pH-sensitive polymer-liposome-based antigen delivery systems potentiated with interferon-γ gene lipoplex for efficient cancer immunotherapy

被引:77
作者
Yuba, Eiji [1 ]
Kanda, Yuhei [1 ]
Yoshizaki, Yuta [1 ]
Teranishi, Ryoma [1 ]
Harada, Atsushi [1 ]
Sugiura, Kikuya [2 ]
Izawa, Takeshi [2 ]
Yamate, Jyoji [2 ]
Sakaguchi, Naoki [3 ]
Koiwai, Kazunori [3 ]
Mono, Kenji [1 ]
机构
[1] Osaka Prefecture Univ, Grad Sch Engn, Dept Appl Chem, Naka Ku, Sakai, Osaka 5998531, Japan
[2] Osaka Prefecture Univ, Grad Sch Life & Environm Sci, Div Vet Sci, Izumisano, Osaka 5988531, Japan
[3] Terumo Corp Ltd, Nakai, Kanagawa 2590151, Japan
关键词
pH-sensitive liposome; Lipoplex; Interferon-gamma; Cancer immunotherapy; Dendritic cell; Cellular immunity; MHC CLASS-I; ADENOVIRUS-MEDIATED DELIVERY; DENDRITIC CELLS; CYTOPLASMIC DELIVERY; IMMUNE-RESPONSES; VACCINE; NANOPARTICLES; ENDOCYTOSIS; EXPRESSION; GENERATION;
D O I
10.1016/j.biomaterials.2015.07.031
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
Potentiation of pH-sensitive liposome-based antigen carriers with IFN-gamma gene lipoplexes was attempted to achieve efficient induction of tumor-specific immunity. 3-Methylglutarylated poly(glycidol) (MGluPG)-modified liposomes and cationic liposomes were used, respectively, for the delivery of antigenic protein ovalbumin (OVA) and IFN-gamma-encoding plasmid DNA (pDNA). The MGluPG-modified liposomes and the cationic liposome-pDNA complexes (lipoplexes) formed hybrid complexes via electrostatic interactions after their mixing in aqueous solutions. The hybrid complexes co-delivered OVA and IFN-gamma-encoding pDNA into DC2.4 cells, a murine dendritic cell line, as was the case of MGluPG-modified liposomes for OVA or the lipoplexes for pDNA. Both the lipoplexes and the hybrid complexes transfected DC2A cells and induced IFN-gamma protein production, but transfection activities of the hybrid complexes were lower than those of the parent lipoplexes. Subcutaneous administration of hybrid complexes to mice bearing E.G7-OVA tumor reduced tumor volumes, which might result from the induction of OVA-specific cytotoxic T lymphocytes (CTLs). However, the hybrid complex-induced antitumor effect was the same level of the MGluPG-modified liposome-mediated antitumor immunity. In contrast, an extremely strong antitumor immune response was derived when these liposomes and lipoplexes without complexation were injected subcutaneously at the same site of tumor-bearing mice. Immunohistochemical analysis of tumor sections revealed that immunization through the liposome-lipoplex combination promoted the infiltration of CTLs to tumors at an early stage of treatment compared with liposomes, resulting in strong therapeutic effects. (C) 2015 Elsevier Ltd. All rights reserved.
引用
收藏
页码:214 / 224
页数:11
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