Extracellular HBV RNAs are heterogeneous in length and circulate as virions and capsid-antibody-complexes in chronic hepatitis B patients

Bai, Lu; Zhang, Xiaonan; Li, Weixia; Wu, Min; Liu, Jiangxia; Kozlowski, Maya; Chen, Liang; Zhang, Jiming; Huang, Yuxian; Yuan, Zhenghong

doi:10.1101/320994

Cited by 3 publications

(5 citation statements)

References 74 publications

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“…HBV belongs to the Hepadnavividae family and contains different forms of genome in virions. The Dane particles contain a partial double‐strand relaxed circular (rc) DNA of ~3.2 kilobases in length, while a small fraction of virions contain pregenomic (pg) RNA or the reverse‐transcription intermediates, that is, a 3′ truncated pgRNA and a short minus‐strand DNA …”

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confidence: 99%

“…pregenomic (pg) RNA or the reverse-transcription intermediates, that is, a 3′ truncated pgRNA and a short minus-strand DNA. (5,6) During HBV infection, the virion enters hepatocyte by binding to its specific receptor, sodium taurocholate cotransporting polypeptide (NTCP). (7) Then, the rcDNA was converted to covalently closed circular DNA (cccDNA) in the nuclei of hepatocyte to serve as the template for transcription of viral RNAs, including pgRNA, which can be used as either mRNA for viral core protein and polymerase protein (P protein) or the template of reverse-transcriptional replication of viral DNA.…”

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confidence: 99%

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Hepatitis B Virus Virions Produced Under Nucleos(t)ide Analogue Treatment Are Mainly Not Infectious Because of Irreversible DNA Chain Termination

Liu

et al. 2019

Hepatology

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Nucleos(t)ide analogues (NAs) have been widely used for the treatment of chronic hepatitis B (CHB). Because viral DNA polymerase lacks proofreading function (3′ exonuclease activity), theoretically, the incorporated NAs would irreversibly terminate viral DNA synthesis. This study explored the natures of nascent hepatitis B virus (HBV) DNA and infectivity of progeny virions produced under NA treatment. HBV infectivity was determined by infection of HepG2‐NTCP cells and primary human hepatocytes (PHHs). Biochemical properties of HBV DNA in the progeny virions were investigated by qPCR, northern blotting, or Southern blotting hybridization, sucrose gradient centrifugation, and in vitro endogenous DNA polymerase assay. Progeny HBV virions produced under NA treatment were mainly not infectious to HepG2‐NTCP cells or PHHs. Biochemical analysis revealed that under NA treatment, HBV DNA in nucleaocapsids or virions were predominantly short minus‐strand DNA with irreversible termination. This finding was supported by the observation of first disappearance of relaxed circular DNA and then the proportional decline of HBV‐DNA levels corresponding to the regions of PreC/C, S, and X genes in serial sera of patients receiving NA treatment. Conclusion: HBV virions produced under NA treatment are predominantly replication deficient because the viral genomes are truncated and elongation of DNA chains is irreversibly terminated. Clinically, our results suggest that the viral loads of CHB patients under NA therapy vary with the different regions of genome being detected by qPCR assays. Our findings also imply that NA prevention of perinatal and sexual HBV transmission as well as infection of transplanted livers works not only by reducing viral loads, but also by producing noninfectious virions.

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confidence: 99%

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Hepatitis B Virus Virions Produced Under Nucleos(t)ide Analogue Treatment Are Mainly Not Infectious Because of Irreversible DNA Chain Termination

Liu

et al. 2019

Hepatology

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“…47 The mature nucleocapsids containing rcDNA are then transferred to post-endoplasmic reticulum (ER) or pre-Golgi membranes, enveloped into virions and released from hepatocytes, 48 or recycled to the nucleus to amplify the cccDNA pool 49 (Figure 1A). The immature capsids, such as empty capsids 50,51 and capsids with incomplete HBV RNA/DNA fragments, 52 could be either released as naked capsids in the form of capsid-antibody complexes (CAC) 53 from hepatocytes or enveloped to form virus-like particles (Figure 1B). Recently, HBV virion production was found to be associated with autophagy.…”

Section: ■ Hbv Life Cyclementioning

confidence: 99%

Treatment of Chronic Hepatitis B Virus Infection Using Small Molecule Modulators of Nucleocapsid Assembly: Recent Advances and Perspectives

Liu

Tong

et al. 2019

ACS Infect. Dis.

