie, Youhua, Lu, Lu, and Yang, Xuanming

Subjects

*T cells, *BISPECIFIC antibodies, *SARS-CoV-2 Delta variant, *CELL receptors, *SARS-CoV-2, *CORONAVIRUS diseases, *CELL-mediated cytotoxicity

Abstract

Neutralizing antibodies exert a potent inhibitory effect on viral entry; however, they are less effective in therapeutic models than in prophylactic models, presumably because of their limited efficacy in eliminating virus-producing cells via Fc-mediated cytotoxicity. Herein, we present a SARS-CoV-2 spike-targeting bispecific T-cell engager (S-BiTE) strategy for controlling SARS-CoV-2 infection. This approach blocks the entry of free virus into permissive cells by competing with membrane receptors and eliminates virus-infected cells via powerful T cell-mediated cytotoxicity. S-BiTE is effective against both the original and Delta variant of SARS-CoV2 with similar efficacy, suggesting its potential application against immune-escaping variants. In addition, in humanized mouse model with live SARS-COV-2 infection, S-BiTE treated mice showed significantly less viral load than neutralization only treated group. The S-BiTE strategy may have broad applications in combating other coronavirus infections. A SARS-CoV-2 spike-targeting bispecific T-cell engager (S-BiTE) strategy is presented that effectively reduces SARS-CoV-2 viral load in a humanized mouse model. [ABSTRACT FROM AUTHOR]

Published

2023

4. Over-expression and purification of isotopically labeled recombinant ligand-binding domain of orphan nuclear receptor human B1-binding factor/human liver receptor homologue 1 for NMR studies

Author

Chen, Xiang, Tong, Xiaotian, Xie, Youhua, Wang, Yuan, Ma, Jinbiao, Gao, DaMing, Wu, Houming, and Chen, Haibao

Subjects

*NUCLEAR magnetic resonance, *MAGNETIC resonance, *NUCLEAR quadrupole resonance, *HEPATITIS B

Abstract

Abstract: The human hepatitis B virus enhancer II B1 binding factor (hB1F), which regulates the expression of hepatitis B virus genes, is identified as a nuclear receptor. It regulates several liver-specific genes and plays an important role in the bile acid biosynthesis pathway. A significantly optimized protocol has been worked out to prepare 15N and/or 13C-labeled hB1F ligand-binding domain in minimal medium with high yields for NMR studies. Under the various conditions optimized for the purification of His6-hB1F ligand-binding domain, the yield of the purified protein is estimated to be 25–30mg from 0.5L of M9 minimal media. Electrospray ionization mass spectrometry data confirm the correctness of the primary sequence. Dynamic light scattering experiment proves that the protein exists as a monomeric form. In addition, the circular dichroism results show that the protein has a well-regulated secondary structure and a high α-helical content in ammonium bicarbonate buffer at 20°C and pH 7.4. Finally, uniformly 15N-labeled protein is characterized by a TROSY–HSQC spectrum, and the dispersion of 15N–1H cross-peaks in the spectrum indicates the presence of well-ordered and properly folded protein as a monomer. [Copyright &y& Elsevier]

Published

2006

5. Expression, purification, and characterization of SARS coronavirus RNA polymerase

Author

Cheng, Ao, Zhang, Wei, Xie, Youhua, Jiang, Weihong, Arnold, Eddy, Sarafianos, Stefan G., and Ding, Jianping

Subjects

*RNA, *NUCLEIC acids, *SARS disease, *COMMUNICABLE diseases

Abstract

Abstract: The RNA-dependent RNA polymerase (RdRp) of SARS coronavirus (SARS-CoV) is essential for viral replication and a potential target for anti-SARS drugs. We report here the cloning, expression, and purification of the N-terminal GST-fused SARS-CoV RdRp and its polymerase catalytic domain in Escherichia coli. During purification, the full-length GST-RdRp was found to cleave into three main fragments: an N-terminal p12 fragment, a middle p30 fragment, and a C-terminal p64 fragment comprising the catalytic domain, presumably due to bacterial proteases. Biochemical assays show that the full-length GST-RdRp has RdRp activity and the p64 and p12 fragments form a complex that exhibits comparable RdRp activity, whereas the GST-p64 protein has no activity, suggesting that the p12 domain is required for polymerase activity possibly via involvement in template-primer binding. Nonnucleoside HIV-1 RT inhibitors are shown to have no evident inhibitory effect on SARS-CoV RdRp activity. This work provides a basis for biochemical and structural studies of SARS-CoV RdRp and for development of anti-SARS drugs. [Copyright &y& Elsevier]

Published

2005

6. Establishment of widely expressed hb1f transgenic mouse lineage and its morphologic analysis.

Author

Wang Shuiliang, He Yan, Xie Youhua, Wang Yuan, Li Jianzhong, Wang Long, Wang Zhugang, and Fu Jiliang

Subjects

*NUCLEAR receptors (Biochemistry), *MORPHOLOGY, *GENES, *CHOLESTEROL, *HOMEOSTASIS, *METABOLISM

Abstract

Human nuclear receptor hB1F is a novel member of the fushi tarazu factor I subfamily of nuclear receptor superfamily. The studies about its homologous genes indicate that hB1F may play a key role in regulating the metabolic homeostasis of cholesterol. After obtaining the founder mice carrying the transgene of hb1f by microinjection, each founder was mated to normal C57 mouse and the positive F1 by PCR identification of the same founder were intercrossed within sisters and brothers to establish the transgenic mouse lineage. The results of F1, F2 and offspring of test cross identification showed that the widely expressed hb1f transgenic mouse lineage was established successfully in this study. The tissue morphology of the transgenic lineage was also analyzed preliminarily. [ABSTRACT FROM AUTHOR]

Published

2004

7. Comprehensive mapping of binding hot spots of SARS-CoV-2 RBD-specific neutralizing antibodies for tracking immune escape variants.

Author

Yi, Chunyan, Sun, Xiaoyu, Lin, Yixiao, Gu, Chenjian, Ding, Longfei, Lu, Xiao, Yang, Zhuo, Zhang, Yaguang, Ma, Liyan, Gu, Wangpeng, Qu, Aidong, Zhou, Xu, Li, Xiuling, Xu, Jianqing, Ling, Zhiyang, Xie, Youhua, Lu, Hongzhou, and Sun, Bing

Subjects

*SARS-CoV-2, *CONVALESCENT plasma, *COVID-19 treatment, *RECOMBINANT proteins, *COVID-19, *VIRAL antibodies, *IMMUNOGLOBULINS

Abstract

Background: The receptor-binding domain (RBD) variants of SARS-CoV-2 could impair antibody-mediated neutralization of the virus by host immunity; thus, prospective surveillance of antibody escape mutants and understanding the evolution of RBD are urgently needed. Methods: Using the single B cell cloning technology, we isolated and characterized 93 RBD-specific antibodies from the memory B cells of four COVID-19 convalescent individuals in the early stage of the pandemic. Then, global RBD alanine scanning with a panel of 19 selected neutralizing antibodies (NAbs), including several broadly reactive NAbs, was performed. Furthermore, we assessed the impact of single natural mutation or co-mutations of concern at key positions of RBD on the neutralization escape and ACE2 binding function by recombinant proteins and pseudoviruses. Results: Thirty-three amino acid positions within four independent antigenic sites (1 to 4) of RBD were identified as valuable indicators of antigenic changes in the RBD. The comprehensive escape mutation map not only confirms the widely circulating strains carrying important immune escape RBD mutations such as K417N, E484K, and L452R, but also facilitates the discovery of new immune escape-enabling mutations such as F486L, N450K, F490S, and R346S. Of note, these escape mutations could not affect the ACE2 binding affinity of RBD, among which L452R even enhanced binding. Furthermore, we showed that RBD co-mutations K417N, E484K, and N501Y present in B.1.351 appear more resistant to NAbs and human convalescent plasma from the early stage of the pandemic, possibly due to an additive effect. Conversely, double mutations E484Q and L452R present in B.1.617.1 variant show partial antibody evasion with no evidence for an additive effect. Conclusions: Our study provides a global view of the determinants for neutralizing antibody recognition, antigenic conservation, and RBD conformation. The in-depth escape maps may have value for prospective surveillance of SARS-CoV-2 immune escape variants. Special attention should be paid to the accumulation of co-mutations at distinct major antigenic sites. Finally, the new broadly reactive NAbs described here represent new potential opportunities for the prevention and treatment of COVID-19. [ABSTRACT FROM AUTHOR]

