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双层中空介孔氧化亚铜纳米粒子用于肿瘤的双重药物序贯治疗。

Double-Layered Hollow Mesoporous Cuprous Oxide Nanoparticles for Double Drug Sequential Therapy of Tumors.

机构信息

School of Biomedical Engineering, Southern Medical University, 1023 Shatai South Road, Baiyun, Guangzhou, Guangdong, 510515, China.

Medical Imaging Center, Nanfang Hospital, Southern Medical University, 1023 Shatai South Road, Baiyun, Guangzhou, Guangdong, 510515, China.

出版信息

Adv Mater. 2024 Jul;36(28):e2313212. doi: 10.1002/adma.202313212. Epub 2024 May 6.

DOI:10.1002/adma.202313212
PMID:38670140
Abstract

Cancer stem cells (CSCs) are one of the determinants of tumor heterogeneity and are characterized by self-renewal, high tumorigenicity, invasiveness, and resistance to various therapies. To overcome the resistance of traditional tumor therapies resulting from CSCs, a strategy of double drug sequential therapy (DDST) for CSC-enriched tumors is proposed in this study and is realized utilizing the developed double-layered hollow mesoporous cuprous oxide nanoparticles (DL-HMCONs). The high drug-loading contents of camptothecin (CPT) and all-trans retinoic acid (ATRA) demonstrate that the DL-HMCON can be used as a generic drug delivery system. ATRA and CPT can be sequentially loaded in and released from CPT3@ATRA3@DL-HMCON@HA. The DDST mechanisms of CPT3@ATRA3@DL-HMCON@HA for CSC-containing tumors are demonstrated as follows: 1) the first release of ATRA from the outer layer induces differentiation from CSCs with high drug resistance to non-CSCs with low drug resistance; 2) the second release of CPT from the inner layer causes apoptosis of non-CSCs; and 3) the third release of Cu from DL-HMCON itself triggers the Fenton-like reaction and glutathione depletion, resulting in ferroptosis of non-CSCs. This CPT3@ATRA3@DL-HMCON@HA is verified to possess high DDST efficacy for CSC-enriched tumors with high biosafety.

摘要

癌症干细胞(CSCs)是肿瘤异质性的决定因素之一,其特征是自我更新、高致瘤性、侵袭性和对各种治疗的耐药性。为了克服 CSCs 导致的传统肿瘤治疗耐药性,本研究提出了针对富含 CSC 肿瘤的双重药物序贯治疗(DDST)策略,并利用所开发的双层中空介孔氧化亚铜纳米粒子(DL-HMCON)来实现这一策略。喜树碱(CPT)和全反式维甲酸(ATRA)的高载药含量表明,DL-HMCON 可用作通用药物递送系统。ATRA 和 CPT 可以顺序装载和释放到 CPT3@ATRA3@DL-HMCON@HA 中。CPT3@ATRA3@DL-HMCON@HA 对富含 CSC 肿瘤的 DDST 机制如下:1)外层的 ATRA 首次释放诱导高耐药性 CSCs 向低耐药性非 CSCs 分化;2)内层的 CPT 第二次释放导致非 CSCs 凋亡;3)DL-HMCON 自身释放的 Cu 引发芬顿样反应和谷胱甘肽耗竭,导致非 CSCs 发生铁死亡。CPT3@ATRA3@DL-HMCON@HA 被证实对富含 CSC 的肿瘤具有高效的 DDST 作用,且具有较高的生物安全性。

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