New insights into the ORF2 capsid protein, a key player of the hepatitis E virus lifecycle

Ankavay, Maliki; Montpellier, Claire; Sayed, Ibrahim M.; Saliou, Jean‐Michel; Wychowski, Czeslaw; Saas, Laure; Duvet, Sandrine; Aliouat-Denis, Cécile-Marie; Farhat, Rayan; d’Autume, Valentin de Masson; Meuleman, Philip; Dubuisson, Jean; Cocquerel, Laurence

doi:10.1101/435933

Cited by 4 publications

(11 citation statements)

References 32 publications

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“…We and others previously showed that the ORF2 protein is translocated into the nucleus of infected cells of patient liver biopsies 14 and in cell culture system 12 . Here, we first analyzed the ORF2 expression in PLC3 cells electroporated with the infectious p6 strain (PLC3/HEV-p6), at different time postelectroporation (p.e.)…”

Section: Resultsmentioning

confidence: 89%

“…It is not glycosylated and is likely derived from the assembly of the intracellular ORF2 (ORF2intra) form present in the cytosolic compartment. Importantly, we showed that a fraction of the ORF2intra form is translocated into the nucleus of infected cells 12 . In contrast, ORF2g and ORF2c proteins (herein referred to as ORF2g/c) are highly glycosylated and secreted in large amounts in culture supernatant (i.e., about 1000x more than ORF2i 13 ) and are the most abundant antigens detected in patient sera 11 .…”

Section: Introductionmentioning

confidence: 86%

“…How these different forms of ORF2 are generated during the HEV lifecycle has not yet been fully investigated. However, their sequence and post-translational modifications suggest that they might be produced 4 either by a distinct addressing into the secretory pathway and the nucleus 11,12 , and/or by a differential translation process 13 .…”

Section: Introductionmentioning

confidence: 99%

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An Arginine-Rich Motif in the ORF2 Capsid Protein Regulates the Hepatitis E Virus Lifecycle and Interactions with the Host Cell

Hervouet

Ferrié

Ankavay

et al. 2021

Preprint

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Producing multifunctional proteins is one of the major strategies developed by viruses to condense their genetic information. Here, we investigated the molecular determinants of the multifunctionality of hepatitis E virus (HEV) ORF2 capsid protein. We previously identified 3 isoforms of ORF2 which are partitioned in different subcellular compartments to perform distinct functions. Notably, the infectious ORF2 (ORF2i) protein is the structural component of the virion, whereas the genome-free secreted and glycosylated ORF2 proteins likely act as a humoral immune decoy. We identified a 5 amino acid Arginine-Rich Motif (ARM) located in the ORF2 N-terminal region as a central regulator of the subcellular localizations and functions of ORF2 isoforms. We showed that the ARM controls ORF2 nuclear translocation, promoting regulation of host antiviral responses. This motif also regulates the dual topology and functionality of ORF2 signal peptide, leading to the production of either cytosolic infectious ORF2i or reticular non-infectious glycosylated ORF2 forms. Furthermore, the ARM likely serves as a cleavage site of the glycosylated ORF2 protein. Finally, it promotes ORF2 membrane association that is likely essential for particle assembly. In conclusion, our observations highlight ORF2 ARM as a unique central regulator of ORF2 addressing that finely controls the HEV lifecycle.

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Section: Resultsmentioning

confidence: 89%

Section: Introductionmentioning

confidence: 86%

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An Arginine-Rich Motif in the ORF2 Capsid Protein Regulates the Hepatitis E Virus Lifecycle and Interactions with the Host Cell

Hervouet

Ferrié

Ankavay

et al. 2021

Preprint

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“…Comparing the virologic parameters in the stool and the plasma of the infected mice revealed high HEV RNA content in the stool compared with the plasma, while HEV ORF2Ag showed an inverse correlation. Stool-derived HEV particles were more infectious than plasma-derived HEV, when they were passaged into naïve mice 65,73 Humanized mice were used to characterize the infectivity of the fraction (fraction 6) of HEVcc that includes only ORF2i. Unlike the HEVcc supernatant, fraction 6 was infectious to the mice indicating that the removal of noninfectious ORF2 Ag increased the infectivity of the HEV preparation, probably due to absence of competitive binding between both infectious and noninfectious ORF2 Ag to the receptor.…”