Published

2021

8. Development of benzimidazole-based compounds as novel capsid assembly modulators for the treatment of HBV infection.

Author

Du, Kaixin, Wang, Xianyang, Bai, Yuxin, Zhang, Xue, Xue, Jie, Li, Shanshan, Xie, Youhua, Sang, Zhipei, Tang, Yu, and Wang, Xin

Subjects

*BENZIMIDAZOLES, *HEPATITIS B, *CHEMICAL libraries, *HEPATITIS B virus, *BENZIMIDAZOLE derivatives

Abstract

Hepatitis B virus (HBV) capsid assembly modulators (CAMs) represent a promising therapeutic approach for the treatment of HBV infection. In this study, the hit compound CDI (IC 50 = 2.46 ± 0.33 μM) was identified by screening of an in-house compound library. And then novel potent benzimidazole derivatives were designed and synthesized as core assembly modulators, and their antiviral effects were evaluated in vitro and in vivo biological experiments. The results indicated that compound 26f displayed the most optimized modulator of HBV capsid assembly (IC 50 = 0.51 ± 0.20 μM, EC 50 = 2.24 ± 0.43 μM, CC 50 = 84.29 μM) and high selectivity index. Moreover, treatment with compound 26f for 14 days significantly decreased serum levels of HBV DNA levels in the Hydrodynamic-Injection (HDI) mouse model. Therefore, compound 26f could be considered as a promising candidate drug for further development of novel HBV CAMs with the desired potency and safety. [Display omitted] • The hit compound CDI (IC 50 = 2.46 ± 0.33 μM) was identified by screening of an in-house compound library (3781 compounds). • Novel benzimidazole derivatives were synthesized as HBV core assembly modulators. • 26f displayed the most optimized modulator of HBV capsid assembly. • 26f displayed potent anti -HBV activities in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2024

9. Protoporphyrin IX and verteporfin potently inhibit SARS-CoV-2 infection in vitro and in a mouse model expressing human ACE2.

Author

Gu, Chenjian, Wu, Yang, Guo, Huimin, Zhu, Yuanfei, Xu, Wei, Wang, Yuyan, Zhou, Yu, Sun, Zhiping, Cai, Xia, Li, Yutang, Liu, Jing, Huang, Zhong, Yuan, Zhenghong, Zhang, Rong, Deng, Qiang, Qu, Di, and Xie, Youhua

Subjects

*SARS-CoV-2, *ANGIOTENSIN converting enzyme, *VIRAL proteins, *METALLOPORPHYRINS, *ANTIVIRAL agents, *INFECTION

Abstract

[Display omitted] The SARS-CoV-2 infection is spreading rapidly worldwide. Efficacious antiviral therapeutics against SARS-CoV-2 is urgently needed. Here, we discovered that protoporphyrin IX (PpIX) and verteporfin, two Food and Drug Administration (FDA)-approved drugs, completely inhibited the cytopathic effect produced by SARS-CoV-2 infection at 1.25 μmol/L and 0.31 μmol/L, respectively, and their EC50 values of reduction of viral RNA were at nanomolar concentrations. The selectivity indices of PpIX and verteporfin were 952.74 and 368.93, respectively, suggesting a broad margin of safety. Importantly, PpIX and verteporfin prevented SARS-CoV-2 infection in mice adenovirally transduced with human angiotensin-converting enzyme 2 (ACE2). The compounds, sharing a porphyrin ring structure, were shown to bind viral receptor ACE2 and interfere with the interaction between ACE2 and the receptor-binding domain of viral S protein. Our study suggests that PpIX and verteporfin are potent antiviral agents against SARS-CoV-2 infection and sheds new light on developing novel chemoprophylaxis and chemotherapy against SARS-CoV-2. [ABSTRACT FROM AUTHOR]

Published

2021

10. Transfected DNA is targeted by STING-mediated restriction.

Author

Gu, Chenjian, Ming, Lijun, Tao, Shuai, Luo, Mengjun, Guo, Huimin, Xie, Youhua, Liu, Jing, and Shen, Zhongliang

Subjects

*TYPE I interferons, *DNA, *ADAPTOR proteins, *GENE transfection, *GENES, *GENE expression

Abstract

DNA transfection is routinely used for delivering expression of gene of interest to target cells. Transfected DNA has been known to activate cellular DNA sensor(s) and innate immune responses, but the effects of such responses on transfected DNA are not fully understood. STING (stimulator of interferon genes) is an important adaptor protein in cellular innate immune response to various DNA and RNA stimuli and upon activation induces significant type I interferon responses. In this work, we characterized the effects of STING on gene expression driven by transfected double-stranded DNA. We observed that gene expression from transfected DNA was repressed in the presence of overexpressed STING, but increased if endogenous STING was knocked down through RNA interference. Endogenous chromosomal genes and chromosome-integrated exogenous genes were not affected by such STING-mediated restriction, which did not depend on DNA circularity or linearity, promoter used, or bacterial sequences in transfected DNA. Mechanistically, STING-mediated repression of transfected DNA correlates with reduced mRNA levels, and partially involves the induction of interferon β production by STING. Collectively, these data indicate that episomal double-stranded DNA is targeted by STING-mediated cell defense. • STING represses gene expression from transfected DNA through reducing mRNA levels. • STING does not affect stable-expressing exogenous gene. • Interferon β production partially involves in STING-mediated restriction. [ABSTRACT FROM AUTHOR]

Published

2021

11. Comparative analysis reveals the species-specific genetic determinants of ACE2 required for SARS-CoV-2 entry.

Author

Ren, Wenlin, Zhu, Yunkai, Wang, Yuyan, Shi, Hongyang, Yu, Yin, Hu, Gaowei, Feng, Fei, Zhao, Xiaomin, Lan, Jun, Wu, Jianping, Kenney, Devin J., Douam, Florian, Tong, Yimin, Zhong, Jin, Xie, Youhua, Wang, Xinquan, Yuan, Zhenghong, Zhou, Dongming, Zhang, Rong, and Ding, Qiang

Subjects

*ANGIOTENSIN converting enzyme, *SARS-CoV-2, *CELL receptors, *VIRAL proteins, *CARRIER proteins, *GENETIC engineering, *MIDDLE East respiratory syndrome

Abstract

Coronavirus interaction with its viral receptor is a primary genetic determinant of host range and tissue tropism. SARS-CoV-2 utilizes ACE2 as the receptor to enter host cell in a species-specific manner. We and others have previously shown that ACE2 orthologs from New World monkey, koala and mouse cannot interact with SARS-CoV-2 to mediate viral entry, and this defect can be restored by humanization of the restrictive residues in New World monkey ACE2. To better understand the genetic determinants behind the ability of ACE2 orthologs to support viral entry, we compared koala and mouse ACE2 sequences with that of human and identified the key residues in koala and mouse ACE2 that restrict viral receptor activity. Humanization of these critical residues rendered both koala and mouse ACE2 capable of binding the spike protein and facilitating viral entry. Our study shed more lights into the genetic determinants of ACE2 as the functional receptor of SARS-CoV-2, which facilitates our understanding of viral entry. Author summary: SARS-CoV-2 spike protein could bind cellular receptor ACE2 for cell entry in a species-specific manner. A diverse of mammalian ACE2 proteins could be used by SARS-CoV-2 for entry, but ACE2 proteins of koala or mouse cannot bind with viral spike protein. We compared the koala or mouse ACE2 with human ACE2, and found Thr at 31 position of koala ACE2 or His at 353 position of mouse ACE2 as the restrictive residue which limits its function as the viral receptor, respectively. Interestingly, koala or mouse ACE2 could gain the receptor function once the restrictive reside was replaced by human counterpart by genetic engineering. This study could facilitate our understanding of the genetic basis of ACE2 as the functional receptor of SARS-CoV-2, which could inform the animal model development. [ABSTRACT FROM AUTHOR]

