This work was presented at the 2010 Keystone Vaccine Symposium, O

This work was presented at the 2010 Keystone Vaccine Symposium, Oct 27–Nov 01, 2010, Seattle, USA. Abstract # 109. Conflict of interest statement: None declared. “
“Effective immunization largely depends on the consideration of immunogenic vaccine antigens and effective adjuvants. Most live attenuated or killed vaccines have been replaced by subunit vaccines, which are safer but typically

are less immunogenic and thus require the presence of strong adjuvants Sirolimus cell line that can induce an early onset of immunity, long duration, and if needed, a shift in the type of the response. Furthermore, the use of effective adjuvant platforms can also help to reduce the number of immunizations required, ideally to a single immunization only. Adjuvants include a large group of molecules that can be divided into delivery systems and immune modulators. Most often immune stimulators are derived from pathogen associated INK1197 molecular patterns (PAMPs) also termed as ‘danger signals’ like bacterial unmethylated CpG, LPS, flagellin and viral double stranded RNA to name a few. These PAMPs are recognized by

cells of the innate immune system, including antigen presenting cells, which express specific pathogen recognition receptors (PRRs) such as Toll like receptors (TLRs). In the present study, we evaluated a novel vaccine platform containing CpG ODNs, polyphosphazenes and cationic innate defense regulator peptide (IDR) 1002. CpG ODNs have been studied extensively in regards to their immune stimulatory activities and are well characterized as vaccine adjuvant in both preclinical and clinical studies [1]. CpG ODN act through TLR9, expressed on human plasmacytoid DCs and B-cells [2], and favor induction of a pro-inflammatory Th1 immune response. Thus, CpG ODN has been used as adjuvants to promote a Th1 or mixed Th1/Th2 response in experimental vaccines against various diseases

[3] and [4]. Interestingly, CpG ODNs have shown greater adjuvanticity when co-administered with other adjuvants [5] and [6]. In the present study, CpG ODNs were co-formulated with synthetic innate defense regulator (IDR) peptides, which have well documented selective immune stimulatory activities that include protection against infections, chemokine induction leading to the recruitment of leukocytes, wound healing, modulation Resminostat of apoptosis, and anti-inflammatory activities [7] and [8]. IDRs are synthetic mimics of host defense peptides, which represent important components of the innate immune system and these peptides also enhance and modulate adaptive immune responses [9] and [10]. We previously demonstrated this adjuvantation with a pertussis vaccine [11]. Polyphosphazenes are an emerging class of well-defined macromolecules that combine immune stimulatory activity and dose-sparing effects with the ease of their assembly into supra-molecular MP structures to achieve optimal delivery [12].

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