Silicone Oil-Based Nanoadjuvants as Candidates for a New Formulation of Intranasal Vaccines.
Agnieszka RazimMarcelina J PyclikKatarzyna Pacyga-PrusSabina GórskaJintao XuMichal A OlszewskiAndrzej GamianAndrzej MycPublished in: Vaccines (2021)
Many conventional vaccines are administered via a needle injection, while most pathogens primarily invade the host via mucosal surfaces. Moreover, protective IgA antibodies are insufficiently induced by parenteral vaccines. Mucosal immunity induces both local and systemic response to pathogens and typically lasts for long periods of time. Therefore, vaccination via mucosal routes has been increasingly explored. However, mucosal vaccines require potent adjuvants to become efficacious. Despite many efforts to develop safe and robust adjuvants for mucosal vaccines, only a few have been approved for use in human formulations. The aim of our study was to design, develop and characterize new silicone oil-based nanoadjuvant candidates for intranasal vaccines with potential to become mucosal adjuvants. We have developed an array of nanoadjuvant candidates (NACs), based on well-defined ingredients. NAC1, 2 and 3 are based on silicone oil, but differ in the used detergents and organic solvents, which results in variations in their droplet size and zeta potential. NACs' cytotoxicity, Tumor Necrosis Factor α (TNF-α) induction and their effect on antigen engulfment by immune cells were tested in vitro. Adjuvant properties of NACs were verified by intranasal vaccination of mice together with ovalbumin (OVA). NACs show remarkable stability and do not require any special storage conditions. They exhibit bio-adhesiveness and influence the degree of model protein engulfment by epithelial cells. Moreover, they induce high specific anti-OVA IgG antibody titers after two intranasal administrations. Nanoadjuvant candidates composed of silicone oil and cationic detergents are stable, exhibit remarkable adjuvant properties and can be used as adjuvants for intranasal immunization.
Keyphrases
- ulcerative colitis
- fatty acid
- rheumatoid arthritis
- early stage
- endothelial cells
- ultrasound guided
- transcription factor
- metabolic syndrome
- drug delivery
- type diabetes
- adipose tissue
- gram negative
- staphylococcus aureus
- escherichia coli
- insulin resistance
- high fat diet induced
- high density
- amino acid
- water soluble
- induced pluripotent stem cells