keyword
https://read.qxmd.com/read/38292874/cytosine-base-editing-inhibits-hepatitis-b-virus-replication-and-reduces-hbsag-expression-in%C3%A2-vitro-and-in%C3%A2-vivo
#21
JOURNAL ARTICLE
Elena M Smekalova, Maria G Martinez, Emmanuel Combe, Anuj Kumar, Selam Dejene, Dominique Leboeuf, Chao-Ying Chen, J Robert Dorkin, Lan Shuan Shuang, Sarah Kieft, Lauren Young, Luis Alberto Barrera, Michael S Packer, Giuseppe Ciaramella, Barbara Testoni, Francine Gregoire, Fabien Zoulim
Chronic hepatitis B virus (HBV) infection remains a global health problem due to the lack of treatments that prevent viral rebound from HBV covalently closed circular (ccc)DNA. In addition, HBV DNA integrates in the human genome, serving as a source of hepatitis B surface antigen (HBsAg) expression, which impairs anti-HBV immune responses. Cytosine base editors (CBEs) enable precise conversion of a cytosine into a thymine within DNA. In this study, CBEs were used to introduce stop codons in HBV genes, HBs and Precore ...
March 12, 2024: Molecular Therapy. Nucleic Acids
https://read.qxmd.com/read/38288308/the-novel-mechanism-facilitating-chronic-hepatitis-b-infection-immunometabolism-and-epigenetic-modification-reprogramming
#22
REVIEW
Zhengmin Wang, Nan Liu, Yang Yang, Zhengkun Tu
Hepatitis B Virus (HBV) infections pose a global public health challenge. Despite extensive research on this disease, the intricate mechanisms underlying persistent HBV infection require further in-depth elucidation. Recent studies have revealed the pivotal roles of immunometabolism and epigenetic reprogramming in chronic HBV infection. Immunometabolism have identified as the process, which link cell metabolic status with innate immunity functions in response to HBV infection, ultimately contributing to the immune system's inability to resolve Chronic Hepatitis B (CHB)...
2024: Frontiers in Immunology
https://read.qxmd.com/read/38265511/enpp1-inhibits-the-transcription-activity-of-the-hepatitis-b-virus-pregenomic-promoter-by-upregulating-the-acetylation-of-lmnb1
#23
JOURNAL ARTICLE
Xinping Ma, Yuan Li, Huihui Zhu, Kai Lu, Yingli Huang, Xiaofang Li, Shuangyin Han, Hui Ding, Suofeng Sun
Current therapies for hepatitis B virus (HBV) infection can slow disease progression but cannot cure the infection, as it is difficult to eliminate or permanently silence HBV covalently closed circular DNA (cccDNA). The interaction between host factors and cccDNA is essential for their formation, stability, and transcriptional activity. Here, we focused on the regulatory role of the host factor ENPP1 and its interacting transcription factor LMNB1 in HBV replication and transcription to better understand the network of host factors that regulate HBV, which may facilitate the development of new antiviral drugs...
January 24, 2024: Archives of Virology
https://read.qxmd.com/read/38253259/pres1bp-mediates-inhibition-of-hepatitis-b-virus-replication-by-promoting-hbx-protein-degradation
#24
JOURNAL ARTICLE
Jun Wang, Xiaoxue Yuan, Yun Wang, Yu Zhang, Ming Han, Hongping Lu, Shunai Liu, Yang Zhang, Feilin Ge, Yan Liu, Jun Cheng
BACKGROUND: PreS1-binding protein (PreS1BP), recognized as a nucleolar protein and tumor suppressor, influences the replication of various viruses, including vesicular stomatitis virus (VSV) and herpes simplex virus type 1 (HSV-1). Its role in hepatitis B virus (HBV) replication and the underlying mechanisms, however, remain elusive. METHODS: We investigated PreS1BP expression levels in an HBV-replicating cell and animal model and analyzed the impact of its overexpression on viral replication metrics...