Published

2021

12. Restriction of exogenous DNA expression by SAMHD1.

Author

Gu, Chenjian, Ming, Lijun, Fang, Yili, Liu, Xuejing, Zhang, Junqi, Zelinskyy, Gennadiy, Deng, Qiang, Liu, Jing, and Xie, Youhua

Subjects

*DNA, *TYPE I interferons, *HEPATITIS B virus, *DNA viruses

Abstract

SAMHD1 (S terile A lpha M otif and H istidine-aspartate D omain containing protein 1) has been documented as a host factor that restricts HIV-1 and some DNA viruses. In this work, we attempted to explore possible effects of SAMHD1 on exogenous DNA and show that SAMHD1 exerts a general inhibition on the expression of exogenous DNA in vitro and in mice. This inhibition is achieved through repressing transcription of exogenous DNA. Intriguingly, unlike SAMHD1's restriction of HIV-1, such restriction does not require the dNTPase or RNase activities, or T592 phosphorylation of SAMHD1. Mechanistically, SAMHD1 enhances the expression of interferon regulatory factor-1 (IRF1), while IRF1 upregulation was demonstrated to inhibit exogenous DNA expression in a similar fashion as SAMHD1. IFNλ1, whose induction has been associated with IRF1 activation, is dispensable for SAMHD1/IRF1-mediated restriction of exogenous DNA, and neither type I nor II interferons appear to be involved. We also demonstrate that SAMHD1/IRF1-mediated restriction can effectively inhibit hepatitis B virus (HBV) antigen expression and progeny virus production in mouse models. In conclusion, these data support restriction of exogenous DNA as a novel function of SAMHD1. [ABSTRACT FROM AUTHOR]

Published

2020

13. Discovery of quinazolin-4-one-based non-covalent inhibitors targeting the severe acute respiratory syndrome coronavirus 2 main protease (SARS-CoV-2 Mpro).

Author

Zhang, Kuojun, Wang, Tianyu, Li, Maotian, Liu, Mu, Tang, He, Wang, Lin, Ye, Ke, Yang, Jiamei, Jiang, Sheng, Xiao, Yibei, Xie, Youhua, Lu, Meiling, and Zhang, Xiangyu

Subjects

*SARS-CoV-2, *PROTEOLYTIC enzymes, *DRUG design

Abstract

The COVID-19 pandemic caused by SARS-CoV-2 continues to pose a great threat to public health while various vaccines are available worldwide. Main protease (Mpro) has been validated as an effective anti-COVID-19 drug target. Using medicinal chemistry and rational drug design strategies, we identified a quinazolin-4-one series of nonpeptidic, noncovalent SARS-CoV-2 Mpro inhibitors based on baicalein, 5,6,7-trihydroxy-2-phenyl-4 H -chromen-4-one. In particular, compound C7 exhibits superior inhibitory activity against SARS-CoV-2 Mpro relative to baicalein (IC 50 = 0.085 ± 0.006 and 0.966 ± 0.065 μM, respectively), as well as improved physicochemical and drug metabolism and pharmacokinetics (DMPK) properties. In addition, C7 inhibits viral replication in SARS-CoV-2-infected Vero E6 cells more effectively than baicalein (EC 50 = 1.10 ± 0.12 and 5.15 ± 1.64 μM, respectively) with low cytotoxicity (CC 50 ＞ 50 μM). An X-ray co-crystal structure reveals a non-covalent mechanism of action, and a noncanonical binding mode not observed by baicalein. These results suggest that C7 represents a promising lead for development of more effective SARS-CoV-2 Mpro inhibitors and anti-COVID-19 drugs. [Display omitted] • A quinazolin-4-one series of noncovalent SARS-CoV-2 Mpro inhibitors were identified. • C7 showed better inhibitory potency against SARS-CoV-2 Mpro than baicalein. • C7 showed better cellular antiviral activity than baicalein with low cytotoxicity. • A crystal structure of D8 in Mpro reveals a noncovalent mechanism of action and distinct binding mode. [ABSTRACT FROM AUTHOR]

Published

2023

14. A virus-like particle of the hepatitis B virus preS antigen elicits robust neutralizing antibodies and T cell responses in mice.

Author

Cai, Xiaodan, Zheng, Weihao, Pan, Shaokun, Zhang, Shengyuan, Xie, Youhua, Guo, Haitao, Wang, Guoxin, Li, Zigang, and Luo, Ming

Subjects

*VIRUS-like particles, *HEPATITIS B treatment, *VIRAL antibodies, *T cell receptors, *VIRAL antigens, *LABORATORY mice

Abstract

The preS antigen of hepatitis B virus (HBV) corresponds to the N-terminal polypeptide in the large (L) antigen in addition to the small (S) antigen. The virus-like particle (VLP) of the S antigen is widely used as a vaccine to protect the population from HBV infection. The presence of the S antigen and its antibodies in patient blood has been used as markers to monitor hepatitis B. However, there is very limited knowledge about the preS antigen. We generated a preS VLP that is formed by a chimeric protein between preS and hemagglutinin (HA), and the matrix protein M1 of influenza virus. The HBV preS antigen is displayed on the surface of preS VLP. Asn112 and Ser98 of preS in VLP were found to be glycosylated and O -glycosylation of Ser98 has not been reported previously. The preS VLP shows a significantly higher immunogenicity than recombinant preS, eliciting robust anti-preS neutralizing antibodies. In addition, preS VLP is also capable of stimulating preS-specific CD8 + and CD4 + T cell responses in Balb/c mice and HBV transgenic mice. Furthermore, preS VLP immunization provided protection against hydrodynamic transfection of HBV DNA in mice. The data clearly suggest that this novel preS VLP could elicit robust immune responses to the HBV antigen, and can be potentially developed into prophylactic and therapeutic vaccines. [ABSTRACT FROM AUTHOR]

Published

2018

15. Inhibition of HBV replication by EVA1A via enhancing cellular degradation of HBV components and its potential therapeutic application.

Author

Yu, Jie, Shen, Zhongliang, Chen, Shiqi, Liu, Hongyan, Du, Zunguo, Mao, Richeng, Wang, Jinyu, Zhang, Yongmei, Zhu, Haoxiang, Yang, Sisi, Li, Jing, Wu, Jingwen, Dong, Minhui, Zhu, Mengqi, Huang, Yuxian, Li, Jianhua, Yuan, Zhenghong, Xie, Youhua, Lu, Mengji, and Zhang, Jiming

Subjects

*CHRONIC hepatitis B, *HEPATITIS B virus, *LIFE cycles (Biology), *HEPATITIS B, *GENE expression

Abstract

Hepatitis B virus (HBV) DNA is much higher during HBeAg-positive chronic HBV infection (EP-CBI) than during HBeAg-negative chronic HBV infection (EN-CBI), although the necroinflammation in liver is minimal and the adaptive immune response is similar in both phases. We previously reported that mRNA levels of EVA1A were higher in EN-CBI patients. In this study, we aimed to investigate whether EVA1A inhibits HBV gene expression and examine the underlying mechanisms. The available cell models for HBV replication and model HBV mice were used to investigate how EVA1A regulates HBV replication and the antiviral activity based on gene therapy. The signaling pathway was determined through RNA sequencing analysis. The results demonstrated that EVA1A can inhibit HBV gene expression in vitro and in vivo. In particular, EVA1A overexpression resulted in accelerated HBV RNA degradation and activation of the PI3K-Akt-mTOR pathway, two processes that directly and indirectly inhibiting HBV gene expression. EVA1A is a promising candidate for treating chronic hepatitis B (CHB). In conclusion, EVA1A is a new host restriction factor that regulates the HBV life cycle via a nonimmune process. • EVA1A can inhibit HBV replication in vitro and in vivo. • This depended on activation of the PI3K-Akt-mTOR signaling pathway and acceleration of HBV RNA degradation. • EVA1A-based gene therapy significantly reduced HBV antigen expression and replication in model CHB mice. • EVA1A is a novel host factor that can suppress HBV replication. [ABSTRACT FROM AUTHOR]

