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DNA中无碱基损伤对面的核苷酸插入动力学。

Nucleotide insertion kinetics opposite abasic lesions in DNA.

作者信息

Randall S K, Eritja R, Kaplan B E, Petruska J, Goodman M F

出版信息

J Biol Chem. 1987 May 15;262(14):6864-70.

PMID:3571289
Abstract

A gel assay is introduced to measure DNA polymerase insertion kinetics at single sites along a DNA template strand. The assay is used to analyze the kinetics of inserting deoxynucleotides opposite a synthetic abasic (apurinic/apyrimidinic) lesions using Drosophila DNA polymerase alpha. The location of the abasic lesion next to different nearest-neighbor bases allows the effects of base stacking on the specificity of insertion to be evaluated. The specificity of nucleotide insertion, Vmax/Km, is 6-11 times greater for A over G and about 20-50 times greater for A over C and T. The insertion specificity at the abasic lesion appears to depend more on differences in Vmax than Km. Apparent Michaelis constants for inserting A and G deoxynucleotides are similar to within about a factor of 2. The insertion of A or G occurs most efficiently at the abasic lesion when T is the 5'-nearest neighbor on the primer strand and least efficiently when G is the 5'-nearest neighbor. The presence of different base stacking partners adjacent to the site of insertion has up to a 4-fold effect on specificity.

摘要

引入了一种凝胶测定法来测量DNA聚合酶沿着DNA模板链在单个位点的插入动力学。该测定法用于分析使用果蝇DNA聚合酶α在与合成无碱基(脱嘌呤/脱嘧啶)损伤相对的位置插入脱氧核苷酸的动力学。无碱基损伤在不同最近邻碱基旁边的位置使得能够评估碱基堆积对插入特异性的影响。核苷酸插入的特异性,即Vmax/Km,对于A相对于G而言高6-11倍,对于A相对于C和T而言高约20-50倍。在无碱基损伤处的插入特异性似乎更多地取决于Vmax的差异而非Km。插入A和G脱氧核苷酸的表观米氏常数在约2倍的范围内相似。当T是引物链上5'-最近邻碱基时,A或G在无碱基损伤处的插入最有效,而当G是5'-最近邻碱基时效率最低。插入位点相邻的不同碱基堆积伙伴的存在对特异性有高达4倍的影响。

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