January 20, 2024: Virus Research
https://read.qxmd.com/read/38234727/replication-driven-hbv-cccdna-loss-in-chimeric-mice-with-humanized-livers
#25
Bai-Hua Zhang, Yuanping Zhou, Ben Tempel, Honggang Pan, Stephen Horrigan, Laura Luckenbaugh, Fabien Zoulim, Jianming Hu, Yong-Yuan Zhang
Hepatitis B virus (HBV) infection is largely noncytopathic and requires the establishment of covalently closed circular DNA (cccDNA), which is considered stable in the nuclei of infected cells. Although challenging, approaches to directly target cccDNA molecules or kill infected cells are recommended to eliminate cccDNA. Herein, cccDNA levels were investigated in HBV-infected chimeric mice with humanized livers. HBV-infected cells support robust replication, progressively retain viral products, and head for cytopathic destruction and cccDNA loss...
December 28, 2023: bioRxiv
https://read.qxmd.com/read/38226815/intrahepatic-homeobox-protein-msx-1-is-a-novel-host-restriction-factor-of-hepatitis-b-virus
#26
JOURNAL ARTICLE
Zhongliang Shen, Shenyan Zhang, Zixiang Gao, Xueping Yu, Jinyu Wang, Shaokun Pan, Ning Kang, Nannan Liu, Huijun Xu, Mu Liu, Yang Yang, Qiang Deng, Jing Liu, Youhua Xie, Jiming Zhang
Covalently closed circular DNA plays a key role for the persistence of hepatitis B virus (HBV) since it serves as the template for viral transcription. Identification of transcription factors that regulate HBV transcription not only provides insights into molecular mechanisms of viral life cycle regulation but may also provide potential antiviral targets. In this work, we identified host MSX1 as a novel restriction factor of HBV transcription. Meanwhile, we observed higher intrahepatic MSX1 expression in chronic hepatitis B virus (CHB) patients in immune active phase compared to those in immune tolerant phase, suggesting possible involvement of MSX1 in the regulation of HBV activity by the host...
January 16, 2024: Journal of Virology
https://read.qxmd.com/read/38215982/sulforaphane-effectively-inhibits-hbv-by-altering-treg-th17-immune-balance-and-the-mif-macrophages-polarizing-axis-in-vitro-and-in-vivo
#27
JOURNAL ARTICLE
Ruqing Xu, Yue Wu, Xia Xiang, Xiaoqin Lv, Miao He, Chang Xu, Guoqi Lai, Tingxiu Xiang
BACKGROUND: Hepatitis B virus (HBV) infection is a major public health problem. After HBV infection, viral antigens shift the immune balance in favor of viral escape. Sulforaphane (SFN) is a traditional Chinese medicine.It regulates multi-biological activities, including anti-inflammation, anticancer, and antiviral. However, few studies reported that SFN can inhibit HBV infection before. METHODS: An immunocompetent HBV CBA/CaJ mouse model and a co-culture model were used to explore the effect of SFN on HBV and whether SFN altered the immune balance after HBV infection...
January 10, 2024: Virus Research
https://read.qxmd.com/read/38190324/structure-activity-relationships-and-discovery-of-s-6-isopropyl-2-methoxy-3-3-methoxypropoxy-10-oxo-5-10-dihydro-6-h-pyrido-1-2-h-1-7-naphthyridine-9-carboxylic-acid-ab-452-a-novel-orally-available-hbv-rna-destabilizer
#28
JOURNAL ARTICLE
Dimitar Gotchev, Bruce D Dorsey, Duyan Nguyen, Ramesh Kakarla, Benjamin Dugan, Shuai Chen, Min Gao, Laurèn Bailey, Fei Liu, Troy Harasym, Tim Chiu, Sunny Tang, Amy C-H Lee, Andrew G Cole, Michael J Sofia
Approved therapies for hepatitis B virus (HBV) treatment include nucleos(t)ides and interferon alpha (IFN-α) which effectively suppress viral replication, but they rarely lead to cure. Expression of viral proteins, especially surface antigen of the hepatitis B virus (HBsAg) from covalently closed circular DNA (cccDNA) and the integrated genome, is believed to contribute to the persistence of HBV. This work focuses on therapies that target the expression of HBV proteins, in particular HBsAg, which differs from current treatments...
