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G对环丁烷二聚体中5-甲基胞嘧啶脱氨作用的加速及其对紫外线诱导的C到T突变热点的影响。

Acceleration of 5-methylcytosine deamination in cyclobutane dimers by G and its implications for UV-induced C-to-T mutation hotspots.

作者信息

Cannistraro Vincent J, Taylor John-Stephen

机构信息

Department of Chemistry, Washington University, St Louis, MO 63130, USA.

出版信息

J Mol Biol. 2009 Oct 9;392(5):1145-57. doi: 10.1016/j.jmb.2009.07.048. Epub 2009 Jul 22.

Abstract

Sunlight-induced C-->T mutation hotspots occur most frequently at methylated CpG sites in tumor suppressor genes and are thought to arise from translesion synthesis past deaminated cyclobutane pyrimidine dimers (CPDs). While it is known that methylation enhances CPD formation in sunlight, little is known about the effect of methylation and sequence context on the deamination of 5-methylcytosine ((m)C) and its contribution to mutagenesis at these hotspots. Using an enzymatic method, we have determined the yields and deamination rates of C and (m)C in CPDs and find that the frequency of UVB-induced CPDs correlates with the oxidation potential of the flanking bases. We also found that the deamination of T(m)C and (m)CT CPDs is about 25-fold faster when flanked by G's than by A's, C's or T's in duplex DNA and appears to involve catalysis by the O6 group of guanine. In contrast, the first deamination of either C or (m)C in AC(m)CG with a flanking G was much slower (t(1/2) >250 h) and rate limiting, while the second deamination was much faster. The observation that C(m)CG dimers deaminate very slowly but at the same time correlate with C-->T mutation hotspots suggests that their repair must be slow enough to allow sufficient time for deamination. There are, however, a greater number of single C-->T mutations than CC-->TT mutations at C(m)CG sites even though the second deamination is very fast, which could reflect faster repair of doubly deaminated dimers.

摘要

阳光诱导的C→T突变热点最常出现在肿瘤抑制基因的甲基化CpG位点,被认为是由跨损伤合成绕过脱氨基的环丁烷嘧啶二聚体(CPD)产生的。虽然已知甲基化会增强阳光中CPD的形成,但关于甲基化和序列背景对5-甲基胞嘧啶((m)C)脱氨基的影响及其对这些热点处诱变的贡献知之甚少。我们采用酶法测定了CPD中C和(m)C的产量及脱氨基速率,发现UVB诱导的CPD频率与侧翼碱基的氧化电位相关。我们还发现,在双链DNA中,当T(m)C和(m)CT CPD侧翼为G时,其脱氨基速度比侧翼为A、C或T时快约25倍,且似乎涉及鸟嘌呤O6基团的催化作用。相比之下,侧翼为G的AC(m)CG中C或(m)C的首次脱氨基要慢得多(t1/2>250小时)且是限速的,而第二次脱氨基则快得多。C(m)CG二聚体脱氨基非常缓慢但同时与C→T突变热点相关这一观察结果表明,其修复速度必须足够慢,以便有足够时间进行脱氨基。然而,在C(m)CG位点,单C→T突变的数量比CC→TT突变多,尽管第二次脱氨基非常快,这可能反映了双脱氨基二聚体的修复速度更快。

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