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Self-Assembled Redox Dual-Responsive Prodrug-Nanosystem Formed by Single Thioether-Bridged Paclitaxel-Fatty Acid Conjugate for Cancer Chemotherapy

机译:由硫醚桥联的紫杉醇-脂肪酸共轭物形成的自组装氧化还原双反应前药-纳米系统用于癌症化学治疗。

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摘要

Chemotherapeutic efficacy can be greatly improved by developing nanoparticulate drug delivery systems (nano-DDS) with high drug loading capacity and smart stimulus-triggered drug release in tumor cells. Herein, we report a novel redox dual-responsive prodrug-nanosystem self-assembled by hydrophobic small-molecule conjugates of paclitaxel (PTX) and oleic acid (OA). Thioether linked conjugates (PTX-S-OA) and dithioether inserted conjugates (PTX-2S-OA) are designed to respond to the redox-heterogeneity in tumor. Dithioether has been reported to show redox dual-responsiveness, but we find that PTX-S-OA exhibits superior redox sensitivity over PTX-2S-OA, achieving more rapid and selective release of free PTX from the prodrug nanoassemblies triggered by redox stimuli. PEGylated PTX-S-OA nanoassemblies, with impressively high drug loading (57.4%), exhibit potent antitumor activity in a human epidermoid carcinoma xenograft. This novel prodrug-nanosystem addresses concerns related to the low drug loading and inefficient drug release from hydrophobic prodrugs of PTX, and provides possibilities for the development of redox dual-sensitive conjugates or polymers for efficient anticancer drug delivery.
机译:通过开发具有高载药量和在肿瘤细胞中智能刺激触发的药物释放的纳米颗粒药物释放系统(nano-DDS),可以大大提高化学疗法的疗效。在这里,我们报道了紫杉醇(PTX)和油酸(OA)的疏水小分子共轭物自组装的新型氧化还原双反应前药-纳米系统。硫醚连接的偶联物(PTX-S-OA)和二硫醚插入的偶联物(PTX-2S-OA)设计用于响应肿瘤中的氧化还原异质性。据报道,二硫醚显示出氧化还原双重反应性,但我们发现PTX-S-OA表现出优于PTX-2S-OA的氧化还原敏感性,实现了由氧化还原刺激触发的前药纳米组件中更快,更选择性地释放游离PTX。具有令人惊讶的高载药量(57.4%)的PEG化PTX-S-OA纳米组件在人表皮样癌异种移植物中表现出强大的抗肿瘤活性。这种新颖的前药-纳米系统解决了与低载药量和从PTX疏水性前药中释放低效药物有关的问题,并为开发用于有效抗癌药物递送的氧化还原双重敏感偶联物或聚合物提供了可能性。

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