January 8, 2024: Journal of Medicinal Chemistry
https://read.qxmd.com/read/38181856/chromatin-binding-protein-hmgn1-promotes-hbv-cccdna-transcription-and-replication-by-regulating-the-phosphorylation-of-histone-3
#29
JOURNAL ARTICLE
Tan Ming, Liu Yuting, Dong Meiling, Cheng Shengtao, Ren Jihua, Zhang Hui, Chen Wanjin, Li Dian, Gao Tingting, Chen Juan, Zhang Zhenzhen
BACKGROUND AND AIMS: Direct elimination of cccDNA remains a formidable obstacle due to the persistent and stable presence of cccDNA in hepatocyte nuclei. The silencing of cccDNA transcription enduringly is one of alternative strategies in the treatment of hepatitis B. Protein binding to cccDNA plays an important role in its transcriptional regulation; thus, the identification of key factors involved in this process is of great importance. APPROACHES AND RESULTS: In the present study, high mobility group nucleosome binding domain 1 (HMGN1) was screened out based on our biotin-avidin enrichment system...
January 3, 2024: Antiviral Research
https://read.qxmd.com/read/38175123/ctcf-regulates-hepatitis-b-virus-cccdna-chromatin-topology
#30
JOURNAL ARTICLE
Mihaela Olivia Dobrica, Christy Susan Varghese, James Michael Harris, Jack Ferguson, Andrea Magri, Roland Arnold, Csilla Várnai, Joanna L Parish, Jane A McKeating
Hepatitis B Virus (HBV) is a small DNA virus that replicates via an episomal covalently closed circular DNA (cccDNA) that serves as the transcriptional template for viral mRNAs. The host protein, CCCTC-binding factor (CTCF), is a key regulator of cellular transcription by maintaining epigenetic boundaries, nucleosome phasing, stabilisation of long-range chromatin loops and directing alternative exon splicing. We previously reported that CTCF binds two conserved motifs within Enhancer I of the HBV genome and represses viral transcription, however, the underlying mechanisms were not identified...
January 2024: Journal of General Virology
https://read.qxmd.com/read/38161502/novel-approaches-to-inhibition-of-hbsag-expression-from-cccdna-and-chromosomal-integrants-a-review
#31
REVIEW
Ahmed H Abdelwahed, Brent D Heineman, George Y Wu
Hepatitis B virus (HBV) is a widely prevalent liver infection that can cause acute or chronic hepatitis. Although current treatment modalities are highly effective in the suppression of viral levels, they cannot eliminate the virus or achieve definitive cure. This is a consequence of the complex nature of HBV-host interactions. Major challenges to achieving sustained viral suppression include the presence of a high viral burden from the HBV DNA and hepatitis B surface antigen (HBsAg), the presence of reservoirs for HBV replication and antigen production, and the HBV-impaired innate and adaptive immune response of the host...
December 28, 2023: Journal of Clinical and Translational Hepatology
https://read.qxmd.com/read/38148074/liver-carcinogenesis-suppression-in-chronic-hepatitis-b-in-the-nucleoside-analogues-era
#32
REVIEW
Hiroki Nishikawa, Soo Ki Kim, Akira Asai
There is a strong association between the distribution of Hepatitis B virus (HBV) carriers and the incidence of hepatocellular carcinoma (HCC). About 60% of HCC in Japan is caused by viral hepatitis. Ten to 15 percent of hepatitis virus-related HCCs derive from HBV. Recently, antiviral therapy against HBV has developed, and interferon therapy and nucleos(t)ide analogues (NAs) are currently the standard of care. NAs exhibit antiviral activity by inhibiting DNA polymerase and suppressing HBV replication. NAs are highly effective in suppressing HBV-DNA and improving alanine aminotransferase...