Published

2023

16. ABCB5 promotes melanoma metastasis through enhancing NF-κB p65 protein stability.

Author

Wang, Shenghao, Tang, Li, Lin, Junyu, Shen, Zhongliang, Yao, Yikun, Wang, Wei, Tao, Shuai, Gu, Chenjian, Ma, Jie, Xie, Youhua, and Liu, Yanfeng

Subjects

*SKIN cancer, *SKIN diseases, *MELANOMA, *METASTASIS, *XENOGRAFTS

Abstract

Melanoma is the most aggressive type of skin cancer. Melanoma has an extremely poor prognosis because of its high potential for vascular invasion, metastasis and recurrence. The mechanism of melanoma metastasis is not well understood. ATP-binding cassette sub-family B member 5 (ABCB5) plays a key role in melanoma growth. However, it is uncertain what function ABCB5 may exert in melanoma metastasis. In this report, we for the first time demonstrate ABCB5 as a crucial factor that promotes melanoma metastasis. ABCB5 positive (ABCB5 + ) malignant melanoma initiating cells (MMICs) display a higher metastatic potential compared with ABCB5 negative (ABCB5 - ) melanoma subpopulation. Knockdown of ABCB5 expression reduces melanoma cell migration and invasion in vitro and melanoma pulmonary metastasis in tumor xenograft mice. ABCB5 and NF-κB p65 expression levels are positively correlated in both melanoma tissues and cell lines. Consequently, ABCB5 activates the NF-κB pathway by inhibiting p65 ubiquitination to enhance p65 protein stability. Our finding highlights ABCB5 as a novel pro -metastasis factor and provides a potential therapeutic target for melanoma. [ABSTRACT FROM AUTHOR]

Published

2017

17. Hepatocyte nuclear factor 1α downregulates HBV gene expression and replication by activating the NF-κB signaling pathway.

Author

Lin, Junyu, Gu, Chenjian, Shen, Zhongliang, Liu, Yanfeng, Wang, Wei, Tao, Shuai, Cui, Xiaoxian, Liu, Jing, and Xie, Youhua

Subjects

*HEPATOCYTE nuclear factors, *GENE expression, *DOWNREGULATION, *HEPATITIS B virus, *VIRAL replication

Abstract

The role of hepatocyte nuclear factor 1α (HNF1α) in the regulation of gene expression and replication of hepatitis B virus (HBV) is not fully understood. Previous reports have documented the induction of the expression of viral large surface protein (LHBs) by HNF1α through activating viral Sp1 promoter. Large amount of LHBs can block the secretion of hepatitis B surface antigen (HBsAg). Here we found that HNF1α overexpression inhibited HBV gene expression and replication in Huh7 cells, resulting in marked decreases in HBsAg, hepatitis B e antigen (HBeAg) and virion productions. In contrast, knockdown of endogenous HNF1α expression enhanced viral gene expression and replication. This HNF1α-mediated inhibition did not depend on LHBs. Instead, HNF1α promoted the expression of NF-κB p65 and slowed p65 protein degradation, leading to nuclear accumulation of p65 and activation of the NF-κB signaling, which in turn inhibited HBV gene expression and replication. The inhibitor of the NF-κB signaling, IκBα-SR, could abrogate this HNF1α-mediated inhibition. While the dimerization domain of HNF1α was dispensable for the induction of LHBs expression, all the domains of HNF1α was required for the inhibition of HBV gene expression. Our findings identify a novel role of HNF1α in the regulation of HBV gene expression and replication. [ABSTRACT FROM AUTHOR]

Published

2017

18. Nuclear factor Y regulates ancient budgerigar hepadnavirus core promoter activity.

Author

Shen, Zhongliang, Liu, Yanfeng, Luo, Mengjun, Wang, Wei, Liu, Jing, Liu, Wei, Pan, Shaokun, and Xie, Youhua

Subjects

*NF-kappa B, *GENETIC regulation, *HEPATITIS viruses, *GENOMES, *GENE expression in viruses

Abstract

Endogenous viral elements (EVE) in animal genomes are the fossil records of ancient viruses and provide invaluable information on the origin and evolution of extant viruses. Extant hepadnaviruses include avihepadnaviruses of birds and orthohepadnaviruses of mammals. The core promoter (Cp) of hepadnaviruses is vital for viral gene expression and replication. We previously identified in the budgerigar genome two EVEs that contain the full-length genome of an ancient budgerigar hepadnavirus (eBHBV1 and eBHBV2). Here, we found eBHBV1 Cp and eBHBV2 Cp were active in several human and chicken cell lines. A region from nt −85 to −11 in eBHBV1 Cp was critical for the promoter activity. Bioinformatic analysis revealed a putative binding site of nuclear factor Y (NF-Y), a ubiquitous transcription factor, at nt −64 to −50 in eBHBV1 Cp. The NF-Y core binding site (ATTGG, nt −58 to −54) was essential for eBHBV1 Cp activity. The same results were obtained with eBHBV2 Cp and duck hepatitis B virus Cp. The subunit A of NF-Y (NF-YA) was recruited via the NF-Y core binding site to eBHBV1 Cp and upregulated the promoter activity. Finally, the NF-Y core binding site is conserved in the Cps of all the extant avihepadnaviruses but not of orthohepadnaviruses. Interestingly, a putative and functionally important NF-Y core binding site is located at nt −21 to −17 in the Cp of human hepatitis B virus. In conclusion, our findings have pinpointed an evolutionary conserved and functionally critical NF-Y binding element in the Cps of avihepadnaviruses. [ABSTRACT FROM AUTHOR]

Published

2016

19. Comparative Transcriptomic Analysis of Primary Duck Hepatocytes Provides Insight into Differential Susceptibility to DHBV Infection.

Author

Yan, Liang, Qu, Su, Liu, Gang, Liu, Lei, Yu, Yao, Ding, Guohui, Zhao, Yanfeng, Li, Yixue, Xie, Youhua, Zhang, Junqi, and Qu, Di

Subjects

*DUCK hepatitis B virus, *HEPATITIS B, *LIVER cells, *DISEASE susceptibility, *BLOOD serum analysis, *COMPARATIVE studies, *DIAGNOSIS

Abstract

Primary duck hepatocytes (PDH) displays differential susceptibility to duck hepatitis B virus when maintained in the media supplemented with fetal bovine serum or dimethyl sulfoxide (DMSO) which has been widely used for the maintenance of hepatocytes, and prolonging susceptibility to hepadnavirus. However the mechanism underlying maintenance of susceptibility to hepadnavirus by DMSO treatment remains unclear. In this study, a global transcriptome analysis of PDHs under different culture conditions was conducted for investigating the effects of DMSO on maintenance of susceptibility of PDH to DHBV in vitro. The 384 differential expressed genes (DEGs) were identified by comparisons between each library pair (PDHs cultured with or without DMSO or fresh isolated PDH). We analyzed canonical pathways in which the DEGs were enriched in Hepatic Fibrosis / Hepatic Stellate Cell Activation, Bile Acid Biosynthesis and Tight Junction signaling. After re-annotation against human genome data, the 384 DEGs were pooled together with proteins belonging to hepatitis B pathway to construct a protein-protein interaction network. The combination of decreased expression of liver-specific genes (CYP3A4, CYP1E1, CFI, RELN and GSTA1 et al) with increased expression of hepatocyte-dedifferentiation-associated genes (PLA2G4A and PLCG1) suggested that in vitro culture conditions results in the fading of hepatocyte phenotype in PDHs. The expression of seven DEGs associated with tight junction formation (JAM3, PPP2R2B, PRKAR1B, PPP2R2C, MAGI2, ACTA2 and ACTG2) was up-regulated after short-term culture in vitro, which was attenuated in the presence of DMSO. Those results could shed light on DHBV infection associated molecular events affected by DMSO. [ABSTRACT FROM AUTHOR]

