Vaccine development: From concept to early clinical testing

doi:10.1016/j.vaccine.2016.10.016

Review

. 2016 Dec 20;34(52):6655-6664.

doi: 10.1016/j.vaccine.2016.10.016. Epub 2016 Oct 18.

Vaccine development: From concept to early clinical testing

Anthony L Cunningham¹, Nathalie Garçon², Oberdan Leo³, Leonard R Friedland⁴, Richard Strugnell⁵, Béatrice Laupèze⁶, Mark Doherty⁷, Peter Stern⁸

Affiliations

¹ Westmead Institute, The Centre for Virus Research, 176 Hawkesbury Road, NSW 2145, Australia. Electronic address: tony.cunningham@sydney.edu.au.
² Bioaster, 321 Avenue Jean Jaurès, 69007 Lyon, France. Electronic address: nathalie.garcon@bioaster.org.
³ Université Libre de Bruxelles, CP300, Rue des Professeurs Jeener et Brachet 12, 6041 Charleroi, Belgium. Electronic address: oleo@ulb.ac.be.
⁴ GSK Vaccines, 5 Crescent Drive, Philadelphia, PA 19112, United States. Electronic address: leonard.r.friedland@gsk.com.
⁵ Department of Microbiology & Immunology, University of Melbourne, Doherty Institute, Melbourne, VIC 3000, Australia. Electronic address: rastru@unimelb.edu.au.
⁶ GSK Vaccines, Avenue Fleming 20, Parc de la Noire Epine, B-1300 Wavre, Belgium. Electronic address: beatrice.n.laupeze@gsk.com.
⁷ GSK Vaccines, Avenue Fleming 20, Parc de la Noire Epine, B-1300 Wavre, Belgium. Electronic address: mark.x.doherty@gsk.com.
⁸ Institute of Cancer Sciences, The University of Manchester, Manchester M20 4BX, United Kingdom. Electronic address: peter.stern@cruk.manchester.ac.uk.

PMID: 27769596
DOI: 10.1016/j.vaccine.2016.10.016

Free article

Review

Vaccine development: From concept to early clinical testing

Anthony L Cunningham et al. Vaccine. 2016.

Free article

. 2016 Dec 20;34(52):6655-6664.

doi: 10.1016/j.vaccine.2016.10.016. Epub 2016 Oct 18.

Authors

Anthony L Cunningham¹, Nathalie Garçon², Oberdan Leo³, Leonard R Friedland⁴, Richard Strugnell⁵, Béatrice Laupèze⁶, Mark Doherty⁷, Peter Stern⁸

Affiliations

¹ Westmead Institute, The Centre for Virus Research, 176 Hawkesbury Road, NSW 2145, Australia. Electronic address: tony.cunningham@sydney.edu.au.
² Bioaster, 321 Avenue Jean Jaurès, 69007 Lyon, France. Electronic address: nathalie.garcon@bioaster.org.
³ Université Libre de Bruxelles, CP300, Rue des Professeurs Jeener et Brachet 12, 6041 Charleroi, Belgium. Electronic address: oleo@ulb.ac.be.
⁴ GSK Vaccines, 5 Crescent Drive, Philadelphia, PA 19112, United States. Electronic address: leonard.r.friedland@gsk.com.
⁵ Department of Microbiology & Immunology, University of Melbourne, Doherty Institute, Melbourne, VIC 3000, Australia. Electronic address: rastru@unimelb.edu.au.
⁶ GSK Vaccines, Avenue Fleming 20, Parc de la Noire Epine, B-1300 Wavre, Belgium. Electronic address: beatrice.n.laupeze@gsk.com.
⁷ GSK Vaccines, Avenue Fleming 20, Parc de la Noire Epine, B-1300 Wavre, Belgium. Electronic address: mark.x.doherty@gsk.com.
⁸ Institute of Cancer Sciences, The University of Manchester, Manchester M20 4BX, United Kingdom. Electronic address: peter.stern@cruk.manchester.ac.uk.

PMID: 27769596
DOI: 10.1016/j.vaccine.2016.10.016

Abstract

In the 21st century, an array of microbiological and molecular allow antigens for new vaccines to be specifically identified, designed, produced and delivered with the aim of optimising the induction of a protective immune response against a well-defined immunogen. New knowledge about the functioning of the immune system and host pathogen interactions has stimulated the rational design of vaccines. The design toolbox includes vaccines made from whole pathogens, protein subunits, polysaccharides, pathogen-like particles, use of viral/bacterial vectors, plus adjuvants and conjugation technology to increase and broaden the immune response. Processes such as recombinant DNA technology can simplify the complexity of manufacturing and facilitate consistent production of large quantities of antigen. Any new vaccine development is greatly enhanced by, and requires integration of information concerning: 1. Pathogen life-cycle & epidemiology. Knowledge of pathogen structure, route of entry, interaction with cellular receptors, subsequent replication sites and disease-causing mechanisms are all important to identify antigens suitable for disease prevention. The demographics of infection, specific risk groups and age-specific infection rates determine which population to immunise, and at what age. 2. Immune control & escape. Interactions between the host and pathogen are explored, with determination of the relative importance of antibodies, T-cells of different types and innate immunity, immune escape strategies during infection, and possible immune correlates of protection. This information guides identification and selection of antigen and the specific immune response required for protection. 3. Antigen selection & vaccine formulation. The selected antigen is formulated to remain suitably immunogenic and stable over time, induce an immune response that is likely to be protective, plus be amenable to eventual scale-up to commercial production. 4. Vaccine preclinical & clinical testing. The candidate vaccine must be tested for immunogenicity, safety and efficacy in preclinical and appropriately designed clinical trials. This review considers these processes using examples of differing pathogenic challenges, including human papillomavirus, malaria, and ebola.

Keywords: Adaptive immunity; Adjuvants; Antigen; Clinical development; Innate immunity; Vaccine.

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Vaccine development: From concept to early clinical testing

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Vaccine development: From concept to early clinical testing

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