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In vitro studies on CNGRC-CPG2 fusion proteins for ligand-directed enzyme prodrug therapy for targeted cancer therapy

机译:CNGRC-CPG2融合蛋白在配体指导的酶前药治疗中的靶向性癌症治疗的体外研究

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摘要

The sequence asparagine-glycine arginine (NGR), flanked by Cysteine (Cys) residues so as to form a disulfide-bridge (CNGRC), has previously been found to target and bind specifically to aminopeptidase N (APN), which is highly expressed on the surface of tumor cells. The goal of this study was to develop and evaluate the potential of fusion proteins carrying the CNGRC sequence linked to the enzyme carboxypeptidase G2 (CPG2) for targeted cancer therapy. We refer to this strategy as ligand-directed enzyme prodrug therapy (LDEPT).
机译:先前发现半胱氨酸(Cys)残基侧翼以形成二硫键(CNGRC)的天冬酰胺-甘氨酸精氨酸(NGR)序列靶向并与氨基肽酶N(APN)特异性结合,在肿瘤细胞的表面。这项研究的目的是开发和评估融合蛋白的潜力,该融合蛋白带有连接至羧肽酶G2(CPG2)的CNGRC序列,可用于靶向癌症治疗。我们将这种策略称为配体指导的酶前药治疗(LDEPT)。

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