Transcription of Hepatitis B Virus Covalently Closed Circular DNA Is Regulated by CpG Methylation during Chronic Infection

Zhang, Yongmei; Mao, Richeng; Yan, Ran; Cai, Dawei; Zhang, Yijun; Zhu, Haoxiang; Kang, Yu; Liu, Hongyan; Wang, Jinyu; Qin, Yanli; Huang, Yuxian; Guo, Haitao; Zhang, Jiming

doi:10.1371/journal.pone.0110442

Cited by 75 publications

(90 citation statements)

References 44 publications

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“…The presence of Cp on CpG island 2 correlates with increased activity of cccDNA (i.e. viral load), while methylation of DNA in CpG islands 2 and 3 correlates with decreased cccDNA activity (Guo et al, 2011; Zhang et al, 2014). Of note, small molecules that drive Cp assembly (Bourne et al, 2008), presumably depleting the concentration of free Cp, led to depletion of cccDNA-bound Cp and decreased production of viral RNA and proteins (Belloni et al, 2013).…”

Section: Cp and Cccdnamentioning

confidence: 99%

Core protein: A pleiotropic keystone in the HBV lifecycle

et al. 2015

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Hepatitis B Virus (HBV) is a small virus whose genome has only four open reading frames. We argue that the simplicity of the virion correlates with a complexity of functions for viral proteins. We focus on the HBV core protein (Cp), a small (183 residue) protein that self-assembles to form the viral capsid. However, its functions are a little more complicated than that. In an infected cell Cp modulates every step of the viral lifecycle. Cp is bound to nuclear viral DNA and affects its epigenetics. Cp correlates with RNA specificity. Cp assembles specifically on a reverse transcriptase-viral RNA complex or, apparently, nothing at all. Indeed Cp has been one of the model systems for investigation of virus self-assembly. Cp participates in regulation of reverse transcription. Cp signals completion of reverse transcription to support virus secretion. Cp carries both nuclear localization signals and HBV surface antigen (HBsAg) binding sites; both of these functions appear to be regulated by contents of the capsid. Cp can be targeted by antivirals -- while self-assembly is the most accessible of Cp activities, we argue that it makes sense to engage the broader spectrum of Cp function. This article forms part of a symposium in Antiviral Research on “From the discovery of the Australia antigen to the development of new curative therapies for hepatitis B: an unfinished story.”

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Section: Cp and Cccdnamentioning

confidence: 99%

Core protein: A pleiotropic keystone in the HBV lifecycle

et al. 2015

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“…The CpG islands were defined based on the following criteria: a GC content of Ն50%, an observed-to-expected CpG dinucleotide ratio of Ն0.60, and a sequence window longer than 100 bp. Bisulfite sequencing primers were designed separately for both CpG islands II (nt 1228 to 1663) and III (nt 2295 to 2446) to avoid overlap between CpG sites (Table 1) (32). DNA samples were modified using the Cells-to-CpG bisulfite conversion kit (Applied Biosystems) according to the manufacturer's specifications.…”

Section: Methodsmentioning

confidence: 99%

“…Island I contains the start site of the S gene, island II spans a region that overlaps enhancer I/II and is proximal to the core promoter, and island III covers the start codon of the polymerase gene and the upstream region of the SP1 promoter (32,33). It was reported that transcription of HBV cccDNA is regulated by CpG methylation during chronic infection (27,33).…”

Section: Persistent Loss Of Serum Hbv Markers In Micementioning

confidence: 99%

Persistent Loss of Hepatitis B Virus Markers in Serum without Cellular Immunity by Combination of Peginterferon and Entecavir Therapy in Humanized Mice

