多价色聚体纳米药物共轭物通过铜超载和谷胱甘肽耗竭实现高效的肿瘤杯突疗法

IF 14.4 1区 化学 Q1 CHEMISTRY, MULTIDISCIPLINARY
Shuang Wang, Xueliang Liu, Dali Wei, Huayuan Zhou, Jiawei Zhu, Qing Yu, Lei Luo, Xinfeng Dai, Yiting Jiang, Lu Yu, Yu Yang* and Weihong Tan*, 
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引用次数: 0

摘要

铜中毒是最近发现的一种铜依赖性细胞死亡形式,具有良好的肿瘤抑制作用,且耐药性极低。然而,由于其对铜离子和肿瘤中富含谷胱甘肽(GSH)的微环境的依赖性,其疗效受到了阻碍。在此,我们开发了具有核糖体样结构的多价适配体纳米药物共轭物(称为 CuPEs@PApt),利用线粒体铜超载和谷胱甘肽耗竭改善肿瘤杯突疗法。多价aptamer(PApt)由用于肿瘤靶向的多价上皮细胞粘附分子aptamer和用于铜螯合的重复PolyT序列组成,可促进过氧化铜-伊利克莫尔纳米点(CuPEs)的高效装载和靶向递送。CuPEs@PApt被肿瘤细胞内化后,释放出的Elesclomol会在线粒体中积聚铜离子,启动铜中毒,而CuP纳米点的溶酶体降解会产生外源Cu2+和H2O2,引发类似芬顿反应的GSH耗竭,从而加强铜中毒。体外和体内实验证实了这一策略在诱导肿瘤细胞杯突和免疫性细胞死亡方面的功效,后者有助于激活抗肿瘤免疫反应,从而协同抑制肿瘤生长。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Polyvalent Aptamer Nanodrug Conjugates Enable Efficient Tumor Cuproptosis Therapy Through Copper Overload and Glutathione Depletion

Polyvalent Aptamer Nanodrug Conjugates Enable Efficient Tumor Cuproptosis Therapy Through Copper Overload and Glutathione Depletion

Cuproptosis, a recently identified form of copper-dependent cell death, shows promising tumor suppressive effects with minimal drug resistance. However, its therapeutic efficacy is hampered by its dependence on copper ions and the glutathione (GSH)-rich microenvironment in tumors. Here, we have developed polyvalent aptamer nanodrug conjugates (termed CuPEs@PApt) with a nucleosome-like structure to improve tumor cuproptosis therapy by exploiting mitochondrial copper overload and GSH depletion. Polyvalent aptamer (PApt), comprising polyvalent epithelial cell adhesion molecule aptamers for tumor targeting and repetitive PolyT sequences for copper chelation, facilitates efficient loading and targeted delivery of copper peroxide-Elesclomol nanodots (CuPEs). Upon internalization by tumor cells, Elesclomol released from CuPEs@PApt accumulates copper ions in mitochondria to initiate cuproptosis, while lysosomal degradation of CuP nanodots generates exogenous Cu2+ and H2O2, triggering a Fenton-like reaction for GSH depletion to enhance cuproptosis. In vitro and in vivo experiments confirm the efficacy of this strategy in inducing tumor cell cuproptosis and immunogenic cell death, the latter contributing to the activation of the antitumor immune response for synergistic tumor growth inhibition.

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来源期刊
CiteScore
24.40
自引率
6.00%
发文量
2398
审稿时长
1.6 months
期刊介绍: The flagship journal of the American Chemical Society, known as the Journal of the American Chemical Society (JACS), has been a prestigious publication since its establishment in 1879. It holds a preeminent position in the field of chemistry and related interdisciplinary sciences. JACS is committed to disseminating cutting-edge research papers, covering a wide range of topics, and encompasses approximately 19,000 pages of Articles, Communications, and Perspectives annually. With a weekly publication frequency, JACS plays a vital role in advancing the field of chemistry by providing essential research.
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