Liposomal vaccine formulations as prophylactic agents: design considerations for modern vaccines
Immunostimulatory lipids and liposome deposition
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Immunostimulatory lipids and liposome deposition
Immunostimulatory lipids might be of value in the vac- cine design process. The lipids can act as adjuvants in the vaccine formulation and enhance the immune response we are looking for (innate or adaptive) as previously reported and reviewed [ 2 , 5 , 6 , 47 ]. In a study developed by Rao et al., two adjuvants (lipid A and CpG-contain- ing oligodeoxynucleotides, CpG-ODN) were studied in a liposomal formulation based on the HIV envelop protein ogp140 [ 55 ]. Both lipid A and CpG-ODN-con- taining liposomes elicited six and threefold anti-ogp140 antibodies, respectively. Immunization of BALBc mice with the HIV antigen incorporated in lipid A-containing liposomes produced a mixed T H 1/T H 2 immune response. Combining both adjuvants in the liposomal formulation generated a T H 1 immune response. Puangpetch et al. presented the effect of using zwitterionic or cationic lipids in vaccine liposomal formulations [ 2 ]. Research- ers compared DOTAP (cationic phospholipid) vs. DOPC (neutral phospholid) containing the adjuvant CpG-ODN. DOTAP-based liposomes with adjuvant enhanced the immune response against Burkholderia pseudomallei, which suggest an alternative approach for the treatment of melioidosis. The published data available suggests that certain lipids can induce, or enhance, immune responses. Very important is the fact that cationic liposomes are the ideal model to design effective vaccines due to their immunostimulatory properties. Finally, the immunostimulation of the vaccine can be affected by the deposition of liposomes at the site of injection which in turn is affected by particle size. Hen- riksen-Lacey et al. reported this in two separate articles [ 6 , 56 ]. On Henriksen-Lacey et al. researchers utilized the phospholipid DDA as the building block for the liposomes containing the adjuvant TDB. The antigen for tuberculosis infection, Ag85B-ESAT-6, was co-admin- istered or incorporated to liposomes in mice. Antigen administered alone to mice did not created a depot at the site of injection, causing the antigen to diffuse away from the site and reduce immune responses. The observations directed them to conclude that cationic liposomes made up of DDA promotes depot formation at the site of injection mainly due to size characteristics between antigen-loaded liposomes and antigen admin- istered alone. Later, Henriksen-Lacey et al. [ 30 ] stud- ied the effect of liposome composition [DOTAP, DDA or DC-Chol (dimethylaminoethane-carbamoyl-choles- terol)] and the depot formation and antigen distribu- tion. DDA and DC-Chol represented the phospholipids where liposomes induced the migration of monocytes to the site of injection and a significant increase of IFN-γ levels. In general, larger liposomes will form a depot at the site of injection meanwhile smaller liposomes will migrate to lymphoid tissue for antigen presentation and processing. Page 7 of 23 De Serrano and Burkhart J Nanobiotechnol (2017) 15:83 Yüklə 1,05 Mb. Dostları ilə paylaş:
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