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级联放大自焚聚合物前药通过破坏氧化还原稳态治疗癌症。

Cascade-amplified self-immolative polymeric prodrug for cancer therapy by disrupting redox homeostasis.

机构信息

School of Chemical Engineering, College of Engineering, Sungkyunkwan University (SKKU), Suwon 16419, Republic of Korea.

School of Chemical Engineering, College of Engineering, Sungkyunkwan University (SKKU), Suwon 16419, Republic of Korea; College of Life Sciences and Health, Wuhan University of Science and Technology (WUST), Wuhan 430065, China.

出版信息

J Control Release. 2023 Jun;358:555-565. doi: 10.1016/j.jconrel.2023.05.015. Epub 2023 May 17.

DOI:10.1016/j.jconrel.2023.05.015
PMID:37182804
Abstract

The amplification of reactive oxygen species (ROS) generation and glutathione (GSH) depletion in cancer cells represents a promising strategy to disrupt redox homeostasis for cancer therapy. Quinone methide and its analogs (QM) have recently been recognized as potential GSH scavengers for anticancer applications; however, an effective QM prodrug is yet to be developed. In this study, we prepare a self-immolative polymeric prodrug (SPP), which could be selectively degraded to generate large quantities of QMs in cancer cells during the spontaneous stepwise head-to-tail degradation of SPP. The amphiphilic SPP is self-assembled into nano-sized micelles, allowing for encapsulating 2-methoxy-β-estradiol (2ME), an anticancer drug that produces a large amount of intracellular ROS. When SPP@2ME, as the cascade-amplified prodrug, is treated on the cancer cells, 2ME is rapidly released at the ROS-rich intracellular environment by degradation of SPP, thus generating more ROS that triggers the degradation of more SPP chains. Such a domino-like cascade-amplified feedback loop significantly amplifies oxidative stress and disrupts the redox homeostasis in cancer cells. This unique strategy provides synergistic anticancer therapeutic efficacy and demonstrates an important perception in innovative and precise nanomedicine.

摘要

活性氧(ROS)生成和谷胱甘肽(GSH)耗竭的扩增代表了破坏癌症治疗中氧化还原平衡的一种很有前途的策略。醌甲醚及其类似物(QM)最近被认为是用于抗癌应用的潜在 GSH 清除剂;然而,有效的 QM 前药尚未开发。在这项研究中,我们制备了一种自耗性聚合前药(SPP),它可以在 SPP 的自发逐步头尾降解过程中在癌细胞中选择性地降解,产生大量的 QM。两亲性 SPP 自组装成纳米尺寸的胶束,允许封装 2-甲氧基-β-雌二醇(2ME),一种产生大量细胞内 ROS 的抗癌药物。当 SPP@2ME(作为级联放大前药)用于癌细胞时,由于 SPP 的降解,2ME 在富含 ROS 的细胞内环境中迅速释放,从而产生更多的 ROS,触发更多的 SPP 链降解。这种类似多米诺骨牌的级联放大反馈环显著增强了氧化应激并破坏了癌细胞中的氧化还原平衡。这种独特的策略提供了协同的抗癌治疗效果,并在创新和精确的纳米医学中展示了重要的认识。

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