首页> 外文期刊>Journal of drug targeting >Single-chain Fv immunoliposomes for the targeting of fibroblast activation protein-expressing tumor stromal cells.
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Single-chain Fv immunoliposomes for the targeting of fibroblast activation protein-expressing tumor stromal cells.

机译:单链Fv免疫脂质体,用于靶向表达成纤维细胞活化蛋白的肿瘤基质细胞。

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摘要

Tumor stromal cells have gained increasing attention as possible target for cancer therapy. Fibroblast activation protein (FAP) represents a cell surface antigen selectively expressed by reactive tumor stromal fibroblasts of various cancers. Here, we describe anti-FAP immunoliposomes as carrier systems for active targeting of FAP-expressing cells. As targeting ligand we used single-chain Fv (scFv) molecules cross-reacting with human and mouse FAP. These scFv molecules were genetically modified to express an additional cysteine residue at the C-terminus allowing a defined and site-directed conjugation. Coupling to Mal-PEG(2000)-DSPE containing liposomes resulted in sterically stabilized scFv immunoliposomes showing strong and specific binding to FAP-expressing cells. These immunoliposomes were highly stable when incubated under physiological conditions (human plasma, 37 degrees C). In addition, we could show that binding to FAP-expressing cells leads to internalization of intact liposomes into the endosomal compartment. Thus, these anti-FAP scFv immunoliposomes should be suitable for target cell-specific delivery and uptake of encapsulated drugs.
机译:肿瘤基质细胞作为癌症治疗的可能靶点越来越受到关注。成纤维细胞活化蛋白(FAP)代表由各种癌症的反应性肿瘤基质成纤维细胞选择性表达的细胞表面抗原。在这里,我们将抗FAP免疫脂质体描述为主动靶向表达FAP的细胞的载体系统。作为靶向配体,我们使用了与人和小鼠FAP交叉反应的单链Fv(scFv)分子。对这些scFv分子进行了基因修饰,使其在C末端表达了一个额外的半胱氨酸残基,从而实现了确定的定点结合。与含有Mal-PEG(2000)-DSPE的脂质体偶联导致空间稳定的scFv免疫脂质体显示出与FAP表达细胞的强特异性结合。这些免疫脂质体在生理条件(人血浆,37摄氏度)下孵育时高度稳定。此外,我们可以证明与表达FAP的细胞结合会导致完整脂质体内化进入内体区室。因此,这些抗FAP scFv免疫脂质体应适合靶细胞特异性递送和摄取包封的药物。

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