Liposomal vaccine formulations as prophylactic agents: design considerations for modern vaccines



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10.1186 2Fs12951-017-0319-9

Mannosylated liposomes
Mannosylated liposomes are becoming an alternative 
method to deliver antigens or antimicrobials to mac-
rophages or DCs [
70

71
]. This approach is due to the fact 
that mannose receptors can be found in these cell types, 
improving directed-targeting [
16
]. Other research teams 
have used cationic lipids like DDA, DOTAP and/or DC-
Chol to enhance or potentiate the immune responses 
due to cell targeting strategies [
48

72

73
]. Korsholm 
et al. determine that DDA liposomes were minimally 
internalized by T cells in the mixed splenocyte cultures
contrasting to high uptake rates for APCs (bone mar-
row dendritic cells) through class II MHC (MHC II), 
leading to an enhanced OVA presentation. The immune 
responses described by Varypataki et al. contrasted to 
Korsholm et al. since DOTAP:DOPC liposomes bearing 
the peptide SIINFEKL and polyI:C assisted in the deliv-
ery of OVA to DCs through MHC I, inducing a CD8
+

cell response.
Understanding and applying innovative ways of cell 
targeting could improve the discovery pipeline for 
novel therapeutic agents, avoiding undesirable immune 
responses that can be detrimental to the patient. These 
therapies could treat inflammatory diseases [like arthri-
tis or chronic obstructive pulmonary disease (COPD)], 
infections or cancer. The following sections will focus on 
how liposome-based vaccines are being utilized for the 
treatment of infections from viral, bacterial, fungal and 
parasitic origins. A special section will discuss liposomal 
vaccines that target the bacterium Mycobacterium tuber-
culosis to treat TB infections.


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De Serrano and Burkhart  J Nanobiotechnol (2017) 15:83 

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