2024: In Vivo
https://read.qxmd.com/read/38140607/recent-advances-in-the-development-of-sulfamoyl-based-hepatitis-b-virus-nucleocapsid-assembly-modulators
#33
REVIEW
Sandesha Nayak, Jayaraj Gowda, Syed Azeem Abbas, Hyejin Kim, Soo Bong Han
Hepatitis B virus (HBV) is the primary contributor to severe liver ailments, encompassing conditions such as cirrhosis and hepatocellular carcinoma. Globally, 257 million people are affected by HBV annually and 887,000 deaths are attributed to it, representing a substantial health burden. Regrettably, none of the existing therapies for chronic hepatitis B (CHB) have achieved satisfactory clinical cure rates. This issue stems from the existence of covalently closed circular DNA (cccDNA), which is difficult to eliminate from the nucleus of infected hepatocytes...
November 30, 2023: Viruses
https://read.qxmd.com/read/38140556/current-status-and-challenges-in-anti-hepatitis-b-virus-agents-based-on-inactivation-inhibition-or-elimination-of-hepatitis-b-virus-covalently-closed-circular-dna
#34
REVIEW
An-Qi Zhuang, Yan Chen, Shan-Mei Chen, Wen-Cheng Liu, Yao Li, Wen-Jie Zhang, Yi-Hang Wu
There has been over half a century since the discovery of hepatitis B virus (HBV) to now, but approximately 300 million patients with chronic hepatitis B (CHB) still live in the world, resulting in about one million deaths every year. Although currently approved antivirals (e.g., nucleoside analogues) are effective at reducing HBV replication, they have almost no impact on the existing HBV covalently closed circular DNA (cccDNA) reservoir. HBV cccDNA is a critical obstacle to the complete elimination of the virus via antiviral therapy...
November 25, 2023: Viruses
https://read.qxmd.com/read/38137971/immunoinformatics-and-evaluation-of-peptide-vaccines-derived-from-global-hepatitis-b-viral-hbx-and-hbc-proteins-critical-for-covalently-closed-circular-dna-integrity
#35
JOURNAL ARTICLE
Umar Saeed, Zahra Zahid Piracha, Salman Alrokayan, Tajamul Hussain, Fahad N Almajhdi, Yasir Waheed
The Hepatitis B virus (HBV) HBx and HBc proteins play a crucial role in associating with covalently closed circular DNA (cccDNA), the primary factor contributing to intrahepatic viral persistence and a major obstacle in achieving a cure for HBV. The cccDNA serves as a reservoir for viral persistence. Targeting the viral HBc and HBx proteins' interaction with cccDNA could potentially limit HBV replication. In this study, we present epitopes identified from global consensus sequences of HBx and HBc proteins that have the potential to serve as targets for the development of effective vaccine candidates...
November 21, 2023: Microorganisms
https://read.qxmd.com/read/38135680/a-small-molecule-icdm-34-identified-by-in-silico-screening-suppresses-hbv-dna-through-activation-of-aryl-hydrocarbon-receptor
#36
JOURNAL ARTICLE
Yutaka Furutani, Yoshinori Hirano, Mariko Toguchi, Shoko Higuchi, Xian-Yang Qin, Kaori Yanaka, Yumi Sato-Shiozaki, Nobuaki Takahashi, Marina Sakai, Pornparn Kongpracha, Takehiro Suzuki, Naoshi Dohmae, Mutsuko Kukimoto-Niino, Mikako Shirouzu, Shushi Nagamori, Harukazu Suzuki, Kaoru Kobayashi, Takahiro Masaki, Hiroo Koyama, Kazuma Sekiba, Motoyuki Otsuka, Kazuhiko Koike, Michinori Kohara, Soichi Kojima, Hideaki Kakeya, Tomokazu Matsuura
IFN-alpha have been reported to suppress hepatitis B virus (HBV) cccDNA via APOBEC3 cytidine deaminase activity through interferon signaling. To develop a novel anti-HBV drug for a functional cure, we performed in silico screening of the binding compounds fitting the steric structure of the IFN-alpha-binding pocket in IFNAR2. We identified 37 compounds and named them in silico cccDNA modulator (iCDM)-1-37. We found that iCDM-34, a new small molecule with a pyrazole moiety, showed anti-HCV and anti-HBV activities...
