Ovalbumin-loaded PEGylated liposomes decorated with DC-targeting

Ovalbumin-loaded PEGylated liposomes decorated with DC-targeting peptides distributed to splenic DC in vivo, induced an adaptive immune response against, ovalbumin and

exhibited dramatic therapeutic activity against established B16-OVA melanoma tumors with complete tumor regression in 80% of treated mice [218]. In other studies Altin’s group reported on DC-targeted gene delivery in vivo and potent antitumor effects in the B16-OVA melanoma model after liposome functionalization Inhibitors,research,lifescience,medical with histidylated flagellin, the major constituent of the bacterial flagella, recognized by the Toll Like Receptor 5 that leads to their activation [221, 222]. LPR (Lipid-Polymer-RNA) mannosylated and histidylated lipopolyplexes loaded with MART1 (Melanoma Antigen Recognized by T cells 1) mRNA delayed the progression of B16F10 melanoma more effectively than untargeted LPR [223]. This study also Inhibitors,research,lifescience,medical illustrated the importance of cytosolic delivery of nucleic acids for in vivo transfection of DC. The authors used a ternary formulation of mRNA or pDNA coding for the reporter gene EGFP (Enhanced Inhibitors,research,lifescience,medical Green Fluorescent Protein) complexed with PEGylated histidylated poly-L-Lysine and imidazole-rich liposomes, both of which promote endosomal

escape [224, 225]. While no in vivo transfection of splenic DC was observed with pDNA, 12% were transfected with mRNA mannosylated LPR and 3% with untargeted LPR demonstrating that buy LY2157299 nuclear

delivery is a limiting Inhibitors,research,lifescience,medical step for DC transfection. Liposomes targeted to dendritic cells by mannosylated ligands have recently been used as a platform for effective cancer immunotherapy [114]. The liposomes used harbored mannosylated ligands at their surface for targeting of antigen presenting cells with a cytotoxic T lymphocyte peptide of the renal carcinoma antigen ErbB2 for induction of an adaptive immune response, Toll Like Receptors (TLRs) agonists as adjuvants and a T helper lymphocyte epitope peptide for improved immune Inhibitors,research,lifescience,medical activation. Of note, the authors developed new functionalized lipid anchors devoid of adjuvant activity for their study: dipalmitoylglycerol maleimide and dipalmitoylglycerol bromoacetate. These liposomes induced an adaptive immune response against the ErbB2 antigen with high therapeutic activity. Targeting of intraperitoneal macrophages by ovalbumin-loaded liposomes armed with dipalmitoylphosphatidylethanolamine conjugated mannotriose increased no antigen-specific cell lysis induction by splenocytes over untargeted liposomes resulting in therapeutic efficacy both as a preventive and therapeutic cancer vaccine [115]. In addition to carrying tumor antigens, liposomal vaccines are armed with immunostimulatory lipids, usually derived from microorganisms, recognized by pathogen recognition receptors leading to immunostimulation (reviewed in [226]). Zhong et al.

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