Published

2016

20. Interleukin-33 mediates both immune-related and non-immune-related inhibitory effects against hepatitis B virus.

Author

Gao, Zixiang, Shen, Zhongliang, Wu, Jingwen, Song, Yingying, Liu, Nannan, Deng, Qiang, Xie, Youhua, and Liu, Jing

Subjects

*HEPATITIS B virus, *LIVER histology, *HEPATITIS B, *INTERLEUKIN-33, *CHRONIC hepatitis B, *HEPATIC fibrosis

Abstract

Chronic infection by hepatitis B virus (HBV) is associated with high risks of liver fibrosis, cirrhosis and hepatocellular carcinoma. HBV covalently closed circular DNA (cccDNA) in the nucleus of infected hepatocyte serves as transcription template. Neither natural resolution of acute infection nor current treatment options for chronic infection are believed to cause cccDNA clearance. We previously showed that injection of IL-33-expressing plasmid facilitated clearance of intrahepatic HBV DNA in a mouse model of HBV persistence. In this work, HBV-targeting therapeutic effects of IL-33 were further explored. Murine IL-33 delivered by recombinant adeno-associated virus (AAV-mIL-33) induced clearance of both serum HBV markers and intrahepatic HBV DNA in two mouse models of HBV persistence based on replicon plasmid and recombinant cccDNA (rcccDNA) respectively. Clearance was associated with serum ALT elevations and liver infiltrations by CD4+ and CD8+ T cells, indicating IL-33-induced cellular immune responses against HBV-harboring cells. Adoptive transfer of splenocytes from AAV-mIL-33-cured mice was indeed sufficient to engender similar clearance in recipient mice. In vitro , intracellular, instead of extracellular, IL-33 was mainly responsible for repressing viral transcription, protein production and genome replication in Huh7 cells transfected with HBV replicon or rcccDNA. IL-33 was shown to be recruited onto rcccDNA minichromosome accompanied by loss of transcriptional activation epigenetic marks. Finally, transfection of IL-33 into HBV-infected HepG2/NTCP cells resulted in reduced transcription, antigen expression and genome replication, suggesting repression of canonical cccDNA. These data demonstrated diverse inhibitory effects on HBV and HBV-infected cells mediated by IL-33, and suggest IL-33 as an interesting therapeutic candidate. • Adeno-associated virus expressing mouse IL-33 (AAV-mIL-33) induced HBV clearance in two mouse models of HBV persistence. • IL-33-induced cellular immune responses engendered HBV clearance in vivo. • IL-33 could repress HBV transcription and replication in both HBV replicon and recombinant cccDNA (rcccDNA) systems. • IL-33 was shown to be recruited onto rcccDNA accompanied by loss of transcriptional activation epigenetic marks. • IL-33 also inhibited HBV gene expression and replication in infection systems. [ABSTRACT FROM AUTHOR]

Published

2022

21. A broadly reactive monoclonal antibody detects multiple genotypes of hepatitis B virus X protein.

Author

Wei, Lili, Shen, Zhongliang, Zhao, Xue, Wu, Yanxin, Liu, Wei, Zhang, Junqi, Xie, Youhua, and Liu, Jing

Subjects

*HEPATITIS B virus, *MONOCLONAL antibodies, *GENOTYPES, *VIRAL proteins, *IMMUNOBLOTTING, *IMMUNOFLUORESCENCE, *LIVER cells

Abstract

A highly specific and broadly reactive monoclonal antibody against hepatitis B virus X (HBx) protein was developed that detected, in both immunoblotting and immunofluorescence, HBx proteins of seven of the eight currently known genotypes of HBV, which were overexpressed in cultured cells. Evaluation of HBx expression levels in cultured hepatocytes using this monoclonal antibody showed that cells transiently and stably transfected with HBV genomes expressed far less HBx protein than cells transiently transfected with an HBx overexpression plasmid routinely used for studying HBx functions. The availability of such sensitive and broadly reactive monoclonal antibodies against HBx will enable more-quantitative studies of HBx functions. [ABSTRACT FROM AUTHOR]

Published

2014

22. Impact of an Altered PROX1 Expression on Clinicopathology, Prognosis and Progression in Renal Cell Carcinoma.

Author

Lv, Tao, Liu, Yanfeng, Zhang, Jianping, Xu, Le, Zhu, Yu, Yin, Hankun, An, Huimin, Lin, Zongming, Xie, Youhua, and Chen, Lian

Subjects

*CANCER invasiveness, *GENE expression, *RENAL cell carcinoma, *TRANSCRIPTION factors, *LYMPH node cancer, *METASTASIS, *PROGNOSIS

Abstract

The transcription factor PROX1 (prospero homeobox 1) has a critical role in the development of various organs, and has been implicated in both oncogenic and tumor-suppressive functions in human cancers. However, the role of PROX1 in the development of renal cell carcinomas (RCCs) has not yet been studied. Here, we reported that PROX1 expression was decreased in human RCC tissues compared with adjacent normal tissues. In RCC tissues, however, poorly differentiated RCC expressed higher PROX1 levels compared with well-differentiated RCC. In addition, the PROX1 immunostaining levels were positively correlated with tumor nuclear grade and lymph node metastasis. Further, high PROX1 expression indicated poor survival for patients. These findings imply that in the different developmental stages of RCC, PROX1 may exert distinct functions according to the specific microenvironment of tumor. Moreover, in vitro experiments revealed that PROX1 overexpression enhanced the proliferation and migration of RCC cells; conversely, PROX1 depletion by siRNA attenuated the proliferation and migration of RCC cells. Collectively, these observations suggest that PROX1 plays an important role in RCC development and progression, and PROX1 may be a novel target for prevention and treatment of RCC. [ABSTRACT FROM AUTHOR]

Published

2014

23. Broad neutralization of SARS-CoV-2 variants by an inhalable bispecific single-domain antibody.

Author

Li, Cheng, Zhan, Wuqiang, Yang, Zhenlin, Tu, Chao, Hu, Gaowei, Zhang, Xiang, Song, Wenping, Du, Shujuan, Zhu, Yuanfei, Huang, Keke, Kong, Yu, Zhang, Meng, Mao, Qiyu, Gu, Xiaodan, Zhang, Yi, Xie, Youhua, Deng, Qiang, Song, Yuanlin, Chen, Zhenguo, and Lu, Lu

Subjects

*SARS-CoV-2, *SARS-CoV-2 Omicron variant, *BISPECIFIC antibodies, *COVID-19 vaccines, *INHALATION administration, *PROTEIN domains

Abstract

The effectiveness of SARS-CoV-2 vaccines and therapeutic antibodies have been limited by the continuous emergence of viral variants and by the restricted diffusion of antibodies from circulation into the sites of respiratory virus infection. Here, we report the identification of two highly conserved regions on the Omicron variant receptor-binding domain recognized by broadly neutralizing antibodies. Furthermore, we generated a bispecific single-domain antibody that was able to simultaneously and synergistically bind these two regions on a single Omicron variant receptor-binding domain as revealed by cryo-EM structures. We demonstrated that this bispecific antibody can be effectively delivered to lung via inhalation administration and exhibits exquisite neutralization breadth and therapeutic efficacy in mouse models of SARS-CoV-2 infections. Importantly, this study also deciphered an uncommon and highly conserved cryptic epitope within the spike trimeric interface that may have implications for the design of broadly protective SARS-CoV-2 vaccines and therapeutics. [Display omitted] • Conserved epitopes outside of the RBM of SARS-CoV-2 spike RBD • A bispecific single-domain antibody (bn03) broadly neutralizes SARS-CoV-2 variants • Two arms of bn03 can bind simultaneously and synergistically to one RBD of spike trimer • Inhalation of bn03 can effectively treat SARS-CoV-2 infection in hACE2 mice Therapeutic effects against SARS-CoV-2 infection are seen in mice after inhalation of an engineered, bispecific, single-domain antibody that simultaneously targets two points on the spike protein receptor-binding domain. [ABSTRACT FROM AUTHOR]

Published

2022

24. Prox1 Directly Interacts with LSD1 and Recruits the LSD1/NuRD Complex to Epigenetically Co-Repress CYP7A1 Transcription.

