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自组装卟啉作为协同癌症治疗的单一治疗剂:一石三鸟策略

Self-Assembling Porphyrins as a Single Therapeutic Agent for Synergistic Cancer Therapy: A One Stone Three Birds Strategy.

作者信息

Chen Jun, Chen Feng, Zhang Lei, Yang Zhangyou, Deng Tao, Zhao Yunfei, Zheng Tianye, Gan Xuelan, Zhong Hangtian, Geng Yanqing, Fu Xinwei, Wang Yuanqiang, Yu Chao

机构信息

Pharmaceutical Engineering Research Center, College of Pharmacy, Chongqing Medical University, Chongqing 400000, China.

Joint International Research Laboratory of Reproduction and Development, School of Public Health, Chongqing Medical University, Chongqing 400000, China.

出版信息

ACS Appl Mater Interfaces. 2021 Jun 23;13(24):27856-27867. doi: 10.1021/acsami.1c04868. Epub 2021 Jun 10.

Abstract

Combining photodynamic therapy (PDT), chemodynamic therapy (CDT), and ferroptosis is a valuable means for an enhanced anticancer effect. However, traditional combination of PDT/CDT/ferroptosis faces several hurdles, including excess glutathione (GSH) neutralization and preparation complexity. In this work, a versatile multifunctional nanoparticle (HCNP) self-assembled from two porphyrin molecules, chlorin e6 and hemin, is developed. The as-constructed HCNPs exhibit a peroxidase-mimic catalytic activity, which can lead to the in situ generation of endogenous O, thereby enhancing the efficacy of PDT. Furthermore, the generation of hydroxyl radicals (OH) in the tumor environment in reaction to the high level of HO and the simultaneous disruption of intracellular GSH endow the HCNPs with the capacity of enhanced CDT, resulting in a more effective therapeutic outcome in combination with PDT. More importantly, GSH depletion further leads to the inactivation of GSH peroxide 4 and induced ferroptosis. Both in vitro and in vivo results showed that the combination of PDT/CDT/ferroptosis realizes highest antitumor efficacy significantly under laser irradiation. Therefore, by integrating the superiorities of O and OH generation capacity, GSH-depletion effect, and bioimaging into a single nanosystem, the HCNPs are a promising single therapeutic agent for tumor PDT/CDT/ferroptosis combination therapy.

摘要

将光动力疗法(PDT)、化学动力疗法(CDT)和铁死亡相结合是增强抗癌效果的一种有效手段。然而,传统的PDT/CDT/铁死亡联合疗法面临着诸多障碍,包括过量谷胱甘肽(GSH)的中和以及制备复杂性。在这项工作中,开发了一种由两种卟啉分子(叶绿素e6和血红素)自组装而成的多功能纳米颗粒(HCNP)。所构建的HCNPs表现出类似过氧化物酶的催化活性,可导致内源性O的原位生成,从而提高PDT的疗效。此外,在肿瘤环境中,由于高水平的HO反应生成羟基自由基(OH)以及同时破坏细胞内GSH,赋予了HCNPs增强的CDT能力,与PDT联合使用时产生更有效的治疗效果。更重要的是,GSH的消耗进一步导致谷胱甘肽过氧化物酶4失活并诱导铁死亡。体外和体内结果均表明,PDT/CDT/铁死亡联合疗法在激光照射下能显著实现最高的抗肿瘤疗效。因此,通过将生成O和OH的能力、GSH消耗效应以及生物成像的优势整合到单个纳米系统中,HCNPs是一种用于肿瘤PDT/CDT/铁死亡联合治疗的有前景的单一治疗剂。

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