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On the basis of the recent advance of basic research on molecular biology of hepatitis B virus (HBV) infection, novel antiviral drugs targeting various steps of the HBV life cycle have been developed in recent years. HBV nucleocapsid assembly is now recognized as a hot target for anti-HBV drug development. Structural and functional analysis of HBV nucleocapsid allowed rational design and improvement of small molecules with the ability to interact with the components of HBV nucleocapsid and modulate the viral nucleocapsid assembly process. Prototypes of small molecule modulators targeting HBV nucleocapsid assembly are being preclinically tested or have moved forward in clinical trials, with promising results. This Review summarizes the recent advances in the approach to develop antiviral drugs based on the modulation of HBV nucleocapsid assembly. The antiviral mechanisms of small molecule modulators beyond the capsid formation and the potential implications will be discussed.

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“…Accordingly, capsids/NCs must exist in vivo , but may be quickly removed from extracellular fluids. Indeed, naked capsids/NCs carrying HBV-specific DNA and RNA species were recently detected in the blood of HBV patients as capsid-antibody-complexes ( Bai et al, 2018 ). Since naked capsids/NCs are able to bind to cell surface-exposed HSPGs and competent for clathrin-mediated endocytosis, their uptake may enhance transmission of HBV genomes ( Cooper and Shaul, 2006 ).…”

Section: Role Of Rabs In Hbv Naked Capsid Releasementioning

confidence: 99%

“…SVPs greatly outnumber mature virions and presumably act as decoys to the immune system, as they are able to adsorb antibodies that might otherwise target viral particles ( Patient et al, 2009 ; Prange, 2012 ; Blondot et al, 2016 ). Naked capsids/NCs can carry HBV-specific DNA and RNA species and may be instrumental in spreading infection ( Bai et al, 2018 ). HBV exploits different intracellular trafficking routes and diverse host factors in order to release its particle types ( Patient et al, 2009 ; Prange, 2012 ).…”

Section: Introductionmentioning

confidence: 99%

Host Cell Rab GTPases in Hepatitis B Virus Infection

Zeyen

Prange

2018

Front. Cell Dev. Biol.

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Hepatitis B virus (HBV) is a leading cause of liver disease and is presently estimated to infect more than 250 million humans. The extremely successful spread of this virus among the human population is explained by its effective transmission strategies and its manifold particle types, including virions, empty envelopes and naked capsids. Due to its tiny genome, HBV depends on cellular machineries to thrive in infected hepatocytes. To enter, traverse and exit the cell, HBV exploits host membrane trafficking pathways, including intracellular highways directed by Rab GTPases. Here, we review recent discoveries focused on how HBV co-opts and perturbs host Rab GTPase functions with an emphasis on Rab7A- and Rab33B-mediated trafficking pathways. Rab7A plays bidirectional roles in the viral life cycle, as it promotes the endocytic uptake of HBV in early stages, but restricts exocytic virion release in late stages. In intermediate stages of HBV propagation, Rab33B is needed to guide the assembly of replicative progeny nucleocapsids. Rab33B acts together with its Atg5-12/16L1 effector, a protein complex required for autophagosome formation, suggesting the concept that HBV exploits this Rab/effector complex as an assembly scaffold and machine. We also discuss whether Rab-directed trafficking pathways engaged by HBV may be applicable to other virus families. Identification of overlapping Rab functions may offer new chances to develop broad-spectrum host-targeted antiviral strategies.

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Extracellular HBV RNAs are heterogeneous in length and circulate as virions and capsid-antibody-complexes in chronic hepatitis B patients

Cited by 3 publications

References 74 publications

Hepatitis B Virus Virions Produced Under Nucleos(t)ide Analogue Treatment Are Mainly Not Infectious Because of Irreversible DNA Chain Termination

Hepatitis B Virus Virions Produced Under Nucleos(t)ide Analogue Treatment Are Mainly Not Infectious Because of Irreversible DNA Chain Termination

Treatment of Chronic Hepatitis B Virus Infection Using Small Molecule Modulators of Nucleocapsid Assembly: Recent Advances and Perspectives

Host Cell Rab GTPases in Hepatitis B Virus Infection

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