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Differential modes of DNA binding by mismatch uracil DNA glycosylase from Escherichia coli: implications for abasic lesion processing and enzyme communication in the base excision repair pathway

机译：大肠杆菌错配的尿嘧啶DNA糖基化酶与DNA结合的差异模式：对基础切除修复途径中的无基础性病变处理和酶通讯的影响

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Mismatch uracil DNA glycosylase (Mug) from Escherichia coli is an initiating enzyme in the base-excision repair pathway. As with other DNA glycosylases, the abasic product is potentially more harmful than the initial lesion. Since Mug is known to bind its product tightly, inhibiting enzyme turnover, understanding how Mug binds DNA is of significance when considering how Mug interacts with downstream enzymes in the base-excision repair pathway. We have demonstrated differential binding modes of Mug between its substrate and abasic DNA product using both band shift and fluorescence anisotropy assays. Mug binds its product cooperatively, and a stoichiometric analysis of DNA binding, catalytic activity and salt-dependence indicates that dimer formation is of functional significance in both catalytic activity and product binding. This is the first report of cooperativity in the uracil DNA glycosylase superfamily of enzymes, and forms the basis of product inhibition in Mug. It therefore provides a new perspective on abasic site protection and the findings are discussed in the context of downstream lesion processing and enzyme communication in the base excision repair pathway.

机译：大肠杆菌的错配尿嘧啶DNA糖基化酶（Mug）是碱基切除修复途径中的起始酶。与其他DNA糖基化酶一样，无碱基产物可能比初始病变更具危害性。由于已知Mug会紧密结合其产品，抑制酶的转化，因此在考虑Mug如何与碱基切除修复途径中的下游酶相互作用时，了解Mug如何与DNA结合非常重要。我们已经使用带移和荧光各向异性测定法证明了Mug的底物和无碱基DNA产物之间的差异结合模式。马克杯可协同结合其产物，对DNA结合，催化活性和盐依赖性的化学计量分析表明，二聚体的形成对催化活性和产物结合均具有功能性意义。这是关于尿嘧啶DNA糖基化酶超家族中协同作用的首次报道，并形成了Mug中产物抑制的基础。因此，它提供了关于无碱基位点保护的新观点，并且在基础切除修复途径的下游病灶处理和酶交流中讨论了这些发现。

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期刊名称 Nucleic Acids Research
作者
Seden Grippon; Qiyuan Zhao; Tom Robinson; Jacqueline J. T. Marshall; Rory J. O’Neill; Hugh Manning; Gordon Kennedy; Christopher Dunsby; Mark Neil; Stephen E. Halford; Paul M. W. French; Geoff S. Baldwin;
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年(卷),期 2011(39),7
年度 2011
页码 2593–2603
总页数 11
原文格式 PDF
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中图分类分子生物学;
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专利

1. Differential modes of DNA binding by mismatch uracil DNA glycosylase from Escherichia coli: implications for abasic lesion processing and enzyme communication in the base excision repair pathway [J] . Grippon Seden, Zhao Qiyuan, Robinson Tom, Nucleic Acids Research . 2011,第7期

机译：大肠杆菌错配的尿嘧啶DNA糖基化酶与DNA结合的差异模式：对基础切除修复途径中的无基础病变加工和酶沟通的影响
2. Differential modes of DNA binding by mismatch uracil DNA glycosylase from Escherichia coli: implications for abasic lesion processing and enzyme communication in the base excision repair pathway [J] . Christopher Dunsby, Geoff S. Baldwin, Gordon Kennedy, Nucleic acids research . 2011,第7期

机译：大肠杆菌错配的尿嘧啶DNA糖基化酶与DNA结合的差异模式：对基础切除修复途径中无基础性病变处理和酶沟通的影响
3. Escherichia coli double-strand uracil-DNA glycosylase: involvement in uracil-mediated DNA base excision repair and stimulation of activity by endonuclease IV. [J] . Sung JS, Mosbaugh DW Biochemistry . 2000,第33期

机译：大肠杆菌双链尿嘧啶-DNA糖基化酶：参与尿嘧啶介导的DNA碱基切除修复和核酸内切酶IV刺激活性。
4. The Effect of Hydration on the Radiation Induction of DNA Base Lesions Processed by Base Excision Repair Enzymes [C] . Akinari Yokoya, Siobhan Cunniffe, Peter ONeill Workshop on Recognition of DNA Damage as Onset of Successful Repair: Computational and Experimental Approaches, Dec 18-19, 2001, Tokai . 2001

机译：水合对碱基切除修复酶处理的DNA碱基损伤辐射诱导的影响
5. Synthesis of fluorinated analogs of oxidative DNA lesions and their use to probe features of recognition and repair by base excision repair glycosylases. [D] . Cao, Sheng. 2010

机译：氧化性DNA损伤的氟化类似物的合成及其在探测碱基切除修复糖基化酶识别和修复特征中的用途。
6. Effects of mutations at tyrosine 66 and asparagine 123 in the active site pocket of Escherichia coli uracil DNA glycosylase on uracil excision from synthetic DNA oligomers: evidence for the occurrence of long-range interactions between the enzyme and substrate [O] . Priya Handa, Narottam Acharya, Umesh Varshney 2002

机译：大肠杆菌尿嘧啶DNA糖基化酶活性位点口袋中酪氨酸66和天冬酰胺123突变对合成DNA低聚物尿嘧啶切除的影响：该酶与底物之间发生长距离相互作用的证据
7. Differential modes of DNA binding by mismatch uracil DNA glycosylase from Escherichia coli: implications for abasic lesion processing and enzyme communication in the base excision repair pathway [O] . Grippon, Seden, Zhao, Qiyuan, Robinson, Tom, 2010

机译：大肠杆菌错配的尿嘧啶DNA糖基化酶与DNA结合的差异模式：对基础切除修复途径中无基础性病变处理和酶沟通的影响
8. DNA Base Excision Repair (BER) and Cancer Gene Therapy: Use of the Human N-mythlpurien DNA Glycosylase (MPG) to Sensitize Breast Cancer Cells to Low Dose Chemotherapy [R] . Harvey, T. , Kelly, M. R. 2003

机译：DNa碱基切除修复（BER）和癌症基因治疗：使用人类N-mythlpurien DNa糖基化酶（mpG）使乳腺癌细胞对低剂量化疗敏感

Differential modes of DNA binding by mismatch uracil DNA glycosylase from Escherichia coli: implications for abasic lesion processing and enzyme communication in the base excision repair pathway

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