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

Hervouet, Kévin; Ferrié, Martin; Ankavay, Maliki; Montpellier, Claire; Camuzet, Charline; Alexandre, Virginie; Dembélé, Aïcha; Lecœur, Cécile; Foe, Arnold Thomas; Bouquet, Peggy; Hot, David; Vausselin, Thibaut; Saliou, Jean‐Michel; Salomé‐Desnoulez, Sophie; Vandeputte, Alexandre; Marsollier, Laurent; Brodin, Priscille; Dreux, Marlène; Rouillé, Yves; Dubuisson, Jean; Aliouat-Denis, Cécile-Marie; Cocquerel, Laurence

doi:10.1101/2021.05.26.445820

Cited by 3 publications

(21 citation statements)

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“…Indeed, by combining the gt3 p6 strain [15] and the highly transfectable PLC3 cells, we identified 3 forms of the ORF2 capsid protein that perform distinct functions in the HEV lifecycle and display different sequences, post-translational modifications and subcellular localization [6,14]. The ORF2i form is the component of infectious particles and derives from the assembly of intracellular ORF2i (ORF2intra) protein [8]. The ORF2i and ORF2intra proteins are not glycosylated and display the same sequence starting at Leu14 corresponding to the middle of the signal peptide (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…These glycosylated forms are produced by translocation of ORF2 proteins into the secretory pathway where they are N-glycosylated on two N-x-S/T sequons [14], O-glycosylated and sialylated, and quickly secreted [6,7]. They are cleaved by cellular proteases notably by the proprotein convertase furin [8]. Here, we capitalized on these distinctive features to generate and characterize four anti-ORF2 monoclonal antibodies, including three antibodies (P1H1, P2H1 and P2H2) directed against the ORF2i form and one antibody (P3H2) directed against the different ORF2 isoforms (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…4C) and are deleterious for viral particle assembly [8]. Of note, HEV RNA replication is not altered in PLC3/HEV-∆ORF3 and PLC3/HEV-5R/5A cells [8].…”

Section: Identification Of Hev-induced Subcellular Structuresmentioning

confidence: 99%

“…The plasmid pBlueScript SK(+) carrying the DNA of the full length genome of adapted gt3 Kernow C-1 p6 strain, (GenBank accession number JQ679013, kindly provided by S.U Emerson) was used [15]. The ORF3-null mutant (HEV-p6-∆ORF3) and the 5R/5A mutant (HEV-p6-5R/5A) of HEV-p6 were generated as described in [16] and [8], respectively. Capped genomic HEV RNAs were prepared with the mMESSAGE mMACHINE kit (Ambion) and delivered to PLC3 or Huh-7.5 cells by electroporation using a Gene Pulser Xcell TM apparatus (Bio-Rad) [6].…”

Section: Plasmids and Transfectionmentioning

confidence: 99%

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The Endocytic Recycling Compartment Serves as a Viral Factory for Hepatitis E Virus

Bentaleb

Hervouet

Montpellier

et al. 2021

Preprint

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Background & Aims: Although Hepatitis E virus (HEV) is the major leading cause of enterically transmitted viral hepatitis worldwide, many gaps remain in the understanding of the HEV lifecycle. Notably, viral factories induced by HEV have not been documented yet and it is currently unknown whether HEV infection leads to cellular membrane modelling as many positive-strand RNA viruses. HEV genome encodes three proteins, the ORF1 replicase, the ORF2 capsid protein and the ORF3 protein involved in virion egress. Previously, we demonstrated that HEV produces different ORF2 isoforms including the virion-associated ORF2i form. Here, we aimed to probe infectious particles and viral factories in HEV-producing cells, using antibodies directed against the different ORF2 isoforms. Methods: We generated monoclonal antibodies that specifically recognize the particle-associated ORF2i form, and antibodies that recognize the different ORF2 isoforms. We used them in confocal and electron microscopy approaches to probe viral factories in HEV-producing cells. We performed an extensive colocalization study of viral proteins with subcellular markers. We analyzed the impact of silencing Rab11, a central player of the endocytic recycling compartment (ERC). Results: One of the antibodies, named P1H1 and targeting the N-terminus of ORF2i, recognized delipidated HEV particles. Confocal and ultrastructural microscopy analyses of HEV-producing cells revealed an unprecedented HEV-induced membrane network containing tubular and vesicular structures. These subcellular structures were enriched in ORF2 and ORF3 proteins, and were dependent on the ORF3 expression and ORF2i capsid protein assembly. Colocalization and silencing analyses revealed that these structures are derived from the ERC. Conclusions: Our study reveals that HEV hijacks the ERC and forms a membrane network of vesicular and tubular structures that might be the hallmark of HEV infection.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

