Phytol-based novel adjuvants in vaccine formulation: I. assessment of safety and efficacy during stimulation of humoral and cell-mediated immune responses

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Abstract

Background: Vaccine efficacy depends significantly on the use of appropriate adjuvant(s) in the formulation. Phytol, a dietary diterpene alcohol, is similar in structure to naturally occurring isoprenoid adjuvants; but little is known of its adjuvanticity. In this report, we describe the relative safety and efficacy of phytol and its hydrogenated derivative PHIS-01 compared to commercial adjuvants. Methods: We tested adjuvant properties using a formulation consisting of either a hapten, phthalate-conjugated to a protein, keyhole limpet hemocyanin (KLH), or ovalbumin (OVA) emulsified with the test adjuvants in mice without any surfactant. Humoral immunity was assessed in terms of titer, specificity, and isotypic profiles. The effect on cell-mediated immunity was studied by assaying the induction of either OVA- or B-lymphoma-specific cytotoxic T-lymphocyte (CTL) activity. Results and Discussion: The phytol compounds, particularly PHIS-0 1, elicit increased titers of all major IgG subclasses, especially IgG2a. Unlike commercial adjuvants, both phytol compounds are capable of inducing specific cytotoxic effector T cell responses specific to both OVA and B-lymphoma tested. Phytols as adjuvants are also distinctive in that they provoke no adverse anti-DNA autoimmune response. Intraperitoneally administered phytol is comparable to complete Freund's adjuvant in toxicity in doses over 40 ug/mouse, but PHIS-0 I has no such toxicity. Conclusion: These results and our ongoing studies on antibacterial immunity show that phytol and PHIS-0 I are novel and effective adjuvants with little toxicity. © 2006'Lim et al; licensee BioMed Central Ltd.

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Lim, S. Y., Meyer, M., Kjonaas, R. A., & Ghosh, S. K. (2006). Phytol-based novel adjuvants in vaccine formulation: I. assessment of safety and efficacy during stimulation of humoral and cell-mediated immune responses. Journal of Immune Based Therapies and Vaccines, 4. https://doi.org/10.1186/1476-8518-4-6

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