Erstellt von Amalin Najiha Mohd Sabri
vor mehr als 6 Jahre
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How vaccines were made historically Live attenuated – vaccinia, BCG, polio (Sabin) Killed – Rabies (Pasteur), Adjuvanted- alum, Sub-units- Hepatitis B surface protein Conjugated vaccines, Hib, covalently linked to tetanus toxoid, Men B omp Pneumococcus CHO linked to CRM197 (diphtheria t) Men C linked to tetanus Future DNA vaccines- work in mice Vectored in vaccinia Prime-boost Polyvalent- 6 in 1, 23 valent PneumoVax H1N1 influenza A vaccine – AS03 & narcolepsy Individualised APC primed against cancers
Ebola vaccine How to make one - Whole-cell killed - Live attenuated - Sub-unit *Conserved sequences : Glycoprotein * Immunogenic (works in guinea pigs) * Adjuvants - antibodies or T cells - DNA plasmid - Vectored - Chimpanzee adenovirus 2. Candidates - Mice, guinea pig, hamster, non-human primate 3. Pre-clinical trials/evaluation - Stability - temperature, time - Purity, toxins, contaminants, LPS, - Mice immunogenicity * Antibody levels * Neutralising antibodies * T cell responses - Toxicity and path – in 2 species mice, rabbits • Distribution - Efficacy in animal models, incl. primates 4. Clinical trials - There are 2 phases * Phase I - immunogenicity in human, tolerability * Phase II - efficacy, likely no trials in humans - Deployment based on safety and immunogenicity in humans and efficacy in animal models 5. Licensure 6. Marketing and distribution
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