Section: Use Of Humanized Mice For Characterization Of Hev Particlementioning

confidence: 99%

“…ORF2g along with a cleaved form of ORF2 Ag (ORF2c) were the major Ags detected in patient serum, indicating that the HEV Ag ELISA assay (HEV-Ag ELISA Plus assay (Bejing Wantai Biological Pharmaceutical) could detect both infectious and noninfectious ORF2 Ag. 65,73 Therefore, the ELISA Ag assay data should be interpreted cautiously, since this assay might not necessarily detect an active infection.…”

Section: Kinetics Of Hev Orf2 Ag During the Course Of Hev Infectionmentioning

confidence: 99%

Updates in Hepatitis E virus (HEV) field; lessons learned from human liver chimeric mice

Sayed

Meuleman

2019

Reviews in Medical Virology

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Summary Hepatitis E virus (HEV) is the most common cause of viral hepatitis globally, and it is an emerging pathogen in developed countries. In vivo studies of HEV have long been hindered due to the lack of an efficient small animal model. Recently, human liver chimeric mice were described as an elegant model to study chronic HEV infection. HEV infection was established in mice with humanized liver that were challenged with stool preparations containing HEV genotype (gt)1 and/or gt3. An increase in viral load and the level of HEV Ag in mouse samples were markers of active infection. Plasma‐derived HEV preparations were less infectious. The kinetics of HEV ORF2 Ag during HEV infection and its impact on HEV diagnosis were described in this model. In addition, the nature of HEV particles and HEV ORF2 Ag were characterized. Moreover, humanized mice were used to study the impact of HEV infection on the hepatic innate transcriptome and evaluation of anti‐HEV therapies. This review highlights recent advances in the HEV field gathered from well‐established experimental mouse models, with an emphasis on this model as a tool for elucidating the course of HEV infection, the study of the HEV life cycle, the interaction of the virus with the host, and the evaluation of new anti‐HEV therapies.

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Hepatitis E: Genotypes, strategies to prevent and manage, and the existing knowledge gaps

2021

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Hepatitis E virus (HEV) is considered an emergent source of viral hepatitis worldwide, with an increasing burden of jaundice, liver failure, extrahepatic illnesses, and deaths in developed countries. With the scarcity of data from efficient animal models, there are still open‐ended questions about designing new models to study pathogenesis, types, virology, and evolution of these viruses. With an emphasis on available data and updates, there is still enough information to understand the HEV life cycle, pathogen interaction with the host, and the valuation of the role of vaccine and new anti‐HEV therapies. However, the World Health Organization (WHO) and the European Association for the Study of the Liver (EASL) preferred to stress prevention and control measures of HEV infections in animals, zoonotic transmission, and foodborne transmission. It is being reviewed that with current knowledge on HEV and existing prevention tools, there is an excellent room for in‐depth information about the virus strains, their replication, pathogenicity, and virulence. The current knowledge set also has gaps regarding standardized and validated diagnostic tools, efficacy and safety of the vaccine, and extrahepatic manifestations specifically in pregnant females, immunocompromised patients, and others. This review highlights the areas for more research exploration, focusing on enlisted research questions based on HEV infection to endorse the need for significant improvement in the current set of knowledge for this public health problem.

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New insights into the ORF2 capsid protein, a key player of the hepatitis E virus lifecycle

Cited by 4 publications

References 32 publications

An Arginine-Rich Motif in the ORF2 Capsid Protein Regulates the Hepatitis E Virus Lifecycle and Interactions with the Host Cell

An Arginine-Rich Motif in the ORF2 Capsid Protein Regulates the Hepatitis E Virus Lifecycle and Interactions with the Host Cell

Updates in Hepatitis E virus (HEV) field; lessons learned from human liver chimeric mice

Hepatitis E: Genotypes, strategies to prevent and manage, and the existing knowledge gaps

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