Gammaherpesvirus entry and fusion: A tale how two human pathogenic viruses enter their host cells

Möhl, Britta S.; Chen, Jia; Longnecker, Richard

doi:10.1016/bs.aivir.2019.05.006

Cited by 33 publications

(32 citation statements)

References 134 publications

(252 reference statements)

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“…In the absence of atomic resolution structures for gB, models were generated in silico using the SWISS-MODEL program [127] and provide some fascinating potential insight into functions of the molecule until a KSHV structure can verify them. The post-fusion structure of EBV gB was used to model KSHV gB [23,128,129]. The model predicts that, like other herpesvirus gB homologs, KSHV gB is comprised of five distinct functional domains and is homologous to type III fusion glycoproteins.…”

Section: Kshv Entry Glycoproteinsmentioning

confidence: 99%

“…A gHgL structural model was also created based on the EBV structures and the model predicts several virus-specific adaptations [23,60,136,137]. gH is predicted to have four domains and binds noncovalently to the smaller gL which is comprised of a single domain.…”

Section: Kshv Entry Glycoproteinsmentioning

confidence: 99%

“…A host-derived lipid bilayer termed the viral envelope is the last layer that surrounds the whole particle [22]. Viral envelope glycoproteins transverse the viral envelope and are responsible for the initial virus–host interactions [23,24]. Viral envelope glycoproteins K8.1A, glycoprotein-B (gB), and the heterodimer of glycoprotein- H and glycoprotein-L (gHgL) are widely regarded as the most important for virus entry and are the best understood of the KSHV glycoproteins.…”

Section: Introductionmentioning

confidence: 99%

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Towards Understanding KSHV Fusion and Entry

Dollery

2019

Viruses

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How viruses enter cells is of critical importance to pathogenesis in the host and for treatment strategies. Over the last several years, the herpesvirus field has made numerous and thoroughly fascinating discoveries about the entry of alpha-, beta-, and gamma-herpesviruses, giving rise to knowledge of entry at the amino acid level and the realization that, in some cases, researchers had overlooked whole sets of molecules essential for entry into critical cell types. Herpesviruses come equipped with multiple envelope glycoproteins which have several roles in many aspects of infection. For herpesvirus entry, it is usual that a collective of glycoproteins is involved in attachment to the cell surface, specific interactions then take place between viral glycoproteins and host cell receptors, and then molecular interactions and triggers occur, ultimately leading to viral envelope fusion with the host cell membrane. The fact that there are multiple cell and virus molecules involved with the build-up to fusion enhances the diversity and specificity of target cell types, the cellular entry pathways the virus commandeers, and the final triggers of fusion. This review will examine discoveries relating to how Kaposi’s sarcoma-associated herpesvirus (KSHV) encounters and binds to critical cell types, how cells internalize the virus, and how the fusion may occur between the viral membrane and the host cell membrane. Particular focus is given to viral glycoproteins and what is known about their mechanisms of action.

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Section: Kshv Entry Glycoproteinsmentioning

confidence: 99%

Section: Kshv Entry Glycoproteinsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Towards Understanding KSHV Fusion and Entry

Dollery

2019

Viruses

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“…Epstein-Barr virus (EBV, Lymphocryptovirus) and Kaposi sarcoma-associated herpesvirus (KSHV, Rhadinovirus) are the only two human-infecting γ-herpesviruses. EBV and KSHV have many commonalities, such as an association with malignancies, broad cell tropism, and a similar entry process into host cells [2][3][4] . EBV primarily infects B cells and epithelial cells 5 , whereas KSHV predominantly infects B cells and endothelial cells.…”

mentioning

confidence: 99%

“…The process by which herpesviruses enter cells is divided into three steps: attachment, receptor binding, and fusion. These steps are mediated by different viral glycoproteins 2,6 . Cell tropism is mainly determined by the interaction between a specific host receptor and the gHgL complex, with or without other glycoproteins 7 .…”

mentioning

confidence: 99%

Molecular basis of EphA2 recognition by gHgL from gammaherpesviruses

Chai

et al. 2020

Nat Commun

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The human γ-herpesviruses Kaposi sarcoma associated herpesvirus (KSHV) and Epstein-Barr virus (EBV) are associated with many human malignancies. Viral glycoprotein H (gH) and glycoprotein L (gL) are crucial for the cell tropism by binding to specific receptors. Recently, EphA2 was identified as the specific entry receptor for both KSHV and EBV. Here, we characterized the crystal structures of KSHV gHgL or EBV gHgL in complex with the ligand binding domain (LBD) of EphA2. Both KSHV and EBV gHgL bind to the channel and peripheral regions of LBD primarily using gL. Extensive interactions with more contacts contribute to the higher affinity of KSHV gHgL to LBD than that of EBV gHgL. These binding characteristics were verified using cell-based fusion assays with mutations in key EphA2 residues. Our experiments suggest that multiple animal γ-herpesviruses could use EphA2 as an entry receptor, implying a potential threat to human health.

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Evaluation of serum Epstein–Barr virus envelope glycoproteins antibodies and their association with systemic autoimmune diseases

Li,

Zhong,

Kang

et al. 2024

Journal of Medical Virology

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Systemic autoimmune diseases (SADs) are a growing spectrum of autoimmune disorders that commonly affect multiple organs. The role of Epstein–Barr virus (EBV) infection or reactivation as a trigger for the initiation and progression of SADs has been established, while the relationship between EBV envelope glycoproteins and SADs remains unclear. Here, we assessed the levels of IgG, IgA, and IgM against EBV glycoproteins (including gp350, gp42, gHgL, and gB) in serum samples obtained from patients with rheumatoid arthritis (RA) and systemic lupus erythematosus (SLE), and found that RA and SLE patients exhibited a statistically significant increase in the levels of 8 and 11 glycoprotein antibodies, respectively, compared to healthy controls (p < 0.05). The LASSO model identified four factors as significant diagnostic markers for RA: gp350 IgG, gp350 IgA, gHgL IgM, and gp42 IgA; whereas for SLE it included gp350 IgG, gp350 IgA, gHgL IgA, and gp42 IgM. Combining these selected biomarkers yielded an area under the curve (AUC) of 0.749 for RA and 0.843 for SLE. We subsequently quantified the levels of autoantibodies associated with SADs in mouse sera following immunization with gp350. Remarkably, none of the tested autoantibody levels exhibited statistically significant alterations. Elevation of glycoprotein antibody concentration suggests that Epstein–Barr virus reactivation and replication occurred in SADs patients, potentially serving as a promising biomarker for diagnosing SADs. Moreover, the absence of cross‐reactivity between gp350 antibodies and SADs‐associated autoantigens indicates the safety profile of a vaccine based on gp350 antigen.

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Gammaherpesvirus entry and fusion: A tale how two human pathogenic viruses enter their host cells

Cited by 33 publications

References 134 publications

Towards Understanding KSHV Fusion and Entry

Towards Understanding KSHV Fusion and Entry

Molecular basis of EphA2 recognition by gHgL from gammaherpesviruses

Evaluation of serum Epstein–Barr virus envelope glycoproteins antibodies and their association with systemic autoimmune diseases

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