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Virus-like particles in vaccine development

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TLDR
This article focuses on the essential role of VLP technology in new-generation vaccines against prevalent and emergent diseases and the implications of large-scale VLP production in the context of process control, monitorization and optimization.
Abstract
Virus-like particles (VLPs) are multiprotein structures that mimic the organization and conformation of authentic native viruses but lack the viral genome, potentially yielding safer and cheaper vaccine candidates. A handful of prophylactic VLP-based vaccines is currently commercialized worldwide: GlaxoSmithKline's Engerix (hepatitis B virus) and Cervarix (human papillomavirus), and Merck and Co., Inc.'s Recombivax HB (hepatitis B virus) and Gardasil (human papillomavirus) are some examples. Other VLP-based vaccine candidates are in clinical trials or undergoing preclinical evaluation, such as, influenza virus, parvovirus, Norwalk and various chimeric VLPs. Many others are still restricted to small-scale fundamental research, despite their success in preclinical tests. This article focuses on the essential role of VLP technology in new-generation vaccines against prevalent and emergent diseases. The implications of large-scale VLP production are discussed in the context of process control, monitorization and optimization. The main up- and down-stream technical challenges are identified and discussed accordingly. Successful VLP-based vaccine blockbusters are briefly presented concomitantly with the latest results from clinical trials and the recent developments in chimeric VLP-based technology for either therapeutic or prophylactic vaccination.

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Vaccine delivery using nanoparticles

TL;DR: N nanoscale size materials such as virus-like particles, liposomes, ISCOMs, polymeric, and non-degradable nanospheres have received attention as potential delivery vehicles for vaccine antigens which can both stabilize vaccine antIGens and act as adjuvants, thereby modulating the immune response to the antigen.
Journal ArticleDOI

Construction and Characterization of Virus-Like Particles: A Review

TL;DR: The main principles in the cloning of viral structural genes, the relevant host systems and the purification procedures that have been developed are discussed and the methods that are used to characterize the structural integrity, stability, and components of newly synthesized VLPs are analyzed.
Journal ArticleDOI

Design of a hyperstable 60-subunit protein icosahedron

TL;DR: The computational design of a 25-nanometre icosahedral nanocage that self-assembles from trimeric protein building blocks is described, and such robust and customizable nanocages should have considerable utility in targeted drug delivery, vaccine design and synthetic biology.
Journal ArticleDOI

Nanoparticle Vaccines Against Infectious Diseases

TL;DR: This review article focuses on the applications of nanocarrier-based vaccine formulations and the strategies used for the functionalization of nanoparticles to accomplish efficient delivery of vaccines in order to induce desired host immunity against infectious diseases.
Journal ArticleDOI

Plug-and-Display: decoration of Virus-Like Particles via isopeptide bonds for modular immunization.

TL;DR: Injecting SpyCatcher-VLPs decorated with a malarial antigen efficiently induced antibody responses after only a single immunization, which should accelerate vaccine development, as well as other applications of nanoparticle devices.
References
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Case-control study of human papillomavirus and oropharyngeal cancer.

TL;DR: Oropharyngeal cancer was significantly associated with oral HPV type 16 (HPV-16) infection, and the degree of association increased with the number of vaginal-sex and oral-sex partners, among subjects with or without the established risk factors of tobacco and alcohol use.
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A review of human carcinogens--Part B: biological agents

TL;DR: In this paper, the carcinogenicity of the biological agents classifi ed as "carcinogenic to humans" (Group 1) and to identify additional tumour sites and mechanisms of carcinogenesis (tables 1 and 2).
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Chapter 2: the burden of hpv-related cancers

TL;DR: Estimates of the global burden of HPV-related cancers, and the proportion that are actually "caused" by infection with HPV types, and therefore potentially preventable, are provided.
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Papillomavirus L1 major capsid protein self-assembles into virus-like particles that are highly immunogenic.

TL;DR: Results indicate that L1 protein has the intrinsic capacity to assemble into empty capsid-like structures whose immunogenicity is similar to infectious virions.
Journal ArticleDOI

Expression, self-assembly, and antigenicity of the Norwalk virus capsid protein.

TL;DR: The availability of large amounts of recombinant Norwalk virus particles will allow the development of rapid, sensitive, and reliable tests for the diagnosis of Norwalkirus infection as well as the implementation of structural studies.
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