Fluorous-tagged bortezomib supramolecular nanomedicine for cancer therapy

Changping Wang , Xin Gao , Zhan Li , Xinyu Wang , Yiwen Li , Yiyun Cheng
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Abstract

Lipidation is a well-established post-translational modification strategy to modulate the structure and function of proteins and peptides. Lipids can improve the overall or local hydrophobicity of the biomolecule, boosting its affinity with the cell membranes. Lipidation, despite its great potential, remains an underutilized technique for translating bioactive molecules into the clinic. Herein, we have optimized the lipidation strategy by involving the fluorous lipidation combined with supramolecular engineering, which can be facilely achieved by grafting an anticancer peptide drug (bortezomib, BTZ) with a series of fluorous lipids bearing a catechol moiety via the dynamic catechol-boronate ester bond. Compared with BTZ, the fluorous-tagged BTZ nanomedicine exhibited an on-demand and traceless release behavior, and enhanced therapeutic effect and biocompatibility. More importantly, the fluorous tag could improve the serum stability of the supramolecular nanomedicine, which allowed efficient in vivo utilization of BTZ to kill cancer cells. This work introduces a novel lipidation strategy for bioactive peptides via the integration of fluorination chemistry and supramolecular engineering strategies.
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用于癌症治疗的氟标记硼替佐米超分子纳米药物
脂化是一种完善的翻译后修饰策略,用于调节蛋白质和肽的结构和功能。脂质可以改善生物分子的整体或局部疏水性,增强其与细胞膜的亲和力。脂化,尽管具有巨大的潜力,仍然是一种未充分利用的技术,将生物活性分子转化为临床。本研究将氟脂化与超分子工程相结合,优化了脂化策略,通过动态儿茶酚-硼酸酯键,将抗癌肽药物硼替佐米(BTZ)与一系列含儿茶酚基团的氟脂质接枝,可以很容易地实现脂化。与BTZ相比,荧光标记的BTZ纳米药物表现出随需释放和无迹释放的行为,并增强了治疗效果和生物相容性。更重要的是,含氟标签可以提高超分子纳米药物的血清稳定性,从而有效地利用BTZ在体内杀死癌细胞。本工作通过氟化化学和超分子工程策略的整合,介绍了一种新的生物活性肽脂化策略。
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