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Redox molecular machines involved in tumor progression

机译:参与肿瘤进展的氧化还原分子机器

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摘要

Significance: We herein review recent advances on the role exerted by protein redox machines engaged in tumor progression, focusing on cell adhesion and migration, regulation of transcriptional response, and tumor metabolic reprogramming, all features belonging to the new hallmarks of cancer. Recent Advances: Several recent insights have reported that oxidative stress, either due to intracellular sources of oxidants, which are frequently deregulated in cancers or to microenvironment factors as hypoxia or stromal cell contact, plays a key role in tumor malignancy, as well as in metabolic pathways control. Indeed, many proteins behave as sensors of intracellular oxidative stress, including protein tyrosine kinases and phosphatases, transcription factors as p53, forkhead box class-Os, nuclear respiratory factor-2, nuclear factor-kB, hypoxia inducible factor, enzymes involved in glycolysis or penthose phosphate pathway as pyruvate kinase-M2 and adenylate monophosphate kinase, or DNA repair enzymes as Ataxia Teleangectasia Mutated. All these proteins have been reported to play essential roles during cancer progression and their sensitivity to oxidative stress has added new levels of complexity to the cancer field. Critical Issues: Main significant issues that need to be addressed in redox cancer biology are (i) sensitivity to a different level of oxidative stress of sensors, that is, they can respond to different oxidative insults/signals, and (ii) the real susceptibility of cancer cells to redox-based therapies due to the acknowledged plasticity of cancer cells to develop adoptive strategies. Future Directions: Definitely, redox machines have the potentiality to develop into novel biomarkers and related target therapies should attain the goal of personalized medicine in the fight against cancer. Antioxid. Redox Signal. 19, 1828-1845.
机译:启示:我们在本文中综述了蛋白质氧化还原机器在肿瘤进展中所发挥的作用的最新进展,这些研究集中于细胞粘附和迁移,转录反应的调控以及肿瘤代谢的重新编程,所有这些特征都属于癌症的新标志。最新进展:近期的一些见解报道了氧化应激,可能是由于细胞内氧化剂的来源(通常在癌症中失控),还是由于微环境因素(如缺氧或基质细胞接触)在肿瘤恶性肿瘤以及代谢中起着关键作用。途径控制。实际上,许多蛋白质可作为细胞内氧化应激的传感器,包括蛋白质酪氨酸激酶和磷酸酶,转录因子p53,叉头盒Os,核呼吸因子2,核因子kB,缺氧诱导因子,糖酵解或磷酸戊糖途径为丙酮酸激酶-M2和腺苷酸单磷酸激酶,或DNA修复酶为失语共济失调突变。据报道,所有这些蛋白质在癌症进展过程中起着至关重要的作用,它们对氧化应激的敏感性为癌症领域增加了新的复杂度。关键问题:氧化还原癌症生物学中需要解决的主要重要问题是(i)对传感器不同水平的氧化应激的敏感性,即它们可以对不同的氧化损伤/信号做出反应,以及(ii)实际易感性由于公认的癌细胞可塑性来开发过继策略,因此将癌细胞用于基于氧化还原的疗法。未来方向:无疑,氧化还原机器具有发展成为新型生物标志物的潜力,相关的靶标治疗应达到抗癌的个性化医学目标。抗氧化。氧化还原信号。 19,1828-1845。

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