Liposomal vaccine formulations as prophylactic agents: design considerations for modern vaccines
Liposomal-based vaccines in fungal infection
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Liposomal-based vaccines in fungal infection
treatment Fungi are eukaryotic organisms that include yeasts, molds and mushrooms. Several yeasts and molds are common pathogenic agents, especially in immunocom- promised patients [ 101 , 102 ]. Antibiotic resistance is being detected, not only in isolates from the USA but also in other developed countries, in different fungal species (like Candida and Aspergillus) [ 103 ]. Due to the threat of antifungal resistance, other therapeutic approaches should be investigated, and liposomal vaccines may play a significant role. To the best of our knowledge, the litera- ture review presents liposome-based vaccines for Can- dida sp. infections but limited information is available for other fungal pathogens. Studies investigating other fun- gal species with elevated infection prevalence, like Asper- gillus, Fusarium, Coccidioidomyces and Zygomycetes sp., have been identified but their treatment approach does not include liposomal vaccines, and we invite fur- ther reading on the topic [ 101 , 104 , 105 ]. We will discuss ahead information available for liposomal vaccine devel- opment for the prophylactic treatment of Candida sp. infections (Table 5 ). The first report dealing with the study and develop- ment of a vaccine to treat candidiasis, encapsulated the mannan adhesin portion of Candida albicans [ 106 ]. The adhesin protion of the mannan of two C. albicans sero- types (A and B) were incorporated in PC:Chol liposomes (3.2:1 molar ratio). Mice were vaccinated (intravenously) during a period of 5–6 weeks and challenged with C. albicans infection, presenting increasing resistance to disseminated disease. Furthermore, antiserum aggluti- nins (IgM-type antibodies) from the immunized mice were studied for their humoral protective characteristics against C. tropicalis infection, demonstrating the effi- cacy of the vaccine. Subsequently, researchers decided to investigate the effectiveness of the monoclonal anti- bodies obtained from the previous study in a vaginal candidiasis model [ 107 ]. Similarly, the vaccine (L-mann) was prepared by the mannan adhesin fraction incorpo- ration into PC:Chol liposomes. Mice were immunized intravenously once a week for 5 weeks prior vaginal Yüklə 1,05 Mb. Dostları ilə paylaş:
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