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首页> 外文期刊>Biochemistry >Translesional synthesis past acetylaminofluorene-derived DNA adducts catalyzed by human DNA polymerase kappa and Escherichia coli DNA polymerase IV
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Translesional synthesis past acetylaminofluorene-derived DNA adducts catalyzed by human DNA polymerase kappa and Escherichia coli DNA polymerase IV

机译:经人类DNA聚合酶kappa和大肠杆菌DNA聚合酶IV催化的乙酰氨基芴衍生的DNA加合物的跨病变合成

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Human DNA polymerase kappa (pol kappa) has a sequence significantly homologous with that of Escherichia coli DNA polymerase IV (pol IV). We used a truncated form of human pol kappa (pol kappa DeltaC) and full-length pol IV to explore the miscoding properties of these enzymes. Oligodeoxynucleotides, modified site-specifically with N-(deoxyguanosin-8-yl)-2-acetylaminofluorene (dG-AAF) and N-(deoxyguanosin-8-yl)-2-aminofluorene (dG-AF), were used as DNA templates in primer extension reactions that included all four dNTPs. Reactions catalyzed by pol kappa DeltaC were partially blocked one base prior to dG-AAF or dG-AF, and also opposite both lesions. At higher enzyme concentrations, a significant fraction of primer was extended. Analysis of the fully extended reaction product revealed incorporation of dTMP opposite dG-AAF, accompanied by much smaller amounts of dCMP, dAMP, and dGMP and some one- and two-base deletions. The product terminating 3' to the adduct site contained AMP misincorporated opposite dC. On templates containing dG-AF dAMP, dTMP, and dCMP were incorporated opposite the lesion in approximately equal amounts, together with some one-base and two-base deletions. Steady-state kinetics analysis confirmed the results obtained from primer extension reactions catalyzed by pol kappa. In contract, primer extension reactions catalyzed by pol IV were blocked effectively by dG-AAF and dG-AF. At high concentrations of pol IV, full-length products were formed containing primarily one- or two-base deletions with dCMP, the correct base, incorporated opposite dG-AF. The miscoding properties of pol kappa observed in this study are consistent with mutational spectra observed when plasmid vectors containing dG-AAF or dG-AF are introduced into simian kidney cells [Shibutani, S., et al. (2001) Biochemistry 40, 3717-3722], supporting a model in which pol kappa plays a role in translesion synthesis past acetylaminofluorene-derived lesions in mammalian cells.
机译:人DNA聚合酶κ(pol kappa)具有与大肠杆菌DNA聚合酶IV(pol IV)明显同源的序列。我们使用人类pol kappa(pol kappa DeltaC)和全长pol IV的截短形式来探索这些酶的错误编码特性。用N-(脱氧鸟苷-8-基)-2-乙酰氨基芴(dG-AAF)和N-(脱氧鸟苷-8-基)-2-氨基芴(dG-AF)进行位点特异性修饰的寡脱氧核苷酸用作DNA模板在引物延伸反应中包括所有四个dNTP。由pol Kappa DeltaC催化的反应在dG-AAF或dG-AF之前的一个碱基处被部分阻断,并且在两个病变的对面。在较高的酶浓度下,引物的很大一部分被延长。对完全扩展的反应产物的分析表明,与dG-AAF相对的是dTMP的掺入,伴随着少量的dCMP,dAMP和dGMP以及一些一碱基和两碱基的缺失。终止于加合物位点3'的产物含有与dC相对并入的AMP。在含有dG-AF dAMP,dTMP和dCMP的模板上,病灶对面以大约相等的量掺入,并带有一些一碱基和两碱基的缺失。稳态动力学分析证实了由pol kappa催化的引物延伸反应获得的结果。合同中,pol IV催化的引物延伸反应被dG-AAF和dG-AF有效阻断。在高浓度pol IV下,形成的全长产物主要含有一碱基或两碱基的缺失,其中dCMP是正确的碱基,与dG-AF相对并入。在这项研究中观察到的pol kappa的误编码特性与将含有dG-AAF或dG-AF的质粒载体引入猿猴肾细胞时观察到的突变光谱一致[Shibutani,S.,et al。 (2001)Biochemistry 40,3717-3722],支持了其中pol kappa在通过乙酰氨基芴衍生的哺乳动物细胞中的病灶转移合成中起作用的模型。

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