December 22, 2023: Cell Death Discovery
https://read.qxmd.com/read/38123992/clinical-applications-of-circulating-hbv-rna-as-a-potential-surrogate-biomarker-for-intrahepatic-cccdna-transcriptional-activity
#37
JOURNAL ARTICLE
Xiaoqi Yu, Maria Pfefferkorn, Florian van Bömmel, Xinxin Zhang, Thomas Berg
No abstract text is available yet for this article.
December 11, 2023: Gut
https://read.qxmd.com/read/38113270/g-quadruplexes-control-hepatitis-b-virus-replication-by-promoting-cccdna-transcription-and-phase-separation-in-hepatocytes
#38
JOURNAL ARTICLE
Guillaume Giraud, Mélanie Rodà, Pélagie Huchon, Maud Michelet, Sarah Maadadi, Daniel Jutzi, Roland Montserret, Marc-David Ruepp, Romain Parent, Christophe Combet, Fabien Zoulim, Barbara Testoni
Phase separation regulates fundamental processes in gene expression and is mediated by the local concentration of proteins and nucleic acids, as well as nucleic acid secondary structures such as G-quadruplexes (G4s). These structures play fundamental roles in both host gene expression and in viral replication due to their peculiar localisation in regulatory sequences. Hepatitis B virus (HBV) covalently closed circular DNA (cccDNA) is an episomal minichromosome whose persistence is at the basis of chronic infection...
December 19, 2023: Nucleic Acids Research
https://read.qxmd.com/read/38110058/mechanism-of-interferon-alpha-therapy-for-chronic-hepatitis-b-and-potential-approaches-to-improve-its-therapeutic-efficacy
#39
REVIEW
Qiong Zhao, Hui Liu, Liudi Tang, Fuxuan Wang, Gideon Tolufashe, Jinhong Chang, Ju-Tao Guo
Hepatitis B virus (HBV) chronically infects 296 million people worldwide and causes more than 820,000 deaths annually due to cirrhosis and hepatocellular carcinoma. Current standard-of-care medications for chronic hepatitis B (CHB) include nucleos(t)ide analogue (NA) viral DNA polymerase inhibitors and pegylated interferon alpha (PEG-IFN-α). NAs can efficiently suppress viral replication and improve liver pathology, but not eliminate or inactivate HBV covalently closed circular DNA (cccDNA). CCC DNA is the most stable HBV replication intermediate that exists as a minichromosome in the nucleus of infected hepatocyte to transcribe viral RNA and support viral protein translation and genome replication...
December 16, 2023: Antiviral Research
https://read.qxmd.com/read/38110037/classifying-hepatitis-b-therapies-with-insights-from-covalently-closed-circular-dna-dynamics
#40
REVIEW
Jie-Li Hu, Ai-Long Huang
The achievement of a functional cure for chronic hepatitis B (CHB) remains limited to a minority of patients treated with currently approved drugs. The primary objective in developing new anti-HBV drugs is to enhance the functional cure rates for CHB. A critical prerequisite for the functional cure of CHB is a substantial reduction, or even eradication of covalently closed circular DNA (cccDNA). Within this context, the changes in cccDNA levels during treatment become as a pivotal concern. We have previously analyzed the factors influencing cccDNA dynamics and introduced a preliminary classification of hepatitis B treatment strategies based on these dynamics...
December 16, 2023: Virologica Sinica
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