Chimeric hepatitis E virus-like particle as a carrier for oral-delivery

Jariyapong, Pitchanee; Li, Xing; Houten, Nienke E. van; Li, Tiancheng; Weerachatyanukul, Wattana; Hsieh, Benjamin; Moscoso, Carlos G.; Chen, Chun Chieh; Niikura, Masahiro; Cheng, Harry H.

doi:10.1016/j.vaccine.2012.10.073

Cited by 38 publications

(47 citation statements)

References 29 publications

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“…Previous studies have shown that the insertion of a peptide at C-terminal of HEV not only affects self-assembling of VLP formation, but also helps the produced VLP be used as carrier for other antigens (21,22). Our results in agreement with previous reports showed that the OSU-a strain of Rotavirus NSP4 was successfully linked to C-terminal of the truncated ORF2 to assemble to VLP.…”

Section: Discussionsupporting

confidence: 92%

A Study on the Virus-Like Particle Formation of Hepatitis E Virus ORF2 and Rotavirus NSP4 Protein in the Eukaryotic and Prokaryotic Expression Systems

Makvandi

Teimoori

Neisi

et al. 2017

Jundishapur J Microbiol

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Background: Hepatitis E virus (HEV) is able to induce fulminant hepatitis E infection in immunosuppressed individuals. Previous studies showed that the Baculovirus expression system (BES) could be used for developing hepatitis E virus-like particles (VLPs). Objectives: In the present study, the formation of VLPs of the recombinant proteins of HEV truncated open reading frame 2 (ORF2; 112 -607) and Rotavirus non-structural protein 4 (NSP4) (OSU-a) were investigated in BES and Escherichia. coli. Methods: To construct VLPs, the truncated ORF2-NSP4 protein was expressed in BES. The expression of protein was confirmed by western blot. This protein was expressed in E. coli. The truncated ORF2-NSP4 gene was subcloned in pET28a, and then transformed into E. coli DH5α. The confirmed colonies were transformed into E. coli BL21. The solubility of protein were checked by SDS-PAGE and western blot analysis. In the final step, to verify the VLP formation in BES and E. coli, the recombinant proteins were stained with 2% uranyl acetate and checked by transmission electron microscopy (TEM). Results:The 75 KDa truncated ORF2-NSP4 protein was successfully expressed in Sf9 cells, assembled, and formed VLP according to TEM results. In the prokaryotic expression system (E. coli), the ORF2-NSP4 gene was successfully subcloned and expressed in BL21 but VLP was not detected in TEM analysis. Conclusions:The truncated ORF2-NSP4 VLP were efficiently expressed in the SF9 cells, as a potential mucosal vaccine against HEV and Rotavirus. In the prokaryotic expression system (E. coli), the ORF2-NSP4 gene was successfully expressed.

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Section: Discussionsupporting

confidence: 92%

A Study on the Virus-Like Particle Formation of Hepatitis E Virus ORF2 and Rotavirus NSP4 Protein in the Eukaryotic and Prokaryotic Expression Systems

Makvandi

Teimoori

Neisi

et al. 2017

Jundishapur J Microbiol

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“…Induction of mucosal immunity through oral vaccine administration is benefi cial due to its convenience; however, there are several diffi culties in oral immunization with non-replicating molecules such as proteolytic enzymes in the gastrointestinal tract and an acidic environment. VLPs derived from harmful human viruses such as the hepatitis-E virus-like particle (HEV-VLP) have previously been found to be tolerant and still intact after exposure to digestive juices (Jariyapong et al 2013). Th is is because the quaternary arrangement of VLP protein protects it from the cleavage of protease enzymes.…”

Section: Stability Of Nodavirus-like Particles Under Harsh Hydrolyticmentioning

confidence: 99%

Nodavirus-based biological container for targeted delivery system

Jariyapong

2014

Artificial Cells, Nanomedicine, and Biotechnology

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Biological containers such as virus-like particles (VLPs) have gained increasing interest in the fields of gene therapy and vaccine development. Several virus-based materials have been studied, but the toxicity, biodistribution, and immunology of these systems still require extensive investigation. The specific goal of this review is to provide information about nodaviruses, which are causative infectious agents of insects and aquatic animals, but not humans. By understanding the structure and biophysical properties of such viruses, further chemical or genetic modification for novel nanocarriers could be developed. Therefore, their application for therapeutic purposes, particularly in humans, is of great interest.

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“…Particles were then manually selected and initially center and orientation was determined by reference-dependent cross-correlation by using a density of the wild-type HEV-VLP [19] as our initial model. Polar Fourier transformation algorithm [20] was used to iteratively carry out origin and orientation refinement.…”

Section: Methodsmentioning

confidence: 99%

“…Moreover, it can accommodate sequence modification at P-domain without interference with HEV-VLP assembly. Genetically engineered chimeric VLPs having modifications in the somewhat isolated protrusion domain, are as stable as wild-type VLPs [9], and like the HEV virion, can tolerate extreme pH values and intestinal proteases [10]. This has exciting implications for an orally deliverable chemotherapeutic agent.…”

Section: Introductionmentioning

confidence: 99%

Chemically Activatable Viral Capsid Functionalized for Cancer Targeting

Chen

Stark

et al. 2016

Nanomedicine (Lond.)

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Aim To design a theranostic capsule using the virus-like nanoparticle of the hepatitis E virus modified to display breast cancer cell targeting functional group (LXY30). Methods Five surface-exposed residues were mutated to cysteine to allow conjugation to maleimide-linked chemical groups via thiol-selective linkages. Engineered virus-like nanoparticles were then covalently conjugated to a breast cancer recognized ligand, LXY30 and an amine-coupled near-infrared fluorescence dye. Results LXY30-HEV VLP was checked for its binding and entry to a breast cancer cell line and for tumor targeting in vivo to breast cancer tissue in mice. The engineered virus-like nanoparticle not only targeted cancer cells, but also appeared immune silent to native hepatitis E virus antibodies due to epitope disruption at the antibody-binding site. Conclusion These results demonstrate the production of a theranostic capsule suitable for cancer diagnostics and therapeutics based on surface modification of a highly stable virus-like nanoparticle.

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Chimeric hepatitis E virus-like particle as a carrier for oral-delivery

Cited by 38 publications

References 29 publications

A Study on the Virus-Like Particle Formation of Hepatitis E Virus ORF2 and Rotavirus NSP4 Protein in the Eukaryotic and Prokaryotic Expression Systems

A Study on the Virus-Like Particle Formation of Hepatitis E Virus ORF2 and Rotavirus NSP4 Protein in the Eukaryotic and Prokaryotic Expression Systems

Nodavirus-based biological container for targeted delivery system

Chemically Activatable Viral Capsid Functionalized for Cancer Targeting

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