The active substance in the candidate malaria vaccine, currently in Phase III, is the recombinant antigen RTS,S which targets the pre-erythrocytic stage of the parasite (see Chapter 3 – Vaccine antigens). Protective immunity against malaria requires the specific stimulation of both humoral and CMI responses, www.selleckchem.com/products/Dasatinib.html with the goal of decreasing the number of infectious parasites available to invade the liver while also destroying any hepatocytes that become infected. The RTS,S vaccine antigen has been formulated with several different adjuvant combinations ( Kester et al., 2009). AS01 has been selected for the final formulation because it demonstrated a better immune response and showed
a trend towards improved efficacy in several clinical trials compared with the other adjuvant combinations. AS15 combines
the effects of four adjuvants: liposome, MPL (TLR4 agonist), CpG (TLR9 agonist) and QS21. AS15, the most complex combination of adjuvants to date, is under investigation for use in cancer immunotherapy ( Brichard and Lejeune, 2007). Antigen-specific cancer immunotherapeutics (ASCI) are designed to treat cancer by targeting antigens that are selectively expressed or over-expressed by tumour cells, but not by normal cells. AS15 has been selected Cabozantinib cost for use in ASCI based on its ability to induce both high antibody titres and robust T-cell responses. AS15 aims to improve the immune response against the target antigen through a stronger immune activation which is sufficient to overcome tumour immuno-suppressive
processes. It has been shown in clinical trials that AS15, in comparison with other adjuvant combinations, elicits the most appropriate immune response for ASCI. The melanoma antigen A3 (MAGE-A3) is the target Resveratrol of current ASCI applications since it is expressed by different tumours. After showing promising results in Phase II studies, MAGE-A3/AS15 is in Phase III clinical studies as cancer-specific immunotherapy against NSCLC and melanoma. The safety profile of aluminium salt adjuvants has been well established through the use of billions of doses of aluminium-containing vaccines administered to infants, children, adolescents, adults and the elderly over more than 80 years. The safety of MF59™ and virosomes has been demonstrated through almost a decade of use. Innovative adjuvants to date have shown an acceptable safety profile in clinical trials across a variety of applications and in post-licensure experience. Increased reactogenicity, especially at the injection site, is consistently found for adjuvanted vaccines compared with those that are non-adjuvanted. The vaccination-related local symptoms which are generally reported with higher frequency are mild to moderate in intensity, of short duration, and do not impact compliance with vaccination schedules. Overall, adjuvanted vaccines are considered to have a positive benefit–risk ratio that is clinically acceptable.