Neo-mannosylated liposomes have been prepared by coupling a mannose derivative bearing a hydrophilic spacer arm to preformed large unilamellar liposomes containing 4-(p-maleimidophenyl) butyryl-phosphatidylethanolamine. Lipopolysaccharide (LPS) was encapsulated in normal or neo-mannosylated liposomes; the neo-mannosylated vesicles showed specificity for the in vitro activation to toxicity of macrophages only in the case of differentiated macrophages presenting mannose receptors at their surface. In vivo, LPS entrapped in neo-mannosylated vesicles showed a reduced toxicity for animals hypersensitive to LPS. Moreover targeting of LPS to tissue macrophages with neo-mannosylated liposomes induced regression of experimental solid tumors in mice (EMT6 sarcoma, 3LL carcinoma) and was effective on lung metastases.

译文

:新-甘露糖基化的脂质体是通过将带有亲水间隔臂的甘露糖衍生物偶联到预先形成的含有4-(对-马来酰亚胺基苯基)丁酰基-磷脂酰乙醇胺的大单层脂质体上而制备的。脂多糖(LPS)封装在正常或新甘露糖基化的脂质体中;仅在分化的巨噬细胞在其表面呈现甘露糖受体的情况下,新甘露糖基化的囊泡才显示出对巨噬细胞毒性的体外活化的特异性。在体内,包裹在新甘露糖基化囊泡中的LPS对LPS过敏的动物显示出降低的毒性。此外,用新甘露糖基化脂质体将LPS靶向组织巨噬细胞可诱导小鼠实验性实体瘤的消退(EMT6肉瘤,3LL癌),并且对肺转移有效。

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