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在肠道噬菌体DNA基因组中对甲基化位点的选择。

Selection against dam methylation sites in the genomes of DNA of enterobacteriophages.

作者信息

McClelland M

出版信息

J Mol Evol. 1984;21(4):317-22. doi: 10.1007/BF02115649.

Abstract

Postreplicative methylation of adenine in Escherichia coli DNA to produce G6m ATC (where 6mA is 6-methyladenine) has been associated with preferential daughter-strand repair and possibly regulation of replication. An analysis was undertaken to determine if these, or other, as yet unknown roles of GATC, have had an effect on the frequency of GATC in E. coli or bacteriophage DNA. It was first ascertained that the most accurate predictions of GATC frequency were based on the observed frequencies of GAT and ATC, which would be expected since these predictors take into account preferences in codon usage. The predicted frequencies were compared with observed GATC frequencies in all available bacterial and phage nucleotide sequences. The frequency of GATC was close to the predicted frequency in most genes of E. coli and its RNA bacteriophages and in the genes of nonenteric bacteria and their bacteriophages. However, for DNA enterobacteriophages the observed frequency of GATC was generally significantly lower than predicted when assessed by the chi square test. No elevation in the rate of mutation of 6mA in GATC relative to other bases was found when pairs of DNA sequences from closely related phages or pairs of homologous genes from enterobacteria were compared, nor was any preferred pathway for mutation of 6mA evident in the E. coli DNA bacteriophages. This situation contrasts with that of 5-methylcytosine, which is hypermutable, with a preferred pathway to thymine. Thus, the low level of GATC in enterobacteriophages is probably due not to 6mA hypermutability, but no selection against GATC in order to bypass a GATC-mediated host function.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

大肠杆菌DNA中腺嘌呤的复制后甲基化产生G6m ATC(其中6mA是6-甲基腺嘌呤)与优先的子链修复以及可能的复制调控有关。开展了一项分析以确定GATC的这些或其他未知作用是否对大肠杆菌或噬菌体DNA中GATC的频率产生了影响。首先确定,对GATC频率最准确的预测是基于观察到的GAT和ATC频率,鉴于这些预测因子考虑了密码子使用偏好,这是可以预期的。将预测频率与所有可用的细菌和噬菌体核苷酸序列中观察到的GATC频率进行了比较。在大肠杆菌及其RNA噬菌体的大多数基因以及非肠道细菌及其噬菌体的基因中,GATC的频率接近预测频率。然而,对于DNA肠道噬菌体,通过卡方检验评估时,观察到的GATC频率通常显著低于预测值。当比较来自密切相关噬菌体的DNA序列对或来自肠道细菌的同源基因对时,未发现GATC中6mA相对于其他碱基的突变率升高,在大肠杆菌DNA噬菌体中也没有明显的6mA突变偏好途径。这种情况与5-甲基胞嘧啶形成对比,5-甲基胞嘧啶具有高突变性,有一条向胸腺嘧啶的偏好突变途径。因此,肠道噬菌体中GATC水平低可能不是由于6mA的高突变性,而是没有针对GATC的选择以绕过GATC介导的宿主功能。(摘要截短于250字)

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