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Bacteriophage T4 nanoparticles for vaccine delivery against infectious diseases

Journal

ADVANCED DRUG DELIVERY REVIEWS
Volume 145, Issue -, Pages 57-72

Publisher

ELSEVIER
DOI: 10.1016/j.addr.2018.06.025

Keywords

Vaccines; Virus like particle; Bacteriophage 74; Phage display; Phage assembly; DNA packaging

Funding

  1. National Institute of Allergy and Infectious Diseases [AI111538, AI081726]
  2. National Science Foundation [MCB-1411989]

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Subunit vaccines containing one or more target antigens from pathogenic organisms represent safer alternatives to whole pathogen vaccines. However, the antigens by themselves are not sufficiently immunogenic and require additives known as adjuvants to enhance immunogenicity and protective efficacy. Assembly of the antigens into virus-like nanoparticles (VLPs) is a better approach as it allows presentation of the epitopes in a more native context. The repetitive, symmetrical, and high density display of antigens on the VLPs mimic pathogen-associated molecular patterns seen on bacteria and viruses. The antigens, thus, might be better presented to stimulate host's innate as well as adaptive immune systems thereby eliciting both humoral and cellular immune responses. Bacteriophages such as phage T4 provide excellent platforms to generate the nanoparticle vaccines. The T4 capsid containing two non-essential outer proteins Soc and Hoc allow high density array of antigen epitopes in the form of peptides, domains, full-length proteins, or even multi-subunit complexes. Co-delivery of DNAs, targeting molecules, and/or molecular adjuvants provides additional advantages. Recent studies demonstrate that the phage T4 VLPs are highly immunogenic, do not need an adjuvant, and provide complete protection against bacterial and viral pathogens. Thus, phage T4 could potentially be developed as a universal VLP platform to design future multivalent vaccines against complex and emerging pathogens. (C) 2018 Elsevier B.V. All rights reserved.

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