Uchida

Imamura

Hayes

et al. 2017

Antimicrob Agents Chemother

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Nucleot(s)ide analogues and peginterferon (PEG-IFN) treatment are the only approved therapies for chronic hepatitis B virus (HBV) infection. However, complete eradication of the virus, as indicated by persistent loss of hepatitis B surface antigen (HBsAg), is rare among treated patients. This is due to long-term persistence of the HBV genome in infected hepatocytes in the form of covalently closed circular DNA (cccDNA). In this study, we investigated whether administration of a large dose of a nucleoside analogue in combination with PEG-IFN can achieve long-term loss of HBsAg in human hepatocyte chimeric mice. Mice were treated with a high dose of entecavir and/or PEG-IFN for 6 weeks. High-dose combination therapy with both drugs resulted in persistently negative HBV DNA in serum. Although small amounts of HBV DNA and cccDNA (0.1 and 0.01 copy/cell, respectively) remained in the mouse livers, some of the mice remained persistently negative for serum HBV DNA at 13 weeks after cessation of the therapy. Serum HBsAg and hepatitis B corerelated antigen (HBcrAg) continued to decrease and eventually became negative at 12 weeks after cessation of the therapy. Analysis of the HBV genome in treated mice showed accumulation of G-to-A hypermutation and CpG III island methylation. Persistent loss of serum HBV DNA and loss of HBV markers by high-dose entecavir and PEG-IFN combination treatment in chimeric mice suggests that control of HBV can be achieved even in the absence of a cellular immune response.

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“…In the HBV-infected liver, free HBV DNA and its products are causally related to the activity of liver disease, but the persistence of HBV infection is maintained by the nuclear cccDNA, which serves as a transcription template for HBV mRNA [111,112] . Although there are several opposing views [113] , it was reported that HBV cccDNA is noncytolytically degraded by agents that upregulate apolipoprotein B mRNA editing enzyme and catalytic polypeptide-like (APOBEC) 3A and 3B [23] .…”

Section: Treatment For Hbv Cccdnamentioning

confidence: 99%

Current and future directions for treating hepatitis B virus infection

Tawada

Yokosuka

2015

WJH

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Hepatitis B virus (HBV) persistently infects approximately 350 million people, and approximately 600000 liverrelated deaths are observed per year worldwide. HBV infection is also one of the major risk factors for hepatocellular carcinoma (HCC). The persistence of serum hepatitis B e antigen (HBeAg) and high level of serum HBV DNA are thought to reflect a high HBV replication status in hepatocytes, causing cirrhosis, HCC and liver-related deaths. It has been reported that antiviral therapy, such as peginterferon and nucleos(t)ide analogues (NUCs), could suppress liver-related death by inhibiting the HBV DNA levels and inducing seroconversion from HBeAg to antibody to HBe antigen. Currently, peginterferon is widely used, but there are also several disadvantages in the use of peginterferon, such as various adverse events, the administration route and duration. It is difficult to predict the effects of treatment and interferon is contraindicated for the patients with advanced fibrosis of the liver and cirrhosis. With respect to NUCs, entecavir and tenofovir disoproxil fumarate are current the first-choice drugs. NUCs can be administered orally, and their anti-viral effects are stronger than that of peginterferon. However, because cessation of NUC administration leads to high levels of viral replication and causes severe hepatitis, they must be administered for a long time. On the other hand, the use of both interferon and NUCs cannot eliminate covalently closed circular DNA of HBV. In this review, we evaluate the natural course of chronic HBV infection and then provide an outline of these representative drugs, such as peginterferon, entecavir and tenofovir disoproxil fumarate.

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Transcription of Hepatitis B Virus Covalently Closed Circular DNA Is Regulated by CpG Methylation during Chronic Infection

Cited by 75 publications

References 44 publications

Core protein: A pleiotropic keystone in the HBV lifecycle

Core protein: A pleiotropic keystone in the HBV lifecycle

Persistent Loss of Hepatitis B Virus Markers in Serum without Cellular Immunity by Combination of Peginterferon and Entecavir Therapy in Humanized Mice

Current and future directions for treating hepatitis B virus infection

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