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Evaluation of the tumor targeting of a FAPα-based doxorubicin prodrug

前药 成纤维细胞活化蛋白 阿霉素 药理学 化学 靶向给药 体外 细胞毒性 药物输送 医学 药品 癌症研究 化疗 癌症 生物化学 内科学 有机化学
作者
Sichao Huang,Rui Fang,Jun Xu,Shenghong Qiu,Huan Zhang,Jun Du,Shaohui Cai
出处
期刊:Journal of Drug Targeting [Taylor & Francis]
卷期号:19 (7): 487-496 被引量:66
标识
DOI:10.3109/1061186x.2010.511225
摘要

Fibroblast activation protein-α (FAPα) is a tumor-associated antigen uniquely expressed by reactive stromal fibroblasts in the majority of human epithelial tumors. FAPα also possesses both post-prolyl peptidase and endopeptidase activities. Consequently, FAPα is increasingly considered as a potential pan-tumor target for designing tumor-targeted prodrugs. We previously conjugated Doxorubicin (Dox) with a FAPα-specific dipeptide (Z-Gly-Pro) to develop a FAPα-targeting prodrug of Dox (FTPD). The aim of current work was to validate the tumor targeting of this targeted-delivery strategy. The results demonstrated that FTPD could effectually release Dox upon the hydrolysis of FAPα as well as the incubation with tumor homogenate of FAPα-positive tumor (4T1 tumor), while it was highly stable in mouse plasma and a variety of tissue homogenates including heart, liver, and so on. And the FAPα-cleaved FTPD exhibited significantly higher cytotoxicity against 4T1 cells in vitro than the uncatalyzed prodrug. Additionally, FTPD produced similar antitumor efficacy in 4T1 tumor-bearing mice to free Dox without obvious cardiotoxic effect. Moreover, subsequent study indicated that the accumulation of FTPD reduced significantly in the heart compared to free Dox. These findings suggest that such FAPα-based prodrug strategy is promising to achieve targeted delivery of antitumor agents.
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