“…4C) and are deleterious for viral particle assembly [8]. Of note, HEV RNA replication is not altered in PLC3/HEV-∆ORF3 and PLC3/HEV-5R/5A cells [8].…”

Section: Identification Of Hev-induced Subcellular Structuresmentioning

confidence: 99%

Section: Plasmids and Transfectionmentioning

confidence: 99%

See 2 more Smart Citations

The Endocytic Recycling Compartment Serves as a Viral Factory for Hepatitis E Virus

Bentaleb

Hervouet

Montpellier

et al. 2021

Preprint

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“…It appears that the HEV capsid interacts with β-TRCP to block the ubiquitin-proteasome-mediated degradation of IκB which subsequently inhibits NF-κB activation (Surjit et al, 2012). Moreover, a recent preprint report suggested that the argininerich motifs of the N-terminal of ORF2 could serve as a nuclear location signal to direct the nuclear translocation of ORF2 therefore inhibit the downregulation of NF-κB-related signaling as well (Hervouet et al, 2021).…”

Section: Regulation Of Innate Immune Response and Cellular Signaling By Hepatitis E Virus-open Reading Framementioning

confidence: 99%

The Hepatitis E Virus Open Reading Frame 2 Protein: Beyond Viral Capsid

Zhou

Yin-qian

et al. 2021

Front. Microbiol.

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Hepatitis E virus (HEV) is a zoonotic pathogen causing hepatitis in both human and animal hosts, which is responsible for acute hepatitis E outbreaks worldwide. The 7.2 kb genome of the HEV encodes three well-defined open reading frames (ORFs), where the ORF2 translation product acts as the major virion component to form the viral capsid. In recent years, besides forming the capsid, more functions have been revealed for the HEV-ORF2 protein, and it appears that HEV-ORF2 plays multiple functions in both viral replication and pathogenesis. In this review, we systematically summarize the recent research advances regarding the function of the HEV-ORF2 protein such as application in the development of a vaccine, regulation of the innate immune response and cellular signaling, involvement in host tropism and participation in HEV pathogenesis as a novel secretory factor. Progress in understanding more of the function of HEV-ORF2 protein beyond the capsid protein would contribute to improved control and treatment of HEV infection.

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A ribavirin-induced ORF2 single-nucleotide variant produces defective hepatitis E virus particles with immune decoy function

Meister

Brüggemann

Nocke

et al. 2022

Proc. Natl. Acad. Sci. U.S.A.

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Hepatitis E virus (HEV) is the causative agent of hepatitis E in humans and is the leading cause of enterically transmitted viral hepatitis worldwide. Ribavirin (RBV) is currently the only treatment option for many patients; however, cases of treatment failures or posttreatment relapses have been frequently reported. RBV therapy was shown to be associated with an increase in HEV genome heterogeneity and the emergence of distinct HEV variants. In this study, we analyzed the impact of eight patient-derived open reading frame 2 (ORF2) single-nucleotide variants (SNVs), which occurred under RBV treatment, on the replication cycle and pathogenesis of HEV. The parental HEV strain and seven ORF2 variants showed comparable levels of RNA replication in human hepatoma cells and primary human hepatocytes. However, a P79S ORF2 variant demonstrated reduced RNA copy numbers released in the supernatant and an impairment in the production of infectious particles. Biophysical and biochemical characterization revealed that this SNV caused defective, smaller HEV particles with a loss of infectiousness. Furthermore, the P79S variant displayed an altered subcellular distribution of the ORF2 protein and was able to interfere with antibody-mediated neutralization of HEV in a competition assay. In conclusion, an SNV in the HEV ORF2 could be identified that resulted in altered virus particles that were noninfectious in vitro and in vivo, but could potentially serve as immune decoys. These findings provide insights in understanding the biology of circulating HEV variants and may guide development of personalized antiviral strategies in the future.

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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

Cited by 3 publications

References 50 publications

The Endocytic Recycling Compartment Serves as a Viral Factory for Hepatitis E Virus

The Endocytic Recycling Compartment Serves as a Viral Factory for Hepatitis E Virus

The Hepatitis E Virus Open Reading Frame 2 Protein: Beyond Viral Capsid

A ribavirin-induced ORF2 single-nucleotide variant produces defective hepatitis E virus particles with immune decoy function

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