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古菌 NucS 内切核酸酶触发的 DNA 脱氨碱基修复的替代途径。

An alternative pathway for repair of deaminated bases in DNA triggered by archaeal NucS endonuclease.

机构信息

Marine Science & Technology Institute, Department of Environmental Science and Engineering, Yangzhou University, China; Guangling College, Yangzhou University, China.

Marine Science & Technology Institute, Department of Environmental Science and Engineering, Yangzhou University, China.

出版信息

DNA Repair (Amst). 2020 Jan;85:102734. doi: 10.1016/j.dnarep.2019.102734. Epub 2019 Oct 24.

Abstract

Recent studies show that NucS endonucleases participate in mismatch repair in several archaea and bacteria. However, the function of archaeal NucS endonucleases has not been completely clarified. Here, we describe a NucS endonuclease from the hyperthermophilic and radioresistant archaeon Thermococcus gammatolerans (Tga NucS) that can cleave uracil (U)- and hypoxanthine (I)-containing dsDNA at 80 °C. Biochemical evidence shows that the cleavage sites of the enzyme are at the second phosphodiester on the 5'- site of U or I, and at the third phosphodiester on the 5'-site of the opposite base of U or I, creating a double strand break with a 4-nt 5'-overhang.The ends of the cleaved product of Tga NucS are ligatable, possessing 5'-phosphate and 3'-hydroxyl termini, which can be utilized by DNA repair proteins or enzymes. Tga NucS displays a preference for U/G- and I/T-containing dsDNA over other pairs with U or I, suggesting that the enzyme is responsible for repair of U and I in DNA that arise from deamination. Biochemical characterization of cleaving U- and I-containing DNA by Tga NucS was also investigated. The DNA-binding results show that the enzyme exhibits a higher affinity for normal, U- and I-containing dsDNA than for normal, U- and I-containing ssDNA. Therefore, we present an alternative pathway for repair of deaminated bases in DNA triggered by archaeal NucS endonuclease in hyperthermophilic archaea.

摘要

最近的研究表明,NucS 内切核酸酶参与了几种古菌和细菌中的错配修复。然而,古菌 NucS 内切核酸酶的功能尚未完全阐明。在这里,我们描述了一种来自高温耐辐射古菌 Thermococcus gammatolerans 的 NucS 内切核酸酶(Tga NucS),它可以在 80°C 下切割含有尿嘧啶(U)和次黄嘌呤(I)的双链 DNA。生化证据表明,该酶的切割位点位于 U 或 I 的 5'-位的第二个磷酸二酯键,以及 U 或 I 的相反碱基的 5'-位的第三个磷酸二酯键,从而产生带有 4-nt 5'-突出的双链断裂。Tga NucS 切割产物的末端是可连接的,具有 5'-磷酸和 3'-羟基末端,可以被 DNA 修复蛋白或酶利用。Tga NucS 对含有 U/G-和 I/T 的双链 DNA 比对其他含有 U 或 I 的双链 DNA 具有偏好性,这表明该酶负责修复脱氨产生的 DNA 中的 U 和 I。我们还研究了 Tga NucS 对含有 U 和 I 的 DNA 的切割。DNA 结合结果表明,该酶对正常的 U-和 I-含有双链 DNA 的亲和力高于正常的 U-和 I-含有单链 DNA。因此,我们提出了一种由古菌 NucS 内切核酸酶在高温古菌中触发的 DNA 脱氨碱基修复的替代途径。

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