Author

Ouyang, Huafang, Qin, Yi, Liu, Yanfeng, Xie, Youhua, and Liu, Jing

Subjects

*GENETIC transcription, *EPIGENETICS, *BLOOD cholesterol, *REPRESSION (Psychology), *BILE acids, *ALPHA fetoproteins, *IMMUNOPRECIPITATION, *DEMETHYLATION

Abstract

Cholesterol 7α-hydroxylase (CYP7A1) catalyzes the first and rate-limiting step in the classical pathway of bile acids synthesis in liver and is crucial for maintaining lipid homeostasis. Hepatocyte nuclear factor 4α (HNF4α) and α1-fetoprotein transcription factor (FTF) are two major transcription factors driving CYP7A1 promoter activity in hepatocytes. Previous researches have shown that Prospero-related homeobox (Prox1) directly interacts with both HNF4α and FTF and potently co-represses CYP7A1 transcription and bile acid synthesis through unidentified mechanisms. In this work, mechanisms involved in Prox1-mediated co-repression were explored by identifying Prox1-associated proteins using immunoprecipitation followed by mass spectrometry (IP-MS) methodology. Multiple components of the epigenetically repressive lysine-specific demethylase 1 (LSD1)/nucleosome remodeling and histone deacetylase (NuRD) complex, most notably LSD1 and histone deacetylase 2 (HDAC2), were found to be associated with Prox1 and GST pulldown assay demonstrated that Prox1 directly interacts with LSD1. Sequential chromatin immunoprecipitation (ChIP) assays showed that Prox1 co-localizes with HNF4α, LSD1 and HDAC2 on CYP7A1 promoter in HepG2 cells. Furthermore, by using ChIP assay on HepG2 cells with endogenous Prox1 knocked down by RNA interference, Prox1 was shown to recruit LSD1 and HDAC2 onto CYP7A1 promoter and cause increased H3K4 demethylation. Finally, bile acids treatment of HepG2 cells, which significantly repressed CYP7A1 transcription, resulted in increased Prox1 and LSD1/NuRD complex occupancy on CYP7A1 promoter with a concurrent increase in H3K4 demethylation and H3/H4 deacetylation. These results showed that Prox1 interacts with LSD1 to recruit the repressive LSD1/NuRD complex to CYP7A1 promoter and co-represses transcription through epigenetic mechanisms. In addition, such Prox1-mediated epigenetic repression is involved in the physiologically essential negative feedback inhibition of CYP7A1 transcription by bile acids. [ABSTRACT FROM AUTHOR]

Published

2013

25. Hepatitis C virus genotype diversity in Shanghai, China.

Author

Pan, Shaokun, Rao, Yuliang, Li, Jiangyan, Yang, Huijuan, Tang, Jing, Zhong, Renqian, Zhai, Jianwei, Liu, Jing, Wang, Hao, Liu, Wei, and Xie, Youhua

Subjects

*HEPATITIS C virus, *GENOTYPE-environment interaction, *VIRAL genomes, *NUCLEOTIDE sequence, *DISEASE prevalence

Abstract

We studied 67 hepatitis C virus (HCV) isolates from 64 hospitalized patients in Shanghai, China. Genotype 1 was prevalent, and genotypes 2, 3, 6 were found for the first time in Shanghai. A rare mixed infection with three subtypes (1a, 1b, 2a) was found. The complete genome sequence of a subtype 3b isolate was determined and analyzed. [ABSTRACT FROM AUTHOR]

Published

2013

26. Evidence for inter- and intra-clade recombinations in rabies virus

Author

Liu, Wei, Liu, Yanfeng, Liu, Jing, Zhai, Jianwei, and Xie, Youhua

Subjects

*EVIDENCE, *RABIES virus, *RNA viruses, *PHYLOGENY, *Y chromosome, *GENOMES, *GENETIC recombination, *EVOLUTIONARY theories, *CONFERENCES & conventions

Abstract

Abstract: Homologous recombination is considered rare in negative-strand RNA viruses and has not been reported for rabies virus. In this study, full-length genomes of 44 rabies virus strains were analyzed for potential homologous recombination events. Phylogenetic analysis classified these strains into three clades. By applying six different recombination detection methods, one inter-clade and one intra-clade potential recombination events were identified with high confidence values. Software-predicted recombination break points of the two events were all located within the polymerase gene. This report presents the first evidence suggesting the possibility of homologous recombination in rabies virus, which could provide valuable insights for understanding the diversity and evolution of rabies virus as well as other negative-strand RNA viruses. [Copyright &y& Elsevier]

Published

2011

27. Identification of natural recombination in duck hepatitis B virus

Author

Liu, Wei, Zhai, Jianwei, Liu, Jing, and Xie, Youhua

Subjects

*HEPATITIS B virus, *RECOMBINANT viruses, *PHYLOGENY, *VIRAL genetics, *VIRUS isolation

Abstract

Abstract: Due to its high similarity to human hepatitis B virus (HBV), duck HBV (DHBV) is often used as an important model for HBV research. While inter-genotypic recombination of HBV is common, it has not been reported with DHBV. In this study, 32 non-redundant DHBV complete genomes were analyzed using phylogenetic methods and classified into two clusters, corresponding to the ‘Chinese’ and ‘Western country’ branches previously reported based on geographical distribution. One ‘Chinese’ branch strain was isolated in Australia and three ‘Western country’ branch strains were isolated in China, suggesting cross-geographical distribution of both branches. Recombination analyses of the 32 DHBV genomes identified two possible inter-genotypic recombination events with high confidence value. These recombination events occurred between the lineages represented, respectively, by the Chinese isolate GD3 (AY536371, ‘Chinese’ branch) and the American isolate DHBV16 (K01834, ‘Western country’ branch), giving rise to two Chinese recombinant isolates CH4 (EU429324) and CH6 (EU429326). The identification of inter-genotypic recombination among circulating DHBV isolates suggests the usefulness of DHBV as a model for studying the mechanism of HBV recombination. [Copyright &y& Elsevier]

Published

2010

28. Synthesis and evaluation of enantiomers of hydroxychloroquine against SARS-CoV-2 in vitro.

Author

Ni, Yong, Liao, Jinbiao, Qian, Zhenlong, Wu, Chunxiu, Zhang, Xiangyu, Zhang, Ji, Xie, Youhua, and Jiang, Sheng

Subjects

*SARS-CoV-2, *HYDROXYCHLOROQUINE, *ENANTIOMERS, *RESOLUTION (Chemistry), *SMALL molecules, *DRUG repositioning

Abstract

[Display omitted] Since the end of 2019, the outbreak of Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) has evolved into a global pandemic. There is an urgent need for effective and low-toxic antiviral drugs to remedy Remdesivir's limitation. Hydroxychloroquine, a broad spectrum anti-viral drug, showed inhibitory activity against SARS-CoV-2 in some studies. Thus, we adopted a drug repurposing strategy, and further investigated hydroxychloroquine. We obtained different configurations of hydroxychloroquine side chains by using chiral resolution technique, and successfully furnished R-/S-hydroxychloroquine sulfate through chemical synthesis. The R configuration of hydroxychloroquine was found to exhibit higher antiviral activity (EC50 = 3.05 μM) and lower toxicity in vivo. Therefore, R-HCQ is a promising lead compound against SARS-CoV-2. Our research provides new strategy for the subsequent research on small molecule inhibitors against SARS-CoV-2. [ABSTRACT FROM AUTHOR]

Published

2022

29. Characterization of a novel isoform of murine interferon regulatory factor 3

Author

Zhai, Jianwei, Gao, Daming, Liu, Wei, Hong, Ran, Qin, Yi, Ouyang, Huafang, Kong, Yuying, Wang, Yuan, Xie, Youhua, and Liu, Jing

