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Autophagy: In the cROSshairs of cancer

机译:自噬:在癌症的十字准线

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Two prominent features of tumors that contribute to oncogenic survival signaling are redox disruption, or oxidative stress phenotype, and high autophagy signaling, making both phenomena ideal therapeutic targets. However, the relationship between redox disruption and autophagy signaling is not well characterized and the clinical impact of reactive oxygen species (ROS)-generating chemotherapeutics on autophagy merits immediate attention as autophagy largely contributes to chemotherapeutic resistance. In this commentary we focus on melanoma, using it as an example to provide clarity to current literature regarding the roles of autophagy and redox signaling which can be applicable to initiation and maintenance of most tumor types. Further, we address the crosstalk between ROS and autophagy signaling during pharmacological intervention and cell fate decisions. We attempt to elucidate the role of autophagy in regulating cell fate following treatment with ROS-generating agents in preclinical and clinical settings and discuss the emerging role of autophagy in cell fate decisions and as a cell death mechanism. We also address technical aspects of redox and autophagy evaluation in experimental design and data interpretation. Lastly, we present a provocative view of the clinical relevance, emerging challenges in dual targeting of redox and autophagy pathways for therapy, and the future directions to be addressed in order to advance both basic and translational aspects of this field. (C) 2016 Elsevier Inc. All rights reserved.
机译:有助于致癌生存信令的肿瘤的两个突出特征是氧化还原的破坏,或氧化应激表型,以及高自噬信号传导,使得这两种理想的治疗靶标。然而,氧化还原破坏和自噬信号传导之间的关系并不具备很好的表征,并且反应性氧物种(ROS)的临床影响是在自噬上的自噬上的自噬上的临床影响在很大程度上有助于化学治疗抗性。在此评论中,我们专注于黑色素瘤,用它作为一个例子,以便为当前文献提供关于自噬和氧化还原信号传导的作用的目前文献,这可以适用于大多数肿瘤类型的起始和维持。此外,在药理学干预和细胞命运决策期间,我们在ROS与自噬信号之间的串扰地址。我们试图阐明自噬在临床前和临床环境中用ROS发电剂治疗后调节细胞命运的作用,并讨论自噬在细胞命运决策中的新兴作用以及细胞死亡机制。我们还解决了实验设计和数据解释中的氧化还原和自噬评估的技术方面。最后,我们展示了临床相关性的挑衅性观点,产生了氧化还原和自噬途径的临床相关性,以及治疗的自噬途径,以及要解决的未来方向,以提高该领域的基本和翻译方面。 (c)2016年Elsevier Inc.保留所有权利。

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