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活性氧物种调节在当前的癌症治疗领域。

Reactive Oxygen Species Modulation in the Current Landscape of Anticancer Therapies.

机构信息

Guy's and St Thomas' NHS Foundation Trust, London, United Kingdom.

Tan Tock Seng Hospital, Singapore, Singapore.

出版信息

Antioxid Redox Signal. 2024 Aug;41(4-6):322-341. doi: 10.1089/ars.2023.0445. Epub 2024 Apr 1.

Abstract

Reactive oxygen species (ROS) are generated during mitochondrial oxidative metabolism, and are tightly controlled through homeostatic mechanisms to maintain intracellular redox, regulating growth and proliferation in healthy cells. However, ROS production is perturbed in cancers where abnormal accumulation of ROS leads to oxidative stress and genomic instability, triggering oncogenic signaling pathways on one hand, while increasing oxidative damage and triggering ROS-dependent death signaling on the other. Our review illuminates how critical interactions between ROS and oncogenic signaling, the tumor microenvironment, and DNA damage response (DDR) pathways have led to interest in ROS modulation as a means of enhancing existing anticancer strategies and developing new therapeutic opportunities. ROS equilibrium exists a delicate balance of pro-oxidant and antioxidant species within cells. "Antioxidant" approaches have been explored mainly in the form of chemoprevention, but there is insufficient evidence to advocate its routine application. More progress has been made the "pro-oxidant" approach of targeting cancer vulnerabilities and inducing oxidative stress. Various therapeutic modalities have employed this approach, including direct ROS-inducing agents, chemotherapy, targeted therapies, DDR therapies, radiotherapy, and immunotherapy. Finally, emerging delivery systems such as "nanosensitizers" as radiotherapy enhancers are currently in development. While approaches designed to induce ROS have shown considerable promise in selectively targeting cancer cells and dealing with resistance to conventional therapies, most are still in early phases of development and challenges remain. Further research should endeavor to refine treatment strategies, optimize drug combinations, and identify predictive biomarkers of ROS-based cancer therapies.

摘要

活性氧 (ROS) 在线粒体氧化代谢过程中产生,并通过体内平衡机制进行严格控制,以维持细胞内的氧化还原状态,调节健康细胞的生长和增殖。然而,在癌症中,ROS 的产生受到干扰,ROS 的异常积累导致氧化应激和基因组不稳定性,一方面触发致癌信号通路,另一方面增加氧化损伤并触发 ROS 依赖性死亡信号。我们的综述阐明了 ROS 与致癌信号、肿瘤微环境和 DNA 损伤反应 (DDR) 途径之间的关键相互作用如何导致人们对 ROS 调节产生兴趣,作为增强现有抗癌策略和开发新治疗机会的一种手段。ROS 平衡存在于细胞内氧化剂和抗氧化剂之间的一种微妙平衡。“抗氧化”方法主要以化学预防的形式进行探索,但没有足够的证据支持其常规应用。在靶向癌症脆弱性和诱导氧化应激的“促氧化剂”方法方面取得了更多进展。各种治疗方式都采用了这种方法,包括直接 ROS 诱导剂、化疗、靶向治疗、DDR 治疗、放疗和免疫治疗。最后,新兴的输送系统,如作为放疗增强剂的“纳米敏化剂”,目前正在开发中。虽然旨在诱导 ROS 的方法在选择性靶向癌细胞和应对对常规疗法的耐药性方面显示出了相当大的前景,但大多数方法仍处于早期开发阶段,仍然存在挑战。进一步的研究应该努力完善治疗策略、优化药物组合,并确定基于 ROS 的癌症治疗的预测性生物标志物。

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