Immunopotentiators in Modern Vaccines (2nd Ed.)
Coordonnateurs : Schijns Virgil, O'Hagan Derek
Immunopotentiators in Modern Vaccines, Second Edition, provides in-depth insights and overviews of the most successful adjuvants, those that have been included in licensed products, also covering the most promising technologies that have emerged in recent years. In contrast to existing books on the subject, the chapters here provide summaries of key data on the mechanisms of action of the individual vaccine adjuvants.
In addition, the book covers key aspects of how the technologies might be further developed and what might be their limitations, while also giving an overview of what made the most advanced adjuvant technologies successful.
1. Vaccine Adjuvants' Mode of Action: Unraveling ‘‘the Immunologist's Dirty Little Secret 2. The Role of Inflammasomes in Adjuvant-Driven Humoral and Cellular Immune Responses 3. Dendritic Cells as Targets of Vaccines and Adjuvants 4. Host-Derived Cytokines and Chemokines as Vaccine Adjuvants 5. Discovery of Immune Potentiators as Vaccine Adjuvants 6. Current Status of Toll-Like Receptor 4 Ligand Vaccine Adjuvants 7. Flagellins as Adjuvants of Vaccines 8. Toll-Like Receptor 7 and 8 Agonists for Vaccine Adjuvant Use 9. CpG Oligodeoxynucleotides as Adjuvants for Clinical Use 10. Advax Adjuvant: A Potent and Safe Immunopotentiator Composed of Delta Inulin 11. Natural Vaccine Adjuvants and Immunopotentiators Derived From Plants, Fungi, Marine Organisms, and Insects 12. Polymeric Particles as Vaccine Delivery Systems 13. MF59: A Safe and Potent Adjuvant for Human Use 14. The Development of the Adjuvant System AS01: A Combination of Two Immunostimulants MPL and QS-21 in Liposomes 15. Development and Evaluation of AS04, a Novel and Improved Adjuvant System Containing 3-O-Desacyl-4'- Monophosphoryl Lipid A and Aluminum Salt 16. ISCOMATRIX Adjuvant in the Development of Prophylactic and Therapeutic Vaccines 17. Development and Evaluation of CAF01 18. Mineral Adjuvants 19. Toxin-Based Mucosal Adjuvants 20. Adjuvants for Skin Vaccination 21. Vaccination to Treat Noninfectious Diseases: Surveying the Opportunities 22. A Framework for Evaluating Nonclinical Safety of Novel Adjuvants and Adjuvanted Preventive Vaccines
Dr. Derek O’Hagan was the Global Head of Vaccine Chemistry and Formulation Research for Novartis Vaccines, based in Cambridge, MA until acquisition by GSK in March, 2015. He managed research teams (~50 total staff) in Cambridge and Siena, Italy. He originally qualified as a pharmacist in the UK, and is a former academic researcher who has worked on vaccine delivery in the industry since 1993. He was formerly a Lecturer in Drug Delivery at the Department of Pharmaceutical Sciences, University of Nottingham, UK, and received research funding from the World Health Organization, The Wellcome Trust and the Medical Research Council. He was recruited into the US in 1993, and moved to progress basic research into clinical evaluation, then subsequently worked on several vaccine delivery systems that were evaluated in the clinic, including novel adjuvants, nucleic acid vaccines and needle free vaccines. In the mid 1990’s, Dr. O’Hagan worked on the emulsion adjuvant MF59, which is now included in a licensed flu vaccine in more than 40 countries and is progressing towards licensure in the US. He has co-authored >140 original research publications, >60 book chapters and reviews and I
- Provides contributions from leading international authorities in the field
- Features immunopotentiators classified by function, with well-illustrated, informative figures presenting the interaction between the immunopotentiators and the host immune system
- Lists advantages and potential hurdles for achieving a practical application for each specific immunopotentiator
- Offers US FDA perspectives which highlight how future adjuvants will be approved for new generation vaccines
Date de parution : 11-2016
Ouvrage de 508 p.
19x23.3 cm
Thème d’Immunopotentiators in Modern Vaccines :
Mots-clés :
Adaptive immunity; Adaptive response; Adjuvant formulation; Adjuvant safety; Adjuvant system; Adjuvant; Adjuvants; Advax; Alum; Aluminum hydroxide adjuvant; Aluminum phosphate adjuvant; Aluminum; Antibodies; Antibody isotypes; Antigen-presenting cells; Antigens; AS04 adjuvant system; CAF01; Calcium phosphate adjuvant; Cancer vaccines; Cancer; Cargo; Cationic; Cell-mediated immunity; Chemokine; Chronic disease; Compounds; CpG ODN; CT and LT; Cytokine; Cytokines; Delivery system; Delivery systems; Delta inulin; Dendritic cell; Dendritic cells; EMA; Epithelium; FDA; Flagellin; Freund Adjuvant; Fungi; GLA; HBV; HPV; HSV; Imidazoquinoline; Immune potentiator; Immune system; Immunepotentiators; Immunogenicity; Immunomodulator; Immunopotentiators; Immunosenescence; Immunostimulant; Infectious disease; Inflammasome; Inflammasomes; Influenza vaccine; Innate immunity; Insects; Keyword; Langmuir isotherm; Laser adjuvant; Lectins; Liposome; Liposomes; Lymph node; Major histocompatibility complex; Marine; Mechanical adjuvants; MF59; Microparticles; Mode of action; Monophosphoryl lipid A; MPL; Mucosal adjuvants; Mucosal immunity; Nanoparticle; NLR; NLRP3; Nonclinical/preclinical safety studies; PAMP; Pathogens; Plant; PLG; Polysaccharides; Proinflammatory; Prophylactic vaccine; Prophylactic vaccines; Prophylactic; PRRs; QS-21; RSV; Saponin; Skin vaccination; SMIP; Squalene; T cell; Th1 immunity; Therapeutic vaccines; Therapeutic; TLR; TLR4 ligands; TLR9; Toll-like receptor 5; Toll-like receptor; Toll-like receptors; Toth isotherm; Toxicology; Toxin; Toxins; Vaccination; Vaccine adjuvants; Vaccine; Vaccines; Viruslike particle
