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首页> 外文期刊>Antioxidants and redox signalling >Emerging roles of the nucleolus in regulating the DNA damage response: The noncanonical DNA repair enzyme APE1/Ref-1 as a paradigmatical example
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Emerging roles of the nucleolus in regulating the DNA damage response: The noncanonical DNA repair enzyme APE1/Ref-1 as a paradigmatical example

机译:核仁在调节DNA损伤反应中的新兴作用:以非典型DNA修复酶APE1 / Ref-1为例

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摘要

Significance: An emerging concept in DNA repair mechanisms is the evidence that some key enzymes, besides their role in the maintenance of genome stability, display also unexpected noncanonical functions associated with RNA metabolism in specific subcellular districts (e.g., nucleoli). During the evolution of these key enzymes, the acquisition of unfolded domains significantly amplified the possibility to interact with different partners and substrates, possibly explaining their phylogenetic gain of functions. Recent Advances: After nucleolar stress or DNA damage, many DNA repair proteins can freely relocalize from nucleoli to the nucleoplasm. This process may represent a surveillance mechanism to monitor the synthesis and correct assembly of ribosomal units affecting cell cycle progression or inducing p53-mediated apoptosis or senescence. Critical Issues: A paradigm for this kind of regulation is represented by some enzymes of the DNA base excision repair (BER) pathway, such as apurinic/apyrimidinic endonuclease 1 (APE1). In this review, the role of the nucleolus and the noncanonical functions of the APE1 protein are discussed in light of their possible implications in human pathologies. Future Directions: A productive cross-talk between DNA repair enzymes and proteins involved in RNA metabolism seems reasonable as the nucleolus is emerging as a dynamic functional hub that coordinates cell growth arrest and DNA repair mechanisms. These findings will drive further analyses on other BER proteins and might imply that nucleic acid processing enzymes are more versatile than originally thought having evolved DNA-targeted functions after a previous life in the early RNA world.
机译:意义:DNA修复机制中的一个新兴概念是证据表明,某些关键酶除了在维持基因组稳定性方面发挥作用外,还显示出与特定亚细胞区域(例如核仁)RNA代谢相关的意外非规范功能。在这些关键酶的进化过程中,未折叠结构域的获得显着放大了与不同配偶体和底物相互作用的可能性,这可能解释了它们的系统发育功能。最新进展:在核仁应力或DNA损伤后,许多DNA修复蛋白可以从核仁自由地重新定位到核质。这个过程可能代表一种监视机制,以监测影响细胞周期进程或诱导p53介导的细胞凋亡或衰老的核糖体单位的合成和正确装配。关键问题:这种调控的范例以DNA碱基切除修复(BER)途径的某些酶为代表,例如嘌呤/嘧啶内切核酸酶1(APE1)。在这篇综述中,鉴于核仁的作用和APE1蛋白的非规范功能,将对它们在人类病理学中的潜在影响进行讨论。未来方向:DNA修复酶与参与RNA代谢的蛋白质之间产生有效的相互作用似乎是合理的,因为核仁逐渐成为协调细胞生长停滞和DNA修复机制的动态功能枢纽。这些发现将推动对其他BER蛋白的进一步分析,并可能暗示核酸加工酶的功能比最初认为的要早得多,因为在早期的RNA世界中,这些酶在进化出DNA靶向功能后,便开始发挥作用。

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