Hepatitis B virus movement through the hepatocyte: An update

Prange, Reinhild

doi:10.1111/boc.202200060

Cited by 17 publications

(11 citation statements)

References 253 publications

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“…Finally, HBVwt/C4 mutant presented high levels of extracellular pgRNA, but no difference in extracellular capsid‐associated DNA, suggesting that HBVwt/C4 variants secret more premature pgRNA‐containing particles in which reverse transcription has not been completed. Notably, HBVwt/C4 variant carries mutations in the late assembly domain‐like PPAY motif (P130A and A131P) involved in the transport of mature nucleocapsids to multivesicular bodies via the ESCRT system for viral release 26,27 . It is likely that the mutations in this domain increase extracellular pgRNA levels through the secretion of immature particles via an ESCRT‐independent pathway in detriment of viral progeny production.…”

Section: Discussionmentioning

confidence: 99%

Impact of core protein naturally selected mutants associated with HBeAg‐negative status in HBV biosynthesis

Elizalde,

Giadans,

Campos

et al. 2023

Journal of Medical Virology

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Hepatitis B e antigen (HBeAg) loss represents a late stage of chronic hepatitis B virus (HBV) infection associated with a drastic decrease in HBV‐DNA, a lower risk of disease progression, and the occurrence of several mutations in the preCore/core region. However, the underlying mechanisms supporting the downregulation of viral replication have yet to be elucidated. In the present study, the analysis of the frequency of subgenotype D1 core protein (HBc) mutations associated with HBeAg status revealed a higher mutation rate in HBeAg‐negative sequences compared to HBeAg‐positive ones. Particularly, 22 amino acids exhibited a higher frequency of mutation in HBeAg‐negative sequences, while the remaining residues showed a high degree of conservation. Subsequently, the assessment of HBc mutants derived from HBeAg‐negative patients in viral structure and replicative capacity revealed that HBc mutations have the ability to modulate the subcellular localization of the protein (either when the protein was expressed alone or in the context of viral replication), capsid assembly, and, depending on specific mutation patterns, alter covalently closed circular DNA (cccDNA) recycling and up‐ or downregulate viral replication. In conclusion, HBc mutations associated with HBeAg‐negative status impact on various stages of the HBV life cycle modulating viral replication during the HBeAg‐negative stage of infection.

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Section: Discussionmentioning

confidence: 99%

Impact of core protein naturally selected mutants associated with HBeAg‐negative status in HBV biosynthesis

Elizalde,

Giadans,

Campos

et al. 2023

Journal of Medical Virology

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“…Previous research shows that HBV-related antigens, namely HBcAg and HBsAg, can increase CD4+ T cell production of inhibitory molecules. Chuang et al [ 67 ] found that HBcAg enhanced PD-1 expression on CD4+ T cells, disrupting their function via JNK, ERK, and PI3K/AKT signaling pathways[ 79 ]. Moreover, the expression of human protein inhibitors of activated STAT1 (dependent on ERK and p38 MAPK signaling pathways) increased in CHB patients, making standard therapies ineffectual.…”

Section: Possible Immunological Mechanisms Of Hbv Reactivationmentioning

confidence: 99%

Overview of the immunological mechanisms in hepatitis B virus reactivation: Implications for disease progression and management strategies

Ma,

Yan,

et al. 2024

World J Gastroenterol

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Hepatitis B virus (HBV) reactivation is a clinically significant challenge in disease management. This review explores the immunological mechanisms underlying HBV reactivation, emphasizing disease progression and management. It delves into host immune responses and reactivation’s delicate balance, spanning innate and adaptive immunity. Viral factors’ disruption of this balance, as are interactions between viral antigens, immune cells, cytokine networks, and immune checkpoint pathways, are examined. Notably, the roles of T cells, natural killer cells, and antigen-presenting cells are discussed, highlighting their influence on disease progression. HBV reactivation’s impact on disease severity, hepatic flares, liver fibrosis progression, and hepatocellular carcinoma is detailed. Management strategies, including anti-viral and immunomodulatory approaches, are critically analyzed. The role of prophylactic anti-viral therapy during immunosuppressive treatments is explored alongside novel immunotherapeutic interventions to restore immune control and prevent reactivation. In conclusion, this comprehensive review furnishes a holistic view of the immunological mechanisms that propel HBV reactivation. With a dedicated focus on understanding its implications for disease progression and the prospects of efficient management strategies, this article contributes significantly to the knowledge base. The more profound insights into the intricate interactions between viral elements and the immune system will inform evidence-based approaches, ultimately enhancing disease management and elevating patient outcomes. The dynamic landscape of management strategies is critically scrutinized, spanning anti-viral and immunomodulatory approaches. The role of prophylactic anti-viral therapy in preventing reactivation during immunosuppressive treatments and the potential of innovative immunotherapeutic interventions to restore immune control and proactively deter reactivation.

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“…The study conducted by Volker Bruss's group demonstrated that the pre-S sequence between Arg 103 and Ser 124 promotes HBV virion assembly ( Bruss, 1997 ). HBcAg forms the icosahedral virus capsid and consists of 183 residues, which can be divided into an assembly domain and a domain responsible for viral genome packaging and replication (arginine-rich RNA-binding C Terminal Domain, CTD) ( Liu et al., 2018 ; Prange, 2022 ; Venkatakrishnan and Zlotnick, 2016 ; Walker et al., 2011 ). Apart from the virologic factors, HBV assembly is also greatly influenced by cellular vesicle trafficking pathways, such as endosomal vesicle trafficking and autophagy, which will be elaborated in the subsequent discussion.…”

Section: Hbv Assembly and Secretionmentioning

confidence: 99%

Interconnection of cellular autophagy and endosomal vesicle trafficking and its role in hepatitis B virus replication and release

Li,

Lin,

Wang

et al. 2024

Virologica Sinica

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Hepatitis B virus movement through the hepatocyte: An update

Cited by 17 publications

References 253 publications

Impact of core protein naturally selected mutants associated with HBeAg‐negative status in HBV biosynthesis

Impact of core protein naturally selected mutants associated with HBeAg‐negative status in HBV biosynthesis

Overview of the immunological mechanisms in hepatitis B virus reactivation: Implications for disease progression and management strategies

Interconnection of cellular autophagy and endosomal vesicle trafficking and its role in hepatitis B virus replication and release

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