Subjects

*INTERFERONS, *TRANSCRIPTION factors, *LABORATORY mice, *NEWCASTLE disease virus, *CELL nuclei, *BIOLOGICAL assay

Abstract

Abstract: Interferon (IFN) regulatory factors (IRFs) are a family of transcription mediators involved in the regulation of type I IFN (IFN-α/β) transcription. Among the nine already identified IRFs, IRF-3 is a constitutively and ubiquitously expressed and plays a critical role in the transcriptional activation of type I IFN and IFN-stimulated genes including IFN-α1, IFN-β and RANTES. In the present study, we report the identification of a novel alternatively spliced transcript of murine Irf-3 gene (mIrf-3) designated mIRF-3a. mIRF-3a is ubiquitously present in mouse tissues along with mIRF-3 and could be translocated into the nucleus in uninfected L929 cells. EMSA and reporter assay demonstrated that mIRF-3a binds to ISRE sequences in murine Ifn-β promoter and represses Ifn-β promoter activation induced by Newcastle disease virus infection. These results suggest that mIRF-3a may act as a modulator of mIRF-3 functions in vivo. [Copyright &y& Elsevier]

Published

2008

30. Suppression of hLRH-1 mediated by a DNA vector-based RNA interference results in cell cycle arrest and induction of apoptosis in hepatocellular carcinoma cell BEL-7402

Author

Wang, Shuiliang, Lan, Fenghua, Huang, Lianghu, Dong, Lihong, Zhu, Zhongyong, Li, Zonghai, Xie, Youhua, and Fu, Jiliang

Subjects

*RNA, *NUCLEIC acids, *ORGANS (Anatomy), *PHYSIOLOGICAL control systems

Abstract

Abstract: RNA interference (RNAi) is the process by which double-stranded RNA directs sequence-specific degradation of mRNA. A DNA vector-based approach has been shown to be able to trigger RNA interference in mammalian cells successfully. LRH-1 is an orphan nuclear receptor predominantly expressed in tissues of endodermal origin, where it controls development and cholesterol homeostasis. In the present study, we demonstrated that the expression of hLRH-1 and cyclin E1 in BEL-7402 cells could be suppressed by up to ∼80% via DNA vector-based RNA interference. The suppression of hLRH-1 resulted in cell cycle arrest mediated by the down-regulation of cyclin E1. Induction of apoptosis and down-regulation of Gadd45β were also shown in hLRH-1 knock down BEL-7402 cells. These results, together with the findings that Gadd45β remained unchanged in cyclin E1 RNAi cells, suggested that the induction of apoptosis by knock down of hLRH-1 was closely related to the down-regulation of Gadd45β. [Copyright &y& Elsevier]

Published

2005

31. In vitro biochemical and thermodynamic characterization of nucleocapsid protein of SARS

Author

Luo, Haibin, Ye, Fei, Sun, Tao, Yue, Liduo, Peng, Shuying, Chen, Jing, Li, Guowei, Du, Yi, Xie, Youhua, Yang, Yiming, Shen, Jianhua, Wang, Yuan, Shen, Xu, and Jiang, Hualiang

Subjects

*POLYMERS, *RESONANCE, *CORONAVIRUSES, *GEL electrophoresis

Abstract

The major biochemical and thermodynamic features of nucelocapsid protein of SARS coronavirus (SARS_NP) were characterized by use of non-denatured gel electrophoresis, size-exclusion chromatographic and surface plasmon resonance (SPR) techniques. The results showed that SARS_NP existed in vitro as oligomer, more probably dimer, as the basic functional unit. This protein shows its maximum conformational stability near pH 9.0, and it seems that its oligomer dissociation and protein unfolding occur simultaneously. Thermal-induced unfolding for SARS_NP was totally irreversible. Both the thermal and chemical denaturant-induced denaturation analyses showed that oligomeric SARS_NP unfolds and refolds through a two-state model, and the electrostatic interactions among the charge groups of SARS_NP made a significant contribution to its conformational stability. [Copyright &y& Elsevier]

Published

2004

32. Molecular cloning, expression, purification, and mass spectrometric characterization of 3C-like protease of SARS coronavirus

Author

Sun, Haifang, Luo, Haibin, Yu, Changying, Sun, Tao, Chen, Jing, Peng, Shuying, Qin, Jun, Shen, Jianhua, Yang, Yiming, Xie, Youhua, Chen, Kaixian, Wang, Yuan, Shen, Xu, and Jiang, Hualiang

Subjects

*SARS disease, *ADULT respiratory distress syndrome, *CORONAVIRUS diseases, *MASS spectrometry

Abstract

Severe acute respiratory syndrome (SARS) is an acute respiratory illness, which has broken out in China. It has been known that SARS coronavirus (SARS_CoV) is a novel human coronavirus and is responsible for SARS infection. Belonging to one of the major proteins associated with SARS_CoV, SARS 3C-like protease (SARS_3CLpro) functions as a cysteine protease engaging in the proteolytic cleavage of the viral precursor polyprotein to a series of functional proteins required for coronavirus replication and is considered as an appealing target for designing anti-SARS agents. To facilitate the studies regarding the functions and structures of SARS_3CLpro, in this report the synthetic genes encoding 3CLpro of SARS_CoV were assembled, and the plasmid was constructed using pQE30 as vector and expressed in Escherichia coli M15 cells. The highly yielded (∼15 mg/L) expressed protease was purified by use of NTA-Ni2+ affinity chromatography and FPLC system, and its sequence was determined by LC/MS with the residue coverage of 46.4%. [Copyright &y& Elsevier]

Published

2003

33. Bioinformatic analysis of human receptor nr5a2(hb1f) genomic sequence.

Author

Zhang Chengkang, Lin Wei, Cai Yanning, Dong Hui, Li Mei, Fu Gang, Xie Youhua, Guyang, Huang M., and Wang Yuan

Subjects

*NUCLEAR receptors (Biochemistry), *NUCLEOTIDE sequence

Abstract

Describes a bioinformatic analysis of human nuclear receptor nr5a2(hb1f) genomic sequence. Implication of sequence comparison and prediction algorithms on the possibility of additional coding regions in the 210 kb genomic sequence besides known exons; Comparison of the structures of nr5a loci in different species.

Published

2002

34. Prior transient exposure to interleukin-21 delivered by recombinant adeno-associated virus vector protects mice from hepatitis B virus persistence.

Author

Shen, Zhongliang, Gao, Zixiang, Gu, Chenjian, Wu, Jingwen, Wang, Jinyu, Zhang, Jiming, Xie, Youhua, and Liu, Jing

Subjects

*HEPATITIS B virus, *ADENO-associated virus, *HEPATITIS B, *RECOMBINANT viruses, *CHRONIC hepatitis B, *INTERLEUKIN-21

Abstract

Chronic infection of hepatitis B virus (HBV) is a high risk factor for hepatic diseases, such as liver fibrosis, cirrhosis and hepatocellular carcinoma. Non-responders and hyporesponders to HBV vaccine are not protected from HBV infection. Patients that achieve autonomous or treatment-induced recovery are at risk of reactivation due to persistence of HBV covalently closed circular DNA (cccDNA) in hepatocytes. Interleukin 21 (IL-21) is a key regulator of HBV clearance in mouse models of HBV persistence: IL-21-based therapies effectively induces HBV clearance and protects mice from subsequent re-challenge. In this study, we explore the possibility of using IL-21 as prophylaxis against HBV by using mouse models of HBV persistence. HBV-naïve mice were transiently exposed to exogenous IL-21 through injection with recombinant adeno-associated virus expressing mouse IL-21 (AAV-IL-21). After extraneous IL-21 protein and DNA had become undetectable, mice were challenged with persistence-inducing HBV replicon plasmid through hydrodynamic injection. Viral persistence was analyzed by measuring viral antigens and DNA markers in serum and intrahepatic HBV DNA. For mechanistic studies, CD8+ T cell functions were blocked by repeated intraperitoneal injections of CD8 monoclonal antibodies in HBV-challenged mice. AAV-IL-21-injected mice quickly cleared HBV after HBV replicon challenge. In contrast, untreated mice and mice injected with control virus (AAV-Ctrl) allowed establishment of HBV persistence. Mechanistically, mice with prior IL-21 exposure displayed marked intrahepatic CD8+ T cell infiltrations, and CD8 blocking experiments demonstrated that CD8+ T cell responses functionally contributed toward clearance. • 1: Transient expression of IL-21 did not cause notable adverse effects in mice. • 2: Mice with prior IL-21 exposure prevented HBV from establishing persistence. • 3: CD8+ T cell contributed toward HBV clearance in IL-21-pretreated mice. • 4: IL-21 pretreatment is a potential prophylactic option for HBV. [ABSTRACT FROM AUTHOR]

