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一种由 pH 敏感邻酯-达沙替尼偶联物组成的小分子纳米药物,用于癌症治疗。

A small molecule nanodrug consisting of pH-sensitive ortho ester-dasatinib conjugate for cancer therapy.

机构信息

Engineering Research Center for Biomedical Materials, School of Life Science, Anhui University, 111 Jiulong Road, Hefei, Anhui Province 230601, PR China.

Engineering Research Center for Biomedical Materials, School of Life Science, Anhui University, 111 Jiulong Road, Hefei, Anhui Province 230601, PR China.

出版信息

Eur J Pharm Biopharm. 2021 Jun;163:188-197. doi: 10.1016/j.ejpb.2021.04.008. Epub 2021 Apr 14.

DOI:10.1016/j.ejpb.2021.04.008
PMID:33864903
Abstract

The main objective of this paper is to develop a self-delivered prodrug system with nanoscale characteristics to enhance the efficacy of tumor therapy. The pH-sensitive prodrug was composed of ortho ester-linked dasatinib (DAS-OE), which was further self-assembled with or without doxorubicin (DOX) to obtain two carrier-free nanoparticles (DOX/DAS-OE NPs or DAS-OE NPs). The prodrug-based nanoparticles united the superiorities of small molecules and nano-assemblies together and displayed well-defined structure, uniform spherical shape, high drug loading ratio and on-demand drug release behavior. The drug loading content of DAS and DOX was 61.6% and 21.9%, respectively, and more than 80.2% of DAS and 60.2% DOX were released from DOX/DAS-OE NPs within 20 h at pH 5.0. Both in vitro and in vivo studies demonstrated that the pH-sensitive ortho ester bonds in the prodrug underwent hydrolysis to release DAS and DOX simultaneously after cellular internalization, resulting in remarkable antitumor effect. Tumor growth inhibition rate was 19.9% (free DAS), 35.5% (free DOX), 66.3% (DAS-OE NPs) and 82.8% (DOX/DAS-OE NPs), respectively. Thus, the ortho ester-linked prodrug system shows great potentials in cancer therapy.

摘要

本文的主要目的是开发一种具有纳米特性的自递药系统,以提高肿瘤治疗的疗效。该 pH 敏感前药由邻酯键连接的达沙替尼(DAS-OE)组成,进一步与或不与阿霉素(DOX)自组装,得到两种无载体纳米颗粒(DOX/DAS-OE NPs 或 DAS-OE NPs)。基于前药的纳米颗粒结合了小分子和纳米组装体的优势,具有明确的结构、均匀的球形、高载药率和按需药物释放行为。DAS 和 DOX 的载药量分别为 61.6%和 21.9%,在 pH 5.0 下,超过 80.2%的 DAS 和 60.2%的 DOX 在 20 小时内从 DOX/DAS-OE NPs 中释放出来。体外和体内研究均表明,前药中的 pH 敏感邻酯键在细胞内化后发生水解,同时释放 DAS 和 DOX,从而产生显著的抗肿瘤作用。肿瘤生长抑制率分别为 19.9%(游离 DAS)、35.5%(游离 DOX)、66.3%(DAS-OE NPs)和 82.8%(DOX/DAS-OE NPs)。因此,邻酯键连接的前药系统在癌症治疗中具有很大的潜力。

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