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Drug content on anticancer efficacy of self-assembling ketal-linked dextran-paclitaxel conjugates

紫杉醇 前药 药理学 药品 化学 药代动力学 右旋糖酐 结合 药物输送 细胞毒性 体内分布 生物制药 靶向给药 癌症 体外 医学 生物化学 生物活性 有机化学 内科学 生药学 数学分析 数学
作者
Tiantian Guo,Haiping Zhong,Xingwei Li,Jingqing Mu,Tao Liu,Na Yu,Yang Zhao,Xing‐Jie Liang,Shutao Guo
出处
期刊:Journal of Controlled Release [Elsevier]
卷期号:359: 175-187 被引量:7
标识
DOI:10.1016/j.jconrel.2023.05.045
摘要

Although polymer-drug conjugates (PDCs) show great promise as versatile drug delivery systems, no antitumor PDCs based on small-molecule drugs are currently on the market, partly because of the lack of validated design principles for PDCs. High drug content is thought to be essential for devising highly efficacious PDCs based on poorly soluble antitumor drugs, but this has not been well validated. Therefore, revisiting the relationship between drug content and PDC performance is vital. In this study, we synthesized four dextran-paclitaxel (PTX) conjugates (designated as DKPs) with different drug contents by linking dextran and PTX via an acid-responsive ketal, and we used the conjugates to construct self-assembled DKP nanoparticles (NPs) for antitumor therapy. We focused on how PTX content influenced the hydrolysis kinetics, cytotoxicity, cellular uptake and intracellular hydrolysis, pharmacokinetics, biodistribution, and antitumor efficacies of the DKP NPs. We found that DKP NPs with lower PTX content showed accelerated drug release and increased tumor accumulation, and consequently enhanced antitumor efficacy. In 4T1-Luc and Panc02-Luc cancer models, the NPs showed considerably improved therapeutic efficacy than the micellar formulation of PTX that is currently in clinical use. Our results indicate that DKP NPs with lower PTX content possess greater antitumor potential, and our findings offer new insights for the connection of drug content-formulation-bioactivity relationship in the rational design of PDC prodrugs.

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