Folate Conjugated Polyethylene Glycol Probe for Tumor-Targeted Drug Delivery of 5-Fluorouracil

叶酸受体 前药 赫拉 结合 化学 聚乙二醇 药物输送 细胞毒性 药理学 PEG比率 药品 体外 靶向给药 体内 生物化学 癌细胞 癌症 医学 生物 内科学 有机化学 数学分析 数学 生物技术 财务 经济
作者
Shabnam Sarwar,Muhammad Abdul Qadir,Rima D. Alharthy,Mahmood Ahmed,Saghir Ahmad,Michiel Vanmeert,Muhammad Usman Mirza,Abdul Hameed
出处
期刊:Molecules [Multidisciplinary Digital Publishing Institute]
卷期号:27 (6): 1780-1780 被引量:15
标识
DOI:10.3390/molecules27061780
摘要

A targeted delivery system is primarily intended to carry a potent anticancer drug to specific tumor sites within the bodily tissues. In the present study, a carrier system has been designed using folic acid (FA), bis-amine polyethylene glycol (PEG), and an anticancer drug, 5-fluorouracil (5-FU). FA and PEG were joined via an amide bond, and the resulting FA-PEG-NH2 was coupled to 5-FU producing folate-polyethylene glycol conjugated 5-fluorouracil (FA-PEG-5-FU). Spectroscopic techniques (UV-Vis, 1HNMR, FTIR, and HPLC) were used for the characterization of products. Prodrug (FA-PEG-5-FU) was analyzed for drug release profile (in vitro) up to 10 days and compared to a standard anticancer drug (5-FU). Folate conjugate was also analyzed to study its folate receptors (FR) mediated transport and in vitro cytotoxicity assays using HeLa cancer cells/Vero cells, respectively, and antitumor activity in tumor-bearing mice models. Folate conjugate showed steady drug release patterns and improved uptake in the HeLa cancer cells than Vero cells. Folate conjugate treated mice group showed smaller tumor volumes; specifically after the 15th day post-treatment, tumor sizes were decreased significantly compared to the standard drug group (5-FU). Molecular docking findings demonstrated importance of Trp138, Trp140, and Lys136 in the stabilization of flexible loop flanking the active site. The folic acid conjugated probe has shown the potential of targeted drug delivery and sustained release of anticancer drug to tumor lesions with intact antitumor efficacy.
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