Published

2021

35. FRI-203-Inhibition of hepatitis B virus replication by FAM176A via activation of PI3K-AKT-mTOR signaling pathway.

Author

Yu, Jie, shen, zhongliang, Zhang, Jiming, and Xie, Youhua

Subjects

*HEPATITIS B virus, *VIRAL replication, *CHRONIC hepatitis B, *RNA sequencing

Published

2019

36. SARS-CoV-2 binds platelet ACE2 to enhance thrombosis in COVID-19.

Author

Zhang, Si, Liu, Yangyang, Wang, Xiaofang, Yang, Li, Li, Haishan, Wang, Yuyan, Liu, Mengduan, Zhao, Xiaoyan, Xie, Youhua, Yang, Yan, Zhang, Shenghui, Fan, Zhichao, Dong, Jianzeng, Yuan, Zhenghong, Ding, Zhongren, Zhang, Yi, and Hu, Liang

Subjects

*COVID-19, *SARS-CoV-2, *BLOOD platelets, *MEAN platelet volume, *BLOOD platelet aggregation, *THROMBIN receptors, *GRANZYMES, *CEREBRAL embolism & thrombosis, *BLOOD platelet disorders

Abstract

Background: Critically ill patients diagnosed with COVID-19 may develop a pro-thrombotic state that places them at a dramatically increased lethal risk. Although platelet activation is critical for thrombosis and is responsible for the thrombotic events and cardiovascular complications, the role of platelets in the pathogenesis of COVID-19 remains unclear. Methods: Using platelets from healthy volunteers, non-COVID-19 and COVID-19 patients, as well as wild-type and hACE2 transgenic mice, we evaluated the changes in platelet and coagulation parameters in COVID-19 patients. We investigated ACE2 expression and direct effect of SARS-CoV-2 virus on platelets by RT-PCR, flow cytometry, Western blot, immunofluorescence, and platelet functional studies in vitro, FeCl3-induced thrombus formation in vivo, and thrombus formation under flow conditions ex vivo. Results: We demonstrated that COVID-19 patients present with increased mean platelet volume (MPV) and platelet hyperactivity, which correlated with a decrease in overall platelet count. Detectable SARS-CoV-2 RNA in the blood stream was associated with platelet hyperactivity in critically ill patients. Platelets expressed ACE2, a host cell receptor for SARS-CoV-2, and TMPRSS2, a serine protease for Spike protein priming. SARS-CoV-2 and its Spike protein directly enhanced platelet activation such as platelet aggregation, PAC-1 binding, CD62P expression, α granule secretion, dense granule release, platelet spreading, and clot retraction in vitro, and thereby Spike protein enhanced thrombosis formation in wild-type mice transfused with hACE2 transgenic platelets, but this was not observed in animals transfused with wild-type platelets in vivo. Further, we provided evidence suggesting that the MAPK pathway, downstream of ACE2, mediates the potentiating role of SARS-CoV-2 on platelet activation, and that platelet ACE2 expression decreases following SARS-COV-2 stimulation. SARS-CoV-2 and its Spike protein directly stimulated platelets to facilitate the release of coagulation factors, the secretion of inflammatory factors, and the formation of leukocyte–platelet aggregates. Recombinant human ACE2 protein and anti-Spike monoclonal antibody could inhibit SARS-CoV-2 Spike protein-induced platelet activation. Conclusions: Our findings uncovered a novel function of SARS-CoV-2 on platelet activation via binding of Spike to ACE2. SARS-CoV-2-induced platelet activation may participate in thrombus formation and inflammatory responses in COVID-19 patients. [ABSTRACT FROM AUTHOR]

Published

2020

37. SAT463 - Characterization of IL-21-expressing recombinant hepatitis B virus (HBV) as a therapeutic agent targeting persisting HBV infection.

Author

Shen, Zhongliang, Wu, Jingwen, Liu, Jing, Xie, Youhua, and Zhang, Jiming

Subjects

*HEPATITIS B virus, *INFECTION, *VIRAL hepatitis, *HEPATITIS B

Published

2020

38. SAT388 - A novel intrahepatic restriction factor, HMGA1, contributes to hepatitis B virus (HBV) replication in immune tolerant phase, serving as an anti-HBV target.

Author

Shen, Zhongliang, Wu, Jingwen, Liu, Jing, Xie, Youhua, and Zhang, Jiming

Subjects

*HEPATITIS B virus, *HEPATITIS A, *VIRAL hepatitis

Published

2020

39. PS-075-AAV-delivered IL-21 activates CD8+ T-cells to clear HBV replicon plasmid and cccDNA in mice.

Author

Shen, Zhongliang, Liu, Jing, Wu, Jingwen, Zhu, Yuanfei, Li, Gaiyun, Wang, Jun, Luo, Mengjun, Deng, Qiang, Zhang, Jiming, and Xie, Youhua

Subjects

*MEDICAL sciences, *MICE, *T cells, *CHRONIC hepatitis B, PERSISTENCE

Published

2019

40. Hepatitis B virus X protein is capable of down-regulating protein level of host antiviral protein APOBEC3G.

Author

Chen, Ruidong, Zhao, Xue, Wang, Yongxiang, Xie, Youhua, and Liu, Jing

Abstract

The apolipoprotein B mRNA editing catalytic polypeptide-like (APOBEC) family proteins bind RNA and single-stranded DNA, and create C-to-U base modifications through cytidine deaminase activity. APOBEC3G restricts human immunodeficiency virus 1 (HIV-1) infection by creating hypermutations in proviral DNA, while HIV-1-encoded vif protein antagonizes such restriction by targeting APOBEC3G for degradation. APOBEC3G also inhibits hepatitis B virus (HBV): APOBEC3G co-expression inhibits HBV replication and evidences exist indicating APOBEC3G-mediated HBV hypermutations in patients. HBV encodes a small non-structural X protein (HBx) with a recognized activating effect on HBV life cycle. In this work, we report the discovery that HBx selectively and dose-dependently decreases the protein level of co-expressed APOBEC3G in transfected Huh-7 cells. The effect was shown to take place post-translationally, but does not rely on protein degradation via proteasome or lysosome. Further work demonstrated that intracellular APOBEC3G is normally exported via exosome secretion and inhibition of exosome biogenesis causes retention of intracellular APOBEC3G. Finally, HBx co-expression specifically enhanced externalization of APOBEC3G via exosomes, resulting in decrease of intracellular APOBEC3G protein level. These data suggest the possibility that in addition to other mechanisms, HBx-mediated activation of HBV might also involve antagonizing of intracellular restriction factor APOBEC3G through promotion of its export. [ABSTRACT FROM AUTHOR]

Published

2017

41. Short-term intratracheal use of PEG-modified IL-2 and glucocorticoid persistently alleviates asthma in a mouse model.

Author

Wu, Kefei, Ma, Jiexian, Bai, Weiya, Cui, Xiaoxian, Han, Tao, Wang, Shiyuan, Xie, Youhua, and Xie, Yanhui

Published

2016

42. Efficient Inhibition of Hepatitis B Virus Infection by a preS1-binding Peptide.

Author

Ye, Xiaoli, Zhou, Ming, He, Yonggang, Wan, Yanmin, Bai, Weiya, Tao, Shuai, Ren, Yanqin, Zhang, Xinxin, Xu, Jianqing, Liu, Jing, Zhang, Junqi, Hu, Kanghong, and Xie, Youhua

Published

2016