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Nitric oxide: Protein tyrosine phosphorylation and protein S-nitrosylation in cancer

机译:一氧化氮:蛋白酪氨酸磷酸化和癌症中的蛋白质S-亚硝基化

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Cancer is a worldwide health problem leading to a high incidence of morbidity and mortality. Malignant transformation can occur by expression of oncogenes, over-expression and deregulated activation of proto-oncogenes, and inactivation of tumor suppressor genes. These cellular actions occur through stimulation of oncogenic signaling pathways. Nitric oxide (NO) can induce genetic changes in cells and its intracellular generation can lead to tumor formation and progression. It can also promote anti-tumor activities. The pro- and anti-tumor activities of NO are dependent on its intracellular concentration, cell compartmentalization, and cell sensitivity. NO affects a number of oncogenic signaling pathways. This review focuses on two oncogenic signaling pathways: NO-EGFR-Src-FAK and NO-Ras-EGFR-ERK1/2 MAP kinases. In these pathways, low to intermediate concentrations of NO/S-nitrosothiols (RSNOs) stimulate oncogenic signaling, while high concentrations of NO/RSNO stimulate anti-oncogenic signaling. Increasing knowledge on pro- and anti-tumorigenic activities of NO and related reactive species such as RSNOs has fostered the research and synthesis of novel NO-based chemotherapeutic agents. RSNOs, effective as NO donors and trans-nitrosylating agents under appropriate conditions, may operate as potential chemotherapeutic agents.
机译:癌症是一个全球健康问题,导致发病率和死亡率的高发病率。通过表达癌细胞,过度表达和造成的原型癌基因的激活和肿瘤抑制基因的失活来发生恶性转化。这些细胞作用通过刺激致癌信号通路而发生。一氧化氮(NO)可以诱导细胞的遗传变化,其细胞内一代可导致肿瘤形成和进展。它还可以促进抗肿瘤活动。 NO的亲和抗肿瘤活性依赖于其细胞内浓度,细胞分区化和细胞敏感性。不影响许多致癌信号通路。本综述侧重于两个致癌信号通路:NO-EGFR-SRC-FAK和NO-RAS-EGFR-ERK1 / 2 MAP激酶。在这些途径中,低至中间浓度的NO / S-亚硝基硫醇(RSNO)刺激致癌信号传导,而高浓度的NO / RSNO刺激抗致癌信号传导。越来越多的关于NO和抗致致致致致瘤活动的知识和相关的反应性物种,如RSNOS,促进了新型无碱化学治疗剂的研究和合成。在适当条件下没有任何供体和反式亚硝基化试剂有效,可以作为潜在的化学治疗剂。

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