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The Double-Faced Role of Nitric Oxide and Reactive Oxygen Species in Solid Tumors

机译:一氧化氮和活性氧在实体瘤中的双重作用

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摘要

Disturbed redox homeostasis represents a hallmark of cancer phenotypes, affecting cellular metabolism and redox signaling. Since reactive oxygen and nitrogen species (ROS/RNS) are involved in regulation of proliferation and apoptosis, they may play a double-faced role in cancer, entailing protumorigenic and tumor-suppressing effects in early and later stages, respectively. In addition, ROS and RNS impact the activity and communication of all tumor constituents, mediating their reprogramming from anti- to protumorigenic phenotypes, and vice versa. An important role in this dichotomic action is played by the variable amounts of O in the tumor microenvironment, which dictates the ultimate outcome of the influence of ROS/RNS on carcinogenesis. Moreover, ROS/RNS levels remarkably influence the cancer response to therapy. The relevance of ROS/RNS signaling in solid tumors is witnessed by the emergence of novel targeted treatments of solid tumors with compounds that target ROS/RNS action and production, such as tyrosine kinase inhibitors and monoclonal antibodies, which might contribute to the complexity of redox regulation in cancer. Prospectively, the dual role of ROS/RNS in the different stages of tumorigenesis through different impact on oxidation and nitrosylation may also allow development of tailored diagnostic and therapeutic approaches.
机译:干扰的氧化还原稳态代表了癌症表型的标志,影响细胞代谢和氧化还原信号。由于活性氧和活性氮(ROS / RNS)参与增殖和凋亡的调节,它们可能在癌症中起双重作用,分别在早期和晚期引起致瘤和抑制肿瘤的作用。另外,ROS和RNS影响所有肿瘤成分的活性和交流,介导它们从抗肿瘤表型到原癌基因表型的重新编程,反之亦然。肿瘤微环境中可变数量的O发挥了这种二分作用的重要作用,这决定了ROS / RNS对癌变的影响的最终结果。此外,ROS / RNS水平显着影响癌症对治疗的反应。 ROS / RNS信号在实体瘤中的相关性可通过用靶向ROS / RNS作用和产生的化合物(例如酪氨酸激酶抑制剂和单克隆抗体)对实体瘤进行新型靶向治疗来证明,这些化合物可能会导致氧化还原的复杂性癌症中的调节。潜在地,ROS / RNS通过对氧化和亚硝基化的不同影响在肿瘤发生的不同阶段的双重作用也可能允许开发定制的诊断和治疗方法。

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