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基于纳米医学的活性氧生成与铜代谢的协同调控用于声动力增强肿瘤治疗

Nanomedicine-enabled concurrent regulations of ROS generation and copper metabolism for sonodynamic-amplified tumor therapy.

作者信息

Bing Jinhong, Zhou Bangguo, Chen Minqi, Shen Yucui, Zhou Min, Lin Han, Wu Wencheng, Shi Jianlin

机构信息

State Key Laboratory of High-performance Ceramics and Superfine Microstructure, Shanghai Institute of Ceramics, Chinese Academy of Sciences, Nanocatalytic Medicine in Specific Therapy for Serious Disease, Chinese Academy of Medical Sciences (2021RU012), Shanghai, 200050, PR China.

Department of Radiology, The First Affiliated Hospital, College of Medicine, Zhejiang University, Hangzhou, 310003, Zhejiang, PR China.

出版信息

Biomaterials. 2025 Jul;318:123137. doi: 10.1016/j.biomaterials.2025.123137. Epub 2025 Jan 27.

Abstract

Sonodynamic therapy (SDT) shows substantial potentials in cancer treatment thanks to the deep tissue penetration of ultrasound. However, its clinical translation suffers from the potential damages to healthy tissues and the resistance of tumors, particularly from cancer stem-like cells (CSCs), to the ultrasound. To address these challenges, we designed a novel glutathione (GSH)-activated nanomedicine to simultaneously enhance the safety and efficacy of SDT by in situ regulating the generation of reactive oxygen species (ROS) and copper metabolism. This nanomedicine, Es@CuTCPP, was created by loading elesclomol (Es) onto CuTCPP nanosheets. By accumulating this nanomedicine in tumors, the Cu(II)-TCPP is reduced to the highly sonosensitive Cu(I)-TCPP by the intra-tumoral-overexpressed GSH, leading to the production of abundant ROS upon ultrasound exposure, which effectively kills large amounts of tumor cells. Concurrently, the released copper ions react with co-released Es to form a CuEs complex, which induces cuproptosis of CSCs surviving the ROS attack by disrupting cellular copper metabolism, evidently amplifying the effectiveness of SDT. This work presents the first paradigm of a GSH-activated and cuproptosis-enhanced SDT approach, offering a promising novel strategy for cancer therapy.

摘要

由于超声具有深层组织穿透性,声动力疗法(SDT)在癌症治疗中显示出巨大潜力。然而,其临床转化面临着对健康组织的潜在损害以及肿瘤尤其是癌症干细胞样细胞(CSCs)对超声的抗性。为应对这些挑战,我们设计了一种新型的谷胱甘肽(GSH)激活的纳米药物,通过原位调节活性氧(ROS)的生成和铜代谢,同时提高SDT的安全性和疗效。这种纳米药物Es@CuTCPP是通过将艾立摩尔(Es)负载到CuTCPP纳米片上制备而成。通过使这种纳米药物在肿瘤中蓄积,肿瘤内高表达的GSH将Cu(II)-TCPP还原为高超声敏性的Cu(I)-TCPP,导致在超声照射时产生大量ROS,从而有效杀死大量肿瘤细胞。同时,释放的铜离子与共同释放的Es反应形成CuEs复合物,该复合物通过破坏细胞铜代谢诱导在ROS攻击下存活的CSCs发生铜死亡,明显增强了SDT的效果。这项工作提出了一种GSH激活和铜死亡增强的SDT方法的首个范例,为癌症治疗提供了一种有前景的新策略。

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