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HypoxamiRs and cancer: From biology to targeted therapy

机译:低氧血症和癌症:从生物学到靶向治疗

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Significance: Hypoxia is a hallmark of the tumor microenvironment and represents a major source of failure in cancer therapy. Recent Advances: Recent work has generated extensive evidence that microRNAs (miRNAs) are significant components of the adaptive response to low oxygen in tumors. Induction of specific miRNAs, collectively termed hypoxamiRs, has become an accepted feature of the hypoxic response in normal and transformed cells. Critical Issues: Overexpression of miR-210, the prototypical hypoxamiR, is detected in most solid tumors, and it has been linked to adverse prognosis in many tumor types. Several miR-210 target genes, including iron-sulfur (Fe-S) cluster scaffold protein (ISCU) and glycerol-3-phosphate dehydrogenase 1-like (GPD1L), have been correlated with prognosis in an inverse fashion to miR-210, suggesting that their down- regulation by miR-210 occurs in vivo and contributes to tumor growth. Additional miRNAs are modulated by decreased oxygen tension in a more tissue-specific fashion, adding another level of complexity over the classic hypoxia-regulated gene network. Future Directions: From a biological standpoint, hypoxamiRs are emerging modifiers of cancer cell response to the adaptive challenges of the microenvironment. From a clinical perspective, assessing the status of these miRNAs may contribute to a detailed understanding of hypoxia-induced mechanisms of resistance and/or to the fine-tuning of future hypoxia-modifying therapies. Antioxid. Redox Signal. 21, 1220-1238.
机译:意义:缺氧是肿瘤微环境的标志,是癌症治疗失败的主要原因。最新进展:最近的工作已产生大量证据,证明microRNA(miRNA)是肿瘤对低氧的适应性反应的重要组成部分。特定的miRNA的诱导(统称为hypoxamiRs)已成为正常细胞和转化细胞中低氧反应的公认特征。关键问题:在大多数实体瘤中都检测到miR-210(典型的hypoxamiR)过表达,并且与许多肿瘤类型的不良预后有关。 miR-210的几个靶基因,包括铁硫(Fe-S)簇状支架蛋白(ISCU)和3-磷酸甘油脱氢酶1样(GPD1L),与miR-210的预后呈负相关,提示它们在体内发生miR-210的下调并有助于肿瘤生长。通过降低的氧气张力以更多的组织特异性方式来调节其他miRNA,从而在经典的缺氧调节基因网络上增加了另一层次的复杂性。未来方向:从生物学的角度来看,hypoxamiRs是癌细胞对微环境适应性挑战的新兴调节剂。从临床角度来看,评估这些miRNA的状态可能有助于对缺氧诱导的耐药机制的详细了解和/或对未来缺氧修饰疗法的微调。抗氧化。氧化还原信号。 21,1220-1238。

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